Your search keyword '"Minnis AM"' showing total 4 results

1. MTN-001: Randomized Pharmacokinetic Cross-Over Study Comparing Tenofovir Vaginal Gel and Oral Tablets in Vaginal Tissue and Other Compartments

Author

Hendrix, CW, Chen, BA, Guddera, V, Hoesley, C, Justman, J, Nakabiito, C, Salata, R, Soto-Torres, L, Patterson, K, Minnis, AM, Gandham, S, Gomez, K, Richardson, BA, Bumpus, NN, Hendrix, CW, Chen, BA, Guddera, V, Hoesley, C, Justman, J, Nakabiito, C, Salata, R, Soto-Torres, L, Patterson, K, Minnis, AM, Gandham, S, Gomez, K, Richardson, BA, and Bumpus, NN

Abstract

Background: Oral and vaginal preparations of tenofovir as pre-exposure prophylaxis (PrEP) for human immunodeficiency virus (HIV) infection have demonstrated variable efficacy in men and women prompting assessment of variation in drug concentration as an explanation. Knowledge of tenofovir concentration and its active form, tenofovir diphosphate, at the putative vaginal and rectal site of action and its relationship to concentrations at multiple other anatomic locations may provide key information for both interpreting PrEP study outcomes and planning future PrEP drug development. Objective: MTN-001 was designed to directly compare oral to vaginal steady-state tenofovir pharmacokinetics in blood, vaginal tissue, and vaginal and rectal fluid in a paired cross-over design. Methods and Findings: We enrolled 144 HIV-uninfected women at 4 US and 3 African clinical research sites in an open label, 3-period crossover study of three different daily tenofovir regimens, each for 6 weeks (oral 300 mg tenofovir disoproxil fumarate, vaginal 1% tenofovir gel [40 mg], or both). Serum concentrations after vaginal dosing were 56-fold lower than after oral dosing (p<0.001). Vaginal tissue tenofovir diphosphate was quantifiable in ≥90% of women with vaginal dosing and only 19% of women with oral dosing. Vaginal tissue tenofovir diphosphate was ≥130-fold higher with vaginal compared to oral dosing (p<0.001). Rectal fluid tenofovir concentrations in vaginal dosing periods were higher than concentrations measured in the oral only dosing period (p<0.03). Conclusions: Compared to oral dosing, vaginal dosing achieved much lower serum concentrations and much higher vaginal tissue concentrations. Even allowing for 100-fold concentration differences due to poor adherence or less frequent prescribed dosing, vaginal dosing of tenofovir should provide higher active site concentrations and theoretically greater PrEP efficacy than oral dosing; randomized topical dosing PrEP trials to the contrary in

Published

2013

2. MTN-001: Randomized Pharmacokinetic Cross-Over Study Comparing Tenofovir Vaginal Gel and Oral Tablets in Vaginal Tissue and Other Compartments

Author

Hendrix, CW, Chen, BA, Guddera, V, Hoesley, C, Justman, J, Nakabiito, C, Salata, R, Soto-Torres, L, Patterson, K, Minnis, AM, Gandham, S, Gomez, K, Richardson, BA, Bumpus, NN, Hendrix, CW, Chen, BA, Guddera, V, Hoesley, C, Justman, J, Nakabiito, C, Salata, R, Soto-Torres, L, Patterson, K, Minnis, AM, Gandham, S, Gomez, K, Richardson, BA, and Bumpus, NN

