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人血清中正常及截短的全反式视黄醇结合蛋白(RBP)和脱辅基视黄醇结合蛋白的分析:慢性肾衰竭时比例的改变

Analysis of normal and truncated holo- and apo-retinol-binding protein (RBP) in human serum: altered ratios in chronic renal failure.

作者信息

Jaconi S, Saurat J H, Siegenthaler G

机构信息

Clinique de Dermatologie, Hôpital Cantonal Universitaire, Genève, Switzerland.

出版信息

Eur J Endocrinol. 1996 May;134(5):576-82. doi: 10.1530/eje.0.1340576.

Abstract

Retinol, the precursor of the retinoic acid hormone, is transported in the serum by a specific carrier, the retinol-binding protein (RBP). Compared to serum of healthy controls, the serum of patients with chronic renal failure (CRF) contains markedly increased levels of the RBP form truncated at the C terminal, des(182Leu-183Leu), (RBP2), which suggests that RBP2 is cleared by the kidney in healthy people but accumulates in serum of CRF patients (Jaconi S, et al. J Lipid Res 1995:36:1247-53). To understand better the mechanism of retinol transport, we have developed a new analytical strategy to analyze the various forms of RBP that circulate in the blood: RBP with and without retinol (holo- and apo-RBP, respectively), RBP bound or not to transthyretin (TTR) and to determine in which of these forms RBP2 circulates. We confirm, but now by direct measurement, that holo-RBP and, to a larger extent, apo-RBP are increased in CRF serum compared to normal serum. We also show that almost all apo-RBP and about 50% of total holo-RBP, corresponding to RBP excess in CRF serum, circulate free and are not complexed to TTR, the remaining 50% being complexed to TTR. This observation suggests that the high levels of free holo-RBP, not bound to TTR, which correspond to the increase in total RBPs measured in CRF serum, may alter the tissue uptake of retinol and be responsible for the signs of hypervitaminosis A observed in these patients. Secondly, we found that the truncation resulting in RBP2 does not alter its binding properties for retinol nor those of holo-RBP2 for TTR. We observed that the high amounts of free holo-RBP2 and holo-RBP in sera of CRF patients were low in normal serum, suggesting that these forms are cleared by the kidney in normal conditions. The possible role of free holo-RBPs is discussed in the context of retinol recycling.

摘要

视黄醇是维甲酸激素的前体,它在血清中由一种特定的载体——视黄醇结合蛋白(RBP)进行转运。与健康对照者的血清相比,慢性肾衰竭(CRF)患者的血清中C末端截短的RBP形式,即去(182Leu - 183Leu)(RBP2)水平显著升高,这表明RBP2在健康人群中由肾脏清除,但在CRF患者的血清中蓄积(Jaconi S等人,《脂质研究杂志》1995年:36:1247 - 53)。为了更好地理解视黄醇转运机制,我们开发了一种新的分析策略来分析血液中循环的各种RBP形式:结合视黄醇和未结合视黄醇的RBP(分别为全RBP和脱辅基RBP)、结合或未结合甲状腺素转运蛋白(TTR)的RBP,并确定RBP2以哪种形式循环。我们通过直接测量证实,与正常血清相比,CRF血清中的全RBP,以及在更大程度上的脱辅基RBP有所增加。我们还表明,几乎所有的脱辅基RBP以及约50%的总全RBP(对应于CRF血清中的RBP过量)以游离形式循环,未与TTR形成复合物,其余50%与TTR形成复合物。这一观察结果表明,未与TTR结合的高水平游离全RBP(对应于CRF血清中测量到的总RBP增加)可能会改变视黄醇的组织摄取,并导致这些患者出现维生素A过多症的症状。其次,我们发现导致RBP2的截短并未改变其对视黄醇的结合特性,也未改变全RBP2对TTR的结合特性。我们观察到,CRF患者血清中大量的游离全RBP2和全RBP在正常血清中含量较低,这表明这些形式在正常情况下由肾脏清除。在视黄醇循环的背景下讨论了游离全RBP的可能作用。

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