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单氟磷酸酯与α2-巨球蛋白和C3的结合。

Binding of monofluorophosphate to alpha2-macroglobulin and C3.

作者信息

Rigalli A, Esteban L, Pera L, Puche R C

机构信息

Laboratorio de Biología Osea, Facultad de Ciencias Mèdicas, Universidad Nacional de Rosario, Argentina.

出版信息

Calcif Tissue Int. 1997 Jan;60(1):86-9. doi: 10.1007/s002239900190.

Abstract

After administering an oral dose of monofluorophosphate (MFP) to human beings or rats, a fraction of the drug appears in plasma that is bound to proteins, establishing a previously undetected compartment of nondiffusible fluoride. This article documents experiments performed in vitro, describing the binding of MFP to two plasma globulins: alpha2-macroglobulin and C3 (a beta-globulin). MFP binds irreversibly to these proteins through a stable bond. MFP binds to purified alpha2-macroglobulin or to C3 with a molar ratio MFP: protein close to unity. MFP binding reduces significantly the biological activity of these proteins, which share in common a macrocyclic 4-residue ring thiolactone (Cys-Gly-Glu-Glu). The binding site of MFP is as yet unknown. Protein-bound MFP appeared in the plasma of volunteers during the 5-7 hours following intake. Peak concentration of protein-bound MFP and maximal reduction of alpha2-macroglobulin activity was observed 2 hours after intake. Clearance of protein-bound MFP coincided with the return of alpha2-macroglobulin to basal levels.

摘要

给人类或大鼠口服单氟磷酸酯(MFP)后,血浆中会出现一部分与蛋白质结合的药物,从而形成了一个之前未被检测到的不可扩散氟化物区室。本文记录了体外实验,描述了MFP与两种血浆球蛋白的结合情况:α2-巨球蛋白和C3(一种β球蛋白)。MFP通过稳定的键与这些蛋白质不可逆地结合。MFP以接近1的MFP:蛋白质摩尔比与纯化的α2-巨球蛋白或C3结合。MFP结合显著降低了这些蛋白质的生物活性,这些蛋白质共同具有一个大环4残基环硫内酯(半胱氨酸-甘氨酸-谷氨酸-谷氨酸)。MFP的结合位点尚不清楚。摄入后5至7小时内,志愿者血浆中出现了与蛋白质结合的MFP。摄入后2小时观察到与蛋白质结合的MFP的峰值浓度以及α2-巨球蛋白活性的最大降低。与蛋白质结合的MFP的清除与α2-巨球蛋白恢复到基础水平同时发生。

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