ライフサイエンスコーパス: cytochrome b5

1 tified by mass spectrometry as calumenin and cytochrome B5.

2 in ActA or the endoplasmic reticulum protein cytochrome b5.

3 presence of an N-terminal domain related to cytochrome b5.

4 been purified to homogeneity and is soluble cytochrome b5.

5 to be involved in binding the heme domain of cytochrome b5.

6 ied that exhibited decreased ability to bind cytochrome b5.

7 s reduced differential absorbance spectra of cytochrome b5.

8 entical to the one elucidated for microsomal cytochrome b5.

9 m the heme propionate carbonyl carbons in OM cytochrome b5.

10 ) is 48% identical to that of rat microsomal cytochrome b5.

11 the lyase reaction, even in the presence of cytochrome b5.

12 g the several reactions that utilize reduced cytochrome b5.

13 e for interprotein electron self-exchange in cytochrome b5.

14 s, catalyzes the NADH-dependent reduction of cytochrome b5.

15 s and revealed the transmembrane topology of cytochrome b5.

16 organ interval flanked by genes Cysteine and Cytochrome B5.

17 wo conserved side chain packing motifs in OM cytochrome b5s.

18 bilizing isomer A relative to isomer B in Mc cytochromes b5.

19 rkably different properties of rat OM and Mc cytochromes b5.

20 rd chemical and thermal denaturation than Mc cytochromes b5.

21 o acid sequence of the full-length house fly cytochrome b5 (134 residues) is 48% identical to that of

22 Cytochrome b5 (a soluble form lacking the 20-amino-acid

23 Cytochrome b5, a microsomal electron-transfer protein, e

24 (CYP101) induced by the soluble fragment of cytochrome b5, a nonphysiological effector of CYP101, we

25 oup of CYP101-bound camphor upon addition of cytochrome b5, a phenomenon also associated with the for

26 he presence of an equimolar concentration of cytochrome b5 and a 10-fold molar excess of NADPH-cytoch

27 % similarity to that of the yeast microsomal cytochrome b5 and a 35% identity and 54% similarity to t

28 ple of an animal flavohemoprotein containing cytochrome b5 and chrome b5 reductase cytodomains.

29 physiological interaction between microsomal cytochrome b5 and cytochrome c (recently reviewed) has i

30 ond-order electron transfer reaction between cytochrome b5 and cytochrome c has been studied by cycli

31 sured for the association between microsomal cytochrome b5 and cytochrome c, clearly indicates that t

32 studies indicate that the binding sites for cytochrome b5 and cytochrome P450 reductase are, as pred

33 teins known to be stable without heme (e.g., cytochrome b5 and hemoglobin apoprotein) are significant

34 oups in the electrostatic binding between OM cytochrome b5 and horse heart cytochrome c was investiga

35 atic stabilization of the complex between OM cytochrome b5 and horse heart cytochrome c.

36 itution with the electron transport proteins cytochrome b5 and NADH-cytochrome b5 reductase.

37 -component redox system comprised of soluble cytochrome b5 and P450 reductase.

38 Cytochrome b5 and phosphorylation enhance 17,20 lyase ac

39 The combination of cytochrome b5 and phosphorylation was not additive.

40 at the structures of bovine liver microsomal cytochrome b5 and rat liver OM cytochrome b5 are almost

41 erized with respect to their ability to bind cytochrome b5 and support substrate oxidation.

42 nate from the formation of a complex between cytochrome b5 and the modified electrode surface which (

43 the removal of the membranous segments from cytochrome b5 and the NADH-cytochrome b5 reductase.

