KRAS 野生型胰腺导管腺癌的分子特征和治疗机会

Cancers Pub Date : 2024-05-13 DOI:10.3390/cancers16101861
Aakash Desai, Alexander Xiao, Daheui Choi, M. D. Toruner, Daniel J. Walden, T. Halfdanarson, Steven R Alberts, Robert R. McWilliams, Amit Mahipal, Daniel H Ahn, Hani Babiker, Gulnaz Stybayeva, Alexander Revzin, S. Kizilbash, Alex Adjei, Tanios B. Bekaii-Saab, A. S. Mansfield, Ryan M. Carr, Wen Wee Ma
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摘要

目的:研究 KRAS 野生型胰腺导管腺癌 (PDAC) 的分子特征和精准医疗的潜力。患者和方法:我们调查了本院的 27 例 KRASWT PDAC 患者。临床数据通过病历审查获得。通过 DNA 测序对每个受试者的肿瘤标本进行体细胞单核苷酸变异、插入和缺失以及拷贝数变异的检测。通过 RNA-seq 检测基因融合。从一名患有 MET 易位的患者身上提取出患者衍生类器官(PDO),并进行体外扩增,以便在加入 2 期临床试验之前预测治疗敏感性。结果转录组分析表明,我们的队列可能会根据 KRAS 信号级联的相对基因表达进行分层。我们发现,从携带 TFG-MET 重排的患者身上提取的 PDO 对多酪氨酸激酶抑制剂克唑替尼具有体外敏感性。该患者参加了 SPARTA 2 期临床试验,并接受了 c-MET 抑制剂维布雷替尼的单药治疗,取得了部分和持久的应答。结论KRASWT PDAC在分子上有别于KRASMUT,富含潜在的可操作基因变异。在我们的研究中,转录组分析显示 KRAS 信号级联可能在 KRASWT PDAC 中起着关键作用。我们报告的一名患有 TFG-MET 重排的 KRASWT PDAC 患者对 cMET 抑制剂产生了反应,这进一步支持了在该亚群中开展精准肿瘤学研究。通过RNA-seq等方法鉴定可靶向的突变,有助于实现精准驱动,根据肿瘤特征选择最佳治疗方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Molecular Characterization and Therapeutic Opportunities in KRAS Wildtype Pancreatic Ductal Adenocarcinoma
Purpose: To investigate the molecular characteristics of and potential for precision medicine in KRAS wildtype pancreatic ductal adenocarcinoma (PDAC). Patients and Methods: We investigated 27 patients with KRASWT PDAC at our institution. Clinical data were obtained via chart review. Tumor specimens for each subject were interrogated for somatic single nucleotide variants, insertion and deletions, and copy number variants by DNA sequencing. Gene fusions were detected from RNA-seq. A patient-derived organoid (PDO) was developed from a patient with a MET translocation and expanded ex vivo to predict therapeutic sensitivity prior to enrollment in a phase 2 clinical trial. Results: Transcriptomic analysis showed our cohort may be stratified by the relative gene expression of the KRAS signaling cascade. The PDO derived from our patient harboring a TFG-MET rearrangement was found to have in vitro sensitivity to the multi-tyrosine kinase inhibitor crizotinib. The patient was enrolled in the phase 2 SPARTA clinical trial and received monotherapy with vebrelitinib, a c-MET inhibitor, and achieved a partial and durable response. Conclusions: KRASWT PDAC is molecularly distinct from KRASMUT and enriched with potentially actionable genetic variants. In our study, transcriptomic profiling revealed that the KRAS signaling cascade may play a key role in KRASWT PDAC. Our report of a KRASWT PDAC patient with TFG-MET rearrangement who responded to a cMET inhibitor further supports the pursuit of precision oncology in this sub-population. Identification of targetable mutations, perhaps through approaches like RNA-seq, can help enable precision-driven approaches to select optimal treatment based on tumor characteristics.
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