Your search keyword '"BIOLOGICAL models"' showing total 14,147 results

1. Synergistic Inhibitory Effect of Gliquidone Against Cisplatin‐Resistant Human Lung Adenocarcinoma.

Author

Qiu, Xi, Liu, Bo, Ye, Pan-Pan, Song, Lin-Lin, Zhang, Xue, Gu, Wei-Ping, Li, Ling, Zhu, Shun-Wei, Zhao, Wei, Yang, Xin-Mei, and Silvestre, Samuel

Subjects

*THERAPEUTIC use of antineoplastic agents, *ADENOCARCINOMA, *BIOLOGICAL models, *CISPLATIN, *DRUG resistance in cancer cells, *RESEARCH funding, *CELL proliferation, *SULFONYLUREAS, *STRUCTURAL equation modeling, *CELL lines, *MICE, *DRUG repositioning, *DRUG efficacy, *ANIMAL experimentation, *LUNG cancer, *TRANSFERASES, *TREATMENT failure, *DRUG synergism

Abstract

Cisplatin (CDDP) can combat various types of cancers, employing a multifaceted approach against these malignant diseases. Despite its efficacy, resistance to CDDP remains a significant clinical challenge, often resulting in treatment failure and disease progression. Currently, efforts are underway to unravel the mechanisms of CDDP drug resistance in cancer treatment. The elevated presence of glutathione S‐transferase pi‐1 (GSTP1‐1) within tumor cells plays a pivotal role in the development of resistance toward the effects of CDDP. GSTP1‐1 contributes to detoxification by conjugating glutathione (GSH) to CDDP, reducing its accumulation and effectiveness in the tumor cells. In this study, the efficacy of gliquidone, an antidiabetic drug, demonstrated its capacity to impede tumor cell proliferation in both lung cancer A549 cell lines and A549/CDDP cell lines. This was achieved by suppressing the expression of GSTP1‐1 within tumor cells (IC50: 16.8 ± 0.8 μM). Furthermore, through the establishment of a nude mouse model featuring lung adenocarcinoma A549/CDDP cell transplantation tumors, gliquidone demonstrated a significant therapeutic effect on the mice tumors, while avoiding discernible side effects. These findings suggest that gliquidone could potentially be repurposed as an adjunct therapy in CDDP‐resistant lung cancer. [ABSTRACT FROM AUTHOR]

Published

2024

2. Regulatory T cells require peripheral CCL2-CCR2 signaling to facilitate the resolution of medication overuse headache-related behavioral sensitization.

Author

Ryu, Sun, Zhang, Jintao, Simoes, Roli, Liu, Xuemei, Guo, Zhaohua, Feng, Li, Unsinger, Jacqueline, Hotchkiss, Richard S., and Cao, Yu-Qing

Subjects

*CHEMOKINES, *SUBSTANCE abuse, *BIOLOGICAL models, *FLOW cytometry, *SUMATRIPTAN, *RESEARCH funding, *CHRONIC pain, *HEADACHE, *CELL proliferation, *CELLULAR signal transduction, *INTERLEUKIN-2, *TREATMENT effectiveness, *MICE, *IMMUNOHISTOCHEMISTRY, *NEUROPEPTIDES, *ANIMAL experimentation, *ANIMAL behavior, *CHEMOKINE receptors, *REGULATORY T cells, *DISEASE complications

Abstract

Background: Medication overuse headache (MOH) is the most common secondary headache disorder, resulting from chronic and excessive use of medication to treat headaches, for example, sumatriptan. In a recent study, we have shown that the peripheral C-C motif ligand 2 (CCL2), C-C motif chemokine receptor 2 (CCR2) and calcitonin-gene-related peptide (CGRP) signaling pathways interact with each other and play critical roles in the development of chronic migraine-related behavioral and cellular sensitization. In the present study, we investigated whether CCL2-CCR2 and CGRP signaling pathways play a role in the development of sumatriptan overuse-induced sensitization, and whether they are involved in its resolution by the low-dose interleukin-2 (LD-IL-2) treatment. Methods: Mice received daily sumatriptan administration for 12 days. MOH-related behavioral sensitization was assessed by measuring changes of periorbital mechanical thresholds for 3 weeks. CCL2-CCR2 and CGRP signaling pathways were inhibited by targeted gene deletion or with an anti-CCL2 antibody. Ca2+-imaging was used to examine whether repetitive sumatriptan treatment enhances CGRP and pituitary adenylate cyclase–activating polypeptide (PACAP) signaling in trigeminal ganglion (TG) neurons. LD-IL-2 treatment was initiated after the establishment of sumatriptan-induced sensitization. Immunohistochemistry and flow cytometry analyses were used to examine whether CCL2-CCR2 signaling controls regulatory T (Treg) cell proliferation and/or trafficking. Results: CCL2, CCR2 and CGRPα global KO mice exhibited robust sumatriptan-induced behavioral sensitization comparable to wild-type controls. Antibody neutralization of peripheral CCL2 did not affect sumatriptan-induced behaviors either. Repeated sumatriptan administration did not enhance the strength of CGRP or PACAP signaling in TG neurons. Nevertheless, LD-IL-2 treatment, which facilitated the resolution of sumatriptan-induced sensitization in wild-type and CGRPα KO mice, was completely ineffective in mice with compromised CCL2-CCR2 signaling. In CCL2 KO mice, we observed normal LD-IL-2-induced Treg expansion in peripheral blood, but the increase of Treg cells in dura and TG tissues was significantly reduced in LD-IL-2-treated CCL2 KO mice relative to wild-type controls. Conclusions: These results indicate that the endogenous CCL2-CCR2 and CGRP signaling pathways are not involved in sumatriptan-induced behavioral sensitization, suggesting that distinct molecular mechanisms underlie chronic migraine and MOH. On the other hand, peripheral CCL2-CCR2 signaling is required for LD-IL-2 to reverse chronic headache-related sensitization. [ABSTRACT FROM AUTHOR]

Published

2024

3. Effect and mechanisms of shikonin on breast cancer cells in vitro and in vivo.

Author

Yu, Chuyi, Xing, Haoyu, Fu, Xiaguo, Zhang, Yingying, Yan, Xiufang, Feng, Jianjia, He, Zhouqin, Ru, Li, Huang, Chunlong, and Liang, Jianming

Subjects

CHINESE medicine, IN vitro studies, BIOLOGICAL models, FLOW cytometry, MITOCHONDRIA, RESEARCH funding, BREAST tumors, ANTINEOPLASTIC agents, HERBAL medicine, QUINONE, APOPTOSIS, CALCIUM-binding proteins, CELL proliferation, KRUSKAL-Wallis Test, TREATMENT effectiveness, IN vivo studies, DESCRIPTIVE statistics, IMMUNODIAGNOSIS, CELL lines, PLANT extracts, MICE, REACTIVE oxygen species, ANIMAL experimentation, ONE-way analysis of variance, CELL survival, DATA analysis software, CELL surface antigens, PHARMACODYNAMICS

Abstract

Background: Breast cancer seriously affects physical and mental health of women. Despite advances in the clinical use of different treatments, breast cancer remains a major cause of mortality. Therefore, it is imperative to identify promising treatment options. In the present study, we investigated the effects of shikonin on 4T1 breast cancer cells and its potential mechanisms of action. Methods: BALB/c-derived mouse breast cancer 4T1 is very close to human breast cancer in growth characteristics and systemic response, so 4T1 cells were selected for further experiments. Cell viability, apoptosis, intracellular reactive oxygen species (ROS), mitochondrial activity, and cellular calreticulin (CRT) exposure were assessed to evaluate the antitumor effects and mechanisms of shikonin in vitro. Orthotopic tumor growth inhibition and splenic immune cell regulation by shikonin were evaluated in 4T1 breast cancer orthotopic mice in vivo. Results: In vitro, shikonin could inhibit cell proliferation, cause apoptosis, disrupt mitochondrial activity, and induce ROS production and CRT exposure. In vivo, shikonin inhibited tumor growth, increased the proportion of CD8+ T cells, and reduced the proportion of regulatory cells (CD25+ Foxp3+ T cells) in the spleen. Conclusions: Shikonin inhibits the growth of 4T1 breast cancer cells by disrupting mitochondrial activity, promoting oxidative stress, and regulating immune function. [ABSTRACT FROM AUTHOR]

Published

2024

4. Ren-Shen-Bu-Qi decoction alleviates exercise fatigue through activating PI3K/AKT/Nrf2 pathway in mice.

Author

Chen, Yangyang, Gao, Tinghui, Bai, Jing, Zhang, Wenjing, Zhou, Yutong, Zhao, Ruichang, Deng, Youhui, Liu, Xiaogang, Huang, Zhangjun, Wang, Songtao, Shen, Caihong, Liu, Sijing, and Guo, Jinlin

Subjects

*PROTEIN analysis, *PREVENTION of weight loss, *LIVER disease prevention, *KIDNEY disease prevention, *BLOOD sugar analysis, *CHINESE medicine, *BIOLOGICAL models, *HIGH performance liquid chromatography, *COMPUTER-assisted molecular modeling, *SUPEROXIDE dismutase, *EXERCISE, *RESEARCH funding, *HERBAL medicine, *FATIGUE (Physiology), *PHARMACEUTICAL chemistry, *POLYMERASE chain reaction, *FLAVONOIDS, *ASPARTATE aminotransferase, *CELLULAR signal transduction, *CARBOXYLIC acids, *BLOOD urea nitrogen, *DESCRIPTIVE statistics, *LACTATE dehydrogenase, *MICE, *CREATINE kinase, *ANIMAL experimentation, *MASS spectrometry, *WESTERN immunoblotting, *SWIMMING, *ALANINE aminotransferase, *UREA, *TRANSFERASES, *STAINS & staining (Microscopy), *LIVER, *LACTIC acid, *GLYCOGEN, *GLUTATHIONE peroxidase, *TIME, *MALONDIALDEHYDE, *NUCLEAR factor E2 related factor

Abstract

Background: Fatigue is a prevalent issue that can lead individuals to a sub-health condition, impacting their work efficiency and quality of life. There are limited effective treatment options available for fatigue. Ren-Shen-Bu-Qi decoction (RSBQD) is a proprietary herbal remedy that is designed to address fatigue. However, the specific pharmacological mechanisms and basis of RSBQD are not yet fully understood. Purpose: This study aimed to investigate the pharmacological effects and mechanisms of RSBQD in a mouse model of exercise fatigue. Materials and methods: UPLC-Q-Orbitrap HRMS was used to analyze the chemical composition of RSBQD. The pharmacological basis and molecular mechanism of RSBQD on exercise fatigue were predicted using network pharmacology analysis. Subsequently, an exercise fatigue mouse model was established and used to analysis the effects of RSBQD. The potential mechanisms were verified by hematoxylin–eosin (HE) staining, real-time fluorescence quantitative PCR (RT-qPCR), Western blot (WB) and molecular docking. Results: The results showed that 88 main components of RSBQD were identified, which have mainly belonged to flavonoids and carboxylic acid compounds. The network pharmacology analysis indicated that RSBQD ameliorate fatigue through PI3K/AKT signaling pathway. Notably, RSBQD prolonged the swimming time and diminished body weight loss of exercise fatigue mice (P < 0.05). Meanwhile, RSBQD significantly alleviated the injury of liver and kidney induced by exhaustive exercise, and decreasing the serum alanine aminotransferase (ALT), aspartate aminotransferase (AST), urea and BUN levels (P < 0.05). In addition, RSBQD was found could relieve exercise fatigue by decreasing the content of creatine kinase (CK), lactate dehydrogenase (LDH), and lactic acid (LA), but increasing the blood glucose (GLU) and liver glycogen (HG) levels (P < 0.05). RSBQD also significantly increased the hepatic superoxide dismutase (SOD), glutathione peroxidase (GSH-Px) but decreased hepatic malondialdehyde (MDA) levels. Moreover, RSBQD was able to upregulate protein level of activated Nrf2 and PI3K/AKT signaling pathways. Conclusions: RSBQD mitigates exercise fatigue by reversing metabolic changes and reducing oxidative damage through the PI3K/AKT/Nrf2 signaling pathway. This study offers pharmacological support for the utilization of RSBQD in exercise fatigue treatment. [ABSTRACT FROM AUTHOR]

Published

2024

5. TLR4-mediated chronic neuroinflammation has no effect on tangle pathology in a tauopathy mouse model.

Author

Basheer, Neha, Muhammadi, Muhammad Khalid, Freites, Carlos Leandro, Avila, Martin, Momand, Miraj Ud Din, Hryntsova, Natalia, Smolek, Tomas, Katina, Stanislav, and Zilka, Norbert

Subjects

BIOLOGICAL models, RESEARCH funding, INTRAPERITONEAL injections, PHOSPHORYLATION, ALZHEIMER'S disease, NEURONS, BRAIN, NEUROINFLAMMATION, TOLL-like receptors, FLUORESCENT antibody technique, DESCRIPTIVE statistics, CHRONIC diseases, NERVE tissue proteins, GENE expression, MICE, TAUOPATHIES, IMMUNOHISTOCHEMISTRY, ANIMAL experimentation, LIPOPOLYSACCHARIDES, COMPARATIVE studies, CELL receptors

Abstract

Introduction: Alzheimer's disease (AD) is marked by the accumulation of fibrillary aggregates composed of pathological tau protein. Although neuroinflammation is frequently observed in conjunction with tau pathology, current preclinical evidence does not sufficiently establish a direct causal role in tau tangle formation. This study aimed to evaluate whether chronic Toll-like receptor 4 (TLR4) stimulation, induced by a high dose of lipopolysaccharide (LPS, 5 mg/kg), exacerbates neurofibrillary tangle (NFT) pathology in a transgenic mouse model of tauopathy that expresses human truncated 151-391/3R tau, an early feature of sporadic AD. Methods: We utilized a transgenic mouse model of tauopathy subjected to chronic TLR4 stimulation via weekly intraperitoneal injections of LPS over nine consecutive weeks. Neurofibrillary tangle formation, microglial activation, and tau hyperphosphorylation in the brainstem and hippocampus were assessed through immunohistochemistry, immunofluorescence, and detailed morphometric analysis of microglia. Results: Chronic LPS treatment led to a significant increase in the number of Iba-1+ microglia in the LPS-treated group compared to the sham group (p < 0.0001). Notably, there was a 1.5- to 1.7-fold increase in microglia per tangle-bearing neuron in the LPS-treated group. These microglia exhibited a reactive yet exhausted phenotype, characterized by a significant reduction in cell area (p < 0.0001) without significant changes in other morphometric parameters, such as perimeter, circumference, solidity, aspect ratio, or arborization degree. Despite extensive microglial activation, there was no observed reduction in tau hyperphosphorylation or a decrease in tangle formation in the brainstem, where pathology predominantly develops in this model. Discussion: These findings suggest that chronic TLR4 stimulation in tau-transgenic mice results in significant microglial activation but does not influence tau tangle formation. This underscores the complexity of the relationship between neuroinflammation and tau pathology, indicating that additional mechanisms may be required for neuroinflammation to directly contribute to tau tangle formation. [ABSTRACT FROM AUTHOR]

Published

2024

6. Genetic background affects the strength of crossover interference in house mice.

Author

Morgan, Andrew P and Payseur, Bret A

Subjects

*BIOLOGICAL models, *RESEARCH funding, *AGE distribution, *MICE, *GENETIC variation, *CHROMOSOMES, *ANIMAL experimentation, *GENETICS, *GENOTYPES, *ALLELES

Abstract

Meiotic recombination is required for faithful chromosome segregation in most sexually reproducing organisms and shapes the distribution of genetic variation in populations. Both the overall rate and the spatial distribution of crossovers vary within and between species. Adjacent crossovers on the same chromosome tend to be spaced more evenly than expected at random, a phenomenon known as crossover interference. Although interference has been observed in many taxa, the factors that influence the strength of interference are not well understood. We used house mice (Mus musculus), a well-established model system for understanding recombination, to study the effects of genetics and age on recombination rate and interference in the male germline. We analyzed crossover positions in 503 progeny from reciprocal F1 hybrids between inbred strains representing the three major subspecies of house mice. Consistent with previous studies, autosomal alleles from M. m. musculus tend to increase recombination rate, while inheriting a M. m. musculus X chromosome decreases recombination rate. Old males transmit an average of 0.6 more crossovers per meiosis (⁠ 5.0 % ⁠) than young males, though the effect varies across genetic backgrounds. We show that the strength of crossover interference depends on genotype, providing a rare demonstration that interference evolves over short timescales. Differences between reciprocal F1s suggest that X-linked factors modulate the strength of interference. Our findings motivate additional comparisons of interference among recently diverged species and further examination of the role of paternal age in determining the number and positioning of crossovers. [ABSTRACT FROM AUTHOR]

Published

2024

7. The high-fat diet and low-dose streptozotocin type-2 diabetes model induces hyperinsulinemia and insulin resistance in male but not female C57BL/6J mice.

Author

Racine, Kathryn C., Iglesias-Carres, Lisard, Herring, Jacob A., Wieland, Kristopher L., Ellsworth, Peter N., Tessem, Jeffery S., Ferruzzi, Mario G., Kay, Colin D., and Neilson, Andrew P.

