Your search keyword '"mouse"' showing total 73,923 results

51. A systematic assessment of robustness in CNS safety pharmacology.

Author

Reiber, Maria, Stirling, Helen, Ahuis, Tim P., Arias, Washington, Aulehner, Katharina, Dreßler, Ute, Kas, Martien J. H., Kela, Johanna, Kerker, Kimberly, Kuosmanen, Tarja, Lorenz, Helga, Pennington, Alexander T., Rüden, Eva‐Lotta, Schauerte, Heike, Seiffert, Isabel, Talbot, Steven R., Torturo, Christina, Virtanen, Sami, Waldron, Ann‐Marie, and Ramboz, Sylvie

Subjects

*DRUG side effects, *INTRAPERITONEAL injections, *DRUG development, *REPRODUCIBLE research, *DECISION making

Abstract

Background and Purpose Experimental Approach Key Results Conclusion and Implications Irwin tests are key preclinical study elements for characterising drug‐induced neurological side effects. This multicentre study aimed to assess the robustness of Irwin tests across multinational sites during three stages of protocol harmonisation. The projects were part of the Enhanced Quality in Preclinical Data framework, aiming to increase success rates in transition from preclinical testing to clinical application.Female and male NMRI mice were assigned to one of three groups (vehicle, MK‐801 0.1 and 0.3 mg kg−1). Irwin scores were assessed at baseline and multiple times following intraperitoneal injection of MK‐801 using local protocols (Stage 1), shared protocols with harmonised environmental design (Stage 2) and fully harmonised Irwin scoring protocols (Stage 3).The analysis based on the four functional domains (motor, autonomic, sedation and excitation) revealed substantial data variability in Stages 1 and 2. Although there was still marked overall heterogeneity between sites in Stage 3 after complete harmonisation of the Irwin scoring scheme, heterogeneity was only moderate within functional domains. When comparing treatment groups versus vehicle, we found large effect sizes in the motor domain and subtle to moderate effects in the excitation‐related and autonomic domains.The pronounced interlaboratory variability in Irwin datasets for the CNS‐active compound MK‐801 needs to be carefully considered when making decisions during drug development. While environmental and general study design had a minor impact, the study suggests that harmonisation of parameters and their scoring can limit variability and increase robustness. [ABSTRACT FROM AUTHOR]

Published

2024

52. Silencing of maternally expressed RNAs in Dlk1-Dio3 domain causes fatal vascular injury in the fetal liver.

Author

Yu, Haoran, Zhao, Yue, Cheng, Rui, Wang, Mengyun, Hu, Xin, Zhang, Ximeijia, Teng, Xiangqi, He, Hongjuan, Han, Zhengbin, Han, Xiao, Wang, Ziwen, Liu, Bingjing, Zhang, Yan, and Wu, Qiong

Subjects

*GENE expression, *LINCRNA, *PHENOTYPES, *GENETIC transcription, *GENOMES

Abstract

The mammalian imprinted Dlk1-Dio3 domain contains multiple lncRNAs, mRNAs, the largest miRNA cluster in the genome and four differentially methylated regions (DMRs), and deletion of maternally expressed RNA within this locus results in embryonic lethality, but the mechanism by which this occurs is not clear. Here, we optimized the model of maternally expressed RNAs transcription termination in the domain and found that the cause of embryonic death was apoptosis in the embryo, particularly in the liver. We generated a mouse model of maternally expressed RNAs silencing in the Dlk1-Dio3 domain by inserting a 3 × polyA termination sequence into the Gtl2 locus. By analyzing RNA-seq data of mouse embryos combined with histological analysis, we found that silencing of maternally expressed RNAs in the domain activated apoptosis, causing vascular rupture of the fetal liver, resulting in hemorrhage and injury. Mechanistically, termination of Gtl2 transcription results in the silencing of maternally expressed RNAs and activation of paternally expressed genes in the interval, and it is the gene itself rather than the IG-DMR and Gtl2-DMR that causes the aforementioned phenotypes. In conclusion, these findings illuminate a novel mechanism by which the silencing of maternally expressed RNAs within Dlk1-Dio3 domain leads to hepatic hemorrhage and embryonic death through the activation of apoptosis. [ABSTRACT FROM AUTHOR]

Published

2024

53. Visual experience reduces the spatial redundancy between cortical feedback inputs and primary visual cortex neurons.

Author

Dias, Rodrigo F., Rajan, Radhika, Baeta, Margarida, Belbut, Beatriz, Marques, Tiago, and Petreanu, Leopoldo

Subjects

*NEURONS, *MICE, *VISUAL cortex

Abstract

The role of experience in the organization of cortical feedback (FB) remains unknown. We measured the effects of manipulating visual experience on the retinotopic specificity of supragranular and infragranular projections from the lateromedial (LM) visual area to layer (L)1 of the mouse primary visual cortex (V1). LM inputs were, on average, retinotopically matched with V1 neurons in normally and dark-reared mice, but visual exposure reduced the fraction of spatially overlapping inputs to V1. FB inputs from L5 conveyed more surround information to V1 than those from L2/3. The organization of LM inputs from L5 depended on their orientation preference and was disrupted by dark rearing. These observations were recapitulated by a model where visual experience minimizes receptive field overlap between LM inputs and V1 neurons. Our results provide a mechanism for the dependency of surround modulations on visual experience and suggest how expected interarea coactivation patterns are learned in cortical circuits. • Visual experience reduces the receptive field overlap between LM inputs and V1 neurons • LM inputs from L5 convey more surround information to V1 neurons than those from L2/3 • The tuning-dependent organization of LM inputs from L5 requires visual experience • Spatial redundancy minimization explains visual experience effects on LM inputs Dias and Rajan et al. compared the functional organization of cortical feedback inputs in the primary visual cortex of normally and dark-reared mice. They found that visual experience reduces the representational redundancy between feedback inputs and primary visual cortex neurons. [ABSTRACT FROM AUTHOR]

Published

2024

54. Single-cell analysis reveals alternations between the aged and young mice prostates.

Author

Li, Yang, Ding, Yuhong, Hou, Yaxin, Liu, Lilong, Liu, Zhenghao, Yao, Zhipeng, Shi, Pengjie, Li, Jinxu, Chen, Ke, and Hu, Junyi

Subjects

CELLULAR aging, GENE expression, URINATION disorders, EPITHELIAL-mesenchymal transition, RNA sequencing

Abstract

Background: Aging of the male prostate is an inevitable process in which the prostate undergoes hyperplasia, and this growth may lead to compression of the urethra, resulting in voiding dysfunction and associated symptoms, and an increased risk of prostate cancer. Despite the significance of prostate aging, the molecular mechanisms involved are still not fully understood. Methods: Prostate split by lobes from young (2 months) and aged (24 months) mice were collected for single-cell RNA sequencing (scRNA-seq) analysis. Tissues from both anterior prostate (AP) and ventral/dorsal/lateral prostate (VDLP) were included in the study. Data analysis included unsupervised clustering using the uniform manifold approximation and projection (UMAP) algorithm to identify distinct cell types based on marker gene expression. Differential gene expression analysis was performed to identify age-related changes in gene expression across different cell types. Functional enrichment analysis was conducted to elucidate biological pathways associated with differentially expressed genes. Additionally, cellular interactions and developmental trajectories were analyzed to characterize cellular dynamics during prostate aging. Results: The single-cell transcriptome analysis of the mouse prostate during aging revealed heterogeneity across various cell types and their changes during the aging process. We found a significant increase in the proportion of mesenchymal and immune cells in aged mice. Our study unveiled alterations in genes and pathways associated with cellular senescence, oxidative stress, and regeneration in epithelial cells. Furthermore, we observed that basal cells may undergo epithelial-mesenchymal transition (EMT) to become mesenchymal cells, particularly prominent in aged mice. Additionally, immune cells, notably macrophages and T cells, exhibited a heightened inflammatory response in aged mice. Conclusion: In summary, our study provides a comparative analysis of the single-cell transcriptome of the aged and young mice prostates, elucidating cellular and molecular changes between the aged and young mice prostates. [ABSTRACT FROM AUTHOR]

Published

2024

55. Gene therapy for epilepsy targeting neuropeptide Y and its Y2 receptor to dentate gyrus granule cells.

Author

Cattaneo, Stefano, Bettegazzi, Barbara, Crippa, Lucia, Asth, Laila, Regoni, Maria, Soukupova, Marie, Zucchini, Silvia, Cantore, Alessio, Codazzi, Franca, Valtorta, Flavia, and Simonato, Michele

Abstract

Gene therapy is emerging as an alternative option for individuals with drug-resistant focal epilepsy. Here, we explore the potential of a novel gene therapy based on Neuropeptide Y (NPY), a well-known endogenous anticonvulsant. We develop a lentiviral vector co-expressing NPY with its inhibitory receptor Y2 in which, for the first time, both transgenes are placed under the control of the minimal CamKIIa(0.4) promoter, biasing expression toward excitatory neurons and allowing autoregulation of neuronal excitability by Y2 receptor-mediated inhibition. Vector-induced NPY and Y2 expression and safety are first assessed in cultures of hippocampal neurons. In vivo experiments demonstrate efficient and nearly selective overexpression of both genes in granule cell mossy fiber terminals following vector administration in the dentate gyrus. Telemetry video-EEG monitoring reveals a reduction in the frequency and duration of seizures in the synapsin triple KO model. This study shows that targeting a small subset of neurons (hippocampal granule cells) with a combined overexpression of NPY and Y2 receptor is sufficient to reduce the occurrence of spontaneous seizures. Synopsis: Co-expressing NPY and its inhibitory receptor Y2 in excitatory hippocampal cells allows inhibitory autoregulation of glutamate release. Expression of both genes in granule cell mossy fiber terminals reduces the frequency and duration of seizures in the synapsin triple KO model of epilepsy. We develop a LV vector with minimal CamKinaseII promoter driving expression of NPY and its receptor Y2. Vector administration in the dentate gyrus allows for efficient and nearly selective in vivo overexpression of NPY and Y2 receptor in granule cell mossy fiber terminals. This reduces the frequency and duration of seizures in the synapsin triple KO model of epilepsy. Co-expressing NPY and its inhibitory receptor Y2 in excitatory hippocampal cells allows inhibitory autoregulation of glutamate release. Expression of both genes in granule cell mossy fiber terminals reduces the frequency and duration of seizures in the synapsin triple KO model of epilepsy. [ABSTRACT FROM AUTHOR]

Published

2024

56. The regenerative effect of exosomes isolated from mouse embryonic fibroblasts in mice created as a sciatic nerve crush injury model.

Author

Bozkurt, Ahmet Sarper, Yılmaz, Şenay Görücü, Kaplan, Davut Sinan, and Bal, Ramazan

Abstract

Background: Exosomes (Exos) are candidates for functional recovery and regeneration following sciatic nerve crushed (SNC) injury due to their composition which can accelerate tissue regeneration. Therefore, mouse embryonic fibroblast-derived exosomes were evaluated for their regenerative capacity in SNC injury. Methods and Results: In the study, 40 Balb/c males (20 ± 5 g) and two pregnant mice (for embryonic fibroblast tissue) were used and crushed injury was induced in the left sciatic nerve with an aneurysm clamp. Sciatic nerve model mice were randomly divided into 5 groups (n = 8; control, n = 8; sham, n = 8; SNC, n = 8; Mouse embryonic fibroblast exosome (mExo), n = 8; SNC + Mouse embryonic fibroblast exosome (SNC + mExo). Rotarod tests for motor functions and hot plate and von Frey tests for sensory functions were analyzed in the groups. Expression changes of exosome genes (RARRES1, NAGS, HOXA13, and MEIS1) immunohistochemical analysis of these gene proteins, and structural exosome NF-200 and S100 proteins were evaluated by confocal microscopy. Behavioral analyses showed that the damage in SNC was significant between groups on day14 and day28 (P < 0.05). In behavioral analyses, it was determined that motor functions and mechanical sensitivity lost in SNC were regained after mExo treatment. While expression of all genes was detected in MEF-derived exosomes, the high expression was MESI1 and the low expression was HOXA13. NF200, an indicator of axon number and neurofilament density, was found to decrease in SNC (P < 0.001) and increase after treatment, but not significantly. The decreased S100 protein levels in SNC and the increase detected after treatment were not significant. Conclusion: The expression of four mRNAs in mExos indicates that these genes may have an effect on regenerative processes after SNC injury. The regenerative process supported by tissue protein expressions demonstrates the therapeutic potential of mExo treatment. [ABSTRACT FROM AUTHOR]

Published

2024

57. The Meiotic Drive: Intragenomic Competition and Selection.

Author

Zakharov, I. A.

