ライフサイエンスコーパス: PGG

1 PGG also inhibited cell proliferation in both cell lines

2 PGG also inhibited IkBKE and MAPK1 genes and the protein

3 PGG binds specifically to arterial elastin and, in doing

4 PGG glucan-treated animals showed increases in total leu

5 PGG inhibited growth of both CRAB and susceptible A. bau

6 PGG is a gallotannin produced by a variety of medicinal

7 PGG.SNV archives 265 million SNVs across 220,147 present

8 nic acid is converted to prostaglandin G(2) (PGG(2)) by the cyclooxygenase activities of prostaglandi

9 e arachidonic acid (AA), prostaglandin G(2) (PGG(2)), and cyclooxygenase 2 (COX-2).

10 the PGHS-cyclooxygenase, prostaglandin G(2) (PGG(2)), by elevating the concentration of either enzyme

11 We report here the purification of a PGG-glucan-binding element from human leukocytes and its

12 taglandin precursors, arachidonic acid (AA), PGG(2) and PGH(2).

13 or, whereas alpha-pentagalloylglucose (alpha-PGG) acts as a mixed-type inhibitor.

14 etween PRO and PGO and eight between PGO and PGG.

15 o using cytotoxicity, elastin stability, and PGG-elastin interaction assays.

16 fferences from WT behavior occur in both apo PGG/GGG and in the form bound to the reaction-intermedia

17 g this time (and were often hotly debated at PGG meetings).

18 gest that the protective effect exhibited by PGG glucan in the rat peritonitis model is mediated, at

19 In conclusion, PGG exhibits antimicrobial activity against CRAB, but du

20 st neighbours on a cyclic network after each PGG round.

21 the fluid space was reduced to 5 A at an EPC:PGG mole ratio of 5:1.

22 keratinocytes (HaCaTs) yielded an IC(50) for PGG of 256 ug/mL.

23 n chelation as a possible mode of action for PGG's activity against CRAB.

24 espectively); similarly, the K(m) values for PGG(2) and 15-HETE formation by V349L oPGHS-1 were diffe

25 With native enzyme, the K(m) values for PGG(2), 11-HETE, and 15-HETE formation were each differe

26 3-proS hydrogen from arachidonate which, for PGG(2) formation, is followed by insertion of O(2) at C-

27 whether protection could be transferred from PGG glucan-treated animals to naive recipients via splee

28 peration in a large-scale public goods game (PGG).

29 -beta-glucotriosyl-(1-3)-beta-glucopyranose (PGG) glucan, a biological-response modifier, in protecti

30 -beta-glucotriosyl-(1-3)-beta-glucopyranose (PGG)-glucan and Bacteroides fragilis polysaccharide A (P

31 -anomers of penta-O-galloyl-D-glucopyranose (PGG), 2 and 3, act as insulin mimetics that bind to and

32 3,4,6-penta- O-galloyl-beta-d-glucopyranose (PGG), binds to capillary morphogenesis gene 2 (CMG2) wit

33 enols, only penta-O-galloyl-alpha-D-glucose (PGG) was able to completely mimic the effects of TA by c

34 enols was tested using pentagalloyl glucose (PGG) as a standard, an important representative element

35 e the natural compound pentagalloyl glucose (PGG) effects on TNF-a activated TNBC cell lines, MDA-MB-

36 tringency expressed in pentagalloyl glucose (PGG) units in concentrations ranging from 1 to 140mumol/

37 ng to the isolation of pentagalloyl glucose (PGG), a bioactive gallotannin.

38 of aortic elastin with pentagalloyl glucose (PGG), an elastin-binding polyphenol, would interfere wit

39 ravenous injections of pentagalloyl glucose (PGG)-loaded nanoparticles conjugated with elastin antibo

40 goeldii (PGG) and elucidates the chromosomal rearrangements in th

41 e since the first Population Genetics Group (PGG) meeting in January 1968.

42 Imprime PGG (Imprime) is an i.v. administered, yeast beta-1,3/1,

43 and evolutionary parameters is available in PGG.SNV, a unique feature compared with other databases.

44 this in terms of altered loop-6 dynamics in PGG/GGG.

45 ical aspects were monitored and evaluated in PGG-treated aortas compared with saline-treated control

46 ranged from 0.17 to 4.7 uM, as expressed in PGG units.

47 Overall, concentrations > 1.0 uM in PGG units are signaling electrochemical impedance, provi

48 These findings indicate PGG anti-cancer ability in inhibiting tumor cell prolife

49 In response, low PGG contributors increase their contributions if both ne

50 With this model, PGG was delivered periadventitially at 2 separate time p

51 Moreover, PGG induced apoptosis, modulating caspases, and TNF supe

52 f wild-type (WT) TIM and a quintuple mutant (PGG/GGG).

