Comparing the interactions of nitrendipine with lysozyme or human serum albumin and the effects of vitamin C and naringin on these interactions by spectroscopy and molecular docking methods

Author:

Meng Xianxin1,Nan Guanjun1,Du Yan1,Zhao Hongwen1,Zheng Hongxia1,Lin Rong2,Yang Guangde1ORCID

Affiliation:

1. School of Pharmacy Xi'an Jiaotong University Xi'an Shaanxi China

2. School of Basic Medical Sciences Xian Jiaotong University Xi'an Shaanxi China

Abstract

AbstractThe interactions between drugs and proteins play a pivotal role in determining the pharmacological effects and disposition of drugs within the human body. This study focuses on exploring the interaction between nitrendipine and lysozyme/human serum albumin. Spectroscopic analysis indicated a compound static quenching, indicative of the formation of stable complexes between the drug and proteins. The addition of vitamin C or naringin resulted in a decrease of the binding constant between nitrendipine and lysozyme/human serum albumin. The presence of these compounds may disrupt the interactions between the drug and proteins, potentially leading to an increased concentration of free nitrendipine in the bloodstream. Nitrendipine binds more easily to human serum albumin at 310 K, and human serum albumin has an average binding site ratio with nitrendipine approximately 0.1 higher than that with lysozyme. Vitamin C has a greater impact on the binding constant of nitrendipine to human serum albumin and lysozyme. Compared to the binary system of proteins with the drug, the ternary system with the addition of vitamin C at 310 K reduces the binding constants of lysozyme and human serum albumin by 85%. In conclusion, this study explores the significance of considering drug–protein interactions in understanding drug behavior and potential drug–food interactions.

Funder

National Natural Science Foundation of China

Publisher

Wiley

Subject

Chemistry (miscellaneous),Biophysics

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