An Intermediate Conformational State of Cytochrome P450cam-CN in Complex with Putidaredoxin

Overview

Journal Biochemistry

Specialty Biochemistry

Date 2019 Apr 18

PMID 30994334

Citations 6

Authors

Shih-Wei Chuo

Lee-Ping Wang

R David Britt

David B Goodin

Affiliations

Soon will be listed here.

Abstract

Cytochrome P450cam is an archetypal example of the vast family of heme monooxygenases and serves as a model for an enzyme that is highly specific for both its substrate and reductase. During catalysis, it undergoes significant conformational changes of the F and G helices upon binding its substrate and redox partner, putidaredoxin (Pdx). Recent studies have shown that Pdx binding to the closed camphor-bound form of ferric P450cam results in its conversion to a fully open state. However, during catalytic turnover, it remains unclear whether this same conformational change also occurs or whether it is coupled to the formation of the critical compound I intermediate. Here, we have examined P450cam bound simultaneously by camphor, CN, and Pdx as a mimic of the catalytically competent ferrous oxy-P450cam-Pdx state. The combined use of double electron-electron resonance and molecular dynamics showed direct observation of intermediate conformational states of the enzyme upon CN and subsequent Pdx binding. This state is coupled to the movement of the I helix and residues at the active site, including Arg-186, Asp-251, and Thr-252. These movements enable occupation of a water molecule that has been implicated in proton delivery and peroxy bond cleavage to give compound I. These findings provide a detailed understanding of how the Pdx-induced conformational change may sequentially promote compound I formation followed by product release, while retaining stereoselective hydroxylation of the substrate of this highly specific monooxygenase.

Citing Articles

Updating the Paradigm: Redox Partner Binding and Conformational Dynamics in Cytochromes P450.

Poulos T, Follmer A Acc Chem Res. 2021; 55(3):373-380.

PMID: 34965086 PMC: 8959394. DOI: 10.1021/acs.accounts.1c00632.

Structural Dynamics of Cytochrome P450 3A4 in the Presence of Substrates and Cytochrome P450 Reductase.

Ducharme J, Sevrioukova I, Thibodeaux C, Auclair K Biochemistry. 2021; 60(28):2259-2271.

PMID: 34196520 PMC: 8711236. DOI: 10.1021/acs.biochem.1c00178.

Active Site Hydrogen Bonding Induced in Cytochrome P450cam by Effector Putidaredoxin.

Mammoser C, Ramos S, Thielges M Biochemistry. 2021; 60(21):1699-1707.

PMID: 34006086 PMC: 8750573. DOI: 10.1021/acs.biochem.1c00075.

Kinetics of cytochrome P450 3A4 inhibition by heterocyclic drugs defines a general sequential multistep binding process.

Guengerich F, McCarty K, Chapman J J Biol Chem. 2021; 296:100223.

PMID: 33449875 PMC: 7948456. DOI: 10.1074/jbc.RA120.016855.

Linkage between Proximal and Distal Movements of P450cam Induced by Putidaredoxin.

Liou S, Chuo S, Qiu Y, Wang L, Goodin D Biochemistry. 2020; 59(21):2012-2021.

PMID: 32369344 PMC: 9749489. DOI: 10.1021/acs.biochem.0c00294.

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