ライフサイエンスコーパス: co-substrate

1 elaxation driven by the interaction with the Co substrate.

2 al pool size and turnover rate of the cycled co-substrate.

3 g of GalOA yields when glucose was used as a co-substrate.

4 converting NO to nitrate ion with oxygen as co-substrate.

5 degrading enzyme that requires pyruvate as a co-substrate.

6 n(II) as a co-factor and 2-oxoglutarate as a co-substrate.

7 rase that utilizes S-adenosylmethionine as a co-substrate.

8 roM, respectively, in the presence of excess co-substrate.

9 he enzyme requires S-adenosylmethionine as a co-substrate.

10 y 13 enzymes in vitro utilizing sucrose as a co-substrate.

11 om Pichia pastoris (PpAOX) and methanol as a co-substrate.

12 L-ascorbic acid (vitamin C) as an essential co-substrate.

13 ellular reductant such as ferredoxin (Fd) as co-substrates.

14 between the available reducing and oxidizing co-substrates.

15 l-Ara4N, when NAD and glutamate are added as co-substrates.

16 the inclusion of appropriate nucleophiles as co-substrates.

17 ing nitric oxide (NO) and dioxygen (O(2)) as co-substrates.

18 atty acid substrates using O(2) and NADPH as co-substrates.

19 lases that use NADPH and molecular oxygen as co-substrates.

20 esolution and analyzed its mode of action on COS substrates.

21 lyst, and in a form that contained iron, the co-substrate 2-oxoglutarate, and the reaction product of

22 d TET enzymes, which use 2-oxoglutarate as a co-substrate(4), CMD1 uses L-ascorbic acid (vitamin C) a

23 t in the absence of CO(2) , only the organic co-substrates acetate, lactate and pyruvate, but not Fe(

24 Co-substrates addition did not increase the ATO degradat

25 ITA binds to the same site on TET2 as the co-substrate alpha-ketoglutarate, inhibiting TET2 cataly

26 sable dependence on the concentration of its co-substrate alpha-ketoglutarate.

27 he binary complexes it forms with either the co-substrate (alpha-ketoglutarate) or the substrate (fum

28 ed a wasteful end-product since it is also a co-substrate and a global regulator of glucose metabolis

29 ichael adduct suggested stabilization of the co-substrate and acyl-binding loops as a possible additi

30 itro kinase assays, ATP-MAc acts as a kinase co-substrate and covalently crosslinks only kinases cont

31 as the activating metal, 2-oxoglutarate as a co-substrate, and ascorbic acid as a cofactor.

32 ith 2 mM Fe(II), amended with 0.6 mM organic co-substrate, and in the presence/absence of CO(2) .

33 although their affinities for each of these co-substrates, and hence their sensitivity to depletion

34 Several cycled co-substrates are well known as energy and electron carr

35 ses (group D), which use reduced flavin as a co-substrate, are less amenable to spectroscopic investi

36 extensin as substrate and 60 microM H2O2 as co-substrate, at 23 degrees pl 4.6 extensin peroxidase g

37 ive yield when CobA is preincubated with the co-substrate ATP.

38 Low concentrations of the co-substrate beta-mercaptoethanol (Kd = approximately 13

39 we have determined the solvent effects of a co-substrate, beta-mercaptoethanol, and of a model nonsu

40 inary approach used here sheds light on the (co)substrate binding mechanism, catalytic step, and (co)

41 time-resolved measurements of intracellular (co-)substrate binding and release.

42 te kinetics indicate that TH has a different co-substrate binding sequence (pterin + O(2) + L-tyr) th

43 The A154T polymorphism is located within the co-substrate binding site.

44 ed similar binding modes for each in the 2OG co-substrate binding site.

45 , a shift from ordered to random addition in co-substrate binding, and a significantly reduced rate o

46 correct target engagement rather than NAD(+) co-substrate binding, and by which the two protomers of

47 function, including S-adenosyl-L-methionine co-substrate binding, beginning with a new sequence alig

48 TlyA interdomain linker as indispensable for co-substrate binding.

49 f serotonin employing varying intracellular (co-)substrate concentrations and interpreted the data us

50 otope effects that increase in proportion to co-substrate concentrations before converging to limitin

51 e reaction and linear pathways, we find that co-substrate cycling imposes an additional flux limit on

52 hematical framework to analyse the effect of co-substrate cycling on metabolic flux.

53 We discuss how the limitations imposed by co-substrate cycling provide experimentally testable hyp

54 ons that could be limited by the dynamics of co-substrate cycling.

55 es of inhibitors based on simple analysis of co-substrate dependency of protein stabilization.

56 srAB dissimilatory sulfite reductase and its co-substrate DsrC.

57 s III histone deacylases that use NAD(+)as a co-substrate during amide bond hydrolysis.

