Modeling Clinical Responses to Targeted Therapies by Patient-Derived Organoids of Advanced Lung Adenocarcinoma

Seok‐Young Kim; Sang-Min Kim; Su-Min Lim; Ji Yeon Lee; Su‐Jin Choi; San‐Duk Yang; Mi Ran Yun; Chang Gon Kim; Seo Rin Gu; Chaewon Park; A‐Young Park; Sun Min Lim; Seong Gu Heo; Hyunki Kim; Byoung Chul Cho

doi:10.1158/1078-0432.ccr-20-5026

Modeling Clinical Responses to Targeted Therapies by Patient-Derived Organoids of Advanced Lung Adenocarcinoma

Seok‐Young Kim(Yonsei University), Sang-Min Kim(Yonsei University), Su-Min Lim(Biocon (Switzerland)), Ji Yeon Lee(Biocon (Switzerland)), Su‐Jin Choi(Yonsei University), San‐Duk Yang(Yonsei University), Mi Ran Yun(Yonsei University), Chang Gon Kim(Yonsei University), Seo Rin Gu(Biocon (Switzerland)), Chaewon Park(Yonsei University), A‐Young Park(Yonsei University), Sun Min Lim(Biocon (Switzerland)), Seong Gu Heo(Yonsei University), Hyunki Kim(Yonsei University), Byoung Chul Cho(Yonsei University)

Clinical Cancer Research

June 3, 2021

10.1158/1078-0432.ccr-20-5026

Cited by 151Open Access

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Abstract

Abstract Purpose: Patient-derived organoids (PDO) of lung cancer has been recently introduced, reflecting the genomic landscape of lung cancer. However, clinical relevance of advanced lung adenocarcinoma organoids remains unknown. Here, we examined the ability of PDOs to predict clinical responses to targeted therapies in individual patients and to identify effective anticancer therapies for novel molecular targets. Experimental Design: Eighty-four organoids were established from patients with advanced lung adenocarcinoma. Formalin-fixed, paraffin-embedded tumor specimens from corresponding patients were analyzed by whole-exome sequencing (n = 12). Organoids were analyzed by whole-exome sequencing (n = 61) and RNA sequencing (n = 55). Responses to mono or combination targeted therapies were examined in organoids and organoid-derived xenografts. Results: PDOs largely retained somatic alterations including driver mutations of matching patient tumors. PDOs were able to recapitulate progression-free survival and objective responses of patients with non–small cell lung cancer receiving clinically approved tyrosine kinase inhibitors. PDOs recapitulated activity of therapeutic strategies under clinical investigation. YUO-071 harboring an EGFR exon 19 deletion and a BRAF G464A mutation and the matching patient responded to dabrafenib/trametinib combination therapy. YUO-004 and YUO-050 harboring an EGFR L747P mutation was sensitive to afatinib, consistent with the response in the matching patient of YUO-050. Furthermore, we utilized organoids to identify effective therapies for novel molecular targets by demonstrating the efficacy of poziotinib against ERBB2 exon 20 insertions and pralsetinib against RET fusions. Conclusions: We demonstrated translational relevance of PDOs in advanced lung adenocarcinoma. PDOs are an important diagnostic tool, which can assist clinical decision making and accelerate development of therapeutic strategies.

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