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致命性前列腺癌中的肿瘤克隆动态变化

Tumor clone dynamics in lethal prostate cancer.

作者信息

Carreira Suzanne, Romanel Alessandro, Goodall Jane, Grist Emily, Ferraldeschi Roberta, Miranda Susana, Prandi Davide, Lorente David, Frenel Jean-Sebastien, Pezaro Carmel, Omlin Aurelius, Rodrigues Daniel Nava, Flohr Penelope, Tunariu Nina, S de Bono Johann, Demichelis Francesca, Attard Gerhardt

机构信息

The Institute of Cancer Research, London SM2 5NG, UK.

Centre for Integrative Biology, University of Trento, Trento 38123, Italy.

出版信息

Sci Transl Med. 2014 Sep 17;6(254):254ra125. doi: 10.1126/scitranslmed.3009448.

DOI:10.1126/scitranslmed.3009448
PMID:25232177
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4422178/
Abstract

It is unclear whether a single clone metastasizes and remains dominant over the course of lethal prostate cancer. We describe the clonal architectural heterogeneity at different stages of disease progression by sequencing serial plasma and tumor samples from 16 ERG-positive patients. By characterizing the clonality of commonly occurring deletions at 21q22, 8p21, and 10q23, we identified multiple independent clones in metastatic disease that are differentially represented in tissue and circulation. To exemplify the clinical utility of our studies, we then showed a temporal association between clinical progression and emergence of androgen receptor (AR) mutations activated by glucocorticoids in about 20% of patients progressing on abiraterone and prednisolone or dexamethasone. Resistant clones showed a complex dynamic with temporal and spatial heterogeneity, suggesting distinct mechanisms of resistance at different sites that emerged and regressed depending on treatment selection pressure. This introduces a management paradigm requiring sequential monitoring of advanced prostate cancer patients with plasma and tumor biopsies to ensure early discontinuation of agents when they become potential disease drivers.

摘要

尚不清楚单个克隆是否会转移并在致命性前列腺癌病程中保持主导地位。我们通过对16例ERG阳性患者的系列血浆和肿瘤样本进行测序,描述了疾病进展不同阶段的克隆结构异质性。通过对21q22、8p21和10q23常见缺失的克隆性进行表征,我们在转移性疾病中鉴定出多个独立克隆,它们在组织和循环中的表现存在差异。为了例证我们研究的临床实用性,我们随后展示了在约20%接受阿比特龙和泼尼松龙或地塞米松治疗后病情进展的患者中,临床进展与糖皮质激素激活的雄激素受体(AR)突变出现之间的时间关联。耐药克隆呈现出具有时间和空间异质性的复杂动态变化,这表明不同部位的耐药机制不同,这些机制会根据治疗选择压力出现和消退。这引入了一种管理模式,需要对晚期前列腺癌患者进行血浆和肿瘤活检的序贯监测,以确保在药物成为潜在疾病驱动因素时尽早停用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/47d8/4422178/5e154f1ffb0f/nihms681846f7.jpg
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Detection of circulating tumor DNA in early- and late-stage human malignancies.早期和晚期人类恶性肿瘤中循环肿瘤DNA的检测
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