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Global Women`s Health
Bioresponsive Vaginal Drug Delivery Devices to Improve Global Women’s Health Giovanni M. Pauletti, Ph.D. Associate Professor of Biopharmaceutics & Pharmacokinetics James L. Winkle College of Pharmacy, University of Cincinnati, Cincinnati, OH (U.S.A.) Objectives Global women’s health Preventive strategies Innovative drug delivery systems Performance in vitro Future opportunities Global Women’s Health Global Women’s Health Facts: Tobacco use among younger women in developing countries HIV-AIDS pandemic is increasingly “female” Physical and sexual violence against women >90% of adolescent mothers live in developing countries Essentially all maternal deaths occur in developing countries Source: WHO – Department of Gender, Women and Health Global Women’s Health Family Planning/Family Size HIV/AIDS Maternal Mortality Global Women’s Health Regional Demand for Family Planning in Africa 100 modern traditional unmet needs 16% 50 28% 23% 23% 0 Western Eastern Middle Southern Regions Source: African Population and Health Research Center Global Women’s Health Impact of Economics on Family Planning Use in Africa 80 60 poorest 20% wealthiest 20% 40 20 0 Western Eastern Middle Southern Regions D. Clifton et al. Family Planning Worldwide, 2008 Global Women’s Health Maternal Mortality Source: World Bank , World Development Indicators Global Women’s Health Global Women’s Health • zero new infections • zero discrimination • zero AIDS-related deaths Preventive Strategies Saving Lives in the Future: Comprehensive primary health care Gender equality Nutrition Prevention of child abuse Social & emotional development Reduction in risky behavior Preventive Strategies Preventive Strategies Preventive Strategies Limitations: use of applicator temperaturedependent viscosity microbial safety distribution Katz et al., Drug Deliv. Transl. Res. (2011) Innovative Drug Delivery Systems Objective Development of an innovative preventive/therapeutic device that meets unique needs of women in underserved African regions: self-administration without applicator low-cost socially acceptable rapid effectiveness safe mucoadhesive biodegradable Innovative Drug Delivery Systems Acidic Buffer Capacity Olmsted et al., Fert. Ster. (2000) Connor, Acquir. Immune Defic. Syndr. (2006) Innovative Drug Delivery Systems Bioresponsive Viscosity Jay et al., Adv. Funct. Mater. (2009) Innovative Drug Delivery Systems Diffusion Coefficient [m2/s] Bioresponsive Viscosity 0.08 HIV 100 nm LP 0.06 0.04 0.02 0.00 pH 4.3 pH 4.5 pH 4.8 Jay et al., Adv. Funct. Mater. (2009) Innovative Drug Delivery Systems Sol – Gel – Xerogel solid dosage form light-weight biocompatible & biodegradable materials Supercritical Drying Solvent Evaporation chemical stability engineered device properties Innovative Drug Delivery Systems Carbopol® 974P Viscosity [cP] 410 0 5 310 0 5 2%CP/4%HPMC Gynol II 210 0 5 110 0 5 0 3.6 3.9 4.2 4.4 4.5 4.8 5 5.2 6 6.2 Hydroxypropyl methylcellulose Innovative Drug Delivery Systems Tampon-like Xerogel Device o.b.® tampon Porosity [%] 54.1 1.9 83.0 2.9 Compression Force [N] 13.2 1.8 11.8 1.1 Hydration Rate [mg/s cm2] 3.5 0.1 13.8 0.7 Innovative Drug Delivery Systems Tampon-like Xerogel Device Gynol II 3% mannitol Innovative Drug Delivery Systems Tampon-like Xerogel Device Engineered Properties: 5% trehalose 3% mannitol porosity (20-90%) hydration rate (1-15 mg/s cm2) Compression force (5-60 N) Innovative Drug Delivery Systems Effect of Pore-forming Agent: Viscosity [cP] 510 0 5 410 2%CP/4%HPMC 05 3% Mannitol 310 0 5 210 0 5 110 0 5 0 3.3 3.6 3.8 3.9 4.2 4.3 4.4 4.5 4.8 5 Innovative Drug Delivery Systems Spreadability Work [Nxs] Partial Rehydration of Tampon-like Xerogel Device 15 gel xerogel 10 5 0 2% CP/5% HPMC 3% mannitol Gynol II Innovative Drug Delivery Systems Spreadability Work [Nxs] Partial Rehydration of Tampon-like Xerogel Device 6 2%CP/4%HPMC 3% Mannitol Gynol II 4 2 0 0.5 1.0 2.0 Seminal Fluid Simulant [mL] 3.0 Innovative Drug Delivery Systems Partial Rehydration of Tampon-like Xerogel Device 2%CP/4%HPMC 3% Mannitol 3% Trehalose Gynol II 2 1 5 Bioadhesion Work [Nxmm] Bioadhesion Work [Nxmm] 3 gel xerogel 4 3 2 1 0 2% CP/5% HPMC 0 0 1 2 Time [min] 3 3% mannitol Gynol II Future Directions Clinical Development of Tampon-like Xerogels: • in vitro testing methods (efficacy/safety) • women’s acceptability/perception • in vivo safety/efficacy • scale-up/production • pharmacokinetics of medicated xerogels • regulatory path Acknowledgments University of Cincinnati Other Collaborators • Dr. Ambikaipakan Balasubramaniam • Dr. Saleem S. Basha • Hua Li • Ankit Mehta • Dr. Sarah Potter • Dr. Donglu Shi • Dr. Andrew Steckl • Shruthi Vaidhanathan • Dr. Liaohai Chen • Dr. Isabella Ellinger • Dr. Yongyong Li • Dr. James Liu Financial Support • Bill & Melinda Gates Foundation • DAMD17-00-1-0202 • NIH (GM-67639; HD-048512) • PhRMA • UC Research Council • UC Institute for Nanoscale Science & Technology