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首页> 外文期刊>Clinical immunology: The official journal of the Clinical Immunology Society >Umbilical cord blood transplantation: basic biology and clinical challenges to immune reconstitution.
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Umbilical cord blood transplantation: basic biology and clinical challenges to immune reconstitution.

机译:脐带血移植:免疫重建的基本生物学和临床挑战。

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Allogeneic stem cell transplantation has continued to evolve as a common procedure for the treatment of hematological malignancies and bone marrow failure. Donor bone marrow and mobilized peripheral stem cells are routinely employed for the reconstitution of immune function in leukemia and lymphoma patients following radiation and/or chemotherapy. Unfortunately, only 30% of patients have an HLA-identical sibling donor and the identification of matched unrelated donors, particularly for minorities, can present an exceptional challenge. The transplantation of umbilical cord blood (UCB) represents the most recent strategy to expand the potential donor pool while maintaining an acceptable level of treatment-related complications. First utilized in children, UCB transplantation permits a higher degree of HLA disparity while demonstrating a reduction in the incidence and severity of graft-versus-host disease (GvHD) compared to previous transplantation modalities. Despite the apparent decrease in GvHD, relapse rates remain comparable to transplantation with bone marrow or mobilized peripheral blood suggesting a strong graft-versus-leukemia/lymphoma (GvL) effect. However, several issues complicate the use of UCB transplantation and its extension to the treatment of adults. Many infections that afflict transplant patients are particularly frequent and more severe in the context of UCB transplantation. UCB T-cells are naive and therefore display less proliferation and IFN-gamma production in response to cognate antigen and also appear to demonstrate defects in signal transduction mechanisms. In addition, UCB contains T regulatory cells (Treg) with more potent suppressor function than adult Treg. Furthermore, adult patients often require more total cells and CD34+ progenitors for transplantation than a single UCB unit can provide. Thus, strategies to expand selected subpopulations from UCB and the use of multi-unit transplantation are areas of active research. This review will provide a condensed summary of theclinical history of UCB transplantation and emphasize the advantages and disadvantages of this approach to hematological malignancies in comparison to other methods of hematopoietic stem cell transplantation. Subsequently, it will mainly focus on the current challenges to immune reconstitution presented by UCB transplantation, recent research into their cellular and molecular mechanisms, and experimental approaches to overcome them.
机译:作为血液恶性肿瘤和骨髓衰竭的常见治疗方法,异基因干细胞移植一直在继续发展。白血病和淋巴瘤患者在放射和/或化疗后,通常使用供体骨髓和动员的外周血干细胞重建免疫功能。不幸的是,只有30%的患者拥有与HLA相同的同胞供体,而对匹配的无关供体(尤其是针对少数族裔)的鉴定可能会带来特殊的挑战。脐带血(UCB)的移植代表了扩大潜在供体库同时保持可接受水平的治疗相关并发症的最新策略。与以前的移植方式相比,UCB移植首先用于儿童,它允许更高程度的HLA差异,同时证明移植物抗宿主病(GvHD)的发生率和严重性降低。尽管GvHD明显降低,但复发率仍与骨髓或动员的外周血移植相当,表明移植物抗白血病/淋巴瘤(GvL)效果强。但是,一些问题使UCB移植的使用及其扩展到成人治疗变得复杂。在UCB移植的背景下,许多困扰移植患者的感染尤其常见,而且更为严重。 UCB T细胞是幼稚的,因此响应同源抗原显示较少的增殖和IFN-γ产生,并且似乎也表现出信号转导机制的缺陷。此外,UCB包含的T调节细胞(Treg)比成人Treg具有更强的抑制功能。此外,成年患者通常需要比单个UCB单元更多的总细胞和CD34 +祖细胞进行移植。因此,从UCB扩展选定亚群的策略以及多单位移植的使用是积极研究的领域。这篇综述将简要概述UCB移植的临床历史,并强调与其他造血干细胞移植方法相比,这种方法对血液系统恶性肿瘤的优缺点。随后,它将主要关注UCB移植对免疫重建提出的当前挑战,对其细胞和分子机制的最新研究以及克服这些挑战的实验方法。

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