Your search keyword '"Wang,Xia"' showing total 110 results

1. ER stress-inducible protein MANF selectively expresses in human spleen.

Author

Liu J, Zhou C, Tao X, Feng L, Wang X, Chen L, Li C, Huang D, Fang S, and Shen Y

Subjects

Adult, B-Lymphocytes immunology, B-Lymphocytes metabolism, Humans, Immunohistochemistry, Macrophages immunology, Macrophages metabolism, Male, Middle Aged, Nerve Growth Factors metabolism, Organ Specificity genetics, Plasma Cells immunology, Plasma Cells metabolism, Protein Transport, T-Lymphocytes immunology, T-Lymphocytes metabolism, Endoplasmic Reticulum Stress genetics, Gene Expression, Nerve Growth Factors genetics, Spleen immunology, Spleen metabolism

Abstract

Mesencephalic astrocyte-derived neurotrophic factor (MANF; also known as arginine-rich, mutated in early tumors; ARMET), is an ER stress-inducible protein, and widely expressed in mammalian tissues. In this study, we are interested in the profile of MANF expression in human splenocytes. Three patients with spleen trauma were enrolled in this study. Immunohistochemistry and immunofluorescence were used to detect MANF expression in the four types of cells, including T cells, B cells, plasma cells, and macrophages in spleens by using the specific antibodies of anti-CD3, anti-CD20, anti-CD138, and anti-CD68, respectively. We found that MANF-positive cells extensively distributed in the red pulp and marginal-zone of spleen, and MANF was almost localized in the cytoplasm of splenocytes. Double immunofluorescent staining results showed that MANF localized mainly in the plasma cells and macrophages, but not in T and B cells. Meanwhile, we found that some MANF-positive cells expressed ER stress-related proteins, including ATF6, XBP1s, BiP, and CHOP. These results suggest that the selective expression of MANF in splenocytes may be involved in plasma cell differentiation and immune regulation., (Copyright © 2015 American Society for Histocompatibility and Immunogenetics. Published by Elsevier Inc. All rights reserved.)

Published

2015

2. Bistable switch in let-7 miRNA biogenesis pathway involving Lin28.

Author

Shi F, Yu W, and Wang X

Subjects

Computer Simulation, Humans, Models, Biological, Software, Gene Expression genetics, MicroRNAs genetics, RNA-Binding Proteins genetics, Signal Transduction genetics

Abstract

miRNAs are small noncoding RNAs capable of regulating gene expression at the post-transcriptional level. A growing body of evidence demonstrated that let-7 family of miRNAs, as one of the highly conserved miRNAs, plays an important role in cell differentiation and development, as well as tumor suppressor function depending on their levels of expression. To explore the physiological significance of let-7 in regulating cell fate decisions, we present a coarse grained model of let-7 biogenesis network, in which let-7 and its regulator Lin28 inhibit mutually. The dynamics of this minimal network architecture indicates that, as the concentration of Lin28 increases, the system undergoes a transition from monostability to a bistability and then to a one-way switch with increasing strength of positive feedback of let-7, while in the absence of Lin28 inhibition, the system loses bistability. Moreover, the ratio of degradation rates of let-7 and Lin28 is critical for the switching sensitivity and resistance to stimulus fluctuations. These findings may highlight why let-7 is required for normal gene expression in the context of embryonic development and oncogenesis, which will facilitate the development of approaches to exploit this regulatory pathway by manipulating Lin28/let-7 axis for novel treatments of human diseases.

Published

2014

3. Genomic analysis provides insights into the origin and divergence of fruit flavor and flesh color of pummelo.

Author

Huang, Yue, Makkumrai, Warangkana, Fu, Jialing, Deng, Chongling, Wu, Qingjiang, Wang, Shaohua, Wang, Lun, Wu, Xiaoxiao, Gao, Junyan, Chen, Chuanwu, Guo, Lina, Chen, Peng, Wu, Fangfang, Deng, Xiuxin, Wang, Xia, and Xu, Qiang

Subjects

POMELO, FRUIT flavors & odors, GENOMICS, GENE expression, LYCOPENE

Abstract

Summary: Pummelo (Citrus maxima) is one of the most important citrus crops and have genetically contributed sweet orange, lemon and most citrus cultivars. It has been cultivated for c. 4000 years in China and is also distributed in many Southeast Asian countries. Nevertheless, the origin and dispersal of pummelo remain elusive.We conducted whole‐genome sequencing for 290 pummelo accessions from China and Southeast Asia (SEA). Our findings indicated that pummelo was originated in Yunnan province. The divergence of the China‐SEA accessions occurred c. 2000 years ago and the divergence was likely facilitated through the Maritime Silk Road.We detected the divergence of genomic regions associated with fruit flavor and color, indicating different selection by human activities in different regions. A gene encoding lycopene cyclase 2 (LCYB2) exhibited a high degree of divergence in expression and sequence between red‐flesh and white‐flesh pummelos. A SNP in the coding region of LCYB2 resulted in a reduction in lycopene β‐cyclizing enzyme activity, leading to the accumulation of lycopene and the development of the red‐flesh trait.This study reveals the origin and evolutionary history of pummelo and provides insights into the genomic basis for the divergence of fruit flavor and color. [ABSTRACT FROM AUTHOR]

Published

2025

4. Nicorandil treatment improves survival and spatial learning in aged granulin knockout mice.

Author

Niedowicz, Dana M., Wang, Wang‐Xia, Prajapati, Paresh, Zhong, Yu, Fister, Shuling, Rogers, Colin B., Sompol, Pradoldej, Powell, David K., Patel, Indumati, Norris, Christopher M., Saatman, Kathryn E., and Nelson, Peter T.

Subjects

*GLIAL fibrillary acidic protein, *FRONTOTEMPORAL dementia, *ENCEPHALITIS, *COGNITIVE testing, *GENE expression

Abstract

Mutations in the human granulin (GRN) gene are associated with multiple diseases, including dementia disorders such as frontotemporal dementia (FTD) and limbic‐predominant age‐related TDP‐43 encephalopathy (LATE). We studied a Grn knockout (Grn‐KO) mouse model in order to evaluate a potential therapeutic strategy for these diseases using nicorandil, a commercially available agonist for the ABCC9/Abcc9‐encoded regulatory subunit of the “K+ATP” channel that is well‐tolerated in humans. Aged (13 months) Grn‐KO and wild‐type (WT) mice were treated as controls or with nicorandil (15 mg/kg/day) in drinking water for 7 months, then tested for neurobehavioral performance, neuropathology, and gene expression. Mortality was significantly higher for aged Grn‐KO mice (particularly females), but there was a conspicuous improvement in survival for both sexes treated with nicorandil. Grn‐KO mice performed worse on some cognitive tests than WT mice, but Morris Water Maze performance was improved with nicorandil treatment. Neuropathologically, Grn‐KO mice had significantly increased levels of glial fibrillary acidic protein (GFAP)‐immunoreactive astrocytosis but not ionized calcium binding adaptor molecule 1 (IBA‐1)‐immunoreactive microgliosis, indicating cell‐specific inflammation in the brain. Expression of several astrocyte‐enriched genes, including Gfap, were also elevated in the Grn‐KO brain. Nicorandil treatment was associated with a subtle shift in a subset of detected brain transcript levels, mostly related to attenuated inflammatory markers. Nicorandil treatment improved survival outcomes, cognition, and inflammation in aged Grn‐KO mice. [ABSTRACT FROM AUTHOR]

Published

2024

5. A transcriptional cascade involving BBX22 and HY5 finely regulates both plant height and fruit pigmentation in citrus.

Author

Fu, Jialing, Liao, Li, Jin, Jiajing, Lu, Zhihao, Sun, Juan, Song, Lizhi, Huang, Yue, Liu, Shengjun, Huang, Ding, Xu, Yuantao, He, Jiaxian, Hu, Bin, Zhu, Yiqun, Wu, Fangfang, Wang, Xia, Deng, Xiuxin, and Xu, Qiang

Subjects

CLONORCHIS sinensis, GENE expression, POMELO, REGULATOR genes, GIBBERELLIC acid, TOMATOES

Abstract

Dwarfing is a pivotal agronomic trait affecting both yield and quality. Citrus species exhibit substantial variation in plant height, among which internode length is a core element. However, the molecular mechanism governing internode elongation remains unclear. Here, we unveiled that the transcriptional cascade consisting of B‐BOX DOMAIN PROTEIN 22 (BBX22) and ELONGATED HYPOCOTYL 5 (HY5) finely tunes plant height and internode elongation in citrus. Loss‐of‐function mutations of BBX22 in an early‐flowering citrus (Citrus hindsii "SJG") promoted internode elongation and reduced pigment accumulation, whereas ectopic expression of BBX22 in SJG, sweet orange (C. sinensis), pomelo (C. maxima) or heterologous expression of BBX22 in tomato (Solanum lycopersicum) significantly decreased internode length. Furthermore, exogenous application of gibberellin A3 (GA3) rescued the shortened internode and dwarf phenotype caused by BBX22 overexpression. Additional experiments revealed that BBX22 played a dual role in regulation internode elongation and pigmentation in citrus. On the one hand, it directly bound to and activated the expression of HY5, GA metabolism gene (GA2 OXIDASE 8, GA2ox8), carotenoid biosynthesis gene (PHYTOENE SYNTHASE 1, PSY1) and anthocyanin regulatory gene (Ruby1, a MYB DOMAIN PROTEIN). On the other hand, it acted as a cofactor of HY5, enhancing the ability of HY5 to regulate target genes expression. Together, our results reveal the critical role of the transcriptional cascade consisting of BBX22 and HY5 in controlling internode elongation and pigment accumulation in citrus. Unraveling the crosstalk regulatory mechanism between internode elongation and fruit pigmentation provides key genes for breeding of novel types with both dwarf and health‐beneficial fortification in citrus. [ABSTRACT FROM AUTHOR]

Published

2024

6. Sex-Biased Expression and Response of microRNAs in Neurological Diseases and Neurotrauma.

Author

Geleta, Urim, Prajapati, Paresh, Bachstetter, Adam, Nelson, Peter T., and Wang, Wang-Xia

Subjects

GENE expression, NEUROLOGICAL disorders, SEX factors in disease, DIMORPHISM (Biology), HUMAN biology, SEX chromosomes

Abstract

Neurological diseases and neurotrauma manifest significant sex differences in prevalence, progression, outcome, and therapeutic responses. Genetic predisposition, sex hormones, inflammation, and environmental exposures are among many physiological and pathological factors that impact the sex disparity in neurological diseases. MicroRNAs (miRNAs) are a powerful class of gene expression regulator that are extensively involved in mediating biological pathways. Emerging evidence demonstrates that miRNAs play a crucial role in the sex dimorphism observed in various human diseases, including neurological diseases. Understanding the sex differences in miRNA expression and response is believed to have important implications for assessing the risk of neurological disease, defining therapeutic intervention strategies, and advancing both basic research and clinical investigations. However, there is limited research exploring the extent to which miRNAs contribute to the sex disparities observed in various neurological diseases. Here, we review the current state of knowledge related to the sexual dimorphism in miRNAs in neurological diseases and neurotrauma research. We also discuss how sex chromosomes may contribute to the miRNA sexual dimorphism phenomenon. We attempt to emphasize the significance of sexual dimorphism in miRNA biology in human diseases and to advocate a gender/sex-balanced science. [ABSTRACT FROM AUTHOR]

Published

2024

7. Asperuloside Promotes Apoptosis of Cervical Cancer Cells through Endoplasmic Reticulum Stress-Mitochondrial Pathway.

Author

Qi, Zhi-min, Wang, Xia, Liu, Xia, and Zhao, Juan

Subjects

FLOW cytometry, PROTEINS, STATISTICS, ENDOPLASMIC reticulum, ANIMAL experimentation, ONCOGENES, WESTERN immunoblotting, ONE-way analysis of variance, GLYCOSIDES, APOPTOSIS, OXIDATIVE stress, MITOCHONDRIA, CELLULAR signal transduction, RATS, GENE expression, CELL proliferation, DESCRIPTIVE statistics, CERVIX uteri tumors, PLANT extracts, CELL lines, REACTIVE oxygen species, DATA analysis software, DATA analysis, CASPASES

