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马心卟啉细胞色素c的光谱研究。

Spectral studies of horse heart porphyrin cytochrome c.

作者信息

Strottmann J M, Stellwagen A, Bryant C, Stellwagen E

出版信息

J Biol Chem. 1984 Jun 10;259(11):6931-6.

PMID:6327700
Abstract

Removal of the heme iron from cytochrome c to generate porphyrin cytochrome c relieves the quenching of porphyrin fluorescence and enhances the fluorescence of the single tryptophan residue and the 4 tyrosine residues. The intensity of the porphyrin fluorescence is not perturbed by denaturation of the protein at neutral pH using either urea or guanidine hydrochloride. However, the amplitude of tryptophan fluorescence is increased by these denaturants from 5 to about 85% of a model tryptophan residue using solutions of 2 microM tryptophan. In contrast to cytochrome c, the tryptophan fluorescence amplitude of denatured porphyrin cytochrome c is independent of pH over the range pH 3.0 to 7.4. Acidification of solutions of either native or denatured porphyrin cytochrome c markedly alters both the visible absorbance and fluorescence of the protein consistent with protonation of two pyrrole nitrogens on the porphyrin. Preliminary analysis of the spectral changes occurring in the acid transition suggests the presence of an intermediate form having only one of these two pyrrole nitrogens protonated.

摘要

从细胞色素c中去除血红素铁以生成卟啉细胞色素c,可消除卟啉荧光的猝灭,并增强单个色氨酸残基和4个酪氨酸残基的荧光。使用尿素或盐酸胍在中性pH下使蛋白质变性,不会干扰卟啉荧光的强度。然而,使用2 microM色氨酸溶液时,这些变性剂会使色氨酸荧光的幅度从5%增加到模型色氨酸残基的约85%。与细胞色素c不同,变性的卟啉细胞色素c的色氨酸荧光幅度在pH 3.0至7.4范围内与pH无关。天然或变性的卟啉细胞色素c溶液的酸化会显著改变蛋白质的可见吸收和荧光,这与卟啉上两个吡咯氮的质子化一致。对酸转变过程中发生的光谱变化的初步分析表明,存在一种中间形式,其中只有这两个吡咯氮中的一个被质子化。

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