Early Detection of Molecular Residual Disease in Localized Lung Cancer by Circulating Tumor DNA Profiling

Chaudhuri Aadel A.; Chabon Jacob J.; Lovejoy Alexander F.; Newman Aaron M.; Stehr Henning; Azad Tej D.; Khodadoust Michael S.; Esfahani Mohammad Shahrokh; Liu Chih Long; Zhou Li; Scherer Florian; Kurtz David M.; Say Carmen; Carter Justin N.; Merriott David J.; Dudley Jonathan C.; Binkley Michael S.; Modlin Leslie; Padda Sukhmani K.; Gensheimer Michael F.; West Robert B.; Shrager Joseph B.; Neal Joel W.; Wakelee Heather A.; Loo Billy W. Jr.; Alizadeh Ash A.; Diehn Maximilian

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Early Detection of Molecular Residual Disease in Localized Lung Cancer by Circulating Tumor DNA Profiling

机译：循环肿瘤DNA分析早期检测局部肺癌分子残留疾病

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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 detected using CAPP-seq and may allow personalized adjuvant treatment while disease burden is lowest.

机译：鉴定分子残留疾病（MRD）治疗局部肺癌后可以促进佐剂疗法的早期干预和个性化。在这里，我们通过深度测序（CAPP-SEQ）循环肿瘤DNA（CTDNA）分析从40名患者的循环肿瘤DNA（CTDNA）分析应用癌症个性化分析到255例治疗II-III阶段肺癌和54例健康成年人。在94％的评估患者中经历复发的患者中，CTDNA可在第一个后处理血液样品中检测，表明MRD的可靠鉴定。 Metertreatment CTDNA检测在72％的患者中位于5.2个月的72％的射线照相进展，53％的患者患有对酪氨酸激酶抑制剂或免疫检查点封闭的有利反应相关的患者。总的来说，这些结果表明，使用CAPP-SEQ可以准确地检测肺癌患者CTDNA MRD，并且可以允许个性化佐剂治疗，而疾病负担是最低的。

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《Cancer discovery.》 |2017年第12期|共10页
作者
Chaudhuri Aadel A.; Chabon Jacob J.; Lovejoy Alexander F.; Newman Aaron M.; Stehr Henning; Azad Tej D.; Khodadoust Michael S.; Esfahani Mohammad Shahrokh; Liu Chih Long; Zhou Li; Scherer Florian; Kurtz David M.; Say Carmen; Carter Justin N.; Merriott David J.; Dudley Jonathan C.; Binkley Michael S.; Modlin Leslie; Padda Sukhmani K.; Gensheimer Michael F.; West Robert B.; Shrager Joseph B.; Neal Joel W.; Wakelee Heather A.; Loo Billy W. Jr.; Alizadeh Ash A.; Diehn Maximilian;
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作者单位

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

Stanford Univ Inst Stem Cell Biol &

Regenerat Med Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

Stanford Univ Div Oncol Dept Med Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

Stanford Univ Div Thorac Surg Stanford Sch Med Dept Cardiothorac Surg Stanford CA 94305 USA;

Roche Sequencing Solut Pleasanton CA USA;

Stanford Univ Div Oncol Dept Med Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Div Oncol Dept Med Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

Stanford Univ Stanford Canc Inst Stanford CA 94305 USA;

Stanford Univ Dept Radiat Oncol Stanford CA 94305 USA;

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正文语种 eng
中图分类肿瘤学;
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1. Early Detection of Molecular Residual Disease in Localized Lung Cancer by Circulating Tumor DNA Profiling [J] . Chaudhuri Aadel A., Chabon Jacob J., Lovejoy Alexander F., Cancer discovery. . 2017,第12期

机译：循环肿瘤DNA分析早期检测局部肺癌分子残留疾病
2. MA17.07 Circulating Tumor DNA Detects Minimal Residual Disease and Predicts Outcome in Localized Lung Cancer [J] . Aadel Chaudhuri, Alexander Lovejoy, Jacob Chabon, Journal of thoracic oncology: official publication of the International Association for the Study of Lung Cancer . 2017,第1期

机译：MA17.07循环肿瘤DNA检测最小的残余疾病，并预测局部肺癌的结果
3. Circulating Tumor DNA Analysis for Detection of Minimal Residual Disease After Chemoradiotherapy for Localized Esophageal Cancer [J] . Azad Tej D., Chaudhuri Aadel A., Fang Penny, Gastroenterology . 2020,第3期

机译：循环肿瘤DNA分析，用于检测局部食管癌中疗法后最小的残留疾病
4. Molecular Characterization of Circulating Tumor Cells Enriched by a Microfluidic Platform in Patients with Small-Cell Lung Cancer [C] . Robert Zeilinger International Molecular Medicine Tri-Conference. . 2019

机译：小细胞肺癌患者微流体平台富集的循环肿瘤细胞的分子表征
5. Investigating the Use of Circulating Tumor DNA for Cancer Surveillance and Early Detection in (Pediatric) Sarcomas and Li-Fraumeni Syndrome [D] . Paramathas, Sangeetha . 2020

机译：研究使用循环肿瘤DNA进行癌症监测和早期检测（儿科）肉瘤和Li-Fraumeni综合征
6. Early Detection of Molecular Residual Disease in Localized Lung Cancer by Circulating Tumor DNA Profiling [O] . Aadel A. Chaudhuri, Jacob J. Chabon, Alexander F. Lovejoy, -1

机译：循环肿瘤DNA谱分析早期检测局部肺癌分子残留病
7. Targeted next-generation sequencing of circulating-tumor DNA for tracking minimal residual disease in localized colon cancer [O] . N. Tarazona, F. Gimeno-Valiente, V. Gambardella, 2019

机译：循环肿瘤DNA的靶向下一代测序，用于跟踪局部结肠癌中最小的残留疾病

Early Detection of Molecular Residual Disease in Localized Lung Cancer by Circulating Tumor DNA Profiling

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