Your search keyword '"Hirt, Deborah"' showing total 4 results

1. Blood concentrations are better predictors of chioroquine poisoning severity than plasma concentrations: a prospective study with modeling of the concentration/effect relationships

Author

Megarbane, Bruno, Bloch, Vanessa, Hirt, Deborah, Debray, Marcel, Resiere, Dabor, Deye, Nicolas, and Baud, Frederic J.

Subjects

Chloroquine -- Complications and side effects, Cardiovascular diseases -- Risk factors, Cardiovascular diseases -- Prognosis, Blood plasma -- Analysis, Drugs -- Health aspects, Drugs -- Diagnosis, Drugs -- Research, Environmental issues, Health, Pharmaceuticals and cosmetics industries

Published

2010

2. What babies need: accelerating access to current and novel antiretroviral drugs in neonates through pharmacokinetic studies

Author

Jacobs, Tom G, Schouwenburg, Stef, Penazzato, Martina, Archary, Moherndran, Ruel, Theodore D, van den Anker, John, Burger, David M, Cressey, Tim R, Abrams, Elaine J, Lyall, Hermione, Bekker, Adrie, Colbers, Angela, Burger, David, Bekker, Adrie, Cressey, Tim, Hirt, Deborah, Lutsar, Irja, Mcilleron, Helen, Standing, Joe, Van den Anker, John, Svensson, Elin, Abrams, Elaine, Amuge, Pauline, Archary, Mo, Bekker, Adrie, Belew, Yodit, Best, Brookie, Burger, David, Bygrave, Helen, Capparelli, Edmund, Casas, Esther, Clarke, Diana, Clayden, Polly, Colbers, Angela, Cressey, Tim, Dangarembizi, Mutsa, De Lisa, Roberto, Denti, Paolo, Domanico, Paul, Essajee, Shaffiq, Frigati, Lisa, Giaquinto, Carlo, Gibb, Diana, Hackett, Stephanie, Hazra, Rohan, Lallemant, Marc, Lewis, Linda, Lockman, Shahin, Mahaka, Imelda, McFarland, Betsy, Meere, Cathal, Mir, Fatima, Mirochnick, Mark, Mofenson, Lynne, Mukui, Irene, Mushavi, Angela, Musiime, Victor, Namusoke-Magongo, Eleanor, Obimbo, Elisabeth, Ojoo, Mary Atieno, Parades, Roger, Perez-Casas, Carmen, Piccolis, Manuele, Pinto, Jorge, Puthanakit, Thanyawee, Rakhmanina, Natella, Reinisch, Annette, Rojo, Pablo, Rouzier, Vanessa, Ruel, Ted, Sam-Agudu, Nadia, Siberry, George, Simione, Teresa, Simon, Katie, Singh, Vindi, Solares, Manjari, Sugandhi, Nandita, Sylla, Mariam, Thior, Ibou, Turkova, Anna, Vicari, Marissa, Walsh, Jenny, Watkins, Melynda, Wolf, Hilary, Hafiz, Asma, Penazzato, Martina, Rangaraj, Ajay, Doherty, Meg, and Vitoria, Marco

Abstract

Although 23 antiretroviral drugs are approved for use in adults, only six are approved by regulatory authorities for use in term neonates born to women with HIV, with even fewer options for preterm neonates. A major hurdle for approvals is the delay in the generation of pharmacokinetic and safety data for antiretrovirals in neonates. The median time between the year of approval from the US Food and Drug Administration of an antiretroviral agent for adults and the first publication date for pharmacokinetic data in neonates less than 4 weeks old is 8 years (range 2–23 years). In this Viewpoint, we address pharmacokinetic research gaps and priorities for current and novel antiretroviral use in neonates. We also consider the challenges and provide guidance on neonatal clinical pharmacology research on antiretroviral agents with the goal of stimulating research and expediting the availability of safe medications for the prevention and treatment of HIV in this vulnerable population.

Published

2022

3. Extended pre-exposure prophylaxis with lopinavir–ritonavir versus lamivudine to prevent HIV-1 transmission through breastfeeding up to 50 weeks in infants in Africa (ANRS 12174): a randomised controlled trial

