Abstract

Despite recent increase in the number of antifungal agents available for the treatment of systemic fungal diseases, morbidity and mortality are substantial; noting that invasive candidiasis (IC) is the fourth most common cause of nosocomial bloodstream infection in the United States chiefly among immunocompromised patients and that IC is associated with the highest crude mortality of all bloodstream infections (ca. 40%). Given the dismal outcomes for IC, combination of antifungal agents is increasingly being considered. However, pharmacodynamic (PD) properties for established and novel combinations of antifungal agents are ill-defined in terms of dose selection, dose fractionation, predictive PD index (PDI), and post-antibiotic effect (PAE) in relation to treatment efficacy and host toxicity. The major goal of this research project is to characterize the PD properties of established and novel combinations of antifungal agents in a neutropenic murine model of IC, aiming for novel insights and progress in IC beyond the present scope of research and therapy, which is usually single agent-based. Towards enabling in vivo PD studies, we made exciting progress in combination delivery (co-delivery) of amphotericin B (AmB) with other antifungal agents via self-assembled polymers, fulfilling requirements in solubility, safety, stability, and synergy, which ca now be achieved by the coincident action of combination antifungal agents administered simultaneously. We hypothesize that AmB and 5-fluoro- cytosine (5-FC) delivered together intravenously will exert potent antifungal activity, with low or no conversion of 5-FC into 5-fluorouracil (5-FU), observed after oral 5-FC, resulting in decreased bone marrow toxicity. We hypothesize that AmB and 17-allylamino-17-demethoxygeldanamycin (17-AAG), a heat shock protein 90 (Hsp90) inhibitor, will exert potent antifungal activity with low renal toxicity. Specifc Aims: (1) To characterize PK of micellar AmB and 5-FC, antifungal activity in a neutropenic murine model of IC, and toxicity in single and multiple dose (dose fractionation) regimens: PAE; predictive PDI (for maximum antifungal efficacy and optimal dosing regimen); and hematology relative to oral 5-FC. (2) To characterize PK of micellar AmB and 17-AAG, antifungal activity in a neutropenic murine model of IC, and toxicity in single and multiple dose regimens: PAE; predictive PDI; and renal and hepatic toxicity. (3) To characterize PK of micellar AmB, 5-FC, and micellar 17- AAG, antifungal activity in a neutropenic murine model of IC, and toxicity in single and multiple dose regimens: PAE; predictive PDI; hematology; renal toxicity; and histopathology in major organs.

Public Health Relevance

Invasive fungal infections are rising worldwide along with the number of immunocompromised patients. While several new antifungal agents have entered clinical practice, the armamentarium of antifungal agents is still limited, and morbidity and mortality remain high. Given the limited success of current treatment regimens for systemic fungal diseases, combination antifungal therapy has high appeal. The goal of this project is to study the antifungal efficacy of combination antifungal therapy in a neutropenic murine model of invasive candidiasis (IC), relating outcomes to pharmacokinetics (PK) of drug combinations. Antifungal efficacy of an established antifungal combination-amphotericin B (AmB) and 5-fluorocytosine (5-FC)-will be characterized in terms of dose/dose regimen in relation to antifungal efficacy and toxicity, exploring intravenous combination delivery (co-delivery) of AmB and 5-FC via self-assembled polymers (polymeric micelles). Similarly, antifungal efficacy of a novel combination-AmB and 17-allylamino-17-demethoxygeldanamycin (17-AAG)-will be characterized in terms of dose/dose regimen in relation to antifungal efficacy and toxicity, exploring the consequences of fungal heat shock protein 90 (Hsp90) inhibition. Outcomes from this research will be defined predictive indices of anti- fungal efficacy in a neutropenic murine model of IC, defining optimum dosing strategies for antifungal combinations. We highlight the novelty and potential clinical impact of a co-delivered, 3-drug combination of AmB, 5- FC, and 17-AAG for the treatment of life-threatening fungal diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI101157-05
Application #
9187972
Study Section
Gene and Drug Delivery Systems Study Section (GDD)
Program Officer
Liu, Baoying
Project Start
2013-01-15
Project End
2018-12-31
Budget Start
2017-01-01
Budget End
2018-12-31
Support Year
5
Fiscal Year
2017
Total Cost
Indirect Cost

  Institution

Name
University of Wisconsin Madison
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
161202122
City
Madison
State
WI
Country
United States
Zip Code
53715

  Publications

Tam, Yu Tong; Huang, Chengbin; Poellmann, Michael et al. (2018) Stereocomplex Prodrugs of Oligo(lactic acid) n-Gemcitabine in Poly(ethylene glycol)- block-poly(d,l-lactic acid) Micelles for Improved Physical Stability and Enhanced Antitumor Efficacy. ACS Nano 12:7406-7414
Zbyszynski, Pawel; Tomasini-Johansson, Bianca R; Peters, Donna M et al. (2018) Characterization of the PEGylated Functional Upstream Domain Peptide (PEG-FUD): a Potent Fibronectin Assembly Inhibitor with Potential as an Anti-Fibrotic Therapeutic. Pharm Res 35:126
Alvarez, Celeste; Andes, David R; Kang, Jeong Yeon et al. (2017) Antifungal Efficacy of an Intravenous Formulation Containing Monomeric Amphotericin B, 5-Fluorocytosine, and Saline for Sodium Supplementation. Pharm Res 34:1115-1124
Shin, Dae Hwan; Kwon, Glen S (2017) Epothilone B-based 3-in-1 polymeric micelle for anticancer drug therapy. Int J Pharm 518:307-311
Tomoda, Keishiro; Chiang, Hsin C; Kozak, Kevin R et al. (2017) Injectable (-)-gossypol-loaded Pluronic P85 micelles for cancer chemoradiotherapy. Int J Radiat Biol 93:402-406
Shin, Dae Hwan; Kwon, Glen S (2017) Pre-clinical evaluation of a themosensitive gel containing epothilone B and mTOR/Hsp90 targeted agents in an ovarian tumor model. J Control Release 268:176-183
Tomoda, Keishiro; Tam, Yu Tong; Cho, Hyunah et al. (2017) Triolimus: A Multi-Drug Loaded Polymeric Micelle Containing Paclitaxel, 17-AAG, and Rapamycin as a Novel Radiosensitizer. Macromol Biosci 17:
Cho, Hyunah; Gao, Jieming; Kwon, Glen S (2016) PEG-b-PLA micelles and PLGA-b-PEG-b-PLGA sol-gels for drug delivery. J Control Release 240:191-201
Tam, Yu Tong; Gao, Jieming; Kwon, Glen S (2016) Oligo(lactic acid)n-Paclitaxel Prodrugs for Poly(ethylene glycol)-block-poly(lactic acid) Micelles: Loading, Release, and Backbiting Conversion for Anticancer Activity. J Am Chem Soc 138:8674-7
Alvarez, Celeste; Shin, Dae Hwan; Kwon, Glen S (2016) Reformulation of Fungizone by PEG-DSPE Micelles: Deaggregation and Detoxification of Amphotericin B. Pharm Res 33:2098-106

Showing the most recent 10 out of 13 publications