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供者受者嵌合细胞诱导嵌合体并延长血管化复合同种异体移植物的存活。

Donor Recipient Chimeric Cells Induce Chimerism and Extend Survival of Vascularized Composite Allografts.

机构信息

Department of Orthopaedics, University of Illinois At Chicago, Molecular Biology Research Building, 900 S. Ashland Ave. Room# 3356, Chicago, IL, 60607, USA.

Department of Plastic Surgery, Cleveland Clinic, Cleveland, OH, USA.

出版信息

Arch Immunol Ther Exp (Warsz). 2021 May 10;69(1):13. doi: 10.1007/s00005-021-00614-9.

Abstract

This study evaluated the efficacy of donor recipient chimeric cell (DRCC) therapy created by fusion of donor and recipient derived bone marrow cells (BMC) in chimerism and tolerance induction in a rat vascularized composite allograft (VCA) model. Twenty-four VCA (groin flaps) from MHC-mismatched ACI (RT1) donors were transplanted to Lewis (RT1) recipients. Rats were randomly divided into (n = 6/group): Group 1-untreated controls, Groups 2-7-day immunosuppression controls, Group 3-DRCC, and Group 4-DRCC with 7-day anti-αβTCR monoclonal antibody and cyclosporine A protocol. DRCC created by polyethylene glycol-mediated fusion of ACI and Lewis BMC were cultured and transplanted (2-4 × 10) to VCA recipients via intraosseous delivery route. Flow cytometry assessed peripheral blood chimerism while fluorescent microscopy and PCR tested the presence of DRCC in the recipient's blood, bone marrow (BM), and lymphoid organs at the study endpoint (VCA rejection). No complications were observed after DRCC intraosseous delivery. Group 4 presented the longest average VCA survival (79.3 ± 30.9 days) followed by Group 2 (53.3 ± 13.6 days), Group 3 (18 ± 7.5 days), and Group 1 (8.5 ± 1 days). The highest chimerism level was detected in Group 4 (57.9 ± 6.2%) at day 7 post-transplant. The chimerism declined at day 21 post-transplant and remained at 10% level during the entire follow-up period. Single dose of DRCC therapy induced long-term multilineage chimerism and extended VCA survival. DRCC introduces a novel concept of customized donor-recipient cell-based therapy supporting solid organ and VCA transplants.

摘要

本研究评估了供体-受体嵌合细胞(DRCC)疗法在大鼠血管化复合异体移植物(VCA)模型中的嵌合和诱导耐受中的疗效,该疗法通过融合供体和受体来源的骨髓细胞(BMC)而产生。24 个 MHC 错配的 ACI(RT1)供体的 VCA(腹股沟皮瓣)被移植到 Lewis(RT1)受体。大鼠随机分为(n = 6/组):第 1 组-未治疗对照组,第 2-7 天免疫抑制对照组,第 3 组-DRCC,第 4 组-DRCC 联合 7 天抗-αβTCR 单克隆抗体和环孢素 A 方案。通过聚乙二醇介导的 ACI 和 Lewis BMC 融合创建 DRCC,通过骨内途径移植(2-4×10)至 VCA 受体。流式细胞术评估外周血嵌合情况,荧光显微镜和 PCR 检测受体血液、骨髓(BM)和淋巴器官中 DRCC 的存在,作为研究终点(VCA 排斥)。DRCC 骨内递送后未观察到并发症。第 4 组的平均 VCA 存活时间最长(79.3±30.9 天),其次是第 2 组(53.3±13.6 天)、第 3 组(18±7.5 天)和第 1 组(8.5±1 天)。移植后第 7 天检测到最高的嵌合率(57.9±6.2%)。嵌合率在移植后第 21 天下降,并在整个随访期间保持在 10%水平。单次 DRCC 治疗诱导长期多谱系嵌合和延长 VCA 存活。DRCC 提出了一种新的概念,即定制的供体-受体细胞为基础的治疗方法,支持实体器官和 VCA 移植。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6721/8110509/c27f9c69c09b/5_2021_614_Fig1_HTML.jpg

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