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抗体的分子重定向将针对溶瘤病毒的免疫防御转化为癌症免疫疗法。

Molecular retargeting of antibodies converts immune defense against oncolytic viruses into cancer immunotherapy.

机构信息

Department of Gastroenterology, Hepatology and Endocrinology, Medical School Hannover, Carl Neuberg Str. 1, 30625, Hannover, Germany.

Institute for Clinical Biochemistry, Medical School Hannover, Carl Neuberg Str. 1, 30625, Hannover, Germany.

出版信息

Nat Commun. 2019 Jul 19;10(1):3236. doi: 10.1038/s41467-019-11137-5.

Abstract

Virus-neutralizing antibodies are a severe obstacle in oncolytic virotherapy. Here, we present a strategy to convert this unfavorable immune response into an anticancer immunotherapy via molecular retargeting. Application of a bifunctional adapter harboring a tumor-specific ligand and the adenovirus hexon domain DE1 for engaging antiadenoviral antibodies, attenuates tumor growth and prolongs survival in adenovirus-immunized mice. The therapeutic benefit achieved by tumor retargeting of antiviral antibodies is largely due to NK cell-mediated triggering of tumor-directed CD8 T-cells. We further demonstrate that antibody-retargeting (Ab-retargeting) is a feasible method to sensitize tumors to PD-1 immune checkpoint blockade. In therapeutic settings, Ab-retargeting greatly improves the outcome of intratumor application of an oncolytic adenovirus and facilitates long-term survival in treated animals when combined with PD-1 checkpoint inhibition. Tumor-directed retargeting of preexisting or virotherapy-induced antiviral antibodies therefore represents a promising strategy to fully exploit the immunotherapeutic potential of oncolytic virotherapy and checkpoint inhibition.

摘要

病毒中和抗体是溶瘤病毒治疗的严重障碍。在这里,我们提出了一种通过分子重定向将这种不利的免疫反应转化为抗癌免疫疗法的策略。应用携带肿瘤特异性配体和腺病毒六邻体域 DE1 的双功能接头来结合抗腺病毒抗体,可减轻肿瘤生长并延长在腺病毒免疫小鼠中的存活时间。通过抗病毒抗体的肿瘤重定向实现的治疗益处主要归因于 NK 细胞介导的肿瘤定向 CD8 T 细胞的触发。我们进一步证明,抗体重定向(Ab 重定向)是一种使肿瘤对 PD-1 免疫检查点阻断敏感的可行方法。在治疗环境中,Ab 重定向极大地改善了肿瘤内应用溶瘤腺病毒的效果,并在与 PD-1 检查点抑制联合使用时促进了治疗动物的长期存活。因此,针对预先存在的或病毒治疗诱导的抗病毒抗体的肿瘤定向重定向代表了充分利用溶瘤病毒治疗和检查点抑制的免疫治疗潜力的有前途的策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/73a2/6642145/0a27cf7e1bef/41467_2019_11137_Fig1_HTML.jpg

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