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P450-containing systems

April 27, 2024

Any enzyme system that includes cytochrome P450 protein or domain can be called a P450-containing system.[1][2][3][4]

P450 enzymes usually function as a terminal oxidase in multicomponent electron-transfer chains, called P450-containing monooxygenase systems, although self-sufficient, non-monooxygenase P450s have been also described. All known P450-containing monooxygenase systems share common structural and functional domain architecture. Apart from the cytochrome itself, these systems contain one or more fundamental redox domains: FAD-containing flavoprotein or domain, FMN domain, ferredoxin and cytochrome b5. These ubiquitous redox domains, in various combinations, are widely distributed in biological systems. FMN domain, ferredoxin or cytochrome b5 transfer electrons between the flavin reductase (protein or domain) and P450. While P450-containing systems are found throughout all kingdoms of life, some organisms lack one or more of these redox domains.

FR/Fd/P450 systems edit

Mitochondrial and some bacterial P450 systems employ soluble Fe2S2 ferredoxins (Fd) that act as single electron carriers between FAD-containing ferredoxin reductase (FR) and P450. In mitochondrial monooxygenase systems, adrenodoxin functions as a soluble electron carrier between NADPH:adrenodoxin reductase and several membrane-bound P450s (CYP11A, CYP11B, CYP27). In bacteria, putidaredoxin, terpredoxin, and rhodocoxin serve as electron carriers between corresponding NADH-dependent ferredoxin reductases and soluble P450s (CYP101, CYP108, CYP116).

NADH putidaredoxin reductase putidaredoxin CYP101 O2
NADH terpredoxin reductase terpredoxin CYP108 O2
NADH rhodocoxin reductase rhodocoxin CYP116 O2
NADPH adrenodoxin reductase adrenodoxin CYP11A1 O2

The general scheme of electron flow in the P450 systems containing adrenodoxin-type ferredoxins is:

NAD(P)H FAD Fe2S2 P450 O2

The sterol demethylase system from Mycobacterium tuberculosis contains flavoprotein reductase A (FprA), bacterial-type Fe3S4 ferredoxin and CYP51 hemoprotein.[5]

NAD(P)H FAD Fe3S4 P450 O2

CPR/P450 systems edit

Eukaryotic microsomal P450 enzymes and some bacterial P450s receive electrons from a FAD- and FMN-containing enzyme known as cytochrome P450 reductase (CPR; EC 1.6.2.4). Microsomal CPR is membrane-bound protein that interacts with different P450s. In Bacillus megaterium and Bacillus subtilis, CPR is a C-terminal domain of CYP102, a single polypeptide self-sufficient soluble P450 system (P450 is an N-terminal domain). The general scheme of electron flow in the CPR/P450 system is:

NADPH FAD FMN P450 O2

CBR/b5/P450 systems edit

The ubiquitous electron-transport protein cytochrome b5 can serve as an effector (activator or inhibitor) of P450s. It was hypothesized that cytochrome b5 is involved in the transfer of the second electron to P450, either from CPR or from NADH:cytochrome b5 reductase (CBR; EC 1.6.2.2):

NADPH CPR cyt b5 P450 O2
NADH CBR cyt b5 P450 O2

The ability of the CBR/cytochrome b5 system to support P450 catalysis has been demonstrated in vitro using purified CBR and cytochrome b5 from Saccharomyces cerevisiae and CYP51 enzyme from Candida albicans. In this system, both the first and second electrons are donated by CBR.

NAD(P)H FAD b5 P450 O2

FMN/Fd/P450 systems edit

An unusual one-component P450 system was originally found in Rhodococcus sp. NCIMB 9784 (CYP116B2). In this system, the N-terminal P450 domain is fused to the reductase domain that shows sequence similarity to phthalate dioxygenase reductase and consists, in its turn, of FMN-binding domain and C-terminal plant-type ferredoxin domain.[6] Similar systems have been identified in the heavy-metal-tolerant bacterium Ralstonia metallidurans (CYP116A1) and in several species of Burkolderia. The general scheme of electron flow in this system appears to be:

NADH FMN Fe2S2 P450 O2

P450-only systems edit

Nitric oxide reductase (P450nor) is a P450 enzyme involved in denitrification in several fungal species. The best-characterized P450nor is CYP55A1 from Fusarium oxysporum. This enzyme does not have monooxygenase activity but is able to reduce nitric oxide (NO·) to form nitrous oxide (N2O) directly using NAD(P)H as electron donor:

NAD(P)H P450 NO·

Fatty acid β-hydroxylase P450BSβ from Bacillus subtilis (CYP152A1) and fatty acid α-hydroxylase P450SPα from Pseudomonas paucimobilis (CYP152B1) catalyse the hydroxylation reaction of long-chain fatty acids using hydrogen peroxide (H2O2) as an oxidant. These enzymes do not require any reduction system for catalysis.

