Literature DB >> 25795780

Effects of membrane mimetics on cytochrome P450-cytochrome b5 interactions characterized by NMR spectroscopy.

Meng Zhang1, Rui Huang1, Sang-Choul Im2, Lucy Waskell2, Ayyalusamy Ramamoorthy3.   

Abstract

Mammalian cytochrome P450 (P450) is a membrane-bound monooxygenase whose catalytic activities require two electrons to be sequentially delivered from its redox partners: cytochrome b5 (cytb5) and cytochrome P450 reductase, both of which are membrane proteins. Although P450 functional activities are known to be affected by lipids, experimental evidence to reveal the effect of membrane on P450-cytb5 interactions is still lacking. Here, we present evidence for the influence of phospholipid bilayers on complex formation between rabbit P450 2B4 (CYP2B4) and rabbit cytb5 at the atomic level, utilizing NMR techniques. General line broadening and modest chemical shift perturbations of cytb5 resonances characterize CYP2B4-cytb5 interactions on the intermediate time scale. More significant intensity attenuation and a more specific protein-protein binding interface are observed in bicelles as compared with lipid-free solution, highlighting the importance of the lipid bilayer in stabilizing stronger and more specific interactions between CYP2B4 and cytb5, which may lead to a more efficient electron transfer. Similar results observed for the interactions between CYP2B4 lacking the transmembrane domain (tr-CYP2B4) and cytb5 imply interactions between tr-CYP2B4 and the membrane surface, which might assist in CYP2B4-cytb5 complex formation by orienting tr-CYP2B4 for efficient contact with cytb5. Furthermore, the observation of weak and nonspecific interactions between CYP2B4 and cytb5 in micelles suggests that lipid bilayer structures and low curvature membrane surface are preferable for CYP2B4-cytb5 complex formation. Results presented in this study provide structural insights into the mechanism behind the important role that the lipid bilayer plays in the interactions between P450s and their redox partners.
© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  cytochrome P450; cytochrome b5; lipid bilayer; membrane bilayer; membrane protein; nuclear magnetic resonance (NMR)

Mesh:

Substances:

Year:  2015        PMID: 25795780      PMCID: PMC4432288          DOI: 10.1074/jbc.M114.597096

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  69 in total

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6.  Bilayer in small bicelles revealed by lipid-protein interactions using NMR spectroscopy.

Authors:  Donghan Lee; Korvin F A Walter; Ann-Kathrin Brückner; Christian Hilty; Stefan Becker; Christian Griesinger
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Review 8.  The cytochromes P450 and b5 and their reductases--promising targets for structural studies by advanced solid-state NMR spectroscopy.

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10.  Probing the transmembrane structure and topology of microsomal cytochrome-p450 by solid-state NMR on temperature-resistant bicelles.

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2.  Effect of polymer charge on functional reconstitution of membrane proteins in polymer nanodiscs.

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4.  Substrate mediated redox partner selectivity of cytochrome P450.

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5.  Evidence that cytochrome b5 acts as a redox donor in CYP17A1 mediated androgen synthesis.

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7.  Expression, purification, and functional reconstitution of 19F-labeled cytochrome b5 in peptide nanodiscs for NMR studies.

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Review 8.  Nanodiscs: A toolkit for membrane protein science.

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9.  Solution structure of the transmembrane domain of the mouse erythropoietin receptor in detergent micelles.

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10.  An Adaptable Phospholipid Membrane Mimetic System for Solution NMR Studies of Membrane Proteins.

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Journal:  J Am Chem Soc       Date:  2017-10-10       Impact factor: 15.419

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