Subjects

*RISK assessment, *BIOLOGICAL models, *ANTIBIOTICS, *FOOD consumption, *SEX distribution, *GLUCOSE tolerance tests, *BODY weight, *HYPERINSULINISM, *INSULIN, *DIETARY fats, *INSULIN resistance, *MICE, *HYPERGLYCEMIA, *BLOOD sugar, *TYPE 2 diabetes, *ANIMAL experimentation, *FACTOR analysis, *AMINOGLYCOSIDES, *BIOMARKERS, *DISEASE risk factors, *DISEASE complications

Abstract

• Both sexes gained weight on high-fat (HF) diet + low-dose streptozotocin (STZ). • Both sexes developed impaired oral glucose tolerance. • Only males developed fasting hyperglycemia. • Only males developed hyperinsulinemia and insulin resistance. • Principal component analysis revealed overall metabolic derangement for males only. • HF diet + low-dose STZ is not useful for studying insulin resistance in female mice. Translation of preclinical findings on the efficacy of dietary interventions for metabolic disease to human clinical studies is challenging due to the predominant use of male rodents in animal research. Our objective was to evaluate a combined high-fat (HF) diet and low-dose streptozotocin (STZ) model for induction of type-2 diabetes (T2D) in male and female C57BL/6J mice. We hypothesized that T2D biomarkers would differ significantly between sexes. Mice were administered either a low-fat (LF) diet (10% kcal from fat), or HF diet (60% kcal from fat) + STZ injections (30 mg/kg/d for 3 days). Both sexes gained weight and developed impaired postprandial oral glucose tolerance on the HF+STZ treatment compared to LF. Only male mice on HF + STZ developed fasting hyperglycemia, fasting hyperinsulinemia and insulin resistance, suggesting that the underlying causes of postprandial hyperglycemia differed between sexes. Principal component analysis of measures such as body weights, glucose and insulin concentrations indicated metabolic derangement for males only on HF+STZ treatment, while LF group males and both groups of females significantly overlapped. Based on our data, we accept our hypothesis that the combined high-fat diet and low-dose STZ model for T2D phenotypes differs significantly in its effect on mice based on sex. The HF diet + low-dose STZ model is not useful for studying insulin resistance in females. Other models are needed to model T2D, and study the effects of dietary interventions in this disease, in females. Sexual dimorphism remains a significant challenge for both preclinical and clinical research. We attempted to induce type-2 diabetes in mice with high-fat diet and low-dose streptozotocin. Both sexes developed impaired oral glucose tolerance. Only males developed fasting hyperglycemia, hyperinsulinemia and insulin resistance. The high-fat diet and low-dose streptozotocin model primarily recapitulates type-2 diabetes in males. Studies of dietary interventions thus require other models to study their effects in females, complicating translation of preclinical findings to humans. Abbreviations: F, Female; HF, high-fat, HOMA-IR, Homeostatic Model Assessment for Insulin Resistance; LF, low-fat; M, male; PC, principal component; STZ, streptozotocin. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

8. TGF-β Promotes Hepatocellular Carcinoma Metastasis Through Through m6A Modification of PCDHGA9.

Author

Wang, Huamin, Guan, Wen, Zhang, Xianzhou, Wu, Yanting, Ou, Yanghui, Zhang, Yali, Zeng, Zhijun, and Yao, Hongliang

Subjects

*PROTEIN analysis, *BIOLOGICAL models, *TISSUE arrays, *IN vitro studies, *WOUND healing, *FLOW cytometry, *EPITHELIAL-mesenchymal transition, *RESEARCH funding, *ADENOSINES, *CELL proliferation, *APOPTOSIS, *IN vivo studies, *CELL motility, *REVERSE transcriptase polymerase chain reaction, *METASTASIS, *TUMOR suppressor genes, *MICE, *ANIMAL experimentation, *WESTERN immunoblotting, *TRANSFORMING growth factors-beta, *HEPATOCELLULAR carcinoma, *PRECIPITIN tests

Abstract

Objective: Hepatocellular carcinoma (HCC) is a highly lethal cancer with significant mortality, primarily attributed to metastasis. Although Protocadherin Gamma Subfamily A, 9 (PCDHGA9) has been identified as a tumor suppressor gene in cancer metastasis, its role in HCC remains ambiguous. This study clarifies the role of PCDHGA9 in HCC by examining its expression, clinical significance, and molecular activities. Methods: Tissue microarray immunofluorescence analysis evaluated the expression of PCDHGA9 and its clinical relevance. In vitro experiments involved manipulating PCDHGA9 levels in SK-HEP-1 cells to assess migration through wound-healing and transwell assays. In vivo, shPCDHGA9 cell injections were utilized to observe effects on tumor growth and metastasis. Protein analysis and Western Blot validated epithelial-mesenchymal transition (EMT)-related proteins. Subsequent to TGF-β treatment, cell proliferation and apoptosis were quantified using cell counting kit-8 and flow cytometry, respectively, followed by investigation of TGF-β effects on PCDHGA9 N6-methyladenosine (m6A) modification via Methylated RNA immunoprecipitation, RT-qPCR, and Western blot analysis. Results: Downregulation of PCDHGA9 expression in HCC tissues is correlated with poor prognosis. In vitro experiments demonstrated that modulating PCDHGA9 expression influenced HCC cell migration. In vivo, PCDHGA9 knockdown is correlated with increased metastasis. Furthermore, TGF-β stimulation promoted cell proliferation and inhibited apoptosis. Mechanistically, TGF-β-mediated m6A modification led to PCDHGA9 decay, promoting EMT in HCC cells. Conclusion: PCDHGA9 serves as a potential tumor suppressor in HCC by inhibiting EMT. During this process, TGF-β is observed to exert regulatory control over m6A modifications of PCDHGA9. [ABSTRACT FROM AUTHOR]

Published

2024

9. Alcohol and fear conditioning produce strain‐specific changes in the dorsal hippocampal transcriptome of adolescent C57BL/6J and DBA/2J mice.

Author

Seemiller, Laurel R., Goldberg, Lisa R., Sebastian, Aswathy, Siegel, Sue Rutherford, Praul, Craig, Zeid, Dana, Albert, Istvan, Beierle, Jacob, Bryant, Camron D., and Gould, Thomas J.

Subjects

*FEAR, *BIOLOGICAL models, *CONDITIONED response, *PHYSIOLOGIC salines, *RESEARCH funding, *INTRAPERITONEAL injections, *ETHANOL, *SEX distribution, *LEARNING, *DESCRIPTIVE statistics, *REVERSE transcriptase polymerase chain reaction, *GENE expression, *MICE, *RNA, *ANIMAL behavior, *ANIMAL experimentation, *ANALYSIS of variance, *HIPPOCAMPUS (Brain), *DATA analysis software, *GENETICS, *SEQUENCE analysis

Abstract

Background: Adolescent sensitivity to alcohol is influenced by genetic background. Data from our laboratory suggested that adolescent C57BL/6J and DBA/2J inbred mice differed in susceptibility to alcohol‐induced deficits in dorsal hippocampus‐dependent contextual fear learning. Methods: To investigate the biological underpinnings of this strain difference, we examined dorsal hippocampus gene expression using RNA‐sequencing after alcohol or saline administration followed by Pavlovian fear conditioning across male and female C57BL/6J and DBA/2J adolescents. Results: Strains exhibited dramatic differences in dorsal hippocampus gene expression. Specifically, C57BL/6J and DBA/2J strains differed by 3526 transcripts in males and 2675 transcripts in females. We identified pathways likely to be involved in mediating alcohol's effects on learning, including networks associated with Chrna7, a gene encoding the nicotinic cholinergic receptor alpha 7 subunit, and Fmr1, a gene encoding the fragile X messenger ribonucleoprotein. Conclusions: These findings provide insight into the mechanisms underlying strain differences in alcohol's effects on learning and suggest that different biological networks are recruited for learning based on genetics, sex, and alcohol exposure. [ABSTRACT FROM AUTHOR]

Published

2024

10. Enhancing Anti-PD-1 Immunotherapy by Targeting MDSCs via Hepatic Arterial Infusion in Breast Cancer Liver Metastases.

Author

Kim, Minhyung, Powers, Colin A., Fisher, Daniel T., Ku, Amy W., Neznanov, Nickolay, Safina, Alfiya F., Wang, Jianmin, Gautam, Avishekh, Balachandran, Siddharth, Krishnamurthy, Anuradha, Gurova, Katerina V., Evans, Sharon S., Gudkov, Andrei V., and Skitzki, Joseph J.

Subjects

*LIVER tumors, *BIOLOGICAL models, *IN vitro studies, *NF-kappa B, *FLOW cytometry, *HEPATIC artery, *RESEARCH funding, *T cells, *T-test (Statistics), *IMMUNOTHERAPY, *BREAST tumors, *INVESTIGATIONAL drugs, *APOPTOSIS, *ENZYME-linked immunosorbent assay, *MYELOID-derived suppressor cells, *COLORECTAL cancer, *IN vivo studies, *METASTASIS, *IMMUNE checkpoint inhibitors, *CELL lines, *MICE, *LOG-rank test, *DRUG efficacy, *MOLECULAR structure, *ANIMAL experimentation, *WESTERN immunoblotting, *INTRA-arterial infusions, *FLUOROURACIL, *SURVIVAL analysis (Biometry), *DATA analysis software, *CELL survival, *IMMUNOCOMPETENCE, *SEQUENCE analysis, *PHARMACODYNAMICS

Abstract

Simple Summary: Various cancer therapies are often ineffective for advanced metastatic liver disease. While immunotherapy can be effective in some cases, it does not provide significant benefits for metastatic cancer in the liver. CBL0137 is an experimental drug that helps form a special type of DNA called Z-DNA, which may help boost the body's immune response against tumors. We investigated how CBL0137 affects metastatic liver tumor models from colon (CT26) and breast (4T1) cancers focusing on how it triggers immune responses. The results showed that CBL0137 hepatic arterial infusion (HAI) enhanced anti-tumor effects by depleting immune-suppressing cells while preserving effector T cells. Combining CBL0137 HAI with conventional immunotherapy improved survival in 4T1 tumors but not in CT26 tumors, highlighting the importance of targeting specific immune cell populations for effective treatment. Background: Surgery, chemotherapy, and radiation often have limited utility for advanced metastatic disease in the liver, and despite its promising activity in select cancers, PD-1 blockade therapy similarly has minimal benefit in this setting. Curaxin, CBL0137, is an experimental anti-cancer drug that disrupts the binding of DNA to histones, destabilizes chromatin, and induces Z-DNA formation which may stimulate anti-tumor immune responses. Methods: Murine cell lines of colon (CT26) and breast (4T1) cancer were interrogated for survival and CBL0137-associated DNA changes in vitro. Immunocompetent models of liver metastases followed by CBL0137 hepatic arterial infusion (HAI) were used to examine in vivo tumor cell DNA alterations, treatment responses, and the immune contexture associated with CBL0137, both alone and in combination with anti-PD-1 therapy. Results: CBL0137 induced immediate changes to favor tumor cell death in vitro and in vivo with an efficient tumor uptake via the HAI route. Toxicity to CBL0137 was minimal and anti-tumor treatment effects were more efficient with HAI compared to intravenous delivery. Immune effects were pronounced with CBL0137 HAI with concurrent depletion of a specific population of myeloid-derived suppressor cells and maintenance of effector T cell populations. Conclusions: Combination of CBL0137 HAI with PD-1 blockade improved survival in 4T1 tumors but not in CT26 tumors, and therapeutic efficacy relies on the finding of simultaneous and targeted depletion of myeloid-derived suppressor cells and skewing of T cell populations to produce synergy with PD-1 blockade therapy. [ABSTRACT FROM AUTHOR]

Published

2024

11. Low-Intensity Focused Ultrasound-Responsive Phase-Transitional Liposomes Loaded with STING Agonist Enhances Immune Activation for Breast Cancer Immunotherapy.

Author

Hu, Cong, Jiang, Yuancheng, Chen, Yixin, Wang, Ying, Wu, Ziling, Zhang, Qi, and Wu, Meng

Subjects

*IN vitro studies, *BIOLOGICAL models, *DIAGNOSTIC imaging, *RESEARCH funding, *KILLER cells, *BREAST tumors, *IMMUNOTHERAPY, *OLIGOPEPTIDES, *ELECTRON microscopy, *TISSUE engineering, *DRUG delivery systems, *IN vivo studies, *DESCRIPTIVE statistics, *TUMOR markers, *PHYSICAL & theoretical chemistry, *MICE, *CELL lines, *ANIMAL experimentation, *NEUROPEPTIDES, *ENDOTHELIAL cells, *ARTIFICIAL membranes, *ULTRASONIC therapy, *SCATTERING (Physics), *MEMBRANE proteins, *MOLECULAR diagnosis, *NANOPARTICLES, *BREAST, *REGULATORY T cells, *DENDRITIC cells

Abstract

Simple Summary: STING agonists face challenges in breast cancer treatment due to their lower accumulation in tumors and rapid clearance from the body, resulting in a short duration of therapeutic effect. Novel phase-transitional liposomes loaded with STING agonists have been developed to overcome these limitations and are specifically designed for low-intensity focused ultrasound (LIFU)-assisted molecular imaging and precise treatment of breast cancer. With the assistance of LIFU, iRGD-modified liposomes (a targeting peptide) undergo a phase transition into microbubbles, leading to enhanced ultrasound molecular imaging of tumors and facilitating breast cancer immunotherapy by releasing STING agonists from the ultrasound-targeted liposomes. Background: Pharmacologically targeting the STING pathway offers a novel approach to cancer immunotherapy. However, small-molecule STING agonists face challenges such as poor tumor accumulation, rapid clearance, and short-lived effects within the tumor microenvironment, thus limiting their therapeutic potential. To address the challenges of poor specificity and inadequate targeting of STING in breast cancer treatment, herein, we report the design and development of a targeted liposomal delivery system modified with the tumor-targeting peptide iRGD (iRGD-STING-PFP@liposomes). With LIFU irradiation, the liposomal system exploits acoustic cavitation, where gas nuclei form and collapse within the hydrophobic region of the liposome lipid bilayer (transient pore formation), which leads to significantly enhanced drug release. Methods: Transmission electron microscopy (TEM) was used to investigate the physicochemical properties of the targeted liposomes. Encapsulation efficiency and in vitro release were assessed using the dialysis bag method, while the effects of iRGD on liposome targeting were evaluated through laser confocal microscopy. The CCK-8 assay was used to investigate the toxicity and cell growth effects of this system on 4T1 breast cancer cells and HUVEC vascular endothelial cells. A subcutaneous breast cancer tumor model was established to evaluate the tumor-killing effects and therapeutic mechanism of the newly developed liposomes. Results: The liposome carrier exhibited a regular morphology, with a particle size of 232.16 ± 19.82 nm, as indicated by dynamic light scattering (DLS), and demonstrated low toxicity to both HUVEC and 4T1 cells. With an encapsulation efficiency of 41.82 ± 5.67%, the carrier exhibited a slow release pattern in vitro after STING loading. Targeting results indicated that iRGD modification enhanced the system's ability to target 4T1 cells. The iRGD-STING-PFP@liposomes group demonstrated significant tumor growth inhibition in the subcutaneous breast cancer mouse model with effective activation of the immune system, resulting in the highest populations of matured dendritic cells (71.2 ± 5.4%), increased presentation of tumor-related antigens, promoted CD8+ T cell infiltration at the tumor site, and enhanced NK cell activity. Conclusions: The iRGD-STING-PFP@liposomes targeted drug delivery system effectively targets breast cancer cells, providing a new strategy for breast cancer immunotherapy. These findings indicate that iRGD-STING-PFP@liposomes could successfully deliver STING agonists to tumor tissue, trigger the innate immune response, and may serve as a potential platform for targeted immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2024

12. Cannabidiol (CBD) Protects Lung Endothelial Cells from Irradiation-Induced Oxidative Stress and Inflammation In Vitro and In Vivo.

Author

Bauer, Lisa, Alkotub, Bayan, Ballmann, Markus, Hasanzadeh Kafshgari, Morteza, Rammes, Gerhard, and Multhoff, Gabriele

Subjects

*CANNABIDIOL, *BIOLOGICAL models, *IN vitro studies, *OXYGENASES, *RADIOTHERAPY, *BLOOD vessels, *APOPTOSIS, *BODY weight, *OXIDATIVE stress, *LUNGS, *IN vivo studies, *TREATMENT effectiveness, *TUMOR markers, *MICE, *CELL lines, *ENDOTHELIAL cells, *ANIMAL experimentation, *DNA damage, *INFLAMMATION, CHEST tumors

Abstract

Simple Summary: Radiotherapy remains a central pillar in the therapy of solid tumors, including lung cancer. However, the clinically applied radiation dose to a lung tumor is limited by the radiation-sensitivity of the surrounding normal tissue such as the lungs and heart. Ionizing irradiation causes reactive oxygen species (ROS)-induced chronic vascular inflammation, which can result in fatal irradiation-induced lung diseases such as pneumonitis and fibrosis. In this study, we demonstrate that cannabidiol (CBD), the non-psychogenic component of cannabis, mediates anti-inflammatory and anti-oxidative effects that protect the microvasculature of the lung against radiation-induced damage using in vitro and in vivo murine models. CBD therefore has the potential to improve the clinical outcome of radiotherapy by reducing normal tissue toxicity in the lung. Objective: Radiotherapy, which is commonly used for the local control of thoracic cancers, also induces chronic inflammatory responses in the microvasculature of surrounding normal tissues such as the lung and heart that contribute to fatal radiation-induced lung diseases (RILDs) such as pneumonitis and fibrosis. In this study, we investigated the potential of cannabidiol (CBD) to attenuate the irradiation damage to the vasculature. Methods: We investigated the ability of CBD to protect a murine endothelial cell (EC) line (H5V) and primary lung ECs isolated from C57BL/6 mice from irradiation-induced damage in vitro and lung ECs (luECs) in vivo, by measuring the induction of oxidative stress, DNA damage, apoptosis (in vitro), and induction of inflammatory and pro-angiogenic markers (in vivo). Results: We demonstrated that a non-lethal dose of CBD reduces the irradiation-induced oxidative stress and early apoptosis of lung ECs by upregulating the expression of the cytoprotective mediator heme-oxygenase-1 (HO-1). The radiation-induced increased expression of inflammatory (ICAM-2, MCAM) and pro-angiogenic (VE-cadherin, Endoglin) markers was significantly reduced by a continuous daily treatment of C57BL/6 mice with CBD (i.p. 20 mg/kg body weight), 2 weeks before and 2 weeks after a partial irradiation of the lung (less than 20% of the lung volume) with 16 Gy. Conclusions: CBD has the potential to improve the clinical outcome of radiotherapy by reducing toxic side effects on the microvasculature of the lung. [ABSTRACT FROM AUTHOR]

Published

2024

13. USP22 promotes gefitinib resistance and inhibits ferroptosis in non‐small cell lung cancer by deubiquitination of MDM2.

