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Wikipedia

Cytochrome b-245, alpha polypeptide

January 01, 1970

Cytochrome b-245 light chain is a protein that in humans is encoded by the CYBA gene involved in superoxide production and phagocytosis.[5]

CYBA
Available structures
PDBOrtholog search: PDBe RCSB
Identifiers
AliasesCYBA, p22-PHOX, Cytochrome b-245, alpha polypeptide, cytochrome b-245 alpha chain, CGD4
External IDsOMIM: 608508; MGI: 1316658; HomoloGene: 80; GeneCards: CYBA; OMA:CYBA - orthologs
Orthologs
SpeciesHumanMouse
Entrez

1535

13057

Ensembl

ENSG00000051523

ENSMUSG00000006519

UniProt

P13498

Q61462

RefSeq (mRNA)

NM_000101

NM_001301284
NM_007806

RefSeq (protein)

NP_000092

NP_001288213
NP_031832

Location (UCSC)Chr 16: 88.64 – 88.65 MbChr 8: 123.15 – 123.16 Mb
PubMed search[3][4]
Wikidata
View/Edit HumanView/Edit Mouse

Cytochrome b-245 is composed of a light chain (alpha) and a heavy chain (beta). This gene encodes the light, alpha subunit, which has been proposed as a primary component of the microbicidal oxidase system of phagocytes. Mutations in this gene are associated with autosomal recessive chronic granulomatous disease (CGD), which is characterized by the failure of activated phagocytes to generate superoxide, which is important for the microbicidal activity of these cells.[6]

Discovery edit

The p22phox protein (phox for phagocytic oxidase) was first identified in 1987 during the purification of the cytochrome b-245mv from human neutrophils.[7] A few years before, this low-potential cytochrome b, also called cytochrome b558 (cytb) because of its spectral properties, was demonstrated as the major component of the microbicidal nicotinamide adenine dinucleotide phosphate (NADPH) oxidase complex in phagocytes.[8][9][10] Cytb, the redox element of the NADPH oxidase complex, is a membrane heterodimer composed of two subunits: p22phox (also called the alpha or small subunit or the light chain of the cytb) and gp91phox (renamed NOX2 in the 2000s) or the beta or heavy chain or large subunit. By screening a cDNA library constructed from human promyelocytic leukemia cells, Parkos et al. isolated a cDNA corresponding to the light chain of cytb.[11] The importance of the role of p22phox was evidenced by the discovery of autosomal recessive chronic granulomatous disease caused by mutations in CYBA and leading to the absence of cytb expression in phagocytes.[5]

Gene edit

The human CYBA gene (OMIM number 233690) encoding the p22phox protein is located on the long arm of chromosome 16 at position 24 (16q24: 88,643,288 to 88,651,084, OMIM 608508), containing 6 exons, 5 introns and spanning 8.5kb (Fig. 1). An update of the promoter region of CYBA contains TATA, CCAC boxes, Sp1, -interferon, and nuclear factor B sites.[12] The p22phox cDNA was also cloned in rat vascular smooth muscle cells (VSMCs) and showed that the rat gene was homologous to both human and mouse genes.[13] P22phox human mRNA is 0.8 kb and has a constitutive expression in a variety of cell types. P22phox expression is not related to the NOX2 transcript expression, suggesting that both subunits have an independent transcription process.[14][15]

