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转移性小细胞肺癌和患者来源模型中神经内分泌转录状态的异质性。

Heterogeneity of neuroendocrine transcriptional states in metastatic small cell lung cancers and patient-derived models.

机构信息

Laboratory of Human Carcinogenesis, Center for Cancer Research, NCI, Bethesda, MD, 20892, USA.

Developmental Therapeutics Branch, Center for Cancer Research, NCI, Bethesda, MD, 20892, USA.

出版信息

Nat Commun. 2022 Apr 19;13(1):2023. doi: 10.1038/s41467-022-29517-9.

DOI:10.1038/s41467-022-29517-9
PMID:35440132
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9018864/
Abstract

Molecular subtypes of small cell lung cancer (SCLC) defined by the expression of key transcription regulators have recently been proposed in cell lines and limited number of primary tumors. The clinical and biological implications of neuroendocrine (NE) subtypes in metastatic SCLC, and the extent to which they vary within and between patient tumors and in patient-derived models is not known. We integrate histology, transcriptome, exome, and treatment outcomes of SCLC from a range of metastatic sites, revealing complex intra- and intertumoral heterogeneity of NE differentiation. Transcriptomic analysis confirms previously described subtypes based on ASCL1, NEUROD1, POU2F3, YAP1, and ATOH1 expression, and reveal a clinical subtype with hybrid NE and non-NE phenotypes, marked by chemotherapy-resistance and exceedingly poor outcomes. NE tumors are more likely to have RB1, NOTCH, and chromatin modifier gene mutations, upregulation of DNA damage response genes, and are more likely to respond to replication stress targeted therapies. In contrast, patients preferentially benefited from immunotherapy if their tumors were non-NE. Transcriptional phenotypes strongly skew towards the NE state in patient-derived model systems, an observation that was confirmed in paired patient-matched tumors and xenografts. We provide a framework that unifies transcriptomic and genomic dimensions of metastatic SCLC. The marked differences in transcriptional diversity between patient tumors and model systems are likely to have implications in development of novel therapeutic agents.

摘要

小细胞肺癌 (SCLC) 的分子亚型是根据关键转录调控因子的表达来定义的,最近在细胞系和有限数量的原发性肿瘤中得到了提出。在转移性 SCLC 中神经内分泌 (NE) 亚型的临床和生物学意义,以及它们在肿瘤内和肿瘤间的变化程度,以及在患者衍生模型中的变化程度尚不清楚。我们整合了来自一系列转移性部位的 SCLC 的组织学、转录组、外显子组和治疗结果,揭示了 NE 分化的复杂的肿瘤内和肿瘤间异质性。转录组分析基于 ASCL1、NEUROD1、POU2F3、YAP1 和 ATOH1 的表达,证实了先前描述的亚型,并揭示了一种具有混合 NE 和非 NE 表型的临床亚型,其特征是对化疗耐药和预后极差。NE 肿瘤更有可能发生 RB1、NOTCH 和染色质修饰基因突变,DNA 损伤反应基因上调,并且更可能对复制应激靶向治疗有反应。相比之下,如果肿瘤是非 NE,患者更有可能从免疫治疗中受益。在患者衍生的模型系统中,转录表型强烈偏向于 NE 状态,这一观察结果在配对的患者匹配肿瘤和异种移植中得到了证实。我们提供了一个统一转移性 SCLC 的转录组和基因组维度的框架。患者肿瘤和模型系统之间转录多样性的显著差异可能对新型治疗药物的开发产生影响。

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