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首页> 外文期刊>Urological research >Is enalapril adequate for the prevention of renal tissue damage caused by unilateral ureteral obstruction and/or hyperoxaluria?
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Is enalapril adequate for the prevention of renal tissue damage caused by unilateral ureteral obstruction and/or hyperoxaluria?

机译:依那普利是否足以预防单侧输尿管阻塞和/或高草酸尿引起的肾组织损害?

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摘要

Unilateral ureteral obstruction (UUO) and hyperoxaluria (HOX) can lead to end-stage renal disease with tubulointerstitial fibrosis. We investigated the effects of enalapril (E), an ACE-inhibitor, on rat kidneys with either UUO or HOX. Sham-operated, UUO, HOX, UUO+HOX, UUO+E and HOX+E rats were killed 14 days after UUO and/or HOX was initiated. Rat kidney sections were histologically scored for tissue damage and monocyte/macrophage infiltration was demonstrated with ED1 antibody and measured by computer image analysis software. Serious glomerular and tubulointerstitial damage was found for UUO and HOX, consisting of glomerular basement membrane thickening, tubular dilatation/collapse, tubular basement membrane thickening and the infiltration of mononuclear leucocytes (mainly macrophages). For HOX, calcium oxalate crystals were visible. Neither the scored histological parameters nor monocyte/macrophage infiltration was significantly decreased when E-treated were compared with untreated groups. We conclude that E did not ameliorate the parameters scored in either UUO or HOX. This being contrary to findings by other research groups, we hypothesize that E may be effective only in short-term UUO/HOX, with transforming growth factor, TGF-beta1, formation becoming partly independent of Ang II in late-stage UUO/HOX, or other fibrogenic cytokines than TGF-beta1 becoming predominant.
机译:单侧输尿管梗阻(UUO)和高草酸尿症(HOX)可以导致末期肾病并伴有肾小管间质纤维化。我们调查了依那普利(E),一种ACE抑制剂对UUO或HOX对大鼠肾脏的影响。假手术的UUO,HOX,UUO + HOX,UUO + E和HOX + E大鼠在UUO和/或HOX启动后14天被处死。从组织学上对大鼠肾脏切片进行组织损伤评分,并用ED1抗体证明单核细胞/巨噬细胞浸润并通过计算机图像分析软件进行测量。发现UUO和HOX严重的肾小球和肾小管间质损害,包括肾小球基底膜增厚,肾小管扩张/塌陷,肾小管基底膜增厚和单核白细胞(主要是巨噬细胞)浸润。对于HOX,草酸钙晶体是可见的。与未经治疗的组相比,经E处理的评分组织学参数和单核细胞/巨噬细胞浸润均未显着降低。我们得出的结论是,E并没有改善UUO或HOX中得分的参数。这与其他研究小组的发现相反,我们假设E可能仅对短期UUO / HOX有效,而转化生长因子TGF-beta1的形成在后期的UUO / HOX中部分独立于Ang II,或TGF-beta1以外的其他成纤维细胞因子占主导地位。

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