NKp30 isoforms and NKp30 ligands are predictive biomarkers of response to imatinib mesylate in metastatic GIST patients

6533b852fe1ef96bd12aad10

RESEARCH PRODUCT

NKp30 isoforms and NKp30 ligands are predictive biomarkers of response to imatinib mesylate in metastatic GIST patients

Serge Leyvraz Katrin S. Reiners Christos Christidis Jean-yves Blay Jonathan M. Pitt Marion Lambert Aurélien Marabelle Frédéric Vély Alexandre Ivagnes Jean-françois Emile Christian Auclair Benedita Rocha Axel Le Cesne Loic Chaigneau Christelle Piperoglou Kariman Chaba Philippe Terrier Eric Vivier Nicolas Isambert Julien Adam Sylvie Rusakiewicz Pierre Validire Bruno Landi Thierry Perniceni Laurence Zitvogel Sarah Jegou Sylvie Bonvalot Michaela Semeraro Sophie Caillat-zucman David Enot Sandrine Aspeslagh Aurélie Perier Christophe Borg Vichnou Poirier-colame Anne Berger Alexander M.m. Eggermont Antoine Toubert Niels Halama Joachim Koch Elke Pogge Von Strandmann Olivier Mir Julien Domont Anne Caignard Jean-michel Coindre

subject

0301 basic medicine medicine.medical_treatment Immunology PDGFRA Targeted therapy 03 medical and health sciences 0302 clinical medicine medicine Immunology and Allergy [ SDV.IMM ] Life Sciences [q-bio]/Immunology neoplasms Original Research Tumor microenvironment GiST business.industry Cancer medicine.disease digestive system diseases 3. Good health Immunosurveillance 030104 developmental biology Imatinib mesylate Oncology 030220 oncology & carcinogenesis Immunology Cancer research [SDV.IMM]Life Sciences [q-bio]/Immunology business Tyrosine kinase

description

International audience; Despite effective targeted therapy acting on KIT and PDGFRA tyrosine kinases, gastrointestinal stromal tumors (GIST) escape treatment by acquiring mutations conveying resistance to imatinib mesylate (IM). Following the identification of NKp30-based immunosurveillance of GIST and the off-target effects of IM on NK cell functions, we investigated the predictive value of NKp30 isoforms and NKp30 soluble ligands in blood for the clinical response to IM. The relative expression and the proportions of NKp30 isoforms markedly impacted both event-free and overall survival, in two independent cohorts of metastatic GIST. Phenotypes based on disbalanced NKp30B/NKp30C ratio (Delta BClow) and low expression levels of NKp30A were identified in one third of patients with dismal prognosis across molecular subtypes. This Delta BClow blood phenotype was associated with a pro-inflammatory and immunosuppressive tumor microenvironment. In addition, detectable levels of the NKp30 ligand sB7-H6 predicted a worse prognosis in metastatic GIST. Soluble BAG6, an alternate ligand for NKp30 was associated with low NKp30 transcription and had additional predictive value in GIST patients with high NKp30 expression. Such GIST microenvironments could be rescued by therapy based on rIFN-alpha and anti-TRAIL mAb which reinstated innate immunity.

year	journal	country	edition	language
2016-04-25

10.1080/2162402x.2015.1137418 https://hal-amu.archives-ouvertes.fr/hal-01765085