Enhanced Vulnerability of LKB1-Deficient NSCLC to Disruption of ATP Pools and Redox Homeostasis by 8-Cl-Ado

Overview

Journal Mol Cancer Res

Specialty Cell Biology

Date 2021 Oct 16

PMID 34654720

Citations 3

Authors

Ana Galan-Cobo

Christine M Stellrecht

Emrullah Yilmaz

Chao Yang

Yu Qian

Xiao Qu

Ishita Akhter

Mary L Ayres

Youhong Fan

Pan Tong

Lixia Diao

Jie Ding

Uma Giri

Jayanthi Gudikote

Monique Nilsson

William G Wierda

Jing Wang

Ferdinandos Skoulidis

John D Minna

Varsha Gandhi

John V Heymach

Affiliations

Soon will be listed here.

Abstract

Loss-of-function somatic mutations of , a tumor suppressor gene encoding LKB1 that contributes to the altered metabolic phenotype of cancer cells, is the second most common event in lung adenocarcinomas and often co-occurs with activating mutations. Tumor cells lacking LKB1 display an aggressive phenotype, with uncontrolled cell growth and higher energetic and redox stress due to its failure to balance ATP and NADPH levels in response to cellular stimulus. The identification of effective therapeutic regimens for patients with LKB1-deficient non-small cell lung cancer (NSCLC) remains a major clinical need. Here, we report that LKB1-deficient NSCLC tumor cells displayed reduced basal levels of ATP and to a lesser extent other nucleotides, and markedly enhanced sensitivity to 8-Cl-adenosine (8-Cl-Ado), an energy-depleting nucleoside analog. Treatment with 8-Cl-Ado depleted intracellular ATP levels, raised redox stress, and induced cell death leading to a compensatory suppression of mTOR signaling in LKB1-intact, but not LKB1-deficient, cells. Proteomic analysis revealed that the MAPK/MEK/ERK and PI3K/AKT pathways were activated in response to 8-Cl-Ado treatment and targeting these pathways enhanced the antitumor efficacy of 8-Cl-Ado. IMPLICATIONS: Together, our findings demonstrate that LKB1-deficient tumor cells are selectively sensitive to 8-Cl-Ado and suggest that therapeutic approaches targeting vulnerable energy stores combined with signaling pathway inhibitors merit further investigation for this patient population.

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