Protein structure and function edit

P22phox is a transmembrane protein that contains 195 amino acids and that has a molecular mass of 22.0 kDa. It associates with NOX2 and with NOX1, NOX3 and NOX4 in a 1:1 complex and has a ubiquitous expression. The main physiological role of p22phox is to contribute to the maturation and the stabilization of the heterodimer that it forms with NOX enzymes (NOX1–4) in order to produce reactive oxygen species (ROS). Association of NOXs with p22phox in the late endoplasmic reticulum seems to be a prerequisite for the localization of the heterodimer to specific membrane compartments such as perinuclear vesicles for NOX4 and plasma membranes in the case of NOX1, 2 and 3.[16][17][18][19] The importance of some sequences of p22phox for its interaction with NOXs has been highlighted.[20] The hydropathic profile of p22phox deduced from the gene sequence is compatible with at least two (possibly three or four) transmembrane passages.[21][22][23][24][25][26][27] However, the most probable are the two or four transmembrane-spanning models because they are compatible with a cytosolic location of both the N- and the C-terminal tail of p22phox. A polyproline-rich region (PRR) (K149 to E162 sequence) in the C-terminus of p22phox contains a consensus motif PxxP that interacts with the SH3 (SRC homology 3) domains of p47phox during NADPH oxidase assembly in phagocytes.[23][28][29][30] This PRR-rich sequence also interacts with the cytosolic organizer NOXO1 homologs to p47phox expressed in nonphagocytic cells, during the activation of NADPH oxidases (NOX1, NOX2 and NOX3), except for NOX4, which is constitutively expressed.[31][32] Phosphorylation of Thr147 close to the PRR region of p22phox enhances NADPH oxidase activity by promoting p47phox binding in phagocytes.[33] ROSs generated by NOX2-p22phox (or cytb) in the phagocytes are microbicide and are able to kill microorganisms during infections. P22phox associated with NOX2 is also found in brain and especially in microglia. Anarchic ROS production by these cells is involved in the pathological process of degenerative diseases.[34][35] P22phox can be associated with NOX1, NOX3 and NOX4 in several cells and tissues, but the level of ROS production is far lower than those produced in phagocytes by cytb. In this case ROSs are considered as signaling messengers rather than toxic products. Excessive ROS generation by NOX enzymes has been linked to a range of diseases including cardiovascular diseases such as atherosclerosis and hypertension, diabetes, neurodegenerative disease and ischemia/reperfusion injury.[34] NOX1, NOX2 and NOX4, which require p22phox to be functional, are important contributors of ROS in tissues and especially vascular cells. Therefore, the variability of ROS production by NOXs could influence the risk of such diseases, although increased oxidative stress by p22phox overexpression has not been functionally characterized or attributed to a particular NOX family member.

Clinical relevance of mutations edit

Mutations in CYBA or CYBB, encoding p22phox or NOX2, respectively, lead to Chronic granulomatous disease because of the absence of cytb in both cases.[14] This means that the synthesis of both subunits is essential for the maturation of cytb.[36] CGD is a rare inherited disorder in which phagocytic cells are unable to kill pathogens during an infection. Patients suffer from severe and recurrent infections early in childhood. Actually, the main treatment is antibiotic and antifungal prophylaxis. Allogenic bone marrow transplantation is possible and genetic therapy is currently under development.[37] The most frequent CGD form is X-linked CGD caused by mutations in CYBB (60% of cases).[38] Mutations in the CYBA gene encoding p22phox are extremely rare (about 6%) and lead to AR-CGD220. However, in countries such as Turkey, Tunisia, Morocco and Jordan AR inheritance can be the predominant form because of the high rate of consanguinity.[39][40][41][42] As of 2010, 55 different mutations of CYBA have been identified.[43] Most CYBA mutations result in the absence of p22phox expression (AR-CGD220). The only missense mutation leading to a normal expression of a nonfunctional p22phox protein is Pro156Gln (AR-CGD22+) located in the potential cytosolic C-terminal tail of p22phox.[44] This mutation in the PRR of p22phox disrupted the interaction between p22phox and p47phox, confirming the importance of this domain in the oxidase activation in neutrophils. Since p22phox is ubiquitous and associated with different NOXs, it could be logical that CGD patients suffer from the consequences of the absence of p22phox expression in tissues. However it is far from being evident. One possibility could be that the humans may be able to compensate for the absence of p22phox and/or NOXs in cells and tissues other than phagocytes. Given the rarity of the AR-CGD220 forms, information on the severity of this type of CGD is difficult to establish. A relationship between the presence of residual ROS production and the survival of CGD patients has been found.[45] In case of CYBA mutations leading to the absence of p22phox, NOX2 expression is also absent and disables cytochrome b558, the redox element of the NADPH oxidase complex. Therefore, these mutations behave similarly to severe X-CGD. The molecular and phenotypic characterization of a p22phox-deficient mouse strain with the Tyr121His missense mutation in CYBA has been described.[46] The p22phox deficiency results in the clinical and biological characteristics of CGD as well as a severe balance disorder in these mice. As the site of p22phox expression is in the inner ear, p22phox has been proposed as being involved in the control of vestibular organogenesis. In addition, mutations of NOX3 in head-tilt mice were associated with vestibular defects.[47][48] Yet the in vivo relevance of p22phox for NOX3 function remains uncertain because AR-CGD220 patients do not suffer from vestibular dysfunction (personal data). One possibility could be that the human brain may be able to compensate the balance defect. In Matsumoto Eosinophilia Shinshu (MES) rats a loss-of-function mutation in CYBA was responsible for spontaneous and severe blood eosinophilia.[49] These rats suffered from a balance defect due to a leak of otoconia in the inner ear, like nmf333 mice. In addition, MES rats retained normal innate immune defense against Staphylococcus aureus infection probably because of the hypereosinophilia. However, the mechanisms by which CYBA mutations lead to eosinophilia remain unknown.

