Cytochrome P450 reductase

Source: Wikipedia, the free encyclopedia.
POR
Gene ontology
Molecular function
Cellular component
Biological process
Sources:Amigo / QuickGO
Ensembl

ENSG00000127948

ENSMUSG00000005514

UniProt

P16435

P37040

RefSeq (mRNA)

NM_000941
NM_001367562

NM_008898

RefSeq (protein)

NP_032924

Location (UCSC)Chr 7: 75.9 – 75.99 MbChr 5: 135.7 – 135.76 Mb
PubMed search[3][4]
Wikidata
View/Edit HumanView/Edit Mouse

Cytochrome P450 reductase (also known as NADPH:ferrihemoprotein oxidoreductase, NADPH:hemoprotein oxidoreductase, NADPH:P450 oxidoreductase, P450 reductase, POR, CPR, CYPOR) is a membrane-bound

NADPH to cytochrome P450[5] and other heme proteins including heme oxygenase in the endoplasmic reticulum[6] of the eukaryotic cell
.

Gene

Human POR gene has 16 exons and the exons 2-16 code for a 677-amino acid [7] POR protein (NCBI NP_000932.2). There is a single copy of 50 kb POR gene (NCBI NM_000941.2) in humans on chromosome 7 (7q11.23).

Paralogs of POR include nitric oxide synthase (EC 1.14.13.39), NADPH:sulfite reductase (EC 1.8.1.2), and methionine synthase reductase (EC 1.16.1.8).[citation needed
]

Protein structure

The 3D crystal structure of human POR has been determined.[8] The molecule is composed of four structural domains: the FMN-binding domain, the connecting domain, the FAD-binding domain, and NADPH-binding domain. The FMN-binding domain is similar to the structure of FMN-containing protein flavodoxin, whereas the FAD-binding domain and NADPH-binding domains are similar to those of flavoprotein ferredoxin-NADP+ reductase (FNR). The connecting domain is situated between the flavodoxin-like and FNR-like domains. Conformation flexibility of POR is a key requirement for interaction with different redox partners like Cytochrome P450 proteins, and biasing the conformation of POR with small molecule ligands may be a way to control interaction with partner proteins and influence metabolism.[9]

Function

In Bacillus megaterium and Bacillus subtilis, POR 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 POR/P450 system is:

NADPH → FAD → FMN → P450 → O2

The definitive evidence for the requirement of POR in cytochrome-P450-mediated reactions came from the work of Lu, Junk and Coon,[10] who dissected the P450-containing mixed function oxidase system into three constituent components: POR, cytochrome P450, and lipids.

Since all microsomal P450 enzymes require POR for catalysis, it is expected that disruption of POR would have devastating consequences. POR knockout mice are embryonic lethal,[11] probably due to lack of electron transport to extrahepatic P450 enzymes since liver-specific knockout of POR yields phenotypically and reproductively normal mice that accumulate hepatic lipids and have remarkably diminished capacity of hepatic drug metabolism.[12]

The reduction of cytochrome P450 is not the only physiological function of POR. The final step of heme oxidation by mammalian heme oxygenase requires POR and O2. In yeast, POR affects the ferrireductase activity, probably transferring electrons to the flavocytochrome ferric reductase.[13]

Clinical significance

More than 200 variations in POR gene have been identified.[14][15]

Five missense mutations (A287P, R457H, V492E, C569Y, and V608F) and a splicing mutation in the POR genes have been found in patients who had hormonal evidence for combined deficiencies of two steroidogenic cytochrome P450 enzymes - P450c17

21-hydroxylase, which catalyzes steroid 21-hydroxylation.[16] Another POR missense mutation Y181D has also been identified.[17] Fifteen of nineteen patients having abnormal genitalia and disordered steroidogenesis were homozygous or apparent compound heterozygous for POR mutations that destroyed or dramatically inhibited POR activity.[18]