Author

Lu, Peng, Li, Zhaoguo, and Xu, Hang

Subjects

*THERAPEUTIC use of antineoplastic agents, *FLOW cytometry, *CELL migration inhibition, *BIOLOGICAL models, *GEFITINIB, *DRUG resistance in cancer cells, *ANTINEOPLASTIC agents, *CELL proliferation, *APOPTOSIS, *TUMOR markers, *REVERSE transcriptase polymerase chain reaction, *CELLULAR signal transduction, *XENOGRAFTS, *MICE, *IMMUNOHISTOCHEMISTRY, *GENE expression, *PROTEOLYTIC enzymes, *CELL death, *DRUG efficacy, *ANIMAL experimentation, *WESTERN immunoblotting, *LUNG tumors, *LUNG cancer, *STAINS & staining (Microscopy), *PRECIPITIN tests, *PHARMACODYNAMICS

Abstract

Background: The emergence of chemoresistance markedly compromised the treatment efficiency of human cancer, including non‐small cell lung cancer (NSCLC). In the present study, we aimed to explore the effects of ubiquitin‐specific peptidase 22 (USP22) and murine double minute 2 (MDM2) in gefitinib resistance in NSCLC. Methods: Immunohistochemistry (IHC) assay, quantitative real‐time polymerase chain reaction (qRT‐PCR) assay and western blot assay were carried out to determine the expression of USP22 and MDM2. Transwell assay and flow cytometry analysis were performed to evaluate cell migration and apoptosis. Cell Counting Kit‐8 (CCK‐8) assay was employed to assess gefitinib resistance. The phenomenon of ferroptosis was estimated by related commercial kits. The oxidized C11‐BODIPY fluorescence intensity by C11‐BODIPY staining. The relation between USP22 and MDM2 was analyzed by ubiquitination assay and co‐immunoprecipitation (Co‐IP) assay. Results: USP22 was abnormally upregulated in NSCLC tissues and cells, and USP22 silencing markedly repressed NSCLC cell migration and facilitated apoptosis and ferroptosis. Moreover, our results indicated that ferroptosis could enhance the suppressive effect of gefitinib on NSCLC cells. Besides, USP22 overexpression enhanced gefitinib resistance and ferroptosis protection in NSCLC cells. Mechanically, USP22 stabilized MDM2 and regulated MDM2 expression through deubiquitination of MDM2. MDM2 deficiency partially restored the effects of USP22 on gefitinib resistance and ferroptosis in NSCLC cells. Of note, we validated the promotional effect of USP22 on gefitinib resistance in NSCLC in vivo through establishing the murine xenograft model. Conclusion: USP22/MDM2 promoted gefitinib resistance and inhibited ferroptosis in NSCLC, which might offer a novel strategy for overcoming gefitinib resistance in NSCLC. [ABSTRACT FROM AUTHOR]

Published

2024

14. Korean Red Ginseng Extract Powder Mitigates Fasting And Postprandial Hyperglycemia in Type 2 Diabetic Mice.

Author

Jo, Min-Jeong, Hwang, Sun Jin, Kwon, Han-Ol, Kim, Jong-Han, Shim, Sung Lye, and Park, Sang-Joon

Subjects

*THERAPEUTIC use of ginseng, *BIOLOGICAL models, *METFORMIN, *PREPROCEDURAL fasting, *INSULIN sensitivity, *GLYCOSYLATED hemoglobin, *MITOCHONDRIA, *RESEARCH funding, *POWDERS, *GLUCOSE tolerance tests, *GLYCEMIC control, *GLUCAGON-like peptide 1, *ORAL drug administration, *MICE, *BLOOD sugar, *MESSENGER RNA, *INSULIN resistance, *ENERGY metabolism, *PANCREAS, *TYPE 2 diabetes, *DRUG efficacy, *ANIMAL experimentation, *GINSENG, *LIVER, *DRUG tolerance

Abstract

Type 2 diabetes mellitus (T2DM) involves insulin resistance and elevated blood sugar levels, causing complications. Red ginseng extract powder (RGEP) from Panax ginseng Meyer shows promise for diabetes treatment. However, its efficacy in managing T2DM remains unclear. Therefore, this study aims to evaluate the effectiveness of RGEP in a mouse model of T2DM. The efficacy of RGEP in treating T2DM was assessed in db/db mice. Mice were divided into seven groups: control, db/db, metformin, and RGEP at 50, 100, 200, and 400 mg/kg. Administered orally for 9 weeks, RGEP effects on glucose regulation and insulin sensitivity were assessed through various metabolic parameters. In addition, mRNA expression levels of genes associated with hepatic gluconeogenesis and insulin sensitivity were examined. Fasting blood sugar showed a significant decrease in all RGEP concentration groups, but OGTT and insulin tolerance test showed a significant decrease at the RGEP concentration of 400 mg/kg, indicating enhanced glycemic control. Moreover, RGEP dose-dependently decreased serum glucose, HbA1c levels, and homeostatic model assessment of insulin resistance values, suggesting its effectiveness in reducing insulin resistance in db/db mice. Furthermore, RGEP downregulated mRNA expression of key components in the gluconeogenesis pathway (G6Pase, FOXO1, GLUT4, and PEPCK), insulin sensitivity (leptin, insulin1, PTP1B, GLP-1, and DPP-4), and mitochondria energy metabolism (PGC1) in either the liver or pancreas, while simultaneously upregulating GLP-1 expression. In conclusion, these findings highlight the potential of RGEP as a complementary therapy for T2DM, indicating therapeutic efficacy in managing diabetic complications through improved metabolic parameters. [ABSTRACT FROM AUTHOR]

Published

2024

15. Protective effect of Huashi Baidu formula against AKI and active ingredients that target SphK1 and PAI-1.

Author

Zhong, Yute, Du, Xia, Wang, Ping, Li, Weijie, Xia, Cong, Wu, Dan, Jiang, Hong, Xu, Haiyu, and Huang, Luqi

Subjects

*RNA analysis, *ACUTE kidney failure prevention, *ANALYSIS of triglycerides, *CHINESE medicine, *BIOLOGICAL models, *PROTEINS, *SUPEROXIDE dismutase, *NF-kappa B, *RESEARCH funding, *COLORIMETRY, *CREATININE, *PHOSPHORYLATION, *HERBAL medicine, *POLYMERASE chain reaction, *ENZYME inhibitors, *TREATMENT effectiveness, *ENZYMES, *BLOOD urea nitrogen, *BLOOD coagulation factors, *MICE, *BIOINFORMATICS, *ATROPHY, *ANIMAL experimentation, *DOXORUBICIN, *WESTERN immunoblotting, *ALBUMINS, *INFLAMMATION, *EXTRACELLULAR matrix, *CYTOKINES, *SEQUENCE analysis, *TUMOR necrosis factors, *INTERLEUKINS, *MALONDIALDEHYDE, *KIDNEYS, *HISTOLOGY, *TRANSFORMING growth factors-beta, *DRUG dosage, *PHARMACODYNAMICS, *DRUG administration, *CHEMICAL inhibitors

Abstract

Background: Huashi Baidu Formula (HBF) is a clinical formula known for its efficacy against coronavirus disease 2019 (COVID-19). HBF may reduce the number of patients with abnormal serum creatinine while improving respiratory symptoms, suggesting that this formula may have potential for treating acute kidney injury (AKI). However, the protective effect of HBF on AKI has not been definitively confirmed, and the mechanism remains unclear. Therefore, the present study explored the renoprotective effects and molecular mechanisms of HBF and screened for its active ingredients to identify new potential applications of renoprotection by HBF. Methods: The present study first assessed the protective effects of HBF on AKI in a DOX-induced mouse model. Then, RNA-seq and bioinformatics analyses were used to explore the related pathological processes and potential molecular mechanisms, which were subsequently validated using qRT-PCR and Western blotting. Furthermore, candidate compounds with potential binding affinity to two pivotal targets, sphingosine kinase 1 (SphK1) and plasminogen activator inhibitor-1 (PAI-1), were screened from the 29 constituents present in the blood using Microscale Thermophoresis (MST). Finally, to identify the active ingredients, the candidate components were re-screened using the SphK1 kinase activity detection system or the uPA/PAI-1 substrate colorimetric assay system. Results: In the DOX-induced AKI mouse model, therapeutic administration of HBF significantly reduced the levels of CRE, BUN, TNF-α, IL-1β, IL-6, and UA in plasma and the levels of MDA, T-CHO, and TG in kidney tissue. Additionally, the levels of TP and Alb in plasma and SOD and CAT in the kidney tissue were significantly increased. Histopathological assessment revealed that HBF reduced tubular vacuolation, renal interstitial inflammatory cell infiltration, tubular atrophy, and positive staining of renal interstitial collagen. RNA-seq and bioinformatics analyses showed that oxidative stress, the immune-inflammatory response, and extracellular matrix (ECM) formation could be the pathological processes that HBF targets to exerts its renoprotective effects. Furthermore, HBF regulated the APJ/SPHK1/NF-κB and APJ/PAI-1/TGFβ signaling axes and reduced the phosphorylation levels of NF-κB p65 and SMAD2 and the expression of cytokines and the ECM downstream of the axis. Finally, six SphK1 inhibitors (paeoniflorin, astragalin, emodin, glycyrrhisoflavone, quercetin, and liquiritigenin) and three PAI-1 inhibitors (glycyrrhisoflavone, licochalcone B, and isoliquiritigenin) were identified as potentially active ingredients in HBF. Conclusion: In brief, our investigation underscores the renoprotective effect of HBF in a DOX-induced AKI model mice, elucidating its mechanisms through distinct pathological processes and identifying key bioactive compounds. These findings offer new insights for broadening the clinical applications of HBF and unravelling its molecular mode of action. [ABSTRACT FROM AUTHOR]

Published

2024

16. Diabetes mellitus exacerbates inflammation in a murine model of ligature‐induced peri‐implantitis: A histological and microtomographic study.

Author

Silva, Davi N. A., Monajemzadeh, Sepehr, Casarin, Maísa, Chalmers, Jaclyn, Lubben, Jacob, Magyar, Clara E., Tetradis, Sotirios, and Pirih, Flavia Q.

Subjects

*DIABETES complications, *BIOLOGICAL models, *OSSEOINTEGRATION, *MACROPHAGES, *RESEARCH funding, *COMPUTED tomography, *PERI-implantitis, *DESCRIPTIVE statistics, *MICE, *ANIMAL experimentation, *HISTOLOGICAL techniques, *OSTEOCLASTS, *MATRIX metalloproteinases, *INFLAMMATION, *DIABETES

Abstract

Aim: To investigate the influence of diabetes mellitus (DM) in a murine model of peri‐implantitis (PI). Materials and Methods: Twenty‐seven 4‐week‐old C57BL/6J male mice had their first and second maxillary left molars extracted. Eight weeks later, one machined implant was placed in each mouse. Four weeks after osseointegration, the mice were divided into three groups: (a) control (C), (b) PI and (c) DM + PI. DM was induced by streptozotocin (STZ) administration. After DM induction, PI was induced using ligatures for 2 weeks. The hemimaxillae were collected for micro‐CT and histological analyses. The primary outcomes consisted of linear (mm) and volumetric (mm3) bone loss. Secondary outcomes were based on histological analysis and included inflammatory infiltrate, osteoclastic activity, matrix organization, composition and remodelling. Data are presented as means ± SEM. Statistical analyses were performed using one‐way ANOVA, followed by Tukey's test. Results: Gingival tissue oedema was detected in the PI and DM + PI groups. Micro‐CT showed significantly increased linear and volumetric bone loss in the DM + PI group compared to the C and PI groups. H&E staining showed greater inflammatory response and bone resorption in the PI and DM + PI groups than in the C group. The DM + PI group had significantly higher osteoclast numbers than the C and PI groups. Picrosirius red stained less for types I and III collagen in the PI and DM + PI groups than in the C group. There was a significant increase in monocyte/macrophage (CD‐11b) counts and matrix metalloproteinases (MMP‐2 and MMP‐8) marker levels and a significant decrease in the matrix metalloproteinases inhibition marker (TIMP‐2) levels in the DM + PI group compared to the C and PI groups. Conclusions: DM exacerbates PI‐induced soft‐tissue inflammation, matrix degradation and bone loss. [ABSTRACT FROM AUTHOR]

Published

2024

17. Non‐coding RNA alterations in occlusal disharmony‐induced anxiety‐like behaviour.

Author

Zhang, Mi, Wu, Ling, Zhang, Sihui, Li, Yuxuan, and Chen, Jiang

Subjects

*BIOLOGICAL models, *RESEARCH funding, *CIRCULAR RNA, *ANXIETY, *DESCRIPTIVE statistics, *CELLULAR signal transduction, *MICE, *ANIMAL experimentation, *SEQUENCE analysis

Abstract

Background: Occlusal disharmony (OD) may induce anxiety‐like behaviours; however, the underlying mechanism remains unclear. Herein, we explored the expression profiles of non‐coding RNAs (ncRNAs), along with their biological function and regulatory network, in anxiety‐like behaviour induced by OD. Materials and Methods: Occlusal disharmony was produced by anterior crossbite of C57BL/6 mice. Behavioural tests, corticosterone (CORT) and serotonin (5‐HT) levels were used to measure anxiety. In addition, RNA sequencing was used to screen all differentially expressed (DE) ncRNAs. Moreover, the RNA‐binding proteins interacting with ncRNAs were predicted by the ENCORI database and confirmed using western blots. Results: The significant differences in behavioural tests and CORT suggested the successful induction of anxiety‐like behaviour by OD. In OD mice, ncRNAs were significantly dysregulated. Gene Ontology (GO) and Kyoto Encyclopedia of Genes and Genomes (KEGG) analyses suggested that the DE ncRNAs were enriched in anxiety‐related pathways. CircRNA10039 was upregulated, and PTBP1 was predicted to interact with circRNA10039. In addition, KEGG pathway analysis showed that PTBP1 may be associated with messenger RNA biogenesis and spliceosomes. Conclusion: OD induced by anterior crossbite can lead to the anxiety‐like behaviours. During this process, ncRNA also changes. CircRNA10039 and PTBP1 may play a role in OD‐induced anxiety‐like behaviours. [ABSTRACT FROM AUTHOR]

Published

2024

18. Molecular Mechanisms of Anticarcinogenic Potential of Hydrocotyle umbellata and Its Major Components.

Author

Kim, Jaeyong, Park, Sang Hyuk, Kim, Doo-Young, Ryu, Hyung Won, and Jun, Hyun Sik

Subjects

*PHYTOTHERAPY, *THERAPEUTIC use of antineoplastic agents, *BIOLOGICAL models, *RESEARCH funding, *ANTINEOPLASTIC agents, *CELL proliferation, *APOPTOSIS, *IN vivo studies, *PLANT extracts, *MICE, *CELL lines, *ANIMAL experimentation, *TUMORS, *PHARMACODYNAMICS, TUMOR prevention

Abstract

Despite the development of several anticancer treatments, there remains a need for new drugs that can overcome resistance and reduce side effects. While the medicinal herb Hydrocotyle umbellata (H. umbellata) has been used to relieve pain and inflammation, its antitumor properties have not yet been explored. In this study, we investigated the anticarcinogenic potential of H. umbellata extract (HUE) and its major components, as well as the underlying molecular mechanisms. Our results showed that HUE inhibited the growth of various tumor cell lines, including B16F10, without affecting non-cancer cells. Furthermore, HUE was effective in treating and preventing tumor growth in mice. Our mechanistic studies revealed that HUE inhibited cellular respiration, thereby reducing tumor cell proliferation. When combined with 2-deoxy-D-glucose, HUE demonstrated an enhanced anticancer effect by increasing the rate apoptosis. Analysis of the ethyl acetate and n-butanol fractions of HUE identified 1,3,4-trihydroxy-2-butanyl-α-d-glucopyranoside and caffeoylquinic acid derivatives as the major components responsible for the observed anticancer effects. In conclusion, our findings suggest that HUE and its two major components have the potential to be developed as effective therapeutic agents for a wide range of tumors by targeting cancer cell metabolism. [ABSTRACT FROM AUTHOR]

Published

2024

19. Celastrus orbiculatus Extract Inhibits Immune Inflammatory Thrombotic State of B-Lymphoma.

Author

Zhu, Miao, Shi, Qing-qing, Ni, Jun, Wu, Wei, Sun, Xing, Sun, Mei, Xu, Kai-lin, Liu, Yan-qing, Gu, Jian, and Gu, Hao

Subjects

PHYTOTHERAPY, THROMBOLYTIC therapy, BIOLOGICAL models, FLOW cytometry, INFLAMMATORY mediators, CELL proliferation, APOPTOSIS, ENZYME-linked immunosorbent assay, NEUTROPHILS, IN vivo studies, CELL cycle, FIBRIN fibrinogen degradation products, DESCRIPTIVE statistics, PLANT extracts, MICE, CELL lines, BLOOD coagulation factors, ANIMAL experimentation, INFLAMMATION, THROMBOPLASTIN, EXTRACELLULAR space, DATA analysis software, B cell lymphoma, IMMUNITY, INTERLEUKINS, TUMOR necrosis factors

Abstract

Objective: To investigate the inhibitory effect of Celastrus orbiculatus extracts (COE) on the proliferation of lymphoma cells and the immune regulation ability on inflammation and thrombophilia in vivo. Methods: The 38B9 lymphoma cells were treated with COE (160 µ g/mL) and CTX (25 µ mol/L). The apoptosis rate and cell cycle of each group were detected by flow cytometry. The secretion of inflammatory factors, including interleukin (IL)-6, IL-10, and tumor necrosis factor α (TNF-α), in cell supernatant was detected by enzyme-linked immunosorbent assay (ELISA). In vivo, BALB/c mice were subcutaneously injected with 38B9 lymphoma cells to establish lymphoma model. COE (3 mg·kg−1·d−1) and CTX (40 mg·kg−1·d−1) were administered to the model mice, respectively. The expression of plasma inflammatory factors (IL-6, IL-10 and TNF-α) and thrombus indexes, including D-dimer (D-D), von Willebrand factor (vWF) and tissue factor (TF), were detected by ELISA before tumor bearing (1 d), after tumor formation (14 d) and after intervention (21 d). PicoGreen dsDNA was used to detect the level of serum neutrophil extracellular traps (NETs). Flow cytometry was used to detect the expression of platelet activation marker calcium-dependent lectin-like receptor 2 (CLEC-2). The tumor growth and survival of mice were recorded. Results: The 38B9 lymphoma cells were apoptotic after the intervention of COE and CTX. The ratio of G2-M phase cells decreased in COE intervented cells compared with the control cells (P<0.05), and S phase cells decreased in CTX intervented cells (P<0.05). Also, the secretion level of IL-6 was significantly reduced after COE or CTX intervention (P<0.05), and IL-10 was significantly increased (P<0.05). Furthermore, the tumor mass was reduced, and the median survival time was longer in COE and CTX intervented tumor-bearing mice than in non-intervented mice. The significantly lower levels of TNF-α, IL-6, NETs, TF, DD and CLEC-2, as well as higher IL-10 were observed in COE and CTX treatment mice in comparision with the control mice (P<0.05). Conclusion: COE has a mild and stable anti-tumor effect, which can reduce the secretion of inflammatory factors by lymphoma cells and regulate thrombophilic state caused by tumor inflammatory microenvironment. [ABSTRACT FROM AUTHOR]

Published

2024

20. Platycodin D and voluntary running synergistically ameliorate memory deficits in 5 × FAD mice via mediating neuromodulation and neuroinflammation.