Author

Nagot, Nicolas, Kankasa, Chipepo, Tumwine, James K, Meda, Nicolas, Hofmeyr, G Justus, Vallo, Roselyne, Mwiya, Mwiya, Kwagala, Mary, Traore, Hugues, Sunday, Amwe, Singata, Mandisa, Siuluta, Chafye, Some, Eric, Rutagwera, David, Neboua, Desire, Ndeezi, Grace, Jackson, Debra, Maréchal, Valérie, Neveu, Dorine, Engebretsen, Ingunn M S, Lombard, Carl, Blanche, Stéphane, Sommerfelt, Halvor, Rekacewicz, Claire, Tylleskär, Thorkild, Van de Perre, Philippe, Van de Perre, Philippe, Nagot, Nicolas, Vallo, Roselyne, Marechal, Valerie, Peries, Marianne, Neveu, Dorine, Foulongne, Vincent, Segondy, Michel, Blanche, Stephane, Treluyer, Jean-Marc, Hirt, Deborah, Tumwine, James K, Ndeezi, Grace, Karamagi, Charles, Musoke, Philippa, Mugaba, Proscovia M, Kwagala, Mary, Murungi, Joan, Muweesi, Hawa Nabuuma, Ninsiima, Evelyn, Baryeija, Simon, Juma, Frederic, Kata, Caleb Bwengye, Katushabe, Stuart, Meda, Nicolas, Ouédraogo, Rasmata, Yé, Diarra, Somé, Eric, Traoré, Hugues A, Nadembega, Christelle, Konaté, Justin, Zongo, Arsène, Ouédraogo, Abass, Néboua, Désiré, Bélemviré, Aissatou, Bambara, Armel, Boncoungou, Justine, Zoungrana, Danielle, Nikodem, Cheryl, Hofmeyr, Justus, Harper, Kim, Jackson, Debra, Sanders, David, Singata, Mandisa, Aku, Amwe, Okegbe-Eze, Collins, Williams, Xoliswa, Mshweshwe, Nolundi, Henge, Vatiswa, Gomba, Fikiswa, Gundu, Tapiwa, Khondowe, Oswell, Kankasa, Chipepo, Mwiya, Mwiya, Lusaka, Mildred, Chizyuka, Mary, Phiri, Mary, Imakando, Billies, Musaku, Mwenechanya, Kapasa, Monica, Rutagwera, David, Clement, Gondwe, Mwaba, Hilton Mwila, Matoba, Japhet, Siuluta, Chafye, Chola, Katai, Mwamutanda, Patricia, Tylleskär, Thorkild, Sommerfelt, Halvor, Engebretsen, Ingunn, Klungsøyr, Jørn, van den Broeck, Jan, Blume, Jörn, and Rekacewicz, Claire

Abstract

Strategies to prevent postnatal mother-to-child transmission of HIV-1 in Africa, including infant prophylaxis, have never been assessed past 6 months of breastfeeding, despite breastfeeding being recommended up to 12 months after birth. We aimed to compare the efficacy and safety of infant prophylaxis with the two drug regimens (lamivudine or lopinavir–ritonavir) to prevent postnatal HIV-1 transmission up to 50 weeks of breastfeeding.

Published

2016

4. Influence of Body Weight on Achieving Indinavir Concentrations Within Its Therapeutic Window in HIV-Infected Thai Patients Receiving Indinavir Boosted With Ritonavir

Author

Cressey, Tim R, Urien, Saik, Hirt, Deborah, Halue, Guttiga, Techapornroong, Malee, Bowonwatanuwong, Chureeratana, Leenasirimakul, Prattana, Treluyer, Jean-Marc, Jourdain, Gonzague, and Lallemant, Marc

Abstract

Indinavir boosted with ritonavir (IDV/r) dosing with 400/100 mg, twice daily, is preferred in Thai adults, but this dose can lead to concentrations close to the boundaries of its therapeutic window. The objectives of this analysis were to validate a population pharmacokinetic model to describe IDV/r concentrations in HIV-infected Thai patients and to investigate the impact of patient characteristics on achieving adequate IDV concentrations. IDV/r concentration data from 513 plasma samples were available. Population means and variances of pharmacokinetic parameters were estimated using a nonlinear mixed effects regression model (NONMEM Version VI). Monte Carlo simulations were performed to estimate the probability of achieving IDV concentrations within its therapeutic window. IDV/r pharmacokinetics were best described by a one-compartment model coupled with a single transit compartment absorption model. Body weight influenced indinavir apparent oral clearance and volume of distribution and allometric scaling significantly reduced the interindividual variability. Final population estimates (interindividual variability in percentage) of indinavir apparent oral clearance and volume of distribution were 21.3 L/h/70 kg (30%) and 90.7 L/70 kg (22%), respectively. Based on model simulations, the probability of achieving an IDV trough concentration greater than 0.1 mg/L was greater than 99% for 600/100 mg and greater than 98% for 400/100 mg, twice daily, in patients weighing 40 to 80 kg. However, the probability of achieving IDV concentrations associated with an increased risk of drug toxicity (greater than 10.0 mg/L) increased from 1% to 10% with 600/100 mg compared with less than 1% with 400/100 mg when body weight decreased from 80 to 40 kg. The validated model developed predicts that 400/100 mg of IDV/r, twice daily, provides indinavir concentrations within the recommended therapeutic window for the majority of patients. The risk of toxic drug concentrations increases rapidly with IDV/r dose of 600/100 mg for patients less than 50 kg and therapeutic drug monitoring of IDV concentrations would help to reduce the risk of IDV-induced nephrotoxicity.

Published

2011