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尿大分子对草酸钙晶体结构和细胞黏附的调控

Control of calcium oxalate crystal structure and cell adherence by urinary macromolecules.

作者信息

Wesson J A, Worcester E M, Wiessner J H, Mandel N S, Kleinman J G

机构信息

Nephrology Division, Medical College of Wisconsin, Milwaukee, USA.

出版信息

Kidney Int. 1998 Apr;53(4):952-7. doi: 10.1111/j.1523-1755.1998.00839.x.

Abstract

Crystal polymorphism is exhibited by calcium oxalates in nephrolithiasis, and we have proposed that a shift in the preferred crystalline form of calcium oxalate (CaOx) from monohydrate (COM) to dihydrate (COD) induced by urinary macromolecules reduces crystal attachment to epithelial cell surfaces, thus potentially inhibiting a critical step in the genesis of kidney stones. We have tested the validity of this hypothesis by studying both the binding of monohydrate and dihydrate crystals to renal tubule cells and the effect of macromolecular urinary solutes on crystal structure. Renal tubule cells grown in culture bound 50% more CaOx monohydrate than dihydrate crystals of comparable size. The effects of macromolecules on the spontaneous nucleation of CaOx were examined in HEPES-buffered saline solutions containing Ca2+ and C2O4(2-) at physiologic concentrations and supersaturation. Many naturally occurring macromolecules known to be inhibitors of crystallization, specifically osteopontin, nephrocalcin and urinary prothrombin fragment 1, were found to favor the formation of calcium oxalate dihydrate in this in vitro system, while other polymers did not affect CaOx crystal structure. Thus, the natural defense against nephrolithiasis may include impeding crystal attachment by an effect of macromolecular inhibitors on the preferred CaOx crystal structure that forms in urine.

摘要

肾结石中的草酸钙存在晶体多态性,我们提出,尿液中的大分子物质可使草酸钙(CaOx)的优势晶型从一水合物(COM)转变为二水合物(COD),这会减少晶体与上皮细胞表面的附着,从而可能抑制肾结石形成过程中的关键步骤。我们通过研究一水合物晶体和二水合物晶体与肾小管细胞的结合情况以及尿液中大分子溶质对晶体结构的影响,来验证这一假设。培养的肾小管细胞对大小相当的CaOx一水合物晶体的结合量比对二水合物晶体的结合量多50%。在含有生理浓度和过饱和度的Ca2+和C2O4(2-)的HEPES缓冲盐溶液中,研究了大分子对CaOx自发成核的影响。发现许多已知的天然结晶抑制剂大分子,特别是骨桥蛋白、肾钙蛋白和尿凝血酶原片段1,在这个体外系统中有利于草酸钙二水合物的形成,而其他聚合物则不影响CaOx晶体结构。因此,预防肾结石的天然防御机制可能包括大分子抑制剂通过影响尿液中形成的优势CaOx晶体结构来阻碍晶体附着。

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