Author

Junxin Liu, Jiahui Jiang, Chuantong He, Longjian Zhou, Yi Zhang, Shuai Zhao, and Zhiyou Yang

Subjects

PHYTOTHERAPY, ALZHEIMER'S disease prevention, NEUROPROTECTIVE agents, CHINESE medicine, HIGH performance liquid chromatography, BIOLOGICAL models, EXERCISE, ALZHEIMER'S disease, ABLATION techniques, DATA analysis, RESEARCH funding, RUNNING, HERBAL medicine, ENZYME-linked immunosorbent assay, POLYMERASE chain reaction, KRUSKAL-Wallis Test, NEUROINFLAMMATION, CELLULAR signal transduction, FLUORESCENT antibody technique, DESCRIPTIVE statistics, PLANT extracts, MICE, MONOAMINE oxidase inhibitors, IMMUNOHISTOCHEMISTRY, MEDICINAL plants, COMBINED modality therapy, ANIMAL experimentation, NEUROPSYCHOLOGICAL tests, STATISTICS, DRUGS, STAINS & staining (Microscopy), DATA analysis software, MEMORY disorders, NEUROTRANSMITTERS, DIET therapy, DRUG synergism, CARDIAC surgery, PHARMACODYNAMICS, THERAPEUTICS

Abstract

Introduction: Alzheimer’s disease (AD) is the leading cause of dementia, and currently, no effective treatments are available to reverse or halt its progression in clinical practice. Although a plethora of studies have highlighted the benefits of physical exercise in combating AD, elder individuals often have limited exercise capacity. Therefore, mild physical exercise and nutritional interventions represent potential strategies for preventing and mitigating neurodegenerative diseases. Our research, along with other studies, have demonstrated that platycodin D (PD) or its metabolite, platycodigenin, derived from the medicinal plant Platycodon grandiflorus, exerts neuroprotective effects against amyloid β (Aβ)-induced neuroinflammation. However, the combined effects of PD and physical exercise on alleviating AD have yet to be explored. The current study aimed to investigate whether combined therapy could synergistically ameliorate memory deficits and AD pathology in 5 × FAD mice. Methods: Five-month-old 5 × FAD mice were randomly assigned to four groups, and received either PD (5 mg/kg/day, p.o.), voluntary running, or a combination of both for 47 days. Nest building test, locomotion test, and Morris water maze test were used to evaluate the cognitive function. Immunohistochemical and ELISA analysis was performed to determine Aβ build-up, microglia and astrocytes hyperactivation, and survival neurons in the hippocampus and perirhinal cortex. Real-time quantitative PCR analysis was used to assess the polarization of microglia and astrocytes. HPLC analysis was performed to measure monoamine neurotransmitters in the hippocampus. Results and discussion: The combination of PD and voluntary running synergistically restored nest-building behavior, alleviated recognition and spatial memory deficits, and showed superior effects compared to monotherapy. In addition, the PD and voluntary running combination reduced Aβ build-up, decreased hyperactivation of microglia and astrocytes in the hippocampus and perirhinal cortex, promoted the polarization of inflammatory M1 microglia and reactive astrocytes toward beneficial phenotypes, and lowered systemic circulating pro-inflammatory cytokines while increasing anti-inflammatory cytokines in 5 × FAD mice. Furthermore, combined therapy effectively protected neurons and increased levels of 5-hydroxytryptamine (5-HT) and dopamine (DA) in the hippocampus of 5 × FAD mice. In conclusion, the combination of PD and voluntary running holds great potential as a treatment for AD, offering promise for delaying onset or progression of AD. [ABSTRACT FROM AUTHOR]

Published

2024

21. NLRP3 inflammasome activation and pyroptosis are dispensable for tau pathology.

Author

Paesmans, Ine, Van Kolen, Kristof, Vandermeeren, Marc, Shih, Pei-Yu, Wuyts, Dirk, Boone, Fleur, Sanchez, Sergio Garcia, Grauwen, Karolien, Van Hauwermeiren, Filip, Van Opdenbosch, Nina, Lamkanfi, Mohamed, van Loo, Geert, and Bottelbergs, Astrid

Subjects

TAU proteins, BIOLOGICAL models, IN vitro studies, HETEROCYCLIC compounds, RESEARCH funding, PHOSPHORYLATION, PROTEIN kinases, ALZHEIMER'S disease, APOPTOSIS, NEUROINFLAMMATION, CELLULAR signal transduction, DESCRIPTIVE statistics, NEURODEGENERATION, PHOSPHATASES, NERVE tissue proteins, TAUOPATHIES, MICE, IMMUNOHISTOCHEMISTRY, ANIMAL experimentation, LIPOPOLYSACCHARIDES, CYTOPLASM, PROTEOMICS, WESTERN immunoblotting, GENETIC mutation, NATURAL immunity, CYTOKINES, SIGNAL peptides, INTERLEUKINS, DISEASE progression, CASPASES, CHEMICAL inhibitors

Abstract

Background: Neuroinflammation is widely recognized as a key factor in the pathogenesis of Alzheimer’s disease (AD), alongside ß-amyloid deposition and the formation of neurofibrillary tangles. The NLR family pyrin domain containing 3 (NLRP3) inflammasome, part of the innate immune system, has been implicated in the neuropathology of both preclinical amyloid and tau transgenic models. Activation of the NLRP3 pathway involves an initial priming step, which increases the expression of Nlrp3 and interleukin (IL)-1β, followed by the assembly of the NLRP3 inflammasome complex, comprising NLRP3, ASC, and caspase-1. This assembly leads to the proteolytic maturation of the pro-inflammatory cytokines IL-1β and IL-18. Additionally, the NLRP3 inflammasome induces Gasdermin D (GSDMD) cleavage, forming membrane pores through which IL-1β and IL-18 are secreted. Inhibition of NLRP3 has been shown to enhance plaque clearance by modulating microglial activation. Furthermore, blocking NLRP3 in tau transgenic mice has been found to reduce tau phosphorylation by affecting the activity of certain tau kinases and phosphatases. Methods: In this study, organotypic brain slice cultures from P301S transgenic mice were treated with lipopolysaccharide (LPS) plus nigericin as a positive control or exposed to tau seeds (K18) to evaluate NLRP3 inflammasome activation. The effect of tau seeding on NLRP3 activity was further examined using Meso Scale Discovery (MSD) assays to measure IL1β secretion levels in the presence and absence of NLRP3 inhibitors. The role of NLRP3 activity was investigated in fullbody Nlrp3 knockout mice crossbred with the tau transgenic P301S model. Additionally, full-body and microglia-selective Gsdmd knockout mice were crossbred with P301S mice, and tau pathology and neurodegeneration were evaluated at early and late stages of the disease using immunohistochemistry and biochemical assays. Results: Activation of the NLRP3 pathway was observed in the mouse organotypic slice culture (OSC) model following stimulation with LPS and nigericin or exposure to tau seeds. However, Nlrp3 deficiency did not mitigate tauopathy or neurodegeneration in P301S mice in vivo, showing only a minor effect on plasma neurofilament (NF-L) levels. Consistently, Gsdmd deficiency did not alter tau pathology in P301S mice. Furthermore, neither full-body nor microglia-selective Gsdmd deletion had an impact on neuronal pathology or the release of pro-inflammatory cytokines. Conclusion: The absence of key components of the NLRP3 inflammasome pathway did not yield a beneficial effect on tau pathology or neurodegeneration in the preclinical Tau-P301S mouse model of AD. Nonetheless, organotypic slice cultures could serve as a valuable ex vivo mechanistic model for evaluating NLRP3 pathway activation and pharmacological inhibitors. [ABSTRACT FROM AUTHOR]

Published

2024

22. Comparative Proteomic and Phosphoproteomic Analyses Reveal Molecular Signatures of Myocardial Infarction and Transverse Aortic Constriction in Aged Mouse Models.

Author

Lin, Fang, Ding, Yue, Liang, Xiaoting, and Luo, Zhiwen

Subjects

*PROTEIN analysis, *MYOCARDIAL infarction, *BIOLOGICAL models, *PHOSPHORYLATION, *CORONARY disease, *RESEARCH funding, *LIQUID chromatography-mass spectrometry, *DATA analysis, *HYPERTENSION, *CARDIAC hypertrophy, *DESCRIPTIVE statistics, *MICE, *BIOINFORMATICS, *PROTEOMICS, *AGING, *ANIMAL experimentation, *ONE-way analysis of variance, *STATISTICS, *DATA analysis software, *BIOMARKERS, *MUSCLE contraction, *ECHOCARDIOGRAPHY

Abstract

In the elderly population, coronary heart disease (CHD) often coexists with hypertension. However, excessive blood pressure reduction can paradoxically increase the incidence of adverse events. Understanding the molecular mechanisms underlying hypertension and CHD in aged populations is crucial for developing targeted therapies and improving clinical outcomes. In this study, we constructed myocardial infarction (MI) and transverse aortic constriction (TAC) modelsY in aged mice to simulate the disease states of CHD and hypertension, respectively. Using integrated proteomic and phosphoproteomic analyses, we investigated the molecular signatures associated with MI and TAC in these models. Our aim was to identify key molecules involved in these conditions and to understand their unique and shared characteristics. Through our comprehensive proteomic and phosphoproteomic analysis, we identified a total of 1583 proteins and 232 phosphorylated proteins. We observed significant upregulation of heart disease markers such as Myh7, Xirp2, and Acta1, indicating the successful establishment of the MI and TAC models. The overlapped differentially expressed proteins (DEPs) and differentially phosphorylated proteins (DPPs) in MI and TAC were involved in heart failure‐related processes including cardiac muscle contraction and hypertrophic cardiomyopathy, further supporting the validity of the models. Among the DEPs, Ppme1 was upregulated in the TAC model but downregulated in the MI model, while Sec31a and Gm56451 displayed the opposite expression patterns. Among the DPPs, Ablim1 and Atp2a2 were found to be significantly upregulated in the TAC model, whereas their expression was markedly reduced in the MI model. In addition, five other DPPs, including REV_Q3TAY5, Cbx3, PITPNB, Eif4b, and A0A1Y7VP73, were elevated in the MI model but decreased in the TAC model. In conclusion, these findings suggest that MI and TAC not only share certain molecular features but also retain their unique characteristics, providing potential biomarkers and therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2024

23. Inhibitory Effect of TCF7L2 on Pancreatic β-Cell Dedifferentiation via ERK/MAPK Signaling Pathway in Diabetes.

Author

Wu, Hui-Hui, Ma, Qian-Wen, Liu, Yi-Meng, Wu, Xia, and Wen, Jie

Subjects

*PANCREATIC analysis, *MITOGEN-activated protein kinases, *RISK assessment, *BIOLOGICAL models, *SMALL interfering RNA, *GLUCOSE intolerance, *RESEARCH funding, *PANCREATIC beta cells, *PLASMIDS, *TRANSCRIPTION factors, *CELLULAR signal transduction, *DIETARY fats, *BLOOD sugar, *MICE, *TYPE 2 diabetes, *ANIMAL experimentation, *PROTEOMICS, *CELL differentiation, *GENETIC techniques, *SINGLE nucleotide polymorphisms, *DISEASE progression, *DISEASE risk factors

Abstract

Background: Transcription factor 7-like 2 (TCF7L2) variants seem to affect diabetes susceptibility through β-cell dysfunction, underlying basis of which has been considered to be β-cell dedifferentiation rather than apoptotic β-cell death. The Extracellular regulated protein kinases/Mitogen-activated protein kinase signaling pathway (ERK/MAPK signaling pathway) has been confirmed to be significantly associated with multiple cellular process, including cellular dedifferentiation. However, the effects of TCF7L2 on β-cell function and ERK/MAPK signaling pathway are poorly understood. Objectives: This study aimed to elucidate the regulation of TCF7L2 in β-cell function and ERK/MAPK signaling pathway, which further participate in glucose metabolism and diabetes progression. Methods: After transfection of TCF7L2 siRNA and lenti-TCF7L2 plasmids, the activation of ERK/MAPK signaling and β-cell dedifferentiation were evaluated respectively. Six week-old male db / db mice were randomly grouped and fed a normal or high-fat diet, and then pancreatic level of TCF7L2 protein were measured respectively when the mice were fed to 8, 12, and 16 weeks of age. Furthermore, the contributions of TCF7L2 to ERK/MAPK signaling and glucose metabolism were investigated in a β-cell-specific TCF7L2 deletion mice model (TCF7L2β−/−). Results: The results demonstrated that impaired TCF7L2 induces β-cell dedifferentiation and decreases insulin secretion of MIN6 cells via ERK/MAPK signaling pathway. Consistently, decreased pancreatic TCF7L2 protein in parallel with reduced functional β-cells were observed in db / db mice after weeks of normal or high-fat diet. However, the differences between were only significant when the mice were fed to 12 weeks of age. After weeks of high-fat diet feeding, impaired glucose tolerance and increased activation of ERK/MAPK signaling were simultaneously observed in TCF7L2β−/− mice. Conclusion: The study indicate that the induction of β-cell dedifferentiation mediated by ERK/MAPK signaling pathway might be an essential component of TCF7L2 variants in the development of diabetes. Plain Language Summary: Inhibitory effect of TCF7L2 on pancreatic β-cell dedifferentiation via ERK/MAPK signaling pathway in diabetes Transcription factor 7-like 2 (TCF7L2) variants seem to affect diabetes susceptibility through β-cell dysfunction, underlying basis of which has been considered to be β-cell dedifferentiation rather than apoptotic β-cell death. Nowadays, how TCF7L2 participates in β-cell dedifferentiation and how pancreatic TCF7L2 protein changes during diabetes progression are poorly understood. The Extracellular regulated protein kinases/Mitogen-activated protein kinase signaling pathway (ERK/MAPK signaling pathway) has been confirmed to be significantly associated with multiple cellular process, including cellular dedifferentiation. Here, we demonstrated that impaired TCF7L2 induces β-cell dedifferentiation and decreases insulin secretion of MIN6 cells via ERK/MAPK signaling pathway. Consistently, declined pancreatic TCF7L2 protein in parallel with reduced mature β-cells were observed in db / db mice after weeks of normal or high-fat diet feeding. Furthermore, the role of TCF7L2 in dedifferentiation and glucose homeostasis were validated in mice with β cell-specific TCF7L2 deletion (TCF7L2β−/−). In conclusion, the study indicate that the induction of β-cell dedifferentiation mediated by ERK/MAPK signaling pathway might be an essential component of TCF7L2 variants in the development of diabetes. [ABSTRACT FROM AUTHOR]

Published

2024

24. miR‐30c‐5p inhibits esophageal squamous cell carcinoma progression by repressing the PI3K/AKT signaling pathway.

