Bumped kinase inhibitor 1369 is effective against Cystoisospora suis in vivo and in vitro

Cystoisosporosis is a leading diarrheal disease in suckling piglets. With the confirmation of resistance against the only available drug toltrazuril, there is a substantial need for novel therapeutics to combat the infection and its negative effects on animal health. In closely related apicomplexan...

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Autores principales: Shrestha, Aruna, Ojo, Kayode K., Koston, Florian, Ruttkowski, Bärbel, Vidadala, Rama S.R., Dorr, Carlie S., Navaluna, Edelmar D., Whitman, Grant R., Barrett, Kayleigh F., Barrett, Lynn K., Hulverson, Matthew A., Choi, Ryan, Michaels, Samantha A., Maly, Dustin J., Hemphill, Andrew, Van Voorhis, Wesley C., Joachim, Anja
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2019
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6453670/
https://www.ncbi.nlm.nih.gov/pubmed/30959327
http://dx.doi.org/10.1016/j.ijpddr.2019.03.004
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author Shrestha, Aruna
Ojo, Kayode K.
Koston, Florian
Ruttkowski, Bärbel
Vidadala, Rama S.R.
Dorr, Carlie S.
Navaluna, Edelmar D.
Whitman, Grant R.
Barrett, Kayleigh F.
Barrett, Lynn K.
Hulverson, Matthew A.
Choi, Ryan
Michaels, Samantha A.
Maly, Dustin J.
Hemphill, Andrew
Van Voorhis, Wesley C.
Joachim, Anja
author_facet Shrestha, Aruna
Ojo, Kayode K.
Koston, Florian
Ruttkowski, Bärbel
Vidadala, Rama S.R.
Dorr, Carlie S.
Navaluna, Edelmar D.
Whitman, Grant R.
Barrett, Kayleigh F.
Barrett, Lynn K.
Hulverson, Matthew A.
Choi, Ryan
Michaels, Samantha A.
Maly, Dustin J.
Hemphill, Andrew
Van Voorhis, Wesley C.
Joachim, Anja
author_sort Shrestha, Aruna
collection PubMed
description Cystoisosporosis is a leading diarrheal disease in suckling piglets. With the confirmation of resistance against the only available drug toltrazuril, there is a substantial need for novel therapeutics to combat the infection and its negative effects on animal health. In closely related apicomplexan species, bumped kinase inhibitors (BKIs) targeting calcium-dependent protein kinase 1 (CDPK1) were shown to be effective in inhibiting host-cell invasion and parasite growth. Therefore, the gene coding for Cystoisospora suis CDPK1 (CsCDPK1) was identified and cloned to investigate activity and thermal stabilization of the recombinant CsCDPK1 enzyme by BKI 1369. In this comprehensive study, the efficacy, safety and pharmacokinetics of BKI 1369 in piglets experimentally infected with Cystoisospora suis (toltrazuril-sensitive, Wien-I and toltrazuril-resistant, Holland-I strains) were determined in vivo and in vitro using an established animal infection model and cell culture, respectively. BKI 1369 inhibited merozoite proliferation in intestinal porcine epithelial cells-1 (IPEC-1) by at least 50% at a concentration of 40 nM, and proliferation was almost completely inhibited (>95%) at 200 nM. Nonetheless, exposure of infected cultures to 200 nM BKI 1369 for five days did not induce structural alterations in surviving merozoites as confirmed by transmission electron microscopy. Five-day treatment with BKI 1369 (10 mg/kg BW twice a day) effectively suppressed oocyst excretion and diarrhea and improved body weight gains in treated piglets without obvious side effects for both toltrazuril-sensitive, Wien-I and resistant, Holland-I C. suis strains. The plasma concentration of BKI 1369 in piglets increased to 11.7 μM during treatment, suggesting constant drug accumulation and exposure of parasites to the drug. Therefore, oral applications of BKI 1369 could potentially be a therapeutic alternative against porcine cystoisosporosis. For use in pigs, future studies on BKI 1369 should be directed towards ease of drug handling and minimizing treatment frequencies.