58 We conclude that measuring and controlling co-substrate dynamics is crucial for understanding and e

59 hydroxylases alike decarboxylate the alphaKG co-substrate, facilitating formation of a high-energy fe

60 and it appeared to increase the strength of CO (substrate for acetyl-CoA synthesis) binding to the r

61 Others enhance production of a co-substrate for a downstream enzyme, thereby pulling ma

62 of Mtb TlyA interaction with its obligatory co-substrate for methyltransferase activity, S-adenosyl-

63 ecule in cellular metabolism and an obligate co-substrate for NAD(+)-consuming enzymes, which regulat

64 is not optimized for utilizing H(2)O(2) as a co-substrate for oxidizing L-Trp.

65 -, but not (S)-2-hydroxyglutarate, acts as a co-substrate for the hypoxia-inducible factor prolyl hyd

66 e presence or absence of the enzyme's native co-substrate glutathione (GSH).

67 lytically consumed NO in the presence of the co-substrate hydrogen peroxide (H(2)O(2)).

68 s a radical SAM enzyme that uses oxygen as a co-substrate in its physiologically relevant function.

69 e (alternatively termed 2-oxoglutarate) as a co-substrate in so many oxidation reactions throughout m

70 c5B approximately (125)I-ubiquitin thioester co-substrate in the nanomolar range ([S](1/2) = 140 +/-

71 re also other metabolites that act as cycled co-substrates in different parts of central metabolism.

72 pletion of s-adenosylmethionine (SAM), a key co-substrate involved in methyl group transfer reactions

73 due to subtle differences in the kinetics of co-substrate ion binding in closely related transporters

74 er is exposed to solvent, the 2-oxoglutarate co-substrate likely adopts an inactive conformation in t

75 ropeptide in the presence and absence of its co-substrates may represent a release mechanism for macr

76 monitored the translocation of substrate and co-substrate Na(+) across the lipid bilayer and the tran

77 This purified hSGLT1 transports co-substrates (Na(+) and glucose) and it is inhibited by

78 ol binding site on SIRT2 contact the sirtuin co-substrate NAD(+) during enzymatic catalysis, and assa

79 eased the nuclear concentration of the SIRT1 co-substrate NAD(+), and decreased chromatin accessibili

80 al structures of MtmW and its complexes with co-substrate NADPH and PEG, suggest a catalytic mechanis

81 bition that is dependent on the level of the co-substrate, O(2), and reductant as well as substrate d

82 ich convert Arg into NO and citrulline using co-substrates O2 and NADPH.

83 re makes use of reactive molecular oxygen as co-substrate of oxygenases to hydroxylate and cleave the

84 ZNF746) was initially identified as a novel co-substrate of parkin and PINK1 that leads to Parkinson

85 ilatory sulfur metabolism, where it works as co-substrate of the dissimilatory sulfite reductase DsrA

86 In addition, the effect of organic co-substrates on Fe(II) oxidation rates or the identity

87 age in greater numbers than controls lacking co-substrate or when PIMT protein binding was poisoned w

88 easurement of oxygen consumption, peroxidase co-substrate oxidation or prostaglandin (PG) detection.

89 ementation with acetate, a common wastewater co-substrate, promoted cell growth and PET fragmentation

90 ing in the absence of alpha-ketoglutarate (a co-substrate required by many mononuclear iron enzymes),

91 bolic interdependence of microorganisms, and co-substrate requirements in the catabolism of xenobioti

92 remodelling factors, the Rea1 ATPase and its co-substrate Rsa4, are present on Nug2-associated partic

93 ry metabolic pathways utilising an expensive co-substrate S-adenosyl-l-methionine (SAM) as the methyl

94 these variants, only D47N and L49A bound the co-substrate S-adenosyl-L-methionine.

95 Inclusion of the PIMT co-substrate, S-adenosylmethionine (AdoMet), during pann

96 ants leading to an uncoupled cleavage of the co-substrate SAM.

97 OA and a highly efficient utilization of the co-substrate sorbitol in providing NADPH.

98 viding structural evidence for substrate and co-substrate specificity and the inability of PvdA to bi

99 ant amount (170-fold) only when dCTP was the co-substrate suggesting that a hydrogen bond exists only

100 The lipophilic nature of the co-substrate suggests that electron transfer to CoQ occu

101 Using acetyl-CoA as a co-substrate, the high affinity binding of acetyl-CoA is

102 We investigated the potential role of the co-substrate, thiocyanate (SCN-), in modulating the cata

103 oxygenases that deploy molecular oxygen as a co-substrate to catalyse the post-translational hydroxyl

104 es use an Fe(II) cofactor and 2-oxoglutarate co-substrate to oxidize organic substrates.

105 They utilize oxygen as a co-substrate to produce free cysteine, an aldehyde, and

106 se domain in the presence and absence of the co-substrate UDP-glucose.

107 the traditional UDP-glycosyltransferase UGT co-substrate UDP-glucuronic acid.

108 ribulose-1,5-bisphosphate, the carbon-fixing co-substrate used by ribulose-1,5-bisphosphate carboxyla

109 e their sensitivity to depletion of specific co-substrates, varies widely.

110 Nucleophiles used successfully as co-substrates were thiosulphate, 2-mercaptoethanol, merc

111 Cycling of co-substrates, whereby a metabolite is converted among a

112 mentation with 1,4-dihydroxy-2-naphthoate, a co-substrate with C35 -PP for MenA.