53 The single-hinge mutants PGG and GGG had k(cat) values 200-fold lower than that o

54 , participants do not know their neighbours' PGG contribution and thus cannot link play in the PD to

55 portion of the in vivo antitumor activity of PGG may be the result of antiangiogenic activity mediate

56 on of acetaminophen, as does the addition of PGG(2) itself.

57 Periadventitial administration of PGG hinders the development of AAA in a clinically relev

58 y, oral or intraperitoneal administration of PGG inhibits angiogenesis in the mouse corneal micropock

59 a linear correlation of the concentration of PGG(2) with an LOD of 0.227microM.

60 We show that targeted delivery of PGG could reverse the aortic dilation, ameliorate the in

61 In this work, we synthetized derivatives of PGG with different sugar cores and phenolic substituents

62 The protective effect of PGG glucan was abrogated by treatment with indomethacin,

63 Safety and efficacy of PGG treatment were first tested in vitro using cytotoxic

64 For in vivo studies, the efficacy of PGG was evaluated within a well-established AAA model in

65 a reduction of the 15-hydroperoxyl group of PGG(2) to form PGH(2) catalyzed by the peroxidase activi

66 ventitial delivery of noncytotoxic levels of PGG inhibits elastin degeneration, attenuates aneurysmal

67 ified prostaglandin extract from the sera of PGG glucan-treated animals protected against mortality i

68 Therefore, simple iv therapy of PGG loaded nanoparticles can be an effective treatment o

69 calability of this effect: in a 1,000-person PGG, participants in the treatment condition successfull

70 ble activity (t-Boc-PGP-OMe, N-acetyl-P, PG, PGG, GP, GG and gly-pro-hyp).

71 V349L oPGHS-1 formed primarily PGG(2), 15S-HETE, and 15R-HETE but only trace amounts of

72 Native forms of oPGHS-1 produced primarily PGG(2) but also several monohydroxy acids, which, in ord

73 for CMG2 than the natural glucose prototype PGG and proved to be a potent angiogenesis inhibitor.

74 The immunomodulator Betafectin(R) PGG-glucan is a homopolymer of glucose derived from yeas

75 Radiolabeled PGG-glucan bound several other neutral glycosphingolipid

76 The binding of radiolabeled PGG-glucan to lactosylceramide was not inhibited by glyc

77 The binding of radiolabeled PGG-glucan to purified lactosylceramide was saturable, s

78 ere found to support binding to radiolabeled PGG-glucan.

79 Remarkably, PGG induced a 154-fold increase in TNF expression in MDA

80 Previous work demonstrated that PGG/GGG has a tenfold higher Km value and 10(3)-fold red

81 now report the serendipitous discovery that PGG (1,2,3,4,6-penta-O-galloyl-beta-D-glucopyranose) is

82 We find that PGG inhibits CMG2 with a submicromolar IC50 and it also

83 These data show that PGG/GGG exists in multiple conformations that are not fu

84 The results obtained showed that PGG reduced the expression of the cytokine GRO-a/CXCL1.

85 bserve a sharp decline of cooperation in the PGG, while in the treatment condition global cooperation

86 with neighbours who contribute little in the PGG.

87 -iso-prostaglandin F2alpha, an isomer of the PGG/H synthase (cyclooxygenase or COX) enzyme product, p

88 n and thus cannot link play in the PD to the PGG.

89 s to a much more international one (with the PGG meetings having made important contributions to the

90 Thus, PGG use may be recommended as an adjunct therapy for TNB

91 The PRP-biosensor was able to bind to PGG with higher sensitivity, displaying lower limit of t

92 ounds on PRP and on alpha-amylase binding to PGG were tested (gallic acid, catechin, ethanol, glucose

93 he cyclooxygenase site of oPGHS-1 leading to PGG(2), 11R-HETE, and 15S-HETE and/or 15R-HETE, respecti

94 H(2), but does have a marked activity toward PGG(2) converting it to PGE(2) and 15-keto-PGE(2).

95 minal hinge was mutated to P166/V167G/W168G (PGG), and the C-terminal hinge was mutated to K174G/T175

96 eukocytes or serum from animals treated with PGG glucan.

97 initial oxygenation of arachidonate to yield PGG(2) catalyzed by the cyclooxygenase activity of the e

98 the molecule is optimally arranged to yield PGG(2) versus monohydroperoxy acid products (Val-349, Tr