Abstract

Objective: To investigate the effects of asperuloside on cervical cancer based on endoplasmic reticulum (ER) stress and mitochondrial pathway. Methods: Different doses (12.5–800 µg/mL) of asperuloside were used to treat cervical cancer cell lines Hela and CaSki to calculate the half maximal inhibitory concentration (IC50) of asperuloside. The cell proliferation was analyzed by clone formation assay. Cell apoptosis, intracellular reactive oxygen species (ROS) and mitochondrial membrane potential were determined by flow cytometry. The protein expressions of cleaved-caspase-3, Bcl-2, Bax, Cyt-c, cleaved-caspase-4 and glucose-regulated protein 78 (GRP78) were analyzed by Western blot. And the inhibitor of ER stress, 4-phenyl butyric acid (4-PBA) was used to treat cervical cancer cells to further verify the role of ER stress in the apoptosis of cervical cancer cells induced by asperuloside. Results: Asperuloside of 325, 650, and 1300 µg/mL significantly inhibited the proliferation and promoted apoptosis of Hela and CaSki cells (P<0.01). All doses of asperuloside significantly increased intracellular ROS levels, reduced mitochondrial membrane potential, significantly reduced Bcl-2 protein expression level, and increased Bax, Cyt-c, GRP78 and cleaved-caspase-4 expressions (P<0.01). In addition, 10 mmol/L 4-PBA treatment significantly promoted cell proliferation and reduced apoptosis (P<0.05), and 650 µg/mL asperuloside could reverse 4-PBA-induced increased cell proliferation, decreased apoptosis and cleaved-caspase-3, -4 and GRP78 protein expressions (P<0.05). Conclusion: Our study revealed the role of asperuloside in cervical cancer, suggesting that asperuloside promotes apoptosis of cervical cancer cells through ER stress-mitochondrial pathway. [ABSTRACT FROM AUTHOR]

Published

2024

8. Modulating Thyroid Hormone Levels in Adult Mice: Impact on Behavior and Compensatory Brain Changes

Author

Dana M. Niedowicz, Doug A. Price, Peter T. Nelson, and Wang-Xia Wang

Subjects

endocrine system, Single sex, Article Subject, business.industry, Endocrinology, Diabetes and Metabolism, Thyroid, Physiology, 030209 endocrinology & metabolism, Disease, RC648-665, Diseases of the endocrine glands. Clinical endocrinology, 03 medical and health sciences, Methimazole, 0302 clinical medicine, medicine.anatomical_structure, In utero, Gene expression, medicine, Propylthiouracil, business, 030217 neurology & neurosurgery, Research Article, medicine.drug, Hormone

Abstract

Thyroid hormone (TH) perturbation is a common medical problem. Because of substantial public health impact, prior researchers have studied hyper- and hypothyroidism in animal models. Although most prior research focused on in utero and/or developmental effects, changes in circulating TH levels are commonly seen in elderly individuals: approximately 20% of persons older than 80 years have clinically impactful hypothyroidism and up to 5% have clinical hyperthyroidism, with women being more often affected than men. TH disease model methodology in mice have varied but usually focus on a single sex, and the impact(s) of TH perturbation on the adult brain are not well understood. We administered thyroxine to middle-aged (13 to 14 months) male and female mice to model hyperthyroidism and TH-lowering drugs propylthiouracil (PTU) and methimazole, to induce hypothyroidism. These pharmacological agents are used commonly in adult humans. Circulating TH-level changes were observed when thyroxine was dosed at 20 µg/mL in drinking water for two weeks. By contrast, PTU and methimazole did not elicit a consistent reproducible effect until two months of treatment. No substantial changes in TH levels were detected in brain tissues of treated animals; however, pronounced changes in gene expression, specifically for TH-processing transcripts, were observed following the treatment with thyroxine. Our study indicated a robust compensatory mechanism by which the brain tissue/cells minimize the TH fluctuation in CNS by altering gene expression. Neurobehavioral changes were related to the TH perturbation and suggested potential associations between cognitive status and hyper- and hypothyroidism.

Published

2021

9. Resequencing of global Lotus corniculatus accessions reveals population distribution and genetic loci, associated with cyanogenic glycosides accumulation and growth traits.

Author

Chen, Cheng, Zhang, Kaixuan, Liu, Fu, Wang, Xia, Yao, Yang, Niu, Xiaolei, He, Yuqi, Hong, Jun, Liu, Fang, Gao, Qiu, Zhang, Yi, Li, Yurong, Wang, Meijuan, Lin, Jizhen, Fan, Yu, Ren, Kui, Shen, Lunhao, Gao, Bin, Ren, Xue, and Yang, Weifei

Subjects

LOTUS corniculatus, MOLECULAR genetics, GENE expression, GENETIC variation, LOCUS (Genetics)

Abstract

Background: Lotus corniculatus is a widely distributed perennial legume whose great adaptability to different environments and resistance to barrenness make it an excellent forage and ecological restoration plant. However, its molecular genetics and genomic relationships among populations are yet to be uncovered. Result: Here we report on a genomic variation map from worldwide 272 L. corniculatus accessions by genome resequencing. Our analysis suggests that L. corniculatus accessions have high genetic diversity and could be further divided into three subgroups, with the genetic diversity centers were located in Transcaucasia. Several candidate genes and SNP site associated with CNglcs content and growth traits were identified by genome-wide associated study (GWAS). A non-synonymous in LjMTR was responsible for the decreased expression of CNglcs synthesis genes and LjZCD was verified to positively regulate CNglcs synthesis gene CYP79D3. The LjZCB and an SNP in LjZCA promoter were confirmed to be involved in plant growth. Conclusion: This study provided a large number of genomic resources and described genetic relationship and population structure among different accessions. Moreover, we attempt to provide insights into the molecular studies and breeding of CNglcs and growth traits in L. corniculatus. [ABSTRACT FROM AUTHOR]

Published

2023

10. Impact of thyroid hormone perturbations in adult mice: brain weight and blood vessel changes, gene expression variation, and neurobehavioral outcomes.

Author

Niedowicz, Dana M., Wang, Wang-Xia, Price, Douglas A., Xie, Kevin, Patel, Ela, and Nelson, Peter T.

Subjects

*GENE expression, *BLOOD vessels, *THYROID hormones, *MICE

Abstract

Mouse models of hyper- and hypothyroidism were used to examine the effects of thyroid hormone (TH) dyshomeostasis on the aging mammalian brain. 13–14 month-old mice were treated for 4 months with either levothyroxine (hyperthyroid) or a propylthiouracil and methimazole combination (PTU/Met; hypothyroid). Hyperthyroid mice performed better on Morris Water Maze than control mice, while hypothyroid mice performed worse. Brain weight was increased in thyroxine-treated, and decreased in PTU/Met-treated animals. The brain weight change was strongly correlated with circulating and tissue T4. Quantitative measurements of microvessels were compared using digital neuropathologic methods. There was an increase in microvessel area in hyperthyroid mice. Hypothyroid mice showed a trend for elevated glial fibrillary acidic protein-immunoreactive astrocytes, indicating an increase in neuroinflammation. Gene expression alterations were associated with TH perturbation and astrocyte-expressed transcripts were particularly affected. For example, expression of Gli2 and Gli3 , mediators in the Sonic Hedgehog signaling pathway, were strongly impacted by both treatments. We conclude that TH perturbations produce robust neurobehavioral, pathological, and brain gene expression changes in aging mouse models. [ABSTRACT FROM AUTHOR]

Published

2023

11. Genome-wide high-resolution mapping of DNA methylation identifies epigenetic variation across different salt stress in Maize (Zea mays L.)

Author

Sun, Lifang, Miao, Xingfen, Cui, Jin, Deng, Jie, Wang, Xia, Wang, Yufeng, Zhang, Yifei, Gao, Shuren, and Yang, Kejun

Published

2018

12. Genome-Wide Identification and Functional Analysis of NAP1 in Triticum aestivum.

Author

Feng, Huimin, Wu, Mila, Wang, Ziqiong, Wang, Xia, Chen, Jianping, Yang, Jian, and Liu, Peng

Subjects

WHEAT, PLANT viruses, FUNCTIONAL analysis, PLANT defenses, GENE expression, PLANT genes

Abstract

As a main molecular chaperone of histone H2A-H2B, nucleosome assembly protein 1 (NAP1) has been widely researched in many species. However, there is little research investigating the function of NAP1 in Triticum aestivum. To understand the capabilities of the family of NAP1 genes in wheat and the relationship between TaNAP1 genes and plant viruses, we performed comprehensive genome-wide analysis and quantitative real-time polymerase chain reaction (qRT-PCR) for testing expression profiling under hormonal and viral stresses. Our results showed that TaNAP1 was expressed at different levels in different tissues, with higher expression in tissues with high meristematic capacity, such as roots. Furthermore, the TaNAP1 family may participate in plant defense mechanisms. This study provides a systematic analysis of the NAP1 gene family in wheat and lays the foundation for further studies on the function of TaNAP1 in the response of wheat plants to viral infection. [ABSTRACT FROM AUTHOR]

Published

2023

13. Difenoconazole Exposure Induces Retinoic Acid Signaling Dysregulation and Testicular Injury in Mice Testes.

Author

Zheng, Xiangqin, Wei, Yuexin, Chen, Jiadong, Wang, Xia, Li, Dinggang, Yu, Chengjun, Hong, Yifan, Shen, Lianju, Long, Chunlan, Wei, Guanghui, and Wu, Shengde

Subjects

TRETINOIN, TESTIS injuries, POISONS, GENITALIA, SPERMATOGENESIS, GENE expression

Abstract

Difenoconazole (DFZ) is a broad-spectrum triazole fungicide that is widely utilized in agriculture. Although DFZ has been demonstrated to induce reproductive toxicity in aquatic species, its toxic effects on the mammalian reproductive system have yet to be fully elucidated. In vivo, male mice were administered 0, 20 or 40 mg/kg/d of DFZ via oral gavage for 35 days. Consequently, DFZ significantly decreased testicular organ coefficient, sperm count and testosterone levels, augmented sperm malformation rates, and elicited histopathological alterations in testes. TUNEL assay showed increased apoptosis in testis. Western blotting results suggested abnormally high expression of the sperm meiosis-associated proteins STRA8 and SCP3. The concentrations of retinoic acid (RA), retinaldehyde (RE), and retinol (ROL) were increased in the testicular tissues of DFZ-treated groups. The mRNA expression level of genes implicated in RA synthesis significantly increased while genes involved in RA catabolism significantly decreased. In vitro, DFZ reduced cell viability and increased RA, RE, and ROL levels in GC-2 cells. Transcriptome analysis revealed a significant enrichment of numerous terms associated with the RA pathway and apoptosis. The qPCR experiment verified the transcriptome results. In conclusion, our results indicate that DFZ exposure can disrupt RA signaling pathway homeostasis, and induce testicular injury in mice testes. [ABSTRACT FROM AUTHOR]

Published

2023

14. DeepsmirUD: Prediction of Regulatory Effects on microRNA Expression Mediated by Small Molecules Using Deep Learning.

Author

Sun, Jianfeng, Ru, Jinlong, Ramos-Mucci, Lorenzo, Qi, Fei, Chen, Zihao, Chen, Suyuan, Cribbs, Adam P., Deng, Li, and Wang, Xia

Subjects

SMALL molecules, GENE expression, DEEP learning, MICRORNA, DRUG repositioning, PHARMACY databases, DNA-binding proteins

Abstract

Aberrant miRNA expression has been associated with a large number of human diseases. Therefore, targeting miRNAs to regulate their expression levels has become an important therapy against diseases that stem from the dysfunction of pathways regulated by miRNAs. In recent years, small molecules have demonstrated enormous potential as drugs to regulate miRNA expression (i.e., SM-miR). A clear understanding of the mechanism of action of small molecules on the upregulation and downregulation of miRNA expression allows precise diagnosis and treatment of oncogenic pathways. However, outside of a slow and costly process of experimental determination, computational strategies to assist this on an ad hoc basis have yet to be formulated. In this work, we developed, to the best of our knowledge, the first cross-platform prediction tool, DeepsmirUD, to infer small-molecule-mediated regulatory effects on miRNA expression (i.e., upregulation or downregulation). This method is powered by 12 cutting-edge deep-learning frameworks and achieved AUC values of 0.843/0.984 and AUCPR values of 0.866/0.992 on two independent test datasets. With a complementarily constructed network inference approach based on similarity, we report a significantly improved accuracy of 0.813 in determining the regulatory effects of nearly 650 associated SM-miR relations, each formed with either novel small molecule or novel miRNA. By further integrating miRNA–cancer relationships, we established a database of potential pharmaceutical drugs from 1343 small molecules for 107 cancer diseases to understand the drug mechanisms of action and offer novel insight into drug repositioning. Furthermore, we have employed DeepsmirUD to predict the regulatory effects of a large number of high-confidence associated SM-miR relations. Taken together, our method shows promise to accelerate the development of potential miRNA targets and small molecule drugs. [ABSTRACT FROM AUTHOR]

Published

2023

15. Effect of Foliar Calcium Fertilization on Fruit Quality, Cell Wall Enzyme Activity and Expression of Key Genes in Chinese Cherry.