Author

Shi, Haochun, Pan, Binyang, Liang, Jiaqi, Cai, Benjie, Wu, Gujie, Bian, Yunyi, Shan, Guangyao, Ren, Shencheng, Huang, Yiwei, and Guo, Weigang

Subjects

*SQUAMOUS cell carcinoma, *BIOLOGICAL models, *WOUND healing, *CANCER invasiveness, *RESEARCH funding, *MICRORNA, *CELL proliferation, *CELLULAR signal transduction, *CELL motility, *DESCRIPTIVE statistics, *MICE, *BIOINFORMATICS, *ANIMAL experimentation, *WESTERN immunoblotting, *PHOSPHOTRANSFERASES, *TRANSFERASES, *ESOPHAGEAL cancer, *DISEASE progression

Abstract

Background: Esophageal squamous cell carcinoma (ESCC) is one of the most common malignant tumors, with high incidence and poor prognosis. Revealing mechanisms of ESCC progression and developing new therapeutic targets remains crucial. The aim of this study was to elucidate the molecular mechanism of miR‐30c‐5p in regulating the malignant progression of ESCC. Methods: TCGA, GEO, and other datasets were used to analyze the differential expression of miR‐30c‐5p in ESCC and adjacent tissues, and its impact on prognosis. Then the effects of miR‐30c‐5p on the proliferation, migration, and invasion of TE‐1 and Eca9706 cells were investigated through proliferation experiments, transwell and wounding healing assays. The regulatory mechanism of miR‐30c‐5p on the PI3K/AKT signaling pathway and its interaction in cancer progression were investigated through Western blots, dual‐luciferase reporter assay, and rescue experiments. Results: miR‐30c‐5p was significantly downregulated in ESCC tissue and represented a poor prognosis. miR‐30c‐5p mimic significantly inhibited the proliferation, migration, and invasion ability of ESCC, while miR‐30c‐5p inhibitor significantly promoted tumor cell progression. Through bioinformatic analysis and experimental results, miR‐30c‐5p interacted directly with PIK3CA mRNA and inhibited subsequent signaling pathway activation. PIK3CA activator could eliminate the inhibitory effects of miR‐30c‐5p mimic on the progression of ESCC, while PIK3CA inhibitors could rescue the promoting effect of miR‐30c‐5p inhibitor group cells. Conclusions: In summary, we found that miR‐30c‐5p inhibited the proliferation, invasion and migration of ESCC by inhibiting PI3K/AKT signaling pathway for the first time, and this study is expected to provide a novel insight and potential therapeutic target for managing ESCC. [ABSTRACT FROM AUTHOR]

Published

2024

25. Identification of key proteins in early-onset Alzheimer's disease based on WGCNA.

Author

Dazhi Li, Yaxin Wang, Jinliang Wang, and Qiqiang Tang

Subjects

BIOLOGICAL models, ALZHEIMER'S disease, T-test (Statistics), RESEARCH funding, BRAIN, GENETIC markers, CHI-squared test, AGE factors in disease, MICE, PROTEOMICS, GENE expression profiling, ANIMAL experimentation, DATA analysis software, DISEASE progression, IMMUNOBLOTTING, ALGORITHMS

Abstract

Introduction: Early-onset Alzheimer's disease (EOAD) is sporadic, highly heterogeneous, and its underlying pathogenic mechanisms remain largely elusive. Proteomics research aims to uncover the biological processes and key proteins involved in disease progression. However, no proteomic studies to date have specifically focused on EOAD brain tissue. Method: We integrated proteomic data from brain tissues of two Alzheimer's disease (AD) cohorts and constructed a protein co-expression network using weighted gene co-expression network analysis (WGCNA). We identified modules associated with EOAD, conducted functional enrichment analysis to understand the biological processes involved in EOAD, and pinpointed potential key proteins within the core modules most closely linked to AD pathology. Results: In this study, we identified a total of 2,749 proteins associated with EOAD. Through protein co-expression network analysis, we discovered 41 distinct co-expression modules. Notably, the proteins within the core module most closely linked to AD pathology were significantly enriched in neutrophil degranulation. Additionally, we identified two potential key proteins within this core module that have not been previously reported in AD and validated their expression levels in 5xFAD mice. Conclusion: In summary, through a protein co-expression network analysis, we identified EOAD-related biological processes and molecular pathways, and screened and validated two key proteins, ERBB2IP and LSP1. These proteins may play an important role in the progression of EOAD, suggesting they could serve as potential therapeutic targets for the disease. [ABSTRACT FROM AUTHOR]

Published

2024

26. Deep-learning-derived input function in dynamic [18F]FDG PET imaging of mice.

Author

Kuttner, Samuel, Luppino, Luigi T., Convert, Laurence, Sarrhini, Otman, Lecomte, Roger, Kampffmeyer, Michael C., Sundset, Rune, and Jenssen, Robert

Subjects

GLUCOSE metabolism, BIOLOGICAL models, BLOOD gases analysis, RADIOPHARMACEUTICALS, PREDICTION models, HUMAN services programs, RESEARCH funding, DEOXY sugars, DYNAMICS, ISOFLURANE, POSITRON emission tomography, FUNCTIONAL status, RETROSPECTIVE studies, RADIOISOTOPES, CATHETERIZATION, MICE, DEEP learning, SPINAL fusion, ANIMAL experimentation, MEDICAL records, ACQUISITION of data, RESEARCH methodology, DIGITAL image processing, REGRESSION analysis

Abstract

Dynamic positron emission tomography and kinetic modeling play a critical role in tracer development research using small animals. Kinetic modeling from dynamic PET imaging requires accurate knowledge of an input function, ideally determined through arterial blood sampling. Arterial cannulation in mice, however, requires complex, time-consuming and terminal surgery, meaning that longitudinal studies are impossible. The aim of the current work was to develop and evaluate a non-invasive, deep-learning-based prediction model (DLIF) that directly takes the PET data as input to predict a usable input function. We first trained and evaluated the DLIF model on 68 [18F] Fluorodeoxyglucose mouse scans with image-derived targets using cross validation. Subsequently, we evaluated the performance of a trained DLIF model on an external dataset consisting of 8 mouse scans where the input function was measured by continuous arterial blood sampling. The results showed that the predicted DLIF and image-derived targets were similar, and the net influx rate constants following from Patlak modeling using DLIF as input function were strongly correlated to the corresponding values obtained using the image-derived input function. There were somewhat larger discrepancies when evaluating the model on the external dataset, which could be attributed to systematic differences in the experimental setup between the two datasets. In conclusion, our non-invasive DLIF prediction method may be a viable alternative to arterial blood sampling in small animal [18F]FDG imaging. With further validation, DLIF could overcome the need for arterial cannulation and allow fully quantitative and longitudinal experiments in PET imaging studies of mice. [ABSTRACT FROM AUTHOR]

Published

2024

27. The Alzheimer's disease 5xFAD mouse model is best suited to investigate pretargeted imaging approaches beyond the blood-brain barrier.

Author

Lopes van den Broek, Sara, Sehlin, Dag, Andersen, Jens V., Aldana, Blanca I., Beschörner, Natalie, Nedergaard, Maiken, Knudsen, Gitte M., Syvänen, Stina, and Herth, Matthias M.

Subjects

ALZHEIMER'S disease diagnosis, BIOLOGICAL models, TRANSGENIC animals, RESEARCH funding, BLOOD-brain barrier, IMMUNOGLOBULINS, BRAIN, POSITRON emission tomography, LIGATURE (Surgery), IN vivo studies, MICE, ANIMAL experimentation, EARLY diagnosis, COMPARATIVE studies, GENETIC mutation, CEREBELLUM, AMYLOID beta-protein precursor, CONTRAST media

Abstract

Alzheimer's disease (AD) is the most common neurodegenerative disease, with an increasing prevalence. Currently, there is no ideal diagnostic molecular imaging agent for diagnosing AD. Antibodies (Abs) have been proposed to close this gap as they can bind selectively and with high affinity to amyloid β (Aβ)--one of the molecular hallmarks of AD. Abs can even be designed to selectively bind Aβ oligomers or isoforms, which are difficult to target with small imaging agents. Conventionally, Abs must be labeled with long-lived radionuclides which typically results in in high radiation burden to healthy tissue. Pretargeted imaging could solve this challenge as it allows for the use of short-lived radionuclides. To develop pretargeted imaging tools that can enter the brain, AD mouse models are useful as they allow testing of the imaging approach in a relevant animal model that could predict its clinical applicability. Several mouse models for AD have been developed with different characteristics. Commonly used models are: 5xFAD, APP/PS1 and tg-ArcSwe transgenic mice. In this study, we aimed to identify which of these models were best suited to investigate pretargeted imaging approaches beyond the blood brain barrier. We evaluated this by pretargeted autoradiography using the Aβ-targeting antibody 3D6 and an 111In-labeled Tz. Evaluation criteria were target-to-background ratios and accessibility. APP/PS1 mice showed Aβ accumulation in high and low binding brain regions and is as such less suitable for pretargeted purposes. 5xFAD and tg-ArcSwe mice showed similar uptake in high binding regions whereas low uptake in low binding regions and are better suited to evaluate pretargeted imaging approaches. 5xFAD mice are advantaged over tg-ArcSwe mice as pathology can be traced early (6 months compared to 18 months of age) and as 5xFAD mice are commercially available. [ABSTRACT FROM AUTHOR]

Published

2024

28. Gardenia jasminoides extract mitigates acetaminophen-induced liver damage in mice.

Author

Tangpradubkiat, Peenaprapa, Chayanupatkul, Maneerat, Werawatganone, Pornpen, Somanawat, Kanjana, Siriviriyakul, Prasong, Klaikeaw, Naruemon, and Werawatganon, Duangporn

Subjects

ANTI-inflammatory agents, FRUIT, BIOLOGICAL models, HEPATOTOXICOLOGY, RADIOIMMUNOASSAY, DATA analysis, RESEARCH funding, KRUSKAL-Wallis Test, FISHER exact test, ASPARTATE aminotransferase, TREATMENT effectiveness, DESCRIPTIVE statistics, PLANT extracts, MICE, ANTIOXIDANTS, ANIMAL experimentation, HISTOLOGICAL techniques, ONE-way analysis of variance, STATISTICS, ALANINE aminotransferase, LIVER, DATA analysis software, MALONDIALDEHYDE, INTERLEUKINS, TUMOR necrosis factors, PHARMACODYNAMICS

Abstract

Background: Acetaminophen (APAP)-induced hepatotoxicity is a potentially life-threatening condition. Gardenia jasminoides fruit extract (GJE), which contains geniposide (Gen) as its major active constituent, possesses anti-inflammatory and antioxidant properties and may help address the underlying pathogenesis of APAP-induced hepatotoxicity. This study aimed to evaluate the effects of GJE in a mouse model of APAP-induced hepatotoxicity. Methods: Twenty-four male ICR mice were divided into 4 groups (n = 6/group): [1] Control group, mice were given distilled water; [2] APAP group, mice received a single dose of 600 mg/kg APAP; [3] APAP + low-dose GJE group, mice received APAP followed 30 min later by 2 doses of low-dose GJE (0.44 g/kg/dose, containing Gen 100 mg/kg/dose) 8 h apart; [4] APAP + high-dose GJE group, mice received APAP followed by 2 doses of high-dose GJE (0.88 g/kg/dose, containing Gen 200 mg/kg/dose). All mice were euthanized 24 h after APAP administration. Liver tissue was used for histological examination and to measure glutathione (GSH) and malondialdehyde (MDA) levels. Serum was used to determine levels of ALT and inflammatory cytokines (tumor necrosis factor- α (TNF-α) and interleukin-6 (IL-6)). Results: Liver histopathology showed moderate to severe hepatic necroinflammation in the APAP group, whereas only mild necroinflammation was observed in both treatment groups. Serum ALT levels were significantly elevated in the APAP group compared to the control group but were significantly reduced after low- and high-dose GJE treatment. Serum TNF- α levels were significantly higher in the APAP group than in the control group and were significantly lower after high-dose GJE treatment (135.5 ± 477.2 vs. 35.5 ± 25.8 vs. 74.7 ± 47.2 vs. 41.4 ± 50.8 pg/mL, respectively). Serum IL-6 followed a similar pattern. Hepatic GSH levels were significantly lower in the APAP group compared to the control group but significantly increased after both low- and high-dose GJE treatment (19.9 ± 4.5 vs. 81.5 ± 12.4 vs. 71.4 ± 7.8 vs. 82.6 ± 6.6 nmol/mg protein, respectively). Conversely, hepatic MDA levels were significantly elevated in the APAP group compared with the control group but significantly decreased after high-dose GJE treatment (108.6 ± 201.5 vs. 40.5 ± 18.0 vs. 40.5 ± 16.8 nmol/mg protein, respectively). Conclusions: Treatment with G. jasminoides fruit extract can alleviate APAP-induced hepatotoxicity, likely through its anti-inflammatory and antioxidant properties. [ABSTRACT FROM AUTHOR]

Published

2024

29. Comparative Study of Cutaneous Squamous Cell Carcinogenesis in Different Hairless Murine Models.

Author

Gkikas, Georgios, Katsiris, Dimitrios, Vitsos, Andreas, Gioran, Anna, Ieronymaki, Dimitra, Kostaki, Maria, Ladopoulos, Georgios, Ioannidou, Vaya, Theodoraki, Elisavet, Chondrogianni, Niki, Sfiniadakis, Ioannis, Papaioannou, Georgios T., and Rallis, Michail Christou

Subjects

*SQUAMOUS cell carcinoma, *BIOLOGICAL models, *PATIENT selection, *RISK assessment, *HYPERCHOLESTEREMIA, *CANCER invasiveness, *HUMAN research subjects, *MELANINS, *BALDNESS, *ULTRAVIOLET radiation, *IN vivo studies, *MICE, *ANIMAL experimentation, *PROTEOLYTIC enzymes, *CHOLESTEROL, *COMPARATIVE studies, *DISEASE incidence, *IMMUNOSUPPRESSION, *DISEASE risk factors

Abstract

Simple Summary: Animal models are crucial for exploration of the causes of and potential treatments for squamous cell carcinoma, a common type of skin cancer. This study compared four different hairless mouse models to determine which is most suitable for studying skin cancer development when exposed to ultraviolet (UV) light. The models varied in their skin characteristics, such as the presence of melanin, cholesterol level, and immune system function. By monitoring various skin health parameters and analyzing proteasome activity, this study found that the SKH-hr2+ApoE and SKH-hr2 models were the most effective for further research into squamous cell carcinoma. In contrast, the SKH-hr1 model, despite its common use, was less suitable. These findings will help guide future research efforts in understanding and developing treatments for skin cancer. Background: In recent decades, a significant global increase in the incidence of non-melanoma skin cancer has been observed. To explore the pathogenesis of and potential therapeutic approaches for squamous cell carcinoma, various in vivo studies using mouse models have been conducted. However, investigations comparing different hairless mouse models, with or without melanin, as well as models with hypercholesterolemia and immunosuppression, in terms of their ability to induce squamous cell carcinoma have yet to be undertaken. Methods: Four mouse strains, namely SKH-hr1, SKH-hr2, SKH-hr2+ApoE, and immunodeficient Nude (Foxn1 knockout), were exposed to UVA and UVB radiation three times per week, initially to 1 Minimal Erythemal Dose (MED), incrementally increased weekly to a maximum dose of 3 MED. Clinical evaluation, photodocumentation, and biophysical parameters were monitored, along with proteasome protein activity and histopathological assessments. Results: The SKH-hr1 model primarily developed actinic keratosis without significant progression to invasive squamous cell carcinoma (SCC), while the SKH-hr2 and SKH-hr2+ApoE models exhibited a higher likelihood and intensity of papilloma and aggressive SCC formation, with the latter showing upregulated proteasome activity. Histopathological analysis confirmed the presence of poorly differentiated, invasive SCCs in the SKH-hr2 and SKH-hr2+ApoE models, contrasting with the less aggressive SCCs in the Nude mice and the mixed lesions observed in the SKH-hr1 mice. Conclusions: The SKH-hr2+ApoE and SKH-hr2 mice were identified as the most suitable for further exploration of squamous cell carcinogenesis. In contrast, the SKH-hr1 mice were found to be the least suitable, even though they are albino. Notably, proteasome analysis revealed a potential role of proteasome activity in squamous cell carcinogenesis. [ABSTRACT FROM AUTHOR]

Published

2024

30. Targeting the Leloir Pathway with Galactose-Based Antimetabolites in Glioblastoma.

Author

Sharpe, Martyn A., Ijare, Omkar B., Raghavan, Sudhir, Baskin, Alexandra M., Baskin, Brianna N., and Baskin, David S.

Subjects

*BIOLOGICAL models, *TISSUE arrays, *GLIOMAS, *ANTIMETABOLITES, *GLYCOSYLATION, *RESEARCH funding, *LECTINS, *DATA analysis, *T-test (Statistics), *IN vivo studies, *DESCRIPTIVE statistics, *POLYSACCHARIDES, *MICE, *ANIMAL experimentation, *WESTERN immunoblotting, *MOLECULAR structure, *STATISTICS, *SURVIVAL analysis (Biometry), *CELL survival, *MICROSCOPY

Abstract

Simple Summary: Glioblastoma (GBM) uses the Leloir pathway to catabolize D-Galactose (Gal) for tumor growth. Selective targeting of the Leloir pathway with Gal-based antimetabolites has potential for the treatment of GBM. Here, we tested the effect of a Gal-based antimetabolite, 4-deoxy-4-fluorogalactose (4DFG) on the viability and metabolism of GBM cells in culture. 4DFG is a good Glut3/Glut14 substrate and acts as a potent glioma chemotherapeutic. GBM cell cultures were used to examine toxicity and alterations in glycan composition. 4DFG is moderately potent against GBM cells in vitro (IC50: 125–300 µM). Glycosylation in GBM was disrupted by 4DFG. The effect of 4DFG on D-glucose (Glc) metabolism in GBM cells was assessed by using 13C NMR-based tracer studies. 13C-NMR-based metabolic flux analysis revealed that both glycolytic and mitochondrial metabolic fluxes of [U-13C]Glc were significantly decreased in the presence of 4DFG in GBM cells. Survival analysis in an intracranial mouse model during treatment with 4DFG (6 × 25 mg/kg of 4DFG, intravenously) showed improved outcomes by three-fold (p < 0.01). 4DFG is metabolized by GBM in vitro and in vivo, and is lethal to GBM tumors, but well tolerated in mice. A functional Gal-scavenging pathway in GBM allows Gal-based antimetabolites to act as chemotherapeutics. Background: Glioblastoma (GBM) uses Glut3 and/or Glut14 and the Leloir pathway to catabolize D-Galactose (Gal). UDP-4-deoxy-4-fluorogalactose (UDP-4DFG) is a potent inhibitor of the two key enzymes, UDP-galactose-4-epimerase (GALE) and UDP-Glucose 6-dehydrogenase (UGDH), involved in Gal metabolism and in glycan synthesis. The Gal antimetabolite 4-deoxy-4-fluorogalactose (4DFG) is a good substrate for Glut3/Glut14 and acts as a potent glioma chemotherapeutic. Methods: Primary GBM cell cultures were used to examine toxicity and alterations in glycan composition via lectin binding in fixed cells and by Western blots. Toxicity/efficacy in vivo data was performed in mouse flank and intracranial models. The effect of 4DFG on D-glucose (Glc) metabolism in GBM cells was assessed by using 13C NMR-based tracer studies. Results: 4DFG is moderately potent against GBM cells (IC50: 125–300 µM). GBM glycosylation is disrupted by 4DFG. Survival analysis in an intracranial mouse model showed that treatment with 4DFG (6 × 25 mg/kg of 4DFG, intravenously) improved outcomes by three-fold (p < 0.01). Metabolic flux analysis revealed that both glycolytic and mitochondrial metabolic fluxes of [U-13C]Glc were significantly decreased in the presence of 4DFG in GBM cells. Conclusion: A functional Gal-scavenging pathway in GBM allows Gal-based antimetabolites to act as chemotherapeutics. 4DFG is metabolized by GBM in vitro and in vivo, is lethal to GBM tumors, and is well tolerated in mice. [ABSTRACT FROM AUTHOR]

Published

2024

31. CCL21 Induces Plasmacytoid Dendritic Cell Migration and Activation in a Mouse Model of Glioblastoma.

Author

Zhao, Lei, Shireman, Jack, Probelsky, Samantha, Rigg, Bailey, Wang, Xiaohu, Huff, Wei X., Kwon, Jae H., and Dey, Mahua

Subjects

*CHEMOKINES, *BIOLOGICAL models, *IMMUNOLOGICAL tolerance, *GLIOMAS, *CARRIER proteins, *T cells, *RESEARCH funding, *CELL motility, *CELLULAR signal transduction, *CELL lines, *MICE, *ANIMAL experimentation, *DENDRITIC cells, *IMMUNOSUPPRESSION

Abstract

Simple Summary: Glioblastoma is known to be highly immunosuppressive in nature. Plasmacytoid dendritic cell infiltration is known to be associated with glioblastoma progression and promotes tumor immunosuppression. We provide important details to indicate that glioblastoma cell-secreted CCL21 plays a dual role both in recruiting plasmacytoid dendritic cells via binding to CCR7 and activating plasmacytoid dendritic cells through the CCR7/ACKR4—β-arrestin/CIITA pathway. Our result also provides a rationale to therapeutically target CCL21 as a potential novel treatment for glioblastoma. Dendritic cells (DCs) are professional antigen-presenting cells that are traditionally divided into two distinct subsets: myeloid DCs (mDCs) and plasmacytoid DCs (pDCs). pDCs are known for their ability to secrete large amounts of cytokine type I interferons (IFN- α). In our previous work, we have demonstrated that pDC infiltration promotes glioblastoma (GBM) tumor immunosuppression through decreased IFN-α secretion via TLR-9 signaling and increased suppressive function of regulatory T cells (Tregs) via increased IL-10 secretion, resulting in poor overall outcomes in mouse models of GBM. Further dissecting the overall mechanism of pDC-mediated GBM immunosuppression, in this study, we identified CCL21 as highly upregulated by multiple GBM cell lines, which recruit pDCs to tumor sites via CCL21-CCR7 signaling. Furthermore, pDCs are activated by CCL21 in the GBM microenvironment through intracellular signaling of β-arrestin and CIITA. Finally, we found that CCL21-treated pDCs directly suppress CD8+ T cell proliferation without affecting regulatory T cells (Tregs) differentiation, which is considered the canonical pathway of immunotolerant regulation. Taken together, our results show that pDCs play a multifaced role in GBM immunosuppression, and CCL21 could be a novel therapeutic target in GBM to overcome pDC-mediated immunosuppression. [ABSTRACT FROM AUTHOR]

Published

2024

32. Dendritic Cells Loaded With Heat Shock Inactivated Glioma Stem Cells Enhance Antitumor Response of Mouse Glioma When Combining With CD47 Blockade.

