Project description:T cell activation is accompanied by extensive changes in epigenome. However, whether and how high-ordered chromatin organization is involved in CD8+ T cell activation is unclear. Here, we showed extensive changes in the three-dimensional genome during CD8+ T cell activation, associated with changes in gene transcription. Moreover, we identified Tripartite motif containing 28 (TRIM28) as an essential mediator in re-organization of spatial chromosomal interactions. Trim28 deficiency impaired CD8+ T cell activation in vitro and in vivo, due to its regulation on autocrine IL-2 production. Mechanistically, TRIM28 bound to genes associated with CD8+ T cell activation and promoted the formation of chromosomal loops. At the loop anchor regions, TRIM28 is likely recruited by CTCF, and required for binding of RNA Pol II and cohesin to form active chromosomal structure. These results thus identify a critical role of TRIM28-dependent chromatin topology in gene transcription during CD8+ T cell activation.

Project description:T cell activation is accompanied by extensive changes in epigenome. However, whether and how high-ordered chromatin organization is involved in CD8+ T cell activation is unclear. Here, we showed extensive changes in the three-dimensional genome during CD8+ T cell activation, associated with changes in gene transcription. Moreover, we identified Tripartite motif containing 28 (TRIM28) as an essential mediator in re-organization of spatial chromosomal interactions. Trim28 deficiency impaired CD8+ T cell activation in vitro and in vivo, due to its regulation on autocrine IL-2 production. Mechanistically, TRIM28 bound to genes associated with CD8+ T cell activation and promoted the formation of chromosomal loops. At the loop anchor regions, TRIM28 is likely recruited by CTCF, and required for binding of RNA Pol II and cohesin to form active chromosomal structure. These results thus identify a critical role of TRIM28-dependent chromatin topology in gene transcription during CD8+ T cell activation.

Project description:T cell activation is accompanied by extensive changes in epigenome. However, whether and how high-ordered chromatin organization is involved in CD8+ T cell activation is unclear. Here, we showed extensive changes in the three-dimensional genome during CD8+ T cell activation, associated with changes in gene transcription. Moreover, we identified Tripartite motif containing 28 (TRIM28) as an essential mediator in re-organization of spatial chromosomal interactions. Trim28 deficiency impaired CD8+ T cell activation in vitro and in vivo, due to its regulation on autocrine IL-2 production. Mechanistically, TRIM28 bound to genes associated with CD8+ T cell activation and promoted the formation of chromosomal loops. At the loop anchor regions, TRIM28 is likely recruited by CTCF, and required for binding of RNA Pol II and cohesin to form active chromosomal structure. These results thus identify a critical role of TRIM28-dependent chromatin topology in gene transcription during CD8+ T cell activation.

Project description:T cell activation is accompanied by extensive changes in epigenome. However, whether and how high-ordered chromatin organization is involved in CD8+ T cell activation is unclear. Here, we showed extensive changes in the three-dimensional genome during CD8+ T cell activation, associated with changes in gene transcription. Moreover, we identified Tripartite motif containing 28 (TRIM28) as an essential mediator in re-organization of spatial chromosomal interactions. Trim28 deficiency impaired CD8+ T cell activation in vitro and in vivo, due to its regulation on autocrine IL-2 production. Mechanistically, TRIM28 bound to genes associated with CD8+ T cell activation and promoted the formation of chromosomal loops. At the loop anchor regions, TRIM28 is likely recruited by CTCF, and required for binding of RNA Pol II and cohesin to form active chromosomal structure. These results thus identify a critical role of TRIM28-dependent chromatin topology in gene transcription during CD8+ T cell activation.

Project description:T cell activation is accompanied by extensive changes in epigenome. However, whether and how high-ordered chromatin organization is involved in CD8+ T cell activation is unclear. Here, we showed extensive changes in the three-dimensional genome during CD8+ T cell activation, associated with changes in gene transcription. Moreover, we identified Tripartite motif containing 28 (TRIM28) as an essential mediator in re-organization of spatial chromosomal interactions. Trim28 deficiency impaired CD8+ T cell activation in vitro and in vivo, due to its regulation on autocrine IL-2 production. Mechanistically, TRIM28 bound to genes associated with CD8+ T cell activation and promoted the formation of chromosomal loops. At the loop anchor regions, TRIM28 is likely recruited by CTCF, and required for binding of RNA Pol II and cohesin to form active chromosomal structure. These results thus identify a critical role of TRIM28-dependent chromatin topology in gene transcription during CD8+ T cell activation.

