ライフサイエンスコーパス: favipiravir

1 e the bias of particular mutations caused by favipiravir.

2 treated with a combination of ribavirin and favipiravir.

3 The mutant viruses remained susceptible to favipiravir.

4 reatment of monoclonal antibodies (ZMAb) and favipiravir.

5 ing a centralised online process to receive: favipiravir (1,800 mg twice daily on Day 1 followed by 4

6 In US317 (526 favipiravir, 169 placebo), favipiravir did not significa

7 complicated influenza who were randomized to favipiravir (1800 mg twice a day on day 1, 800 mg twice

8 ipants were randomized to receive placebo or favipiravir (1800 mg twice daily [BID] day 1, 800 mg BID

9 s and fever of <=48 hours were randomized to favipiravir (1800 mg twice daily [BID] on day 1, 800 mg

10 In US316 (301 favipiravir, 322 placebo), favipiravir was associated wi

11 in Hartley guinea pigs, we demonstrate that favipiravir, a broad-spectrum antiviral agent and leadin

12 In the case of favipiravir, a polymerase inhibitor with activity agains

13 d trial, in which all patients would receive favipiravir along with standardized care.

14 Favipiravir, an antiviral developed for the treatment of

15 Favipiravir, an oral, RNA-dependent RNA polymerase inhib

16 meric 3-hydroxypyrazine/3-pyrazinone pair of favipiravir and its 6-substituted analogues, 6-Cl, 6-Br,

17 There was no significant interaction between favipiravir and lopinavir-ritonavir (interaction coeffic

18 in testing whether viruses are resistant to favipiravir and may help demonstrate the effect of favip

19 We found a synergistic interaction between favipiravir and ribavirin in vitro and an increased surv

20 s infection, and the broad-acting antivirals favipiravir and ribavirin, exhibited significant deficit

21 For all compounds except favipiravir and TFM, the fastest degradation was observe

22 The pharmacokinetics of oral favipiravir and the relationships of plasma concentratio

23 A combination of favipiravir and zanamivir successfully cleared influenza

24 left untreated or treated with ribavirin or favipiravir, and we put the results in perspective with

25 ws no antagonistic effect when combined with favipiravir, another broadly acting antiviral nucleoside

26 Measurement of the tissue uptake of favipiravir as determined by PET may be a more important

27 Our data do not support favipiravir at commonly used doses in outpatients with u

28 to better understand the antiviral effect of favipiravir by developping the first mathematical model

29 ipeline to show that the mutagenic effect of favipiravir can be measured by whole-genome sequencing o

30 These results suggest that favipiravir can induce norovirus mutagenesis in vivo, wh

31 We demonstrate that favipiravir causes mutations and show that favipiravir p

32 eration sequencing (NGS) to demonstrate that favipiravir causes mutations in influenza RNA.

33 Wide interindividual variability existed in favipiravir concentrations, and this regimen failed to r

34 inistration was associated with lower plasma favipiravir concentrations.

35 her mean ratios of the metabolite T-705M1 to favipiravir, consistent with greater metabolism, and wer

36 lphenol (TFM), florasulam, voriconazole, and favipiravir, covering key fluorine motifs (benzylic-CF(3

37 All participants received oral favipiravir (day 0: 6,000 mg; day 1 to day 9: 2,400 mg/d

38 Moreover, a high dose of favipiravir decreased virus transmission by direct conta

39 In contrast, the results with favipiravir demonstrate that an antiviral drug at nontox

40 roviding a proof-of-principle for the use of favipiravir derivatives or mutagenic nucleosides in the

41 sease progression, early treatment with oral favipiravir did not prevent their disease progression fr

42 In US317 (526 favipiravir, 169 placebo), favipiravir did not significantly reduce time to allevia

43 er research is needed to ascertain if higher favipiravir doses are effective and safe for patients wi

44 okinetics in humans, our model predicts that favipiravir doses larger than 1200 mg twice a day should

45 This favipiravir dosing regimen demonstrated significant anti

46 Favipiravir drug levels were lower in the combination ar

47 Our model estimates favipiravir EC50 in vivo to 2.89 ug.mL-1, which is much

48 fficacy, and factors associated with reduced favipiravir exposure.

49 upport the further preclinical evaluation of favipiravir for Lassa fever and other VHFs.

50 zation to RNA polymerase inhibitor AVIFAVIR (favipiravir) for the treatment of COVID-19 patients.

51 ion, application of PET to the evaluation of favipiravir has demonstrated the importance of dosing re

52 One of these, T-705 (favipiravir), has a mechanism of action that is not full

53 s assessing the efficacy and tolerability of favipiravir in acute influenza.

54 d, randomized controlled outpatient trial of favipiravir in asymptomatic or mildly symptomatic adults

55 The role of favipiravir in preventing disease progression in coronav

56 lect data on the safety and effectiveness of favipiravir in reducing mortality and viral load in pati

57 nfection, demonstrating the effectiveness of favipiravir in this case.

58 ules to accurately and quantitatively detect favipiravir-induced mutations and to sample orders of ma

59 mutagen, but the precise mutation bias that favipiravir induces in influenza virus RNAs has not been

60 igh-error rates allowing facile insertion of Favipiravir into viral RNA, provoking C-to-U and G-to-A

61 Favipiravir is a broad-spectrum antiviral drug that may

62 Favipiravir is a broad-spectrum antiviral which is effec

63 a standard diagnostic pipeline to show that favipiravir is acting on the virus by revealing the muta

64 Despite limited data, favipiravir is administered to patients with coronavirus

65 Favipiravir is an important selective antiviral against

66 Favipiravir is cleared through the kidney as previously

67 The RNA polymerase inhibitor favipiravir is currently in clinical trials as a treatme

68 Favipiravir is routinely used in many countries, but eff

69 This will be important if favipiravir is used during a future influenza pandemic.

70 on perceived potency and clinical efficacy, favipiravir is widely used to treat COVID-19.