Author

Tan, Qijia, Li, Feng, Wang, Jun, Liu, Yi, Cai, Yingqian, Zou, Yuxi, and Jiang, Xiaodan

Subjects

*BIOLOGICAL models, *FLOW cytometry, *IMMUNIZATION, *IN vitro studies, *T-cell lymphoma, *GLIOMAS, *MONOCYTES, *RESEARCH funding, *PHYSIOLOGICAL effects of heat, *IMMUNOTHERAPY, *TREATMENT effectiveness, *CANCER vaccines, *IN vivo studies, *DESCRIPTIVE statistics, *MICE, *MEMBRANE glycoproteins, *ANIMAL experimentation, *CELL death, *STEM cells, *TUMOR antigens, *DENDRITIC cells

Abstract

Background: For glioma patients, the long-term advantages of dendritic cells (DCs) immunization remain unknown. It is extremely important to develop new treatment strategies that enhance the immunotherapy effect of DC-based vaccines. DCs exposed to glioma stem cells (GSCs) are considered promising vaccines against glioma. Methods: Glioma stem cells were isolated from mouse glioma GL261 cells (GCs). Both were subjected to severe (47°C) and mild (42°C) heat shock to induce immunogenic cell death (ICD). Membrane mobilization of calreticulin (CRT) and release of heat shock proteins (HSPs) were detected by flow cytometry. Dendritic cells were then exposed to heat-inactivated cells and co-culturing of T cells tested for immunotherapeutic efficacy in vitro. In vivo, we investigated the GSC targeting effect of the GSC-DC vaccine combined with CD47 blockade. Results: Heat shock induced ICD in GCs and GSCs, as indicated by significant release of calreticulin, HSP70, and HSP90. Heat shock condition ICD lysates induce maturation and activation-associated marker expression on monocyte-derived DCs. Accordingly, DCs pulsed with GCs and GSCs inactivated reduced colony formation, sphere formation, migration, and invasion of glioma and GSCs in vitro. Glioma stem cell-DC vaccine in combination with anti-CD47 antibody significantly enhanced survival in mice with glioma, induced production of interferon (IFN)-γ, and enhanced T-cell expansion in vivo. Of note, DCs pulsed with inactivated GSCs were more effective to control tumor growth than DCs pulsed with inactive GCs. Conclusions: Severe heat shock induces ICD in vitro. These data showed that administration of anti-CD47 antibody combined with GSC-DC vaccine may represent an effective immunotherapeutic strategy for cancer patients in clinical. [ABSTRACT FROM AUTHOR]

Published

2024

33. Mixture prior distributions and Bayesian models for robust radionuclide image processing.

Author

Muyang Zhang, Aykroyd, Robert G., and Tsoumpas, Charalampos

Subjects

STATISTICAL models, BIOLOGICAL models, POISSON distribution, DIAGNOSTIC imaging, CLUSTER analysis (Statistics), DATA analysis, PROBABILITY theory, RESEARCH evaluation, DESCRIPTIVE statistics, MICE, SIMULATION methods in education, ANIMAL experimentation, STATISTICS, DIGITAL image processing, MACHINE learning, RADIONUCLIDE imaging, ALGORITHMS, SENSITIVITY & specificity (Statistics)

Abstract

The diagnosis of medical conditions and subsequent treatment often involves radionuclide imaging techniques. To refine localisation accuracy and improve diagnostic confidence, compared with the use of a single scanning technique, a combination of two (or more) techniques can be used but with a higher risk of misalignment. For this to be reliable and accurate, recorded data undergo processing to suppress noise and enhance resolution. A step in image processing techniques for such inverse problems is the inclusion of smoothing. Standard approaches, however, are usually limited to applying identical models globally. In this study, we propose a novel Laplace and Gaussian mixture prior distribution that incorporates different smoothing strategies with the automatic model-based estimation of mixture component weightings creating a locally adaptive model. A fully Bayesian approach is presented using multi-level hierarchical modelling and Markov chain Monte Carlo (MCMC) estimation methods to sample from the posterior distribution and hence perform estimation. The proposed methods are assessed using simulated γ-eye™ camera images and demonstrate greater noise reduction than existing methods but without compromising resolution. As well as image estimates, the MCMC methods also provide posterior variance estimates and hence uncertainty quantification takes into consideration any potential sources of variability. The use of mixture prior models, part Laplace random field and part Gaussian random field, within a Bayesian modelling approach is not limited to medical imaging applications but provides a more general framework for analysing other spatial inverse problems. Locally adaptive prior distributions provide a more realistic model, which leads to robust results and hence more reliable decision-making, especially in nuclear medicine. They can become a standard part of the toolkit of everyone working in image processing applications. [ABSTRACT FROM AUTHOR]

Published

2024

34. "Huanglianjiedu Decoction" Against Pancreatic Adenocarcinoma Proliferation of by Downregulating the PI3K/AKT/mTOR and MAPK/ERK1/2 Signaling Pathways.

Author

Dong, MD, Shu, Xu, MD, Panling, Yang, MD, Peiwen, Jiao, MD, Juying, Cheng, MD, PhD, Chien-shan, and Chen, MD, PhD, Lianyu

Subjects

ADENOCARCINOMA, CHINESE medicine, MITOGEN-activated protein kinases, IN vitro studies, BIOLOGICAL models, RESEARCH funding, PHENOMENOLOGICAL biology, T-test (Statistics), CELL proliferation, HERBAL medicine, ANIMALS, CELLULAR signal transduction, IN vivo studies, BIOCHEMISTRY, DESCRIPTIVE statistics, PANCREATIC tumors, CELL lines, MICE, MASS spectrometry, ONCOGENES, ANALYSIS of variance, TRANSFERASES, STAINS & staining (Microscopy), COMPARATIVE studies, INTERLEUKINS, DISEASE progression

Abstract

Background: Huanglianjiedu decoction (HLJDD) is a classical Traditional Chinese Medicine (TCM) prescription with thousand years of clinical use against various malignancies, including pancreatic adenocarcinoma (PAAD). However, its potential bioactive component and molecular mechanism remains unclear. Aims: This study is to inspect the HLJDD mechanisms of action against PAAD via integrated computational and pharmacochemistry strategy, in vivo and in vitro experiments to validate associated targets and pathways. Methods: A PAAD xenograft model was established by subcutaneous injecting Panc02 cells into C57BL/6 mice. Ultra-high performance liquid chromatography with tandem mass spectrometry (UHPLC-MS/MS) was engaged to determine constituents of HLJDD and assessed for pharmacokinetic scheme using the TCM Systems Pharmacology Platform (TCM-SP). Differentially expressed genes (DEGs) of PAAD was retrieved from the transcriptome dataset GSE43795, followed by recognizing overlapping targets the oncogenes and target genes of PAAD and HLJDD, respectively. Putative signaling pathways of HLJDD in treating PAAD were enriched using KEGG and GO analyses. The anti-PAAD effects of HLJDD was assessed in vivo and in vitro, besides, the potential mechanism was validated using immunoblotting and immunohistochemical assays. Results: HLJDD significantly suppressed the growth of transplanted PAAD tumors, constrained PAAD progression, and induced apoptosis and S-phase arrest. Seventy-five active components meeting the drug-likeness criteria and 278 target genes of HLJDD were identified. KEGG analysis indicated that the top three enriched pathways were cancer, AGE-RAGE signaling, and IL-17 signaling pathways. Disease enrichment analysis highlighted immune, pharmacological, and cancer-related diseases as the top three categories. A total of 47 potential target genes were identified. Immunoblotting revealed that HLJDD inhibited PI3K and MAPK-related signaling pathways, while immunohistochemical staining confirmed that HLJDD suppressed the expression of phosphorylated MAPK and ERK1/2. Conclusion: HLJDD inhibited PAAD in vitro and in vivo via the modulation of multiple mechanisms, including regulation of PI3K/AKT/mTOR and MAPK/ERK1/2 signaling pathways. [ABSTRACT FROM AUTHOR]

Published

2024

35. Enhancement of cognitive function in mice with Alzheimer's disease through hyperbaric oxygen-induced activation of cellular autophagy.

Author

Qian-Qian Fan, Yong-Min Chen, Yong-Sen Fu, Xiao-Shan Li, Ji Zeng, Shao-Zhen Bian, Bin-Bin Li, and Zhen-Hua Song

Subjects

ALZHEIMER'S disease treatment, BIOLOGICAL models, PROTEINS, COGNITIVE testing, AUTOPHAGY, ALZHEIMER'S disease, RESEARCH funding, TREATMENT effectiveness, CELLULAR signal transduction, DESCRIPTIVE statistics, MICE, IMMUNOHISTOCHEMISTRY, GENE expression, ANIMAL experimentation, WESTERN immunoblotting, HYPERBARIC oxygenation, STAINS & staining (Microscopy), DATA analysis software, COMPARATIVE studies, MOLECULAR pathology

Abstract

Objective: In this study, we examined the effectiveness of hyperbaric oxygen (HBO) therapy in ameliorating cognitive deficits in mice with Alzheimer's disease (AD), while also assessing its impact on the autophagic pathway within the context of AD. Methods: 20 double-transgenic mice expressing the amyloid precursor protein and presenilin 1 (APP/PS1) were purposefully selected and randomly assigned to groups A and B. Concurrently, 20 C57BL/6 mice were chosen and randomly categorized into groups C and D, each consisting of 10 mice. Mice in groups B and D received HBO treatment. The Morris water maze assay was used to assess changes in mouse behavior. Immunohistochemistry techniques were used to quantify the expression levels of amyloid-beta 42 (Ab42) and microtubuleassociated protein 1A/1B-light chain 3 (LC3) in hippocampal tissues, while western blot analysis was used to investigate the levels of LC3-II, p62, phosphoinositide 3-kinase (PI3K), and mammalian target of rapamycin (mTOR) proteins within hippocampal tissues. Results: Mice allocated to group B exhibited reduced escape latency and prolonged dwell time in the target quadrant compared to other groups. Histological examination revealed conspicuous plaque-like deposits of Ab42 in the hippocampal tissues of mice in groups A and B. Group B displayed diminished Ab42-positive reactants and augmented microtubule-associated protein 1A/1B-LC3-positive reactants compared to group A. LC3-positive reactants were also detected in the hippocampal tissues of mice in groups C and D, surpassing the levels observed in groups A and B. Furthermore, group B demonstrated significantly lower expression of mTOR protein and markedly higher expression of LC3-II protein in mouse hippocampal tissues when compared to group A (P < 0.05). Conversely, there were no significant disparities noted in PI3K and p62 protein expression between groups B and A. Notably, no discernible discrepancies were observed in the expression levels of mTOR, PI3K, LC3-II, and p62 proteins between groups C and D within mouse hippocampal tissues. Conclusion: HBO treatment demonstrates efficacy in enhancing cognitive function in mice with AD and holds promise as a potential therapeutic intervention for AD by facilitating the activation of the mTOR pathwaymediated autophagy. [ABSTRACT FROM AUTHOR]

Published

2024

36. Targeting IGF1/IGF1r signaling relieve pain and autophagic dysfunction in NTG-induced chronic migraine model of mice.

Author

Wang, Tianxiao, Zhu, Chenlu, zhang, Kaibo, Gao, Jinggui, Xu, Yunhao, Duan, Chenyang, Wu, Shouyi, Peng, Cheng, Guan, Jisong, and Wang, Yonggang

Subjects

*BIOLOGICAL models, *AUTOPHAGY, *INTRAPERITONEAL injections, *PHOSPHORYLATION, *T-test (Statistics), *RESEARCH funding, *CELL proliferation, *NEURONS, *POLYMERASE chain reaction, *CELLULAR signal transduction, *NITROGLYCERIN, *ALLERGIES, *CALCITONIN, *FLUORESCENT antibody technique, *MANN Whitney U Test, *DESCRIPTIVE statistics, *GENE expression, *MICE, *MESSENGER RNA, *PAIN, *ANIMAL experimentation, *WESTERN immunoblotting, *SOMATOMEDIN, *DATA analysis software, *MIGRAINE, *ALLODYNIA, *NONPARAMETRIC statistics

Abstract

Background: Chronic migraine is a severe and common neurological disorder, yet its precise physiological mechanisms remain unclear. The IGF1/IGF1r signaling pathway plays a crucial role in pain modulation. Studies have shown that IGF1, by binding to its receptor IGF1r, activates a series of downstream signaling cascades involved in neuronal survival, proliferation, autophagy and functional regulation. The activation of these pathways can influence nociceptive transmission. Furthermore, alterations in IGF1/IGF1r signaling are closely associated with the development of various chronic pain conditions. Therefore, understanding the specific mechanisms by which this pathway contributes to pain is of significant importance for the development of novel pain treatment strategies. In this study, we investigated the role of IGF1/IGF1r and its potential mechanisms in a mouse model of chronic migraine. Methods: Chronic migraine was induced in mice by repeated intraperitoneal injections of nitroglycerin. Mechanical and thermal hypersensitivity responses were assessed using Von Frey filaments and radiant heat, respectively. To determine the role of IGF1/IGF1r in chronic migraine (CM), we examined the effects of the IGF1 receptor antagonist ppp (Picropodophyllin) on pain behaviors and the expression of calcitonin gene-related peptide (CGRP) and c-Fos. Result: In the nitroglycerin-induced chronic migraine model in mice, neuronal secretion of IGF1 is elevated within the trigeminal nucleus caudalis (TNC). Increased phosphorylation of the IGF1 receptor occurs, predominantly co-localizing with neurons. Treatment with ppp alleviated basal mechanical hypersensitivity and acute mechanical allodynia. Furthermore, ppp ameliorated autophagic dysfunction and reduced the expression of CGRP and c-Fos. Conclusion: Our findings demonstrate that in the chronic migraine (CM) model in mice, there is a significant increase in IGF1 expression in the TNC region. This upregulation of IGF1 leads to enhanced phosphorylation of IGF1 receptors on neurons. Targeting and inhibiting this signaling pathway may offer potential preventive strategies for mitigating the progression of chronic migraine. [ABSTRACT FROM AUTHOR]

Published

2024

37. Proteomic analysis and experimental validation reveal the blood–brain barrier protective of Huanshaodan in the treatment of SAMP8 mouse model of Alzheimer's disease.

