Development of antibody-dependent cell cytotoxicity function in HIV-1 antibodies

HIV-1抗体中抗体依赖性细胞毒性功能的发展

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作者：Laura E Doepker #,Sonja Danon #,Elias Harkins,Duncan K Ralph,Zak Yaffe,Meghan E Garrett,Amrit Dhar,Cassia Wagner,Megan M Stumpf,Dana Arenz,James A Williams,Walter Jaoko,Kishor Mandaliya,Kelly K Lee,Frederick A Matsen 4th,Julie M Overbaugh

期刊：

Elife

影响因子：

6.400

时间：

2021

起止号：

2021 Jan 11:10:e63444.

doi：

10.7554/eLife.63444

研究方向：

免疫

疾病类型：

艾滋病

细胞类型：

其它细胞

Abstract

A prerequisite for the design of an HIV vaccine that elicits protective antibodies is understanding the developmental pathways that result in desirable antibody features. The development of antibodies that mediate antibody-dependent cellular cytotoxicity (ADCC) is particularly relevant because such antibodies have been associated with HIV protection in humans. We reconstructed the developmental pathways of six human HIV-specific ADCC antibodies using longitudinal antibody sequencing data. Most of the inferred naive antibodies did not mediate detectable ADCC. Gain of antigen binding and ADCC function typically required mutations in complementarity determining regions of one or both chains. Enhancement of ADCC potency often required additional mutations in framework regions. Antigen binding affinity and ADCC activity were correlated, but affinity alone was not sufficient to predict ADCC potency. Thus, elicitation of broadly active ADCC antibodies may require mutations that enable high-affinity antigen recognition along with mutations that optimize factors contributing to functional ADCC activity.

Development of antibody-dependent cell cytotoxicity function in HIV-1 antibodies

HIV-1抗体中抗体依赖性细胞毒性功能的发展

Abstract

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