首页> 外文期刊>The Journal of Clinical Investigation: The Official Journal of the American Society for Clinical Investigation >Glomerular-specific alterations of VEGF-A expression lead to distinct congenital and acquired renal diseases.
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Glomerular-specific alterations of VEGF-A expression lead to distinct congenital and acquired renal diseases.

机译:VEGF-A 表达的肾小球特异性改变导致明显的先天性和后天性肾脏疾病。

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摘要

Kidney disease affects over 20 million people in the United States alone. Although the causes of renal failure are diverse, the glomerular filtration barrier is often the target of injury. Dysregulation of VEGF expression within the glomerulus has been demonstrated in a wide range of primary and acquired renal diseases, although the significance of these changes is unknown. In the glomerulus, VEGF-A is highly expressed in podocytes that make up a major portion of the barrier between the blood and urinary spaces. In this paper, we show that glomerular-selective deletion or overexpression of VEGF-A leads to glomerular disease in mice. Podocyte-specific heterozygosity for VEGF-A resulted in renal disease by 2.5 weeks of age, characterized by proteinuria and endotheliosis, the renal lesion seen in preeclampsia. Homozygous deletion of VEGF-A in glomeruli resulted in perinatal lethality. Mutant kidneys failed to develop a filtration barrier due to defects in endothelial cell migration, differentiation, and survival. In contrast, podocyte-specific overexpression of the VEGF-164 isoform led to a striking collapsing glomerulopathy, the lesion seen in HIV-associated nephropathy. Our data demonstrate that tight regulation of VEGF-A signaling is critical for establishment and maintenance of the glomerular filtration barrier and strongly supports a pivotal role for VEGF-A in renal disease.
机译:仅在美国,肾脏疾病就影响了2000多万人。虽然肾功能衰竭的病因多种多样,但肾小球滤过屏障往往是损伤的目标。肾小球内VEGF表达失调已在多种原发性和获得性肾脏疾病中得到证实,尽管这些变化的意义尚不清楚。在肾小球中,VEGF-A 在足细胞中高度表达,足细胞构成血液和尿路之间屏障的主要部分。在本文中,我们发现VEGF-A的肾小球选择性缺失或过表达会导致小鼠肾小球疾病。VEGF-A 的足细胞特异性杂合性导致 2.5 周龄时发生肾脏疾病,其特征是蛋白尿和内皮病,这是先兆子痫的肾脏病变。肾小球中VEGF-A的纯合缺失导致围产期致死。突变肾脏由于内皮细胞迁移、分化和存活缺陷而未能形成过滤屏障。相比之下,VEGF-164亚型的足细胞特异性过表达导致明显的塌陷性肾小球病,这是HIV相关肾病中的病变。我们的数据表明,VEGF-A 信号转导的严格调节对于肾小球滤过屏障的建立和维持至关重要,并有力地支持 VEGF-A 在肾脏疾病中的关键作用。

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