LBPO.IM02 · 免疫学 · Late-Breaking
Progenitor-to-intermediate differentiation of exhausted CD8+T cells is enhanced by HPK1 inhibition during anti-PD-1 therapy
作者与单位
摘要 Abstract
Cancer treatment has been transformed by immunotherapies that enhance anti-tumor T-cell responses. Here we demonstrate that highly selective inhibition of the intracellular immune checkpoint HPK1 improves the efficacy of anti-PD-1/PD-L1 blockade. Single-cell profiling of ex vivo antigen-stimulated T cells reveals that HPK1 inhibition expands tumor-specific clones that substantially overlap with those responsive to PD-1 blockade. HPK1 inhibition induces progenitor exhausted CD8 + T cells (T PEX cells) to differentiate and acquire phenotypic and functional features of intermediate exhausted CD8 + T cells (T IEX cells). In a mouse tumor model, HPK1 inhibition enhances T PEX cell expansion in tumor-draining lymph nodes and migration to tumors during PD-1 blockade. Moreover, HPK1 inhibition promotes lymph node T PEX cells' differentiation into tumor T IEX cells during PD-1 blockade, highlighting an underappreciated immunotherapy mechanism. Our findings reveal that HPK1 inhibition induces progenitor-to-intermediate differentiation of exhausted CD8 + T cells, enhancing the efficacy of anti-PD-1/PD-L1 blockade.
利益披露 Disclosure
Y. Lee, None..
S. Jeon, None.
S. Lim,
1ST Biotherapeutics, Inc. Employment.
M. Jeon, None..
H. Nam, None.
A. Park,
1ST Biotherapeutics, Inc. Employment.
B. Gu,
1ST Biotherapeutics, Inc. Employment.
J. Kim, None..
S. Kim, None..
J. Jang, None..
C. Kim, None..
S. Hwang, None..
G. Song, None..
J. Cheong, None..
B. Min, None..
S. Park, None..
S. Seo, None.
J. Lee,
1ST Biotherapeutics, Inc. g., Board of Directors, non-salaried role).
M. Kang, None.
J. Kim,
1ST Biotherapeutics, Inc. g., Board of Directors, non-salaried role).
E. Shin,
1ST Biotherapeutics, Inc. ).