POR Deficiency – Mixed Oxidase Disease

See also: Cytochrome P450 oxidoreductase deficiency

POR deficiency is the newest form of congenital adrenal hyperplasia first described in 2004.[16] The index patient was a newborn 46,XX Japanese girl with craniosynostosis, hypertelorism, mid-face hypoplasia, radiohumeral synostosis, arachnodactyly and disordered steroidogenesis. However, the clinical and biochemical characteristics of patients with POR deficiency are long known in the literature as so-called mixed oxidase disease, as POR deficiency typically shows a steroid profile that suggests combined deficiencies of steroid 21-hydroxylase and 17α-hydroxylase/17,20 lyase activities. The clinical spectrum of POR deficiency ranges from severely affected children with ambiguous genitalia, adrenal insufficiency, and the Antley-Bixler skeletal malformation syndrome (ABS) to mildly affected individuals with polycystic ovary syndrome-like features. Some of the POR patients were born to mothers who became virilized during pregnancy, suggesting deficient placental aromatization of fetal androgens due to a lesion in microsomal aromatase resulting in low estrogen production, which was later confirmed by lower aromatase activities caused by POR mutations.[19][20] However, it has also been suggested that fetal and maternal virilization in POR deficiency might be caused by increased dihydrotestosterone synthesis by the fetal gonad through an alternative "backdoor pathway" first described in the marsupials and later confirmed in humans.[21] Gas chromatography/mass spectrometry analysis of urinary steroids from pregnant women carrying a POR-deficient fetus described in an earlier report also supports the existence of this pathway,[22][23] and the relevance of the backdoor pathway along with POR dependent steroidogenesis have become clearer from recent studies.[21] The role of POR mutations beyond CAH are being investigated; and questions such as how POR mutations cause bony abnormalities and what role POR variants play in drug metabolism by hepatic P450s are being addressed in recent publications.[24][25][26][27][28] However, reports of ABS in some offspring of mothers who were treated with fluconazole, an antifungal agent which interferes with cholesterol biosynthesis at the level of CYP51 activity - indicate that disordered drug metabolism may result from deficient POR activity.[29]

Williams syndrome

Mb from the POR gene (POR). Cells with this genetic deletion show reduced transcription of POR, it seems, due to the loss of a cis-regulatory element that alters expression of this gene.[30] Some persons with Williams syndrome show characteristics of POR deficiency, including radioulnar synostosis and other skeletal abnormalities.[31] Cases of mild impairment of cortisol and androgen synthesis have been noted,[32] however, despite the fact that deficient POR impairs androgen synthesis, patients with Williams syndrome often show increased androgen levels.[33] A similar increase in testosterone has been observed in a mouse model that has globally decreased POR expression.[34]

See also

References

  1. ^ a b c GRCh38: Ensembl release 89: ENSG00000127948Ensembl, May 2017
  2. ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000005514Ensembl, May 2017
  3. ^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  4. ^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
  5. PMID 23353702
    .
  6. PMID 19931102
    . CPR was shown to be localized in the endoplasmic reticulum in the early 1960s (Williams and Kamin, 1962).
  7. PMID 2513880
    .
  8. PMID 21808038
    .
  9. PMID 33859207
    .
  10. PMID 4389465
    .
  11. PMID 11742006
    .
  12. PMID 12697746
    .
  13. PMID 9368374
    .
  14. PMID 24847272
    .
  15. PMID 27068427
    .
  16. ^
    PMID 14758361
    .
  17. S2CID 32705841
    .
  18. PMID 15793702
    .
  19. PMID 32060549
    .
  20. PMID 17595315
    .
  21. ^
    PMID 21802064
    .
  22. PMID 31611378
    .
  23. S2CID 22583190
    .
  24. PMID 20849814
    .
  25. PMID 20844025
    .
  26. S2CID 29109570
    .
  27. PMID 20940534
    .
  28. PMID 20697309
    .
  29. S2CID 23498012
    .
  30. PMID 16826523
    .
  31. S2CID 33765973
    .
  32. PMID 8835601
    .
  33. PMID 8074154
    .
  34. S2CID 8292025
    .

External links
Retrieved from "https://en.wikipedia.org/w/index.php?title=Cytochrome_P450_reductase&oldid=1181082529"