Subjects

*MEIOTIC drive, *HOMOLOGOUS chromosomes, *NEUROSPORA, *CENTROMERE, *GENE frequency

Abstract

The article considers the distribution and mechanisms of the meiotic drive as a phenomenon manifested in unequal transmission of gene alleles and/or homologous chromosomes into gametes during meiosis. The meiotic drive has been studied in the most detail in Drosophila, mice, corn, and ascomycete fungi of the genera Neurospora and Podospora. The consequence of the meiotic drive is a shift in the frequencies of alleles in the gene pool and the maintenance of nonadaptive traits in the population. [ABSTRACT FROM AUTHOR]

Published

2024

58. The role of cerebellar FOXP1 in the development of motor and communicative behaviors in mice.

Author

Chasse, R., McLeod, R., Surian, A., Fitch, R. H., and Li, J.

Subjects

*GROSS motor ability, *LANGUAGE acquisition, *AUTISM spectrum disorders, *AUDITORY perception, *SPINAL cord

Abstract

The gene FOXP2 is well established for a role in human speech and language; far less is known about FOXP1. However, this related gene has also been implicated in human language development as well as disorders associated with features of autism spectrum disorder (ASD). FOXP1 protein expression has also recently been identified in the cerebellum—a neural structure previously shown to express FOXP2 protein. The current study sought to elucidate the behavioral implications of a conditional knock‐out of Foxp1 using an En1‐Cre driver, which is active in the entirety of the cerebellum and a subset of neurons in the midbrain and spinal cord, in mice using a test battery including motor tasks associated with cerebellar dysfunction, as well as communicative and autistic‐relevant behaviors. Male and female mice with a conditional knock‐out (cKO, n = 31) and wildtype littermate controls (WT, n = 34) were assessed for gross and orofacial motor control, motor‐coordination learning, locomotion, social behavior, anxiety, auditory processing and expressive vocalizations. Overall results suggest Foxp1 plays a specific role in the development of communicative systems, and phenotypic expression of disruptions may interact with sex. Robust motor deficits associated with Foxp1 protein loss may particularly affect vocalizations based on significant orofacial motor deficits in cKO subjects could also contribute to vocalization anomalies. In summary, the current study provides key insights into the role of Foxp1 in cerebellar function and associated behaviors in mice, with implications for an improved understanding of communicative and motor‐based neurodevelopmental disabilities in humans. [ABSTRACT FROM AUTHOR]

Published

2024

59. Comparison of Chikungunya Virus-Induced Disease Progression and Pathogenesis in Type-I Interferon Receptor-Deficient Mice (A129) and Two Wild-Type (129Sv/Ev and C57BL/6) Mouse Strains.

Author

Graham, Victoria A., Easterbrook, Linda, Rayner, Emma, Findlay-Wilson, Stephen, Flett, Lucy, Kennedy, Emma, Fotheringham, Susan, Kempster, Sarah, Almond, Neil, and Dowall, Stuart

Subjects

*TYPE I interferons, *CHIKUNGUNYA virus, *VACCINE trials, *SYMPTOMS, *DISEASE progression

Abstract

Chikungunya virus (CHIKV) is a mosquito-borne alphavirus causing a debilitating febrile illness with rheumatic disease symptoms of arthralgia and arthritis. Since its spread outside of Africa in 2005, it continues to cause outbreaks and disseminates into new territories. Intervention strategies are urgently required, including vaccination and antiviral approaches. To test efficacy, the use of small animal models is required. Two mouse strains, A129, with a deficiency in their type-I interferon (IFN) receptor, and C57BL/6 are widely used. A direct comparison of these strains alongside the wild-type parental strain of the A129 mice, 129Sv/Ev, was undertaken to assess clinical disease progression, viral loads in key tissues, histological changes and levels of sera biomarkers. Our results confirm the severe disease course in A129 mice which was not observed in the parental 129Sv/Ev strain. Of the two wild-type strains, viral loads were higher in 129Sv/Ev mice compared to C57BL/6 counterparts. Our results have established these models and parameters for the future testing of vaccines and antiviral approaches. [ABSTRACT FROM AUTHOR]

Published

2024

60. Sodium-dependent phosphate transporter PiT1/SLC20A1 as the receptor for the endogenous retroviral envelope syncytin-B involved in mouse placenta formation.

Author

Mousseau, Guillaume, Préault, Noémie, Souquere, Sylvie, Bireau, Caroline, Cassonnet, Patricia, Bacquin, Agathe, Beck, Laurent, Pierron, Gérard, Jacob, Yves, Dupressoir, Anne, and Heidmann, Thierry

Subjects

*EMBRYOLOGY, *CELL fusion, *FETAL tissues, *PREGNANCY proteins, *CELL receptors

Abstract

Syncytins are envelope genes of retroviral origin that play a critical role in the formation of a syncytial structure at the fetomaternal interface via their fusogenic activity. The mouse placenta is unique among placental mammals since the fetomaternal interface comprises two syncytiotrophoblast layers (ST-I and ST-II) instead of one observed in all other hemochorial placentae. Each layer specifically expresses a distinct mouse syncytin, namely syncytin-A (SynA) for ST-I and syncytin-B (SynB) for ST-II, which have been shown to be essential to placentogenesis and embryonic development. The cellular receptor for SynA has been identified as the membrane protein LY6E and is not the receptor for SynB. Here, by combining a cell-cell fusion assay with the screening of a human ORFeome-derived expression library, we identified the transmembrane multipass sodium-dependent phosphate transporter 1 PiT1/SLC20A1 as the receptor for SynB. Transfection of cells with the cloned receptor, but not the closely related PiT2/SLC20A2, leads to their fusion with cells expressing SynB, with no cross-reactive fusion activity with SynA. The interaction between the two partners was further demonstrated by immunoprecipitation. PiT1/PiT2 chimera and truncation experiments identified the PiT1 N-terminus as the major determinant for SynB-mediated fusion. RT-qPCR analysis of PiT1 expression on a panel of mouse adult and fetal tissues revealed a concomitant increase of PiT1 and SynB specifically in the developing placenta. Finally, electron microscopy analysis of the placenta of PiT1 null embryo before they die (E11.5) disclosed default of ST-II formation with lack of syncytialization, as previously observed in cognate SynB null placenta, and consistent with the present identification of PiT1 as the SynB partner. [ABSTRACT FROM AUTHOR]

Published

2024

61. Complement Factor B Inhibition or Deletion Is Not Sufficient to Prevent Neurodegeneration in a Murine Model of Glaucoma.

Author

Dolan, Katie, Liao, Sha-Mei, Crowley, Maura, Xiang, Chuanxi, Adams, Christopher M., Brown, Ann, Vo, Nhi, Chen, Amy, Delgado, Omar, Buchanan, Natasha, Guo, Chenying, and Prasanna, Ganesh

Subjects

*GLYCIDYL methacrylate, *COMPLEMENT inhibition, *INTRAOCULAR pressure, *OPTIC nerve, *HYALURONIC acid, *RETINAL ganglion cells

Abstract

Purpose: Activation of the classical complement pathway is thought to contribute to the development and progression of glaucoma. The role of alternative complement or amplification pathways in glaucoma is not well understood. We evaluated complement factor B (FB) expression in postmortem human ocular tissues with or without glaucoma and the effect of FB inhibition and deletion in a mouse ocular hypertensive model of glaucoma induced by photopolymerized hyaluronic acid glycidyl methacrylate (HAGM). Methods: Human CFB mRNA in human eyes was assessed by RNAscope and TaqMan. HAGM model was performed on C57BL6/J mice. The effect of FB in HAGM model was evaluated with an oral FB inhibitor and Cfb−/− mice. Complement mRNA and proteins in mouse eyes were assessed by TaqMan and western blot, respectively. Results:CFB mRNA in human glaucomatous macular neural retina and optic nerve head was upregulated. Cfb mRNA is also upregulated in the HAGM model. Oral FB inhibitor, ED-79-GX17, dosed daily at 200 mg/kg for 3 days after intraocular pressure (IOP) induction in wild-type mice showed complement inhibition in ocular tissues and significantly inhibited systemic complement levels. Daily dosing of ED-79-GX17 for 30 days or Cfb deletion was also unable to prevent retinal ganglion cell or axon loss 30 days after IOP induction in mice. Conclusion: The alternative complement component FB may not substantially contribute to RGC loss in the HAGM mouse glaucoma model despite upregulation of Cfb expression and activation of the alternative pathway. The relevance of these findings to human glaucoma remains to be determined. [ABSTRACT FROM AUTHOR]

Published

2024

62. Loss of STING impairs lactogenic differentiation.

Author

Vickers, Ramiah R., Wyatt, Garhett L., Sanchez, Lilia, VanPortfliet, Jordyn J., West, A. Phillip, and Porter, Weston W.

Subjects

*TYPE I interferons, *MAMMARY glands, *REACTIVE oxygen species, *BREAST cancer, *EPITHELIAL cells

Abstract

Heightened energetic and nutrient demand during lactogenic differentiation of the mammary gland elicits upregulation of various stress responses to support cellular homeostasis. Here, we identify the stimulator of interferon genes (STING) as an immune supporter of the functional development of mouse mammary epithelial cells (MECs). An in vitro model of MEC differentiation revealed that STING is activated in a cGAS-independent manner to produce both type I interferons and proinflammatory cytokines in response to the accumulation of mitochondrial reactive oxygen species. Induction of STING activity was found to be dependent on the breast tumor suppressor gene single-minded 2 (SIM2). Using mouse models of lactation, we discovered that loss of STING activity results in early involution of #3 mammary glands, severely impairing lactational performance. Our data suggest that STING is required for successful functional differentiation of the mammary gland and bestows a differential lactogenic phenotype between #3 mammary glands and the traditionally explored inguinal 4|9 pair. These findings affirm unique development of mammary gland pairs that is essential to consider in future investigations into normal development and breast cancer initiation. [ABSTRACT FROM AUTHOR]

Published

2024

63. Myonuclear position and blood vessel organization during skeletal muscle postnatal development.

Author

Sequeira, Catarina, Martha Wackerbarth, Lou, Pena, Andreia, Sá-Pereira, Mafalda, Franco, Cláudio A., and Gomes, Edgar R.

Subjects

*MUSCLE growth, *BLOOD vessels, *PUERPERIUM, *MICE, *ADULTS

Abstract

Skeletal muscle development is a complex process involving myoblast fusion to generate multinucleated fibers. Myonuclei first align in the center of the myotubes before migrating to the periphery of the myofiber. Blood vessels (BVs) are important contributors to the correct development of skeletal muscle, and myonuclei are found next to BVs in adult muscle. Here, we show that most myonuclear migration to the periphery occurs between embryonic day 17.5 and postnatal day 1 in mouse. Furthermore, myonuclear accretion after postnatal day 7 does not result in centrally nucleated myofibers as observed in the embryo. Instead, myonuclei remain at the periphery of the myofiber without moving to the center. Finally, we show that hypovascularization of skeletal muscle alters the interaction between myonuclei and BVs, suggesting that BVs may contribute to myonuclear positioning during skeletal muscle postnatal development. Overall, this work provides a comprehensive analysis of skeletal muscle development during the highly dynamic postnatal period, bringing new insights about myonuclear positioning and its interaction with BVs. [ABSTRACT FROM AUTHOR]

Published

2024

64. Determination of Ibuprofen Enantiomers in Mouse Blood Using Liquid Chromatography–Tandem Mass Spectrometry and Its Application to a Pharmacokinetic Study.

