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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Flow cross-matching identifies patients at risk for postoperative elaboration of cytotoxic antibodies.
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Flow cross-matching identifies patients at risk for postoperative elaboration of cytotoxic antibodies.

机译:流交叉匹配可识别出有可能在术后精心制作细胞毒性抗体的患者。

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BACKGROUND: Cytotoxic IgG against class I antigens can contribute to renal dysfunction or failure after transplantation. However, the clinical relevance of IgG measured by flow cytometric cross-matching is controversial. This study correlated pre- and postoperative flow reactivity with clinical outcome among renal transplant patients with negative preoperative cytotoxic cross-matches. METHODS: Nonsensitized primary renal allograft patients (n = 157) with negative preoperative cytotoxic cross-matches (complement-dependent lymphocytotoxicity assays) were stratified on the basis of IgG reactivity measured by flow cytometric cross-matching (FCXM) as FCXM negative (Neg) or positive against class I (T-pos FCXM) or class II (B-pos FCXM) antigens. The groups were compared in terms of frequency of early rejection and 1-year graft survival. RESULTS: Patient distribution was 67% Neg, 14% T-pos FCXM, 14% B-pos FCXM, and 5% IgM FCXM. The incidence of early rejection was 25+/-3% for Neg and 51+/-3% for T- and B-pos FCXM (P < 0.05). One-year graft survival for Neg versus T-pos and B-pos FCXM was 97+/-3% versus 44+/-10% (P < 0.05) and 77+/-5% (P = 0.06), respectively. Rejections requiring plasmapheresis were found only among patients with T-pos FCXM. Among 29 patients, FCXM and complement-dependent lymphocytotoxicity assays were performed 10+/-2 and 28+/-4 days after transplantation. Pre- and posttransplant antibody levels were relatively unchanged among Neg and B-pos FCXM patient groups. In contrast, patients with T-pos FCXM produced cytotoxic IgG against class I after transplantation, which may have contributed to the severe graft dysfunction experienced by this group. CONCLUSIONS: FCXM is a useful tool to stratify primary renal transplant candidates in terms of potential risk for severe rejection. Furthermore, demonstration of preoperative flow reactivity against class I may identify a subgroup of patients at risk for early elaboration of cytotoxic alloantibody.
机译:背景:针对I类抗原的细胞毒性IgG可能导致肾功能障碍或移植后衰竭。然而,通过流式细胞术交叉匹配测量的IgG的临床相关性存在争议。这项研究将术前细胞毒性交叉匹配阴性的肾移植患者的术前和术后血流反应性与临床结果相关联。方法:根据术前细胞毒性交叉匹配阴性(补体依赖性淋巴细胞毒性试验)的非致敏原发性肾移植患者(n = 157),根据流式细胞术交叉匹配(FCXM)测得的IgG反应性分层为FCXM阴性(Neg)对I类(T-pos FCXM)或II类(B-pos FCXM)抗原呈阳性。比较各组的早期排斥频率和1年移植物存活率。结果:患者分布为67%Neg,14%T-pos FCXM,14%B-pos FCXM和5%IgM FCXM。 Neg早期排斥的发生率为25 +/- 3%,T-和B-pos FCXM为51 +/- 3%(P <0.05)。 Neg与T-pos和B-pos FCXM的一年移植物存活率分别为97 +/- 3%和44 +/- 10%(P <0.05)和77 +/- 5%(P = 0.06)。仅在T-pos FCXM患者中发现需要血浆清除的排斥反应。在29例患者中,在移植后10 +/- 2天和28 +/- 4天进行了FCXM和补体依赖性淋巴细胞毒性试验。在Neg和B-pos FCXM患者组中,移植前和移植后抗体水平相对不变。相反,患有T-pos FCXM的患者在移植后产生了针对I类的细胞毒性IgG,这可能是导致该组严重的移植物功能障碍的原因。结论:就严重排斥反应的潜在风险而言,FCXM是一种有用的工具,可以对主要的肾脏移植候选者进行分层。此外,针对I类的术前血流反应性的证明可能会识别出具有早期制定细胞毒性同种抗体风险的患者亚组。

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