Author

Wu, Yongfei, Yang, Xuelian, Wang, Xia, Yan, Li, Hu, Xiaojing, and Lian, Manjing

Subjects

FOLIAR feeding, FRUIT quality, CAROTENES, PECTINESTERASE, POLYPHENOL oxidase, GENE expression, SWEET cherry, CHERRIES

Abstract

Chinese cherries are early flowering and early fruiting, with both edible and ornamental values. This study aims to explore the effects of pre-harvest spraying with different concentrations of CaCl2, amino acid calcium, and sugar alcohol calcium on the quality of Chinese cherry and the expression of genes related to cell wall softening. The goal is to identify suitable calcium-based agents for pre-harvest spraying on Chinese cherry. The results of the study demonstrated that all three exogenous calcium treatments significantly increased the mineral content compared to the control group. Moreover, these treatments also led to a significant increase in various fruit quality parameters such as hundred fruit weight, firmness, soluble solid, soluble sugar, titratable, vitamin C, soluble protein, β-Carotene content and superoxide dismutase, peroxidase activities. Additionally, they were found to effectively reduce rot rate, polyphenol oxidase activity, malondialdehyde content and relative conductivity. The activity of pectin methylesterase, polygalacturonase, cellulase and β-galactose was reduced by amino acid calcium and sugar alcohol calcium. All three types of exogenous calcium down-regulated the expression of PME and ChCaBP1. Additionally, amino acid calcium and sugar alcohol calcium decreased the expression of PG, Cx, and BGal. Exogenous calcium reduces the size of stomata in the fruit epidermis, leading to a decrease in both fruit respiration rate and transpiration. Of the three calcium preparations, amino acid calcium and sugar alcohol calcium were more effective than CaCl2, with 0.12 g·L−1sugar alcohol calcium and 0.06 g·L−1 amino acid calcium being the most effective. [ABSTRACT FROM AUTHOR]

Published

2023

16. Overexpression of a Senescence-Related Gene CpSRG1 from Wintersweet (Chimonanthus praecox) Promoted Growth and Flowering, and Delayed Senescence in Transgenic Arabidopsis.

Author

Cao, Yinzhu, Li, Guixiang, Wang, Xia, Huang, Renwei, Luo, Jianghui, Li, Mingyang, Liu, Daofeng, and Sui, Shunzhao

Subjects

GENETIC overexpression, GENETIC regulation, GENE expression, ARABIDOPSIS, WOOD chemistry

Abstract

Plant senescence is a complex process that is controlled by developmental regulation and genetic programs. A senescence-related gene CpSRG1, which belongs to the 2OG-Fe(II) dioxygenase superfamily, was characterized from wintersweet, and the phylogenetic relationship of CpSRG1 with homologs from other species was investigated. The expression analysis by qRT-PCR (quantitative real-time PCR) indicated that CpSRG1 is abundant in flower organs, especially in petals and stamens, and the highest expression of CpSRG1 was detected in stage 6 (withering period). The expression patterns of the CpSRG1 gene were further confirmed in CpSRG1pro::GUS (β-glucuronidase) plants, and the activity of the CpSRG1 promoter was enhanced by exogenous Eth (ethylene), SA (salicylic acid), and GA3 (gibberellin). Heterologous overexpression of CpSRG1 in Arabidopsis promoted growth and flowering, and delayed senescence. Moreover, the survival rates were significantly higher and the root lengths were significantly longer in the transgenic lines than in the wild-type plants, both under low nitrogen stress and GA3 treatment. This indicated that the CpSRG1 gene may promote the synthesis of assimilates in plants through the GA pathway, thereby improving growth and flowering, and delaying senescence in transgenic Arabidopsis. Our study has laid a satisfactory foundation for further analysis of senescence-related genes in wintersweet and wood plants. It also enriched our knowledge of the 2OG-Fe(II) dioxygenase superfamily, which plays a variety of important roles in plants. [ABSTRACT FROM AUTHOR]

Published

2022

17. Identification of key mitochondria-related genes and their potential crosstalk role with immune pattern in Idiopathic pulmonary fibrosis.

Author

Huang, Jun, Wang, Xia, Zeng, Youjie, Xu, Huilin, Zhang, Siyi, Ding, Zhigang, and Guo, Ren

Subjects

*IDIOPATHIC pulmonary fibrosis, *INTERSTITIAL lung diseases, *GENE expression, *RECEIVER operating characteristic curves, *PULMONARY fibrosis

Abstract

• ALDH18A1, ACAT1, MCCC1, and PDHA1 were identified as key differentially expressed mitochondria-related genes (DEMTRGs) in IPF. • The potential functions of key DEMTRGs were assessed through a comprehensive bioinformatics analysis. • The four key DEMTRGs may pave the way for further exploration of novel therapeutic targets for IPF. Idiopathic pulmonary fibrosis (IPF) stands out as a life-threatening and one of the most severe interstitial lung diseases. The pathogenesis of IPF is not fully understood, while recent studies have highlighted the association of mitochondrial dysfunction with IPF. This study is dedicated to pinpointing crucial genes related to mitochondria that potentially impact the advancement of IPF, thereby offering new perspectives on the pathogenesis of this condition. The Gene Expression Omnibus (GEO) database was utilized to download three datasets (GSE32537, GSE92592, and GSE150910), following which a comprehensive analysis was conducted to identify differentially expressed mitochondria-related genes (DEMTRGs) in the IPF lung tissues. Subsequently, GO and KEGG enrichment analysis of the DEMTRGs was performed. Next, external datasets and in vivo experiments were performed to validate their expression. Additionally, a Logistic regression model based on key DEMTRGs was constructed, and the model's ability to distinguish between IPF and controls was evaluated using the area under the receiver operating characteristic (ROC) curve (AUC). Finally, gene set enrichment analysis (GSEA) and CIBERSORT algorithm were conducted. We identified five key DEMTRGs (ALDH18A1, ALDH1B1, MCCC1, ACAT1, and PDHA1), ALDH18A1 and ALDH1B1 exhibited upregulated expression levels, whereas MCCC1, ACAT1, and PDHA1 showed downregulation in the lung tissue of individuals with IPF. The expression levels of these key DEMTRGs were validated by an independent external dataset (GSE53845) and the bleomycin-induced pulmonary fibrosis mice. In addition, the ROCs indicated that the diagnostic model constructed based on key DEMTRGs could effectively distinguish between IPF and controls (AUC>0.8). GSEA analysis and immune-related analysis shed light on the potential mechanisms through which these key DEMTRGs influence IPF. Our research has pinpointed key genes associated with mitochondria that may ultimately contribute to the progression of IPF by exerting regulatory effects on mitochondrial function, thereby influencing multiple cellular processes. [ABSTRACT FROM AUTHOR]

Published

2024

18. Colorectal Cancer Patient‐Derived 2D and 3D Models Efficiently Recapitulate Inter‐ and Intratumoral Heterogeneity.

Author

Zhao, Yuanyuan, Zhang, Bing, Ma, Yiming, Zhao, Fuqiang, Chen, Jianan, Wang, Bingzhi, Jin, Hua, Zhou, Fulai, Guan, Jiawei, Zhao, Qian, Wang, Hongying, Liu, Qian, Zhao, Fangqing, and Wang, Xia

Subjects

COLORECTAL cancer, DRUG resistance in cancer cells, GENE expression profiling, GENE expression, HETEROGENEITY, TUMOR growth

Abstract

Pre‐existing drug resistance and tumorigenicity of cancer cells are highly correlated with therapeutic failure and tumor growth. However, current cancer models are limited in their application to the study of intratumor functional heterogeneity in personalized oncology. Here, an innovative two‐dimensional (2D) and three‐dimensional (3D) model for patient‐derived cancer cells (PDCCs) and air–liquid interface (ALI) organotypic culture is established from colorectal cancer (CRC). The PDCCs recapitulate the genomic landscape of their parental tumors with high efficiency, high proliferation rate, and long‐term stability, while corresponding ALI organotypic cultures retain histological architecture of their original tumors. Interestingly, both 2D and 3D models maintain the transcriptomic profile of the corresponding primary tumors and display the same trend in response to 5‐Fluoruracil, regardless of their difference in gene expression profiles. Furthermore, single‐cell‐derived clones() are efficiently established and pre‐existing drug‐resistant clones and highly tumorigenic clones within individual CRC tumors are identified. It is found that tumorigenic cancer cells do not necessarily possess the stem cells characteristics in gene expression. This study provides valuable platform and resource for exploring the molecular mechanisms underlying the pre‐existing drug resistance and tumorigenicity in cancer cells, as well as for developing therapeutic targets specifically for pre‐existing drug‐resistant or highly tumorigenic clones. [ABSTRACT FROM AUTHOR]

Published

2022

19. Unique ER PR expression pattern in breast cancers with CHEK2 mutation: a hormone receptor and HER2 analysis based on germline cancer predisposition genes.

Author

Wei, Grace, Teng, Mingxiang, Rosa, Marilin, and Wang, Xia

Subjects

CANCER genes, HORMONE receptors, CHECKPOINT kinase 2, BREAST cancer, CANCER genetics, TUMOR suppressor genes, GENETIC mutation, HEREDITARY nonpolyposis colorectal cancer, HORMONE receptor positive breast cancer, PROTEIN kinases, RETROSPECTIVE studies, GERM cells, CELL receptors, ESTROGEN receptors, GENE expression, RESEARCH funding, BREAST tumors, PROGESTERONE receptors

Abstract

Purpose: Estrogen-receptor (ER) and progesterone-receptor (PR) expression levels in breast cancer, which have been principally compared via binomial descriptors, can vary widely across tumors. We sought to characterize ER and PR expression levels using semi-quantitative analyses of receptor staining in germline pathogenic variant (PV) carriers of cancer predisposition genes.Methods: We conducted a retrospective chart review of patients who underwent germline genetic testing for cancer predisposition genes at a tertiary cancer center genetics clinic. We performed comparisons of semi-quantitative ER and PR percentage staining levels across carriers and non-carriers of cancer predisposition genes.Results: Breast cancers from BRCA1 PV carriers expressed significantly lower ER (15.2% vs 78.2%, p < 0.001) and lower PR (6.8% vs 41.1%, p < 0.001) staining compared to non-PV carriers. Similarly, breast cancers of BRCA2 (66.7% vs 78.2%, p = 0.005) and TP53 (50.6% vs 78.2%, p = 0.015) PV tumors also displayed moderate decreases in ER staining. Conversely, CHEK2 tumors displayed higher ER (93.1% vs 78.2%, p = 0.005) and PR (72% vs 48.8%, p = 0.001) staining when compared to non-PV carriers. We observed a wide range of dispersion across the ER and PR staining levels of the carriers and noncarriers. ER and PR ranges of dispersion of CHEK2 tumors were uniquely narrower than all other groups.Conclusion: The findings of our study suggest that precise expression levels of ER and PR in breast cancers can vary widely. These differences are further augmented when comparing expression staining across PV and non-PV carriers, suggesting potentially unique tumorigenesis and progression pathways influenced by germline cancer predisposition genes. [ABSTRACT FROM AUTHOR]

Published

2022

20. miR-1968-5p is involved in the pathogenesis of lupus nephritis of NZBWF1 mice by targeting csf1.

Author

Li, Shipeng, Wang, Xia, Zhu, Xinxin, Xue, Yuan, Zhang, Junmei, Tan, Xiaohua, Deng, Jianghong, Li, Chao, Kuang, Weiying, and Li, Caifeng

Subjects

*LUPUS nephritis, *GENE expression, *PATHOGENESIS, *SYSTEMIC lupus erythematosus, *LABORATORY mice, *POLYMERASE chain reaction

Abstract

Objective: Lupus nephritis is one of the most common and severe systemic lupus erythematosus complications. However, the pathogenesis of lupus nephritis is still poorly understood. Increasing evidence has shown that microRNAs (miRNAs) are extensively involved in the pathophysiology of autoimmune diseases. NZBWF1 is the classical mouse model of lupus nephritis. The present study aimed to investigate the expression profiling of mRNA and miRNAs of NZBWF1 mice with lupus nephritis using microarray, and explored the potential molecular mechanism of miRNA. Methods: miRNA and mRNA microarrays were performed to identify miRNA and mRNA expression changes between pre-diseased (8-week-old) NZBWF1 mice and diseased NZBWF1 mice with lupus nephritis (28-week-old). Quantitative polymerase chain reaction (qPCR) validated these results. The target of miRNA was confirmed through a dual-luciferase reporter and stimulated mesangial cells experiment. Results: The combined miRNA and mRNA analysis identified 43 differentially expressed miRNAs and 1796 differentially expressed mRNAs between pre-disease (8-week-old) (n = 4) and diseased (28-week-old) NZBWF1 mice. We found that miR-1968-5p was significantly decreased, and csf1 mRNA was significantly increased in lupus nephritis mouse and verified by RT-PCR. csf1 has been demonstrated to play important roles in SLE. Bioinformatics analysis predicted that the csf1 was a potential target gene of miR-1968-5p. A dual-luciferase reporter assay confirmed the target binding. In cell experiments, overexpression or knockdown of miR resulted in a decrease or increase of csf1 expression, respectively. Conclusion: These results suggest that miR-1968-5p may be involved in the pathogenesis of lupus nephritis of NZBWF1 mice by targeting csf1. [ABSTRACT FROM AUTHOR]

Published

2021

21. Genome-Wide Investigation of the NAC Transcription Factor Family in Miscanthus sinensis and Expression Analysis Under Various Abiotic Stress.

