Author:
Mei Yihan,Liu Yu,Liu Wenbing,Chen Manling,Liu Xiaoyu,Wang Shangshang,Mou Junli,Xing Haiyan,Tang Kejing,Tian Zheng,Rao Qing,Wang Min,Gu Runxia,Qiu Shaowei,Wang Jianxiang
Abstract
AbstractBesides chemotherapy and hematopoietic stem cell transplantation (HSCT), autologous T cells can also serve as a new treatment approach for AML patients. However, the features of tumor-reactive T cells and their distinctive markers still lack full description. To evaluate the characteristics of tumor-reactive T cells, we collected bone marrow (BM) T cells from newly diagnosed AML patients with RUNX1::RUNX1T1 as examples for paired single-cell RNA sequencing and single-cell V(D)J sequencing. Based on the STARTRAC-like algorithm, we defined bystander T cells and tumor-reactive T cells. Compared with bystander T cells, tumor-reactive T cells presented as senescent-like cytotoxic terminally differentiated T cells (Temra) with upregulated NK-related markers. Additionally, we found ADGRG1 could serve as the specific marker of CD8+ T tumor-reactive T cell and validated it through the Runx1Runx1t1/+; Mx1-Cre mouse model. In chimeric antigen receptor (CAR)-T and target cell system, ADGRG1 was selectively upregulated upon antigen-TCR encounter. Moreover, ADGRG1+CD8+ T cells released a higher level of IFN-γ and showed higher cell-killing ability when exposed to matched AML blasts. Together, our findings depict the single-cell profile of tumor-reactive T cells in AML BM and propose that ADGRG1 can act as an indicator of T cell tumor reactivity in AML, which may be further harnessed for adoptive cell therapy and tumor-reactive TCR enrichment.
Funder
National Key Research and Development Program of China
CAMS Innovation Fund for Medical Sciences
National Natural Science Foundation of China
Clinical Research Foundation of National Clinical Research Center for Blood Diseases
Tianjin Municipal Science and Technology Commission Grant
Publisher
Springer Science and Business Media LLC