Project description:Many genes have been implicated in WAT lipid metabolism, including tripartite motif containing 28 (Trim28), a gene proposed to primarily influence adiposity via epigenetic mechanisms in embryonic development. We set out to determine if adipose specific deletion of Trim28 led to changes in adipose tissue function and molecular phenotype. We performed transcriptomics analysis on adipose tissue taken from WT and adipose specific Trim28 KO mice to investigate their molecular phenotype, and to identify pathways altered in KO animals.

Project description:Cell fate decision is mediated by epigenetic mechanisms. We have analyzed naive T cell differentiation into Th17 cells, which is regulated by environmental cytokines and their downstream transcription factors. RORγt is a lineage-specific master transcription factor for Th17 cells. Although epigenetic mechanisms have been implicated in Th17 cell differentiation, how transcription factors interact to activate epigenetic program is unclear. Here we show that tripartite motif containing 28 (TRIM28) expression in Th17 cells is required for cytokine production and autoimmune diseases. Genome-wide occupancy analysis reveals that TRIM28 bound regions contain many super-enhancers, which are impaired after TRIM28 or STAT3 but not RORγt deletion. Importantly, TRIM28 exists in a complex with STAT3 and RORγt; TRIM28 recruitment to the Il17 gene requires STAT3, and further promotes RORγt recruitment. TRIM28 thus is a key player in the epigenetic activation during T cell differentiation.

Project description:Cell fate decision is mediated by epigenetic mechanisms. We have analyzed naive T cell differentiation into Th17 cells, which is regulated by environmental cytokines and their downstream transcription factors. RORγt is a lineage-specific master transcription factor for Th17 cells. Although epigenetic mechanisms have been implicated in Th17 cell differentiation, how transcription factors interact to activate epigenetic program is unclear. Here we show that tripartite motif containing 28 (TRIM28) expression in Th17 cells is required for cytokine production and autoimmune diseases. Genome-wide occupancy analysis reveals that TRIM28 bound regions contain many super-enhancers, which are impaired after TRIM28 or STAT3 but not RORγt deletion. Importantly, TRIM28 exists in a complex with STAT3 and RORγt; TRIM28 recruitment to the Il17 gene requires STAT3, and further promotes RORγt recruitment. TRIM28 thus is a key player in the epigenetic activation during T cell differentiation.

Project description:The Tripartite motif-containing 28 (TRIM28) transcription factor is upregulated in high-grade prostate cancers and was recently proposed as a therapeutic target for castration-resistant prostate cancers. To study the role of TRIM28 in prostate cancer progression in vivo, we used a genetically engineered mouse model, combining prostate-specific Trim28 inactivation with inactivation of Trp53 and Pten. We analyzed the prostates using single cell RNA-Seq.

Project description:Epigenetic mechanism contributes to immune landscapes in cancer. Here we identify the SETDB1-TRIM28 complex as a critical suppressor of antitumor immunity. An epigenetic CRISPR-Cas9 screen of 1,218 chromatin regulators identified TRIM28 as a novel suppressor of PD-L1 expression. We revealed that expression of the SETDB1-TRIM28 complex negatively correlates with infiltration of effector CD8+ T cells. Inhibition of SETDB1-TRIM28 simultaneously upregulates PD-L1 and activates the cGAS-STING innate immune response to increase infiltration of CD8+ T cells. Mechanistically, SETDB1-TRIM28 inhibition leads to micronuclei formation in cytoplasm, a known activator of the cGAS-STING pathway. Thus, SETDB1-TRIM28 inhibition bridges the innate and adaptive immunity. Indeed, SETDB1 knockout enhances the antitumor effects of immune checkpoint blockade anti-PD-L1 in an ovarian cancer mouse model in a cGAS dependent manner. Our findings establish SETDB1-TRIM28 complex as a regulator of antitumor immunity and its loss activates cGAS-STING innate immunity to boost antitumor effects of immune checkpoint blockades.