Xingxing Shao scite author profile

Xingxing Shao

3Publications

48Citation Statements Received

213Citation Statements Given

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136

207

Affiliations

Center for Life Sciences, Tsinghua University

Publications

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Transmembrane domain-mediated Lck association underlies bystander and costimulatory ICOS signaling

Wan

Shao

et al. 2018

Cell Mol Immunol

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The B7-family inducible costimulator (ICOS) activates phosphoinositide-3 kinase (PI3K) and augments calcium mobilization triggered by the T-cell receptor (TCR). We surprisingly found that the entire cytoplasmic domain of ICOS is dispensable for its costimulation of calcium mobilization. This costimulatory function relies on the unique transmembrane domain (TMD) of ICOS, which promotes association with the tyrosine kinase Lck. TMD-enabled Lck association is also required for p85 recruitment to ICOS and subsequent PI3K activation, and Lck underlies both the bystander and costimulatory signaling activity of ICOS. TMD-replaced ICOS, even with an intact cytoplasmic domain, fails to support T FH development or GC formation in vivo. When transplanted onto a chimeric antigen receptor (CAR), the ICOS TMD enhances interactions between T cells and antigen-presenting target cells. Therefore, by revealing an unexpected function of the ICOS TMD, our study offers a new perspective for the understanding and potential application of costimulation biology.

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BCL6 controls contact-dependent help delivery during follicular T-B cell interactions

et al. 2021

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BCL6 is required for development of follicular T helper (Tfh) cells to support germinal center (GC) formation. However, it is not clear what unique functions programmed by BCL6 can explain its absolute essentiality in T cells for GC formation. We found that ablation of one Bcl6 allele did not appreciably alter early T cell activation and follicular localization but inhibited GC formation and Tfh cell maintenance. BCL6 impinged on Tfh calcium signaling and also controlled Tfh entanglement with and CD40L delivery to B cells. Amounts of BCL6 protein and nominal frequencies of Tfh cells markedly changed within hours after strengths of T-B cell interactions were altered in vivo, while CD40L overexpression rectified both defective GC formation and Tfh cell maintenance because of the BCL6 haploinsufficiency. Our results reveal BCL6 functions in Tfh cells that are essential for GC formation and suggest that BCL6 helps maintain Tfh cell phenotypes in a T cell non-autonomous manner.

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A role for Hes1 in constraining germinal center B cell formation

Shao¹,

Liu²,

Qi³

2023

Cell Insight

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Xingxing Shao

Transmembrane domain-mediated Lck association underlies bystander and costimulatory ICOS signaling

BCL6 controls contact-dependent help delivery during follicular T-B cell interactions

A role for Hes1 in constraining germinal center B cell formation

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