Clinical implications of plasma EGFR T790M and ctDNA shedding across metastatic sites in plasma-or tissue-confirmed EGFR mutant non-small cell lung cancer treated with lazertinib: a prospective multicenter cohort study-

Kim, Min Jee; Jung, Junghee; Ji, Wonjun; Choi, Chang-Min; Kim, Seung Joon; Cho, Hyung Jun; Hwang, Yong Gi; Kim, Eun Young; Lee, Shin Yup; Yoo, Seung Soo; Choi, Sunha; Oh, In-Jae; Kim, Young-Chul; Park, Chul-Kyu; Yoon, Seong Hoon; Kim, Yun Seong; Kim, Mi-Hyun; Lee, Min Ki; Eom, Jung Seop; Kim, Soo Han; Lee, Jeong Eun; Chung, Chaeuk; Yeo, Chang Dong; Lee, Sang Haak; Lee, Jae Cheol

doi:10.21037/tlcr-2025-aw-1216

YUHSpace

BROWSE

12 19

Cited 0 times in

Clinical implications of plasma EGFR T790M and ctDNA shedding across metastatic sites in plasma-or tissue-confirmed EGFR mutant non-small cell lung cancer treated with lazertinib: a prospective multicenter cohort study-

Authors: Kim, Min Jee ; Jung, Junghee ; Ji, Wonjun ; Choi, Chang-Min ; Kim, Seung Joon ; Cho, Hyung Jun ; Hwang, Yong Gi ; Kim, Eun Young ; Lee, Shin Yup ; Yoo, Seung Soo ; Choi, Sunha ; Oh, In-Jae ; Kim, Young-Chul ; Park, Chul-Kyu ; Yoon, Seong Hoon ; Kim, Yun Seong ; Kim, Mi-Hyun ; Lee, Min Ki ; Eom, Jung Seop ; Kim, Soo Han ; Lee, Jeong Eun ; Chung, Chaeuk ; Yeo, Chang Dong ; Lee, Sang Haak ; Lee, Jae Cheol

Citation: TRANSLATIONAL LUNG CANCER RESEARCH, Vol.15(1), 2026-01

Article Number: 13

Journal Title: TRANSLATIONAL LUNG CANCER RESEARCH

ISSN: 2218-6751

Issue Date: 2026-01

Keywords: Non-small cell lung cancer (NSCLC) ; plasma epidermal growth factor receptor T790M (plasma EGFR T790M) ; metastatic distribution ; prognosis ; lazertinib

Abstract: Background: Third-generation epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors improve outcomes in EGFR T790M-positive non-small cell lung cancer (NSCLC), but the prognostic value of plasma-detected T790M remains uncertain. We evaluated the clinical significance of baseline plasma T790M in patients treated with lazertinib, accounting for metastatic distribution and coexisting genomic alterations. Methods: In this prospective multicenter cohort, we analyzed 117 patients with EGFR-mutant NSCLC who received lazertinib after T790M confirmation in tissue or plasma. Plasma EGFR mutations were profiled using next-generation sequencing before treatment. Progression-free survival (PFS) and overall survival (OS) were compared by plasma T790M status, metastatic sites, and co-alterations. Results: Of 117 patients, 92 were plasma T790M-positive and 25 were plasma T790M-negative. Plasma T790M positivity was associated with shorter PFS (10.0 vs. 23.0 months, P=0.03) and OS (20.0 months vs. not reached, P=0.006). All patients with liver or adrenal metastases were plasma T790M-positive, and involvement of either site predicted poorer outcomes than in patients without these metastases. Bone metastasis also portended a worse prognosis, irrespective of plasma T790M status. Among co-alterations, EGFR C797S or MYC alterations correlated with shorter PFS. Conclusions: Baseline plasma T790M, interpreted alongside metastatic distribution, provided prognostic information in EGFR-mutant NSCLC treated with lazertinib. Liver and adrenal metastases occurred exclusively in plasma T790M-positive patients and were associated with markedly worse outcomes, consistent with a ctDNA-shedding phenotype. Bone metastasis was an adverse prognostic factor independent of plasma T790M, underscoring the combined prognostic impact of molecular and metastatic features.