Author

Li, Yuexin, Li, Jinglai, Yang, Huanhuan, Luo, Huan, Liu, Shiqi, Han, Furong, Ruan, Zhipeng, and Xiong, Zhili

Subjects

*PROPIONIC acid, *INTRAVENOUS therapy, *MASS spectrometry, *ANIONS, *ENANTIOMERS, *LIQUID chromatography-mass spectrometry

Abstract

The aim of this study was to establish a simple, fast, and sensitive method with liquid chromatography–tandem mass spectrometry (LC–MS/MS) for simultaneously determining ibuprofen enantiomers using mouse blood in very small volumes. LC–MS/MS equipped with an electrospray ionization (ESI) source was used in negative ion mode and multiple‐reaction monitoring mode. Enantiomer chromatographic separation was carried out on a Lux® 5 μm Cellulose‐3 (250 × 4.6 mm, 5 μm) column at a flow rate of 0.6 mL/min. Samples were pretreated by extracting only 5 μL of blood with 40 μL of acetonitrile (containing 1.3% formic acid) so that a concentration‐time profile could be completed using a single mouse. 2‐(4‐Propylphenyl) propanoic acid was used as an internal standard. Standard curves for each enantiomer were linear from 0.04 to 80.00 μg/mL, demonstrating a lower limit of quantitation (LLOQ) than all previously reported methods. This method was completely validated and successfully executed to investigate the pharmacokinetics of ibuprofen enantiomers after intravenous administration of racemic ibuprofen, (S)‐(+)‐ibuprofen, and (R)‐(−)‐ibuprofen in Kunming mice, respectively. The results showed that the pharmacokinetic profiles of the (R)‐(−)‐ibuprofen and (S)‐(+)‐ibuprofen were significantly different, indicating the unidirectional inversion of R‐(−)‐ibuprofen to (S)‐(+)‐ibuprofen. [ABSTRACT FROM AUTHOR]

Published

2024

65. CDNF Exerts Anxiolytic, Antidepressant-like, and Procognitive Effects and Modulates Serotonin Turnover and Neuroplasticity-Related Genes.

Author

Tsybko, Anton, Eremin, Dmitry, Ilchibaeva, Tatiana, Khotskin, Nikita, and Naumenko, Vladimir

Subjects

*UNFOLDED protein response, *SLEEP duration, *FRONTAL lobe, *MONOAMINE oxidase, *RECOMBINANT proteins

Abstract

Cerebral dopamine neurotrophic factor (CDNF) is an unconventional neurotrophic factor because it does not bind to a known specific receptor on the plasma membrane and functions primarily as an unfolded protein response (UPR) regulator in the endoplasmic reticulum. Data on the effects of CDNF on nonmotor behavior and monoamine metabolism are limited. Here, we performed the intracerebroventricular injection of a recombinant CDNF protein at doses of 3, 10, and 30 μg in C57BL/6 mice. No adverse effects of the CDNF injection on feed and water consumption or locomotor activity were observed for 3 days afterwards. Decreases in body weight and sleep duration were transient. CDNF-treated animals demonstrated improved performance on the operant learning task and a substantial decrease in anxiety and behavioral despair. CDNF in all the doses enhanced serotonin (5-HT) turnover in the murine frontal cortex, hippocampus, and midbrain. This alteration was accompanied by changes in the mRNA levels of the 5-HT1A and 5-HT7 receptors and in monoamine oxidase A mRNA and protein levels. We found that CDNF dramatically increased c-Fos mRNA levels in all investigated brain areas but elevated the phosphorylated-c-Fos level only in the midbrain. Similarly, enhanced CREB phosphorylation was found in the midbrain in experimental animals. Additionally, the upregulation of a spliced transcript of XBP1 (UPR regulator) was detected in the midbrain and frontal cortex. Thus, we can hypothesize that exogenous CDNF modulates the UPR pathway and overall neuronal activation and enhances 5-HT turnover, thereby affecting learning and emotion-related behavior. [ABSTRACT FROM AUTHOR]

Published

2024

66. Multiple promoter and enhancer differences likely contribute to augmented G6PC2 expression in human versus mouse pancreatic islet alpha cells.

Author

Martin, Cyrus C., Oeser, James K., Wangmo, Tenzin, Flemming, Brian P., Attie, Alan D., Keller, Mark P., and O'Brien, Richard M.

Subjects

*GENE expression, *ISLANDS of Langerhans, *INSULIN sensitivity, *NON-coding RNA, *GLUCOSE metabolism, *GENE enhancers

Abstract

G6PC2 encodes a glucose-6-phosphatase catalytic subunit that opposes the action of glucokinase in pancreatic islets, thereby modulating the sensitivity of insulin and glucagon secretion to glucose. In mice, G6pc2 is expressed at ~20-fold higher levels in ß-cells than in a-cells, whereas in humans G6PC2 is expressed at only ~5-fold higher levels in ß-cells. We therefore hypothesize that G6PC2 likely influences glucagon secretion to a greater degree in humans. With a view to generating a humanized mouse that recapitulates augmented G6PC2 expression levels in a-cells, we sought to identify the genomic regions that confer differential mouse G6pc2 expression in a-cells versus ß-cells as well as the evolutionary changes that have altered this ratio in humans. Studies in islet-derived cell lines suggest that the elevated G6pc2 expression in mouse ß-cells versus a-cells is mainly due to a difference in the relative activity of the proximal G6pc2 promoter in these cell types. Similarly, the smaller difference in G6PC2 expression between a-cells and ß-cells in humans is potentially explained by a change in relative proximal G6PC2 promoter activity. However, we show that both glucocorticoid levels and multiple differences in the relative activity of eight transcriptional enhancers between mice and humans likely contribute to differential G6PC2 expression. Finally, we show that a mouse-specific non-coding RNA, Gm13613, whose expression is controlled by G6pc2 enhancer I, does not regulate G6pc2 expression, indicating that altered expression of Gm13613 in a humanized mouse that contains both the human promoter and enhancers should not affect G6PC2 function. [ABSTRACT FROM AUTHOR]

Published

2024

67. Computational modelling of mouse atrio ventricular node action potential and automaticity.

Author

Bartolucci, Chiara, Mesirca, Pietro, Ricci, Eugenio, Sales‐Bellés, Clara, Torre, Eleonora, Louradour, Julien, Mangoni, Matteo Elia, and Severi, Stefano

Subjects

*ATRIOVENTRICULAR node, *HEART conduction system, *ELECTRIC properties of hearts, *HEART physiology, *CELL compartmentation

Abstract

The atrioventricular node (AVN) is a crucial component of the cardiac conduction system. Despite its pivotal role in regulating the transmission of electrical signals between atria and ventricles, a comprehensive understanding of the cellular electrophysiological mechanisms governing AVN function has remained elusive. This paper presents a detailed computational model of mouse AVN cell action potential (AP). Our model builds upon previous work and introduces several key refinements, including accurate representation of membrane currents and exchangers, calcium handling, cellular compartmentalization, dynamic update of intracellular ion concentrations, and calcium buffering. We recalibrated and validated the model against existing and unpublished experimental data. In control conditions, our model reproduces the AVN AP experimental features, (e.g. rate = 175 bpm, experimental range [121, 191] bpm). Notably, our study sheds light on the contribution of L‐type calcium currents, through both Cav1.2 and Cav1.3 channels, in AVN cells. The model replicates several experimental observations, including the cessation of firing upon block of Cav1.3 or INa,r current. If block induces a reduction in beating rate of 11%. In summary, this work presents a comprehensive computational model of mouse AVN cell AP, offering a valuable tool for investigating pacemaking mechanisms and simulating the impact of ionic current blockades. By integrating calcium handling and refining formulation of ionic currents, our model advances understanding of this critical component of the cardiac conduction system, providing a platform for future developments in cardiac electrophysiology. Key points: This paper introduces a comprehensive computational model of mouse atrioventricular node (AVN) cell action potentials (APs).Our model is based on the electrophysiological data from isolated mouse AVN cells and exhibits an action potential and calcium transient that closely match the experimental records.By simulating the effects of blocking specific ionic currents, the model effectively predicts the roles of L‐type Cav1.2 and Cav1.3 channels, T‐type calcium channels, sodium currents (TTX‐sensitive and TTX‐resistant), and the funny current (If) in AVN pacemaking.The study also emphasizes the significance of other ionic currents, including IKr, Ito, IKur, in regulating AP characteristics and cycle length in AVN cells.The model faithfully reproduces the rate dependence of action potentials under pacing, opening the possibility of use in impulse propagation models.The population‐of‐models approach showed the robustness of this new AP model in simulating a wide spectrum of cellular pacemaking in AVN. [ABSTRACT FROM AUTHOR]

Published

2024

68. Propagation of sharp wave‐ripple activity in the mouse hippocampal CA3 subfield in vitro.

Author

Schieferstein, Natalie, del Toro, Ana, Evangelista, Roberta, Imbrosci, Barbara, Swaminathan, Aarti, Schmitz, Dietmar, Maier, Nikolaus, and Kempter, Richard

Subjects

*HIPPOCAMPUS physiology, *SLOW wave sleep, *SLEEP physiology, *SLEEP movements, *SLEEP interruptions

Abstract

Sharp wave‐ripple complexes (SPW‐Rs) are spontaneous oscillatory events that characterize hippocampal activity during resting periods and slow‐wave sleep. SPW‐Rs are related to memory consolidation – the process during which newly acquired memories are transformed into long‐lasting memory traces. To test the involvement of SPW‐Rs in this process, it is crucial to understand how SPW‐Rs originate and propagate throughout the hippocampus. SPW‐Rs can originate in CA3, and they typically spread from CA3 to CA1, but little is known about their formation within CA3. To investigate the generation and propagation of SPW‐Rs in CA3, we recorded from mouse hippocampal slices using multi‐electrode arrays and patch‐clamp electrodes. We characterized extracellular and intracellular correlates of SPW‐Rs and quantified their propagation along the pyramidal cell layer of CA3. We found that a hippocampal slice can be described by a speed and a direction of propagation of SPW‐Rs. The preferred propagation direction was from CA3c (the subfield closer to the dentate gyrus) toward CA3a (the subfield at the boundary to CA2). In patch‐clamp recordings from CA3 pyramidal neurons, propagation was estimated separately for excitatory and inhibitory currents associated with SPW‐Rs. We found that propagation speed and direction of excitatory and inhibitory currents were correlated. The magnitude of the speed of propagation of SPW‐Rs within CA3 was consistent with the speed of propagation of action potentials in axons of CA3 principal cells. Key points: Hippocampal sharp waves are considered important for memory consolidation; therefore, it is of interest to understand the mechanisms of their generation and propagation.Here, we used two different approaches to study the propagation of sharp waves in mouse CA3 in vitro: multi‐electrode arrays and multiple single‐cell recordings.We find a preferred direction of propagation of sharp waves from CA3c toward CA3a – both in the local field potential and in sharp wave‐associated excitatory and inhibitory synaptic activity.The speed of sharp wave propagation is consistent with the speed of action potential propagation along the axons of CA3 pyramidal neurons.These new insights into the dynamics of sharp waves in the CA3 network will inform future experiments and theoretical models of sharp‐wave generation mechanisms. [ABSTRACT FROM AUTHOR]

Published

2024

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

Author

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

Subjects

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

Abstract

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

Published

2024

70. Functionalized Protein Binders in Developmental Biology.

Author

Schnider, Sophie T., Vigano, M. Alessandra, Affolter, Markus, and Aguilar, Gustavo

Abstract

Developmental biology has greatly profited from genetic and reverse genetic approaches to indirectly studying protein function. More recently, nanobodies and other protein binders derived from different synthetic scaffolds have been used to directly dissect protein function. Protein binders have been fused to functional domains, such as to lead to protein degradation, relocalization, visualization, or posttranslational modification of the target protein upon binding. The use of such functionalized protein binders has allowed the study of the proteome during development in an unprecedented manner. In the coming years, the advent of the computational design of protein binders, together with further advances in scaffold engineering and synthetic biology, will fuel the development of novel protein binder–based technologies. Studying the proteome with increased precision will contribute to a better understanding of the immense molecular complexities hidden in each step along the way to generate form and function during development. [ABSTRACT FROM AUTHOR]

Published

2024

71. Phoenixin knockout mice show no impairment in fertility or differences in metabolic response to a high‐fat diet, but exhibit behavioral differences in an open field test.

