Monitoring therapeutic response and resistance: analysis of circulating tumor DNA in patients with ALK+ lung cancer.

Authors

Leora Horn
Jennifer G Whisenant
Heather Wakelee
Karen L Reckamp
Huan Qiao
Ticiana A Leal
Liping Du
Jennifer Hernandez
Vincent Huang
George R Blumenschein
Saiama N Waqar
Sandip P Patel
Jorge Nieva
Geoffrey R Oxnard
Rachel E Sanborn, Earle A. Chiles Research Institute, Providence Cancer Center, Portland, ORFollow
Tristan Shaffer
Kavita Garg
Allison Holzhausen
Kimberly Harrow
Chris Liang
Lee P Lim
Mark Li
Christine M Lovly

Document Type

Article

Publication Date

8-22-2019

Publication Title

J Thorac Oncol

Abstract

INTRODUCTION: Despite initial effectiveness of ALK tyrosine kinase inhibitors (TKIs) in patients with ALK+ non-small cell lung cancer (NSCLC), therapeutic resistance will ultimately develop. Serial tracking of genetic alterations detected in circulating tumor DNA (ctDNA) can be an informative strategy to identify response and resistance. This study evaluated the utility of analyzing ctDNA as a function of response to ensartinib, a potent second-generation ALK TKI.

METHODS: Pre-treatment plasma was collected from 76 patients with ALK+ NSCLC who were ALK TKI naïve or had received prior ALK TKI, and analyzed for specific genetic alterations. Longitudinal plasma samples were analyzed from a subset (N=11) of patients. Analysis of pre-treatment tumor biopsies from 22 patients was compared with plasma.

RESULTS: Disease-associated genetic alterations were detected in 74% (56/76) of patients, the most common being EML4-ALK. Concordance of ALK fusion between plasma and tissue was 91% (20/22). Twenty-four ALK kinase domain mutations were detected in 15 patients, all had previously received an ALK TKI; G1269A was the most prevalent (4/24). Patients with a detectable EML4-ALK variant 1 (V1) fusion had improved response (9/17, 53%) to ensartinib compared to patients with EML4-ALK V3 fusion (1/7, 14%). Serial changes in ALK alterations were observed during therapy.

CONCLUSIONS: Clinical utility of ctDNA was demonstrated, both at pre-treatment by identifying a potential subgroup of ALK+ NSCLC patients that may derive more benefit from ensartinib and longitudinally by tracking resistance. Prospective application of this technology may translate to improved outcomes for NSCLC patients treated with ALK TKIs.

Clinical Institute

Cancer

Department

Oncology

Department

Earle A. Chiles Research Institute

Recommended Citation

Horn, Leora; Whisenant, Jennifer G; Wakelee, Heather; Reckamp, Karen L; Qiao, Huan; Leal, Ticiana A; Du, Liping; Hernandez, Jennifer; Huang, Vincent; Blumenschein, George R; Waqar, Saiama N; Patel, Sandip P; Nieva, Jorge; Oxnard, Geoffrey R; Sanborn, Rachel E; Shaffer, Tristan; Garg, Kavita; Holzhausen, Allison; Harrow, Kimberly; Liang, Chris; Lim, Lee P; Li, Mark; and Lovly, Christine M, "Monitoring therapeutic response and resistance: analysis of circulating tumor DNA in patients with ALK+ lung cancer." (2019). Articles, Abstracts, and Reports. 2045.
https://digitalcommons.providence.org/publications/2045