Author

Nie, Gang, Yang, Zhongfu, He, Jie, Liu, Aiyu, Chen, Jiayi, Wang, Shuan, Wang, Xia, Feng, Guangyan, Li, Dandan, Peng, Yan, Huang, Linkai, and Zhang, Xinquan

Subjects

ABIOTIC stress, TRANSCRIPTION factors, MISCANTHUS, CHROMOSOME duplication, GENE families, ISOELECTRIC point, SUPPLY & demand, ENERGY crops

Abstract

The NAC transcription factor family is deemed to be a large plant-specific gene family that plays important roles in plant development and stress response. Miscanthus sinensis is commonly planted in vast marginal land as forage, ornamental grass, or bioenergy crop which demand a relatively high resistance to abiotic stresses. The recent release of a draft chromosome-scale assembly genome of M. sinensis provided a basic platform for the genome-wide investigation of NAC proteins. In this study, a total of 261 M. sinensis NAC genes were identified and a complete overview of the gene family was presented, including gene structure, conserved motif compositions, chromosomal distribution, and gene duplications. Results showed that gene length, molecular weights (MW), and theoretical isoelectric points (pI) of NAC family were varied, while gene structure and motifs were relatively conserved. Chromosomal mapping analysis found that the M. sinensis NAC genes were unevenly distributed on 19 M. sinensis chromosomes, and the interchromosomal evolutionary analysis showed that nine pairs of tandem duplicates genes and 121 segmental duplications were identified, suggesting that gene duplication, especially segmental duplication, is possibly associated with the amplification of M. sinensis NAC gene family. The expression patterns of 14 genes from M. sinensis SNAC subgroup were analyzed under high salinity, PEG, and heavy metals, and multiple NAC genes could be induced by the treatment. These results will provide a very useful reference for follow-up study of the functional characteristics of NAC genes in the mechanism of stress-responsive and potential roles in the development of M. sinensis. [ABSTRACT FROM AUTHOR]

Published

2021

22. Long Noncoding RNA Facilitates Endometrial Cancer Development by Regulating and Gene Expressions.

Author

Liu, Tong, Wang, Xia, Zhai, Jingfang, Wang, Qing, and Zhang, Bei

Subjects

*IN vivo studies, *GENE expression, *ENDOMETRIAL tumors

Abstract

Objective: Long noncoding RNA urothelial carcinoma associated 1 (UCA1) was found to facilitate endometrial cancer cell metastasis, and high UCA1 expression predicted endometrial cancer development and patients' worsened outcomes. This research aimed to investigate the cancer promoting role and mechanism of UCA1 in endometrial cancer. Materials and Methods: Around 64 endometrioid adenocarcinoma patients' tissue specimens were analyzed by qRT-PCR. Primary endometrial cancer cell culture was established in vitro. UCA1 overexpression or knockdown was executed by adenoviral transduction. Cell proliferation, apoptosis, colony formation, transwell invasion, and epithelia-to-mesenchymal transition of primary endometrial cancer cells were assessed. Interactions among UCA1, microRNAs (miRNAs), and mRNAs were investigated by luciferase reporter assay and argonaute 2 (AGO2)-RNA immunoprecipitation. Nude mouse xenograft assay was used to explore the role of UCA1 in endometrial cancer in vivo. Results:UCA1 was significantly upregulated in endometrial cancer tissues compared to normal tissues. High expression of UCA1 associated with endometrial cancer progression and patients' decreased survival. Overexpressing UCA1 significantly increased the malignancy of primary endometrial cancer cells in vitro, while UCA1 knockdown showed opposite effect. Kruppel-like factor 5 (KLF5) and relaxin like family peptide receptor 1 (RXFP1) were found as two UCA1 co-expressing genes in endometrial cancer. UCA1 increased the malignancy of endometrial cells partially through KLF5, and it increased the relaxin 2-induced endometrial cancer cell metastasis through RXFP1. UCA1 reduced the si-RNA-induced silencing of KLF5 and RXFP1 genes in endometrial cancer cells. MiR-143-3p and miR-1-3p were found to interact with both UCA1 and KLF5 mRNA. In addition, knockdown of UCA1 suppressed tumor growth in endometrial cancer in vivo. Conclusion:UCA1 might facilitate endometrial cancer development by upregulating KLF5 and RXFP1 gene expression by sponging miR-143-3p and miR-1-3p. [ABSTRACT FROM AUTHOR]

Published

2021

23. Modulating Thyroid Hormone Levels in Adult Mice: Impact on Behavior and Compensatory Brain Changes.

Author

Niedowicz, Dana M., Wang, Wang-Xia, Price, Doug A., and Nelson, Peter T.

Subjects

BRAIN physiology, THYROID hormones, HYPOTHYROIDISM, HORMONE antagonists, HYPERTHYROIDISM, ANIMAL experimentation, AGE distribution, THYROXINE, COGNITION, NEUROLOGIC manifestations of general diseases, SEX distribution, GENE expression, THYROID antagonists, MICE

Abstract

Thyroid hormone (TH) perturbation is a common medical problem. Because of substantial public health impact, prior researchers have studied hyper- and hypothyroidism in animal models. Although most prior research focused on in utero and/or developmental effects, changes in circulating TH levels are commonly seen in elderly individuals: approximately 20% of persons older than 80 years have clinically impactful hypothyroidism and up to 5% have clinical hyperthyroidism, with women being more often affected than men. TH disease model methodology in mice have varied but usually focus on a single sex, and the impact(s) of TH perturbation on the adult brain are not well understood. We administered thyroxine to middle-aged (13 to 14 months) male and female mice to model hyperthyroidism and TH-lowering drugs propylthiouracil (PTU) and methimazole, to induce hypothyroidism. These pharmacological agents are used commonly in adult humans. Circulating TH-level changes were observed when thyroxine was dosed at 20 µg/mL in drinking water for two weeks. By contrast, PTU and methimazole did not elicit a consistent reproducible effect until two months of treatment. No substantial changes in TH levels were detected in brain tissues of treated animals; however, pronounced changes in gene expression, specifically for TH-processing transcripts, were observed following the treatment with thyroxine. Our study indicated a robust compensatory mechanism by which the brain tissue/cells minimize the TH fluctuation in CNS by altering gene expression. Neurobehavioral changes were related to the TH perturbation and suggested potential associations between cognitive status and hyper- and hypothyroidism. [ABSTRACT FROM AUTHOR]

Published

2021

24. Identification of the Valid Reference Genes for Quantitative RT-PCR in Annual Ryegrass (Lolium multiflorum) under Salt Stress

Author

Wang Xia, Linkai Huang, Xinquan Zhang, and Xiao Ma

Subjects

Salinity, Soil salinity, reference gene, Pharmaceutical Science, Genes, Plant, Real-Time Polymerase Chain Reaction, Article, Analytical Chemistry, lcsh:QD241-441, annual ryegrass, lcsh:Organic chemistry, Gene Expression Regulation, Plant, Stress, Physiological, Reference genes, Drug Discovery, Gene expression, Lolium, Reference gene, Physical and Theoretical Chemistry, Gene, salt stress, biology, Gene Expression Profiling, Organic Chemistry, food and beverages, qRT-PCR, Lolium multiflorum, Reference Standards, biology.organism_classification, Real-time polymerase chain reaction, Agronomy, Chemistry (miscellaneous), Organ Specificity, Molecular Medicine

Abstract

Annual ryegrass (Lolium multiflorum) is a cool-season annual grass cultivated worldwide for its high yield and quality. With the areas of saline soil increasing, investigation of the molecular mechanisms of annual ryegrass tolerance under salt stress has become a significant topic. qRT-PCR has been a predominant assay for determination of the gene expression, in which selecting a valid internal reference gene is a crucial step. The objective of present study was to evaluate and identify suitable reference genes for qRT-PCR in annual ryegrass under salt stress. The results calculated by RefFinder indicated that eEF1A(s) was the most stable reference gene in leaves, whereas EF1-a was the least stable, meanwhile, TBP-1 was the most optimal in roots and in all samples, and the eIF-5A shouldn’t be utilized for normalization of the gene expression. eEF1A(s) is more suitable than TBP-1 as reference gene in leaves when verified with P5CS1 and Cyt-Cu/Zn SOD genes. We should choose optimal reference genes in specific tissues instead of the most stable one selected from different conditions and tissues.

Published

2015

25. Aberrant Methylation and Differential Expression of SLC2A1, TNS4, GAPDH, ATP8A2, and CASZ1 Are Associated with the Prognosis of Lung Adenocarcinoma.

Author

Wang, Xia, Shi, Dongming, Zhao, Dejun, and Hu, Danping

Subjects

*LUNG cancer prognosis, *ADENOCARCINOMA, *CELLULAR signal transduction, *GENE expression, *METHYLATION, *MULTIVARIATE analysis, *REGRESSION analysis, *STATISTICS, *SURVIVAL analysis (Biometry), *TISSUES

Abstract

Lung cancer is one of the leading triggers for cancer death worldwide. In this study, the relationship of the aberrantly methylated and differentially expressed genes in lung adenocarcinoma (LUAD) with cancer prognosis was investigated, and 5 feature genes were identified eventually. Specifically, we firstly downloaded the LUAD-related mRNA expression profile (including 57 normal tissue samples and 464 LUAD tissue samples) and Methy450 expression data (including 32 normal tissue samples and 373 LUAD tissue samples) from the TCGA database. The package "limma" was used to screen differentially expressed genes and aberrantly methylated genes, which were intersected for identifying the hypermethylated downregulated genes (DGs Hyper) and the hypomethylated upregulated genes (UGs Hypo). GO annotation and KEGG pathway enrichment analysis were further performed, and it was found that these DGs Hyper and UGs Hypo were predominantly activated in the biological processes and signaling pathways such as the regulation of vasculature development, DNA-binding transcription activator activity, and Ras signaling pathway, indicating that these genes play a vital role in the initiation and progression of LUAD. Additionally, univariate and multivariate Cox regression analyses were conducted to find the genes significantly associated with LUAD prognosis. Five genes including SLC2A1, TNS4, GAPDH, ATP8A2, and CASZ1 were identified, with the former three highly expressed and the latter two poorly expressed in LUAD, indicating poor prognosis of LUAD patients as judged by survival analysis. [ABSTRACT FROM AUTHOR]

Published

2020

26. Retaining MKP1 expression and attenuating JNK-mediated apoptosis by RIP1 for cisplatin resistance through miR-940 inhibition

Author

Wang, Qiong, Shi, Shaoqing, He, Weiyang, Padilla, Mabel T., Zhang, Lin, Wang, Xia, Zhang, Bin, and Lin, Yong

Subjects

MAP Kinase Kinase 4, apoptosis, JNK Mitogen-Activated Protein Kinases, cisplatin, chemoresistance, Gene Expression, RNA-Binding Proteins, Antineoplastic Agents, Dual Specificity Phosphatase 1, Gene Expression Regulation, Neoplastic, Nuclear Pore Complex Proteins, lung cancer, MicroRNAs, Drug Resistance, Neoplasm, Cell Line, Tumor, Gene Knockdown Techniques, Humans, RIP1, JNK, RNA, Messenger, MKP1, Research Paper, Signal Transduction

Abstract

The elucidation of chemoresistance mechanisms is important to improve cancer patient survival. In this report, we investigated the role and mechanism through which receptor-interacting protein 1 (RIP1), a mediator in cell survival and death signaling, participates in cancer's response to chemotherapy. In lung cancer cells, knockdown of RIP1 substantially increased cisplatin-induced apoptotic cytotoxicity, which was associated with robust JNK activation. The expression of the JNK inactivating phosphatase, MKP1, was substantially reduced in RIP1 knockdown cells. Although MKP1 protein stability was not altered by RIP1 suppression, the synthesis rate of MKP1 was dramatically reduced in RIP1-suppressed cells. Furthermore, we found that the expression of miR-940 was substantially increased in RIP1 knockdown cells. Knockdown of miR-940 restored MKP1 expression and attenuated cisplatin-induced JNK activation and cytotoxicity. Importantly, ectopic expression of MKP1 effectively attenuated cisplatin-induced JNK activation and cytotoxicity. In addition, activation of the JNK upstream signaling kinase, MKK4, was also potentiated in RIP1 knockdown cells. Altogether, our results suggest that RIP1 contributes to cisplatin resistance by suppressing JNK activation that involves releasing miR-940-mediated inhibition of MKP1 and suppressing activation of MKK4. Intervention targeting the RIP1/miR-940/MKP1/JNK pathway may be used to sensitize platinum-based chemotherapy.

