Overall survival with circulating tumor DNA-guided therapy in advanced non-small-cell lung cancer

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作者
Justin Jee
Emily S. Lebow
Randy Yeh
Jeeban P. Das
Azadeh Namakydoust
Paul K. Paik
Jamie E. Chaft
Gowtham Jayakumaran
A. Rose Brannon
Ryma Benayed
Ahmet Zehir
Mark Donoghue
Nikolaus Schultz
Debyani Chakravarty
Ritika Kundra
Ramyasree Madupuri
Yonina R. Murciano-Goroff
Hai-Yan Tu
Chong-Rui Xu
Andrés Martinez
Clare Wilhelm
Jesse Galle
Bobby Daly
Helena A. Yu
Michael Offin
Matthew D. Hellmann
Piro Lito
Kathryn C. Arbour
Marjorie G. Zauderer
Mark G. Kris
Kenneth K. Ng
Juliana Eng
Isabel Preeshagul
W. Victoria Lai
John J. Fiore
Afsheen Iqbal
Daniela Molena
Gaetano Rocco
Bernard J. Park
Lee P. Lim
Mark Li
Candace Tong-Li
Madhawa De Silva
David L. Chan
Connie I. Diakos
Malinda Itchins
Stephen Clarke
Nick Pavlakis
Adrian Lee
Natasha Rekhtman
机构
[1] Memorial Sloan Kettering Cancer Center,Weill Cornell Medicine
[2] Cornell University,Guangdong Lung Cancer Institute
[3] Guangdong Provincial People’s Hospital and Guangdong Academy of Medical Sciences,GenesisCare
[4] Resolution Bioscience,undefined
[5] Agilent Technologies,undefined
[6] University of Sydney,undefined
[7] Massachusetts Institute of Technology,undefined
来源
Nature Medicine | 2022年 / 28卷
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摘要
Circulating tumor DNA (ctDNA) sequencing guides therapy decisions but has been studied mostly in small cohorts without sufficient follow-up to determine its influence on overall survival. We prospectively followed an international cohort of 1,127 patients with non-small-cell lung cancer and ctDNA-guided therapy. ctDNA detection was associated with shorter survival (hazard ratio (HR), 2.05; 95% confidence interval (CI), 1.74–2.42; P < 0.001) independently of clinicopathologic features and metabolic tumor volume. Among the 722 (64%) patients with detectable ctDNA, 255 (23%) matched to targeted therapy by ctDNA sequencing had longer survival than those not treated with targeted therapy (HR, 0.63; 95% CI, 0.52–0.76; P < 0.001). Genomic alterations in ctDNA not detected by time-matched tissue sequencing were found in 25% of the patients. These ctDNA-only alterations disproportionately featured subclonal drivers of resistance, including RICTOR and PIK3CA alterations, and were associated with short survival. Minimally invasive ctDNA profiling can identify heterogeneous drivers not captured in tissue sequencing and expand community access to life-prolonging therapy.
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页码:2353 / 2363
页数:10
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