Chenyang Li scite author profile

Members of the BTB-ZF transcription factor family regulate the immune system. Our laboratory identified that family member Zbtb20 contributes to the differentiation, recall responses, and metabolism of CD8 T cells. Here, we report a characterization of the transcriptional and epigenetic signatures controlled by Zbtb20 at single-cell resolution during the effector and memory phases of the CD8 T cell response. Without Zbtb20, transcriptional programs associated with memory CD8 T cell formation were up-regulated throughout the CD8 T response. A signature of open chromatin was associated with genes controlling T cell activation, consistent with the known impact on differentiation. In addition, memory CD8 T cells lacking Zbtb20 were characterized by open chromatin regions with overrepresentation of AP-1 transcription factor motifs and elevated RNA- and protein-level expressions of the corresponding AP-1 components. Finally, we describe motifs and genomic annotations from the DNA targets of Zbtb20 in CD8 T cells identified by cleavage under targets and release under nuclease (CUT&RUN). Together, these data establish the transcriptional and epigenetic networks contributing to the control of CD8 T cell responses by Zbtb20.

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TimiGP: inferring inter-cell functional interactions and clinical values in the tumor immune microenvironment through gene pairs

Zhang

Schaafsma

et al. 2022

Preprint

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Determining how immune cells functionally interact in the tumor microenvironment and identifying their biological roles and clinical values are critical for understanding cancer progression and developing new therapeutic strategies. Here we introduce TimiGP, a computational method to infer inter-cell functional interaction networks and annotate the corresponding prognostic effect from bulk gene expression and survival statistics data. When applied to metastatic melanoma, TimiGP overcomes the prognostic bias caused by immune co-infiltration and identifies the prognostic value of immune cells consistent with their anti- or pro-tumor roles. It reveals the functional interaction network in which the interaction X→Y indicates a more positive impact of cell X than Y on survival. This network provides immunological insights to facilitate the development of prognostic models, as evidenced by our computational-friendly, biologically interpretable, independently validated models. By leveraging single-cell RNA-seq data for specific immune cell subsets, TimiGP has the flexibility to delineate the tumor microenvironment at different resolutions and is readily applicable to a wide range of cancer types.

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Characterizing control of memory CD8 T cell differentiation by BTB-ZF transcription factor Zbtb20

Preiss

Kamal

Williams

et al. 2022

Preprint

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Members of the BTB-ZF transcription factor family regulate the immune system. Our lab identified that family member Zbtb20 contributes to the differentiation, recall responses and metabolism of CD8 T cells. Here, we report a characterization of the transcriptional and epigenetic signatures controlled by Zbtb20 at single-cell resolution during the effector and memory phases of the CD8 T cell response. Without Zbtb20, transcriptional programs associated with memory CD8 T cell formation were upregulated throughout the CD8 T response. A signature of open chromatin was associated with genes controlling T cell activation, consistent with the known impact on differentiation. Additionally, memory CD8 T cells lacking Zbtb20 were characterized by open chromatin regions with overrepresentation of AP-1 transcription factor motifs and elevated RNA- and protein-level expression of the corresponding AP-1 components. Finally, we describe motifs and genomic annotations from the DNA targets of Zbtb20 in CD8 T cells identified by CUT&RUN. Together, these data establish the transcriptional and epigenetic networks contributing to the control of CD8 T cell responses by Zbtb20.

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Chenyang Li

Characterizing control of memory CD8 T cell differentiation by BTB-ZF transcription factor Zbtb20

TimiGP: inferring inter-cell functional interactions and clinical values in the tumor immune microenvironment through gene pairs

Characterizing control of memory CD8 T cell differentiation by BTB-ZF transcription factor Zbtb20

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