Published

2014

27. A Customized Quantitative PCR MicroRNA Panel Provides a Technically Robust Context for Studying Neurodegenerative Disease Biomarkers and Indicates a High Correlation Between Cerebrospinal Fluid and Choroid Plexus MicroRNA Expression

Author

Peter T. Nelson, Gregory A. Jicha, Wang-Xia Wang, and David W. Fardo

Subjects

0301 basic medicine, Cost effectiveness, Neuroscience (miscellaneous), Gene Expression, Biology, Bioinformatics, Real-Time Polymerase Chain Reaction, Article, 03 medical and health sciences, Cellular and Molecular Neuroscience, Cerebrospinal fluid, microRNA, Humans, Gene Expression Profiling, Brain, Neurodegenerative Diseases, Gene expression profiling, MicroRNAs, 030104 developmental biology, Real-time polymerase chain reaction, Neurology, Choroid Plexus, Biomarker (medicine), Choroid plexus, RNA extraction, Biomarkers

Abstract

MicroRNA (miRNA) expression varies in association with different tissue types and in diseases. Having been found in body fluids including blood and cerebrospinal fluid (CSF), miRNAs constitute potential biomarkers. CSF miRNAs have been proposed as biomarkers for neurodegenerative diseases; however, there is a lack of consensus about the best candidate miRNA biomarkers and there has been variability in results from different research centers, perhaps due to technical factors. Here, we sought to optimize technical parameters for CSF miRNA studies. We examined different RNA isolation methods and performed miRNA expression profiling with TaqMan® miRNA Arrays. More specifically, we developed a customized CSF-miRNA low-density array (TLDA) panel that contains 47 targets: miRNAs shown previously to be relevant to neurodegenerative disease, miRNAs that are abundant in CSF, data normalizers, and controls for potential blood and tissue contamination. The advantages of using this CSF-miRNA TLDA panel include specificity, sensitivity, fast processing and data analysis, and cost effectiveness. We optimized technical parameters for this assay. Further, the TLDA panel can be tailored to other specific purposes. We tested whether the profile of miRNAs in the CSF resembled miRNAs isolated from brain tissue (hippocampus or cerebellum), blood, or the choroid plexus. We found that the CSF miRNA expression profile most closely resembles that of choroid plexus tissue, underscoring the potential importance of choroid plexus-derived signaling through CSF miRNAs. In summary, the TLDA miRNA array panel will enable evaluation and discovery of CSF miRNA biomarkers and can potentially be utilized in clinical diagnosis and disease stage monitoring.

Published

2016

28. Patterns of microRNA expression in normal and early Alzheimer’s disease human temporal cortex: white matter versus gray matter

Author

Arnold J. Stromberg, Qingwei Huang, Yanling Hu, Wang-Xia Wang, and Peter T. Nelson

Subjects

Pathology, medicine.medical_specialty, Statistics as Topic, Biology, Nerve Fibers, Myelinated, Article, Pathology and Forensic Medicine, White matter, Cellular and Molecular Neuroscience, Alzheimer Disease, microRNA, Gene expression, medicine, Humans, Northern blot, Nerve Tissue, Aged, Oligonucleotide Array Sequence Analysis, Aged, 80 and over, Temporal cortex, Amyloid beta-Peptides, Gene Expression Profiling, Neurofibrillary Tangles, medicine.disease, Temporal Lobe, Gene expression profiling, MicroRNAs, medicine.anatomical_structure, Cerebral cortex, Postmortem Changes, Female, Neurology (clinical), Alzheimer's disease

Abstract

MicroRNA (miRNA) expression was assessed in human cerebral cortical gray matter (GM) and white matter (WM) in order to provide the first insights into the difference between GM and WM miRNA repertoires across a range of Alzheimer's disease (AD) pathology. RNA was isolated separately from GM and WM portions of superior and middle temporal cerebral cortex (N = 10 elderly females, postmortem interval < 4 h). miRNA profiling experiments were performed using state-of-the-art Exiqon© LNA-microarrays. A subset of miRNAs that appeared to be strongly expressed according to the microarrays did not appear to be conventional miRNAs according to Northern blot analyses. Some well-characterized miRNAs were substantially enriched in WM as expected. However, most of the miRNA expression variability that correlated with the presence of early AD-related pathology was seen in GM. We confirm that downregulation of a set of miRNAs in GM (including several miR-15/107 genes and miR-29 paralogs) correlated strongly with the density of diffuse amyloid plaques detected in adjacent tissue. A few miRNAs were differentially expressed in WM, including miR-212 that is downregulated in AD and miR-424 which is upregulated in AD. The expression of certain miRNAs correlates with other miRNAs across different cases, and particular subsets of miRNAs are coordinately expressed in relation to AD-related pathology. These data support the hypothesis that patterns of miRNA expression in cortical GM may contribute to AD pathogenetically, because the aggregate change in miRNA expression observed early in the disease would be predicted to cause profound changes in gene expression.

Published

2010

29. Differential and dynamic regulation of miR398 in response to ABA and salt stress in Populus tremula and Arabidopsis thaliana

Author

Guiliang Tang, Wang-Xia Wang, Qi-Jun Chen, Venugopal Mendu, Xiaoqing Tang, Benjamin Willcut, Randy D. Dinkins, Ligang Ren, and Xiaoyun Jia

Subjects

Arabidopsis, Endogeny, Plant Science, chemistry.chemical_compound, Superoxide Dismutase-1, Species Specificity, Gene Expression Regulation, Plant, Botany, Gene expression, microRNA, Genetics, Arabidopsis thaliana, Abscisic acid, Gene, Plant Proteins, biology, Superoxide Dismutase, Abiotic stress, fungi, food and beverages, General Medicine, biology.organism_classification, Cell biology, Kinetics, MicroRNAs, Populus, chemistry, RNA, Plant, Salts, Agronomy and Crop Science, Abscisic Acid

Abstract

MicroRNAs (miRNAs) are endogenous small RNAs of ~22 nucleotides (nt) that play a key role in down regulation of gene expression at the post-transcriptional level in plants and animals. Various studies have identified numerous miRNAs that were either up regulated or down regulated upon stress treatment. Here, we sought to understand the temporal regulation of miRNAs in different plant species under abscisic acid (ABA) and salt (NaCl) stress. Our results showed that the regulation of miR398 in response to ABA and salt stress was more dynamic in plants than previously reported. In poplars, miR398 was first induced upon 3-4 h of ABA or salt stress. However, this induction declined after 48 h and finally accumulated again over a prolonged stress (72 h). We referred to this kind of regulation as dynamic regulation. In contrast, such dynamic regulation of miR398 under salt stress was completely absent in Arabidopsis, in which miR398 was steadily and unidirectionally suppressed. Interestingly, ABA treatment caused a deviate dynamic regulation of miR398 in Arabidopsis, showing an opposite response as compared to that in poplars. We referred to the difference in regulation between Arabidopsis and poplars as differential regulation. Furthermore, the expression of the miR398 target, copper superoxide dismutase1 (CSD1), was in reverse correlation with the miR398 level, suggesting a control of this specific target expression predominantly by miR398 under abiotic stress. Together, these data consistently show a correlated regulation between miR398 and its representative target, CSD1, by ABA and salt stresses, and raise the possibility that regulation of miRNAs in plants is twofold: a dynamic regulation within a plant species and a differential regulation between different plant species.

Published

2009

30. Energizing miRNA research: A review of the role of miRNAs in lipid metabolism, with a prediction that miR-103/107 regulates human metabolic pathways

Author

Bernard R. Wilfred, Wang-Xia Wang, and Peter T. Nelson

Subjects

Endocrinology, Diabetes and Metabolism, Computational biology, Cell fate determination, Biology, Biochemistry, Article, Enzyme activator, Endocrinology, Acetyl Coenzyme A, microRNA, Gene expression, Adipocytes, Genetics, Animals, Humans, RNA, Messenger, Molecular Biology, Gene, Cells, Cultured, Lipid metabolism, Lipid Metabolism, Enzyme Activation, MicroRNAs, Phosphotransferases (Alcohol Group Acceptor), Metabolic pathway, Energy Metabolism, Ribosomes, Metabolic Networks and Pathways, Function (biology)

Abstract

MicroRNAs (miRNAs) are powerful regulators of gene expression. Although first discovered in worm larvae, miRNAs play fundamental biological roles-including in humans-well beyond development. MiRNAs participate in the regulation of metabolism (including lipid metabolism) for all animal species studied. A review of the fascinating and fast-growing literature on miRNA regulation of metabolism can be parsed into three main categories: (1) adipocyte biochemistry and cell fate determination; (2) regulation of metabolic biochemistry in invertebrates; and (3) regulation of metabolic biochemistry in mammals. Most research into the 'function' of a given miRNA in metabolic pathways has concentrated on a given miRNA acting upon a particular 'target' mRNA. Whereas in some biological contexts the effects of a given miRNA:mRNA pair may predominate, this might not be the case generally. In order to provide an example of how a single miRNA could regulate multiple 'target' mRNAs or even entire human metabolic pathways, we include a discussion of metabolic pathways that are predicted to be regulated by the miRNA paralogs, miR-103 and miR-107. These miRNAs, which exist in vertebrate genomes within introns of the pantothenate kinase (PANK) genes, are predicted by bioinformatics to affect multiple mRNA targets in pathways that involve cellular Acetyl-CoA and lipid levels. Significantly, PANK enzymes also affect these pathways, so the miRNA and 'host' gene may act synergistically. These predictions require experimental verification. In conclusion, a review of the literature on miRNA regulation of metabolism leads us believe that the future will provide researchers with many additional energizing revelations.

Published

2007

31. Mitochondria-associated microRNAs in rat hippocampus following traumatic brain injury

Author

Wang-Xia Wang, Nishant P. Visavadiya, Peter T. Nelson, Jignesh D. Pandya, Patrick G. Sullivan, and Joe E. Springer

Subjects

Male, Cytoplasm, Biology, Hippocampus, Article, Rats, Sprague-Dawley, Developmental Neuroscience, mir-223, miR-150, microRNA, Gene expression, medicine, Gene silencing, Animals, Cells, Cultured, Neurodegeneration, Argonaute, medicine.disease, Mitochondria, Rats, MicroRNAs, Neurology, Brain Injuries, biology.protein, Neuroscience, Dicer

Abstract

Traumatic brain injury (TBI) is a major cause of death and disability. However, the molecular events contributing to the pathogenesis are not well understood. Mitochondria serve as the powerhouse of cells, respond to cellular demands and stressors, and play an essential role in cell signaling, differentiation, and survival. There is clear evidence of compromised mitochondrial function following TBI, however, the underlying mechanisms and consequences are not clear. MicroRNAs (miRNAs) are small non-coding RNA molecules that regulate gene expression post-transcriptionally, and function as important mediators of neuronal development, synaptic plasticity, and neurodegeneration. Several miRNAs show altered expression following TBI, however, the relevance of mitochondria in these pathways is unknown. Here, we present evidence supporting the association of miRNA with hippocampal mitochondria, as well as changes in mitochondria-associated miRNA expression following a controlled cortical impact (CCI) injury in rats. Specifically, we found that the miRNA processing proteins Argonaute (AGO) and Dicer are present in mitochondria fractions from uninjured rat hippocampus, and immunoprecipitation of AGO associated miRNA from mitochondria suggests the presence of functional RNA-induced silencing complexes. Interestingly, RT-qPCR miRNA array studies revealed that a subset of miRNA is enriched in mitochondria relative to cytoplasm. At 12 hour following CCI, several miRNAs are significantly altered in hippocampal mitochondria and cytoplasm. In addition, levels of miR-155 and miR-223, both of which play a role in inflammatory processes, are significantly elevated in both cytoplasm and mitochondria. We propose that mitochondria-associated miRNAs may play an important role in regulating the response to TBI.