Author

Su, Yunfang, Liu, Ningning, Wang, Pan, Shang, Congcong, Sun, Ruiqin, Ma, Jinlian, Li, Zhonghua, Ma, Huifen, Sun, Yiran, Zhang, Zijuan, Song, Junying, Xie, Zhishen, Xu, Jiangyan, and Zhang, Zhenqiang

Subjects

*CHINESE medicine, *BIOLOGICAL models, *DONEPEZIL, *ALZHEIMER'S disease, *RESEARCH funding, *BLOOD-brain barrier, *FLUORESCENT antibody technique, *MICE, *RNA, *IMMUNOHISTOCHEMISTRY, *MEDICINAL plants, *PROTEOMICS, *ANIMAL experimentation, *MASS spectrometry, *WESTERN immunoblotting, *FLUORESCENCE in situ hybridization, *COGNITION disorders, *FIBRINOGEN, *SEQUENCE analysis

Abstract

Background: Huanshaodan (HSD) is a Chinese Herbal Compound which has a definite clinical effect on Alzheimer's disease (AD), however, the underlying mechanism remains unclear. The aim of this study is to preliminarily reveal the mechanism of HSD in the treatment of AD model of SAMP8 mice. Methods: Chemical composition of HSD and its drug-containing serum were identified by Q-Orbitrap high resolution liquid mass spectrometry. Six-month-old SAMP8 mice were treated with HSD and Donepezil hydrochloride by gavage for 2 months, and Wogonin for 28 days. Behavioral test was performed to test the learning and memory ability of mice. Immunofluorescence (IF) or Western-blot methods were used to detect the levels of pSer404-tau and β-amyloid (Aβ) in the brain of mice. Hematoxylin–eosin (H&E) staining and Transmission electron microscopy (TEM) assay was applied to observe the pathological changes of neurons. Proteomic technology was carried out to analyze and identify the protein network of HSD interventions in AD. Then the pathological process of the revealed AD-related differential proteins was investigated by IF, Q-PCR, Western-blot, Fluorescence in situ hybridization (FISH) and 16S rRNA sequencing methods. Results: The results showed that HSD and Wogonin, one of the components in its drug-containing serum, can effectively improve the cognitive impairments of SAMP8 mice, protect hippocampal neurons and synapses, and reduce the expression of pSer404-tau and Aβ. HSD and Wogonin reduced the levels of fibrinogen β chain (FGB) and γ chain (FGG), the potential therapeutic targets revealed by proteomics analysis, reduced the colocalization of FGB and FGG with Aβ, ionized calcium binding adaptor molecule 1 (Iba-1), glial fibrillary acidic protein (GFAP), increased level of and myelin basic protein (MBP). Meanwhile, HSD and Wogonin increased ZO-1 and Occludin levels, improved brain microvascular injury, and reduced levels of bacteria/bacterial DNA and lipopolysaccharide (LPS) in the brain of mice. In addition, 16S rRNA sequencing indicated that HSD regulated the structure of intestinal microbiota of mice. Conclusion: The effects of HSD on AD may be achieved by inhibiting the levels of fibrinogen and the interactions on glia cells in the brain, and by modulating the structure of intestinal microbiota and improving the blood–brain barrier function. [ABSTRACT FROM AUTHOR]

Published

2024

38. The quantification and mRNA expression levels of cochlear synapses in C57BL/6j mice following repeated exposure to noise.

Author

Qian, Minfei, Yao, Zhuowei, Wang, Qixuan, Zhou, Yaqi, Huang, Zhiwu, and Li, Jiping

Subjects

*BRAIN stem physiology, *BIOLOGICAL models, *NOISE-induced deafness, *NOISE, *RESEARCH funding, *POLYMERASE chain reaction, *NEURODEGENERATION, *FLUORESCENT antibody technique, *DESCRIPTIVE statistics, *MESSENGER RNA, *MICE, *GENE expression profiling, *ANIMAL experimentation, *DATA analysis software, *HIDDEN hearing loss, *COCHLEA, *AUDITORY evoked response, *HAIR cells

Abstract

Background: Noise-induced cochlear synaptopathy has recently emerged as a focus in hearing research. Purpose: This study aimed to examine the impact of repeated noise exposure on the quantification and mRNA expression levels of cochlear synapses. Methods: Measurements were conducted at baseline, 1 day, and 14 days post-exposure to 88 or 97 dB SPL noise (2 h/day for 7 days, frequency range 2-20 kHz). Auditory brainstem responses (ABRs), immunofluorescence and quantitative real-time PCR (qRT-PCR) were used to examine the results. Results: 1. Exposure to 88 dB SPL caused minimal changes in ABRs, ribbon morphology and medial olivocochlear (MOC) efferent synapses; elevation of synaptophysin(SYP) and α9α10 nAchR mRNA levels were observed. 2. Exposure to 97 dB SPL caused threshold shift and synaptopathy of ribbon and MOC; downregulation of α10nAchR, SYP and ctbp2 mRNA levels were observed. Conclusion: Noise-induced cochlear synaptic degeneration involves both afferent and efferent synaptopathy. [ABSTRACT FROM AUTHOR]

Published

2024

39. The Effects of Vitamin D on Movement and Cognitive Function in Senile Mice After Sevoflurane Anaesthesia.

Author

Zhang, Jialei, Zhang, Xiaoling, Zhao, Jun, and Wu, Jie

Subjects

*MOTOR ability, *BIOLOGICAL models, *SEVOFLURANE, *ENZYME-linked immunosorbent assay, *DESCRIPTIVE statistics, *MICE, *ANIMAL experimentation, *MEMORY, *VITAMIN D, *COGNITION, *OLD age

Abstract

Background: Vitamin D (VD) is a neuroactive steroid involved in many brain functions, such as neurotrophic, neuroimmune control and neurotransmission, which affects the growth and function of the brain. The purpose of this study is to explore the effect of VD on motor and cognitive function of aged mice after sevoflurane anesthesia. Method: We established sevoflurane anesthesia model and VD(-) and VD(+) mice model. The VD concentration of mice in each group was determined by enzyme-linked immunosorbent assay (ELISA). An open-field test was used to evaluate the mice's capacity for movement and exploration. A Y-maze test was used to gauge the mice's short-term memory. The primary purpose of the water-maze experiment was to examine mice's long-term spatial memory. Results: The ELISA results showed that the model was successfully constructed. In the open-field test, VD increased the exercise distance of mice (P <.05). In the Y-maze experiment, VD improved short-term memory impairment in mice (P <.05). In the water-maze test, VD increased the activity time and platform crossing number of mice in the target quadrant. (P <.05). Conclusion: Sevoflurane anesthesia caused cognitive dysfunction in aged mice, including reduced learning ability, memory loss, lower motor and exploratory abilities and depression, and VD deficiency aggravated these impairments. By supplementing with VD, learning ability and long-term memory were enhanced, motor and exploratory abilities were improved, and depression levels were reduced. Anxiety was also improved. [ABSTRACT FROM AUTHOR]

Published

2024

40. A Novel Chimeric Oncolytic Virus Mediates a Multifaceted Cellular Immune Response in a Syngeneic B16 Melanoma Model.

Author

Glauß, Sonja, Neumeyer, Victoria, Hanesch, Lorenz, Marek, Janina, Hartmann, Nina, Wiedemann, Gabriela M., and Altomonte, Jennifer

Subjects

*MELANOMA treatment, *METABOLISM in viruses, *ONCOLYTIC virotherapy, *BIOLOGICAL models, *MELANOMA, *T cells, *MONONUCLEAR leukocytes, *T-test (Statistics), *STATISTICAL significance, *RESEARCH funding, *IMMUNOTHERAPY, *IN vivo studies, *REVERSE transcriptase polymerase chain reaction, *DESCRIPTIVE statistics, *MICE, *SPLEEN, *KAPLAN-Meier estimator, *LOG-rank test, *ANIMAL experimentation, *ONE-way analysis of variance, *DATA analysis software, *VIRUSES, *IMMUNITY

Abstract

Simple Summary: Cancer immunotherapy has evolved rapidly in the last decade. A newly emerging immunotherapeutic approach utilizes oncolytic viruses to enhance the ability of the body's own immune system to recognize and clear tumor cells. We have recently developed a novel chimeric oncolytic virus and demonstrated its anti-tumoral effects in various preclinical mouse models. To gain mechanistic insights into the immune response to this form of therapy at the cellular level and to identify targets to potentially further improve the therapy, we analyzed the immune cell signature in the tumors, blood, and lymphoid tissue in a syngeneic melanoma mouse model by flow cytometry. Both local and systemic immune responses were observed. Furthermore, selective depletion of cytotoxic T cells indicated that these cells are the main players in mediating the therapeutic response to this novel virotherapy. Background/Objectives: Oncolytic virotherapy is a promising approach in cancer immunotherapy. We have previously described a recombinant hybrid oncolytic virus (OV), VSV-NDV, which has a favorable safety profile and therapeutic immunogenicity, leading to direct oncolysis, abscopal effects, and prolonged survival in syngeneic in vivo tumor models. While OVs are known to mediate systemic anti-tumor immune responses, the detailed characterization of local and systemic immune responses to fusogenic oncolytic virotherapy remains unexplored. Methods and Results: We analyzed immune cell compartments in the spleen, blood, tumor-draining lymph nodes (TDLNs), and tumors over the course of VSV-NDV therapy in a bilateral syngeneic melanoma mouse model. Our results revealed significant local infiltration and activation of T lymphocytes in tumors and globally in the blood and spleen. Notably, in vivo CD8+ T cell depletion led to complete abrogation of the tumor response, highlighting the crucial role of T cells in promoting the therapeutic effects of oncolytic VSV-NDV. In vitro co-culture experiments enabled the interrogation of human immune cell responses to VSV-NDV-mediated oncolysis. Human peripheral blood mononuclear cells (PBMCs) were efficiently stimulated by exposure to VSV-NDV-infected cancer cells, which recapitulates the in vivo murine findings. Conclusions: Taken together, these data characterize a broad anti-tumor immune cell response to oncolytic VSV-NDV therapy and suggest that CD8+ T cells play a decisive role in therapeutic outcome, which supports the further development of this chimeric vector as a multimechanistic immunotherapy for solid cancers. [ABSTRACT FROM AUTHOR]

Published

2024

41. Combined PET Radiotracer Approach Reveals Insights into Stromal Cell-Induced Metabolic Changes in Pancreatic Cancer In Vitro and In Vivo.

Author

Doctor, Alina, Laube, Markus, Meister, Sebastian, Kiss, Oliver C., Kopka, Klaus, Hauser, Sandra, and Pietzsch, Jens

Subjects

*IN vitro studies, *GLUCOSE, *BIOLOGICAL models, *RESEARCH funding, *CANCER, *ANIMALS, *CELL physiology, *POSITRON emission tomography, *RADIOISOTOPES, *DESCRIPTIVE statistics, *IN vivo studies, *TUMOR markers, *XENOGRAFTS, *PANCREATIC tumors, *MICE, *CELL lines, *FIBROBLASTS, *BIOTRANSFORMATION (Metabolism), *DUCTAL carcinoma, *STROMAL cells, *HYPOXEMIA

Abstract

Simple Summary: Pancreatic cancer is surrounded by a dense fibrotic environment due to the activity of pancreatic stellate cells (PSCs). This hinders the effectiveness of treatment by limiting drug penetration and oxygen delivery. To better understand this, PSCs and cancer cells were studied in laboratory models using radiotracer imaging techniques. The results indicated that while glucose uptake and hypoxia were similar between cancer cells alone and in combination with PSCs, a specific marker of fibrosis (FAPα) was significantly higher in PSC-rich environments. In mice, the marker in question decreased in tumors with only PSCs, indicating that the cells had died. Conversely, the biomarker increased over time in tumors containing both cancer cells and PSCs, suggesting that mouse cells had invaded. This study sheds light on how the tumor environment influences metabolism and thus provides insights for more targeted theranostic applications. In turn, this approach supports the development of more reliable models. Background/Objective Pancreatic stellate cells (PSCs) in pancreatic adenocarcinoma (PDAC) are producing extracellular matrix, which promotes the formation of a dense fibrotic microenvironment. This makes PDAC a highly heterogeneous tumor-stroma-driven entity, associated with reduced perfusion, limited oxygen supply, high interstitial fluid pressure, and limited bioavailability of therapeutic agents. Methods In this study, spheroid and tumor xenograft models of human PSCs and PanC-1 cells were characterized radiopharmacologically using a combined positron emission tomography (PET) radiotracer approach. [18F]FDG, [18F]FMISO, and [18F]FAPI-74 were employed to monitor metabolic activity, hypoxic metabolic state, and functional expression of fibroblast activation protein alpha (FAPα), a marker of activated PSCs. Results In vitro, PanC-1 and multi-cellular tumor spheroids demonstrated comparable glucose uptake and hypoxia, whereas FAPα expression was significantly higher in PSC spheroids. In vivo, glucose uptake as well as the transition to hypoxia were comparable in PanC-1 and multi-cellular xenograft models. In mice injected with PSCs, FAPα expression decreased over a period of four weeks post-injection, which was attributed to the successive death of PSCs. In contrast, FAPα expression increased in both PanC-1 and multi-cellular xenograft models over time due to invasion of mouse fibroblasts. Conclusion The presented models are suitable for subsequently characterizing stromal cell-induced metabolic changes in tumors using noninvasive molecular imaging techniques. [ABSTRACT FROM AUTHOR]

Published

2024

42. An Exogenous Ketone Ester Slows Tumor Progression in Murine Breast and Renal Cancer Models.

Author

Ogbonna, Henry Nnaemeka, Roberts, Zachary, Godwin, Nicholas, Muri, Pia, Turbitt, William J., Swalley, Zoey N., Dempsey, Francesca R., Stephens, Holly R., Zhang, Jianqing, Plaisance, Eric P., and Norian, Lyse A.

Subjects

*KIDNEY tumors, *BIOLOGICAL models, *IN vitro studies, *IMMUNOGENETICS, *CANCER invasiveness, *KETOGENIC diet, *RESEARCH funding, *BREAST tumors, *ANTINEOPLASTIC agents, *KETONES, *CANCER patients, *DESCRIPTIVE statistics, *METASTASIS, *MICE, *ANIMAL experimentation, *HYPOXEMIA

Abstract

Simple Summary: Exogenous ketone esters (KEs) are compounds that elevate blood ketones without dietary restriction and they show promise as anti-cancer agents. This study examined the effects of an exogenous ketone ester-supplemented (eKET) diet in mouse models of metastatic breast and kidney cancers. Our eKET diet slowed tumor growth and reduced metastatic spread to the lungs in both cancer types. The mechanisms behind these effects differed: the eKET diet downregulated genes involved in Wnt and TGFβ signaling in mammary cancers, whereas it downregulated genes related to hypoxia and DNA damage repair in tumor-bearing kidneys. The diet was safe for use overall but was associated with some negative physiological effects in mice with renal cancer. Thus, eKET diets could be an effective addition to current cancer treatments, but additional work is needed to fully understand their limitations. Background/Objectives: Ketone esters (KEs) exhibit promise as anti-cancer agents but their impact on spontaneous metastases remains poorly understood. Although consumption of a ketogenic diet (KD) that is low in carbohydrates and high in fats can lead to KE production in vivo, the restrictive composition of KDs may diminish adherence in cancer patients. Methods: We investigated the effects of an exogenous ketone ester-supplemented (eKET), carbohydrate-replete diet on tumor growth, metastasis, and underlying mechanisms in orthotopic models of metastatic breast (4T1-Luc) and renal (Renca-Luc) carcinomas. Mice were randomized to diet after tumor challenge. Results: Administration of KEs did not alter tumor cell growth in vitro. However, in mice, our eKET diet increased circulating β-hydroxybutyrate and inhibited primary tumor growth and lung metastasis in both models. Body composition analysis illustrated the overall safety of eKET diet use, although it was associated with a loss of fat mass in mice with renal tumors. Immunogenetic profiling revealed divergent intratumoral eKET-related changes by tumor type. In mammary tumors, Wnt and TGFβ pathways were downregulated, whereas in renal tumors, genes related to hypoxia and DNA damage repair were downregulated. Conclusions: Thus, our eKET diet exerts potent antitumor and antimetastatic effects in both breast and renal cancer models, albeit with different modes of action and physiologic effects. Its potential as an adjuvant dietary approach for patients with diverse cancer types should be explored further. [ABSTRACT FROM AUTHOR]

Published

2024

43. Accurate Co-Localization of Luciferase Expression and Fluorescent Anti-CEA Antibody Targeting of Liver Metastases in an Orthotopic Mouse Model of Colon Cancer.

Author

Lee, Kyung-Ha, Cox, Kristin E., Amirfakhri, Siamak, Jaiswal, Sunidhi, Liu, Shanglei, Hosseini, Mojgan, Lwin, Thinzar M., Yazaki, Paul J., Hoffman, Robert M., and Bouvet, Michael

Subjects

*THERAPEUTIC use of monoclonal antibodies, *LIVER tumors, *BIOLOGICAL models, *RESEARCH funding, *COLORECTAL cancer, *TREATMENT effectiveness, *FLUORESCENT antibody technique, *METASTASIS, *MICE, *LUMINESCENCE spectroscopy, *OXIDOREDUCTASES, *ANIMAL experimentation, *ORGANIC compounds

Abstract

Simple Summary: The present study demonstrated that a humanized anti-CEA antibody conjugated to a near-infrared dye accurately co-localized with luciferase expressing colorectal cancer liver metastases in an orthotopic mouse model. The present study validates the metastatic tumor targeting specificity of the anti-CEA antibody. Background: The present study aimed to validate the accuracy of a tumor-specific antibody to target liver metastases of colorectal cancer. Methods: A humanized anti-CEA antibody conjugated to a fluorescent dye (M5A-IR800) was tested for targeting human colorectal cancer liver metastases (CRLMs) expressing luciferase in an orthotopic mouse model. Orthotopic mouse models of CRLMs were established by implanting fragments of a luciferase-expressing human colorectal cancer cell line, LS174T, in the liver of nude mice. Mice received 50 µg M5A-IR800 72 h prior to imaging. To test co-localization, bioluminescence imaging was performed using D-luciferin, which was given via intraperitoneal injection just prior to imaging. Results: Tumors were able to be visualized non-invasively through the skin with the luciferase–luciferin signal. Intra-abdominal imaging showed accurate labeling of CRLMs with M5A-IR800, which co-localized with the luciferase–luciferin signal. Conclusions: The present results validate the accuracy of a tumor-specific anti-CEA antibody in targeting liver metastases of colorectal cancer. [ABSTRACT FROM AUTHOR]

Published

2024

44. Impact of Optimized Ku–DNA Binding Inhibitors on the Cellular and In Vivo DNA Damage Response.

Author

Mendoza-Munoz, Pamela L., Kushwaha, Narva Deshwar, Chauhan, Dineshsinha, Ali Gacem, Karim Ben, Garrett, Joy E., Dynlacht, Joseph R., Charbonnier, Jean-Baptiste, Gavande, Navnath S., and Turchi, John J.