Author

McIlwraith, Emma K., Loganathan, Neruja, Mak, Kimberly W. Y., He, Wenyuan, and Belsham, Denise D.

Subjects

*KNOCKOUT mice, *ESTRUS, *MELANOCORTIN receptors, *HOMEOSTASIS, *MEMBRANE proteins

Abstract

Phoenixin (PNX) is a conserved secreted peptide that was identified 10 years ago with numerous studies published on its pleiotropic functions. PNX is associated with estrous cycle length, protection from a high‐fat diet, and reduction of anxiety behavior. However, no study had yet evaluated the impact of deleting PNX in the whole animal. We sought to evaluate a mouse model lacking the PNX parent gene, small integral membrane protein 20 (Smim20), and the resulting effect on reproduction, energy homeostasis, and anxiety. We found that the Smim20 knockout mice had normal fertility and estrous cycle lengths. Consistent with normal fertility, the hypothalamii of the knockout mice showed no changes in the levels of reproduction‐related genes, but the male mice had some changes in energy homeostasis‐related genes, such as melanocortin receptor 4 (Mc4r). When placed on a high‐fat diet, the wildtype and knockout mice responded similarly, but the male heterozygous mice gained slightly less weight. When placed in an open field test box, the female knockout mice traveled less distance in the outer zone, indicating alterations in anxiety or locomotor behavior. In summary, the homozygous knockout of PNX did not alter fertility and modestly alters a few neuroendocrine genes in response to a high‐fat diet, especially in the female mice. However, it altered the behavior of mice in an open field test. PNX therefore may not be crucial for reproductive function or weight, however, we cannot rule out possible compensatory mechanisms in the knockout model. Understanding the role of PNX in physiology may ultimately lead to an enhanced understanding of neuroendocrine mechanisms involving this enigmatic peptide. [ABSTRACT FROM AUTHOR]

Published

2024

72. Cryo-Fluorescence Tomography as a Tool for Visualizing Whole-Body Inflammation Using Perfluorocarbon Nanoemulsion Tracers.

Author

Leach, Benjamin I., Lister, Deanne, Adams, Stephen R., Bykowski, Julie, Schwartz, Amy B., McConville, Patrick, Dimant, Hemi, and Ahrens, Eric T.

Subjects

*MAGNETIC resonance imaging, *RETICULO-endothelial system, *HIGH resolution imaging, *FLUORESCENCE quenching, *CELL populations

Abstract

Purpose: We explore the use of intravenously delivered fluorescent perfluorocarbon (PFC) nanoemulsion tracers and multi-spectral cryo-fluorescence tomography (CFT) for whole-body tracer imaging in murine inflammation models. CFT is an emerging technique that provides high-resolution, three-dimensional mapping of probe localization in intact animals and tissue samples, enabling unbiased validation of probe biodistribution and minimizes reliance on laborious histological methods employing discrete tissue panels, where disseminated populations of PFC-labeled cells may be overlooked. This methodology can be used to streamline the development of new generations of non-invasive, cellular-molecular imaging probes for in vivo imaging. Procedures: Mixtures of nanoemulsions with different fluorescent emission wavelengths were administered intravenously to naïve mice and models of acute inflammation, colitis, and solid tumor. Mice were euthanized 24 h post-injection, frozen en bloc, and imaged at high resolution (~ 50 µm voxels) using CFT at multiple wavelengths. Results: PFC nanoemulsions were visualized using CFT within tissues of the reticuloendothelial system and inflammatory lesions, consistent with immune cell (macrophage) labeling, as previously reported in in vivo magnetic resonance and nuclear imaging studies. The CFT signals show pronounced differences among fluorescence wavelengths and tissues, presumably due to autofluorescence, differential fluorescence quenching, and scattering of incident and emitted light. Conclusions: CFT is an effective and complementary methodology to in vivo imaging for validating PFC nanoemulsion biodistribution at high spatial localization, bridging the resolution gap between in vivo imaging and histology. [ABSTRACT FROM AUTHOR]

Published

2024

73. Transcriptomic Plasticity of the Circadian Clock in Response to Photoperiod: A Study in Male Melatonin-Competent Mice.

Author

Cox, Olivia H., Gianonni-Guzmán, Manuel A., Cartailler, Jean-Philippe, Cottam, Matthew A., and McMahon, Douglas G.

Subjects

*GABA, *GENE expression, *SUPRACHIASMATIC nucleus, *ION channels, *RNA sequencing, *PHYSIOLOGY, *MOLECULAR clock

Abstract

Seasonal daylength, or circadian photoperiod, is a pervasive environmental signal that profoundly influences physiology and behavior. In mammals, the central circadian clock resides in the suprachiasmatic nuclei (SCN) of the hypothalamus where it receives retinal input and synchronizes, or entrains, organismal physiology and behavior to the prevailing light cycle. The process of entrainment induces sustained plasticity in the SCN, but the molecular mechanisms underlying SCN plasticity are incompletely understood. Entrainment to different photoperiods persistently alters the timing, waveform, period, and light resetting properties of the SCN clock and its driven rhythms. To elucidate novel candidate genes for molecular mechanisms of photoperiod plasticity, we performed RNA sequencing on whole SCN dissected from mice raised in long (light:dark [LD] 16:8) and short (LD 8:16) photoperiods. Fewer rhythmic genes were detected in mice subjected to long photoperiod, and in general, the timing of gene expression rhythms was advanced 4-6 h. However, a few genes showed significant delays, including Gem. There were significant changes in the expression of the clock-associated gene Timeless and in SCN genes related to light responses, neuropeptides, gamma aminobutyric acid (GABA), ion channels, and serotonin. Particularly striking were differences in the expression of the neuropeptide signaling genes Prokr2 and Cck, as well as convergent regulation of the expression of 3 SCN light response genes, Dusp4, Rasd1, and Gem. Transcriptional modulation of Dusp4 and Rasd1 and phase regulation of Gem are compelling candidate molecular mechanisms for plasticity in the SCN light response through their modulation of the critical NMDAR-MAPK/ERK-CREB/CRE light signaling pathway in SCN neurons. Modulation of Prokr2 and Cck may critically support SCN neural network reconfiguration during photoperiodic entrainment. Our findings identify the SCN light response and neuropeptide signaling gene sets as rich substrates for elucidating novel mechanisms of photoperiod plasticity. Data are also available at http://circadianphotoperiodseq.com/, where users can view the expression and rhythmic properties of genes across these photoperiod conditions. [ABSTRACT FROM AUTHOR]

Published

2024

74. Neurobiological mechanisms underlying oxytocin-mediated parental behavior in rodents.

Author

Inada, Kengo

Abstract

Parental behavior is essential for mammalian offspring to survive. Because of this significance, elucidating the neurobiological mechanisms that facilitate parental behavior has received strong interest. Decades of studies utilizing pharmacology and molecular biology have revealed that in addition to its facilitatory effects on parturition and lactation, oxytocin (OT) promotes the expression of parental behavior in rodents. Recent studies have also described the modulation of sensory processing by OT and the interaction of the OT system with other brain regions associated with parental behavior. However, the precise neurobiological mechanisms underlying the facilitation of caregiving behaviors by OT remain unclear. In this Review , I summarize the findings from rats and mice with a view toward integrating past and recent progress. I then review recent advances in the understanding of the molecular, cellular, and circuit mechanisms of OT-mediated parental behavior. Based on these observations, I propose a hypothetical model that would explain the mechanisms underlying OT-mediated parental behavior. Finally, I conclude by discussing some major remaining questions and propose potential future research directions. • Parental behavior is essential for mammalian offspring to survive. • Decades of studies have described that oxytocin promotes parental behavior. • Recent research has started to reveal how oxytocin promotes parental behavior. [ABSTRACT FROM AUTHOR]

Published

2024

75. Mode of action of dieldrin-induced liver tumors: application to human risk assessment.

Author

Klaunig, James E. and Cohen, Samuel M.

Subjects

*HEALTH risk assessment, *LIVER tumors, *CELL junctions, *PRECANCEROUS conditions, *GENE expression

Abstract

Dieldrin is an organochlorine insecticide that was widely used until 1970 when its use was banned because of its liver carcinogenicity in mice. Several long-term rodent bioassays have reported dieldrin to induce liver tumors in in several strains of mice, but not in rats. This article reviews the available information on dieldrin liver effects and performs an analysis of mode of action (MOA) and human relevance of these liver findings. Scientific evidence strongly supports a MOA based on CAR activation, leading to alterations in gene expression, which result in increased hepatocellular proliferation, clonal expansion leading to altered hepatic foci, and ultimately the formation of hepatocellular adenomas and carcinomas. Associative events include increased liver weight, centrilobular hypertrophy, increased expression of Cyp2b10 and its resulting increased enzymatic activity. Other associative events include alterations of intercellular gap junction communication and oxidative stress. Alternative MOAs are evaluated and shown not to be related to dieldrin administration. Weight of evidence shows that dieldrin is not DNA reactive, it is not mutagenic, and it is not genotoxic in general. Furthermore, activation of other pertinent nuclear receptors, including PXR, PPARα, AhR, and estrogen are not related to dieldrin-induced liver tumors nor is there liver cytotoxicity. In previous studies, rats, dogs, and non-human primates did not show increased cell proliferation or production of pre-neoplastic or neoplastic lesions following dieldrin treatment. Thus, the evidence strongly indicates that dieldrin-induced mouse liver tumors are due to CAR activation and are specific to the mouse, which are qualitatively not relevant to human hepatocarcinogenesis. Thus, there is no carcinogenic risk to humans. This conclusion is also supported by a lack of positive epidemiologic findings for evidence of liver carcinogenicity. Based on current understanding of the mode of action of dieldrin-induced liver tumors in mice, the appropriate conclusion is that dieldrin is a mouse specific liver carcinogen and it does not pose a cancer risk to humans. [ABSTRACT FROM AUTHOR]

Published

2024

76. FicD regulates adaptation to the unfolded protein response in the murine liver.

Author

Casey, Amanda K., Stewart, Nathan M., Zaidi, Naqi, Gray, Hillery F., Cox, Amelia, Fields, Hazel A., and Orth, Kim

Subjects

*UNFOLDED protein response, *HIGH-fat diet, *METABOLIC regulation, *POST-translational modification, *PHYSIOLOGICAL stress, *ENDOPLASMIC reticulum

