Project description:Aging is associated with the accumulation of Gzmk+CD8+ T cells in the blood and multiple tissues that have features of exhaustion. We have found that by genetically activating NF-kB in fibroblasts (though the deletion of the NF-kB inhibitor Tnfaip3 with the pan-fibroblast Dermo1-cre, Tnfaip3 CKO) we are able to recapitulate this age-related accumulation of Gzmk+CD8+ T cells in the lungs of young mice. We additionally generated a Gzmk reporter mouse (GATOR) that allows the identification and isolation of these cells via tdTomato expression. In the first study associated with this record, we used scRNA and TCR sequencing to compare lung resident CD3+ T cells from young Tnfaip3 CKO mice with those from young control and aged wild-type mice. As a follow-up to this initial study we utilized scRNAseq to compare the transcriptome and TCRs of lung resident Gzmk+ CD8+ T cells from aged WT mice, young Tnfaip3 CKO;GATOR mice, and young GATOR mice chronically infected with LCMV clone 13 (as a "gold standard" for T cell exhaustion).

Project description:In this study we used scRNA sequencing to compare lung fibroblast and epithelial populations from young and aged mice. We identified enrichment of a NF-kB activation signature in aged relative to young fibroblasts, particularly in the adventitial population.

Project description:Aging is one of the greatest rick factor of COVID-19. We use single cell RNA sequencing to compare the immune responses in the lung bewteen aged (19-month-old) and young (3-week-old) mice.

Project description:This study investigates age-related alterations in the brain proteome of mice using quantitative proteomics. Brain tissues from young (2-month-old) and aged (24-month-old) mice were solubilized with PTS buffer, and the extracted proteins were subjected to tandem mass tag (TMT) labeling and mass spectrometry analysis.

Project description:Single cell RNA sequencing from lungs of young (2-3 month old) and aged (20-22 month old) mice.

Project description:We performe RNA-sequencing (RNA-seq) and differential gene expression analysis on hippocampal tissues from young (3-month-old) Hdac1 cKO and control mice.

Project description:Analysis of iWAT tissues from young (2 month) and aged (12 month) C57bl/6 male mice with vehicle or CL treatments. CL-induced tissue remodeling is severely impaired in aged mice. Results provide insight into molecular mechanisms underlying age-related changes in iWAT.

Project description:The impact of Thbs1 gene deletion on BMEC activity during physiological aging is unknown. In this experiment, RNA Seq analysis was performed on BMECs derived from aged (18 month-old) Thbs1 knockout mice. BMECs derived from young (3 month-old) and aged (18 month-old) control mice were used as controls for comparison.

Project description:The impact of Thbs1 gene deletion on HSC activity during physiological aging is unknown. In this experiment, RNA Seq analysis was performed on BM HSCs derived from aged (18 month-old) Thbs1 knockout mice. HSCs derived from young (3 month-old) and aged (18 month-old) control mice were used as controls for comparison.

Project description:The impact of Thbs1 gene deletion on BM MSC activity during physiological aging is unknown. In this experiment, RNA Seq analysis was performed on BM MSCs derived from aged (18 month-old) Thbs1 knockout mice. MSCs derived from young (3 month-old) and aged (18 month-old) control mice were used as controls for comparison.