Late Treatment With Autologous Expanded Regulatory T-cell Therapy After Alemtuzumab Induction Is Safe and Facilitates Immunosuppression Minimization in Living Donor Renal Transplantation.

IF 5.3 2区医学 Q1 IMMUNOLOGY

Transplantation Pub Date : 2024-11-01 Epub Date: 2024-10-22 DOI:10.1097/TP.0000000000005065

Matthew O Brook, Conor Hennessy, Joanna Hester, Salim Hammad, Alaa Alzhrani, Ines Rombach, Susan Dutton, Giovanna Lombardi, Kathryn J Wood, Peter Friend, Paul N Harden, Fadi Issa

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引用次数: 0

Abstract

Background: The TWO Study (Transplantation Without Overimmunosuppression) aimed to investigate a novel approach to regulatory T-cell (Treg) therapy in renal transplant patients, using a delayed infusion protocol at 6 mo posttransplant to promote a Treg-skewed lymphocyte repopulation after alemtuzumab induction. We hypothesized that this would allow safe weaning of immunosuppression to tacrolimus alone. The COVID-19 pandemic led to the suspension of alemtuzumab use, and therefore, we report the unique cohort of 7 patients who underwent the original randomized controlled trial protocol. This study presents a unique insight into Treg therapy combined with alemtuzumab and is therefore an important proof of concept for studies in other diseases that are considering lymphodepletion.

Methods: Living donor kidney transplant recipients were randomized to receive autologous polyclonal Treg at week 26 posttransplantation, coupled with weaning doses of tacrolimus, (Treg therapy arm) or standard immunosuppression alone (tacrolimus and mycophenolate mofetil). Primary outcomes were patient survival and rejection-free survival.

Results: Successful cell manufacturing and cryopreservation until the 6-mo infusion were achieved. Patient and transplant survival was 100%. Acute rejection-free survival was 100% in the Treg-treated group at 18 mo after transplantation. Although alemtuzumab caused a profound depletion of all lymphocytes, including Treg, after cell therapy infusion, there was a transient increase in peripheral Treg numbers.

Conclusions: The study establishes that delayed autologous Treg therapy is both feasible and safe, even 12 mo after cell production. The findings present a new treatment protocol for Treg therapy, potentially expanding its applications to other indications.

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阿仑妥珠单抗诱导后的自体扩增调节性T细胞疗法是安全的，并能促进活体肾移植中免疫抑制最小化。

研究背景TWO研究（无过度免疫抑制移植）旨在研究肾移植患者调节性T细胞（Treg）治疗的新方法，在移植后6个月采用延迟输注方案，以促进阿仑珠单抗诱导后Treg倾斜淋巴细胞的重新填充。我们假设这将使免疫抑制安全断奶，仅使用他克莫司。COVID-19 大流行导致阿仑妥珠单抗暂停使用，因此我们报告了接受原始随机对照试验方案的 7 例患者的独特队列。这项研究对Treg疗法与阿仑妥珠单抗的结合提出了独特的见解，因此对正在考虑淋巴消耗的其他疾病的研究来说是一个重要的概念验证：方法：活体肾移植受者在移植后第26周随机接受自体多克隆Treg治疗，同时服用他克莫司（Treg治疗组）或单独使用标准免疫抑制剂（他克莫司和霉酚酸酯）。主要结果是患者存活率和无排斥存活率：结果：细胞制造和冷冻保存成功，直至输注6个月。患者和移植存活率为 100%。Treg治疗组在移植后18个月的无急性排斥反应存活率为100%。虽然阿仑妥珠单抗在细胞疗法输注后会导致包括Treg在内的所有淋巴细胞大量耗竭，但外周Treg的数量却有短暂增加：这项研究证实，延迟自体 Treg 治疗既可行又安全，即使在细胞生产 12 个月后也是如此。研究结果提出了一种新的 Treg 治疗方案，有可能将其应用扩展到其他适应症。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Transplantation 医学-免疫学

CiteScore

8.50

自引率

11.30%

发文量

1906

审稿时长

1 months

期刊介绍： The official journal of The Transplantation Society, and the International Liver Transplantation Society, Transplantation is published monthly and is the most cited and influential journal in the field, with more than 25,000 citations per year. Transplantation has been the trusted source for extensive and timely coverage of the most important advances in transplantation for over 50 years. The Editors and Editorial Board are an international group of research and clinical leaders that includes many pioneers of the field, representing a diverse range of areas of expertise. This capable editorial team provides thoughtful and thorough peer review, and delivers rapid, careful and insightful editorial evaluation of all manuscripts submitted to the journal. Transplantation is committed to rapid review and publication. The journal remains competitive with a time to first decision of fewer than 21 days. Transplantation was the first in the field to offer CME credit to its peer reviewers for reviews completed. The journal publishes original research articles in original clinical science and original basic science. Short reports bring attention to research at the forefront of the field. Other areas covered include cell therapy and islet transplantation, immunobiology and genomics, and xenotransplantation.