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人凝血酶原的尿F1激活肽在体外对未稀释的人尿中的草酸钙结晶具有强效抑制作用。

The urinary F1 activation peptide of human prothrombin is a potent inhibitor of calcium oxalate crystallization in undiluted human urine in vitro.

作者信息

Ryall R L, Grover P K, Stapleton A M, Barrell D K, Tang Y, Moritz R L, Simpson R J

机构信息

Department of Surgery, Flinders Medical Centre, Bedford Park, Australia.

出版信息

Clin Sci (Lond). 1995 Nov;89(5):533-41. doi: 10.1042/cs0890533.

Abstract
  1. The urinary F1 activation peptide of prothrombin is the predominant protein incorporated into calcium oxalate crystals precipitated from human urine. The aim of this study was to examine the effect of pure urinary prothrombin F1 on calcium oxalate crystallization in human urine. 2. Urinary prothrombin F1 was purified from demineralized calcium oxalate crystals precipitated from human urine, and its effects on calcium oxalate crystallization induced by addition of an oxalate load were tested in undiluted, ultrafiltered urine from healthy men, at final concentrations of 0 to 10 mg/l. 3. Urinary prothrombin F1 did not affect the amount of oxalate required to induce crystallization, but the volume of material deposited increased in proportion to increasing concentrations of urinary prothrombin F1. However, the mean particle size decreased in reverse order: this was confirmed by scanning electron microscopy, which showed it to be the result of a reduction in crystal aggregation rather than in the size of individual crystals. Analysis of 14C-oxalate data revealed a dose-dependent decrease in calcium oxalate deposition with an increase in urinary prothrombin F1 concentration, indicating that the increase in particle volume recorded by the Coulter Counter resulted from inclusion of urinary prothrombin F1 into the crystalline architecture, rather than increased deposition of calcium oxalate. 4. It was concluded that urinary prothrombin F1 may be an important macromolecular determinant of stone formation.
摘要
  1. 凝血酶原的尿F1激活肽是从人尿中沉淀出的草酸钙晶体中所含的主要蛋白质。本研究的目的是检测纯尿凝血酶原F1对人尿中草酸钙结晶的影响。2. 从人尿中沉淀出的脱矿质草酸钙晶体中纯化尿凝血酶原F1,并在来自健康男性的未稀释、超滤尿中测试其对添加草酸盐负荷诱导的草酸钙结晶的影响,最终浓度为0至10mg/l。3. 尿凝血酶原F1不影响诱导结晶所需的草酸盐量,但沉积物质的体积随尿凝血酶原F1浓度的增加成比例增加。然而,平均粒径呈相反顺序减小:扫描电子显微镜证实了这一点,表明这是晶体聚集减少而非单个晶体尺寸减小的结果。对14C-草酸盐数据的分析显示,随着尿凝血酶原F1浓度的增加,草酸钙沉积呈剂量依赖性减少,这表明库尔特计数器记录的颗粒体积增加是由于尿凝血酶原F1纳入晶体结构,而非草酸钙沉积增加。4. 得出的结论是,尿凝血酶原F1可能是结石形成的重要大分子决定因素。

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