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正常人和肾病患者中备解素的代谢

Metabolism of properdin in normal subjects and patients with renal disease.

作者信息

Ziegler J B, Rosen F S, Alper C A, Grupe W, Lepow I H

出版信息

J Clin Invest. 1975 Sep;56(3):761-7. doi: 10.1172/JCI108147.

Abstract

Properdin deposition has been recognized in glomeruli of patients with acute and chronic nephritis and lupus nephritis, and low serum properdin levels have been found in these disorders. These findings suggest that properdin may be involved in the production of glomerular damage and that low properdin levels may be due to hypercatabolism. The study was designed to examine the metabolism of properdin in normal subjects and to look for an abnormality in five patients with systemic lupus erythematosus with renal involvement and in six patients with membranoproliferative glomerulonephritis or dense deposit disease (MPGN). Highly purified human properdin was prepared by elution from zymosan, followed by DEAE-cellulose and carboxymethyl-Sephadex chromatography, and labeled with 125I by the iodine monochloride method. Parameters of metabolism were determined by monitoring plasma and urinary radioactivity at frequent intervals after the intravenous injection of 1-2 muCi of labeled material. The fractional catabolic rate (FCR) of properdin in normal subjects was found to have a very narrow range of 0.78-1.0,% of the plasma pool per hour (mean 0.95%). In systemic lupus erythematosus, the FCR was regularly elevated with a range of 1.21-2.30% (mean 1.70%). In MPGN, FCR was elevated in three patients (1.22, 1.94, and 2.08%) and within or below the normal range in three (0.78, 1.00, and 1.00%). Properdin levels were reduced in two patients who had the highest FCR's noted in the study. Properdin synthetic rates in normals varied from 4.1 to 14.3 mug/kg per h (mean 9.1) and was not found to be reduced in any patient. Properdin catabolism was found to be normal in a patient deficient in the C3b inactivator. These studies show that properdin is hypercatabolized in patients with renal disease and that decreased properdin levels when they occur in these patients can be entirely explained on the basis of this hypercatabolism.

摘要

在急性和慢性肾炎以及狼疮性肾炎患者的肾小球中已发现备解素沉积,并且在这些疾病中发现血清备解素水平较低。这些发现表明备解素可能参与肾小球损伤的产生,且低备解素水平可能是由于分解代谢亢进所致。本研究旨在检测正常受试者中备解素的代谢情况,并寻找5例有肾脏受累的系统性红斑狼疮患者以及6例膜增生性肾小球肾炎或致密物沉积病(MPGN)患者的异常情况。通过从酵母聚糖上洗脱,随后进行二乙氨基乙基纤维素和羧甲基葡聚糖凝胶色谱法制备高纯度的人备解素,并用一氯化碘法将其标记为125I。在静脉注射1 - 2μCi标记物质后,通过频繁监测血浆和尿液放射性来确定代谢参数。正常受试者中备解素的分解代谢率(FCR)每小时占血浆池的比例范围非常窄,为0.78 - 1.0%(平均0.95%)。在系统性红斑狼疮中,FCR有规律地升高,范围为1.21 - 2.30%(平均1.70%)。在MPGN中,3例患者的FCR升高(分别为1.22、1.94和2.08%),3例患者的FCR在正常范围内或低于正常范围(分别为0.78、1.00和1.00%)。在本研究中FCR最高的2例患者备解素水平降低。正常受试者中备解素的合成率为每小时4.1至14.3μg/kg(平均9.1),且未发现任何患者的合成率降低。在一名缺乏C3b灭活剂的患者中发现备解素分解代谢正常。这些研究表明,肾病患者的备解素分解代谢亢进,且这些患者中出现的备解素水平降低完全可以根据这种分解代谢亢进来解释。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f26f/301925/4b7bdc1ce9e8/jcinvest00171-0249-a.jpg

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