Abstract

The unfolded protein response (UPR) is a cellular stress response that is activated when misfolded proteins accumulate in the endoplasmic reticulum (ER). Regulation of the UPR response must be adapted to the needs of the cell as prolonged UPR responses can result in disrupted cellular function and tissue damage. Previously, we discovered that the enzyme FicD (also known as Fic or HYPE) through its AMPylation and deAMPylation activity can modulate the UPR response via post-translational modification of BiP. FicD AMPylates BiP during homeostasis and deAMPylates BiP during stress. We hypothesized that FicD regulation of the UPR will play a role in mitigating the deleterious effects of UPR activation in tissues with frequent physiological stress. Here, we explore the role of FicD in the murine liver. As seen in our pancreatic studies, livers lacking FicD exhibit enhanced UPR signaling in response to short term physiologic fasting and feeding stress. However, in contrast to studies on the pancreas, livers, as a more regenerative tissue, remained remarkably resilient in the absence of FicD. The livers of FicD −/− did not show marked changes in UPR signaling or damage after either chronic high fat diet (HFD) feeding or acute pathological UPR induction. Intriguingly, FicD −/− mice showed changes in UPR induction and weight loss patterns following repeated pathological UPR induction. These findings indicate that FicD regulates UPR responses during mild physiological stress and in adaptation to repeated stresses, but there are tissue specific differences in the requirement for FicD regulation. • Loss of FicD results in altered UPR signaling and metabolism regulation in fasting and feeding liver. • FicD is not required for UPR signaling during chronic high fat diet feeding or initial UPR induction by tunicamycin. • Loss of FicD alters adaptation to repetitive acute ER stress. • Our observations suggest requirement of FicD may be both tissue and stressor dependent. [ABSTRACT FROM AUTHOR]

Published

2024

77. Stage-specific expression of Toll-like receptors in the seminiferous epithelium of mouse testis.

Author

Doğan, Göksel, Sandıkçı, Mustafa, and Karagenç, Levent

Subjects

*SPERMATOGENESIS, *TOLL-like receptors, *TESTIS, *GERM cells, *CELL populations, *EPITHELIUM

Abstract

Genes encoding Toll-like receptors (TLRs) are expressed by germ cells in the mouse testis. Nevertheless, the expression of TLRs by germ cells has only been demonstrated for TLR-3, TLR-9, and TLR-11. Furthermore, the expression of each TLR in relation to the stage of spermatogenesis remains uncertain. We aimed in the present study to examine the expression pattern of all TLRs in germ cells throughout the cycle of seminiferous epithelium in the adult mouse testis. Immunohistochemistry was used to evaluate the expression of TLRs. Results of the present study reveal the expression of TLRs by specific populations of germ cells. Expression of TLRs, except for TLR-7, at endosomal compartments, acrosomes, and/or residual bodies was another interesting and novel finding of the present study. We further demonstrate that the expression of TLR-1, -2, -3, -4, -5, -7, -11, -12, and -13 follows a distinct spatiotemporal pattern throughout the cycle of seminiferous epithelium. While TLR-1, -3, -5, -11, and -12 are expressed in all stages, TLR-4 is expressed only in early and middle stages of spermatogenic cycle. On the other hand, TLR-2, -7, and -13 are expressed only in early stage of spermatogenic cycle. Evidence demonstrating the expression of TLRs in a stage specific manner throughout spermatogenesis strengthen the hypothesis that the expression of various TLRs by germ cells is a developmentally regulated process. However, if TLRs play a role in the regulation of proliferation, growth, maturation, and differentiation of germ cells throughout the cycle of the seminiferous epithelium warrants further investigations. [ABSTRACT FROM AUTHOR]

Published

2024

78. Characterization of the gastrointestinal microbiome of the Syrian hamster (Mesocricetus auratus) and comparison to data from mice.

Author

Böswald, Linda F., Popper, Bastian, Matzek, Dana, Neuhaus, Klaus, and Wenderlein, Jasmin

Subjects

GOLDEN hamster, PHYSIOLOGY, SPECIES specificity, GASTROINTESTINAL contents, PELLETED feed

Abstract

Syrian hamsters (Mesocricetus auratus) have been increasingly used as rodent models in recent years, especially for SARS‐CoV‐2 since the pandemic. However, the physiology of this animal model is not yet well‐understood, even less when considering the digestive tract. Generally, the gastrointestinal microbiome influences the immune system, drug metabolism, and vaccination efficacy. However, a detailed understanding of the gastrointestinal microbiome of hamsters is missing. Therefore, we analyzed 10 healthy 11‐week‐old RjHan:AURA hamsters fed a pelleted standard diet. Their gastrointestinal content was sampled (i.e., forestomach, glandular stomach, ileum, cecum, and colon) and analyzed using 16S rRNA gene amplicon sequencing. Results displayed a distinct difference in the bacterial community before and after the cecum, possibly due to the available nutrients and digestive functions. Next, we compared hamsters with the literature data of young‐adult C57BL/6J mice, another important animal model. We sampled the same gastrointestinal regions and analyzed the differences in the microbiome between both rodents. Surprisingly, we found strong differences in their specific gastrointestinal bacterial communities. For instance, Lactobacillaceae were more abundant in hamsters' forestomach and ileum, while Muribaculaceae dominated in the mouse forestomach and ileum. Similarly, in mouse cecum and colon, Muribaculaceae were dominant, while in hamsters, Lachnospiraceae and Erysipelotrichaceae dominated the bacterial community. Molecular strains of Muribaculaceae in both rodent species displayed some species specificity. This comparison allows a better understanding of the suitability of the Syrian hamster as an animal model, especially regarding its comparability to other rodent models. Thereby, this work contributes to the characterization of the hamster model and allows better experimental planning. [ABSTRACT FROM AUTHOR]

Published

2024

79. Western diet-induced cognitive and metabolic dysfunctions in aged mice are prevented by rosmarinic acid in a sex-dependent fashion.

Author

Giona, Letizia, Musillo, Chiara, De Cristofaro, Gaia, Ristow, Michael, Zarse, Kim, Siems, Karsten, Tait, Sabrina, Cirulli, Francesca, and Berry, Alessandra

Abstract

Unhealthy lifestyles, such as chronic consumption of a Western Diet (WD), have been associated with increased systemic inflammation and oxidative stress (OS), a condition that may favour cognitive dysfunctions during aging. Polyphenols, such as rosmarinic acid (RA) may buffer low-grade inflammation and OS, characterizing the aging brain that is sustained by WD, promoting healthspan. The aim of this study was to evaluate the ability of RA to prevent cognitive decline in a mouse model of WD-driven unhealthy aging and to gain knowledge on the specific molecular pathways modulated within the brain. Aged male and female C57Bl/6N mice were supplemented either with RA or vehicle for 6 weeks. Following 2 weeks on RA they started being administered either with WD or control diet (CD). Successively all mice were tested for cognitive abilities in the Morris water maze (MWM) and emotionality in the elevated plus maze (EPM). Glucose and lipid homeostasis were assessed in trunk blood while the hippocampus was dissected out for RNAseq transcriptomic analysis. RA prevented insulin resistance in males while protecting both males and females from WD-dependent memory impairment. In the hippocampus, RA modulated OS pathways in males and immune- and sex hormones-related signalling cascades (Lhb and Lhcgr genes) in females. Moreover, RA overall resulted in an upregulation of Glp1r, recently identified as a promising target to prevent metabolic derangements. In addition, we also found an RA-dependent enrichment in nuclear transcription factors, such as NF-κB, GR and STAT3, that have been recently suggested to promote healthspan and longevity by modulating inflammatory and cell survival pathways. Oral RA supplementation may promote brain and metabolic plasticity during aging through antioxidant and immune-modulating properties possibly affecting the post-reproductive hormonal milieu in a sex-dependent fashion. Thus, its supplementation should be considered in the context of precision medicine as a possible strategy to preserve cognitive functions and to counteract metabolic derangements. [Display omitted] • Western diet (WD) precipitates aging in mice in a sex-dependent manner. • Rosmarinic acid (RA) prevents WD-mediated metabolic derangements in males. • RA decreases anxiety and enhances cognition in both sexes. • RA modulates oxidative stress, immune- and sex hormones-related pathways in the hippocampus. • RA supplementation could be a feasible strategy to promote healthspan. [ABSTRACT FROM AUTHOR]

Published

2024

80. Temporal progression of subchondral bone alterations in OA models involving induction of compromised meniscus integrity in mice and rats: A scoping review.

Author

Oláh, Tamás, Cucchiarini, Magali, and Madry, Henning

Abstract

To categorize the temporal progression of subchondral bone alterations induced by compromising meniscus integrity in mouse and rat models of knee osteoarthritis (OA). Scoping review of investigations reporting subchondral bone changes with appropriate negative controls in the different mouse and rat models of OA induced by compromising meniscus integrity. The available literature provides appropriate temporal detail on subchondral changes in these models, covering the entire spectrum of OA with an emphasis on early and mid-term time points. Microstructural changes of the subarticular spongiosa are comprehensively described; those of the subchondral bone plate are not. In mouse models, global subchondral bone alterations are unidirectional, involving an advancing sclerosis of the trabecular structure over time. In rats, biphasic subchondral bone alterations begin with an osteopenic degeneration and loss of subchondral trabeculae, progressing to a late sclerosis of the entire subchondral bone. Rat models, independently from the applied technique, relatively faithfully mirror the early bone loss detected in larger animals, and the late subchondral bone sclerosis observed in human advanced OA. Mice and rats allow us to study the microstructural consequences of compromising meniscus integrity at high temporal detail. Thickening of the subchondral bone plate, an early loss of thinner subarticular trabecular elements, followed by a subsequent sclerosis of the entire subchondral bone are all important and reliable hallmarks that occur in parallel with the advancing articular cartilage degeneration. Thoughtful decisions on the study design, laterality, selection of controls and volumes of interest are crucial to obtain meaningful data. [ABSTRACT FROM AUTHOR]

Published

2024

81. Immunity and Protective Efficacy of a Plant-Based Tobacco Mosaic Virus-like Nanoparticle Vaccine against Influenza a Virus in Mice.

Author

Madapong, Adthakorn, Petro-Turnquist, Erika M., Webby, Richard J., McCormick, Alison A., and Weaver, Eric A.

Subjects

TOBACCO mosaic virus, INFLUENZA vaccines, PLANT viruses, VIRUS diseases, VIRAL vaccines

Abstract

Background: The rapid production of influenza vaccines is crucial to meet increasing pandemic response demands. Here, we developed plant-made vaccines comprising centralized consensus influenza hemagglutinin (HA-con) proteins (H1 and H3 subtypes) conjugated to a modified plant virus, tobacco mosaic virus (TMV) nanoparticle (TMV-HA-con). Methods: We compared immune responses and protective efficacy against historical H1 or H3 influenza A virus infections among TMV-HA-con, HA-con protein combined with AddaVax™ adjuvant, and whole-inactivated virus vaccine (Fluzone®). Results: Immunogenicity studies demonstrated robust IgG, IgM, and IgA responses in the TMV-HA-con and HA-con protein vaccinated groups, with relatively low induction of interferon (IFN)-γ+ T-cell responses across all vaccinated groups. The TMV-HA-con and HA-con protein groups displayed partial protection (100% and 80% survival) with minimal weight loss following challenge with two H1N1 strains. The HA-con protein group exhibited 80% and 100% survival against two H3 strains, whereas the TMV-HA-con groups showed reduced protection (20% survival). The Fluzone® group conferred 20–100% survival against two H1N1 strains and one H3N1 strain, but did not protect against H3N2 infection. Conclusions: Our findings indicate that TMV-HA and HA-con protein vaccines with adjuvant induce protective immune responses against influenza A virus infections. Furthermore, our results underscore the potential of plant-based production using TMV-like nanoparticles for developing influenza A virus candidate vaccines. [ABSTRACT FROM AUTHOR]

Published

2024

82. Compared Antileishmanial Activity of Clomiphene and Tamoxifen.

Author

Sifontes-Rodríguez, Sergio, Escalona-Montaño, Alma Reyna, Mondragón Flores, Ricardo, Mollineda-Diogo, Niurka, Monzote Fidalgo, Lianet, Mondragón-Castelán, Mónica Edith, Alardin-Gutiérrez, Fedra, López-Enzana, Lourdes Araceli, Sánchez-Almaraz, Daniel Andrés, Pérez-Olvera, Ofelia, and Aguirre-García, María Magdalena

