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Unlocking antitumor immunity with adenosine receptorblockers 被引量:1
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作者 Victoria A.Remley Joel Linden +1 位作者 Todd W.Bauer Julien Dimastromatteo 《Cancer Drug Resistance》 CAS 2023年第4期748-767,共20页
Tumors survive by creating a tumor microenvironment(TME)that suppresses antitumor immunity.The TME suppresses the immune system by limiting antigen presentation,inhibiting lymphocyte and natural killer(NK)cell activat... Tumors survive by creating a tumor microenvironment(TME)that suppresses antitumor immunity.The TME suppresses the immune system by limiting antigen presentation,inhibiting lymphocyte and natural killer(NK)cell activation,and facilitating T cell exhaustion.Checkpoint inhibitors like anti-PD-1 and anti-CTLA4 are immunostimulatory antibodies,and their blockade extends the survival of some but not all cancer patients.Extracellular adenosine triphosphate(ATP)is abundant in inflamed tumors,and its metabolite,adenosine(ADO),is a driver of immunosuppression mediated by adenosine A2A receptors(A2AR)and adenosine A2B receptors(A2BR)found on tumor-associated lymphoid and myeloid cells.This review will focus on adenosine as a key checkpoint inhibitor-like immunosuppressive player in the TME and how reducing adenosine production or blocking A2AR and A2BR enhances antitumor immunity. 展开更多
关键词 IMMUNOTHERAPY adenosine adenosine receptors adenosine A2A receptors(A2AR) adenosine a2b receptors(a2bR) tumor cells immune cells tumor microenvironment
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