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边缘区 B 细胞对于同种异体致敏后形成抗供体 IgG 是必需的。

Marginal Zone B Cells Are Necessary for the Formation of Anti-donor IgG After Allogeneic Sensitization.

机构信息

Department of Pathology, Johns Hopkins School of Medicine, Baltimore, MD.

出版信息

Transplantation. 2024 Jun 1;108(6):1357-1367. doi: 10.1097/TP.0000000000004931. Epub 2024 Feb 16.

Abstract

BACKGROUND

The formation of anti-major histocompatibility complex (MHC) antibodies is a significant barrier for many patients awaiting organ transplantation. Patients with preformed anti-MHC antibodies have limited options for suitable donors, and the formation of donor-specific anti-MHC antibodies after transplantation is a harbinger of graft rejection. Despite the recognized importance of anti-MHC antibodies, the mechanisms responsible for the differentiation of B cells after exposure to allogeneic antigens are poorly understood.

METHODS

To evaluate the differentiation of B cells in response to allogeneic antigen, we used a model of H-2 b C57Bl/6 sensitization with H-2 d antigen. We used a class I MHC tetramer-based approach to identify allogeneic B cells and flow cytometric crossmatch to identify allogeneic IgM and IgG.

RESULTS

We found that although the formation of anti-H-2 d IgG was robust, few class-switched B cells and germinal center B cells were formed. Antigen-specific B cells did not express classical memory B-cell markers after sensitization but had an IgM + CD21 + marginal zone B-cell phenotype. The frequency of marginal zone B cells increased after sensitization. Depletion of marginal zone B cells before sensitization or skin grafting resulted in a significant diminution of anti-H-2 d IgG and fewer germinal center B cells. Adoptive transfer experiments revealed that marginal zone B cells more efficiently differentiated into germinal center B cells and anti-donor IgG-producing cells than follicular B cells.

CONCLUSIONS

These results demonstrate an important role for marginal zone B cells as a reservoir of alloreactive B cells that are activated by allogeneic antigens.

摘要

背景

抗主要组织相容性复合体(MHC)抗体的形成是许多等待器官移植的患者面临的重大障碍。预先存在抗 MHC 抗体的患者可供选择的合适供体有限,而移植后形成的供体特异性抗 MHC 抗体是移植物排斥的先兆。尽管抗 MHC 抗体的重要性已得到公认,但对于接触同种异体抗原后 B 细胞分化的机制仍知之甚少。

方法

为了评估 B 细胞对同种异体抗原的反应分化,我们使用了 H-2 b C57Bl/6 致敏与 H-2 d 抗原的模型。我们使用基于 I 类 MHC 四聚体的方法来鉴定同种异体 B 细胞,并使用流式细胞术交叉匹配来鉴定同种异体 IgM 和 IgG。

结果

我们发现,尽管抗 H-2 d IgG 的形成很强烈,但形成的类别转换 B 细胞和生发中心 B 细胞很少。抗原特异性 B 细胞在致敏后不表达经典的记忆 B 细胞标记物,但具有 IgM + CD21 + 边缘区 B 细胞表型。致敏后边缘区 B 细胞的频率增加。致敏前或皮肤移植时耗尽边缘区 B 细胞会导致抗 H-2 d IgG 显著减少,生发中心 B 细胞减少。过继转移实验表明,边缘区 B 细胞比滤泡 B 细胞更有效地分化为生发中心 B 细胞和产生抗供体 IgG 的细胞。

结论

这些结果表明边缘区 B 细胞作为对同种异体抗原具有反应性的 B 细胞的储备库,在其中发挥重要作用。

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