作者
Aadel A Chaudhuri, Jacob J Chabon, Alexander F Lovejoy, Aaron M Newman, Henning Stehr, Tej D Azad, Michael S Khodadoust, Mohammad Shahrokh Esfahani, Chih Long Liu, Li Zhou, Florian Scherer, David M Kurtz, Carmen Say, Justin N Carter, David J Merriott, Jonathan C Dudley, Michael S Binkley, Leslie Modlin, Sukhmani K Padda, Michael F Gensheimer, Robert B West, Joseph B Shrager, Joel W Neal, Heather A Wakelee, Billy W Loo Jr, Ash A Alizadeh, Maximilian Diehn
发表日期
2017/12/1
期刊
Cancer discovery
卷号
7
期号
12
页码范围
1394-1403
出版商
American Association for Cancer Research
简介
Identifying molecular residual disease (MRD) after treatment of localized lung cancer could facilitate early intervention and personalization of adjuvant therapies. Here, we apply cancer personalized profiling by deep sequencing (CAPP-seq) circulating tumor DNA (ctDNA) analysis to 255 samples from 40 patients treated with curative intent for stage I–III lung cancer and 54 healthy adults. In 94% of evaluable patients experiencing recurrence, ctDNA was detectable in the first posttreatment blood sample, indicating reliable identification of MRD. Posttreatment ctDNA detection preceded radiographic progression in 72% of patients by a median of 5.2 months, and 53% of patients harbored ctDNA mutation profiles associated with favorable responses to tyrosine kinase inhibitors or immune checkpoint blockade. Collectively, these results indicate that ctDNA MRD in patients with lung cancer can be accurately …
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