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性别、T 细胞与微生物组在小鼠天然 ABO 抗体产生中的作用。

Sex, T Cells, and the Microbiome in Natural ABO Antibody Production in Mice.

机构信息

Department of Medical Microbiology and Immunology, University of Alberta, Edmonton, AB, Canada.

Alberta Transplant Institute and Canadian Donation and Transplantation Research Program, Edmonton, AB, Canada.

出版信息

Transplantation. 2023 Nov 1;107(11):2353-2363. doi: 10.1097/TP.0000000000004658. Epub 2023 Jun 8.

Abstract

BACKGROUND

"Natural" ABO antibodies (Abs) are produced without known exposure to A/B carbohydrate antigens, posing significant risks for hyperacute rejection during ABO-incompatible transplantation. We investigated anti-A "natural" ABO antibodies versus intentionally induced Abs with regard to the need for T-cell help, the impact of sex, and stimulation by the microbiome.

METHODS

Anti-A was measured by hemagglutination assay of sera from untreated C57BL/6 wild-type (WT) or T cell-deficient mice of both sexes. Human ABO-A reagent blood cell membranes were injected intraperitoneally to induce anti-A Abs. The gut microbiome was eliminated by maintenance of mice in germ-free housing.

RESULTS

Compared with WT mice, CD4 + T-cell knockout (KO), major histocompability complex-II KO, and αβ/γδ T-cell receptor KO mice produced much higher levels of anti-A nAbs; females produced dramatically more anti-A nAbs than males, rising substantially with puberty. Sensitization with human ABO-A reagent blood cell membranes did not induce additional anti-A in KO mice, unlike WT. Sex-matched CD4 + T-cell transfer significantly suppressed anti-A nAbs in KO mice and rendered mice responsive to A-sensitization. Even under germ-free conditions, WT mice of several strains produced anti-A nAbs, with significantly higher anti-A nAbs levels in females than males.

CONCLUSIONS

Anti-A nAbs were produced without T-cell help, without microbiome stimulation, in a sex- and age-dependent manner, suggestive of a role for sex hormones in regulating anti-A nAbs. Although CD4 + T cells were not required for anti-A nAbs, our findings indicate that T cells regulate anti-A nAb production. In contrast to anti-A nAbs, induced anti-A production was T-cell dependent without a sex bias.

摘要

背景

“天然”ABO 抗体(Abs)在没有已知的 A/B 碳水化合物抗原暴露的情况下产生,在 ABO 不相容移植中会导致严重的超急性排斥反应风险。我们研究了抗-A“天然”ABO 抗体与故意诱导的 Abs 之间的关系,包括 T 细胞帮助的必要性、性别影响以及微生物组的刺激作用。

方法

通过未经处理的 C57BL/6 野生型(WT)或两性 T 细胞缺陷型小鼠血清的血凝测定法测量抗-A。将人 ABO-A 试剂血细胞膜腹膜内注射以诱导抗-A Abs。通过将小鼠维持在无菌饲养中消除肠道微生物组。

结果

与 WT 小鼠相比,CD4+T 细胞敲除(KO)、主要组织相容性复合物-II KO 和 αβ/γδ T 细胞受体 KO 小鼠产生的抗-A nAbs 水平更高;雌性产生的抗-A nAbs 明显多于雄性,随着青春期显著增加。与 WT 不同的是,用人类 ABO-A 试剂血细胞膜致敏不会在 KO 小鼠中诱导额外的抗-A。性别匹配的 CD4+T 细胞转移显著抑制 KO 小鼠中的抗-A nAbs,并使小鼠对 A 致敏有反应。即使在无菌条件下,几个品系的 WT 小鼠也会产生抗-A nAbs,雌性的抗-A nAbs 水平明显高于雄性。

结论

抗-A nAbs 在没有 T 细胞帮助、没有微生物组刺激的情况下,以性别和年龄依赖的方式产生,提示性激素在调节抗-A nAbs 中起作用。虽然 CD4+T 细胞不是抗-A nAbs 所必需的,但我们的发现表明 T 细胞调节抗-A nAb 的产生。与抗-A nAbs 不同,诱导的抗-A 产生是 T 细胞依赖性的,没有性别偏见。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c4b2/10593149/4221acfab75a/tpa-107-2353-g001.jpg

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