首页> 美国卫生研究院文献>The Journal of Biological Chemistry >Lipocalin-2 (24p3/Neutrophil Gelatinase-associated Lipocalin (NGAL)) Receptor Is Expressed in Distal Nephron and Mediates Protein Endocytosis
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Lipocalin-2 (24p3/Neutrophil Gelatinase-associated Lipocalin (NGAL)) Receptor Is Expressed in Distal Nephron and Mediates Protein Endocytosis

机译:Lipocalin-2(24p3 / Neutrophil明胶酶相关的Lipocalin(NGAL))受体在远端肾单位表达并介导蛋白质内吞作用。

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摘要

In the kidney, bulk reabsorption of filtered proteins occurs in the proximal tubule via receptor-mediated endocytosis (RME) through the multiligand receptor complex megalin-cubilin. Other mechanisms and nephron sites for RME of proteins are unclear. Recently, the secreted protein 24p3 (lipocalin-2, neutrophil gelatinase-associated lipocalin (NGAL)), which is expressed in the distal nephron, has been identified as a sensitive biomarker of kidney damage. A high-affinity receptor for 24p3 (24p3R) that is involved in endocytotic iron delivery has also been cloned. We investigated the localization of 24p3R in rodent kidney and its role in RME of protein-metal complexes and albumin. Immunostaining of kidney tissue showed expression of 24p3R in apical membranes of distal tubules and collecting ducts, but not of proximal tubule. The differential expression of 24p3R in these nephron segments was confirmed in the respective cell lines. CHO cells transiently transfected with 24p3R or distal tubule cells internalized submicromolar concentrations of fluorescence-coupled proteins transferrin, albumin, or metallothionein (MT) as well as the toxic cadmium-MT (Cd2+7-MT) complex, which caused cell death. Uptake of MT or transferrin and Cd2+7-MT toxicity were prevented by picomolar concentrations of 24p3. An EC50 of 123 ± 50 nm was determined for binding of MT to 24p3R by microscale thermophoresis. Hence, 24p3R binds proteins filtered by the kidney with high affinity and may contribute to RME of proteins, including 24p3, and to Cd2+7-MT toxicity in distal nephron segments.
机译:在肾脏中,通过多配体受体复合物megalin-cubilin通过受体介导的内吞作用(RME)在近端小管中发生大量重吸收过滤蛋白。蛋白质RME的其他机制和肾单位位尚不清楚。最近,在远端肾单位表达的分泌蛋白24p3(lipocalin-2,与中性粒细胞明胶酶相关的lipocalin(NGAL))已被鉴定为肾脏损害的敏感生物标记。还克隆了参与胞吞铁传递的24p3(24p3R)高亲和力受体。我们调查了24p3R在啮齿动物肾脏中的定位及其在蛋白质金属复合物和白蛋白的RME中的作用。肾脏组织的免疫染色显示24p3R在远端小管和收集管的顶膜中表达,但在近端小管中不表达。在各个细胞系中证实了在这些肾单位区段中24p3R的差异表达。用24p3R瞬时转染的CHO细胞或远端小管细胞将亚微摩尔浓度的荧光偶联蛋白转铁蛋白,白蛋白或金属硫蛋白(MT)以及有毒的镉MT(Cd 2 + 7-MT)内在化复杂,导致细胞死亡。皮摩尔浓度的24p3可防止MT或运铁蛋白的摄取以及Cd 2 + 7-MT的毒性。通过微尺度热泳确定MT与24p3R的结合的EC 50为123±50nm。因此,24p3R以高亲和力结合被肾脏滤过的蛋白质,并且可能对包括24p3在内的蛋白质的RME产生作用,并导致远端肾单位节段的Cd 2 + 7-MT毒性。

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