44 1 repeats, a structural motif in common with cytochrome b5, and a HECT domain in common with E6-AP ub

45 orming an electron transfer chain with NADH, cytochrome b5, and NADH-dependent cytochrome b5 reductas

46 with insect NADPH cytochrome P450 reductase, cytochrome b5, and NADPH, the purified CYP4C7 metabolize

47 er microsomal cytochrome b5 and rat liver OM cytochrome b5 are almost identical when compared at medi

48 yme systems, we now show that the actions of cytochrome b5 are independent of the state of P450c17 ph

49 Identification of soluble cytochrome b5 as a member of the reductive activation sy

50 egrees C while the dissociation of heme from cytochrome b5 at room temperature occurs 3 orders of mag

51 Cytochrome b5 augments the 17,20-lyase activity of cytoc

52 mals, a flavohemoprotein (b5+b5R) containing cytochrome b5 (b5) and b5 reductase (b5R) domains.

53 Two acidic residues, Glu-48 and Glu-49, of cytochrome b5 (b5) are essential for stimulating the 17,

54 The membrane heme protein cytochrome b5 (b5) can enhance, inhibit, or have no effe

55 the need for the substrate testosterone and cytochrome b5 (b5) for reduction and as to whether reduc

56 ncreasing ionic strength and the presence of cytochrome b5 (b5) on these two systems.

57 Cytochrome b5 (b5) stimulates the rate of the 17,20-lyas

58 amined are enhanced by the accessory protein cytochrome b5 (b5), but the exact role of b5 in P450 17A

59 trates, and binding of the soluble domain of cytochrome b5 (b5).

60 Cygb and the reducing systems, cytochrome b5 (B5)/cytochrome b5 reductase (B5R) and cyt

61 Cytochrome b5 binding to CYP17A1 is also mutually exclus

62 We have found that Dap1p, like cytochrome b5, binds to heme and that Dap1p targets the

63 (rOM b5) and ferric bovine liver microsomal cytochrome b5 (bMc b5).

64 s to synthesize the Saccharomyces cerevisiae cytochrome b5 by using both LCR and assembly PCR.

65 f full-length microsomal cytochrome-P450 and cytochrome-b5 by solid-state NMR spectroscopy.

66 The small heme-containing protein cytochrome b5 can facilitate, inhibit, or have no effect

67 These data indicate that microsomal cytochrome b5 can play a major role in the in vivo metab

68 , and in vitro plant systems have shown that cytochrome b5 can, at least in some circumstances, also

69 A microsomal cytochrome b5 cDNA from the house fly, Musca domestica,

70 full-length mammalian 72-kDa cytochrome P450-cytochrome b5 complex in lipid bilayers.

71 ) resonances were monitored as a function of cytochrome b5 concentration by 1H-15N TROSY-HSQC experim

72 The effector activity of the particular rat cytochrome b5 construct used for NMR studies was confirm

73 In vitro studies have demonstrated that cytochrome b5 (Cyb5) also modulates P450 function.

74 ins NADH-cytochrome b5 reductase (CYB5R) and cytochrome b5 (CYB5), it catalyzes the reduction of N-hy

75 finity (a Kd of 13 +/- 3 mM, for the reduced cytochrome b5-CYP-S-CO complex compared to a Kd of 26 +/

76 evious molecular dynamics (MD) simulation of cytochrome b5 (cyt b5) at 25 degrees C displayed localiz

77 (Mb) and its physiological partner protein, cytochrome b5 (cyt b5) can be "symmetrized": the [Mb:cyt

78 We report here on two such ET complexes: cytochrome b5 (cyt b5) in reaction with its physiologica

79 Cytochrome b5 (cyt b5) is a membrane-anchored electron-c

80 Mammalian cytochrome b5 (cyt b5) is a membrane-bound protein capab

81 stigate localized dynamics on the surface of cytochrome b5 (cyt b5) that result in the formation of a

82 th membrane-bound P450 and its redox partner cytochrome b5 (cytb5 ) have been found to be important f

83 uentially delivered from its redox partners: cytochrome b5 (cytb5) and cytochrome P450 reductase, bot

84 Microsomal cytochrome b5 (cytb5) is a membrane-bound protein that m

85 ds that produce various heme proteins (e.g., cytochrome b5, cytochrome b562, and hemoglobin) in the p

