首页> 外文期刊>Bone marrow transplantation >Anti-CD13 Abs in children with extensive chronic GVHD and their relation to soluble CD13 after allogeneic blood and marrow transplantation from a Children's Oncology Groups Study, ASCT0031.
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Anti-CD13 Abs in children with extensive chronic GVHD and their relation to soluble CD13 after allogeneic blood and marrow transplantation from a Children's Oncology Groups Study, ASCT0031.

机译:来自儿童肿瘤学小组研究(ASCT0031)的同种异体血液和骨髓移植后患有广泛性慢性GVHD的儿童的抗CD13抗体及其与可溶性CD13的关系。

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Our group previously demonstrated a strong association between elevated plasma soluble CD13 enzyme activity and newly diagnosed extensive chronic GVHD (cGVHD) in children. As cytotoxic anti-CD13 Abs have been documented after blood and marrow transplant (BMT) in association with CMV infection and cGVHD, we hypothesized that soluble CD13 contributes to cGVHD pathogenesis by induction of CD13 reactive Abs and that anti-CD13 Abs could be additional biomarkers for newly diagnosed pediatric extensive cGVHD. Using prospectively collected plasma samples from pediatric allogeneic BMT (allo-BMT) subjects with cGVHD and controls without cGVHD enrolled in a large multi-institution Children's Oncology Group cGVHD therapeutic trial, we evaluated whether soluble CD13 correlates with induction of anti-CD13 Abs. We found that CD13 reactive Abs are present in a proportion of patients after allo-BMT, but did not seem to correlate with the presence of soluble CD13. Anti-CD13 Abs also did not meet our criteria as a diagnostic biomarker for cGVHD. These data do not confirm that induction of CD13 reactive Abs is a mechanism for cGVHD in children nor are part of the pathogenesis of cGVHD associated with elevated soluble CD13. The exact role of CD13 in cGVHD remains to be determined.
机译:我们的研究小组以前证明血浆可溶性CD13酶活性升高与新诊断的儿童广泛性慢性GVHD(cGVHD)之间有很强的联系。由于已经在与CMV感染和cGVHD相关的血液和骨髓移植(BMT)后记录了细胞毒性抗CD13 Abs,我们假设可溶性CD13通过诱导CD13反应性Abs促成cGVHD发病机理,并且抗CD13 Abs可能是其他生物标记物用于新诊断的小儿广泛性cGVHD。使用参加大型多机构儿童肿瘤小组cGVHD治疗试验的,有cGVHD的小儿同种BMT(allo-BMT)受试者的前瞻性采集血浆样品,我们评估了可溶性CD13是否与抗CD13抗体的诱导相关。我们发现异基因BMT后一部分患者中存在CD13反应性抗体,但似乎与可溶性CD13的存在无关。抗CD13抗体也不能满足我们作为cGVHD诊断生物标志物的标准。这些数据并未证实CD13反应性Abs的诱导是儿童cGVHD的机制,也不是与可溶性CD13升高相关的cGVHD发病机理的一部分。 CD13在cGVHD中的确切作用尚待确定。

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