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Merck
  • Synergy between the ectoenzymes CD39 and CD73 contributes to adenosinergic immunosuppression in human malignant gliomas.

Synergy between the ectoenzymes CD39 and CD73 contributes to adenosinergic immunosuppression in human malignant gliomas.

Neuro-oncology (2013-06-06)
Shuo Xu, Qian-Qian Shao, Jin-Tang Sun, Ning Yang, Qi Xie, Dong-Hai Wang, Qi-Bing Huang, Bin Huang, Xin-Yu Wang, Xin-Gang Li, Xun Qu
摘要

The importance of ectoenzymes CD39 and CD73 in mediating adenosinergic immunosuppression has been recognized, but their roles in human malignant glioma-associated immunosuppression remain largely unknown. In this study, the ectoenzyme characteristics of malignant glioma cells and infiltrating CD4(+) T lymphocytes isolated from newly diagnosed malignant glioma patients were investigated. The ectoenzyme activities of both cell populations were determined by nucleotide hydrolysis assay. The immunosuppressive property of the CD39-CD73 synergic effect was evaluated via responder T-cell proliferation assay. We observed that CD39(-)CD73(+) glioma cells and infiltrating CD4(+)CD39(high)CD73(low) T lymphocytes exhibited 2 distinct but complementary ectoenzyme phenotypes, which were further verified by enzyme activity assay. The nucleotide hydrolysis cascade was incomplete unless CD39 derived from T lymphocytes and CD73 collaborated synergistically. We demonstrated that increased suppression of responder CD4(+) T-cell proliferation suppression was induced by CD4(+)CD39(+) T cells in the presence of CD73(+) glioma cells, which could be alleviated by the CD39 inhibitor ARL67156, the CD73 inhibitor APCP, or the adenosine receptor A2aR antagonist SCH58261. In addition, survival analysis suggested that CD73 downregulation was a positive prognostic factor related to the extended disease-free survival of glioblastoma patients. Our data indicate that glioma-derived CD73 contributes to local adenosine-mediated immunosuppression in synergy with CD39 from infiltrating CD4(+)CD39(+) T lymphocytes, which could become a potential therapeutic target for treatment of malignant glioma and other immunosuppressive diseases.

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Sigma-Aldrich
三磷酸腺苷双磷酸酶 来源于马铃薯, ATPase ≥200 units/mg protein, lyophilized powder
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三磷酸腺苷双磷酸酶 来源于马铃薯, ATPase ≥200 units/mg protein, lyophilized powder
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三磷酸腺苷双磷酸酶 来源于马铃薯, ATPase ≥3.0 units/mg protein, lyophilized powder
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三磷酸腺苷双磷酸酶 来源于马铃薯, ATPase ≥60 units/mg protein, lyophilized powder (partially purified)
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马铃薯来源腺苷三磷酸双磷酶, recombinant, expressed in Pichia pastoris, ATPase ≥1000 units/mg protein, lyophilized powder
Sigma-Aldrich
三磷酸腺苷双磷酸酶 来源于马铃薯, High Activity, ATPase ≥600 units/mg protein, lyophilized powder