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


ABSTRACT: 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 (?BClow) and low expression levels of NKp30A were identified in one third of patients with dismal prognosis across molecular subtypes. This ?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-? and anti-TRAIL mAb which reinstated innate immunity.

SUBMITTER: Rusakiewicz S 

PROVIDER: S-EPMC5283614 | biostudies-literature | 2017

REPOSITORIES: biostudies-literature

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

Rusakiewicz Sylvie S   Perier Aurélie A   Semeraro Michaela M   Pitt Jonathan M JM   Pogge von Strandmann Elke E   Reiners Katrin S KS   Aspeslagh Sandrine S   Pipéroglou Christelle C   Vély Frédéric F   Ivagnes Alexandre A   Jegou Sarah S   Halama Niels N   Chaigneau Loic L   Validire Pierre P   Christidis Christos C   Perniceni Thierry T   Landi Bruno B   Berger Anne A   Isambert Nicolas N   Domont Julien J   Bonvalot Sylvie S   Terrier Philippe P   Adam Julien J   Coindre Jean-Michel JM   Emile Jean-François JF   Poirier-Colame Vichnou V   Chaba Kariman K   Rocha Benedita B   Caignard Anne A   Toubert Antoine A   Enot David D   Koch Joachim J   Marabelle Aurélien A   Lambert Marion M   Caillat-Zucman Sophie S   Leyvraz Serge S   Auclair Christian C   Vivier Eric E   Eggermont Alexander A   Borg Christophe C   Blay Jean-Yves JY   Le Cesne Axel A   Mir Olivier O   Zitvogel Laurence L  

Oncoimmunology 20160425 1


Despite effective targeted therapy acting on <i>KIT</i> and <i>PDGFRA</i> 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  ...[more]

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