Tumour-intrinsic PDL1 signals regulate the Chk2 DNA damage response in cancer cells and mediate resistance to Chk1 inhibitors

被引:0
|
作者
Murray, Clare E. [1 ,2 ]
Kornepati, Anand V. R. [1 ,2 ,22 ]
Ontiveros, Carlos [1 ,2 ]
Liao, Yiji [3 ,4 ]
de la Pena Avalos, Barbara [5 ]
Rogers, Cody M. [5 ]
Liu, Zexuan [6 ]
Deng, Yilun [6 ]
Bai, Haiyan [3 ,4 ]
Kari, Suresh [6 ]
Padron, Alvaro S. [6 ]
Boyd, Jacob T. [1 ,2 ]
Reyes, Ryan [1 ,2 ]
Clark, Curtis A. [1 ,2 ,23 ]
Svatek, Robert S. [7 ,8 ]
Li, Rong [9 ,24 ]
Hu, Yanfen [9 ,25 ]
Wang, Meiling [5 ]
Conejo-Garcia, Jose R. [11 ]
Byers, Lauren A. [12 ]
Ramkumar, Kavya [12 ]
Sood, Anil K. [13 ]
Lee, Jung-Min [14 ]
Burd, Christin E. [15 ,16 ,17 ]
Vadlamudi, Ratna K. [6 ,8 ]
Gupta, Harshita B. [5 ]
Zhao, Weixing [5 ]
Dray, Eloise [5 ]
Sung, Patrick [5 ,8 ]
Curiel, Tyler J. [1 ,2 ,3 ,4 ,6 ,10 ,18 ,19 ,20 ,21 ,26 ]
机构
[1] Univ Texas Hlth San Antonio, Grad Sch Biomed Sci, San Antonio, TX 78229 USA
[2] Univ Texas Hlth San Antonio, Long Sch Med, San Antonio, TX 78229 USA
[3] Dartmouth Geisel Sch Med, Dartmouth Canc Ctr, Hanover, NH 03755 USA
[4] Dartmouth Hlth, Geisel Sch Med Dartmouth, Dept Microbiol & Immunol, Hanover, NH 03766 USA
[5] Univ Texas Hlth San Antonio, Dept Biochem & Struct Biol, San Antonio, TX USA
[6] Univ Texas Hlth San Antonio, Dept Med, San Antonio, TX 78229 USA
[7] Univ Texas Hlth San Antonio, Dept Urol, San Antonio, TX USA
[8] Univ Texas Hlth San Antonio, Mays Canc Ctr, San Antonio, TX USA
[9] Univ Texas Hlth San Antonio, Dept Mol Med, San Antonio, TX USA
[10] UT Southwestern, Dallas, TX 75390 USA
[11] Duke Canc Ctr, Durham, NC USA
[12] Univ Texas MD Anderson Canc Ctr, Dept Thorac & Head & Neck Med Oncol, Houston, TX USA
[13] UT MD Anderson Canc Ctr, Dept Gynecol Oncol & Reprod Med, Houston, TX USA
[14] NCI, Womens Malignancies Branch, Ctr Canc Res, Bethesda, MD USA
[15] Ohio State Univ, Dept Mol Genet, Columbus, OH 43210 USA
[16] Ohio State Univ, Dept Canc Biol, Columbus, OH USA
[17] Ohio State Univ, Dept Genet, Columbus, OH USA
[18] Dartmouth Hlth, Lebanon, NH 03766 USA
[19] Dartmouth Canc Ctr, Lebanon, NH 03766 USA
[20] Geisel Sch Med Dartmouth, Hanover, NH 03755 USA
[21] Dartmouth Coll, Dept Microbiol & Immunol, Hanover, NH 03755 USA
[22] NYU, Grossman Sch Med, Grossman Sch Med, New York, NY 10012 USA
[23] Univ Alabama Birmingham, Sch Med, Dept Radiol, Birmingham, AL 35233 USA
[24] George Washington Univ, Sch Med & Hlth Sci, Dept Biochem & Mol Med, Washington, DC 20037 USA
[25] George Washington Univ, Sch Med & Hlth Sci, Dept Pathol, Washington, DC USA
[26] Duke Univ, Dept Integrat Immunobiol, Durham, NC 27710 USA
来源
MOLECULAR CANCER | 2024年 / 23卷 / 01期
基金
美国国家卫生研究院;
关键词
DNA damage repair; DDR inhibitors; Synthetic lethality; Immune checkpoints; PDL1; Chk2; PD-L1; REPAIR; ATR; MECHANISM; DISTINCT; KINASE; ROLES; CMTM6;
D O I
10.1186/s12943-024-02147-z
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
BackgroundAside from the canonical role of PDL1 as a tumour surface-expressed immune checkpoint molecule, tumour-intrinsic PDL1 signals regulate non-canonical immunopathological pathways mediating treatment resistance whose significance, mechanisms, and therapeutic targeting remain incompletely understood. Recent reports implicate tumour-intrinsic PDL1 signals in the DNA damage response (DDR), including promoting homologous recombination DNA damage repair and mRNA stability of DDR proteins, but many mechanistic details remain undefined.MethodsWe genetically depleted PDL1 from transplantable mouse and human cancer cell lines to understand consequences of tumour-intrinsic PDL1 signals in the DNA damage response. We complemented this work with studies of primary human tumours and inducible mouse tumours. We developed novel approaches to show tumour-intrinsic PDL1 signals in specific subcellular locations. We pharmacologically depleted tumour PDL1 in vivo in mouse models with repurposed FDA-approved drugs for proof-of-concept clinical translation studies.ResultsWe show that tumour-intrinsic PDL1 promotes the checkpoint kinase-2 (Chk2)-mediated DNA damage response. Intracellular but not surface-expressed PDL1 controlled Chk2 protein content post-translationally and independently of PD1 by antagonising PIRH2 E3 ligase-mediated Chk2 polyubiquitination and protein degradation. Genetic tumour PDL1 depletion specifically reduced tumour Chk2 content but not ATM, ATR, or Chk1 DDR proteins, enhanced Chk1 inhibitor (Chk1i) synthetic lethality in vitro in diverse human and murine tumour models, and improved Chk1i efficacy in vivo. Pharmacologic tumour PDL1 depletion with cefepime or ceftazidime replicated genetic tumour PDL1 depletion by reducing tumour Chk2, inducing Chk1i synthetic lethality in a tumour PDL1-dependent manner, and reducing in vivo tumour growth when combined with Chk1i.ConclusionsOur data challenge the prevailing surface PDL1 paradigm, elucidate important and previously unappreciated roles for tumour-intrinsic PDL1 in regulating the ATM/Chk2 DNA damage response axis and E3 ligase-mediated protein degradation, suggest tumour PDL1 as a biomarker for Chk1i efficacy, and support the rapid clinical potential of pharmacologic tumour PDL1 depletion to treat selected cancers.
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页数:24
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