ライフサイエンスコーパス: pteridine

1 te to the beneficial vascular effects of the pteridine.

2 rst and NADP+ dissociating after the reduced pteridine.

3 acked significant activity for non-quinonoid pteridines.

4 ine metabolites were prepared in the purine, pteridine, [1,2,5]-thiadiazolo[3,4-d]pyrimidine, and qui

5 zyme, which had a ratio of 0.84 mol of bound pteridine:1 mol of nNOS 160 kDa subunit.

6 no-5-deaza-7H-6,7,8,9-tetrahydropyrido[3,4-g]pteridine (23), followed by regioselective alkylation of

7 t screening lead, 4-amino-7-aryl-substituted pteridine (5) (AK IC(50) = 440 nM), led to the identific

8 arates and detects the following six urinary pteridines: 6-biopterin, 6-hydroxymethylpterin, d-neopte

9 thways, demonstrating variable production of pteridine and human milk oligosaccharide products.

10 (pugD), that causes variegated reductions in pteridine and ommochrome pigmentation of the Drosophila

11 ween the adenosine fragment of NADPH and the pteridine and p-aminobenzoyl fragments of methotrexate,

12 Both the pteridine and p-aminobenzoyl rings are located in the hy

13 Pteridine and PABA levels in transgenic fruit were >20-f

14 The positions of the pteridine and pABA rings of PT523 and the nicotinamide a

15 iants and identified the correlation between pteridines and genetic variants.

16 ion (I/R) injury, we synthesized a series of pteridines and pyridopyrazines.

17 um eye is pigmented only by ommochromes, not pteridines, and indicate that Tcv is potentially useful

18 elanosomes, red and yellow xanthophores with pteridine- and/or carotenoid-containing vesicles, and ir

19 Pteridines are a class of compounds excreted in urine, t

20 Because pteridines are derived from GTP, the pigment defect may

21 The detection limits of these pteridines are under 1 x 10(-10) M.

22 e needed for proper investigation of urinary pteridines as breast cancer biomarkers.

23 preliminary studies have implicated urinary pteridines as candidate biomarkers in a growing number o

24 These findings, alongside the known role of pteridines as redox shuttles, suggest a previously unrec

25 e present study, SD-208, a 2,4-disubstituted pteridine, ATP-competitive inhibitor of the TGFbeta rece

26 ovide a basis for the further development of pteridine-based compounds, and we expect our multitarget

27 enzymes that are required for riboflavin and pteridine biosyntheses.

28 We show that the pteridine biosynthesis pathway, which ancestrally produc

29 st energy production, nucleotide metabolism, pteridine biosynthesis, and fatty acid oxidation as key

30 he distances between the nicotinamide C4 and pteridine C6 and C7 are very short, 2.1 and 1.7 A in the

31 vides experimental proof of the existence of pteridine conformers through rotation about the C(6)-C(9

32 f the probe phosphoramidite, purification of pteridine-containing sequences and a deprotection proced

33 This engineering maneuver raised fruit pteridine content by 3- to 140-fold and fruit folate con

34 llow bodies, suggesting that ommochromes and pteridines contribute to O. fasciatus body color.

35 aa identity), which are hypothesized to be a pteridine-dependent dioxygenase and a regulatory protein

36 amino-5-deaza-6,7,8,9-tetrahydropyrido[3,4-g]pteridine derivatives 3-9 with different benzyl and a be

37 Computational fragment-based design of novel pteridine derivatives along with iterations of crystallo

38 All the pteridine derivatives except 2-amino-O4-benzylpteridine-

39 Eight different pteridine derivatives were well separated in 0.1 M Tris-

40 Novel substituted pteridine-derived inhibitors of monocarboxylate transpor

41 hen alkylated by 2,4-diamino-6-(bromomethyl)-pteridine followed by ester saponification at room tempe

42 taining donor-acceptor systems, in which the pteridine fragment of the molecule acts as an acceptor,

43 benzoic acid with 2,4-diamino-6-(bromomethyl)pteridine gave the target compounds.

44 h are folate biosynthesis intermediates; and pteridine glycosides not previously found in plants.

45 synthesized from 2, 4-diamino-6-(bromomethyl)pteridine in 50-75% yield by reaction with the sodium sa

46 ector enables us to detect minute amounts of pteridines in body fluid.

47 The accumulated pteridines included neopterin, monapterin, and hydroxyme

48 these results, we identified a set of other pteridines, including the essential cofactor tetrahydrob

49 The method detection limit for the pteridines is between 0.025 and 0.5 mug/L, and for creat

50 fluorescence (LIF) detection, to monitor the pteridine levels in urine.

51 these results into a comprehensive model of pteridine metabolism and discuss its implications in che

52 Thus, the control of pteridine metabolism has relevance to the mechanism of L

53 reductase-thymidylate synthase in Leishmania pteridine metabolism, using purified enzymes and knockou

54 lar copper homeostasis and redox balance via pteridine metabolism.

55 secondary metabolic enzymes and encodes new pteridine metabolites functionalized with cis-amide acyl

56 ic acid breaks down into fragments while the pteridine moiety remains intact likely evolving into 6-f

57 ing data, and (2) the calculated pKa for the pteridine N1 of the inhibitor while bound to the protein

58 The pteridine nucleoside analog 3-methyl isoxanthopterin (3-

59 nd P6(5) structures a water molecule bridges pteridine O4 and Trp-22(N epsilon 1) with ideal geometry

60 phosphinic acid esters with a 6-(bromomethyl)pteridine or the corresponding (bromomethyl)pyridopyrmid

61 Engineered fruit with intermediate levels of pteridine overproduction attained the highest folate lev

62 When transgenic PABA- and pteridine-overproduction traits were combined by crossin

63 Plants synthesize folate from pteridine, p-aminobenzoate (PABA), and glutamate moietie

64 Folates are synthesized from pteridine, p-aminobenzoate (PABA), and glutamate precurs

65 tabolites to be synthesized by a hybrid NRPS-pteridine pathway.