Abstract

Background: Oral and vaginal preparations of tenofovir as pre-exposure prophylaxis (PrEP) for human immunodeficiency virus (HIV) infection have demonstrated variable efficacy in men and women prompting assessment of variation in drug concentration as an explanation. Knowledge of tenofovir concentration and its active form, tenofovir diphosphate, at the putative vaginal and rectal site of action and its relationship to concentrations at multiple other anatomic locations may provide key information for both interpreting PrEP study outcomes and planning future PrEP drug development. Objective: MTN-001 was designed to directly compare oral to vaginal steady-state tenofovir pharmacokinetics in blood, vaginal tissue, and vaginal and rectal fluid in a paired cross-over design. Methods and Findings: We enrolled 144 HIV-uninfected women at 4 US and 3 African clinical research sites in an open label, 3-period crossover study of three different daily tenofovir regimens, each for 6 weeks (oral 300 mg tenofovir disoproxil fumarate, vaginal 1% tenofovir gel [40 mg], or both). Serum concentrations after vaginal dosing were 56-fold lower than after oral dosing (p<0.001). Vaginal tissue tenofovir diphosphate was quantifiable in ≥90% of women with vaginal dosing and only 19% of women with oral dosing. Vaginal tissue tenofovir diphosphate was ≥130-fold higher with vaginal compared to oral dosing (p<0.001). Rectal fluid tenofovir concentrations in vaginal dosing periods were higher than concentrations measured in the oral only dosing period (p<0.03). Conclusions: Compared to oral dosing, vaginal dosing achieved much lower serum concentrations and much higher vaginal tissue concentrations. Even allowing for 100-fold concentration differences due to poor adherence or less frequent prescribed dosing, vaginal dosing of tenofovir should provide higher active site concentrations and theoretically greater PrEP efficacy than oral dosing; randomized topical dosing PrEP trials to the contrary in

Published

2013

3. MTN-001: Randomized Pharmacokinetic Cross-Over Study Comparing Tenofovir Vaginal Gel and Oral Tablets in Vaginal Tissue and Other Compartments

Author

Hendrix, CW, Chen, BA, Guddera, V, Hoesley, C, Justman, J, Nakabiito, C, Salata, R, Soto-Torres, L, Patterson, K, Minnis, AM, Gandham, S, Gomez, K, Richardson, BA, Bumpus, NN, Hendrix, CW, Chen, BA, Guddera, V, Hoesley, C, Justman, J, Nakabiito, C, Salata, R, Soto-Torres, L, Patterson, K, Minnis, AM, Gandham, S, Gomez, K, Richardson, BA, and Bumpus, NN

Abstract

Background: Oral and vaginal preparations of tenofovir as pre-exposure prophylaxis (PrEP) for human immunodeficiency virus (HIV) infection have demonstrated variable efficacy in men and women prompting assessment of variation in drug concentration as an explanation. Knowledge of tenofovir concentration and its active form, tenofovir diphosphate, at the putative vaginal and rectal site of action and its relationship to concentrations at multiple other anatomic locations may provide key information for both interpreting PrEP study outcomes and planning future PrEP drug development. Objective: MTN-001 was designed to directly compare oral to vaginal steady-state tenofovir pharmacokinetics in blood, vaginal tissue, and vaginal and rectal fluid in a paired cross-over design. Methods and Findings: We enrolled 144 HIV-uninfected women at 4 US and 3 African clinical research sites in an open label, 3-period crossover study of three different daily tenofovir regimens, each for 6 weeks (oral 300 mg tenofovir disoproxil fumarate, vaginal 1% tenofovir gel [40 mg], or both). Serum concentrations after vaginal dosing were 56-fold lower than after oral dosing (p<0.001). Vaginal tissue tenofovir diphosphate was quantifiable in ≥90% of women with vaginal dosing and only 19% of women with oral dosing. Vaginal tissue tenofovir diphosphate was ≥130-fold higher with vaginal compared to oral dosing (p<0.001). Rectal fluid tenofovir concentrations in vaginal dosing periods were higher than concentrations measured in the oral only dosing period (p<0.03). Conclusions: Compared to oral dosing, vaginal dosing achieved much lower serum concentrations and much higher vaginal tissue concentrations. Even allowing for 100-fold concentration differences due to poor adherence or less frequent prescribed dosing, vaginal dosing of tenofovir should provide higher active site concentrations and theoretically greater PrEP efficacy than oral dosing; randomized topical dosing PrEP trials to the contrary in

