Modulation of Lung Cancer Cell Plasticity and Heterogeneity with the Restoration of Cisplatin Sensitivity by Neurotensin Antibody

Overview

Journal Cancer Lett

Specialty Oncology

Date 2018 Dec 25

PMID 30583074

Citations 13

Authors

Zherui Wu

Ludovic Fournel

Nicolas Stadler

Jin Liu

Agnes Boullier

Nadia Hoyeau

Jean Francois Flejou

Veronique Duchatelle

Nouzha Djebrani-Oussedik

Mikael Agopiantz

Evelyne Segal-Bendirdjian

Anne Gompel

Marco Alifano

Olle Melander

Jean Tredaniel

Patricia Forgez

Affiliations

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Abstract

Overall survival of patients with metastatic non-small cell lung cancer (NSCLC) has significantly improved with platinum-based salt treatments and recently with targeted therapies and immunotherapies. However, treatment failure occurs due to acquired or emerging tumor resistance. We developed a monoclonal antibody against the proform of neurotensin (LF-NTS mAb) that alters the homeostasis of tumors overexpressing NTSR1. Neurotensin is frequently overexpressed along with its high affinity receptor (NTSR1) in tumors from epithelial origins. This ligand/receptor complex contributes to the progression of many tumor types by activation of the cellular effects involved in tumor progression (proliferation, survival, migration, and invasion). We demonstrate that LF-NTS mAb operates on the plasticity of tumor cells overexpressing NTSR1 and lowers their aggressiveness. The mAb enables the restoration of platinum-based therapies responsiveness, while also decreasing metastatic processes. Efficacy dosage with long-term treatment showed no obvious adverse events, while demonstrating improvement in the performance status. Our data suggests that LF-NTS mAb is an ideal candidate to be safely added to the conventional standard of care in order to improve its efficacy.

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Ferroptosis as a Potential Cell Death Mechanism Against Cisplatin-Resistant Lung Cancer Cell Line.

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