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Immunoregulacyjna rola limfocytów B w odpowiedzi na alloprzeszczep nerki

机译:B淋巴细胞在肾脏同种异体移植反应中的免疫调节作用

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B cells are a group of diverse phenotype and function subsets, which can both stimulate and inhibit the immune response to an allograft. They participate in the rejection process by influencing differentiation, proliferation and effector functions of T lymphocytes. B cells injure the graft via the ADCC (antibody-dependent cellular cytotoxicity) reaction and humoral rejection through plasmocyte production of donor-specific antibodies.A converse, suppressive mode of B cells can attribute to the development of tolerance and protect the graft from rejection. This function is provided by the regulatory B cells, which negatively control the immune response by producing suppressor cytokines (IL-10, IL-35, TGF-β), natural antibodies and through cellular interactions. In effect they inhibit the development of Th1 and Th17 effector cells, and induce differentiation of regulatory T cells.Operational immune tolerance in human kidney transplant recipients was associated with increased number of na?ve and transitional B cells of regulatory function, and increased gene expression for differentiation of B cells. However, in chronic alloantibody transplant rejection the distorted distribution and function of regulatory B cells was found, which implies their pivotal role in graft tolerance.Currently, the immunosuppressive regimens unselectively inhibit the activity of T and B cells, by interfering with their effector and immunoregulatory functions. They do not fully control the chronic rejection reaction, which is the major cause of graft loss. Comprehension of the mechanisms of immunologic homeostasis dependent on B cells can help develop immunosuppressive protocols targeted at tolerance.
机译:B细胞是一组不同的表型和功能亚型,可以刺激和抑制对同种异体移植物的免疫反应。它们通过影响T淋巴细胞的分化,增殖和效应子功能参与排斥过程。 B细胞通过ADCC(抗体依赖性细胞毒性)反应损伤移植物,并通过产生供体特异性抗体的浆细胞产生体液排斥反应。相反,B细胞的抑制模式可归因于耐受性的发展并保护移植物免受排斥。该功能由调节性B细胞提供,该B细胞通过产生抑制性细胞因子(IL-10,IL-35,TGF-β),天然抗体并通过细胞相互作用来负控制免疫反应。实际上,它们抑制Th1和Th17效应细胞的发育,并诱导调节性T细胞的分化。人肾移植受者的操作免疫耐受与调节功能的幼稚和过渡性B细胞数量增加以及基因表达增加有关用于B细胞的分化。然而,在慢性同种抗体移植排斥反应中,发现了调节性B细胞的分布和功能失真,这暗示了它们在移植耐受中的关键作用。目前,免疫抑制方案通过干扰T和B细胞的效应子和免疫调节来选择性地抑制T和B细胞的活性。职能。它们不能完全控制慢性排斥反应,这是移植物丢失的主要原因。理解依赖于B细胞的免疫稳态的机制可以帮助开发针对耐受性的免疫抑制方案。

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