86 formed on a solution containing a mixture of cytochrome b5, cytochrome c and polylysine, cytochrome b

87 Cytochrome b5 decreases the apparent Km for P450 reducta

88 tes that FA2H protein contains an N-terminal cytochrome b5 domain and four potential transmembrane do

89 de transmembrane sequences and a part of the cytochrome b5 domain are essential for the basal stabili

90 FA2H lacking the N-terminal cytochrome b5 domain had little activity, indicating tha

91 Expression of the S. cerevisiae FAH1 cytochrome b5 domain in Escherichia coli produces a solu

92 aliana FAH1 gene, which does not contain the cytochrome b5 domain, in the fah1Delta strain produced a

93 84-amino acid protein with an amino-terminal cytochrome b5 domain.

94 -affinity iron uptake system in an animal, a cytochrome b5 electron donor for ferric iron reduction,

95 tion potential (outer mitochondrial membrane cytochrome b5, Eo = -102 mV; microsomal cytochrome b5, E

96 rane cytochrome b5, Eo = -102 mV; microsomal cytochrome b5, Eo = 3 mV) in the presence of another pro

97 Two distinct forms of cytochrome b5 exist in the rat hepatocyte.

98 Suppressing cytochrome b5 expression in human adrenal NCI-H295A cell

99 ochrome b5 reductase provides electrons, via cytochrome b5, for a range of biochemical reactions in c

100 can instead accept the second electron from cytochrome b5, for human steroidogenic CYP17A1, the cyto

101 ly demethylates m6A of targeted mRNA such as cytochrome b5 form A (CYB5A) to increase its mRNA stabil

102 ectroscopy reveal properties very similar to cytochromes b5 from vertebrates.

103 In erythrocytes, soluble cytochrome b5 functions in methemoglobin reduction.

104 orientation on electrochemical properties of cytochrome b5 have been performed.

105 yed by the outer mitochondrial membrane (OM) cytochrome b5 heme propionate groups in the electrostati

106 Anti-cytochrome b5 IgG decreased NADPH- and NADH-dependent HE

107 ntally, the interaction of cytochrome c with cytochrome b5 immobilized on a negatively charged monola

108 Interestingly, the addition of cytochrome b5 improved the coupling of the mutant, resul

109 at of NADPH, and assess the possible role of cytochrome b5 in HER formation.

110 human P450-oxidoreductase (OR), and/or human cytochrome b5 in Saccharomyces cerevisiae and analyzed t

111 d out the conditional deletion of microsomal cytochrome b5 in the liver to create the hepatic microso

112 The inclusion of cytochrome b5 in the reconstituted enzyme system is with

113 The inclusion of cytochrome b5 in the reconstituted system of 2D6 and 2C9

114 tion of P450c17 and the allosteric action of cytochrome b5 increase 17,20 lyase activity, but it has

115 sociation constant for manganese-substituted cytochrome b5 increased with temperature from 4 nM at 20

116 The resonance Raman spectrum of MnII cytochrome b5 indicated a high-spin pentacoordinate stru

117 ), the dissociation of manganese substituted cytochrome b5 into the apoprotein and free Mn protoporph

118 indicates that the site of interaction on OM cytochrome b5 is almost identical to the one elucidated

119 When the reduction potential of cytochrome b5 is measured with the aid of several differ

120 The cytochrome b5 is reduced by house fly cytochrome P450 re

121 3 (CER3) and endoplasmic reticulum-localized cytochrome b5 isoforms (CYTB5s).

122 conserved NAD(P)H reductase that contains a cytochrome b5-like domain at the N terminus and a cytoch

123 s two membrane-spanning domains as well as a cytochrome b5-like domain that is characteristic of nonm

124 accharomyces cerevisiae genome data base for cytochrome b5-like sequences identified a 1.152-kilobase

125 able effect on expression of CYP1A1, CYP2D6, cytochrome b5, liver or intestinal fatty acid binding pr

126 as much as 30% of the manganese-substituted cytochrome b5 may dissociate to free Mn-protoporphyrin I

127 rs a mechanism whereby allosteric binding of cytochrome b5 might selectively enhance the lyase reacti

128 In vitro, cytochrome b5 modulates the rate of cytochrome P450-depe

129 and which constitutes part of the surface of cytochrome b5, modulates its reduction potential.