Subjects

*RADIOTHERAPY, *BIOLOGICAL models, *RESEARCH funding, *BRCA genes, *PHOSPHORYLATION, *CELL physiology, *CELL proliferation, *IN vivo studies, *XENOGRAFTS, *DESCRIPTIVE statistics, *MICE, *CELL lines, *IMMUNOHISTOCHEMISTRY, *DNA repair, *ANIMAL experimentation, *MOLECULAR structure, *WESTERN immunoblotting, *TUMORS, *LUNG cancer, *DATA analysis software, *STAINS & staining (Microscopy), *ELECTROPHORESIS, *DNA-binding proteins, *CHEMICAL inhibitors

Abstract

Simple Summary: DNA-dependent protein kinase (DNA-PK) is a key player in repairing DNA damage. Ku proteins detect DNA damage and activate DNA-PK. Blocking DNA-PK can make cancer treatments such as radiation more effective. We have developed Ku–DNA binding inhibitors (Ku-DBis) that stop DNA-PK activation, making cancer cells more sensitive to radiation. We recently discovered new Ku-DBis that enter cells better than predecessor compounds, allowing cellular and in vivo analyses. Some non-small cell lung cancer (NSCLC) cells, especially those lacking ATM, were very sensitive to these inhibitors and radiation. However, cells lacking BRCA1 were resistant, which reduced the effectiveness of radiation. In animal studies of NSCLC, Ku-DBi treatment inhibited DNA-PK and enhanced a radiation-dependent decrease in tumor cell proliferation. This is the first time a Ku-targeted inhibitor has been shown to work in living organisms, suggesting their potential application in cancer treatment. Background: DNA-dependent protein kinase (DNA-PK) is a validated cancer therapeutic target involved in DNA damage response (DDR) and non-homologous end-joining (NHEJ) repair of DNA double-strand breaks (DSBs). Ku serves as a sensor of DSBs by binding to DNA ends and activating DNA-PK. Inhibition of DNA-PK is a common strategy to block DSB repair and improve efficacy of ionizing radiation (IR) therapy and radiomimetic drug therapies. We have previously developed Ku–DNA binding inhibitors (Ku-DBis) that block in vitro and cellular NHEJ activity, abrogate DNA-PK autophosphorylation, and potentiate cellular sensitivity to IR. Results and Conclusions: Here we report the discovery of oxindole Ku-DBis with improved cellular uptake and retained potent Ku-inhibitory activity. Variable monotherapy activity was observed in a panel of non-small cell lung cancer (NSCLC) cell lines, with ATM-null cells being the most sensitive and showing synergy with IR. BRCA1-deficient cells were resistant to single-agent treatment and antagonistic when combined with DSB-generating therapies. In vivo studies in an NSCLC xenograft model demonstrated that the Ku-DBi treatment blocked IR-dependent DNA-PKcs autophosphorylation, modulated DDR, and reduced tumor cell proliferation. This represents the first in vivo demonstration of a Ku-targeted DNA-binding inhibitor impacting IR response and highlights the potential therapeutic utility of Ku-DBis for cancer treatment. [ABSTRACT FROM AUTHOR]

Published

2024

45. Simultaneous Autophagy and Androgen Receptor Inhibition in a Prostate Cancer Xenograft Model.

Author

Salemi, Souzan, Kranzbühler, Benedikt, Baumgartner, Valentin, Breitenmoser, Lara, Kuzmanov, Aleksandar, Lehner, Fabienne, and Eberli, Daniel

Subjects

*ABIRATERONE acetate, *BIOLOGICAL models, *COMBINATION drug therapy, *AUTOPHAGY, *DATA analysis, *RESEARCH funding, *PROSTATE tumors, *CHLOROQUINE, *XENOGRAFTS, *DESCRIPTIVE statistics, *MICE, *GENE expression, *PROSTATE-specific membrane antigen, *ANIMAL experimentation, *ANALYSIS of variance, *STATISTICS, *DATA analysis software, *ANDROGEN receptors, *PHARMACODYNAMICS, *CHEMICAL inhibitors

Abstract

Simple Summary: Recent advancements in anticancer drug treatments face significant challenges due to drug resistance, often leading to only partial or short-term responses in patients. Our previous in vitro studies indicated that autophagy is linked to drug resistance in prostate cancer (PCa). Consequently, combination therapies targeting multiple pathways could help overcome resistance and extend treatment efficacy. To validate our earlier findings, we conducted in vivo experiments. Our data demonstrated that combining Abiraterone (Abi) with an autophagy inhibitor such as Chloroquine (Chl) not only reduces autophagy but also suppresses tumors more effectively than Abi alone. Thus, the combination of Abi with autophagy inhibitors represents a promising therapeutic strategy that could potentially offer a novel approach for patients. Objective: Abi, when used in conjunction with prednisone, is an established treatment for advanced PCa. Our goal was to explore the level of autophagy induced by Abi treatment, both alone and in combination with the autophagy inhibitor Chl, in a castrated mouse xenograft model. Methods: LNCaP cells were injected into the left and right sides of the back of nude mice that had been previously castrated. Mice were divided into four groups and treated daily with intraperitoneal injections of vehicle (control), Abi (10 mg/kg), Abi (10 mg/kg) combined with Chl (10 mg/kg), or Chl (10 mg/kg), and were monitored for periods of 2 and 3 weeks. Results: A significant reduction in tumor weight was observed in mice treated with the combination therapy, as opposed to those receiving vehicle control, Abi, or Chl alone. Mice receiving Abi + Chl exhibited reduced expression of ATG5, Beclin 1, and LC3 punctuations, along with an increase in P62, as determined by immunofluorescence and WES analysis. AR expression decreased significantly in all treatment groups compared to the control. PSMA expression was highest in the vehicle and combined treatment groups after 3 weeks, with a significant reduction observed with Chl treatment. Conclusions: These findings demonstrate that Abi + Chl treatment lowers autophagy levels and suppresses tumors more effectively than Abi alone. [ABSTRACT FROM AUTHOR]

Published

2024

46. CD103 + cDC1 Dendritic Cell Vaccine Therapy for Osteosarcoma Lung Metastases.

Author

Yang, Yuanzheng, Zhou, Yifan, Wang, Jian, Zhou, You, Watowich, Stephanie S., and Kleinerman, Eugenie S.

Subjects

*THERAPEUTIC use of antineoplastic agents, *OSTEOSARCOMA, *LYMPH nodes, *BIOLOGICAL models, *FLUOROIMMUNOASSAY, *RESEARCH funding, *T cells, *T-test (Statistics), *CANCER vaccines, *TREATMENT effectiveness, *IMMUNE system, *MANN Whitney U Test, *DESCRIPTIVE statistics, *METASTASIS, *MICE, *CELL lines, *SPLEEN, *IMMUNOHISTOCHEMISTRY, *LUNG tumors, *ANIMAL experimentation, *GENE expression profiling, *ONE-way analysis of variance, *STAINS & staining (Microscopy), *DATA analysis software, *DENDRITIC cells

Abstract

Simple Summary: Patients with relapsed, refractory, or metastatic osteosarcoma have few therapeutic options. Our findings demonstrated the efficacy of a DC vaccine generated using CD103+ cDC1 cells and OS cell lysates against the primary tumor and lung metastases, as well as its ability to induce a systemic immune response. This cDCV therapy elicited an increase in the infiltration of CD8+ T-cells into the primary and metastatic tumors as well as the TdLNs. cDCV efficacy was increased when combined with anti-CTLA-4. The failure of immunotherapies has been linked to their inability to induce infiltration of T-cells into the tumor. Therefore, our data suggest the potential for this novel immunotherapy using innate immune cells (type 1 CD103+ dendritic cells) alone or in combination with checkpoint blockade for patients with relapsed or metastatic OS, a tumor type that is refractory to the majority of current immunotherapies. Background: We generated a CD103+DC vaccine using K7M3 OS cell lysates (cDCV) and investigated its ability to induce regression of primary tumors, established lung metastases, and a systemic immune response. Methods: A bilateral tumor model was used to assess cDCV therapy efficacy and systemic immunity induction. K7M3 cells were injected into mice bilaterally. Right-sided tumors received PBS (control) or cDCV. Left-sided tumors were untreated. Tumor growth was compared between the vaccine-treated and untreated tumor on the contralateral side and compared to the control group. The immune cell profiles of the tumors, and tumor-draining lymph nodes (TdLNs) and spleen were evaluated. To determine the efficacy of systemic cDCV therapy against established lung metastases, K7M3 cells were injected intratibially. Leg amputation was performed 5 weeks later. Mice were treated intravenously with PBS or cDCV and euthanized 6 weeks later. Lungs, TdLNs and spleen were collected. The number and size of the lung nodules were quantified. The immune cell profile of tumor, and lymph nodes and spleen were also evaluated. Using this same model, we evaluated the effect of cDCV + anti-CTLA-4. Results: cDCV therapy inhibited the treated and untreated tumors and increased the number of T-cells in these tumors and the lymph nodes compared to control-treated mice. Systemic cDCV therapy administered following amputation decreased the size and number of lung metastases, and increased T-cell numbers in the tumor and lymph nodes. Combining anti-CTLA-4 with cDCV therapy increased cDCV efficacy against lung metastases. Conclusions: Intratumor cDCV generated a systemic immune response inhibiting the growth of both the treated and untreated tumors, with increased T-cells in the tumor and lymph nodes. Systemic cDCV was effective against established lung metastases. Efficacy was increased by anti-CTLA4. cDCVs may provide a novel therapeutic approach for relapsed/metastatic OS patients. [ABSTRACT FROM AUTHOR]

Published

2024

47. Effects of passive smoking on cortical spreading depolarization in male and female mice.

Author

Takizawa, Tsubasa, Ihara, Keiko, Unekawa, Miyuki, Iba, Chisato, Kagawa, Shizuko, Watanabe, Narumi, Nakayama, Shingo, Sakurai, Kaori, Miyazaki, Naoki, Ishida, Noriyuki, Takemura, Ryo, Shibata, Mamoru, Izawa, Yoshikane, Chubachi, Shotaro, Fukunaga, Koichi, and Nakahara, Jin

Subjects

*MIGRAINE prevention, *BIOLOGICAL models, *RESEARCH funding, *EVOKED potentials (Electrophysiology), *ISOFLURANE, *SEX distribution, *DESCRIPTIVE statistics, *MICE, *ENVIRONMENTAL exposure, *ANIMAL experimentation, *POTASSIUM chloride, *DISEASE susceptibility, *COMPARATIVE studies, *PASSIVE smoking

Abstract

Background: Patients with migraine are typically advised to avoid passive smoking because it may aggravate headaches and other health conditions. However, there is insufficient high-quality evidence on the association between passive smoking and migraine, which warrants further investigation using animal models. Therefore, using a mouse model, we examined the effect of passive smoking on susceptibility to cortical spreading depolarization (CSD), the biological basis of migraine with aura. Findings: Fifty C57BL/6 mice (25 males and 25 females) were exposed for one hour to cigarette smoke or room air. Subsequently, potassium chloride (KCl) was administered under isoflurane anesthesia to induce CSD, and the CSD threshold, frequency of induction, and propagation velocity were determined. The threshold to induce CSD (median [interquartile range (IQR)]) was significantly lower in female mice (adjusted p = 0.01) in the smoking group (0.05 [0.05, 0.088]) than in the sham group (0.125 [0.1, 0.15]); however, there was no significant difference in the male mice (adjusted p = 0.77). CSD frequency or propagation velocity did not differ significantly between the two groups for either sex. Conclusions: Female mice in the smoking group showed lower CSD threshold compared to the sham group, suggesting a potential sex-specific difference in the effect of smoking on the pathogenesis of CSD and migraine with aura. This finding may contribute to the understanding of migraine pathophysiology in association with passive smoking and sex difference. [ABSTRACT FROM AUTHOR]

Published

2024

48. In vivo dissection of the mouse tyrosine catabolic pathway with CRISPR-Cas9 identifies modifier genes affecting hereditary tyrosinemia type 1.

Author

Rivest, Jean-François, Carter, Sophie, Goupil, Claudia, Antérieux, Pénélope, Cyr, Denis, Ung, Roth-Visal, Soglio, Dorothée Dal, Mac-Way, Fabrice, Waters, Paula J, Paganelli, Massimiliano, and Doyon, Yannick

Subjects

*BIOLOGICAL models, *GENE therapy, *CELLULAR signal transduction, *IN vivo studies, *STAPHYLOCOCCUS aureus, *DESCRIPTIVE statistics, *GENES, *MICE, *AMINO acid metabolism disorders, *CRISPRS, *TYROSINE, *GENOME editing, *ANIMAL experimentation, *METABOLISM, *GENETIC mutation, *LIVER, *PHENOTYPES, *VIRUSES

Abstract

Hereditary tyrosinemia type 1 is an autosomal recessive disorder caused by mutations (pathogenic variants) in fumarylacetoacetate hydrolase, an enzyme involved in tyrosine degradation. Its loss results in the accumulation of toxic metabolites that mainly affect the liver and kidneys and can lead to severe liver disease and liver cancer. Tyrosinemia type 1 has a global prevalence of approximately 1 in 100,000 births but can reach up to 1 in 1,500 births in some regions of Québec, Canada. Mutating functionally related "modifier' genes (i.e. genes that, when mutated, affect the phenotypic impacts of mutations in other genes) is an emerging strategy for treating human genetic diseases. In vivo somatic genome editing in animal models of these diseases is a powerful means to identify modifier genes and fuel treatment development. In this study, we demonstrate that mutating additional enzymes in the tyrosine catabolic pathway through liver-specific genome editing can relieve or worsen the phenotypic severity of a murine model of tyrosinemia type 1. Neonatal gene delivery using recombinant adeno-associated viral vectors expressing Staphylococcus aureus Cas9 under the control of a liver-specific promoter led to efficient gene disruption and metabolic rewiring of the pathway, with systemic effects that were distinct from the phenotypes observed in whole-body knockout models. Our work illustrates the value of using in vivo genome editing in model organisms to study the direct effects of combining pathological mutations with modifier gene mutations in isogenic settings. [ABSTRACT FROM AUTHOR]

Published

2024

49. Zoledronic acid enhances tumor growth and metastatic spread in a mouse model of jaw osteosarcoma.

Author

Nham, Than‐Thuy, Guiho, Romain, Brion, Régis, Amiaud, Jérôme, Le Royer, Bénédicte Brounais, Gomez‐Brouchet, Anne, Rédini, Françoise, and Bertin, Hélios

Subjects

*OSTEOSARCOMA, *RISK assessment, *BIOLOGICAL models, *NF-kappa B, *VASCULAR endothelial growth factors, *ACID phosphatase, *RESEARCH funding, *JAW tumors, *TUMOR markers, *DESCRIPTIVE statistics, *METASTASIS, *MICE, *IMMUNOHISTOCHEMISTRY, *MESSENGER RNA, *GENE expression, *ZOLEDRONIC acid, *ANIMAL experimentation, *LUNG tumors, *CELL receptors, *DISEASE risk factors

Abstract

Objectives: Investigation of the therapeutic effect of zoledronic acid (ZA) in a preclinical model of jaw osteosarcoma (JO). Materials and Methods: The effect of 100 μg/kg ZA administered twice a week was assessed in a xenogenic mouse model of JO. The clinical (tumor growth, development of lung metastasis), radiological (bone microarchitecture by micro‐CT analysis), and molecular and immunohistochemical (TRAP, RANK/RANKL, VEGF, and CD146) parameters were investigated. Results: Animals receiving ZA exhibited an increased tumor volume compared with nontreated animals (71.3 ± 14.3 mm3 vs. 51.9 ± 19.9 mm3 at D14, respectively; p = 0.06) as well as increased numbers of lung metastases (mean 4.88 ± 4.45 vs. 0.50 ± 1.07 metastases, respectively; p = 0.02). ZA protected mandibular bone against tumor osteolysis (mean bone volume of 12.81 ± 0.53 mm3 in the ZA group vs. 11.55 ± 1.18 mm3 in the control group; p = 0.01). ZA induced a nonsignificant decrease in mRNA expression of the osteoclastic marker TRAP and an increase in RANK/RANKL bone remodeling markers. Conclusion: The use of bisphosphonates in the therapeutic strategy for JO should be further explored, as should the role of bone resorption in the pathophysiology of the disease. [ABSTRACT FROM AUTHOR]

Published

2024

50. Circular RNA CircACAP2 regulates temporomandibular joint osteoarthritis via miR‐21‐5p/PLAG1 axis.

Author

Chen, Hongyu, Qu, Zhuli, Shi, Tingting, Zhao, Huaqiang, Huang, Shengdong, and Ma, Chuan

Subjects

*BIOLOGICAL models, *TEMPOROMANDIBULAR joint, *ARTICULAR cartilage, *RESEARCH funding, *CIRCULAR RNA, *MICRORNA, *CELL physiology, *CELL proliferation, *APOPTOSIS, *TRANSCRIPTION factors, *MICE, *GENETIC polymorphisms, *ADENOMA, *OSTEOARTHRITIS, *ANIMAL experimentation, *OXIDOREDUCTASES, *CARTILAGE cells, *DISEASE progression

Abstract

Objectives: The pathogenesis of temporomandibular joint osteoarthritis (TMJOA) remains not fully understood. Our previous studies demonstrated that miR‐21‐5p may participate in the TMJOA development and the interaction between circRNA‐ACAP2 (CircACAP2) and miR‐21‐5p. Our present study aimed to explore the biological functions and regulatory mechanisms of CircACAP2 in TMJOA. Materials and Methods: The differential expression pattern of CircACAP2 in OA and normal tissues or cells was detected. CircACAP2 biological functions experiments were performed in chondrocytes by overexpression and interference techniques. The interaction of CircACAP2 with miR‐21‐5p and downstream target mRNA, polymorphic adenoma gene 1 (PLAG1), was predicted by bioinformatic databases and then demonstrated by dual‐luciferase reporter assay. The biological role of CircACAP2 in TMJOA was investigated and validated in a mouse model. Results: The expression level of CircACAP2 was markedly reduced in OA cartilage and directly related to chondrocyte proliferation and apoptosis as well as ECM metabolism in the cartilage. CircACAP2 functioned in chondrocytes via targeting miR‐21‐5p and PLAG1. Overexpressing of CircACAP2 alleviated TMJOA in mouse models. Conclusions: The present study unveiled that CircACAP2/miR‐21‐5p/PLAG1 axis may play an important regulatory role in TMJOA progression, which may highlight a potentially effective intervention and therapeutic strategy for the treatment of TMJOA. [ABSTRACT FROM AUTHOR]

Published

2024