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移植后可溶性CD30水平的相对降低可预测接受三种不同免疫抑制方案的胰岛移植受者的急性移植功能。

Relative reductions in soluble CD30 levels post-transplant predict acute graft function in islet allograft recipients receiving three different immunosuppression protocols.

作者信息

Hire Kelly, Hering Bernhard, Bansal-Pakala Pratima

机构信息

Schulze Diabetes Institute, Department of Surgery, University of Minnesota, Minneapolis, MN 55455, USA.

出版信息

Transpl Immunol. 2010 Aug;23(4):209-14. doi: 10.1016/j.trim.2010.06.007. Epub 2010 Jun 22.

DOI:10.1016/j.trim.2010.06.007
PMID:20600901
Abstract

Despite advances in islet transplantation, challenges remain in monitoring for anti-islet immune responses. Soluble CD30 (sCD30) has been investigated as a predictor of acute rejection in kidney, lung, and heart transplantation as well as in a single study in human islet cell recipients. In this study, sCD30 levels were retrospectively assessed in 19 allograft recipients treated with three different immunosuppression induction therapies. Soluble CD30 levels were assessed at pre-transplant; early post-transplant (day 4-day 7); one-month post-transplant; and late post-transplant (day 90-day 120) and then correlated with eventual graft outcomes at 1-year follow-up. Results showed no correlation between mean serum sCD30 levels at any point in time pre- or post-transplant and graft function at 1-year follow-up. However, analysis demonstrated that mean sCD30 levels at day 28 or day 90-day 120 decreased from pre-transplant levels in recipients with long-term islet allograft function compared to recipients with partial or non-graft function (a decrease of 43.6+/-25.6% compared to 16.7+/-35.2%, p<0.05). In another finding, immunosuppression with the ATG protocol led to a greater reduction in sCD30 levels post-transplant overall. A larger reduction post-transplant correlated with full graft function. The results demonstrate that a relative reduction in sCD30 levels post-transplant may be applicable as a biomarker to monitor graft function in islet allograft recipients. Additionally, knowledge of the impact of various immunosuppression protocols on the timing and extent of changes in post-transplant sCD30 levels could aid in patient-specific tailoring of immunosuppression.

摘要

尽管胰岛移植取得了进展,但在监测抗胰岛免疫反应方面仍存在挑战。可溶性CD30(sCD30)已被研究作为肾、肺和心脏移植以及一项针对人类胰岛细胞接受者的单一研究中急性排斥反应的预测指标。在本研究中,对19例接受三种不同免疫抑制诱导治疗的同种异体移植受者的sCD30水平进行了回顾性评估。在移植前、移植后早期(第4天至第7天)、移植后1个月和移植后期(第90天至第120天)评估可溶性CD30水平,然后将其与1年随访时的最终移植结果相关联。结果显示,移植前或移植后任何时间点的平均血清sCD30水平与1年随访时的移植功能之间均无相关性。然而,分析表明,与部分或无移植功能的受者相比,长期胰岛同种异体移植功能受者在第28天或第90天至第120天的平均sCD30水平较移植前水平降低(分别为43.6±25.6%和16.7±35.2%,p<0.05)。另一项发现是,采用抗胸腺细胞球蛋白(ATG)方案进行免疫抑制导致移植后sCD30水平总体下降幅度更大。移植后更大幅度的下降与移植功能完全恢复相关。结果表明,移植后sCD30水平的相对降低可能作为一种生物标志物用于监测胰岛同种异体移植受者的移植功能。此外,了解各种免疫抑制方案对移植后sCD30水平变化的时间和程度的影响,有助于针对患者进行免疫抑制的个性化调整。

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