71 Higher favipiravir levels with average Cmin>20 ug/mL were assoc

72 Previous research has identified that favipiravir likely acts as a mutagen, but the precise mu

73 For the favipiravir+lopinavir-ritonavir, favipiravir+placebo, lo

74 We aimed to evaluate the effect of favipiravir, lopinavir-ritonavir or the combination of b

75 ate certainty) and systemic corticosteroids, favipiravir, molnupiravir, and umifenovir probably also

76 s were lower in the combination arm than the favipiravir monotherapy arm, possibly due to poor absorp

77 They also suggest that favipiravir monotherapy merits further study in patients

78 ravir and may help demonstrate the effect of favipiravir on viruses in a clinical setting.

79 S-CoV-2-infected hamsters with a low dose of favipiravir or hydroxychloroquine with(out) azithromycin

80 -to-moderate COVID-19 were 1:1 randomized to favipiravir or placebo.

81 -ritonavir placebo, lopinavir-ritonavir plus favipiravir placebo, or both placebos.

82 pants had undetectable virus at Day 5 in the favipiravir+placebo arm compared to placebo only (46.3%

83 primary analysis, the mean viral load in the favipiravir+placebo arm had changed by -0.57 log10 (95%

84 For the favipiravir+lopinavir-ritonavir, favipiravir+placebo, lopinavir-ritonavir+placebo, and pl

85 200 mg/50 mg 4 times daily on Days 2 to 7), favipiravir plus lopinavir-ritonavir placebo, lopinavir-

86 o hypoxia occurred in 46 (18.4%) patients on favipiravir plus standard care and 37 (14.8%) on standar

87 Patients were randomized 1:1 to favipiravir plus standard care or standard care alone.

88 We demonstrate here that Favipiravir predominantly exerts an antiviral effect thr

89 t favipiravir causes mutations and show that favipiravir primarily acts as a guanine analogue and sec

90 lness alleviation compared to placebo and to favipiravir recipients with lower average Cmin values in

91 ow that the broad-range antiviral nucleoside favipiravir reduces viral load in vivo by exerting antiv

92 Favipiravir remained highly effective against lethal LAS

93 Favipiravir requires further evaluation with considerati

94 Here we report the structure of favipiravir ribonucleoside triphosphate (favipiravir-RTP

95 ls an unusual, nonproductive binding mode of favipiravir-RTP at the catalytic site of SARS-CoV-2 RdRp

96 of favipiravir ribonucleoside triphosphate (favipiravir-RTP) in complex with the SARS-CoV-2 RNA-depe

97 CoV-2 amplicon-based sequencing, we assessed favipiravir's impact on mutagenesis.

98 Recently, the nucleotide analogue favipiravir showed a high antiviral efficacy, with 100%

99 However, high doses of favipiravir significantly reduced infectious virus titer

100 In this model, once daily treatment with favipiravir significantly reduced viral titers in tissue

101 Favipiravir suppressed Lassa virus replication in cell c

102 We studied the therapeutic potential of favipiravir (T-705) for Lassa fever, both alone and in c

103 Susceptibility to favipiravir (T-705) was assessed using plaque reduction

104 Favipiravir (T705; 6-fluoro-3-hydroxypyrazine-2-carboxam

105 [(18)F]favipiravir tissue uptake and distribution was similar i

106 revealed a trend toward improved survival in favipiravir- treated patients; however, the effect of tr

107 e events were observed in 13.8% and 14.8% of favipiravir-treated and placebo-treated subjects, respec

108 ysis indicated a longer survival time in the favipiravir-treated group (P = .015).

109 The case-fatality rate in favipiravir-treated patients was lower than in untreated

110 Uric acid elevation was more frequent among favipiravir-treated subjects (19.9% vs 2.8%).

111 e associated with survival (P < .001), while favipiravir treatment showed no statistically significan

112 Favipiravir treatment was offered to patients with EVD o

113 rs, alterations in blood chemistry findings, favipiravir treatment, and outcome.

114 TAT2 knockout (KO) hamsters is responsive to favipiravir treatment, which protected all animals from

115 Fluorine-18 labeling of favipiravir was achieved in a one-pot, two-step synthesi

116 Favipiravir was administered at 1800 mg 2x/day on day 1

117 ribution in mice naive to and pre-dosed with favipiravir was assessed by PET and gamma counting of ti

118 In US316 (301 favipiravir, 322 placebo), favipiravir was associated with a 14.4-hour reduction (m

119 In both trials favipiravir was associated with reduced viral titers, RN

120 rent study, a method for synthesis of [(18)F]favipiravir was developed and the biodistribution in mic

121 Oral favipiravir was part of the current standard of care in

122 The main mechanism of action of favipiravir was to decrease virus infectivity, with an e

123 Favipiravir was well tolerated but lacked efficacy in TT

124 Favipiravir was well tolerated.

125 nificantly different between adults starting favipiravir within <72 h of symptoms compared to others.

126 The exact mechanism of how favipiravir works to inhibit influenza is still unclear.