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不同大鼠品系组合中对供体特异性输血的IgG同种抗体反应作为肾移植存活的预测指标。

IgG alloantibody responses to donor-specific blood transfusion in different rat strain combinations as a predictor of renal allograft survival.

作者信息

Wasowska B, Baldwin W M, Sanfilippo F

机构信息

Department of Pathology, Duke University, Durham, North Carolina.

出版信息

Transplantation. 1992 Jan;53(1):175-80. doi: 10.1097/00007890-199201000-00035.

Abstract

Donor-specific blood transfusion prolongs the survival of fully allogeneic ACI (RT1a) renal allografts in PVG (RT1c) recipients from 7-10 days to greater than 100 days. We have observed significant differences in the alloantibody (Ab1) responses to ACI renal allografts in control and DSBT-treated PVG recipients: DSBT is associated with decreased IgG and IgM alloantibody circulating in serum, deposited in the allograft, and produced in culture by splenocytes. In the present studies the effects of DSBT on alloantibody production and renal allograft survival were extended to examine other recipient strains: F344 (RT1lv1), BN (RT1n), W/F (RT1u) and LEW (RT1l). Animals of each recipient strain were injected i.v. with 0.5 ml of ACI blood alone or followed by a renal allograft. Studies on the kinetics of IgM and IgG alloantibody responses were performed by flow cytometry on lymphocytes from donor ACI, PVG, and PVG.R1 (RT1.Aa class I MHC antigen on PVG background) rats. In F344 and PVG rats, DSBT from ACI rats elicited a transient IgM response that peaked at day 7 and was not followed by a switch to IgG. In control PBS transfused F344 recipients, an ACI renal allograft stimulated both IgM and IgG alloantibody production. DSBT pretreatment significantly decreased circulating IgG alloantibody following ACI renal transplantation and prolonged graft survival in F344 recipients. In DSBT-treated F344 recipients that rejected ACI renal allografts acutely, small amounts of IgG (5-12 mode channel shift) were detected in sera harvested 7 days after transplantation, whereas almost no IgG was detected in the sera from DSBT treated F344 rats that accepted their renal allografts indefinitely. In contrast, DSBT alone from ACI to BN, W/F, or LEW strains elicited a transient IgM response that peaked at day 7 and was followed by a strong IgG response that peaked on days 10-14 and remained high through day 21. DSBT failed to prolong ACI renal allograft survival in any of these strains (survival less than 11 days in control and DSBT rats). The alloantibody response to DSBT in all five recipient strains examined was directed primarily to RT1.Aa class I MHC antigens, as determined by binding studies on lymphocytes from ACI, PVG and PVG.R1 rats and alloantibody blocking studies using biotinylated rat monoclonal antibodies to distinct epitopes of the RT1.Aa antigen. The relative magnitude of blocking of R2/10P and R2/15S binding by sera from BN, W/F, and LEW rats was: control allograft recipients greater than DSBT pretreated allograft recipients greater than DSBT alone.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

供体特异性输血可使完全异基因的 ACI(RT1a)肾移植在 PVG(RT1c)受体中的存活时间从 7 - 10 天延长至超过 100 天。我们观察到对照和经供体特异性输血治疗的 PVG 受体对 ACI 肾移植的同种异体抗体(Ab1)反应存在显著差异:供体特异性输血与血清中循环的 IgG 和 IgM 同种异体抗体减少、移植肾中沉积的同种异体抗体减少以及脾细胞培养产生的同种异体抗体减少有关。在本研究中,供体特异性输血对同种异体抗体产生和肾移植存活的影响扩展至其他受体品系:F344(RT1lv1)、BN(RT1n)、W/F(RT1u)和 LEW(RT1l)。每个受体品系的动物静脉注射 0.5 ml ACI 血,单独注射或随后进行肾移植。通过流式细胞术对来自供体 ACI、PVG 和 PVG.R1(PVG 背景上的 RT1.Aa 类 I 型 MHC 抗原)大鼠的淋巴细胞进行 IgM 和 IgG 同种异体抗体反应动力学研究。在 F344 和 PVG 大鼠中,来自 ACI 大鼠的供体特异性输血引发短暂的 IgM 反应,在第 7 天达到峰值,之后未转变为 IgG。在输注对照 PBS 的 F344 受体中,ACI 肾移植刺激了 IgM 和 IgG 同种异体抗体的产生。供体特异性输血预处理显著降低了 ACI 肾移植后循环中的 IgG 同种异体抗体,并延长了 F344 受体的移植存活时间。在急性排斥 ACI 肾移植的经供体特异性输血治疗的 F344 受体中,移植后 7 天采集的血清中检测到少量 IgG(5 - 12 模式通道偏移),而在无限期接受肾移植的经供体特异性输血治疗的 F344 大鼠血清中几乎未检测到 IgG。相比之下,从 ACI 到 BN、W/F 或 LEW 品系单独进行供体特异性输血引发短暂的 IgM 反应,在第 7 天达到峰值,随后是强烈的 IgG 反应,在第 10 - 14 天达到峰值并持续至第 21 天保持高位。供体特异性输血未能延长这些品系中任何一个的 ACI 肾移植存活时间(对照和经供体特异性输血治疗的大鼠存活时间均小于 11 天)。通过对来自 ACI、PVG 和 PVG.R1 大鼠的淋巴细胞进行结合研究以及使用针对 RT1.Aa 抗原不同表位的生物素化大鼠单克隆抗体进行同种异体抗体阻断研究确定,在所检测的所有五个受体品系中,对供体特异性输血的同种异体抗体反应主要针对 RT1.Aa 类 I 型 MHC 抗原。BN、W/F 和 LEW 大鼠血清对 R2/10P 和 R2/15S 结合的阻断相对程度为:对照移植受体大于经供体特异性输血预处理的移植受体大于单独进行供体特异性输血。(摘要截取自 400 字)

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