Published

2015

32. PEDF protects human retinal pigment epithelial cells against oxidative stress via upregulation of UCP2 expression.

Author

Wang, Xia, Liu, Xu, Ren, Yuan, Liu, Ying, Han, Shuangyu, Zhao, Jingkang, Gou, Xingchun, and He, Yuan

Subjects

*RHODOPSIN, *OXIDATIVE stress, *EPITHELIAL cells, *UNCOUPLING proteins, *GENE expression, *IMMUNOFLUORESCENCE, *ONE-way analysis of variance, *MULTIPLE comparisons (Statistics)

Abstract

To investigate the protective function of pigment epithelium-derived factor (PEDF) against oxidative stress (OS) in ARPE-19 cells, ARPE-19 cells were divided into different OS groups and treated with various concentrations of H2O2 (0, 75, 150 and 200 µmol/l) for 24 h. To establish the protective group, 200 ng/ml of PEDF was administered to ARPE-19 cells. Cell Counting Kit-8 assays and cell growth curve experiments were performed to determine levels of cell viability; lactate dehydrogenase and propidium iodide (PI) staining assays were also performed. The expression levels of genes associated with apoptosis as well as uncoupling protein 2 (UCP2) were detected by reverse transcription-quantitative, or semi-quantitative polymerase chain reaction. Furthermore, an OS injury animal model was established in both C57BL/6 and BALB/c mice via injection of 5 µg of PEDF in the vitreous cavity and subsequent injection of 150 µM H2O2 following a 24 h time interval. Hematoxylin and eosin (H&E) staining, as well as UCP2 immunofluorescent labeling were also performed. One-way analysis of variance was used to determine statistically significant differences, followed by multiple comparison analysis using the Newman Keuls method. The results of cell viability assays demonstrated that the numbers of apoptotic cells were increased following treatment with H2O2 in a dose-dependent manner; however, this effect was reversed following treatment with PEDF. The expression levels of caspase 3 and B cell lymphoma (Bcl2) associated X genes associated with apoptosis were inhibited, whereas levels of the anti-apoptotic gene Bcl2 were enhanced following treatment with PEDF in different passages of ARPE-19 cells. Significant differences were demonstrated in the levels of UCP2 gene expression between the PEDF+ H2O2 treated group and cells treated with H2O2 alone. Labeling of the UCP2 detector in the confocal images demonstrated decreased UCP2 protein staining in the retinal pigment epithelium (RPE) cells and RPE layers following H2O2 injury; however, this effect was inhibited following treatment with PEDF. H&E staining was performed to investigate the thickness of the RPE layers, and the results revealed that thicknesses were significantly increased in sections treated with PEDF during OS, due to increased numbers of RPE cells. Furthermore, PEDF was demonstrated to increase UCP2 gene expression in ARPE-19 cells and animal RPE layers under OS, which suggested that PEDF may protect RPE cells and tissues during oxidative injury. [ABSTRACT FROM AUTHOR]

Published

2019

33. Identification of potential functional genes in papillary thyroid cancer by co‑expression network analysis.

Author

Ao, Zeng-Xin, Chen, Yuan-Cheng, Lu, Jun-Min, Shen, Jie, Peng, Lin-Ping, Lin, Xu, Peng, Cheng, Zeng, Chun-Ping, Wang, Xia-Fang, Zhou, Rou, Chen, Zhi, Xiao, Hong-Mei, and Deng, Hong-Wen

Subjects

THYROID cancer, GENE regulatory networks, GENE expression, GENETIC transcription, FUNCTIONAL analysis, GENETICS

Abstract

Interactions between multiple genes are involved in the development of complex diseases. However, there are few analyses of gene interactions associated with papillary thyroid cancer (PTC). Weighted gene co‑expression network analysis (WGCNA) is a novel and powerful method that detects gene interactions according to their co‑expression similarities. In the present study, WGCNA was performed in order to identify functional genes associated with PTC using R package. First, differential gene expression analysis was conducted in order to identify the differentially expressed genes (DEGs) between PTC and normal samples. Subsequently, co‑expression networks of the DEGs were constructed for the two sample groups, respectively. The two networks were compared in order to identify a poorly preserved module. Concentrating on the significant module, validation analysis was performed to confirm the identified genes and combined functional enrichment analysis was conducted in order to identify more functional associations of these genes with PTC. As a result, 1062 DEGs were identified for network construction. A brown module containing 118 highly related genes was selected as it exhibited the lowest module preservation. After validation analysis, 61 genes in the module were confirmed to be associated with PTC. Following the enrichment analysis, two PTC‑related pathways were identified: Wnt signal pathway and transcriptional misregulation in cancer. LRP4, KLK7, PRICKLE1, ETV4 and ETV5 were predicted to be candidate genes regulating the pathogenesis of PTC. These results provide novel insights into the etiology of PTC and the identification of potential functional genes. [ABSTRACT FROM AUTHOR]

Published

2018

34. The Epstein Barr virus circRNAome.

Author

Ungerleider, Nathan, Concha, Monica, Lin, Zhen, Roberts, Claire, Wang, Xia, Cao, Subing, Baddoo, Melody, Moss, Walter N., Yu, Yi, Seddon, Michael, Lehman, Terri, Tibbetts, Scott, Renne, Rolf, Dong, Yan, and Flemington, Erik K.

Subjects

DNA-binding proteins, MOLECULAR biology, HYDROLASES, RNA sequencing, HERPESVIRUSES

Abstract

Our appreciation for the extent of Epstein Barr virus (EBV) transcriptome complexity continues to grow through findings of EBV encoded microRNAs, new long non-coding RNAs as well as the more recent discovery of over a hundred new polyadenylated lytic transcripts. Here we report an additional layer to the EBV transcriptome through the identification of a repertoire of latent and lytic viral circular RNAs. Utilizing RNase R-sequencing with cell models representing latency types I, II, and III, we identified EBV encoded circular RNAs expressed from the latency Cp promoter involving backsplicing from the W1 and W2 exons to the C1 exon, from the EBNA BamHI U fragment exon, and from the latency long non-coding RPMS1 locus. In addition, we identified circular RNAs expressed during reactivation including backsplicing from exon 8 to exon 2 of the LMP2 gene and a highly expressed circular RNA derived from intra-exonic backsplicing within the BHLF1 gene. While expression of most of these circular RNAs was found to depend on the EBV transcriptional program utilized and the transcription levels of the associated loci, expression of LMP2 exon 8 to exon 2 circular RNA was found to be cell model specific. Altogether we identified over 30 unique EBV circRNAs candidates and we validated and determined the structural features, expression profiles and nuclear/cytoplasmic distributions of several predominant and notable viral circRNAs. Further, we show that two of the EBV circular RNAs derived from the RPMS1 locus are detected in EBV positive clinical stomach cancer specimens. This study increases the known EBV latency and lytic transcriptome repertoires to include viral circular RNAs and it provides an essential foundation and resource for investigations into the functions and roles of this new class of EBV transcripts in EBV biology and diseases. [ABSTRACT FROM AUTHOR]

Published

2018

35. The miR-15/107 group of microRNA genes: evolutionary biology, cellular functions, and roles in human diseases

Author

Bernard R. Wilfred, John R. Finnerty, Guogen Mao, Peter T. Nelson, Wang-Xia Wang, and Sébastien S. Hébert

Subjects

Heart Diseases, Neovascularization, Physiologic, Biology, Article, Evolution, Molecular, Structural Biology, Phylogenetics, Neoplasms, microRNA, Gene expression, medicine, Gene silencing, Animals, Humans, Molecular Biology, Gene, Cell Proliferation, Oligonucleotide Array Sequence Analysis, Genetics, Regulation of gene expression, Cerebral Cortex, Neovascularization, Pathologic, Neurodegeneration, Neurodegenerative Diseases, medicine.disease, MicroRNAs, Gene Expression Regulation, DNA microarray

Abstract

The miR-15/107 group of microRNA (miRNA) gene is increasingly appreciated to serve key functions in humans. These miRNAs regulate gene expression involved in cell division, metabolism, stress response, and angiogenesis in vertebrate species. The miR-15/107 group has also been implicated in human cancers, cardiovascular disease and neurodegenerative disease, including Alzheimer's disease. Here we provide an overview of the following: (1) the evolution of miR-15/107 group member genes; (2) the expression levels of miRNAs in mammalian tissues; (3) evidence for overlapping gene-regulatory functions by different miRNAs; (4) the normal biochemical pathways regulated by miR-15/107 group miRNAs; and (5) the roles played by these miRNAs in human diseases. Membership in this group is defined based on sequence similarity near the mature miRNAs' 5′ end: all include the sequence AGCAGC. Phylogeny of this group of miRNAs is incomplete; thus, a definitive taxonomic classification (e.g., designation as a “superfamily”) is currently not possible. While all vertebrates studied to date express miR-15a, miR-15b, miR-16, miR-103, and miR-107, mammals alone are known to express miR-195, miR-424, miR-497, miR-503, and miR-646. Multiple different miRNAs in the miR-15/107 group are expressed at moderate to high levels in human tissues. We present data on the expression of all known miR-15/107 group members in human cerebral cortical gray matter and white matter using new miRNA profiling microarrays. There is extensive overlap in the mRNAs targeted by miR-15/107 group members. We show new data from cultured H4 cancer cells that demonstrate similarities in mRNAs targeted by miR-16 and miR-103 and also support the importance of the mature miRNAs' 5′ seed region in mRNA target recognition. In conclusion, the miR-15/107 group of miRNA genes is a fascinating topic of study for evolutionary biologists, miRNA biochemists, and clinically oriented translational researchers alike.

Published

2010

36. Anti-Argonaute RIP-Chip shows that miRNA transfections alter global patterns of mRNA recruitment to microribonucleoprotein complexes

Author

Bernard R. Wilfred, Arnold J. Stromberg, Peter T. Nelson, Yanling Hu, and Wang-Xia Wang

Subjects

Macromolecular Substances, Eukaryotic Initiation Factor-2, Biology, Transfection, Article, Mice, Cell Line, Tumor, microRNA, Gene expression, Gene silencing, Animals, Humans, Immunoprecipitation, RNA, Messenger, Molecular Biology, Ribonucleoprotein, Oligonucleotide Array Sequence Analysis, Regulation of gene expression, Microarray analysis techniques, Antibodies, Monoclonal, Argonaute, Molecular biology, Cell biology, MicroRNAs, Ribonucleoproteins, Argonaute Proteins, RIP-Chip

Abstract

MicroRNAs (miRNAs) play key roles in gene expression regulation by guiding Argonaute (AGO)-containing microribonucleoprotein (miRNP) effector complexes to target polynucleotides. There are still uncertainties about how miRNAs interact with mRNAs. Here we employed a biochemical approach to isolate AGO-containing miRNPs from human H4 tumor cells by co-immunoprecipitation (co-IP) with a previously described anti-AGO antibody. Co-immunoprecipitated (co-IPed) RNAs were subjected to downstream Affymetrix Human Gene 1.0 ST microarray analysis. During rigorous validation, the “RIP-Chip” assay identified target mRNAs specifically associated with AGO complexes. RIP-Chip was performed after transfecting brain-enriched miRNAs (miR-107, miR-124, miR-128, and miR-320) and nonphysiologic control miRNA to identify miRNA targets. As expected, the miRNA transfections altered the mRNA content of the miRNPs. Specific mRNA species recruited to miRNPs after miRNA transfections were moderately in agreement with computational target predictions. In addition to recruiting mRNA targets into miRNPs, miR-107 and to a lesser extent miR-128, but not miR-124 or miR-320, caused apparent exclusion of some mRNAs that are normally associated with miRNPs. MiR-107 and miR-128 transfections also result in decreased AGO mRNA and protein levels. However, AGO mRNAs were not recruited to miRNPs after either miR-107 or miR-128 transfection, confirming that miRNAs may alter gene expression without stable association between particular mRNAs and miRNPs. In summary, RIP-Chip assays constitute an optimized, validated, direct, and high-throughput biochemical assay that provides data about specific miRNA:mRNA interactions, as well as global patterns of regulation by miRNAs.

