将供体-受体嵌合细胞(DRCC)移植作为缓解全身辐照损伤的桥梁疗法

Maria Siemionow, Krzysztof Bieda, Katarzyna Stawarz, Malgorzata Cyran, Lucile Chambily, Krzysztof Kusza
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摘要

近年来,以细胞为基础的疗法已成为减轻辐射所致损伤的一种有前途的方法。急性辐射综合征(ARS)是在短时间内暴露于高剂量辐射的结果。本研究旨在比较供体-受体嵌合细胞(DRCC)疗法在减轻10灰度(Gy)全身辐照(TBI)剂量诱发的急性辐射综合征方面的疗效。30 只经过辐照的 Lewis 大鼠被用作 ARS 模型,在五个实验组(n=6/组)(生理盐水对照组、异基因骨髓移植组(isoBMT)、异基因 BMT 组(alloBMT)、DRCC 组和 alloBMT+DRCC 组)中评估全身骨内移植不同细胞疗法的疗效。DRCC 是通过聚乙二醇介导融合 24 名 ACI(RT1a)和 24 名 Lewis(RT11)大鼠供体的骨髓细胞而产生的。流式细胞术(FC)和共聚焦显微镜(CM)证实了 DRCC 的产生和嵌合状态。通过全血细胞计数分析评估血液参数的恢复情况。移植物抗宿主病(GvHD)症状通过临床和肾脏、皮肤和小肠活检组织病理学进行评估。FC 和 CM 证实了 DRCC 融合的可行性和嵌合状态。生理盐水对照组的死亡率为 100%,而 DRCC 移植后的存活率为 100%,这与外周血参数的显著恢复有关。此外,DRCC和alloBMT+DRCC移植后未观察到GvHD的临床或组织病理学迹象。这些发现证实了 DRCC 在减轻 GvHD、促进造血功能恢复和提高创伤性脑损伤引起的 ARS 后动物存活率方面的疗效。 此外,DRCC 治疗的耐受性和免疫调节特性也支持其临床应用的可行性。因此,本研究将DRCC作为一种创新的桥接疗法,用于缓解创伤性脑损伤的急性影响,对干细胞研究和再生医学具有广泛的意义。
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Donor-Recipient Chimeric Cells (DRCC) Transplantation as the Bridging Therapy for Mitigating Total Body Irradiation-Induced Injury.
In recent years, cell-based therapies have emerged as a promising approach for mitigating radiation-induced injury. Acute radiation syndrome (ARS) results from exposure to high doses of radiation over a short time period. This study aimed to compare the efficacy of donor-recipient chimeric cell (DRCC) therapy in mitigating ARS induced by a total body irradiation (TBI) dose of 10 gray (Gy). Thirty irradiated Lewis rats were employed as ARS models to assess the efficacy of systemic-intraosseous transplantation of different cellular therapies in five experimental groups (n=6/group): saline control, isogeneic bone marrow transplantation (isoBMT), allogeneic BMT (alloBMT), DRCC, and alloBMT+DRCC. DRCC were created by polyethylene glycol-mediated fusion of bone marrow cells from 24 ACI (RT1a) and 24 Lewis (RT11) rat donors. The creation of DRCC and chimeric state were confirmed by flow cytometry (FC) and confocal microscopy (CM). Recovery of blood parameters was evaluated via complete blood count analysis. GvHD (graft-versus-host disease) signs were assessed clinically and histopathologically using kidney, skin, and small intestine biopsies. FC and CM confirmed the fusion feasibility and the chimeric state of DRCC. A 100% mortality rate was observed in the saline control group, whereas a 100% survival was recorded following DRCC transplantation, correlating with significant recovery of peripheral blood parameters. Additionally, no clinical or histopathological signs of GvHD were observed after DRCC and alloBMT+DRCC transplantation. These findings confirm efficacy of DRCC in mitigating GvHD, promoting hematopoietic recovery, and increasing animal survival following TBI-induced ARS.​​ Moreover, tolerogenic and immunomodulatory properties of DRCC therapy support its feasibility for clinical applications. Therefore, this study introduces DRCC as an innovative bridging therapy for alleviating the acute effects of TBI, with broad implications for stem cell research and regenerative medicine.
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