癌症研究
免疫系统
免疫检查点
嵌合抗原受体
主旨
间质细胞
医学
免疫疗法
免疫学
作者
Alexandre de Nonneville,Pascal Finetti,Maelle Picard,Audrey Monneur,Maria A. Pantaleo,Annalisa Astolfi,Jerzy Ostrowski,Daniel Birnbaum,Émilie Mamessier,François Bertucci
出处
期刊:Cancers
[Multidisciplinary Digital Publishing Institute]
日期:2022-03-03
卷期号:14 (5): 1306-1306
被引量:5
标识
DOI:10.3390/cancers14051306
摘要
The treatment of gastrointestinal stromal tumors (GIST) must be improved through the development of more reliable prognostic factors and of therapies able to overcome imatinib resistance. The immune system represents an attractive tool. CSPG4, a cell surface proteoglycan, emerged as a potential therapeutic target for immune therapy in different cancers, including cell therapy based on CSPG4-specific chimeric antigen receptor (CAR)-redirected cytokine-induced killer lymphocytes (CSPG4-CAR.CIKs) in sarcomas. CSPG4 expression has never been studied in GIST. We analyzed CSPG4 mRNA expression data of 309 clinical GIST samples profiled using DNA microarrays and searched for correlations with clinicopathological and immune features. CSPG4 expression, higher in tumors than normal digestive tissues, was heterogeneous across tumors. High expression was associated with AFIP low-risk, gastric site, and localized stage, and independently with longer postoperative disease-free survival (DFS) in localized stage. The correlations between CSPG4 expression and immune signatures highlighted a higher anti-tumor immune response in "CSPG4-high" tumors, relying on both the adaptive and innate immune system, in which the boost of NK cells by CSPG4-CAR.CIKs might be instrumental, eventually combined with immune checkpoint inhibitors. In conclusion, high CSPG4 expression in GIST is associated with better DFS and offers an immune environment favorable to a vulnerability to CAR.CIKs.
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