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直接高效液相色谱分析揭示质子化对同分异构视黄醛的正丁胺席夫碱异构化性质的影响:视黄醛蛋白对异构化途径的选择

Effect of protonation on the isomerization properties of n-butylamine Schiff base of isomeric retinal as revealed by direct HPLC analyses: selection of isomerization pathways by retinal proteins.

作者信息

Koyama Y, Kubo K, Komori M, Yasuda H, Mukai Y

机构信息

Faculty of Science, Kwansei Gakuin University, Nishinomiya, Japan.

出版信息

Photochem Photobiol. 1991 Sep;54(3):433-43. doi: 10.1111/j.1751-1097.1991.tb02038.x.

Abstract

Alumina adsorption chromatography and ion-pair reversed-phase chromatography were developed to analyze the isomers of unprotonated and protonated n-butylamine Schiff base of retinal (RSB and PRSB), respectively. Photoisomerization starting from the all-trans, 11-cis and 13-cis isomers was traced for RSB in n-hexane, acetonitrile, methanol and 1-butanol, and for PRSB in methanol, acetonitrile and 1-butanol. The quantum yields of photoisomerization for the all-trans, 9-cis, 11-cis and 13-cis isomers were determined for RSB and PRSB in the above solvents except 1-butanol. On the other hand, photoisomerization of isomeric retinal bound (through Schiff base linkage) to bovine serum albumin (RBSA) in aqueous solution (pH 3, 7 and 12) as well as thermal isomerization of RSB (in n-hexane), PRSB (in methanol) and RBSA (in aqueous solution, pH 7) were traced starting from the all-trans, 11-cis, and 13-cis isomers. Protonation of RSB drastically changes the pathway of photoisomerization and increases the quantum yields of isomeric RSB. The solvent polarity increases the quantum yields of RSB differently depending on the configuration. Protonation enhances thermal isomerization also. The results of the above model systems are compared with those of retinal proteins to rationalize their selection of the particular isomerization pathways.

摘要

分别开发了氧化铝吸附色谱法和离子对反相色谱法来分析视网膜未质子化和质子化正丁胺席夫碱(RSB和PRSB)的异构体。追踪了在正己烷、乙腈、甲醇和1-丁醇中的RSB以及在甲醇、乙腈和1-丁醇中的PRSB从全反式、11-顺式和13-顺式异构体开始的光异构化过程。测定了在上述除1-丁醇外的溶剂中RSB和PRSB的全反式、9-顺式、11-顺式和13-顺式异构体的光异构化量子产率。另一方面,追踪了在水溶液(pH 3、7和12)中通过席夫碱键与牛血清白蛋白结合的异构化视网膜(RBSA)的光异构化过程,以及从全反式、11-顺式和13-顺式异构体开始的RSB(在正己烷中)、PRSB(在甲醇中)和RBSA(在pH 7的水溶液中)的热异构化过程。RSB的质子化极大地改变了光异构化途径并提高了异构化RSB的量子产率。溶剂极性根据构型不同程度地增加了RSB的量子产率。质子化也增强了热异构化。将上述模型系统的结果与视网膜蛋白的结果进行比较,以合理化它们对特定异构化途径的选择。

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