脐带血移植后供体t细胞和骨髓嵌合率高于其他细胞来源。

IF 3.2 3区医学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY

Cytotherapy Pub Date : 2025-07-18 DOI:10.1016/j.jcyt.2025.07.003

Rubiya Nadaf, Helena Lee, Omima Mustafa, Denise Bonney, Oana Mirci-Danicar, Ramya Hanasoge-Nataraj, Srividhya Senthil, Claire Horgan, Alison Logan, Kay Poulton, Robert Wynn

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引用次数: 0

摘要

来自不同细胞来源的造血细胞移植（HCT）后多谱系和长期供体嵌合的差异尚未得到很好的表征，但这些信息对于了解每种移植物类型的独特临床用途至关重要。我们分析了472例儿童同种异体HCT受体（2010-2020年）的供体嵌合结果，包括115例非相关脐带血（CB）移植和357例非脐带血移植（骨髓或动员的外周血）。在CB受体中，原发性移植物衰竭发生率更高（4.3% vs. 0.8%, P < 0.05），但在移植患者中，中性粒细胞恢复时的初始平均供体嵌合率相当（两组均为99%，P = 0.5）。在移植后6个月和12个月，CB组的平均全血捐献者嵌合率明显更高(6个月时为100% vs. 93.8%；99.2% vs. 12个月时的91%；P < 0.0001)。在24个月的随访中，平均供体嵌合在CB受体中保持接近完全（99.2%），但在非CB受体中下降(75%；P < 0.0001)。6个月时的血统特异性平均嵌合值也有利于CB组，供体骨髓（CD15 +）嵌合率（100% vs. 85.2%, P = 0.001）和供体t细胞（CD3 +）嵌合率（93% vs. 70%, P < 0.0001）更高。采用非配对双尾t检验比较平均嵌合值，采用Kaplan-Meier方法评估持续完全供体嵌合的累积概率。随着时间的推移，CB受体发生混合嵌合的风险显著降低(风险比，0.5；95% ci, 0.3-0.6, p = 0.002)。总之，CB移植与更持久和完整的多系供体嵌合有关，这一发现可能反映了CB T细胞介导残留宿主造血和免疫细胞排斥的独特免疫能力。随着时间的推移，这种强大的供体优势在骨髓和淋巴细胞间室中尤为明显，这表明移植物抗宿主造血作用是有效和持续的。这些发现强调了CB作为干细胞来源的持续和独特的作用——不仅通过增强移植物抗白血病活性来减少恶性疾病移植后的复发，而且在非恶性疾病（包括代谢疾病，稳定的酶递送至关重要）中维持长期供体来源的造血和功能性移植物的完整性。

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Donor T-cell and myeloid chimerism is higher after cord blood transplant than with other cell sources.

Differences in multi-lineage and long-term donor chimerism after hematopoietic cell transplantation (HCT) from different cell sources are not well characterized, yet such information is crucial for understanding the distinct clinical utilities of each graft type. We analyzed donor chimerism outcomes in 472 pediatric allogeneic HCT recipients (2010-2020), including 115 unrelated cord blood (CB) grafts and 357 non-CB grafts (bone marrow or mobilized peripheral blood). Primary graft failure occurred more frequently in CB recipients (4.3% vs. 0.8%, P < 0.05), but among engrafted patients, initial mean donor chimerism at neutrophil recovery was comparable (∼99% in both groups, P = 0.5). At 6- and 12-months post-transplant, mean whole blood donor chimerism was significantly higher in the CB cohort (100% vs. 93.8% at 6 months; 99.2% vs. 91% at 12 months; P < 0.0001 for both). At 24 months' follow-up, mean donor chimerism remained nearly complete in CB recipients (99.2%) but declined in non-CB recipients (75%; P < 0.0001). Lineage-specific mean chimerism values at 6 months also favored the CB group, with higher donor myeloid (CD15⁺) chimerism (100% vs. 85.2%, P = 0.001) and donor T-cell (CD3⁺) chimerism (93% vs. 70%, P < 0.0001). Statistical analyses were performed using unpaired 2-tailed t-tests for comparing mean chimerism values and Kaplan-Meier methods were used to assess the cumulative probability of sustained complete donor chimerism. CB recipients had a significantly lower risk of developing mixed chimerism over time (hazard ratio, 0.5; 95% CI, 0.3-0.6, P = 0.002). In conclusion, CB transplantation is associated with more durable and complete multi-lineage donor chimerism, a finding that likely reflects the unique immunologic capacity of CB T cells to mediate rejection of residual host hematopoietic and immune cells. This robust donor dominance is particularly evident over time and across both myeloid and lymphoid compartments, suggesting a potent and sustained graft-versus-host hematopoietic effect. These findings underscore a continued and distinct role for CB as a stem cell source-not only in reducing post-transplant relapse in malignant disease through enhanced graft-versus-leukemia activity, but also in sustaining long-term donor-derived hematopoiesis and functional graft integrity in non-malignant disorders, including metabolic diseases in which stable enzyme delivery is critical.

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来源期刊

Cytotherapy 医学-生物工程与应用微生物

CiteScore

6.30

自引率

4.40%

发文量

683

审稿时长

49 days

期刊介绍： The journal brings readers the latest developments in the fast moving field of cellular therapy in man. This includes cell therapy for cancer, immune disorders, inherited diseases, tissue repair and regenerative medicine. The journal covers the science, translational development and treatment with variety of cell types including hematopoietic stem cells, immune cells (dendritic cells, NK, cells, T cells, antigen presenting cells) mesenchymal stromal cells, adipose cells, nerve, muscle, vascular and endothelial cells, and induced pluripotential stem cells. We also welcome manuscripts on subcellular derivatives such as exosomes. A specific focus is on translational research that brings cell therapy to the clinic. Cytotherapy publishes original papers, reviews, position papers editorials, commentaries and letters to the editor. We welcome "Protocols in Cytotherapy" bringing standard operating procedure for production specific cell types for clinical use within the reach of the readership.