An IGHG1 variant exhibits polarized prevalence and confers enhanced IgG1 antibody responses against life-threatening organisms

Wenbo Sun; Tingyu Yang; Fengming Sun; Panhong Liu; Ji Gao; Xianmei Lan; Wei Xu; Yuhong Pang; Tong Li; Cuifeng Li; Qingtai Liang; Haoze Chen; Xiaohang Liu; Wenting Tan; Huanhuan Zhu; Fang Wang; Fanjun Cheng; Weiwei Zhai; Han Na Kim; Jingren Zhang; Linqi Zhang; Lu Lu; Qiaoran Xi; Guohong Deng; Yanyi Huang; Xin Jin; Xiangjun Chen; Wanli Liu

doi:10.1038/s41590-024-01944-4

An IGHG1 variant exhibits polarized prevalence and confers enhanced IgG1 antibody responses against life-threatening organisms

Wenbo Sun
, Tingyu Yang
, Fengming Sun
, Panhong Liu
, Ji Gao
, Xianmei Lan
, Wei Xu
, Yuhong Pang
, Tong Li
, Cuifeng Li
, Qingtai Liang
, Haoze Chen
, Xiaohang Liu
, Wenting Tan
, Huanhuan Zhu
, Fang Wang
, Fanjun Cheng
, Weiwei Zhai
, Han Na Kim
, Jingren Zhang

Linqi Zhang, Lu Lu, Qiaoran Xi, Guohong Deng, Yanyi Huang, Xin Jin, Xiangjun Chen, Wanli Liu

Samsung Advanced Institute for Health Sciences and Technology (SAIHST)

Research output: Contribution to journal › Article › peer-review

7 Scopus citations

Abstract

Evolutionary pressures sculpt population genetics, whereas immune adaptation fortifies humans against life-threatening organisms. How the evolution of selective genetic variation in adaptive immune receptors orchestrates the adaptation of human populations to contextual perturbations remains elusive. Here, we show that the G396R coding variant within the human immunoglobulin G1 (IgG1) heavy chain presents a concentrated prevalence in Southeast Asian populations. We uncovered a 190-kb genomic linkage disequilibrium block peaked in close proximity to this variant, suggestive of potential Darwinian selection. This variant confers heightened immune resilience against various pathogens and viper toxins in mice. Mechanistic studies involving severe acute respiratory syndrome coronavirus 2 infection and vaccinated individuals reveal that this variant enhances pathogen-specific IgG1⁺ memory B cell activation and antibody production. This G396R variant may have arisen on a Neanderthal haplotype background. These findings underscore the importance of an IGHG1 variant in reinforcing IgG1 antibody responses against life-threatening organisms, unraveling the intricate interplay between human evolution and immune adaptation.

Original language	English
Pages (from-to)	1809-1819
Number of pages	11
Journal	Nature Immunology
Volume	25
Issue number	10
DOIs	https://doi.org/10.1038/s41590-024-01944-4
State	Published - Oct 2024

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10.1038/s41590-024-01944-4

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Sun, W., Yang, T., Sun, F., Liu, P., Gao, J., Lan, X., Xu, W., Pang, Y., Li, T., Li, C., Liang, Q., Chen, H., Liu, X., Tan, W., Zhu, H., Wang, F., Cheng, F., Zhai, W., Kim, H. N., ... Liu, W. (2024). An IGHG1 variant exhibits polarized prevalence and confers enhanced IgG1 antibody responses against life-threatening organisms. Nature Immunology, 25(10), 1809-1819. https://doi.org/10.1038/s41590-024-01944-4

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title = "An IGHG1 variant exhibits polarized prevalence and confers enhanced IgG1 antibody responses against life-threatening organisms",

abstract = "Evolutionary pressures sculpt population genetics, whereas immune adaptation fortifies humans against life-threatening organisms. How the evolution of selective genetic variation in adaptive immune receptors orchestrates the adaptation of human populations to contextual perturbations remains elusive. Here, we show that the G396R coding variant within the human immunoglobulin G1 (IgG1) heavy chain presents a concentrated prevalence in Southeast Asian populations. We uncovered a 190-kb genomic linkage disequilibrium block peaked in close proximity to this variant, suggestive of potential Darwinian selection. This variant confers heightened immune resilience against various pathogens and viper toxins in mice. Mechanistic studies involving severe acute respiratory syndrome coronavirus 2 infection and vaccinated individuals reveal that this variant enhances pathogen-specific IgG1+ memory B cell activation and antibody production. This G396R variant may have arisen on a Neanderthal haplotype background. These findings underscore the importance of an IGHG1 variant in reinforcing IgG1 antibody responses against life-threatening organisms, unraveling the intricate interplay between human evolution and immune adaptation.",

