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Characterization of calcium binding properties of lithostathine

机译:利他他汀钙结合特性的表征

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摘要

The pancreas secretes primarily two types of metabolially important proteins: digestive enzymes and hormones. Lithostathine (LIT) is the only protein excreted from the pancreas that has no known digestive or hormonal activity. Human lithostathine is a 144-amino acid glycoprotein synthesized by the exocrine pancreas that has been implicated in various physiological functions, including inhibition of pancreatic stone formation. To better understand the physiological function of LIT, we expressed the recombinant LIT protein in Escherichia coli and measured its calcium binding properties by equilibrium dialysis and electron paramagnetic resonance (EPR) spectroscopy. Equilibrium dialysis with ~(45)Ca~(2+) showed that LIT binds Ca~(2+) with 1:1 stoichiometry. EPR studies using the divalent vanadyl (VO~(2+)) ion as a paramagnetic substitute for Ca~(2+) also showed that VO~(2+) binds to LIT with a metal: protein binding stoichiometry of 1:1 and that VO~(2+) competes with Ca~(2+) in binding to LIT. Mutations of a cluster of acidic residues on the molecular surface (E30A, D31A, E33A, D37A, D72A, and D73A) resulted in almost complete loss (95-100%) of binding of Ca~(2+) and VO~(2+), showing that these residues are critical for calcium binding by LIT.
机译:胰腺主要分泌两种重要的代谢蛋白质:消化酶和激素。 Lithostathine(LIT)是从胰腺排出的唯一蛋白,没有已知的消化或激素活性。人lithostathine是由外分泌胰腺合成的一种144个氨基酸的糖蛋白,与多种生理功能有关,包括抑制胰腺结石的形成。为了更好地了解LIT的生理功能,我们在大肠杆菌中表达了重组LIT蛋白,并通过平衡透析和电子顺磁共振(EPR)光谱测量了其钙结合特性。 〜(45)Ca〜(2+)的平衡透析显示LIT以1:1的化学计量比结合Ca〜(2+)。使用二价钒基(VO〜(2+))离子作为Ca〜(2+)的顺磁性替代物的EPR研究还显示,VO〜(2+)以1:1的金属:蛋白质结合化学计量与LIT结合。 VO〜(2+)与Ca〜(2+)竞争结合LIT。分子表面(E30A,D31A,E33A,D37A,D72A和D73A)上的酸性残基簇的突变导致Ca〜(2+)和VO〜(2)的结合几乎完全丧失(95-100%) +),表明这些残基对于LIT的钙结合至关重要。

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