Published

2010

37. Effect of Mono-2-ethyhexyl Phthalate on DNA Methylation in Human Prostate Cancer LNCaP Cells.

Author

WU, Jian Hui, CHEN, Jiao, WANG, Yong, XIA, Bin, WANG, Rong, ZHAO, Yan, WANG, Xia Qin, SONG, Qi, YAO, Shun Heng, ZHANG, Yun Hui, and SUN, Zu Yue

Subjects

DNA methylation, PROSTATE cancer, METHYLCYTOSINE, ENZYME-linked immunosorbent assay, GENE expression

Abstract

Objective To evaluate whether mono (2-ethylhexyl) phthalate (MEHP) affects genomic DNA methylation and the methylation status of some specific genes such as patched gene ( PTCH ) and smoothened gene ( SMO ) in LNCaP cells. Methods LNCaP cells were treated with MEHP (0, 1, 5, 10, and 25 μmol/L) for 3 days. An ELISA assay was preformed to detect genomic methylation, including 5-methylcytosine (5-mC) and 5-hydroxymethylcytosine (5-hmC) content. A pyrosequencing assay was applied to assess DNA methylation in PTCH and SMO gene promoters. The correlation between DNA methylation and gene expression was assessed. Results The proportion of cytosines with 5-mC methylation in LNCaP cells was significantly decreased by MEHP (1, 5, 10, and 25 μmol/L) in a dose-dependent manner ( P < 0.01). For genes in the Hedgehog pathway, there was no significant MEHP concentration-dependent difference in the DNA methylation of PTCH and SMO . Conclusion MEHP might affect the progression of prostate cancer through its effect on global DNA methylation. [ABSTRACT FROM AUTHOR]

Published

2017

38. Identification of novel genetic loci for osteoporosis and/or rheumatoid arthritis using cFDR approach.

Author

Zhou, Rou, Lin, Xu, Li, Ding-You, Wang, Xia-Fang, Greenbaum, Jonathan, Chen, Yuan-Cheng, Zeng, Chun-Ping, Lu, Jun-Min, Ao, Zeng-Xing, Peng, Lin-Ping, Bai, Xiao Chun, Shen, Jie, and Deng, Hong-Wen

Subjects

OSTEOPOROSIS, JOINT pain, BONE diseases, FEMALE athlete triad (Syndrome), VITAMIN D deficiency

Abstract

There are co-morbidity between osteoporosis (OP) and rheumatoid arthritis (RA). Some genetic risk factors have been identified for these two phenotypes respectively in previous research; however, they accounted for only a small portion of the underlying total genetic variances. Here, we sought to identify additional common genetic loci associated with OP and/or RA. The conditional false discovery rate (cFDR) approach allows detection of additional genetic factors (those respective ones as well as common pleiotropic ones) for the two associated phenotypes. We collected and analyzed summary statistics provided by large, multi-center GWAS studies of FNK (femoral neck) BMD (a major risk factor for osteoporosis) (n = 53,236) and RA (n = 80,799). The conditional quantile-quantile (Q-Q) plots can assess the enrichment of SNPs related to FNK BMD and RA, respectively. Furthermore, we identified shared loci between FNK BMD and RA using conjunction cFDR (ccFDR). We found strong enrichment of p-values in FNK BMD when conditional Q-Q was done on RA and vice versa. We identified 30 novel OP-RA associated pleiotropic loci that have not been reported in previous OP or RA GWAS, 18 of which located in the MHC (major histocompatibility complex) region previously reported to play an important role in immune system and bone health. We identified some specific novel polygenic factors for OP and RA respectively, and identified 30 novel OP-RA associated pleiotropic loci. These discovery findings may offer novel pathobiological insights, and suggest new targets and pathways for drug development in OP and RA patients. [ABSTRACT FROM AUTHOR]

Published

2017

39. Characterization of TRAF genes and their responses to Vibrio anguillarum challenge in Argopecten scallops.

Author

Wang, Xia, Qu, Xiaoxu, Lu, Xia, Chen, Min, Ning, Junhao, Liu, Haijun, Liu, Guilong, Xu, Xin, Zhang, Xiaotong, Yu, Kai, Xu, He, Liu, Bo, and Wang, Chunde

Subjects

*VIBRIO anguillarum, *SCALLOPS, *BAY scallop, *TUMOR necrosis factors, *GENE expression

Abstract

The tumor necrosis factor receptor-related factor (TRAF) family has been reported to be involved in many immune pathways, such as TNFR, TLR, NLR, and RLR in animals. However, little is known about the roles of TRAF genes in the innate immune of Argopecten scallops. In this study, we first identified five TRAF genes, including TRAF 2 , TRAF 3 , TRAF 4 , TRAF 6 and TRAF 7 , but not TRAF 1 and TRAF 5 , from both the bay scallop A. irradians (Air) and the Peruvian scallop A. purpuratus (Apu). The phylogenetic analysis showed that the TRAF genes in Argopecten scallops (AiTRAF) belong to the branch of molluscan TRAF family, which lacks TRAF 1 and TRAF 5. Since TRAF 6 is a key bridge factor in the tumor necrosis factor superfamily and plays an important role in innate and adaptive immunity, we cloned the ORFs of the TRAF 6 gene in both A. irradians and A. purpuratus , as well as in two reciprocal hybrids (Aip for the hybrid Air × Apu and Api for the hybrid Apu × Air). Differences in conformational and post-translational modification resulted from the variation in amino acid sequences may cause differences in activity among them. Analysis of conserved motifs and protein structural domains revealed that AiTRAF contains typical structural domains similar to those of other mollusks and has the same conserved motifs. Tissue expression of TRAF in Argopecten scallops challenged by Vibrio anguillarum was examined by qRT-PCR. The results showed that AiTRAF were higher in gill and hepatopancreas. When challenged by Vibrio anguillarum , the expression of AiTRAF was significantly increased compared with the control group, indicating that AiTRAF may play an important role in the immunity of scallops. In addition, the expression of TRAF was higher in Api and Aip than in Air when challenged by Vibrio anguillarum , suggesting that TRAF may have contributed to the high resistance of Api and Aip to Vibrio anguillarum. The results of this study may provide new insights into the evolution and function of TRAF genes in bivalves and ultimately benefit scallop breeding. • Hybrids between two Argopecten scallops exhibited higher resistance to Vibrio. • Differences in sequence and structures between the TRAF genes of the hybrids and purebred cohorts may result in the difference in activity between them. • Elevated mRNA expression of TRAF gene in the hybrids in response to Vibrio challenge may contribute to the higher resistance of hybrids to Vibrio. [ABSTRACT FROM AUTHOR]

Published

2023

40. Cystatin C Shifts APP Processing from Amyloid-β Production towards Non-Amyloidgenic Pathway in Brain Endothelial Cells.

Author

Wang, Xia-Fei, Liu, Dong-Xin, Liang, Yue, Xing, Li-Li, Zhao, Wen-Hui, Qin, Xiao-Xue, Shang, De-Shu, Li, Bo, Fang, Wen-Gang, Cao, Liu, Zhao, Wei-Dong, and Chen, Yu-Hua

Subjects

*CYSTATINS, *AMYLOID, *BRAIN physiology, *ENDOTHELIAL cells, *ALZHEIMER'S disease, *NEURITIS, *PROTEOLYTIC enzymes

Abstract

Amyloid-β (Aβ), the major component of neuritic plaques in Alzheimer’s disease (AD), is derived from sequential proteolytic cleavage of amyloid protein precursor (APP) by secretases. In this study, we found that cystatin C (CysC), a natural cysteine protease inhibitor, is able to reduce Aβ40 secretion in human brain microvascular endothelial cells (HBMEC). The CysC-induced Aβ40 reduction was caused by degradation of β-secretase BACE1 through the ubiquitin/proteasome pathway. In contrast, we found that CysC promoted secretion of soluble APPα indicating the activated non-amyloidogenic processing of APP in HBMEC. Further results revealed that α-secretase ADAM10, which was transcriptionally upregulated in response to CysC, was required for the CysC-induced sAPPα secretion. Knockdown of SIRT1 abolished CysC-triggered ADAM10 upregulation and sAPPα production. Taken together, our results demonstrated that exogenously applied CysC can direct amyloidogenic APP processing to non-amyloidgenic pathway in brain endothelial cells, mediated by proteasomal degradation of BACE1 and SIRT1-mediated ADAM10 upregulation. Our study unveils previously unrecognized protective role of CysC in APP processing. [ABSTRACT FROM AUTHOR]

Published

2016

41. Methylation status and AP1 elements are involved in EBV-mediated miR-155 expression in EBV positive lymphoma cells.

Author

Yin, Qinyan, Wang, Xia, Roberts, Claire, Flemington, Erik K., and Lasky, Joseph A.

Subjects

*MICRORNA, *GENE expression, *EPSTEIN-Barr virus, *DNA methylation, *TRANSCRIPTION factors, *CELL communication

Abstract

The relationship between Epstein Barr Virus (EBV) and miR-155 is well established. EBV infection induces miR-155 expression, which is expressed at higher levels in EBV latency type III cells compared to EBV latency type I cells. However, the mechanism by which EBV latency genes activate miR-155 expression is still unclear. Here we present data showing that DNA methylation regulates miR-155 expression. We also provide evidence that the AP1 signaling pathway is involved in EBV-mediated miR-155 activation, and that Bay11 influences signaling of the miR-155 promoter AP1 element. Lastly, we show that LMP2A, LMP1 and EBNAs cannot activate miR-155 expression alone, indicating that the regulation of miR-155 by EBV is dependent on more than one EBV gene or cell signaling pathway. We conclude that the regulation of miR-155 in EBV-positive cells occurs through multiple cell signaling processes involving EBV-mediated chromatin remodeling, cell signaling regulation and transcription factor activation. [ABSTRACT FROM AUTHOR]

Published

2016

42. Novel human ABCC9/SUR2 brain-expressed transcripts and an eQTL relevant to hippocampal sclerosis of aging.

Author

Nelson, Peter T., Wang, Wang‐Xia, Wilfred, Bernard R., Wei, Angela, Dimayuga, James, Huang, Qingwei, Ighodaro, Eseosa, Artiushin, Sergey, and Fardo, David W.

Subjects

*DIAGNOSIS of neurological disorders, *GENE expression, *AGING, *BRAIN, *NEUROLOGICAL disorders -- Genetic aspects, *SINGLE nucleotide polymorphisms

Abstract

ABCC9 genetic polymorphisms are associated with increased risk for various human diseases including hippocampal sclerosis of aging. The main goals of this study were 1 > to detect the ABCC9 variants and define the specific 3′ untranslated region (3′ UTR) for each variant in human brain, and 2 > to determine whether a polymorphism (rs704180) associated with risk for hippocampal sclerosis of aging pathology is also associated with variation in ABCC9 transcript expression and/or splicing. Rapid amplification of ABCC9 cDNA ends (3′ RACE) provided evidence of novel 3′ UTR portions of ABCC9 in human brain. In silico and experimental studies were performed focusing on the single nucleotide polymorphism, rs704180. Analyses from multiple databases, focusing on rs704180 only, indicated that this risk allele is a local expression quantitative trait locus ( eQTL). Analyses of RNA from human brains showed increased ABCC9 transcript levels in individuals with the risk genotype, corresponding with enrichment for a shorter 3′ UTR which may be more stable than variants with the longer 3′ UTR. Micro RNA transfection experiments yielded results compatible with the hypothesis that miR-30c causes down-regulation of SUR2 transcripts with the longer 3′ UTR. Thus we report evidence of complex ABCC9 genetic regulation in brain, which may be of direct relevance to human disease. [ABSTRACT FROM AUTHOR]

Published

2015

43. De novo Transcriptome Assembly and the Putative Biosynthetic Pathway of Steroidal Sapogenins of Dioscorea composita.

Author

Wang, Xia, Chen, Dijia, Wang, Yuqi, and Xie, Jun

Subjects

*BIOSYNTHESIS, *SAPOGENINS, *YAMS, *ETHANOL as fuel, *POLYMERASE chain reaction, *GENE expression

Abstract

The plant Dioscorea composita has important applications in the medical and energy industries, and can be used for the extraction of steroidal sapogenins (important raw materials for the synthesis of steroidal drugs) and bioethanol production. However, little is known at the genetic level about how sapogenins are biosynthesized in this plant. Using Illumina deep sequencing, 62,341 unigenes were obtained by assembling its transcriptome, and 27,720 unigenes were annotated. Of these, 8,022 unigenes were mapped to 243 specific pathways, and 531 unigenes were identified to be involved in 24 secondary metabolic pathways. 35 enzymes, which were encoded by 79 unigenes, were related to the biosynthesis of steroidal sapogenins in this transcriptome database, covering almost all the nodes in the steroidal pathway. The results of real-time PCR experiments on ten related transcripts (HMGR, MK, SQLE, FPPS, DXS, CAS, HMED, CYP51, DHCR7, and DHCR24) indicated that sapogenins were mainly biosynthesized by the mevalonate pathway. The expression of these ten transcripts in the tuber and leaves was found to be much higher than in the stem. Also, expression in the shoots was low. The nucleotide and protein sequences and conserved domains of four related genes (HMGR, CAS, SQS, and SMT1) were highly conserved between D. composita and D. zingiberensis; but expression of these four genes is greater in D. composita. However, there is no expression of these key enzymes in potato and no steroidal sapogenins are synthesized. [ABSTRACT FROM AUTHOR]

Published

2015

44. Gene Expression Profile in the Early Stage of Angiotensin II-induced Cardiac Remodeling: a Time Series Microarray Study in a Mouse Model.