author = "Wenbo Sun and Tingyu Yang and Fengming Sun and Panhong Liu and Ji Gao and Xianmei Lan and Wei Xu and Yuhong Pang and Tong Li and Cuifeng Li and Qingtai Liang and Haoze Chen and Xiaohang Liu and Wenting Tan and Huanhuan Zhu and Fang Wang and Fanjun Cheng and Weiwei Zhai and Kim, \{Han Na\} and Jingren Zhang and Linqi Zhang and Lu Lu and Qiaoran Xi and Guohong Deng and Yanyi Huang and Xin Jin and Xiangjun Chen and Wanli Liu",

note = "Publisher Copyright: {\textcopyright} The Author(s), under exclusive licence to Springer Nature America, Inc. 2024.",

year = "2024",

month = oct,

doi = "10.1038/s41590-024-01944-4",

language = "English",

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Sun, W, Yang, T, Sun, F, Liu, P, Gao, J, Lan, X, Xu, W, Pang, Y, Li, T, Li, C, Liang, Q, Chen, H, Liu, X, Tan, W, Zhu, H, Wang, F, Cheng, F, Zhai, W, Kim, HN, Zhang, J, Zhang, L, Lu, L, Xi, Q, Deng, G, Huang, Y, Jin, X, Chen, X & Liu, W 2024, 'An IGHG1 variant exhibits polarized prevalence and confers enhanced IgG1 antibody responses against life-threatening organisms', Nature Immunology, vol. 25, no. 10, pp. 1809-1819. https://doi.org/10.1038/s41590-024-01944-4

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T1 - An IGHG1 variant exhibits polarized prevalence and confers enhanced IgG1 antibody responses against life-threatening organisms

AU - Sun, Wenbo

AU - Yang, Tingyu

AU - Sun, Fengming

AU - Liu, Panhong

AU - Gao, Ji

AU - Lan, Xianmei

AU - Xu, Wei

AU - Pang, Yuhong

AU - Li, Tong

AU - Li, Cuifeng

AU - Liang, Qingtai

AU - Chen, Haoze

AU - Liu, Xiaohang

AU - Tan, Wenting

AU - Zhu, Huanhuan

AU - Wang, Fang

AU - Cheng, Fanjun

AU - Zhai, Weiwei

AU - Kim, Han Na

AU - Zhang, Jingren

AU - Zhang, Linqi

AU - Lu, Lu

AU - Xi, Qiaoran

AU - Deng, Guohong

AU - Huang, Yanyi

AU - Jin, Xin

AU - Chen, Xiangjun

AU - Liu, Wanli

PY - 2024/10

Y1 - 2024/10

N2 - Evolutionary pressures sculpt population genetics, whereas immune adaptation fortifies humans against life-threatening organisms. How the evolution of selective genetic variation in adaptive immune receptors orchestrates the adaptation of human populations to contextual perturbations remains elusive. Here, we show that the G396R coding variant within the human immunoglobulin G1 (IgG1) heavy chain presents a concentrated prevalence in Southeast Asian populations. We uncovered a 190-kb genomic linkage disequilibrium block peaked in close proximity to this variant, suggestive of potential Darwinian selection. This variant confers heightened immune resilience against various pathogens and viper toxins in mice. Mechanistic studies involving severe acute respiratory syndrome coronavirus 2 infection and vaccinated individuals reveal that this variant enhances pathogen-specific IgG1+ memory B cell activation and antibody production. This G396R variant may have arisen on a Neanderthal haplotype background. These findings underscore the importance of an IGHG1 variant in reinforcing IgG1 antibody responses against life-threatening organisms, unraveling the intricate interplay between human evolution and immune adaptation.

AB - Evolutionary pressures sculpt population genetics, whereas immune adaptation fortifies humans against life-threatening organisms. How the evolution of selective genetic variation in adaptive immune receptors orchestrates the adaptation of human populations to contextual perturbations remains elusive. Here, we show that the G396R coding variant within the human immunoglobulin G1 (IgG1) heavy chain presents a concentrated prevalence in Southeast Asian populations. We uncovered a 190-kb genomic linkage disequilibrium block peaked in close proximity to this variant, suggestive of potential Darwinian selection. This variant confers heightened immune resilience against various pathogens and viper toxins in mice. Mechanistic studies involving severe acute respiratory syndrome coronavirus 2 infection and vaccinated individuals reveal that this variant enhances pathogen-specific IgG1+ memory B cell activation and antibody production. This G396R variant may have arisen on a Neanderthal haplotype background. These findings underscore the importance of an IGHG1 variant in reinforcing IgG1 antibody responses against life-threatening organisms, unraveling the intricate interplay between human evolution and immune adaptation.

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AN - SCOPUS:85203505692

SN - 1529-2908

VL - 25

SP - 1809

EP - 1819

JO - Nature Immunology

JF - Nature Immunology

IS - 10

ER -

An IGHG1 variant exhibits polarized prevalence and confers enhanced IgG1 antibody responses against life-threatening organisms

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