130 decreased by 3.6-fold in hepatic microsomal cytochrome b5 null mice.

131 n the liver to create the hepatic microsomal cytochrome b5 null mouse.

132 50 enzymes showed that in hepatic microsomal cytochrome b5 null NADH-mediated metabolism was essentia

133 similar shifts in the reduction potential of cytochrome b5 occur when it forms a complex with physiol

134 mitochondrial membrane isoform of mammalian cytochrome b5 (OM b5) is considerably more stable than i

135 xial ligands in outer mitochondrial membrane cytochrome b5 (OM cyt b5) has been replaced by a methion

136 d in bacteria, human P450c17 required either cytochrome b5 or phosphorylation for 17,20 lyase activit

137 ion of both flavonoid 3',5'-hydroxylases and cytochrome b5 Overall, this work provides new insight in

138 The NAD(P)H cytochrome b5 oxidoreductase, Ncb5or (previously named b

139 onate located on the exposed heme edge of OM cytochrome b5 participates in the electrostatic binding

140 onate located on the exposed heme edge in OM cytochrome b5 participates in the electrostatic stabiliz

141 F5H uniquely requires the cytochrome b5 protein CB5D as an obligatory redox partne

142 ic Iron Reductase) and Fire-like, as well as cytochrome b5 protein Firewood, are required for iron ab

143 The house fly cytochrome b5 protein was overexpressed in Escherichia c

144 ow-spin heme similar to those found in other cytochrome b5 proteins.

145 osomal cytochrome P450 reductase and soluble cytochrome b5 reconstitute the activity of the porcine m

146 The structure and stability of cytochrome b5 reconstituted with manganese protoporphyri

147 and the reducing systems, cytochrome b5 (B5)/cytochrome b5 reductase (B5R) and cytochrome P450 reduct

148 emia caused by an erythrocytic deficiency of cytochrome b5 reductase (b5R; type I) in African-America

149 Cytochrome b5 reductase (cb5r) (EC 1.6.6.2) catalyzes th

150 Cytochrome b5 reductase (cb5r), a member of the ferredox

151 gle base pair change in a gene encoding NADH:cytochrome b5 reductase (CBR1, At5g17770).

152 er with the electron transport proteins NADH-cytochrome b5 reductase (CYB5R) and cytochrome b5 (CYB5)

153 asured in CHO cell lines overexpressing NADH:cytochrome b5 reductase (NBR), NADPH:cytochrome P450 red

154 ion of long chain fatty acids 7 (Elovl7) and cytochrome B5 reductase 2 (Cyb5r2) and the synaptic regu

155 Here, we identify cytochrome b5 reductase 3 (Cyb5r3) down-regulation as a

156 NADH cytochrome b5 reductase 3 (CYB5R3) is critical for reduc

157 Here, we show that cytochrome b5 reductase 3 (CYB5R3), an enzyme known to r

158 s reduced to the Fe(2+) state by endothelial cytochrome b5 reductase 3 (CYB5R3, also known as diaphor

159 sights into NO-sGC-cGMP signaling and reveal cytochrome b5 reductase 3 as the first identified physio

160 Mechanistically, we show that cytochrome b5 reductase 3 directly reduces oxidized sGC

161 in vascular smooth muscle cells reveal that cytochrome b5 reductase 3 expression and activity is cri

162 n and form protein-protein complexes between cytochrome b5 reductase 3, also known as methemoglobin r

163 NADH:cytochrome b5 reductase activates the mitomycins to alky

164 anide reductase activity (indicative of NADH:cytochrome b5 reductase activity) coupled to inhibition

