Abstract

EXCEED THE SPACE PROVIDED. As a part of our on-going research focusing on therapeutic strategies against HIV transmission and disease progression, the long-term goal of this program is to develop novel therapeutic strategies against HIV replication in lymphoid tissues. While the tissues that harbor residual HIV outside the lymphatic system remains elusive, it is clear that a low but detectable fraction of HIV is found in visceral (e.g., mesenteric) lymph nodes, even in the presence of highly active anti-retroviral (combination drug) therapies (HAARTs). Our recent analysis of indinavir (an HIV protease inhibitor) levels in tissues (i.e., lymph nodes) and blood indicated that drug, particularly protease inhibitor, exposure in lymph nodes is far less than that of systemic (blood) exposure in human subjects under HAARTs. Increasing drug exposure to lymphoid tissues without increasing drug toxicity may further reduce the virus levels and intracellular virus concentrations in these tissues. Using an anti-HIV protease inhibitor, indinavir, as a model drug, we recently designed lipid-drug complexes of about 50-60 nm in diameter that permitted a significant enhancement in localization of indinavir in lymph nodes. The novel approach to form the lipid-drug complex permitted almost complete incorporation of drug into the complex, thereby greatly simplifying the drug formulation process. When administered subcutaneously to macaques (M. nemestrina), the lipid-associated drug complexes accumulated at high concentrations in lymph nodes; we observed drug concentrations in lymph nodes as much as 20-30-fold higher than in blood. Such levels of drug accumulation in lymph nodes could not be achieved with free drug. With enhanced delivery of drugs to lymph nodes of HIV-2287-infected macaques, at higher concentrations and for a longer duration, while keeping drug-associated toxicity at bay, we will determine whether increasing local drug concentration will further reduce the virus load in the lymphatic system by testing the following hypotheses: Hypothesis 1: Enhanced anti-HIV drug accumulation in lymph nodes throughout the lymphatic system can be achieved using a novel lipid-associated form. Hypothesis 2: Lipid-mediated enhanced drug accumulation strategy will further reduce the frequency of virus-infected cells or virus concentration in lymphoid tissues. As proof-of-principle, data collected using a highly sensitive virus quantitation and localization system for lymphoid tissues, from this study, will discern the differential effects of free and lipid-associated indinavir. In addition, these data will provide a solid foundation encompassing pharmacologic and therapeutic, as well as safety issues, essential for further evaluation of the novel drug-targeting strategies to enhance drug availability in lymph nodes and other tissues where virus typically persists. PERFORMANCE SITE ========================================Section End===========================================

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI052663-03
Application #
6830757
Study Section
AIDS and Related Research 8 (AARR)
Program Officer
Bridges, Sandra H
Project Start
2002-12-15
Project End
2007-11-30
Budget Start
2004-12-01
Budget End
2007-11-30
Support Year
3
Fiscal Year
2005
Total Cost
$714,427
Indirect Cost

  Institution

Name
University of Washington
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
605799469
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Kraft, John C; McConnachie, Lisa A; Koehn, Josefin et al. (2018) Mechanism-based pharmacokinetic (MBPK) models describe the complex plasma kinetics of three antiretrovirals delivered by a long-acting anti-HIV drug combination nanoparticle formulation. J Control Release 275:229-241
Freeling, Jennifer P; Koehn, Josefin; Shu, Cuiling et al. (2014) Long-acting three-drug combination anti-HIV nanoparticles enhance drug exposure in primate plasma and cells within lymph nodes and blood. AIDS 28:2625-7
Endsley, Aaron N; Ho, Rodney J Y (2012) Elucidation of the time course of adenosine deaminase APOBEC3G and viral infectivity factor vif in HIV-2(287) -infected infant macaques. J Med Primatol 41:52-9
Crouthamel, Matthew H; Kelly, Edward J; Ho, Rodney J Y (2012) Development and characterization of transgenic mouse models for conditional gene knockout in the blood-brain and blood-CSF barriers. Transgenic Res 21:113-30
Ho, Rodney J Y; Chien, Jenny Y (2012) Drug delivery trends in clinical trials and translational medicine: growth in biologic molecule development and impact on rheumatoid arthritis, Crohn's disease, and colitis. J Pharm Sci 101:2668-74
Endsley, Aaron N; Ho, Rodney J Y (2012) Enhanced anti-HIV efficacy of indinavir after inclusion in CD4-targeted lipid nanoparticles. J Acquir Immune Defic Syndr 61:417-24
Ho, Rodney J Y (2011) Editorial: human genome information. J Pharm Sci 100:4045-6
Chien, Jenny Y; Ho, Rodney J Y (2011) Drug delivery trends in clinical trials and translational medicine: evaluation of pharmacokinetic properties in special populations. J Pharm Sci 100:53-8
Ho, Martin T; Kelly, Edward J; Bodor, Miklos et al. (2011) Novel cytochrome P450-2D6 promoter sequence variations in hepatitis C positive and negative subjects. Ann Hepatol 10:327-32
Ho, Beatrice E; Shen, Danny D; McCune, Jeannine S et al. (2010) Effects of Garlic on Cytochromes P450 2C9- and 3A4-Mediated Drug Metabolism in Human Hepatocytes. Sci Pharm 78:473-81

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