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工程化抗体促进中性粒细胞依赖控制结核分枝杆菌。

Fc-engineered antibodies promote neutrophil-dependent control of Mycobacterium tuberculosis.

机构信息

Ragon Institute of MGH, MIT and Harvard, Cambridge, MA, USA.

Department of Immunology and Infectious Diseases, Harvard T. H. Chan School of Public Health, Boston, MA, USA.

出版信息

Nat Microbiol. 2024 Sep;9(9):2369-2382. doi: 10.1038/s41564-024-01777-9. Epub 2024 Aug 22.

Abstract

Mounting evidence indicates that antibodies can contribute towards control of tuberculosis (TB). However, the underlying mechanisms of humoral immune protection and whether antibodies can be exploited in therapeutic strategies to combat TB are relatively understudied. Here we engineered the receptor-binding Fc (fragment crystallizable) region of an antibody recognizing the Mycobacterium tuberculosis (Mtb) capsule, to define antibody Fc-mediated mechanism(s) of Mtb restriction. We generated 52 Fc variants that either promote or inhibit specific antibody effector functions, rationally building antibodies with enhanced capacity to promote Mtb restriction in a human whole-blood model of infection. While there is likely no singular Fc profile that universally drives control of Mtb, here we found that several Fc-engineered antibodies drove Mtb restriction in a neutrophil-dependent manner. Single-cell RNA sequencing analysis showed that a restrictive Fc-engineered antibody promoted neutrophil survival and expression of cell-intrinsic antimicrobial programs. These data show the potential of Fc-engineered antibodies as therapeutics able to harness the protective functions of neutrophils to promote control of TB.

摘要

越来越多的证据表明,抗体可以有助于控制结核病(TB)。然而,体液免疫保护的潜在机制以及抗体是否可以被用于治疗结核病的策略来对抗 TB 相对研究较少。在这里,我们对识别结核分枝杆菌(Mtb)荚膜的抗体的受体结合 Fc(片段结晶)区域进行了工程改造,以确定抗体 Fc 介导的 Mtb 限制机制。我们生成了 52 种 Fc 变体,这些变体可以促进或抑制特定的抗体效应功能,从而合理地构建出具有增强能力的抗体,以在人类感染全血模型中促进 Mtb 限制。虽然可能没有单一的 Fc 特征能够普遍驱动 Mtb 的控制,但在这里我们发现,几种 Fc 工程化的抗体以中性粒细胞依赖的方式驱动 Mtb 限制。单细胞 RNA 测序分析表明,一种限制性 Fc 工程化抗体促进了中性粒细胞的存活和细胞内固有抗菌程序的表达。这些数据表明,Fc 工程化抗体具有作为治疗剂的潜力,能够利用中性粒细胞的保护功能来促进结核病的控制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2c39/11371646/857487cfcf3e/41564_2024_1777_Fig1_HTML.jpg

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