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Selective urinary excretion of phosphatidyl ethanolamine in patients with chronic glomerular diseases
Authors:Keiji Mimura  Susumu Yukawa  Takao Maeda  Masahiro Kinoshita  Yoichi Yamada  Yasushi Saika  Toshihiko Miyai  Masayoshi Nagae  Masatoshi Mune  Hiroshi Nomoto
Institution:Department of Internal Medicine (Division of Metabolism), Wakayama Medical College, Wakayama, Japan.
Abstract:Urinary phospholipids and lipoproteins in chronic glomerular diseases were analyzed. The subjects used were 26 patients consisting of 14 with chronic glomerulonephritis and 12 with nephrotic syndrome. Nine healthy normals served as controls. Phospholipids were isolated by one-dimensional thin-layer chromatography (TLC) using an internal standard for quantification and partially by two-dimensional TLC and, furthermore, quantified by two different methods to ascertain the kinds of phospholipids. Urinary lipoproteins were isolated by density gradient ultracentrifugation and analyzed by electrophoresis. The urinary excretion of phosphatidyl ethanolamine (PE) was recognized exclusively in the patient group and that of phosphatidyl serine (PS) in most cases with nephrotic syndrome. The daily urinary PE excretion rate was closely correlated to the urinary albumin excretion rate. However, phosphatidyl choline (PC) and sphingomyelin (SPH), which are main phospholipids in serum and red blood cell membranes, in most cases were hardly detected in urine. These observations were confirmed by two-dimensional TLC using valuable spot tests for identification of phospholipids and also by the two different quantification methods. In density gradient ultracentrifugation, urinary lipoproteins did not form such peaks as seen in the profiles of serum lipoproteins. The presence of urinary lipoproteins in two nephrotic patients has been shown, but although the method used was not very sensitive, it was suggested that lipoproteins were hardly excreted into urine as the lipoprotein deficient fraction (LPDF) (d > 1.21 g/ml), in which albumin is predominant. PE was found mainly in LPDF of urine, although the amount of PE in urinary lipoproteins was very limited. These data gave a basis for a postulate that the urinary excretion of PE may not be related to the excretion of lipoproteins but to LPDF albumins. From the practical absence of PC and SPH in urine, it was further postulated that choline-containing phospholipids (PC, SPH) may not have been excreted in sufficient quantities in these patients.
Keywords:Address reprint requests to Dr K  Mimura  Department of Internal Medicine (Division of Metabolism)  Wakayama Medical College  7-Bancho-1  Wakayama 640  Japan  
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