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一顿饱腹感餐对正常和病态肥胖受试者血清及尿液中前脂肪酶原肽浓度的影响。

Effect of a satiating meal on the concentrations of procolipase propeptide in the serum and urine of normal and morbidly obese subjects.

作者信息

Bowyer R C, Rowston W M, Jehanli A M, Lacey J H, Hermon-Taylor J

机构信息

Department of Surgery, St George's Hospital Medical School, London.

出版信息

Gut. 1993 Nov;34(11):1520-5. doi: 10.1136/gut.34.11.1520.

Abstract

The effect of a satiating meal on the serum and urinary concentrations of procolipase propeptide (Ala-Pro-Gly-Pro-Arg, APGPR) immunoreactivity, as measured by enzyme linked immunosorbent assay (ELISA) specific for free APGPR, has been studied in normal and morbidly obese human subjects. The normal subjects displayed a biphasic response with coordinate increases in both serum and urine APGPR immunoreactivity both occurring within the first two hours after the meal. In two of three of the morbidly obese subjects, this early rise in APGPR concentration in urine was not seen but was followed by a slow rise in urinary APGPR immunoreactivity at four to six hours. In both the normal and obese groups, the urinary immunoreactive signal was found to coelute with synthetic APGPR on gel chromatography. In rats, procolipase propeptide (Val-Pro-Asp-Pro-Arg, VPDPR) specifically inhibits fat intake early in the postprandial period when given peripherally or centrally. This study suggests that in humans APGPR reaches the circulation shortly after feeding and is excreted in the urine. These findings are consistent with the hypothesis that human procolipase propeptide may also act as a satiety signal. In addition the late appearance of the peptide in some of the morbidly obese patients could be associated with perturbation of appetite control in these subjects.

摘要

通过针对游离前胶原酶原肽(Ala-Pro-Gly-Pro-Arg,APGPR)的酶联免疫吸附测定(ELISA),研究了一顿饱腹感餐对正常和病态肥胖人类受试者血清及尿液中APGPR免疫反应性浓度的影响。正常受试者呈现双相反应,餐后两小时内血清和尿液中APGPR免疫反应性均相应增加。在三名病态肥胖受试者中的两名中,未观察到尿液中APGPR浓度的早期升高,但在四至六小时时尿液中APGPR免疫反应性出现缓慢升高。在正常组和肥胖组中,凝胶色谱法显示尿液免疫反应信号与合成APGPR共洗脱。在大鼠中,前胶原酶原肽(Val-Pro-Asp-Pro-Arg,VPDPR)经外周或中枢给药时,在餐后早期可特异性抑制脂肪摄入。本研究表明,在人类中,APGPR在进食后不久进入循环并经尿液排泄。这些发现与人类前胶原酶原肽可能也作为饱腹感信号的假设一致。此外,该肽在一些病态肥胖患者中的延迟出现可能与这些受试者食欲控制的紊乱有关。

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本文引用的文献

1
The existence of pro-colipase in pancreatic juice.胰液中前磷脂酶的存在。
Biochim Biophys Acta. 1981 Nov 23;666(2):299-300. doi: 10.1016/0005-2760(81)90121-1.
3
Evolutionary studies on pancreatic colipase.胰腺辅脂酶的进化研究
Biochim Biophys Acta. 1983 Feb 7;750(2):340-5. doi: 10.1016/0005-2760(83)90038-3.
6
Cephalic phase of pancreatic secretion in man.人类胰腺分泌的头期
Gut. 1968 Apr;9(2):214-21. doi: 10.1136/gut.9.2.214.
10
A self-rating scale for bulimia. The 'BITE'.一种贪食症自评量表。“BITE”量表。
Br J Psychiatry. 1987 Jan;150:18-24. doi: 10.1192/bjp.150.1.18.

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