AI Article Synopsis

  • Cryptosporidium parasites cause intestinal infections, known as cryptosporidiosis, which predominantly affect populations in developing countries and lack effective treatments.
  • A newly developed CDPK1 inhibitor, 1294, has shown significant promise in reducing parasite infections in lab studies, with a low effective concentration.
  • In animal tests, 1294 effectively cleared the infection in most mice and reduced tissue damage, suggesting it could be a viable candidate for future cryptosporidiosis therapies.

Article Abstract

Cryptosporidium parasites infect intestinal cells, causing cryptosporidiosis. Despite its high morbidity and association with stunting in the developing world, current therapies for cryptosporidiosis have limited efficacy. Calcium-dependent protein kinases (CDPKs) are essential enzymes in the biology of protozoan parasites. CDPK1 was cloned from the genome of Cryptosporidium parvum, and potent and specific inhibitors have been developed based on structural studies. In this study, we evaluated the anti-Cryptosporidium activity of a novel CDPK1 inhibitor, 1294, and demonstrated that 1294 significantly reduces parasite infection in vitro, with a half maximal effective concentration of 100 nM. Pharmacokinetic studies revealed that 1294 is well absorbed, with a half-life supporting daily administration. Oral therapy with 1294 eliminated Cryptosporidium parasites from 6 of 7 infected severe combined immunodeficiency-beige mice, and the parasites did not recur in these immunosuppressed mice. Mice treated with 1294 had less epithelial damage, corresponding to less apoptosis. Thus, 1294 is an important lead for the development of drugs for treatment of cryptosporidiosis.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3778970PMC
http://dx.doi.org/10.1093/infdis/jit327DOI Listing

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