Allene oxide synthase (CYP74A; EC 4.2.1.92), fatty acid hydroperoxide lyase (CYP74B), prostacyclin synthase (CYP8; EC 5.3.99.4) and thromboxane synthase (CYP5; EC 5.3.99.5) are examples of P450 enzymes that do not require a reductase or molecular oxygen for their catalytic activity. Substrates for all these enzymes are fatty acid derivatives containing partially reduced dioxygen (either hydroperoxy or epidioxy groups).

References edit

  1. ^ Degtyarenko, K.N.; Kulikova, T.A. (2001). "Evolution of bioinorganic motifs in P450-containing systems". Biochem. Soc. Trans. 29 (2): 139–147. doi:10.1042/BST0290139. PMID 11356142.
  2. ^ Hanukoglu, I. (1996). "Electron transfer proteins of cytochrome P450 systems" (PDF). Adv. Mol. Cell Biol. Advances in Molecular and Cell Biology. 14: 29–56. doi:10.1016/S1569-2558(08)60339-2. ISBN 9780762301133.
  3. ^ McLean, K.J.; Sabri, M.; Marshall, K.R.; Lawson, R.J.; Lewis, D.G.; Clift, D.; Balding, P.R.; Dunford, A.J.; Warman, A.J.; McVey, J.P.; Quinn, A.-M.; Sutcliffe, M.J.; Scrutton, N.S.; Munro, A.W. (2005). "Biodiversity of cytochrome P450 redox systems". Biochem. Soc. Trans. 33 (4): 796–801. doi:10.1042/BST0330796. PMID 16042601.
  4. ^ Ohta, D.; Mizutani, M. (2004). "Redundancy or flexibility: molecular diversity of the electron transfer components for P450 monooxygenases in higher plants". Front. Biosci. 9 (1–3): 1587–1597. doi:10.2741/1356. PMID 14977570.
  5. ^ McLean, K.J.; Warman, A.J.; Seward, H.E.; Marshall, K.R.; Girvan, H.M.; Cheesman, M.R.; Waterman, M.R.; Munro, A.W. (2006). "Biophysical characterization of the sterol demethylase P450 from Mycobacterium tuberculosis, its cognate ferredoxin, and their interactions". Biochemistry. 45 (27): 8427–8443. doi:10.1021/bi0601609. PMID 16819841.
  6. ^ Roberts, G.A.; Çelik, A.; Hunter, D.J.B.; Ost, T.W.B.; White, J.H.; Chapman, S.K.; Turner, N.J.; Flitsch, S.L. (2003). "A self-sufficient cytochrome P450 with a primary structural organisation that includes a flavin domain and a [2Fe-2S] redox center" (PDF). J. Biol. Chem. 278 (49): 48914–48920. doi:10.1074/jbc.M309630200. PMID 14514666.