Clinical relevance of single-nucleotide polymorphisms edit

Contrary to CYBB, CYBA supports a relatively high number of single-nucleotide polymorphisms (SNPs) that could influence the level of ROS generation. These SNPs were mainly associated with cardiovascular diseases such as hypertension,[50] coronary artery disease (CAD), coronary heart disease (CHD)[51][52] and also cerebral ischemic diseases.[53][54] The first and most widely studied is the C242T polymorphism is located in exon 4 at position 214 from the ATG and resulting in a non conservative His72 substitution for a Tyr.[5] Inoue et al. first found that the T allele of the C242 polymorphism might have a protective effect against CAD.[55] Despite some evidence of the effect of this polymorphism on ROS generation at the cellular level, the association of the CYBA C242T polymorphism with cardiovascular diseases has been widely reported but with conflicting results.[52] Single SNP analysis may explain the discrepancies among CYBA association studies. A global approach such as haplotype analysis is probably a better approach to understand the impact of CYBA genetic variability on diseases.[56][57][58] CYBA variants together with polymorphism analysis of lipid metabolism or stress oxidant pathway genes are of great interest as well.[59][60][61] However, for future investigations regarding the effect of these polymorphisms, it is crucial that the number of patients under study provide sufficient statistical power. In addition, genetics studies that include control of external factors should be extremely informative. Finally, since 2010 nine Chinese meta-analyses of the C242T polymorphism have been published in relation with CAD,[62][63][64][65][66] hypertension[50] atherosclerosis or diabetes and its complications[54] and ischemic cerebrovascular diseases.[53][54] The results from these meta-analyses were controversial. Several factors could influence these data: the search strategy, the identification of relevant studies (publication bias), the statistical analysis including a sufficient sampling, the prevalence of the studied polymorphism in the studied population [minor allele frequency (MAF)] and the type of population (population-based or not, for example). Results of these meta-analyses need to be confirmed with larger samples. In addition, a meta-analysis based on genome-wide association study data will be of great interest in the future.

Notes edit

References edit

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External links edit

  • Overview of all the structural information available in the PDB for UniProt: P13498 (Cytochrome b-245 light chain) at the PDBe-KB.

