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Selective protein enrichment in calcium oxalate stone matrix: a window to pathogenesis?选择性蛋白质在草酸钙结石基质中的富集:发病机制的窗口?
Urolithiasis. 2019 Dec;47(6):521-532. doi: 10.1007/s00240-019-01131-3. Epub 2019 Apr 16.
2
Analyses of long non-coding RNA and mRNA profiling using RNA sequencing in calcium oxalate monohydrate-stimulated renal tubular epithelial cells.采用 RNA 测序分析草酸钙一水合物刺激的肾小管上皮细胞中的长非编码 RNA 和 mRNA 谱。
Urolithiasis. 2019 Jun;47(3):225-234. doi: 10.1007/s00240-018-1065-7. Epub 2018 Jun 15.
3
Stone former urine proteome demonstrates a cationic shift in protein distribution compared to normal.结石形成者尿液蛋白质组与正常相比表现出阳离子分布的偏移。
Urolithiasis. 2017 Aug;45(4):337-346. doi: 10.1007/s00240-017-0969-y. Epub 2017 Mar 17.
4
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5
Label-free proteomic methodology for the analysis of human kidney stone matrix composition.用于分析人肾结石基质成分的无标记蛋白质组学方法。
Proteome Sci. 2016 Feb 27;14:4. doi: 10.1186/s12953-016-0093-x. eCollection 2016.
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Prevalence of kidney stones in the United States.美国肾结石的患病率。
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10
Urolithiasis through the ages: data on more than 200,000 urinary stone analyses.尿石症的历史演变:20 多万例尿石分析数据。
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探讨蛋白质影响草酸钙肾结石形成的机制。

Exploring mechanisms of protein influence on calcium oxalate kidney stone formation.

机构信息

Division of Nephrology, Department of Medicine, Medical College of Wisconsin, 9200 W Wisconsin Avenue, Milwaukee, WI, 53295, USA.

Department of Biomedical Engineering, Max McGee National Research Center, Cardiovascular Center, Center for Advancing Population Science, Medical College of Wisconsin and Marquette University, 8701 Watertown Plank Road, Milwaukee, WI, 53226, USA.

出版信息

Urolithiasis. 2021 Aug;49(4):281-290. doi: 10.1007/s00240-021-01247-5. Epub 2021 Feb 15.

DOI:10.1007/s00240-021-01247-5
PMID:33587148
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8316271/
Abstract

Calcium oxalate monohydrate (COM) crystals are the primary constituent of most kidney stones, but urine proteins in stone matrix are believed to be critical elements for stone formation from these crystals. Recent data have shown that hundreds of proteins appear in the stone matrix with no explanation for inclusion of so many proteins. We have proposed a stone formation model with protein stimulated COM aggregation based on polyanion-polycation aggregation, which is supported by finding that matrix is highly enriched in strongly anionic and strongly cationic proteins. Many other proteins may be drawn to such aggregates due to their limited solubility in water or charge effects. Finding similar protein enrichment in both polyarginine (pR) induced aggregates of urine proteins and COM stone matrix would support this hypothesis. Purified proteins (PP) were obtained from random urine samples of six healthy adults by ultradiafiltration. Protein aggregation was induced by adding pR to PP solutions at two concentrations; 0.25 and 0.5 µg pR/µg of PP. Samples of each fraction and the original PP mixture were lyophilized and analyzed by tandem mass spectrometry. Aggregates induced by pR addition to PP samples collected a protein mixture that mimicked the protein distribution observed in COM matrix, supporting our hypothesis. The apparently discordant behavior of certain abundant anionic proteins preferentially joining the pR aggregate, when they had demonstrated reduced abundance in COM stone matrix, suggests that this model was overdriven to aggregate. The reversal of aggregate preference of albumin at low pR addition supports this interpretation.

摘要

一水合草酸钙 (COM) 晶体是大多数肾结石的主要成分,但尿液蛋白被认为是这些晶体形成结石的关键因素。最近的数据表明,有数百种蛋白质出现在结石基质中,对于如此多的蛋白质被包含在内,没有任何解释。我们提出了一种基于聚阴离子-聚阳离子聚集的蛋白刺激 COM 聚集的结石形成模型,这一模型得到了支持,因为发现基质中富含强阴离子和强阳离子蛋白。由于其在水中的溶解度有限或电荷效应,许多其他蛋白质可能会被吸引到这样的聚集体中。在多聚精氨酸 (pR) 诱导的尿液蛋白和 COM 结石基质的聚集物中发现类似的蛋白富集,将支持这一假设。通过超滤从 6 名健康成年人的随机尿液样本中获得纯化蛋白 (PP)。通过向 PP 溶液中添加 pR 来诱导蛋白聚集,pR 的添加浓度为 0.25 和 0.5μg pR/μg PP。对每个级分的样品和原始 PP 混合物进行冻干,并通过串联质谱分析。pR 添加到 PP 样品中诱导的聚集物产生了一种类似于 COM 基质中观察到的蛋白分布的蛋白混合物,支持了我们的假设。某些丰富的阴离子蛋白的行为明显不一致,它们优先与 pR 聚集物结合,而在 COM 结石基质中的丰度降低,这表明该模型的聚集过度驱动。在低 pR 添加时白蛋白聚集偏好的逆转支持了这一解释。