Subjects

SELECTIVE estrogen receptor modulators, ORAL drug administration, LEISHMANIA mexicana, PERITONEAL macrophages, DRUG repositioning, PARASITIC diseases

Abstract

Drug repositioning is an efficient strategy to search for new treatment alternatives that is especially valuable for neglected parasitic diseases such as leishmaniasis. Tamoxifen and raloxifene are selective estrogen receptor modulators (SERMs) that have shown antileishmanial activity. Clomiphene is a SERM structurally similar to tamoxifen, whose antileishmanial potential is unknown. That is why the objective of the present work was to evaluate its antileishmanial activity in vitro and in vivo in comparison with tamoxifen. The inhibitory effect against promastigotes of L. amazonensis, L. major, and L. mexicana was evaluated for both compounds, as well as the cytotoxicity against mouse peritoneal macrophages, the growth inhibitory activity in intracellular amastigotes of L. mexicana, and the in vivo activity in mice experimentally infected with L. mexicana. Clomiphene was about twice as active as tamoxifen against both promastigotes and intracellular amastigotes, with IC50 values of 1.7–3.3 µM for clomiphene and 2.9–6.4 µM for tamoxifen against all three species of promastigotes and 2.8 ± 0.2 µM and 3.7 ± 0.3 µM, respectively, against L. mexicana amastigotes. Clomiphene structurally affected several parasite organelles in a concentration-dependent fashion, leading to the death of both promastigotes and intracellular amastigotes. Interestingly, the macrophage host cell did not appear damaged by any of the clomiphene concentrations tested. With oral administration at 20 mg/kg for 14 days, both compounds showed similar effects in terms of reducing the growth of the lesions, as well as the weight of the lesions and the parasite load at the end of the follow-up period. The results showed the potential of SERMs as antileishmanial drugs and support further testing of clomiphene and other compounds of this pharmacological group. [ABSTRACT FROM AUTHOR]

Published

2024

83. 不同强度累积和持续运动对胰岛素抵抗小鼠肠黏膜通透性的影响.

Author

梁 飞

Abstract

BACKGROUND: The relationship between insulin resistance and intestinal mucosal permeability may be related to excess fat, inflammation and oxidative stress. At present, the influence of different kinds of exercise on this relationship has not been fully studied, and the relevant mechanism needs to be further studied. OBJECTIVE: To study the effects of continuous exercise and cumulative exercise on intestinal mucosal permeability of insulin-resistant mice induced by high fat diet, and to compare the effects of different intensities of exercise, thereby evaluating the health-promoting effects of cumulative exercise. METHODS: Four-week-old male C57BL/6J mice were fed high-fat diet to induce insulin resistance, and mice with successful modeling were randomly divided into five groups: high-fat insulin resistance group, general dietary insulin resistance group, moderate-intensity continuous exercise group, moderate-intensity cumulative exercise group, and high-intensity cumulative exercise group. Mice in the high-fat insulin resistance group received high-fat diet and mice in the other groups were fed normally. All the exercise groups received 8 weeks of different forms of treadmill training. Mice in the moderate-intensity sustained exercise group exercised for 50 minutes at a speed of 11 m/min. Mice in the moderate-intensity cumulative exercise group were subjected to 12.5 minutes of exercise, four times a day (3 hours between sessions), at a speed of 11 m/min. Mice in the high-intensity cumulative exercise group exercised for 7.5 minutes once, four times a day (3 hours between sessions), at a speed of 19 m/min. At 48 hours after the final session, the levels of lipopolysaccharide and D-lactic acid in serum of mice were detected, the pathological changes of ileal tissue were observed by hematoxylin-eosin staining, and the expression of intestinal compact linking protein was detected by western blot. The expression of interleukin-10, tumor necrosis factor αin blood and ileum and intestinal secreted immunoglobulin A were detected by ELISA. RESULTS AND CONCLUSION: High-fat diet-induced insulin resistance was associated with body mass gain. The serum levels of endotoxin and D-lactic acid significantly increased, and the levels of tumor necrosis factor-α in serum and small intestine were significantly increased. Long-term regular cumulative exercise and continuous exercise could reduce the body mass of insulin-resistant mice, significantly improve glucose metabolism, and correct or improve insulin resistance symptoms. Both long-term regular cumulative exercise and continuous exercise could increase the expression of zonula occludens protein 1 and increase the secretion of secreted immunoglobulin A in intestinal mucosal tissue, thereby improving intestinal mucosal permeability, enhancing intestinal immune function, reducing the content of lipopolysaccharide in serum, and reducing the expression of pro-inflammatory factors in circulating blood and intestinal tissue. Finally, it could protect the intestinal mucosal barrier of insulin-resistant mice. Compared with medium-intensity cumulative exercise and continuous exercise, high-intensity cumulative exercise had more obvious effects on reducing body mass, improving insulin resistance symptoms and protecting intestinal mucosal barrier in insulin-resistant mice. [ABSTRACT FROM AUTHOR]

Published

2024

84. A systematic review on the selection of reference genes for gene expression studies in rodents: are the classics the best choice?

Author

Bunde, Tiffany T., Pedra, Ana C. K., de Oliveira, Natasha R., Dellagostin, Odir A., and Bohn, Thaís L. O.

Abstract

Rodents are commonly used as animal models in studies investigating various experimental conditions, often requiring gene expression analysis. Quantitative real-time reverse transcription PCR (RT-qPCR) is the most widely used tool to quantify target gene expression levels under different experimental conditions in various biological samples. Relative normalization with reference genes is a crucial step in RT-qPCR to obtain reliable quantification results. In this work, the main reference genes used in gene expression studies among the three rodents commonly employed in scientific research—hamster, rat, and mouse—are analyzed and described. An individual literature search for each rodent was conducted using specific search terms in three databases: PubMed, Scopus, and Web of Science. A total of 157 articles were selected (rats = 73, mice = 79, and hamsters = 5), identifying various reference genes. The most commonly used reference genes were analyzed according to each rodent, sample type, and experimental condition evaluated, revealing a great variability in the stability of each gene across different samples and conditions. Classic genes, which are expected to be stably expressed in both samples and conditions analyzed, demonstrated greater variability, corroborating existing concerns about the use of these genes. Therefore, this review provides important insights for researchers seeking to identify suitable reference genes for their validation studies in rodents. [ABSTRACT FROM AUTHOR]

Published

2024

85. Relevance, strategies, and added value of mouse models in androgenetics.

Author

Singh, Vertika and Schimenti, John C.

Subjects

*MEDICAL genetics, *HUMAN reproduction, *HUMAN genetics, *MALE infertility, *BASE pairs

Abstract

Background Objectives Results and Discussion Conclusion Male Infertility is a prevalent condition worldwide, and a substantial fraction of cases are thought to have a genetic basis. Investigations into the responsible genes is limited experimentally, so mice have been used extensively to identify genes required for fertility and to understand their functions.To review the progress made in reproductive genetics based on experiments in mice, the impact upon clinical fertility genetics, and discuss how evolving technologies will continue to advance our understanding of human infertility genes.Gene knockout studies in mice have shown that several hundreds of genes are required for normal fertility and that this number is much higher in males than in females. In addition to gene discovery, the mouse is a powerful platform for functionally dissecting genetic pathways, modeling putative human infertility variants, identifying contraceptive targets, and developing in vitro gametogenesis.These ongoing studies in mice have made an enormous contribution to our understanding of the genetics of human reproduction in the sense that the “parts list” of genes for mammalian gametogenesis is being elucidated. This would have been impossible to do in humans, and in vitro systems are not yet adequate to associate genes with andrological phenotypes, especially in the germline.   [ABSTRACT FROM AUTHOR]

Published

2024

86. A Flow Cytometry-Based Examination of the Mouse White Blood Cell Differential in the Context of Age and Sex.

Author

Arlt, Elise, Kindermann, Andrea, Fritsche, Anne-Kristin, Navarrete Santos, Alexander, Kielstein, Heike, and Bazwinsky-Wutschke, Ivonne

Subjects

*LEUCOCYTES, *BLOOD testing, *BLOOD cells, *LABORATORY mice, *REFERENCE values

Abstract

Analysis of the white blood cell differential as part of a flow cytometry-based approach is a common routine diagnostic tool used in clinics and research. For human blood, the methodological approach, suitable markers, and gating strategies are well-established. However, there is a lack of information regarding the mouse blood count. In this article, we deliver a fast and easy protocol for reprocessing mouse blood for the purpose of flow cytometric analysis, as well as suitable markers and gating strategies. We also present two possible applications: for the analysis of the whole blood count, with blood from a cardiac puncture, and for the analysis of a certain leukocyte subset at multiple time points in the framework of a mouse experiment, using blood from the facial vein. Additionally, we provide orientation values by applying the method to 3-month-old and 24-month-old male and female C57BL/6J mice. Our analyses demonstrate differences in the leukocyte fractions depending on age and sex. We discuss the influencing factors and limitations that can affect the results and that, therefore, need to be considered when applying this method. The present study fills the gap in the knowledge related to the rare information on flow cytometric analysis of mouse blood and, thus, lays the foundation for further investigations in this area. [ABSTRACT FROM AUTHOR]

Published

2024

87. The mitochondrial calcium uniporter inhibitor Ru265 increases neuronal excitability and reduces neurotransmission via off‐target effects.

Author

Xu, Peng, Swain, Sarpras, Novorolsky, Robyn J., Garcia, Esperanza, Huang, Zhouyang, Snutch, Terrance P., Wilson, Justin J., Robertson, George S., and Renden, Robert B.

Subjects

*ACTION potentials, *ISCHEMIC stroke, *CALCIUM ions, *CELL death, *CALCIUM

Abstract

Background and Purpose: Excitotoxicity due to mitochondrial calcium (Ca2+) overloading can trigger neuronal cell death in a variety of pathologies. Inhibiting the mitochondrial calcium uniporter (MCU) has been proposed as a therapeutic avenue to prevent calcium overloading. Ru265 (ClRu(NH3)4(μ‐N)Ru(NH3)4Cl]Cl3) is a cell‐permeable inhibitor of the mitochondrial calcium uniporter (MCU) with nanomolar affinity. Ru265 reduces sensorimotor deficits and neuronal death in models of ischemic stroke. However, the therapeutic use of Ru265 is limited by the induction of seizure‐like behaviours. Experimental Approach: We examined the effect of Ru265 on synaptic and neuronal function in acute brain slices and hippocampal neuron cultures derived from mice, in control and where MCU expression was genetically abrogated. Key Results: Ru265 decreased evoked responses from calyx terminals and induced spontaneous action potential firing of both the terminal and postsynaptic principal cell. Recordings of presynaptic Ca2+ currents suggested that Ru265 blocks the P/Q type channel, confirmed by the inhibition of currents in cells exogenously expressing the P/Q type channel. Measurements of presynaptic K+ currents further revealed that Ru265 blocked a KCNQ current, leading to increased membrane excitability, underlying spontaneous spiking. Ca2+ imaging of hippocampal neurons showed that Ru265 increased synchronized, high‐amplitude events, recapitulating seizure‐like activity seen in vivo. Importantly, MCU ablation did not suppress Ru265‐induced increases in neuronal activity and seizures. Conclusions and Implications: Our findings provide a mechanistic explanation for the pro‐convulsant effects of Ru265 and suggest counter screening assays based on the measurement of P/Q and KCNQ channel currents to identify safe MCU inhibitors. [ABSTRACT FROM AUTHOR]