66 The effect of pugD on pteridine pigmentation is most dramatic: the only remain

67 unexpected discovery of the participation of pteridine pigments in wing and wing-vein coloration, ind

68 optimized for simultaneous detection of six pteridines previously implicated in breast cancer and cr

69 rate that engineering a moderate increase in pteridine production can significantly enhance the folat

70 Previously, we increased pteridine production in tomato fruit up to 140-fold by o

71 protozoans depend upon exogenous sources of pteridines (pterins or folates) for growth.

72 A small compound library of pteridines, purines, and pyrimidines was used to probe c

73 tively with ligands that target the adjacent pteridine-recognition subsite.

74 ich correlates with decreased levels of both pteridine (red) and ommachrome (brown) pigments.

75 methods were used to examine essentiality of pteridine reductase (PTR1) in pterin metabolism in the A

76 The upregulation of pteridine reductase (PTR1) is a major contributor to ant

77 Pteridine reductase (PTR1) is a target for drug developm

78 Pteridine reductase (PTR1) is an NADPH-dependent short-c

79 As pteridine reductase (PTR1) levels are unchanged in SKO a

80 A broad spectrum pteridine reductase (PTR1) was recently identified in Le

81 opterin transporter (BT1) and broad-spectrum pteridine reductase (PTR1).

82 rotozoan Trypanosoma brucei has a functional pteridine reductase (TbPTR1), an NADPH-dependent short-c

83 of the pterin- and folate-salvaging enzymes pteridine reductase 1 (PTR1) and dihydrofolate reductase

84 Mutants lacking pteridine reductase 1 (PTR1) had low levels of H4B, rema

85 Pteridine reductase 1 (PTR1) is a folate pathway enzyme

86 Pteridine reductase 1 (PTR1) is a novel broad spectrum e

87 The enzyme pteridine reductase 1 (PTR1) is a potential target for n

88 volving new molecular targets are important; pteridine reductase 1 (PTR1), an enzyme that reduces dih

89 g apparent picomolar inhibition of T. brucei pteridine reductase 1 (PTR1), nanomolar inhibition of L.

90 ducts, we combined target-based screening on pteridine reductase 1 with phenotypic screening on Trypa

91 a targets beyond dihydrofolate reductase and pteridine reductase 1.

92 The pteridine reductase PruA, which reduces specific dihydro

93 new scaffold for the development of improved pteridine reductase-1 (PTR1) inhibitors and anti-trypano

94 in VcCry1, but that hydrogen bonding to the pteridine ring amine hydrogens is stronger in VcCry-1.

95 a and indicates that the conformation of the pteridine ring and its interactions with the enzyme diff

96 enter of the pore, leads to puckering of the pteridine ring and promotes formation of the transition

97 ra of MTHF suggests that the carbonyl of its pteridine ring in EcPhr experiences stronger hydrogen bo

98 site, coupled with the fixed position of the pteridine ring in the center of the pore, leads to pucke

99 f these data shows that PT523 binds with its pteridine ring in the same orientation observed for meth

100 moiety may stabilize puckering at C6 of the pteridine ring in the transition state.

101 The glutamate residue and the aromatic pteridine ring interact with the primary and secondary r

102 n of the bound N3 pK(a), such that a neutral pteridine ring is preferred for pairwise interaction wit

103 ich the aminobenzoic moiety and the aromatic pteridine ring of folic acid remain outside the cyclodex

104 late (H(4)F) which contains the redox-active pteridine ring of H(4)B.

105 Our data demonstrate that the pteridine ring of MTHF in EcPhr has different interactio

106 he nicotinamide ring of the cofactor and the pteridine ring of the substrate, DHF, at the hourglass c

107 one being more stable-in which the aromatic pteridine ring penetrates into the CD cavity while the g

108 rlaps the more bulky side of the substrate's pteridine ring).

109 de ring, and the N3-O4 amide function on the pteridine ring.

110 ctors on opposite sides of the planes of the pteridine rings.

111 erties of PTR1 suggested a role in essential pteridine salvage as well as in antifolate resistance.

112 e these findings, limitations including poor pteridine specificity, asynchronous or nonexistent renal

113 Pteridines, such as pterins, folates, and flavins, are h

114 edented nonribosomal peptide synthetase-like-pteridine synthase hybrid biosynthetic gene cluster in P

115 Pteridine synthesis capacity is known to drop in ripenin

116 skins were associated with melanogenesis and pteridine synthesis including mitf, ednrb, mc1r, tyr, ml

117 ng GTP cyclohydrolase I, the first enzyme of pteridine synthesis.

118 of GTP cyclohydrolase I, the first enzyme of pteridine synthesis.

119 Among the pteridines, the most potent against P. carinii DHFR and

120 anthopterin B2, a previously uncharacterized pteridine, to bind CutA in both species.

121 reports cationic adduct formation of urinary pteridines under ESI-positive ionization for the first t

122 uid chromatography-mass spectroscopy (LC-MS) pteridine urinalyses among others have helped to enable

123 e methods for modification of azoloannulated pteridines with (hetero)aromatic nucleophiles using a nu