External links edit

    April 27, 2024
    p450, containing, systems, enzyme, system, that, includes, cytochrome, p450, protein, domain, called, p450, containing, system, p450, enzymes, usually, function, terminal, oxidase, multicomponent, electron, transfer, chains, called, p450, containing, monooxyge. Any enzyme system that includes cytochrome P450 protein or domain can be called a P450 containing system 1 2 3 4 P450 enzymes usually function as a terminal oxidase in multicomponent electron transfer chains called P450 containing monooxygenase systems although self sufficient non monooxygenase P450s have been also described All known P450 containing monooxygenase systems share common structural and functional domain architecture Apart from the cytochrome itself these systems contain one or more fundamental redox domains FAD containing flavoprotein or domain FMN domain ferredoxin and cytochrome b5 These ubiquitous redox domains in various combinations are widely distributed in biological systems FMN domain ferredoxin or cytochrome b5 transfer electrons between the flavin reductase protein or domain and P450 While P450 containing systems are found throughout all kingdoms of life some organisms lack one or more of these redox domains Contents 1 FR Fd P450 systems 2 CPR P450 systems 3 CBR b5 P450 systems 4 FMN Fd P450 systems 5 P450 only systems 6 References 7 External linksFR Fd P450 systems editMitochondrial and some bacterial P450 systems employ soluble Fe2S2 ferredoxins Fd that act as single electron carriers between FAD containing ferredoxin reductase FR and P450 In mitochondrial monooxygenase systems adrenodoxin functions as a soluble electron carrier between NADPH adrenodoxin reductase and several membrane bound P450s CYP11A CYP11B CYP27 In bacteria putidaredoxin terpredoxin and rhodocoxin serve as electron carriers between corresponding NADH dependent ferredoxin reductases and soluble P450s CYP101 CYP108 CYP116 NADH putidaredoxin reductase putidaredoxin CYP101 O2 NADH terpredoxin reductase terpredoxin CYP108 O2 NADH rhodocoxin reductase rhodocoxin CYP116 O2 NADPH adrenodoxin reductase adrenodoxin CYP11A1 O2 The general scheme of electron flow in the P450 systems containing adrenodoxin type ferredoxins is NAD P H FAD Fe2S2 P450 O2 The sterol demethylase system from Mycobacterium tuberculosis contains flavoprotein reductase A FprA bacterial type Fe3S4 ferredoxin and CYP51 hemoprotein 5 NAD P H FAD Fe3S4 P450 O2CPR P450 systems editEukaryotic microsomal P450 enzymes and some bacterial P450s receive electrons from a FAD and FMN containing enzyme known as cytochrome P450 reductase CPR EC 1 6 2 4 Microsomal CPR is membrane bound protein that interacts with different P450s In Bacillus megaterium and Bacillus subtilis CPR is a C terminal domain of CYP102 a single polypeptide self sufficient soluble P450 system P450 is an N terminal domain The general scheme of electron flow in the CPR P450 system is NADPH FAD FMN P450 O2CBR b5 P450 systems editThe ubiquitous electron transport protein cytochrome b5 can serve as an effector activator or inhibitor of P450s It was hypothesized that cytochrome b5 is involved in the transfer of the second electron to P450 either from CPR or from NADH cytochrome b5 reductase CBR EC 1 6 2 2 NADPH CPR cyt b5 P450 O2 NADH CBR cyt b5 P450 O2 The ability of the CBR cytochrome b5 system to support P450 catalysis has been demonstrated in vitro using purified CBR and cytochrome b5 from Saccharomyces cerevisiae and CYP51 enzyme from Candida albicans In this system both the first and second electrons are donated by CBR NAD P H FAD b5 P450 O2FMN Fd P450 systems editAn unusual one component P450 system was originally found in Rhodococcus sp NCIMB 9784 CYP116B2 In this system the N terminal P450 domain is fused to the reductase domain that shows sequence similarity to phthalate dioxygenase reductase and consists in its turn of FMN binding domain and C terminal plant type ferredoxin domain 6 Similar systems have been identified in the heavy metal tolerant bacterium Ralstonia metallidurans CYP116A1 and in several species of Burkolderia The general scheme of electron flow in this system appears to be NADH FMN Fe2S2 P450 O2P450 only systems editNitric oxide reductase P450nor is a P450 enzyme involved in denitrification in several fungal species The best characterized P450nor is CYP55A1 from Fusarium oxysporum This enzyme does not have monooxygenase activity but is able to reduce nitric oxide NO to form nitrous oxide N2O directly using NAD P H as electron donor NAD P H P450 NO Fatty acid b hydroxylase P450BSb from Bacillus subtilis CYP152A1 and fatty acid a hydroxylase P450SPa from Pseudomonas paucimobilis CYP152B1 catalyse the hydroxylation reaction of long chain fatty acids using hydrogen peroxide H2O2 as an oxidant These enzymes do not require any reduction system for catalysis Allene oxide synthase CYP74A EC 4 2 1 92 fatty acid hydroperoxide lyase CYP74B prostacyclin synthase CYP8 EC 5 3 99 4 and thromboxane synthase CYP5 EC 5 3 99 5 are examples of P450 enzymes that do not require a reductase or molecular oxygen for their catalytic activity Substrates for all these enzymes are fatty acid derivatives containing partially reduced dioxygen either hydroperoxy or epidioxy groups References edit Degtyarenko K N Kulikova T A 2001 Evolution of bioinorganic motifs in P450 containing systems Biochem Soc Trans 29 2 139 147 doi 10 1042 BST0290139 PMID 11356142 Hanukoglu I 1996 Electron transfer proteins of cytochrome P450 systems PDF Adv Mol Cell Biol Advances in Molecular and Cell Biology 14 29 56 doi 10 1016 S1569 2558 08 60339 2 ISBN 9780762301133 McLean K J Sabri M Marshall K R Lawson R J Lewis D G Clift D Balding P R Dunford A J Warman A J McVey J P Quinn A M Sutcliffe M J Scrutton N S Munro A W 2005 Biodiversity of cytochrome P450 redox systems Biochem Soc Trans 33 4 796 801 doi 10 1042 BST0330796 PMID 16042601 Ohta D Mizutani M 2004 Redundancy or flexibility molecular diversity of the electron transfer components for P450 monooxygenases in higher plants Front Biosci 9 1 3 1587 1597 doi 10 2741 1356 PMID 14977570 McLean K J Warman A J Seward H E Marshall K R Girvan H M Cheesman M R Waterman M R Munro A W 2006 Biophysical characterization of the sterol demethylase P450 from Mycobacterium tuberculosis its cognate ferredoxin and their interactions Biochemistry 45 27 8427 8443 doi 10 1021 bi0601609 PMID 16819841 Roberts G A Celik A Hunter D J B Ost T W B White J H Chapman S K Turner N J Flitsch S L 2003 A self sufficient cytochrome P450 with a primary structural organisation that includes a flavin domain and a 2Fe 2S redox center PDF J Biol Chem 278 49 48914 48920 doi 10 1074 jbc M309630200 PMID 14514666 External links editDirectory of P450 containing Systems Portal nbsp Biology Retrieved from https en wikipedia org w index php title P450 containing systems amp oldid 1189979580 CPR P450 systems, wikipedia, wiki, book, books, library,

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