Published

2024

88. Impact of ibrutinib on inflammation in a mouse model of Graves' orbitopathy.

Author

Charm Kim, Jin Hwan Park, Yeon Jeong Choi, Hyung Oh Jun, Jin Kwon Chung, Tae Kwann Park, Jin Sook Yoon, Jae Wook Yang, and Sun Young Jang

Subjects

BRUTON tyrosine kinase, HORMONE receptors, GENE expression, INTERLEUKIN-1, LABORATORY mice

Abstract

Introduction: Bruton's tyrosine kinase (BTK) and interleukin (IL)-2 Inducible Tcell Kinase (ITK) inhibitors have anti-inflammatory properties. We investigated the therapeutic effect of ibrutinib, an orally bioavailable BTK/ITK inhibitor, in a mouse model of Graves' orbitopathy (GO). Methods: Genetic immunization was performed through intramuscular administration of the recombinant plasmid, pCMV6-hTSHR cDNA, to 8-weekold female BALB/c mice. Serum levels of T3, T4, and thyroid-stimulating hormone receptor (TSHR) antibodies (TRAbs) were quantified using enzymelinked immunosorbent assay. Histopathological changes in orbital tissues were examined using immunohistochemistry (IHC) staining for TSHR and various inflammatory markers. Following successful genetic immunization, ibrutinib was orally administered daily for 2 weeks in the GO model mice. After treatment, the mRNA and protein expression levels of BTK, ITK, IL-1b, and IL-6 in orbital tissues were evaluated using real-time PCR and Western blotting. Results: In total, 20 mice were sacrificed to confirm successful genetic immunization. The GO mouse group exhibited significantly increased serum T3, T4, and TRAb levels. IHC revealed increased expression of TSHR, IL-1b, IL-6, transforming growth factor-b1, interferon-g, CD40, CD4, BTK, and ITK in the GO mouse model. The orbital inflammation was significantly attenuated in ibrutinibtreated mice. The mRNA and protein expression levels of BTK, ITK, IL-1b, and IL-6 in orbital tissue were lower in ibrutinib-treated GO mouse group compared to the phosphate-buffered saline-treated GO mouse group. Conclusion: The GO mouse model demonstrated enhanced BTK and ITK expression. Ibrutinib, a BTK/ITK inhibitor, suppressed the inflammatory cytokine production. These findings highlight the potential involvement of BTK/ITK in the inflammatory pathogenesis of GO, suggesting its role as a novel therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2024

89. Does tolerance to ethanolinduced ataxia explain the sensitized response to ethanol?

Author

Reed, Cheryl and Phillips, Tamara J.

Subjects

GENETIC correlations, LABORATORY mice, ATAXIA, PHOTOELECTRIC cells, TESTING equipment

Abstract

Under conditions of repeated exposure to ethanol, a sensitized locomotor stimulant response develops in some strains of mice. It has been hypothesized that the sensitized response is a consequence of tolerance development to the sedative/incoordinating effects of ethanol. Conversely, ethanol-induced sensitization and tolerance may be independent effects of repeated ethanol exposure. A published study in C57BL/6J by DBA/2J recombinant inbred strains concluded that the two phenomena are not genetically related and thus perhaps mechanistically distinct. To extend evaluation beyond the genetic variance found in C57BL/6J and DBA/2J mice and examine phenotypic associations, we simultaneously measured ethanol-induced sensitization and tolerance in a genetically diverse panel of 15 standard inbred mouse strains and a genetically heterogeneous stock that was produced by the intercrossing of eight inbred mouse strains. Changes in activity counts and ataxia ratio across repeated ethanol treatments indexed sensitization and tolerance, respectively. Photocell beam breaks provided the measure of activity, and foot slip errors corrected for activity in a grid test provided a measure of coordination. The results were strain and individual dependent. The genetic correlation between magnitude of sensitization and tolerance was not significant in the panel of inbred strains, but when individual data were correlated, without regard to strain, there was a significant correlation. This relationship was also significant in the genetically heterogeneous population of mice. However, magnitude of tolerance explained only 10% of the variance in sensitization among individuals of the inbred strain population, whereas it explained 44% of the variance among individuals of the eight-strain cross. When repeated exposures to ethanol were disassociated from the test apparatus, this relationship in the eight-strain cross disappeared. Furthermore, days to peak sensitization and tolerance across days did not perfectly mirror each other. Overall, our data do not support shared genetic mechanisms in sensitization and tolerance development but suggest a partial relationship among individuals that could be related to drug-environment associations. [ABSTRACT FROM AUTHOR]

Published

2024

90. 成纤维细胞生长因子受体 1，2 在小鼠肾发育中的动态表达.

Author

薄双玲, 马太芳, 白慧健, 杨羽甜, 孙亚洁, and 赵欣晨

Abstract

BACKGROUND: The temporal and spatial expression of fibroblast growth factor receptors 1 and 2 remains a controversial issue during kidney development, so the relationship between them and kidney development remains unclear. OBJECTIVE: To observe the dynamic expression of fibroblast growth factor receptors 1 and 2 during kidney development of mice, and to investigate the relationship between them and kidney development. METHODS: The kidneys of fetal mice [embryotic days (E) 12, 14, 16, and 18] and neonatal mice [neonatal days (N) 1, 3, 7, 14, 24, and 40] were selected to examine the temporal and spatial expression of fibroblast growth factor receptors 1 and 2 by immunohistochemistry method in kidney tissues, and quantitative analysis was performed using western blot assay. RESULTS AND CONCLUSION: (1) Immunohistochemistry showed that fibroblast growth factor receptor 1 was mainly localized in metanephric tissue surrounding the tip of the ureteral bud at E12. Subsequently, fibroblast growth factor receptor 1 was expressed in immature renal corpuscles at various stages, some distal convoluted tubules and capillary loops. The positive site was mainly concentrated in the generative region. Fibroblast growth factor receptor 2 was initially expressed in both ureteral buds and metanephric tissue. Fibroblast growth factor receptor 2 was localized in immature renal corpuscles, distal tubules, collecting ducts and thin segments of medullary loops with kidney development. However, the expression of renal corpuscles was weak. (2) Stereology and western blot assay showed that the expression of fibroblast growth factor receptor 1 was high before birth and gradually decreased after birth, while the expression was very low after N7 day. The expression level of fibroblast growth factor receptor 2 increased gradually with the kidney development and tended to be stable after N7 day. (3) The results exhibit that fibroblast growth factor receptors 1 and 2 are expressed spatially and temporally during kidney development. It is speculated that fibroblast growth factor receptors 1 and 2 may influence nephron development and maturation, and fibroblast growth factor receptor 2 is critical during the formation of ureteral buds and morphology. [ABSTRACT FROM AUTHOR]

Published

2024

91. Disruption of Lipid Profile, Glucose Metabolism, and Leptin Levels following Citalopram Administration and High-Carbohydrate and High-Cholesterol Diet in Mice.

Author

Hammer, Tomáš, Kotolová, Hana, Procházka, Jiří, and Karpíšek, Michal

Subjects

*HIGH cholesterol diet, *HIGH-carbohydrate diet, *HDL cholesterol, *LIPID metabolism, *LDL cholesterol, *ADIPOKINES

Abstract

Introduction: Depression therapy has been linked to negative effects on energy metabolism, which can be attributed to various factors, including an ongoing inflammatory process commonly seen in metabolic disorders. Unhealthy lifestyle choices of patients and the impact of antidepressants on body weight and lipid and glucose metabolism also contribute to these metabolic side effects. Although not as pronounced as other psychopharmaceuticals, the increasing use of antidepressants raises concerns about their potential impact on public health. The study aimed to evaluate the short- and long-term effects of the antidepressant citalopram and its long-term combination with a special diet on metabolic parameters in mice. Methods: Animals were randomly divided into 5 groups – control, control + special diet, citalopram (10 mg/kg for 35 days), citalopram + special diet (10 mg/kg for 35 days), and citalopram (10 mg/kg for 7 days). After a described time of administration, animals were anesthetized, blood and fat and liver tissues were collected. Biochemical parameters of lipid metabolism (total cholesterol, HDL cholesterol, LDL cholesterol, triglycerides) and glucose were analyzed using spectrophotometry and relevant adipokines and cytokines were evaluated by ELISA. Results: After a week of application of citalopram, we observed dyslipidemia that persisted even at the end of the 5-week experiment. Furthermore, after 5 weeks of citalopram administration, we observed a significant decrease in body weight gain and decreased leptin levels. Changes in lipid metabolism, higher levels of adipokines leptin and PAI-1 were observed due to the special diet after 5 weeks. Conclusions: Our research suggests that the effects of citalopram and a diet on the metabolism of mice can be significant, both in the short term (1 week) and in the long term (5 weeks). [ABSTRACT FROM AUTHOR]

Published

2024

92. Performance of three multiplex real-time PCR assays for simultaneous detection of 12 infectious pathogens in mice affected with respiratory and digestive diseases.

Author

Hye-young Wang, Jaeil Ahn, Jonghoon Lee, Sang Chul Kang, and Hyunil Kim

Subjects

DIGESTIVE system diseases, RESPIRATORY diseases, PATHOGENIC microorganisms, ANIMAL experimentation, SENDAI virus, MYCOPLASMA, PSEUDOMONADACEAE

Abstract

Introduction: Research quality can be improved with reliable and reproducible experimental results when animal experiments are conducted using laboratory animals with guaranteed microbiological and genetic quality through health monitoring. Therefore, health monitoring requires the rapid and accurate diagnosis of infectious diseases in laboratory animals. Methods: This study presents a performance evaluation of a commercially available multiplex real-time PCR (mRT-PCR) assay for the rapid detection of 12 infectious pathogens (Set 1: Sendai virus [SeV, formally murine respirovirus], Mycoplasma spp., Rodentibacter pneumotropicus, and Rodentibacter heylii; Set 2: Helicobacter spp., Murine norovirus [MNV], Murine hepatitis virus [MHV], and Salmonella spp.; Set 3: Staphylococcus aureus, Streptobacillus moniliformis, Corynebacterium kutscheri, and Pseudomonas aeruginosa). To evaluate the efficacy of the mRT-PCR assay, 102 clinical samples encompassing fecal and cecal specimens were analyzed. The resulting data were then compared with the findings from sequence analysis for validation. Results: The assay’s detection limit ranged from 1 to 100 copies per reaction. Specificity testing involving various viruses and bacteria indicated no crossreactivity between strains. Additionally, the assay exhibited good reproducibility, with mean coefficients of variation for inter- and intra assay variation below 3%. The overall positive rate was 52.9% (n  =  54), with the mRT-PCR assay findings matching sequence analysis results (κ  =  1). MHV (n  =  29, 28.4%) was the most prevalent pathogen, followed by Helicobacter spp. (n  =  28, 27.5%), R. heylii (n  =  18, 17.6%), Mycoplasma spp. (n  =  14, 13.7%), MNV (n  =  12, 11.8%), S. aureus (n  =  9, 8.8%), P. aeruginosa (n  =  4, 3.9%), and R. pneumotropicus (n  =  1, 0.9%). Discussion: This assay offers a rapid turnaround time of 100 min, including 30 min for DNA preparation and 70 min for target DNA/RNA amplification. It ensures accuracy, minimizing false positives or negatives, making it a convenient tool for the simultaneous detection of infectious diseases in many samples. Overall, the propose-d assay holds promise for the effective detection of the most important pathogens in laboratory animal health monitoring. [ABSTRACT FROM AUTHOR]

Published

2024

93. Exploring mouse necropsy through augmented reality: developing a web application for enhanced learning and visualization.