Published

2013

4. Fungal planet description sheets: 154-213

Author

Universitat Rovira i Virgili, Crous PW; Wingfield MJ; Guarro J; Cheewangkoon R; van der Bank M; Swart WJ; Stchigel AM; Cano-Lira JF; Roux J; Madrid H; Damm U; Wood AR; Shuttleworth LA; Hodges CS; Munster M; de jesús yáñez-Morales M; Zúñiga-Estrada L; Cruywagen EM; de Hoog GS; Silvera C; Najafzadeh J; Davison EM; Davison PJN; Barrett MD; Barrett RL; Manamgoda DS; Minnis AM; Kleczewski NM; Flory SL; Castlebury LA; Clay K; Hyde KD; Maússe-Sitoe SND; Chen S; Lechat C; Hairaud M; Lesage-Meessen L; Pawłowska J; Wilk M; Śliwińska-Wyrzychowska A, Universitat Rovira i Virgili, and Crous PW; Wingfield MJ; Guarro J; Cheewangkoon R; van der Bank M; Swart WJ; Stchigel AM; Cano-Lira JF; Roux J; Madrid H; Damm U; Wood AR; Shuttleworth LA; Hodges CS; Munster M; de jesús yáñez-Morales M; Zúñiga-Estrada L; Cruywagen EM; de Hoog GS; Silvera C; Najafzadeh J; Davison EM; Davison PJN; Barrett MD; Barrett RL; Manamgoda DS; Minnis AM; Kleczewski NM; Flory SL; Castlebury LA; Clay K; Hyde KD; Maússe-Sitoe SND; Chen S; Lechat C; Hairaud M; Lesage-Meessen L; Pawłowska J; Wilk M; Śliwińska-Wyrzychowska A

Abstract

Novel species of microfungi described in the present study include the following from South Africa: Camarosporium aloes, Phaeococcomyces aloes and Phoma aloes from Aloe, C. psoraleae, Diaporthe psoraleae and D. psoraleae-pinnatae from Psoralea, Colletotrichum euphorbiae from Euphorbia, Coniothyrium prosopidis and Peyronellaea prosopidis from Prosopis, Diaporthe cassines from Cassine, D. diospyricola from Diospyros, Diaporthe maytenicola from Maytenus, Harknessia proteae from Protea, Neofusicoccum ursorum and N. cryptoaustrale from Eucalyptus, Ochrocladosporium adansoniae from Adansonia, Pilidium pseudoconcavum from Greyia radlkoferi, Stagonospora pseudopaludosa from Phragmites and Toxicocladosporium ficiniae from Ficinia. Several species were also described from Thailand, namely: Chaetopsina pini and C. pinicola from Pinus spp., Myrmecridium thailandicum from reed litter, Passalora pseudotithoniae from Tithonia, Pallidocercospora ventilago from Ventilago, Pyricularia bothriochloae from Bothriochloa and Sphaerulina rhododendricola from Rhododendron. Novelties from Spain include Cladophialophora multiseptata, Knufia tsunedae and Pleuroascus rectipilus from soil and Cyphellophora catalaunica from river sediments. Species from the USA include Bipolaris drechsleri from Microstegium, Calonectria blephiliae from Blephilia, Kellermania macrospora (epitype) and K. pseudoyuccigena from Yucca. Three new species are described from Mexico, namely Neophaeosphaeria agaves and K. agaves from Agave and Phytophthora ipomoeae from Ipomoea. Other African species include Calonectria mossambicensis from Eucalyptus (Mozambique), Harzia cameroonensis from an unknown creeper (Cameroon), Mastigosporella anisophylleae from Anisophyllea (Zambia) and Teratosphaeria terminaliae from Terminalia (Zimb

Published

2013