Donor-derived cytomegalovirus-specific CD8+ T cells restricted to shared, donor-specific, or host-specific HLA after HLA mismatched hematopoietic stem cell transplantation

IF 1.6 4区 医学 Q4 IMMUNOLOGY Transplant immunology Pub Date : 2024-08-05 DOI:10.1016/j.trim.2024.102099
Kazuhiro Ikegame , Keiko Fukunaga , Yuko Osugi , Katsuji Kaida , Masahiro Teramoto , Takayuki Inoue , Masaya Okada , Kyoko Yoshihara , Hiroya Tamaki , Satoshi Yoshihara , Hiroshi Fujiwara
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Abstract

Immune reconstitution after human leukocyte antigen (HLA)-mismatched (haploidentical) hematopoietic stem cell transplantation (haplo-HCT) can significantly influence long-term outcomes. The three possible HLA haplotypes after transplantation are: one carried by both the patient and the donor (shared HLA), one by donor only (donor-specific HLA), and one by patient only (host-specific HLA), and the donor T cells remain restricted to one of these three haplotypes. Understanding the presence of donor T cells restricted to each haplotype may provide more detailed insights into post-transplant immune response and potentially provide valuable information for the development of chimeric antigen receptor T cell or T cell receptor T cell constructs. In this study, patients or donors with HLA-A24 or HLA-A2 were tested with HLA-A*24:02- and A*02:01-restricted cytomegalovirus (CMV)-specific tetramers for detecting the respective HLA-restricted T cells. Sixty-four samples from 40 patients were assayed. More than half of the patients at day 90 and all patients by day 900 had shared HLA-restricted T cells. After day 90, half of the patients had donor-specific HLA-restricted T cells, but no host-specific HLA-restricted T cells were found. In the comparative analysis of the transplant types, shared HLA-restricted T cells were positive in all three categories: haplo-HCT (50%), 2-haplo-mis-HCT (75%), and spousal HCT (67%). Furthermore, donor-specific HLA-restricted T cells demonstrated positivity in haplo-HCT at 57% and in 2-haplo-mis-HCT at 60%, with a threshold of 0.01%. Donor-specific HLA-restricted T cells for spousal HCT were not examined due to the lack of an appropriate HLA combination for the tetramers.

The presence of shared HLA-restricted T cells explains the host defense after HLA-haploidentical transplantation, while the presence of donor-specific HLA-restricted T cells may account for host defense against hematotropic viruses, such as CMV. However, this study failed to detect host-specific HLA-restricted T cells, leaving the host defense against epitheliotropic viruses unresolved, thus requiring further investigation.

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在 HLA 不匹配的造血干细胞移植后,来源于供体的巨细胞病毒特异性 CD8+ T 细胞受限于共享、供体特异性或宿主特异性 HLA。
人类白细胞抗原(HLA)不匹配(单倍体)造血干细胞移植(haplo-HCT)后的免疫重建会严重影响长期预后。移植后可能出现的三种HLA单倍型分别是:患者和供体均携带的一种(共享HLA),仅供体携带的一种(供体特异性HLA),以及仅患者携带的一种(宿主特异性HLA)。了解受限于每种单倍型的供体T细胞的存在情况,可以更详细地了解移植后的免疫反应,并有可能为嵌合抗原受体T细胞或T细胞受体T细胞构建体的开发提供有价值的信息。在这项研究中,使用 HLA-A*24:02- 和 A*02:01- 限制性巨细胞病毒(CMV)特异性四聚体对 HLA-A24 或 HLA-A2 患者或供体进行了检测,以检测相应的 HLA 限制性 T 细胞。对 40 名患者的 64 份样本进行了检测。超过一半的患者在第 90 天和所有患者在第 900 天共享 HLA 限制性 T 细胞。第 90 天后,半数患者有供体特异性 HLA 限制性 T 细胞,但没有发现宿主特异性 HLA 限制性 T 细胞。在移植类型的比较分析中,共享的 HLA 限制性 T 细胞在所有三类移植中均呈阳性:单倍体-HCT(50%)、2-单倍体-同种异体-HCT(75%)和配偶 HCT(67%)。此外,捐献者特异性 HLA 限制性 T 细胞在单倍体-HCT 中的阳性率为 57%,在 2-单倍体-混杂型 HCT 中的阳性率为 60%,阈值为 0.01%。由于缺乏四聚体的适当 HLA 组合,配偶 HCT 的捐献者特异性 HLA 限制性 T 细胞未进行检测。共享的 HLA 限制性 T 细胞的存在解释了 HLA 同种异体移植后的宿主防御,而供体特异性 HLA 限制性 T 细胞的存在可能解释了宿主对 CMV 等血液病毒的防御。然而,这项研究未能检测到宿主特异性 HLA 限制性 T 细胞,因此宿主对上皮细胞病毒的防御能力问题仍未解决,需要进一步研究。
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来源期刊
Transplant immunology
Transplant immunology 医学-免疫学
CiteScore
2.10
自引率
13.30%
发文量
198
审稿时长
48 days
期刊介绍: Transplant Immunology will publish up-to-date information on all aspects of the broad field it encompasses. The journal will be directed at (basic) scientists, tissue typers, transplant physicians and surgeons, and research and data on all immunological aspects of organ-, tissue- and (haematopoietic) stem cell transplantation are of potential interest to the readers of Transplant Immunology. Original papers, Review articles and Hypotheses will be considered for publication and submitted manuscripts will be rapidly peer-reviewed and published. They will be judged on the basis of scientific merit, originality, timeliness and quality.
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