165 DNA insertional mutants of the gene encoding cytochrome b5 reductase in Arabidopsis thaliana, CBR1.

166 The results implicate NADH:cytochrome b5 reductase in the differential bioactivatio

167 These results indicate that cytochrome b5 reductase is not essential during vegetati

168 terminus of E3 to the N terminus of the NADH-cytochrome b5 reductase lacking the myristoyl group and

169 In all eukaryotes, NADH:cytochrome b5 reductase provides electrons, via cytochro

170 Because NADH:cytochrome b5 reductase resides predominantly in the mit

171 Interaction of Mtln with NADH-dependent cytochrome b5 reductase stimulates complex I functioning

172 A cytosolic form of NADH:cytochrome b5 reductase was generated.

173 The orientation of the cytochrome b5 reductase was reversed, from cytosolic to

174 y cell transfectants overexpressing rat NADH:cytochrome b5 reductase were generated.

175 hrome b5-like domain at the N terminus and a cytochrome b5 reductase-like domain at the C terminus.

176 An NADH:cytochrome b5 reductase-transfected clone expressed 9-fo

177 ous segments from cytochrome b5 and the NADH-cytochrome b5 reductase.

178 and beta globin form a complex with eNOS and cytochrome b5 reductase.

179 on transport proteins cytochrome b5 and NADH-cytochrome b5 reductase.

180 with NADH, cytochrome b5, and NADH-dependent cytochrome b5 reductase.

181 ced nicotinamide adenine dinucleotide (NADH)-cytochrome b5 reductase.

182 e binding, while membrane binding of control cytochrome b5 remained unaffected.

183 eractions with the allosteric redox partner, cytochrome b5, required for CYP 17A1's lyase activity.

184 erric rat liver outer mitochondrial membrane cytochrome b5 (rOM b5) and ferric bovine liver microsoma

185 Cytochrome b5 seems to play a role in HER formation, mos

186 The X-ray crystal structure of rat liver OM cytochrome b5 solved to 2.7 A resolution shows that the

187 The results indicate that cytochrome b5 stimulates a step following the first elec

188 Dap1 is a heme-binding protein related to cytochrome b5 that activates Erg11, so that cells lackin

189 In the presence of cytochrome b5 the variant readily metabolized 17EE and w

190 y acids, CER1-LIKE1 interacted with CER3 and cytochrome B5 to form a functional complex leading to th

191 sed amounts of POR, the allosteric action of cytochrome b5 to promote POR-P450c17 interaction, and Se

192 a possible route for electron transfer from cytochrome b5 to the di-iron centre.

193 cytochrome b5, cytochrome c and polylysine, cytochrome b5 undergoes reversible electrochemistry at t

194 catalyzes the reduction of two molecules of cytochrome b5 using NADH as the physiological electron d

195 The resonance Raman spectrum of MnIII cytochrome b5 was consistent with a high-spin hexacoordi

196 ctric constant on the reduction potential of cytochrome b5 was corroborated by preparing the V45L/V61

197 To achieve these aims, 13C-labeled heme OM cytochrome b5 was expressed in Escherichia coli as previ

198 Interestingly, cytochrome b5 was found to dramatically inhibit both P45

199 Data for cytochrome b5 were analyzed and, when the self-associati

200 Mutants of cytochrome b5 were designed to achieve reorientation of

201 rent K(m) for NADH increased; the K(m)'s for cytochrome b5 were unchanged relative to that of the wil

202 Dap1p is related to cytochrome b5, which activates cytochrome P450 proteins,

203 Cytochrome b5, which augments several P450 activities, i

204 which is activated by a di-iron centre, and cytochrome b5, which regenerates the di-iron centre.

205 thionine synthase in the presence of soluble cytochrome b5 with a Vmax of 2.8 +/- 0.1 micromol min(-1

206 Titrations of [13C]heme-labeled OM cytochrome b5 with horse heart cytochrome c were carried

207 The association of cytochrome b5 with the reduced CYP101-camphor-carbon mon