Author

Dang, Meng-Qiu, Zhao, Xue-Chen, Lai, Song, Wang, Xia, Wang, Lei, Zhang, Yun-Long, Liu, Yang, Yu, Xiao-Hong, Liu, Ying, Li, Hui-Hua, and Xia, Yun-Long

Subjects

GENE expression, ANGIOTENSIN II, VENTRICULAR remodeling, MICROARRAY technology, BLOOD pressure, ECHOCARDIOGRAPHY, LABORATORY mice

Abstract

Background/Aims: Angiotensin II (Ang II) plays a critical role in the cardiac remodeling contributing to heart failure. However, the gene expression profiles induced by Ang II in the early stage of cardiac remodeling remain unknown. Methods: Wild-type male mice (C57BL/6 background, 10-weeek-old) were infused with Ang II (1500 ng/kg/min) for 7 days. Blood pressure was measured. Cardiac function and remodeling were examined by echocardiography, H&E and Masson staining. The time series microarrays were then conducted to detected gene expression profiles. Results: Microarray results identified that 1,489 genes were differentially expressed in the hearts at day 1, 3 and 7 of Ang II injection. These genes were further classified into 26 profiles by hierarchical cluster analysis. Of them, 4 profiles were significant (No. 19, 8, 21 and 22) and contained 904 genes. Gene Ontology showed that these genes mainly participate in metabolic process, oxidation-reduction process, extracellular matrix organization, apoptotic process, immune response, and others. Significant pathways included focal adhesion, ECM-receptor interaction, cytokine-cytokine receptor interaction, MAPK and insulin signaling pathways, which were known to play important roles in Ang II-induced cardiac remodeling. Moreover, gene co-expression networks analysis suggested that serine/cysteine peptidase inhibitor, member 1 (Serpine1, also known as PAI-1) localized in the core of the network. Conclusions: Our results indicate that many genes are mainly involved in metabolism, inflammation, cardiac fibrosis and hypertrophy. Serpine1 may play a central role in the development of Ang II-induced cardiac remodeling at the early stage. © 2015 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2015

45. RIP1 potentiates BPDE-induced transformation in human bronchial epithelial cells through catalase-mediated suppression of excessive reactive oxygen species.

Author

Wang, Qiong, Chen, Wenshu, Xu, Xiuling, Li, Bilan, He, Weiyang, Padilla, Mabel T., Jang, Jun-Ho, Nyunoya, Toru, Amin, Shantu, Wang, Xia, and Lin, Yong

Subjects

OXYGEN in the body, EPITHELIAL cells, BRONCHI, CATALASE, CIGARETTE smoke, GENE expression, CELL-mediated cytotoxicity

Abstract

Cell survival signaling is important for the malignant phenotypes of cancer cells. Although the role of receptor-interacting protein 1 (RIP1) in cell survival signaling is well documented, whether RIP1 is directly involved in cancer development has never been studied. In this report, we found that RIP1 expression is substantially increased in human non-small cell lung cancer and mouse lung tumor tissues. RIP1 expression was remarkably increased in cigarette smoke-exposed mouse lung. In human bronchial epithelial cells (HBECs), RIP1 was significantly induced by cigarette smoke extract or benzo[a]pyrene diol epoxide (BPDE), the active form of the tobacco-specific carcinogen benzo(a)pyrene. In RIP1 knockdown HBECs, BPDE-induced cytotoxicity was significantly increased, which was associated with induction of cellular reactive oxygen species (ROS) and activation of mitogen-activated protein kinases (MAPKs), including c-jun N-terminal kinase (JNK), extracellular signal-regulated kinase (ERK) and p38. Scavenging ROS suppressed BPDE-induced MAPK activation and inhibiting ROS or MAPKs substantially blocked BPDE-induced cytotoxicity, suggesting ROS-mediated MAPK activation is involved in BPDE-induced cell death. The ROS-reducing enzyme catalase is destabilized in an ERK- and JNK-dependent manner in RIP1 knockdown HBECs and application of catalase effectively blocked BPDE-induced ROS accumulation and cytotoxicity. Importantly, BPDE-induced transformation of HBECs was significantly reduced when RIP1 expression was suppressed. Altogether, these results strongly suggest an oncogenic role for RIP1, which promotes malignant transformation through protecting DNA-damaged cells against carcinogen-induced cytotoxicity associated with excessive ROS production. [ABSTRACT FROM PUBLISHER]

Published

2013

46. Using Synthetic Biology to Distinguish and Overcome Regulatory and Functional Barriers Related to Nitrogen Fixation.

Author

Wang, Xia, Yang, Jian-Guo, Chen, Li, Wang, Ji-Long, Cheng, Qi, Dixon, Ray, and Wang, Yi-Ping

Subjects

*SYNTHETIC biology, *NITROGEN fixation, *KLEBSIELLA pneumoniae, *MICROCLUSTERS, *ESCHERICHIA coli, *GENE expression, *PROMOTERS (Genetics)

Abstract

Biological nitrogen fixation is a complex process requiring multiple genes working in concert. To date, the Klebsiella pneumoniae nif gene cluster, divided into seven operons, is one of the most studied systems. Its nitrogen fixation capacity is subject to complex cascade regulation and physiological limitations. In this report, the entire K. pneumoniae nif gene cluster was reassembled as operon-based BioBrick parts in Escherichia coli. It provided ∼100% activity of native K. pneumoniae system. Based on the expression levels of these BioBrick parts, a T7 RNA polymerase–LacI expression system was used to replace the σ54-dependent promoters located upstream of nif operons. Expression patterns of nif operons were critical for the maximum activity of the recombinant system. By mimicking these expression levels with variable-strength T7-dependent promoters, ∼42% of the nitrogenase activity of the σ54-dependent nif system was achieved in E. coli. When the newly constructed T7-dependent nif system was challenged with different genetic and physiological conditions, it bypassed the original complex regulatory circuits, with minor physiological limitations. Therefore, we have successfully replaced the nif regulatory elements with a simple expression system that may provide the first step for further research of introducing nif genes into eukaryotic organelles, which has considerable potentials in agro-biotechnology. [ABSTRACT FROM AUTHOR]

Published

2013

47. Involvement of large conductance Ca-activated K channel in laminar shear stress-induced inhibition of vascular smooth muscle cell proliferation.

Author

Jia, Xiaoling, Yang, Jingyun, Song, Wei, Li, Ping, Wang, Xia, Guan, Changdong, Yang, Liu, Huang, Yan, Gong, Xianghui, Liu, Meili, Zheng, Lisha, and Fan, Yubo

Subjects

CALCIUM-dependent potassium channels, SHEARING force, VASCULAR smooth muscle, CELL proliferation, VASCULAR diseases, CELL nuclei, DNA synthesis, GENE expression

Abstract

The large conductance Ca-activated K (BK) channel in vascular smooth muscle cell (VSMC) is an important potassium channel that can regulate vascular tone. Recent work has demonstrated that abnormalities in BK channel function are associated with changes in cell proliferation and the onset of vascular disease. However, until today there are rare reports to show whether this channel is involved in VSMC proliferation in response to fluid shear stress (SS). Here we investigated a possible role of BK channel in VSMC proliferation under laminar SS. Rat aortic VSMCs were plated in parallel-plate flow chambers and exposed to laminar SS with varied durations and magnitudes. VSMC proliferation was assessed by measuring proliferating cell nuclear antigen (PCNA) expression and DNA synthesis. BK protein and gene expression was determined by flow cytometery and RT-PCR. The involvement of BK in SS-induced inhibition of proliferation was examined by BK inhibition using a BK specific blocker, iberiotoxin (IBTX), and by BK transfection in BK non-expressing CHO cells. The changes in [Ca] were determined using a calcium-sensitive dye, fluo 3-AM. Membrane potential changes were detected with a potential-sensitive dye, DiBAC(3). We found that laminar SS inhibited VSMC proliferation and stimulated BK channel expression. Furthermore, laminar SS induced an increase in [Ca] and membrane hyperpolarization. Besides in VSMC, the inhibitory effect of BK channel activity on cell proliferation in response to SS was also confirmed in BK-transfected CHO cells showing a decline in proliferation. Blocking BK channel reversed its inhibitory effect, providing additional support for the involvement of BK in SS-induced proliferation reduction. Our results suggest, for the first time, that BK channel mediates laminar SS-induced inhibition of VSMC proliferation. This finding is important for understanding the mechanism by which SS regulates VSMC proliferation, and should be helpful in developing strategies to prevent flow-initiated vascular disease formation. [ABSTRACT FROM AUTHOR]

Published

2013

48. Crocetin induces cytotoxicity and enhances vincristine-induced cancer cell death via p53-dependent and -independent mechanisms.

Author

Zhong, Ying-jia, Shi, Fang, Zheng, Xue-lian, Wang, Qiong, Yang, Lan, Sun, Hong, He, Fan, Zhang, Lin, Lin, Yong, Qin, Yong, Liao, Lin-chuan, and Wang, Xia

Subjects

CELL-mediated cytotoxicity, VINCRISTINE, CELL death, SMALL cell lung cancer, CANCER cell proliferation, FLOW cytometry, GENE expression, CANCER chemotherapy

Abstract

Aim:To investigate the anticancer effect of crocetin, a major ingredient in saffron, and its underlying mechanisms.Methods:Cervical cancer cell line HeLa, non-small cell lung cancer cell line A549 and ovarian cancer cell line SKOV3 were treated with crocetin alone or in combination with vincristine. Cell proliferation was examined using MTT assay. Cell cycle distribution and sub-G1 fraction were analyzed using flow cytometric analysis after propidium iodide staining. Apoptosis was detected using the Annexin V-FITC Apoptosis Detection Kit with flow cytometry. Cell death was measured based on the release of lactate dehydrogenase (LDH). The expression levels of p53 and p21WAF1/Cip1 as well as caspase activation were examined using Western blot analysis.Results:Treatment of the 3 types of cancer cells with crocetin (60-240 μmol/L) for 48 h significantly inhibited their proliferation in a concentration-dependent manner. Crocetin (240 μmol/L) significantly induced cell cycle arrest through p53-dependent and -independent mechanisms accompanied with p21WAF1/Cip1 induction. Crocetin (120-240 μmol/L) caused cytotoxicity in the 3 types of cancer cells by enhancing apoptosis in a time-dependent manner. In the 3 types of cancer cells, crocetin (60 μmol/L) significantly enhanced the cytotoxicity induced by vincristine (1 μmol/L). Furthermore, this synergistic effect was also detected in the vincristine-resistant breast cancer cell line MCF-7/VCR.Conclusion:Ccrocetin is a potential anticancer agent, which may be used as a chemotherapeutic drug or as a chemosensitizer for vincristine. [ABSTRACT FROM AUTHOR]

Published

2011

49. Gender Difference in Proteome of Brown Adipose Tissues between Male and Female Rats Exposed to a High Fat Diet.

Author

Choi, Duk Kwon, Oh, Tae Seok, Choi, Jung-Won, Mukherjee, Rajib, Wang, Xia, Liu, Hao, and Yun, Jong Won

Subjects

SEX differences (Biology), BROWN adipose tissue, HIGH-fat diet, BODY temperature regulation, OXIDATION, GENE expression, PROTEIN synthesis, LABORATORY rats

Abstract

Background: Although the importance of gender as a key determinant in health and illness has been recognized for a long time, systematic studies of gender differences in medicine are still lacking. We hypothesized that interscapular brown adipocyte tissue (BAT), is not only a key tissue contributing to energy expenditure, but also regulates diet-induced thermogenesis, and may be an ideal target for studying gender differences in obesity development in response to a high fat diet (HFD). Methods: We therefore performed differential proteome analysis of BAT from lean and obese rats of both genders fed a HFD using 2-DE combined with MALDI-TOF-MS. Results: When exposed to a HFD, male rats gained more body weight with increased values of plasma biochemical parameters than did female rats. Among 595 matched spots, 48 differentially expressed identified spots showed significant gender differences, whereas 7 proteins showed no gender differences, but did show a HFD response. Conclusions: Proteomic investigations into gender-dimorphic protein modulation in BAT may provide conclusive results showing higher expression of numerous proteins involved in thermogenesis and fat oxidation as well as lower expression of proteins contributing to fat synthesis in female rats than in male rats. Copyright © 2011 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2011

50. Residual Embryonic Cells as Precursors of a Barrett's-like Metaplasia

Author

Wang, Xia, Ouyang, Hong, Yamamoto, Yusuke, Kumar, Pooja Ashok, Wei, Tay Seok, Dagher, Rania, Vincent, Matthew, Lu, Xin, Bellizzi, Andrew M., Ho, Khek Yu, Crum, Christopher P., Xian, Wa, and McKeon, Frank

Subjects

*BARRETT'S esophagus, *EMBRYOLOGY, *METAPLASIA, *LABORATORY mice, *GASTROESOPHAGEAL reflux, *GENE expression, *CELL lines, *EPITHELIUM

Abstract

Summary: Barrett''s esophagus is an intestine-like metaplasia and precursor of esophageal adenocarcinoma. Triggered by gastroesophageal reflux disease, the origin of this metaplasia remains unknown. p63-deficient mice, which lack squamous epithelia, may model acid-reflux damage. We show here that p63 null embryos rapidly develop intestine-like metaplasia with gene expression profiles similar to Barrett''s metaplasia. We track its source to a unique embryonic epithelium that is normally undermined and replaced by p63-expressing cells. Significantly, we show that a discrete population of these embryonic cells persists in adult mice and humans at the squamocolumnar junction, the source of Barrett''s metaplasia. We show that upon programmed damage to the squamous epithelium, these embryonic cells migrate toward adjacent, specialized squamous cells in a process that may recapitulate early Barrett''s. Our findings suggest that certain precancerous lesions, such as Barrett''s, initiate not from genetic alterations but from competitive interactions between cell lineages driven by opportunity. PaperClip: Display Omitted [Copyright &y& Elsevier]

Published

2011