4.7 Article

Bumped-Kinase Inhibitors for Cryptosporidiosis Therapy

Journal

JOURNAL OF INFECTIOUS DISEASES
Volume 215, Issue 8, Pages 1275-1284

Publisher

OXFORD UNIV PRESS INC
DOI: 10.1093/infdis/jix120

Keywords

Cryptosporidiosis treatment; calcium-dependent protein kinase 1; bumped kinase inhibitors

Funding

  1. National Institute of Allergy and Infectious Diseases, National Institutes of Health [R01AI089441, R01AI111341, R01A1112427, R01HD080670]
  2. BMGF [OPP 1134302]
  3. US Department of Agriculture National Institute of Food and Agriculture [2014-06183]

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Bumped kinase inhibitors (BKIs) of Cryptosporidium parvum calcium-dependent protein kinase 1 (CpCDPK1) are leading candidates for treatment of cryptosporidiosis- associated diarrhea. Potential cardiotoxicity related to anti-human ethe-a-go-go potassium channel (hERG) activity of the first-generation anti-Cryptosporidium BKIs triggered further testing for efficacy. A luminescence assay adapted for high-throughput screening was used to measure inhibitory activities of BKIs against C. parvum in vitro. Furthermore, neonatal and interferon. knockout mouse models of C. parvum infection identified BKIs with in vivo activity. Additional iterative experiments for optimum dosing and selecting BKIs with minimum levels of hERG activity and frequencies of other safety liabilities included those that investigated mammalian cell cytotoxicity, C. parvum proliferation inhibition in vitro, anti-human Src inhibition, hERG activity, in vivo pharmacokinetic data, and efficacy in other mouse models. Findings of this study suggest that fecal concentrations greater than parasite inhibitory concentrations correlate best with effective therapy in the mouse model of cryptosporidiosis, but a more refined model for efficacy is needed.

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