Author

Atmaca, Hasan Tarik

Subjects

WEB-based user interfaces, VETERINARY pathology, ANIMAL carcasses, AUGMENTED reality, LABORATORY mice

Abstract

Necropsy, the examination of animal carcasses to determine the cause of death, is an essential skill for many professionals. Traditional training methods, however, are costly and time-consuming. The article suggests that Web-based Augmented Reality (WebAR) can offer an immersive and cost-effective training experience for laboratory animal necropsy. It describes using photogrammetry techniques to create a virtual necropsy environment consisting of 10 necropsy steps. A questionnaire was used to evaluate the usability, educational value, and drawbacks of the designed application by students who tested it. The paper outlines best practices for developing WebAR simulations, including high-fidelity 3D models and interactive elements. Additionally, it presents methods for creating new WebAR applications using specific programs or scripts. This paper highlights the potential benefits of WebAR for laboratory animal necropsy training, emphasizing its accessibility, cost-effectiveness, and scalability. [ABSTRACT FROM AUTHOR]

Published

2024

94. 拉曼光谱结合机器学习算法分类中药药性 的动物研究.

Author

陈子任, 张硕, and 徐丛剑

Abstract

Objective To explore the construction and verification of the classification model for the five properties of traditional Chinese medicine: warm, cool, cold, hot, and neutral. Methods Urine samples of mice after taking Chinese medicine of different properties were selected as research objects, and Raman spectroscopy-related technology was used for detection. The obtained data set was classified into training set and test set, and the classification model was constructed using four machine learning methods: random forest, extreme gradient boosting, support vector machine, and logistic regression. The model performance was evaluated using precision, recall, F1 score, and accuracy. Results A total of 4 888 sets of spectra were collected in this study, of which 80%, totaling 3 910 sets of spectral data, were used to build the model, and the remaining 20%, totaling 978 sets of spectral data, were used to test model performance. The accuracy of the random forest model was 92%, the extreme gradient boosting model was 87%, the support vector machine model was 83%, and the logistic regression model was 75%. The Raman shifts with the highest classification weights were 872, 1 012, 1 108, 1 190 and 1 668 cm-1. Conclusion Raman spectroscopy combined with machine learning algorithms can be used to classify the five medicinal properties of traditional Chinese medicine, among which the random forest model has the best effect. [ABSTRACT FROM AUTHOR]

Published

2024

95. Pathophysiological processes underlying hidden hearing loss revealed in Kcnt1/2 double knockout mice.

Author

Schubert, Nick M. A., Reijntjes, Daniël O. J., van Tuinen, Marcel, Vijayakumar, Sarath, Jones, Timothy A., Jones, Sherri M., and Pyott, Sonja J.

Subjects

*HIDDEN hearing loss, *HEARING disorders, *KNOCKOUT mice, *OLDER people, *PRESBYCUSIS, *INNER ear, *HEARING aids

Abstract

Presbycusis is a prevalent condition in older adults characterized by the progressive loss of hearing due to age‐related changes in the cochlea, the auditory portion of the inner ear. Many adults also struggle with understanding speech in noise despite having normal auditory thresholds, a condition termed "hidden" hearing loss because it evades standard audiological assessments. Examination of animal models and postmortem human tissue suggests that hidden hearing loss is also associated with age‐related changes in the cochlea and may, therefore, precede overt age‐related hearing loss. Nevertheless, the pathological mechanisms underlying hidden hearing loss are not understood, which hinders the development of diagnostic biomarkers and effective treatments for age‐related hearing loss. To fill these gaps in knowledge, we leveraged a combination of tools, including transcriptomic profiling and morphological and functional assessments, to identify these processes and examine the transition from hidden to overt hearing loss. As a novel approach, we took advantage of a recently characterized model of hidden hearing loss: Kcnt1/2 double knockout mice. Using this model, we find that even before observable morphological pathology, hidden hearing loss is associated with significant alteration in several processes, notably proteostasis, in the cochlear sensorineural structures, and increased susceptibility to overt hearing loss in response to noise exposure and aging. Our findings provide the first insight into the pathophysiology associated with the earliest and, therefore, most treatable stages of hearing loss and provide critical insight directing future investigation of pharmaceutical strategies to slow and possibly prevent overt age‐related hearing loss. [ABSTRACT FROM AUTHOR]

Published

2024

96. Neuroanatomical Relationship Between Nucleus Accumbens A2AR Neurons and Orexin Neurons in the Mouse Brain.

Author

Jian-ping Zhang and Rui-xi Li

Subjects

*GREEN fluorescent protein, *NUCLEUS accumbens, *GLUTAMATE transporters, *ADENO-associated virus, *DENDRITES

Abstract

To explore morphological evidence for neuronal circuits between adenosine A2A receptor (A2AR) neurons in the nucleus accumbens (NAc) and orexin neurons. The utilized adeno-associated virus (AAV) encoding humanized Renilla green fluorescent protein (hrGFP) as a tracer to visualize the expression of the A2AR neurons in the NAc and their axon distributions in orexin neurons. The Cre-dependent AAV was injected into the NAc in adenosine A2AR-Cre mice. Immunohistochemistry was then used to visualize hrGFP and their projections in orexin neurons. The data revealed that NAc A2AR neurons, mainly expressed in g-aminobutyric acidergic (GABAergic) projection neurons, projected to the hypothalamus, with apparent contacts of hrGFP containing boutons onto orexin-immunoreactive (IR) soma and dendrites. We also observed strong staining of orexin-IR varicose terminals in the NAc, with apparent contacts of orexin-IR terminals onto A2AR neurons. Furthermore, in the NAc, orexin-IR varicosities contained vesicular glutamate transporter 2 (VGluT2) and synaptophysin (Syp). These data provide morphological evidence for exploring the function between NAc A2AR neurons and orexin neuron in the hypothalamus, particularly in regulating sleep processes. [ABSTRACT FROM AUTHOR]

Published

2024

97. Mouse developmental defects, but not paraganglioma tumorigenesis, upon conditional Complex II loss in early Sox10+ cells.

Author

Lewis, Elizabeth P., Al Khazal, Fatimah, Wilbanks, Brandon, Gades, Naomi M., Ortega‐Sáenz, Patricia, López‐Barneo, José, Adameyko, Igor, and Maher, L. James

Subjects

*KREBS cycle, *NEURAL crest, *CHROMAFFIN cells, *SUCCINATE dehydrogenase, *NEURAL tube defects

Abstract

In humans, loss of heterozygosity for defective alleles of any of the four subunits of mitochondrial tricarboxylic acid cycle enzyme succinate dehydrogenase (SDH, also Complex II of the electron transport chain) can lead to paraganglioma tumors in neuroendocrine cells. With the goal of developing mouse models of this rare disorder, we have developed various SDH conditional loss strategies. Based on recent lineage tracing studies, we hypothesized that conditional SDHC loss in early embryogenesis during migration of primordial neural crest cells that form the susceptible chromaffin cells of the adrenal medulla might induce paraganglioma. We triggered low levels of detectable SDHC loss in Sox10+ cells at E11.5 of mouse development. We report that, rather than developing adrenal medulla paraganglioma (pheochromocytoma), offspring survived with evidence of neural crest cell dysfunction. Phenotypes included mild lower extremity gait anomalies suggestive of neural tube closure defects and patches of unpigmented fur consistent with neural crest‐derived melanocyte dysfunction. These defects were not observed in mice lacking Sdhc knockout. Our results add to existing data suggesting that, unlike humans, even early embryonic (Sox10‐driven) SDHx loss is inadequate to trigger paraganglioma in mice of the genetic backgrounds that have been investigated. Instead, low levels of tricarboxylic acid cycle‐deficient neural crest cells cause mild developmental defects in hind limb and melanocyte function. This new model may be of interest for studies of metabolism during early neural crest cell development. [ABSTRACT FROM AUTHOR]

Published

2024

98. Comprehensive Analysis of Age- and Sex-Related Expression of the Chaperone Protein Sigma-1R in the Mouse Brain.

Author

Tarmoun, Khadija, Lachance, Véronik, Le Corvec, Victoria, Bélanger, Sara-Maude, Beaucaire, Guillaume, and Kourrich, Saïd

Subjects

*MOLECULAR chaperones, *DENTATE gyrus, *CELL physiology, *EMOTION regulation, *ENDOPLASMIC reticulum

Abstract

Sigma-1R (S1R) is a ubiquitously distributed protein highly expressed in the brain and liver. It acts as a ligand-inducible chaperone protein localized at the endoplasmic reticulum. S1R participates in several signaling pathways that oversee diverse cellular and neurological functions, such as calcium and proteome homeostasis, neuronal activity, memory, and emotional regulation. Despite its crucial functions, S1R expression profile in the brain with respect to age and sex remains elusive. To shed light on this matter, we assessed S1R distribution in the mouse brain across different developmental stages, including juvenile, early adult, and middle-aged mice. Using immunohistochemistry, we found that S1R is predominantly expressed in the hippocampus in juvenile mice, particularly in CA1 and CA3 regions. Notably, S1R is not expressed in the subgranular layer of the dentate gyrus of juvenile mice. We observed dynamic changes in S1R levels during development, with most brain regions showing either an abrupt or gradual decline as mice transition from juveniles to adults. Sexual dimorphism is observed before puberty in the hippocampus and hypothalamus and during adulthood in the hippocampus and cortex. [ABSTRACT FROM AUTHOR]

Published

2024

99. Thymic epithelial organoids mediate T-cell development.

Author

Hübscher, Tania, Lorenzo-Martıń, L. Francisco, Barthlott, Thomas, Tillard, Lucie, Langer, Jakob J., Rouse, Paul, Blackburn, C. Clare, Holländer, Georg, and Lutolf, Matthias P.

Subjects

*DEVELOPMENTAL biology, *EPITHELIAL cells, *CELL populations, *PROGENITOR cells, *TRANSLATIONAL research

Abstract

Although the advent of organoids has opened unprecedented perspectives for basic and translational research, immune system-related organoids remain largely underdeveloped. Here, we established organoids from the thymus, the lymphoid organ responsible for T-cell development. We identified conditions enabling mouse thymic epithelial progenitor cell proliferation and development into organoids with diverse cell populations and transcriptional profiles resembling in vivo thymic epithelial cells (TECs) more closely than traditional TEC cultures. In contrast to these two-dimensional cultures, thymic epithelial organoids maintained thymus functionality in vitro and mediated physiological T-cell development upon reaggregation with T-cell progenitors. The reaggregates showed in vivo-like epithelial diversity and the ability to attract T-cell progenitors. Thymic epithelial organoids are the first organoids originating from the stromal compartment of a lymphoid organ. They provide new opportunities to study TEC biology and T-cell development in vitro, paving the way for future thymic regeneration strategies in ageing or acute injuries. [ABSTRACT FROM AUTHOR]

Published

2024

100. A cell-autonomous role for primary cilium-mediated signaling in long-range commissural axon guidance.

Author

Dumoulin, Alexandre, Wilson, Nicole H., Tucker, Kerry L., and Stoeckli, Esther T.

Subjects

*NEURAL circuitry, *CILIA & ciliary motion, *COGNITION disorders, *CHICKENS, *NEURONS

Abstract

Ciliopathies are characterized by the absence or dysfunction of primary cilia. Despite the fact that cognitive impairments are a common feature of ciliopathies, how cilia dysfunction affects neuronal development has not been characterized in detail. Here, we show that primary cilium-mediated signaling is required cell-autonomously by neurons during neural circuit formation. In particular, a functional primary cilium is crucial during axonal pathfinding for the switch in responsiveness of axons at a choice point or intermediate target. Using different animal models and in vivo, ex vivo and in vitro experiments, we provide evidence for a crucial role of primary cilium-mediated signaling in long-range axon guidance. The primary cilium on the cell body of commissural neurons transduces long-range guidance signals sensed by growth cones navigating an intermediate target. In extension of our finding that Shh is required for the rostral turn of post-crossing commissural axons, we suggest a model implicating the primary cilium in Shh signaling upstream of a transcriptional change of axon guidance receptors, which in turn mediate the repulsive response to floorplate-derived Shh shown by post-crossing commissural axons. [ABSTRACT FROM AUTHOR]

Published

2024