Interaction Modes of Microsomal Cytochrome P450s with Its Reductase and the Role of Substrate Binding.

Francisco Esteves,Philippe Urban,Gilles Truan,José Rueff,Michel Kranendonk

doi:10.3390/ijms21186669

Abstract

The activity of microsomal cytochromes P450 (CYP) is strictly dependent on the supply of electrons provided by NADPH cytochrome P450 oxidoreductase (CPR). The variant nature of the isoform-specific proximal interface of microsomal CYPs implies that the interacting interface between the two proteins is degenerated. Recently, we demonstrated that specific CPR mutations in the FMN-domain (FD) may induce a gain in activity for a specific CYP isoform. In the current report, we confirm the CYP isoform dependence of CPR’s degenerated binding by demonstrating that the effect of four of the formerly studied FD mutants are indeed exclusive of a specific CYP isoform, as verified by cytochrome c inhibition studies. Moreover, the nature of CYP’s substrate seems to have a modulating role in the CPR:CYP interaction. In silico molecular dynamics simulations of the FD evidence that mutations induces very subtle structural alterations, influencing the characteristics of residues formerly implicated in the CPR:CYP interaction or in positioning of the FMN moiety. CPR seems therefore to be able to form effective interaction complexes with its structural diverse partners via a combination of specific structural features of the FD, which are functional in a CYP isoform dependent manner, and dependent on the substrate bound.

Highlights

Human mitochondrial and microsomal cytochromes P450 (CYP) form a superfamily of membrane-bound hemeproteins with monooxygenase activity [1,2]
Microsomal CYP isoforms are dependent on NADPH cytochrome P450 oxidoreductase (CPR)—containing flavin adenine dinucleotide (FAD) and flavin mononucleotide (FMN) domains—for supply of electrons in their catalytic activities to metabolize a myriad of compounds, both endobiotics including vitamins, steroids and hormones, and xenobiotics, such as therapeutic drugs, carcinogens and environmental chemicals [3,4,5]
We previously studied the underlying molecular mechanisms on CPR:CYP interaction and electron transfer (ET), by creating and selecting seven mutants in the FD of human CPR, each supporting a gain in activity for a specific CYP isoform [16]

Summary

Introduction

Human mitochondrial and microsomal cytochromes P450 (CYP) form a superfamily of membrane-bound hemeproteins with monooxygenase activity [1,2]. Microsomal CYPs do not possess such signature sequences to guide their interaction with the FMN-domain (FD) of CPR for ET [6]. This suggests that CPR:CYP electron transport system is more versatile and does not depend on uniquely conserved structural features present on CPR–CYPs interaction interface. Instead, it relies on a degenerate interaction between the FD and the proximal side of the structurally diverse microsomal CYP isoforms [6,8,9,10]

Methods

Results

Discussion

Conclusion