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Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models

An excess phosphate burden in renal disease has pathological consequences for bone, kidney, and heart. Therapies to decrease intestinal phosphate absorption have been used to address the problem, but with limited success. Here, we describe the in vivo effects of a novel potent inhibitor of the intes...

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Autores principales: Wang, Xiaojun, Xu, Yanping, Yu, Xiaohong, Dey, Asim, Zhang, Hong Y., Zink, Charity M., Wodka, Derek, Porter, Gina, Matter, William F., Porras, Leah, Reidy, Charles A., Peterson, Jeffrey A., Mattioni, Brian E., Haas, Joseph V., Kowala, Mark C., Wetterau, John R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8863579/
https://www.ncbi.nlm.nih.gov/pubmed/35194979
http://dx.doi.org/10.1002/prp2.938
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author Wang, Xiaojun
Xu, Yanping
Yu, Xiaohong
Dey, Asim
Zhang, Hong Y.
Zink, Charity M.
Wodka, Derek
Porter, Gina
Matter, William F.
Porras, Leah
Reidy, Charles A.
Peterson, Jeffrey A.
Mattioni, Brian E.
Haas, Joseph V.
Kowala, Mark C.
Wetterau, John R.
author_facet Wang, Xiaojun
Xu, Yanping
Yu, Xiaohong
Dey, Asim
Zhang, Hong Y.
Zink, Charity M.
Wodka, Derek
Porter, Gina
Matter, William F.
Porras, Leah
Reidy, Charles A.
Peterson, Jeffrey A.
Mattioni, Brian E.
Haas, Joseph V.
Kowala, Mark C.
Wetterau, John R.
author_sort Wang, Xiaojun
collection PubMed
description An excess phosphate burden in renal disease has pathological consequences for bone, kidney, and heart. Therapies to decrease intestinal phosphate absorption have been used to address the problem, but with limited success. Here, we describe the in vivo effects of a novel potent inhibitor of the intestinal sodium‐dependent phosphate cotransporter NPT2b, LY3358966. Following treatment with LY3358966, phosphate uptake into plasma 15 min following an oral dose of radiolabeled phosphate was decreased 74% and 22% in mice and rats, respectively, indicating NPT2b plays a much more dominant role in mice than rats. Following the treatment with LY3358966 and radiolabeled phosphate, mouse feces were collected for 48 h to determine the ability of LY3358966 to inhibit phosphate absorption. Compared to vehicle‐treated animals, there was a significant increase in radiolabeled phosphate recovered in feces (8.6% of the dose, p < .0001). Similar studies performed in rats also increased phosphate recovered in feces (5.3% of the dose, p < .05). When used in combination with the phosphate binder sevelamer in rats, there was a further small, but not significant, increase in fecal phosphate. In conclusion, LY3358966 revealed a more prominent role for NPT2b on acute intestinal phosphate uptake into plasma in mice than rats. However, the modest effects on total intestinal phosphate absorption observed in mice and rats with LY3359866 when used alone or in combination with sevelamer highlights the challenge to identify new more effective therapeutic targets and/or drug combinations to treat the phosphate burden in patients with renal disease.
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spelling pubmed-88635792022-02-27 Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models Wang, Xiaojun Xu, Yanping Yu, Xiaohong Dey, Asim Zhang, Hong Y. Zink, Charity M. Wodka, Derek Porter, Gina Matter, William F. Porras, Leah Reidy, Charles A. Peterson, Jeffrey A. Mattioni, Brian E. Haas, Joseph V. Kowala, Mark C. Wetterau, John R. Pharmacol Res Perspect Original Articles An excess phosphate burden in renal disease has pathological consequences for bone, kidney, and heart. Therapies to decrease intestinal phosphate absorption have been used to address the problem, but with limited success. Here, we describe the in vivo effects of a novel potent inhibitor of the intestinal sodium‐dependent phosphate cotransporter NPT2b, LY3358966. Following treatment with LY3358966, phosphate uptake into plasma 15 min following an oral dose of radiolabeled phosphate was decreased 74% and 22% in mice and rats, respectively, indicating NPT2b plays a much more dominant role in mice than rats. Following the treatment with LY3358966 and radiolabeled phosphate, mouse feces were collected for 48 h to determine the ability of LY3358966 to inhibit phosphate absorption. Compared to vehicle‐treated animals, there was a significant increase in radiolabeled phosphate recovered in feces (8.6% of the dose, p < .0001). Similar studies performed in rats also increased phosphate recovered in feces (5.3% of the dose, p < .05). When used in combination with the phosphate binder sevelamer in rats, there was a further small, but not significant, increase in fecal phosphate. In conclusion, LY3358966 revealed a more prominent role for NPT2b on acute intestinal phosphate uptake into plasma in mice than rats. However, the modest effects on total intestinal phosphate absorption observed in mice and rats with LY3359866 when used alone or in combination with sevelamer highlights the challenge to identify new more effective therapeutic targets and/or drug combinations to treat the phosphate burden in patients with renal disease. John Wiley and Sons Inc. 2022-02-22 /pmc/articles/PMC8863579/ /pubmed/35194979 http://dx.doi.org/10.1002/prp2.938 Text en © 2022 The Authors. Pharmacology Research & Perspectives published by John Wiley & Sons Ltd, British Pharmacological Society and American Society for Pharmacology and Experimental Therapeutics. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Wang, Xiaojun
Xu, Yanping
Yu, Xiaohong
Dey, Asim
Zhang, Hong Y.
Zink, Charity M.
Wodka, Derek
Porter, Gina
Matter, William F.
Porras, Leah
Reidy, Charles A.
Peterson, Jeffrey A.
Mattioni, Brian E.
Haas, Joseph V.
Kowala, Mark C.
Wetterau, John R.
Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models
title Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models
title_full Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models
title_fullStr Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models
title_full_unstemmed Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models
title_short Effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (NPT2b) on intestinal phosphate absorption in mouse and rat models
title_sort effects of pharmacological inhibition of the sodium‐dependent phosphate cotransporter 2b (npt2b) on intestinal phosphate absorption in mouse and rat models
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8863579/
https://www.ncbi.nlm.nih.gov/pubmed/35194979
http://dx.doi.org/10.1002/prp2.938
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