January 01, 1970
cytochrome, alpha, polypeptide, cytochrome, light, chain, protein, that, humans, encoded, cyba, gene, involved, superoxide, production, phagocytosis, cybaavailable, structurespdbortholog, search, pdbe, rcsblist, codes1wlpidentifiersaliasescyba, phox, cytochrom. Cytochrome b 245 light chain is a protein that in humans is encoded by the CYBA gene involved in superoxide production and phagocytosis 5 CYBAAvailable structuresPDBOrtholog search PDBe RCSBList of PDB id codes1WLPIdentifiersAliasesCYBA p22 PHOX Cytochrome b 245 alpha polypeptide cytochrome b 245 alpha chain CGD4External IDsOMIM 608508 MGI 1316658 HomoloGene 80 GeneCards CYBA OMA CYBA orthologsGene location Human Chr Chromosome 16 human 1 Band16q24 2Start88 643 275 bp 1 End88 651 083 bp 1 Gene location Mouse Chr Chromosome 8 mouse 2 Band8 8 E1Start123 151 515 bp 2 End123 159 669 bp 2 RNA expression patternBgeeHumanMouse ortholog Top expressed inmonocytespleenbone marrowright lungright uterine tubeupper lobe of left lungbone marrow cellsright lobe of thyroid glandbloodlymph nodeTop expressed inkidneyspleenyolk sacproximal tubulethymuscalvariaright lungright lung lobeleft lunguterusMore reference expression dataBioGPSMore reference expression dataGene ontologyMolecular functionSH3 domain binding metal ion binding protein binding heme binding protein heterodimerization activity electron transfer activity oxidoreductase activity superoxide generating NAD P H oxidase activityCellular componentcytoplasm endosome phagocytic vesicle membrane Golgi apparatus membrane plasma membrane perinuclear endoplasmic reticulum secretory granule neuronal cell body NADPH oxidase complex dendrite apical plasma membrane mitochondrion nucleus endoplasmic reticulum membrane stress fiber focal adhesion specific granule membrane tertiary granule membraneBiological processpositive regulation of reactive oxygen species biosynthetic process cellular response to organic substance positive regulation of phagocytosis cytochrome complex assembly response to interleukin 1 positive regulation of endothelial cell proliferation antigen processing and presentation of exogenous peptide antigen via MHC class I TAP dependent regulation of release of sequestered calcium ion into cytosol cellular response to tumor necrosis factor cellular response to organic cyclic compound negative regulation of glomerular filtration by angiotensin smooth muscle hypertrophy positive regulation of defense response to bacterium cell redox homeostasis reactive oxygen species metabolic process superoxide anion generation respiratory burst regulation of blood pressure cellular response to mechanical stimulus positive regulation of cell growth vascular endothelial growth factor receptor signaling pathway response to nutrient levels cellular response to gamma radiation positive regulation of interleukin 6 production positive regulation of tumor necrosis factor production cellular response to amino acid stimulus hydrogen peroxide biosynthetic process positive regulation of toll like receptor 2 signaling pathway positive regulation of superoxide anion generation innate immune response inflammatory response positive regulation of mucus secretion cellular response to glucose stimulus superoxide metabolic process positive regulation of smooth muscle cell proliferation response to aldosterone positive regulation of NAD P H oxidase activity cellular response to L glutamine response to hypoxia cellular response to angiotensin response to activity neutrophil degranulation cellular response to oxidative stress electron transport chain positive regulation of blood pressureSources Amigo QuickGOOrthologsSpeciesHumanMouseEntrez153513057EnsemblENSG00000051523ENSMUSG00000006519UniProtP13498Q61462RefSeq mRNA NM 000101NM 001301284NM 007806RefSeq protein NP 000092NP 001288213NP 031832Location UCSC Chr 16 88 64 88 65 MbChr 8 123 15 123 16 MbPubMed search 3 4 WikidataView Edit HumanView Edit Mouse Cytochrome b 245 is composed of a light chain alpha and a heavy chain beta This gene encodes the light alpha subunit which has been proposed as a primary component of the microbicidal oxidase system of phagocytes Mutations in this gene are associated with autosomal recessive chronic granulomatous disease CGD which is characterized by the failure of activated phagocytes to generate superoxide which is important for the microbicidal activity of these cells 6 Contents 1 Discovery 2 Gene 3 Protein structure and function 4 Clinical relevance of mutations 5 Clinical relevance of single nucleotide polymorphisms 6 Notes 7 References 8 External linksDiscovery editThe p22phox protein phox for phagocytic oxidase was first identified in 1987 during the purification of the cytochrome b 245mv from human neutrophils 7 A few years before this low potential cytochrome b also called cytochrome b558 cytb because of its spectral properties was demonstrated as the major component of the microbicidal nicotinamide adenine dinucleotide phosphate NADPH oxidase complex in phagocytes 8 9 10 Cytb the redox element of the NADPH oxidase complex is a membrane heterodimer composed of two subunits p22phox also called the alpha or small subunit or the light chain of the cytb and gp91phox renamed NOX2 in the 2000s or the beta or heavy chain or large subunit By screening a cDNA library constructed from human promyelocytic leukemia cells Parkos et al isolated a cDNA corresponding to the light chain of cytb 11 The importance of the role of p22phox was evidenced by the discovery of autosomal recessive chronic granulomatous