继发性复发性妊娠失败中父系 HLA 衍生物表位与活产:临床试验的新发现

IF 5.9 4区 医学 Q2 CELL BIOLOGY HLA Pub Date : 2024-10-17 DOI:10.1111/tan.15723
Maria Christine Krog, Emma T. M. Peereboom, Kirsten Geneugelijk, Benedict M. Matern, Astrid Marie Kolte, Ole Bjarne Christiansen, Rudi Steffensen, Henriette Svarre Nielsen, Eric Spierings
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引用次数: 0

摘要

复发性妊娠流产(RPL)是指在妊娠 24 周前发生两次或两次以上的妊娠流产,全世界有 1%-3%的妇女会受到影响。大约 40% 的复发性妊娠流产病例属于继发性复发性妊娠流产(sRPL),即妇女在面临妊娠流产之前已经生育过。RPL 的根本原因尚不清楚,但与免疫相关的因素可能起了一定作用。此前,我们的 RPL 科室曾对有过四次妊娠失败史的 sRPL 妇女进行了一项使用免疫球蛋白(IVIG)的随机对照试验,结果显示 IVIG 治疗的总体效果并不显著。然而,一些证据表明,部分 sRPL 患者可能从中获益。在用于随机对照试验的队列中,我们使用预测的间接可识别 HLA 表位(PIRCHE-II)算法,研究了母体 HLA 二类表位与胎儿 HLA 衍生表位在 sRPL 中的作用。在安慰剂组中,与再次妊娠失败的 sRPL 妇女相比,具有抗 HLA 抗体反应的 sRPL 母亲在活产时的 PIRCHE-II 评分更高。而 IVIG 治疗组则没有观察到这种差异。此外,作为 T 细胞记忆的代表,在未接受治疗的活产夫妇中,两个父系单倍型之间重叠肽的数量较多。这种效应主要是由 II 类衍生肽驱动的。这些结果表明,sRPL 母亲和父亲的特定组合,尤其是那些具有抗 HLA 抗体反应的组合,可能会产生较高的 PIRCHE-II 分数,从而有助于成功活产。了解这些免疫相互作用可为sRPL的个性化诊断和治疗策略提供启示。
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Paternal HLA-Derived Epitopes and Live Birth in Secondary Recurrent Pregnancy Loss: New Insights From a Clinical Trial

Recurrent pregnancy loss (RPL), defined as two or more pregnancy losses before the 24th week of gestation, affects 1%–3% of women worldwide. Approximately, 40% of RPL cases are secondary RPL (sRPL), where women have given birth before facing pregnancy losses. The underlying causes of RPL remain unclear, but immune-related factors may play a role. Previously, a randomised controlled trial using immunoglobulin (IVIG) in sRPL women with a history of four pregnancy losses performed in our RPL unit did not show significant effects of IVIG treatment overall. Yet, some evidence suggests potential benefits for a subset of sRPL patients. In the cohort used for the randomised controlled trial, we examined the role of maternal HLA class II-presented fetal HLA-derived epitopes in sRPL using the predicted indirectly recognisable HLA epitopes (PIRCHE-II) algorithm. In the placebo group, sRPL mothers with an anti-HLA antibody response had higher PIRCHE-II scores when having a live birth compared with sRPL women who experienced another pregnancy loss. This difference was not observed in the IVIG-treated group. Furthermore, as a proxy for T-cell memory, the number of overlapping peptides between the two paternal haplotypes in couples having live births without treatment displayed a larger number of overlapping peptides. This effect was primarily driven by class II-derived peptides. These results suggest that specific combinations of sRPL mothers and fathers, particularly those with an anti-HLA antibody response, may generate higher PIRCHE-II scores, which could contribute to successful live births. Understanding these immune interactions may provide insights for personalised diagnostic and therapeutic strategies in sRPL.

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来源期刊
HLA
HLA Immunology and Microbiology-Immunology
CiteScore
3.00
自引率
28.80%
发文量
368
期刊介绍: HLA, the journal, publishes articles on various aspects of immunogenetics. These include the immunogenetics of cell surface antigens, the ontogeny and phylogeny of the immune system, the immunogenetics of cell interactions, the functional aspects of cell surface molecules and their natural ligands, and the role of tissue antigens in immune reactions. Additionally, the journal covers experimental and clinical transplantation, the relationships between normal tissue antigens and tumor-associated antigens, the genetic control of immune response and disease susceptibility, and the biochemistry and molecular biology of alloantigens and leukocyte differentiation. Manuscripts on molecules expressed on lymphoid cells, myeloid cells, platelets, and non-lineage-restricted antigens are welcomed. Lastly, the journal focuses on the immunogenetics of histocompatibility antigens in both humans and experimental animals, including their tissue distribution, regulation, and expression in normal and malignant cells, as well as the use of antigens as markers for disease.
期刊最新文献
The Full-Length Genomic Sequence of the HLA-B*46:01:25 Allele The HLA-A Allele, HLA-A*11:01:01:07, Identified by Third-Generation Sequencing The HLA-B*27:264 Allele Identified in a Volunteer Donor for Haematopoietic Stem Cell Transplant Characterisation of the Novel HLA-A*23:147 Allele Using New Next-Generation Sequencing Methods Identification of the Novel HLA-DPA1*01:214 Allele in a Brazilian Bone Marrow Donor
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