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通过儿科急性淋巴细胞白血病的疾病演变,靶向病变和蛋白质组预测治疗敏感性。

Targetable lesions and proteomes predict therapy sensitivity through disease evolution in pediatric acute lymphoblastic leukemia.

机构信息

Department of Pediatrics, University of British Columbia, Vancouver, Canada.

Michael Cuccione Childhood Cancer Research Program at the BC Children's Hospital Research Institute, Vancouver, Canada.

出版信息

Nat Commun. 2023 Nov 21;14(1):7161. doi: 10.1038/s41467-023-42701-9.

Abstract

Childhood acute lymphoblastic leukemia (ALL) genomes show that relapses often arise from subclonal outgrowths. However, the impact of clonal evolution on the actionable proteome and response to targeted therapy is not known. Here, we present a comprehensive retrospective analysis of paired ALL diagnosis and relapsed specimen. Targeted next generation sequencing and proteome analysis indicate persistence of actionable genome variants and stable proteomes through disease progression. Paired viably-frozen biopsies show high correlation of drug response to variant-targeted therapies but in vitro selectivity is low. Proteome analysis prioritizes PARP1 as a pan-ALL target candidate needed for survival following cellular stress; diagnostic and relapsed ALL samples demonstrate robust sensitivity to treatment with two PARP1/2 inhibitors. Together, these findings support initiating prospective precision oncology approaches at ALL diagnosis and emphasize the need to incorporate proteome analysis to prospectively determine tumor sensitivities, which are likely to be retained at disease relapse.

摘要

儿童急性淋巴细胞白血病 (ALL) 基因组表明,复发通常源于亚克隆的生长。然而,克隆进化对可操作的蛋白质组和对靶向治疗的反应的影响尚不清楚。在这里,我们对配对的 ALL 诊断和复发标本进行了全面的回顾性分析。靶向下一代测序和蛋白质组分析表明,在疾病进展过程中,可操作的基因组变异和稳定的蛋白质组得以保留。配对的可存活冷冻活检显示,药物反应与针对变异的靶向治疗具有高度相关性,但体外选择性较低。蛋白质组分析将 PARP1 作为细胞应激后生存所需的泛 ALL 靶候选物进行优先级排序;诊断和复发的 ALL 样本对两种 PARP1/2 抑制剂的治疗表现出很强的敏感性。总之,这些发现支持在 ALL 诊断时启动前瞻性精准肿瘤学方法,并强调需要进行蛋白质组分析以前瞻性地确定肿瘤敏感性,这些敏感性很可能在疾病复发时保留下来。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1a45/10663560/4b9b7c830d89/41467_2023_42701_Fig1_HTML.jpg

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