通过 SIRPα 变体的分子工程提高巨噬细胞对治疗性抗体的反应。
Improving macrophage responses to therapeutic antibodies by molecular engineering of SIRPα variants.
机构信息
Institute for Stem Cell Biology and Regenerative Medicine; Stanford University School of Medicine; Stanford, CA USA ; Ludwig Center for Cancer Stem Cell Research and Medicine; Stanford University School of Medicine; Stanford, CA USA ; Stanford Cancer Institute; Stanford University School of Medicine; Stanford, CA USA.
出版信息
Oncoimmunology. 2013 Sep 1;2(9):e25773. doi: 10.4161/onci.25773. Epub 2013 Jul 29.
CD47 transduces inhibitory signals through signal-regulatory protein α (SIRPα), a plasma membrane receptor expressed by macrophages. Many cancers upregulate CD47 to evade immunosurveillance. We have recently engineered SIRPα variants that potently antagonize CD47 for use as anticancer immunotherapeutics. These high-affinity SIRPα variants synergize with antineoplastic antibodies by lowering the threshold for macrophage-mediated destruction of malignant cells.
CD47 通过信号调节蛋白α(SIRPα)转导抑制信号,SIRPα 是一种表达于巨噬细胞的质膜受体。许多癌症通过上调 CD47 来逃避免疫监视。我们最近设计了强效拮抗 CD47 的 SIRPα 变体,可将其用作抗癌免疫疗法。这些高亲和力的 SIRPα 变体通过降低巨噬细胞介导的恶性细胞破坏的阈值与抗肿瘤抗体协同作用。
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