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spelling pubmed-64536702019-04-17 Bumped kinase inhibitor 1369 is effective against Cystoisospora suis in vivo and in vitro Shrestha, Aruna Ojo, Kayode K. Koston, Florian Ruttkowski, Bärbel Vidadala, Rama S.R. Dorr, Carlie S. Navaluna, Edelmar D. Whitman, Grant R. Barrett, Kayleigh F. Barrett, Lynn K. Hulverson, Matthew A. Choi, Ryan Michaels, Samantha A. Maly, Dustin J. Hemphill, Andrew Van Voorhis, Wesley C. Joachim, Anja Int J Parasitol Drugs Drug Resist Article Cystoisosporosis is a leading diarrheal disease in suckling piglets. With the confirmation of resistance against the only available drug toltrazuril, there is a substantial need for novel therapeutics to combat the infection and its negative effects on animal health. In closely related apicomplexan species, bumped kinase inhibitors (BKIs) targeting calcium-dependent protein kinase 1 (CDPK1) were shown to be effective in inhibiting host-cell invasion and parasite growth. Therefore, the gene coding for Cystoisospora suis CDPK1 (CsCDPK1) was identified and cloned to investigate activity and thermal stabilization of the recombinant CsCDPK1 enzyme by BKI 1369. In this comprehensive study, the efficacy, safety and pharmacokinetics of BKI 1369 in piglets experimentally infected with Cystoisospora suis (toltrazuril-sensitive, Wien-I and toltrazuril-resistant, Holland-I strains) were determined in vivo and in vitro using an established animal infection model and cell culture, respectively. BKI 1369 inhibited merozoite proliferation in intestinal porcine epithelial cells-1 (IPEC-1) by at least 50% at a concentration of 40 nM, and proliferation was almost completely inhibited (>95%) at 200 nM. Nonetheless, exposure of infected cultures to 200 nM BKI 1369 for five days did not induce structural alterations in surviving merozoites as confirmed by transmission electron microscopy. Five-day treatment with BKI 1369 (10 mg/kg BW twice a day) effectively suppressed oocyst excretion and diarrhea and improved body weight gains in treated piglets without obvious side effects for both toltrazuril-sensitive, Wien-I and resistant, Holland-I C. suis strains. The plasma concentration of BKI 1369 in piglets increased to 11.7 μM during treatment, suggesting constant drug accumulation and exposure of parasites to the drug. Therefore, oral applications of BKI 1369 could potentially be a therapeutic alternative against porcine cystoisosporosis. For use in pigs, future studies on BKI 1369 should be directed towards ease of drug handling and minimizing treatment frequencies. Elsevier 2019-04-02 /pmc/articles/PMC6453670/ /pubmed/30959327 http://dx.doi.org/10.1016/j.ijpddr.2019.03.004 Text en © 2019 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Shrestha, Aruna
Ojo, Kayode K.
Koston, Florian
Ruttkowski, Bärbel
Vidadala, Rama S.R.
Dorr, Carlie S.
Navaluna, Edelmar D.
Whitman, Grant R.
Barrett, Kayleigh F.
Barrett, Lynn K.
Hulverson, Matthew A.
Choi, Ryan
Michaels, Samantha A.
Maly, Dustin J.
Hemphill, Andrew
Van Voorhis, Wesley C.
Joachim, Anja
Bumped kinase inhibitor 1369 is effective against Cystoisospora suis in vivo and in vitro
title Bumped kinase inhibitor 1369 is effective against Cystoisospora suis in vivo and in vitro
title_full Bumped kinase inhibitor 1369 is effective against Cystoisospora suis in vivo and in vitro
title_fullStr Bumped kinase inhibitor 1369 is effective against Cystoisospora suis in vivo and in vitro
title_full_unstemmed Bumped kinase inhibitor 1369 is effective against Cystoisospora suis in vivo and in vitro
title_short Bumped kinase inhibitor 1369 is effective against Cystoisospora suis in vivo and in vitro
title_sort bumped kinase inhibitor 1369 is effective against cystoisospora suis in vivo and in vitro
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6453670/
https://www.ncbi.nlm.nih.gov/pubmed/30959327
http://dx.doi.org/10.1016/j.ijpddr.2019.03.004
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