disease caused by mutations in CYBA and leading to the absence of cytb expression in phagocytes 5 Gene editThe human CYBA gene OMIM number 233690 encoding the p22phox protein is located on the long arm of chromosome 16 at position 24 16q24 88 643 288 to 88 651 084 OMIM 608508 containing 6 exons 5 introns and spanning 8 5kb Fig 1 An update of the promoter region of CYBA contains TATA CCAC boxes Sp1 interferon and nuclear factor B sites 12 The p22phox cDNA was also cloned in rat vascular smooth muscle cells VSMCs and showed that the rat gene was homologous to both human and mouse genes 13 P22phox human mRNA is 0 8 kb and has a constitutive expression in a variety of cell types P22phox expression is not related to the NOX2 transcript expression suggesting that both subunits have an independent transcription process 14 15 Protein structure and function editP22phox is a transmembrane protein that contains 195 amino acids and that has a molecular mass of 22 0 kDa It associates with NOX2 and with NOX1 NOX3 and NOX4 in a 1 1 complex and has a ubiquitous expression The main physiological role of p22phox is to contribute to the maturation and the stabilization of the heterodimer that it forms with NOX enzymes NOX1 4 in order to produce reactive oxygen species ROS Association of NOXs with p22phox in the late endoplasmic reticulum seems to be a prerequisite for the localization of the heterodimer to specific membrane compartments such as perinuclear vesicles for NOX4 and plasma membranes in the case of NOX1 2 and 3 16 17 18 19 The importance of some sequences of p22phox for its interaction with NOXs has been highlighted 20 The hydropathic profile of p22phox deduced from the gene sequence is compatible with at least two possibly three or four transmembrane passages 21 22 23 24 25 26 27 However the most probable are the two or four transmembrane spanning models because they are compatible with a cytosolic location of both the N and the C terminal tail of p22phox A polyproline rich region PRR K149 to E162 sequence in the C terminus of p22phox contains a consensus motif PxxP that interacts with the SH3 SRC homology 3 domains of p47phox during NADPH oxidase assembly in phagocytes 23 28 29 30 This PRR rich sequence also interacts with the cytosolic organizer NOXO1 homologs to p47phox expressed in nonphagocytic cells during the activation of NADPH oxidases NOX1 NOX2 and NOX3 except for NOX4 which is constitutively expressed 31 32 Phosphorylation of Thr147 close to the PRR region of p22phox enhances NADPH oxidase activity by promoting p47phox binding in phagocytes 33 ROSs generated by NOX2 p22phox or cytb in the phagocytes are microbicide and are able to kill microorganisms during infections P22phox associated with NOX2 is also found in brain and especially in microglia Anarchic ROS production by these cells is involved in the pathological process of degenerative diseases 34 35 P22phox can be associated with NOX1 NOX3 and NOX4 in several cells and tissues but the level of ROS production is far lower than those produced in phagocytes by cytb In this case ROSs are considered as signaling messengers rather than toxic products Excessive ROS generation by NOX enzymes has been linked to a range of diseases including cardiovascular diseases such as atherosclerosis and hypertension diabetes neurodegenerative disease and ischemia reperfusion injury 34 NOX1 NOX2 and NOX4 which require p22phox to be functional are important contributors of ROS in tissues and especially vascular cells Therefore the variability of ROS production by NOXs could influence the risk of such diseases although increased oxidative stress by p22phox overexpression has not been functionally characterized or attributed to a particular NOX family member Clinical relevance of mutations editMutations in CYBA or CYBB encoding p22phox or NOX2 respectively lead to Chronic granulomatous disease because of the absence of cytb in both cases 14 This means that the synthesis of both subunits is essential for the maturation of cytb 36 CGD is a rare inherited disorder in which phagocytic cells are unable to kill pathogens during an infection Patients suffer from severe and recurrent infections early in childhood Actually the main treatment is antibiotic and antifungal prophylaxis Allogenic bone marrow transplantation is possible and genetic therapy is currently under development 37 The most frequent CGD form is X linked CGD caused by mutations in CYBB 60 of cases 38 Mutations in the CYBA gene encoding p22phox are extremely rare about 6 and lead to AR CGD220 However in countries such as Turkey Tunisia Morocco and Jordan AR inheritance can be the predominant form because of the high rate of consanguinity 39 40 41 42 As of 2010 55 different mutations of CYBA have been identified 43 Most CYBA mutations result in the absence of p22phox expression AR CGD220 The only missense mutation leading to a normal expression of a nonfunctional p22phox protein is Pro156Gln AR CGD22 located in the potential cytosolic C terminal tail of p22phox 44 This mutation in the PRR of p22phox disrupted the interaction between p22phox and p47phox confirming the importance of this domain in the oxidase activation in neutrophils Since p22phox is ubiquitous and associated with different NOXs it could be logical that CGD patients suffer from the consequences of the absence of p22phox expression in tissues However it is far from being evident One possibility could be that the humans may be able to compensate for the absence of p22phox and or NOXs in cells and