| Literature DB >> 35122027 |
Fan Yang1, Samuel W Brady2, Chao Tang1, Huiying Sun1, Lijuan Du1, Malwine J Barz3, Xiaotu Ma2, Yao Chen1, Houshun Fang1, Xiaomeng Li1, Pandurang Kolekar2, Omkar Pathak2, Jiaoyang Cai1, Lixia Ding1, Tianyi Wang1, Arend von Stackelberg3, Shuhong Shen1, Cornelia Eckert3,4, Jeffery M Klco5, Hongzhuan Chen6,7, Caiwen Duan1,6, Yu Liu1, Hui Li1, Benshang Li1, Renate Kirschner-Schwabe8,9, Jinghui Zhang10, Bin-Bing S Zhou11,12.
Abstract
Chemotherapy is a standard treatment for pediatric acute lymphoblastic leukemia (ALL), which sometimes relapses with chemoresistant features. However, whether acquired drug-resistance mutations in relapsed ALL pre-exist or are induced by treatment remains unknown. Here we provide direct evidence of a specific mechanism by which chemotherapy induces drug-resistance-associated mutations leading to relapse. Using genomic and functional analysis of relapsed ALL we show that thiopurine treatment in mismatch repair (MMR)-deficient leukemias induces hotspot TP53 R248Q mutations through a specific mutational signature (thio-dMMR). Clonal evolution analysis reveals sequential MMR inactivation followed by TP53 mutation in some patients with ALL. Acquired TP53 R248Q mutations are associated with on-treatment relapse, poor treatment response and resistance to multiple chemotherapeutic agents, which could be reversed by pharmacological p53 reactivation. Our findings indicate that TP53 R248Q in relapsed ALL originates through synergistic mutagenesis from thiopurine treatment and MMR deficiency and suggest strategies to prevent or treat TP53-mutant relapse.Entities:
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Year: 2021 PMID: 35122027 DOI: 10.1038/s43018-021-00230-8
Source DB: PubMed Journal: Nat Cancer ISSN: 2662-1347