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首页> 外文期刊>American journal of transplantation: official journal of the American Society of Transplantation and the American Society of Transplant Surgeons >Donor-specific indirect pathway analysis reveals a B-cell-independent signature which reflects outcomes in kidney transplant recipients.
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Donor-specific indirect pathway analysis reveals a B-cell-independent signature which reflects outcomes in kidney transplant recipients.

机译:供体特异性间接途径分析揭示了B细胞独立的特征,反映了肾移植受体的预后。

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To investigate the role of donor-specific indirect pathway T cells in renal transplant tolerance, we analyzed responses in peripheral blood of 45 patients using the trans-vivo delayed-type hypersensitivity assay. Subjects were enrolled into five groups-identical twin, clinically tolerant (TOL), steroid monotherapy (MONO), standard immunosuppression (SI) and chronic rejection (CR)-based on transplant type, posttransplant immunosuppression and graft function. The indirect pathway was active in all groups except twins but distinct intergroup differences were evident, corresponding to clinical status. The antidonor indirect pathway T effector response increased across patient groups (TOL < MONO < SI < CR; p < 0.0001) whereas antidonor indirect pathway T regulatory response decreased (TOL > MONO = SI > CR; p < 0.005). This pattern differed from that seen in circulating na?ve B-cell numbers and in a cross-platform biomarker analysis, where patients on monotherapy were not ranked closest to TOL patients, but rather were indistinguishable from chronically rejecting patients. Cross-sectional analysis of the indirect pathway revealed a spectrum in T-regulatory:T-effector balance, ranging from TOL patients having predominantly regulatory responses to CR patients having predominantly effector responses. Therefore, the indirect pathway measurements reflect a distinct aspect of tolerance from the recently reported elevation of circulating na?ve B cells, which was apparent only in recipients off immunosuppression.
机译:为了研究供体特异性间接途径T细胞在肾移植耐受中的作用,我们使用体内延迟型超敏反应分析了45位患者外周血的反应。根据移植类型,移植后免疫抑制和移植功能,将受试者分为五个组,分别为同卵双胞胎,临床耐受性(TOL),类固醇单一疗法(MONO),标准免疫抑制(SI)和慢性排斥(CR)。除双胞胎外,所有组的间接途径均活跃,但明显的组间差异是明显的,与临床状况相对应。各个患者组之间的抗供体间接途径T效应子应答增加(TOL MONO = SI> CR; p <0.005)。这种模式不同于在循环中的初次B细胞数量和跨平台生物标志物分析中所看到的模式,在后者中,采用单一疗法的患者的排名并非最接近TOL患者,而与长期排斥的患者没有区别。间接途径的横断面分析揭示了T调节:T效应子平衡的范围,从具有主要调节反应的TOL患者到主要具有效应反应的CR患者不等。因此,间接途径的测量反映了与最近报道的循环中幼稚B细胞的升高不同的耐受性,这仅在免疫抑制受体中可见。

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