Hematopoietic cell-based and non-hematopoietic cell-based strategies for immune tolerance induction in living-donor renal transplantation: A systematic review

IF 3.6 2区 医学 Q2 IMMUNOLOGY Transplantation Reviews Pub Date : 2023-08-19 DOI:10.1016/j.trre.2023.100792
Chandrashekar Annamalai , Vivek Kute , Carl Sheridan , Ahmed Halawa
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Abstract

Introduction

Despite its use to prevent acute rejection, lifelong immunosuppression can adversely impact long-term patient and graft outcomes. In theory, immunosuppression withdrawal is the ultimate goal of kidney transplantation, and is made possible by the induction of immunological tolerance. The purpose of this paper is to review the safety and efficacy of immune tolerance induction strategies in living-donor kidney transplantation, both chimerism-based and non-chimerism-based. The impact of these strategies on transplant outcomes, including acute rejection, allograft function and survival, cost, and immune monitoring, will also be discussed.

Materials and methods

Databases such as PubMed, Scopus, and Web of Science, as well as additional online resources such as EBSCO, were exhaustively searched. Adult living-donor kidney transplant recipients who developed chimerism-based tolerance after concurrent bone marrow or hematopoietic stem cell transplantation or those who received non-chimerism-based, non-hematopoietic cell therapy using mesenchymal stromal cells, dendritic cells, or regulatory T cells were studied between 2000 and 2021. Individual sources of evidence were evaluated critically, and the strength of evidence and risk of bias for each outcome of the transplant tolerance study were assessed.

Results

From 28,173 citations, 245 studies were retrieved after suitable exclusion and duplicate removal. Of these, 22 studies (2 RCTs, 11 cohort studies, 6 case-control studies, and 3 case reports) explicitly related to both interventions (chimerism- and non-chimerism-based immune tolerance) were used in the final review process and were critically appraised. According to the findings, chimerism-based strategies fostered immunotolerance, allowing for the safe withdrawal of immunosuppressive medications. Cell-based therapy, on the other hand, frequently did not induce tolerance except for minimising immunosuppression. As a result, the rejection rates, renal allograft function, and survival rates could not be directly compared between these two groups. While chimerism-based tolerance protocols posed safety concerns due to myelosuppression, including infections and graft-versus-host disease, cell-based strategies lacked these adverse effects and were largely safe.

There was a lack of direct comparisons between HLA-identical and HLA-disparate recipients, and the cost implications were not examined in several of the retrieved studies. Most studies reported successful immunosuppressive weaning lasting at least 3 years (ranging up to 11.4 years in some studies), particularly with chimerism-based therapy, while only a few investigators used immune surveillance techniques. The studies reviewed were often limited by selection, classification, ascertainment, performance, and attrition bias.

Conclusions

This review demonstrates that chimerism-based hematopoietic strategies induce immune tolerance, and a substantial number of patients are successfully weaned off immunosuppression. Despite the risk of complications associated with myelosuppression. Non-chimerism-based, non-hematopoietic cell protocols, on the other hand, have been proven to facilitate immunosuppression minimization but seldom elicit immunological tolerance. However, the results of this review must be interpreted with caution because of the non-randomised study design, potential confounding, and small sample size of the included studies. Further validation and refinement of tolerogenic protocols in accordance with local practice preferences is also warranted, with an emphasis on patient selection, cost ramifications, and immunological surveillance based on reliable tolerance assays.

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基于造血细胞和非造血细胞的策略诱导活体肾移植免疫耐受:系统综述
引言尽管终身免疫抑制可以预防急性排斥反应,但它会对患者和移植物的长期结果产生不利影响。从理论上讲,免疫抑制退出是肾移植的最终目标,并通过诱导免疫耐受而成为可能。本文的目的是综述基于嵌合和非嵌合的活体供肾移植中免疫耐受诱导策略的安全性和有效性。还将讨论这些策略对移植结果的影响,包括急性排斥反应、同种异体移植物功能和存活率、成本和免疫监测。材料和方法对PubMed、Scopus和Web of Science等数据库以及EBSCO等其他在线资源进行了详尽的搜索。2000年至2021年间,研究了在同时进行骨髓或造血干细胞移植后产生嵌合耐受的成年活体供肾移植受者,或使用间充质基质细胞、树突状细胞或调节性T细胞接受非嵌合、非造血细胞治疗的受者。对个体证据来源进行了严格评估,并评估了移植耐受性研究的每个结果的证据强度和偏倚风险。结果从28173篇引文中检索到245篇经过适当排除和重复删除的研究。其中,22项研究(2项随机对照试验、11项队列研究、6项病例对照研究和3份病例报告)与这两种干预措施(基于嵌合和非嵌合的免疫耐受)明确相关,并在最终审查过程中进行了严格评估。根据研究结果,基于嵌合的策略促进了免疫耐受,允许安全地停药免疫抑制药物。另一方面,基于细胞的治疗除了尽量减少免疫抑制外,通常不会诱导耐受。因此,不能直接比较这两组之间的排斥反应率、同种异体肾功能和存活率。虽然基于嵌合的耐受方案由于骨髓抑制(包括感染和移植物抗宿主病)而引起安全问题,但基于细胞的策略缺乏这些不良反应,基本上是安全的。HLA完全相同和HLA完全不同的受试者之间缺乏直接的比较,并且在几项检索到的研究中没有检查成本影响。大多数研究报告免疫抑制断奶成功,持续时间至少为3 年(最高11.4 几年的研究),特别是基于嵌合的治疗,而只有少数研究人员使用了免疫监测技术。所审查的研究往往受到选择、分类、确定、表现和流失偏见的限制。结论本综述表明,基于嵌合的造血策略可诱导免疫耐受,大量患者已成功摆脱免疫抑制。尽管存在骨髓抑制相关并发症的风险。另一方面,基于非嵌合的非造血细胞方案已被证明有助于免疫抑制最小化,但很少引起免疫耐受。然而,由于非随机研究设计、潜在的混杂因素以及纳入研究的样本量小,因此必须谨慎解读本综述的结果。还需要根据当地实践偏好进一步验证和完善耐受性方案,重点是患者选择、成本影响和基于可靠耐受性测定的免疫监测。
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来源期刊
Transplantation Reviews
Transplantation Reviews IMMUNOLOGY-TRANSPLANTATION
CiteScore
7.50
自引率
2.50%
发文量
40
审稿时长
29 days
期刊介绍: Transplantation Reviews contains state-of-the-art review articles on both clinical and experimental transplantation. The journal features invited articles by authorities in immunology, transplantation medicine and surgery.
期刊最新文献
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