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IgA EGFR 抗体在体内介导肿瘤杀伤。

IgA EGFR antibodies mediate tumour killing in vivo.

机构信息

Immunotherapy Laboratory, Laboratory for Translational Immunology, UMC Utrecht, Utrecht, The Netherlands.

出版信息

EMBO Mol Med. 2013 Aug;5(8):1213-26. doi: 10.1002/emmm.201201929.

Abstract

Currently all approved anti-cancer therapeutic monoclonal antibodies (mAbs) are of the IgG isotype, which rely on Fcgamma receptors (FcγRs) to recruit cellular effector functions. In vitro studies showed that targeting of FcαRI (CD89) by bispecific antibodies (bsAbs) or recombinant IgA resulted in more effective elimination of tumour cells by myeloid effector cells than targeting of FcγR. Here we studied the in vivo anti-tumour activity of IgA EGFR antibodies generated using the variable sequences of the chimeric EGFR antibody cetuximab. Using FcαRI transgenic mice, we demonstrated significant in vivo anti-tumour activity of IgA2 EGFR against A431 cells in peritoneal and lung xenograft models, as well as against B16F10-EGFR cells in a lung metastasis model in immunocompetent mice. IgA2 EGFR was more effective than cetuximab in a short-term syngeneic peritoneal model using EGFR-transfected Ba/F3 target cells. The in vivo cytotoxic activity of IgA2 EGFR was mediated by macrophages and was significantly decreased in the absence of FcαRI. These results support the potential of targeting FcαRI for effective antibody therapy of cancer.

摘要

目前所有批准的抗癌治疗性单克隆抗体(mAbs)都是 IgG 同种型,它依赖于 Fcγ 受体(FcγRs)招募细胞效应功能。体外研究表明,双特异性抗体(bsAbs)或重组 IgA 靶向 FcαRI(CD89)比靶向 FcγR 更有效地消除髓样效应细胞中的肿瘤细胞。在这里,我们研究了使用嵌合 EGFR 抗体西妥昔单抗的可变序列产生的 IgA EGFR 抗体的体内抗肿瘤活性。使用 FcαRI 转基因小鼠,我们证明了 IgA2 EGFR 在腹膜和肺异种移植模型中对 A431 细胞,以及在免疫活性小鼠的肺转移模型中对 B16F10-EGFR 细胞具有显著的体内抗肿瘤活性。在使用 EGFR 转染的 Ba/F3 靶细胞的短期同种异体腹膜模型中,IgA2 EGFR 比西妥昔单抗更有效。IgA2 EGFR 的体内细胞毒性活性由巨噬细胞介导,在缺乏 FcαRI 的情况下显著降低。这些结果支持靶向 FcαRI 用于癌症有效抗体治疗的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d718/3944462/cdee7a0a9d5b/emmm0005-1213-f1.jpg

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