tissues other than phagocytes Given the rarity of the AR CGD220 forms information on the severity of this type of CGD is difficult to establish A relationship between the presence of residual ROS production and the survival of CGD patients has been found 45 In case of CYBA mutations leading to the absence of p22phox NOX2 expression is also absent and disables cytochrome b558 the redox element of the NADPH oxidase complex Therefore these mutations behave similarly to severe X CGD The molecular and phenotypic characterization of a p22phox deficient mouse strain with the Tyr121His missense mutation in CYBA has been described 46 The p22phox deficiency results in the clinical and biological characteristics of CGD as well as a severe balance disorder in these mice As the site of p22phox expression is in the inner ear p22phox has been proposed as being involved in the control of vestibular organogenesis In addition mutations of NOX3 in head tilt mice were associated with vestibular defects 47 48 Yet the in vivo relevance of p22phox for NOX3 function remains uncertain because AR CGD220 patients do not suffer from vestibular dysfunction personal data One possibility could be that the human brain may be able to compensate the balance defect In Matsumoto Eosinophilia Shinshu MES rats a loss of function mutation in CYBA was responsible for spontaneous and severe blood eosinophilia 49 These rats suffered from a balance defect due to a leak of otoconia in the inner ear like nmf333 mice In addition MES rats retained normal innate immune defense against Staphylococcus aureus infection probably because of the hypereosinophilia However the mechanisms by which CYBA mutations lead to eosinophilia remain unknown Clinical relevance of single nucleotide polymorphisms editContrary to CYBB CYBA supports a relatively high number of single nucleotide polymorphisms SNPs that could influence the level of ROS generation These SNPs were mainly associated with cardiovascular diseases such as hypertension 50 coronary artery disease CAD coronary heart disease CHD 51 52 and also cerebral ischemic diseases 53 54 The first and most widely studied is the C242T polymorphism is located in exon 4 at position 214 from the ATG and resulting in a non conservative His72 substitution for a Tyr 5 Inoue et al first found that the T allele of the C242 polymorphism might have a protective effect against CAD 55 Despite some evidence of the effect of this polymorphism on ROS generation at the cellular level the association of the CYBA C242T polymorphism with cardiovascular diseases has been widely reported but with conflicting results 52 Single SNP analysis may explain the discrepancies among CYBA association studies A global approach such as haplotype analysis is probably a better approach to understand the impact of CYBA genetic variability on diseases 56 57 58 CYBA variants together with polymorphism analysis of lipid metabolism or stress oxidant pathway genes are of great interest as well 59 60 61 However for future investigations regarding the effect of these polymorphisms it is crucial that the number of patients under study provide sufficient statistical power In addition genetics studies that include control of external factors should be extremely informative Finally since 2010 nine Chinese meta analyses of the C242T polymorphism have been published in relation with CAD 62 63 64 65 66 hypertension 50 atherosclerosis or diabetes and its complications 54 and ischemic cerebrovascular diseases 53 54 The results from these meta analyses were controversial Several factors could influence these data the search strategy the identification of relevant studies publication bias the statistical analysis including a sufficient sampling the prevalence of the studied polymorphism in the studied population minor allele frequency MAF and the type of population population based or not for example Results of these meta analyses need to be confirmed with larger samples In addition a meta analysis based on genome wide association study data will be of great interest in the future Notes editThe 2016 version of this article was updated by an external expert under a dual publication model The corresponding academic peer reviewed article was published in Gene and can be cited as Marie Jose Stasia 2 April 2016 CYBA encoding p22 phox the cytochrome b558 alpha polypeptide gene structure expression role and physiopathology Gene Gene Wiki Review Series 586 1 27 35 doi 10 1016 J GENE 2016 03 050 ISSN 0378 1119 PMC 5637546 PMID 27048830 Wikidata Q38799163 References edit a b c GRCh38 Ensembl release 89 ENSG00000051523 Ensembl May 2017 a b c GRCm38 Ensembl release 89 ENSMUSG00000006519 Ensembl May 2017 Human PubMed Reference National Center for Biotechnology Information U S National Library of Medicine Mouse PubMed Reference National Center for Biotechnology Information U S National Library of Medicine a b c Dinauer MC Pierce EA Bruns GA Curnutte JT Orkin SH Nov 1990 Human neutrophil cytochrome b light chain p22 phox Gene structure chromosomal location and mutations in cytochrome negative autosomal 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jzus B1400241 PMC 4432989 PMID 25990054 External links editOverview of all the structural information available in the PDB for UniProt P13498 Cytochrome b 245 light chain at the PDBe KB Retrieved from https en wikipedia org w index php title Cytochrome b 245 alpha polypeptide amp oldid 1215931501, wikipedia, wiki, book, books, library,

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