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A novel CCR2 antagonist inhibits atherogenesis in apoE deficient mice by achieving high receptor occupancy
CC Chemokine Receptor 2 (CCR2) and its endogenous ligand CCL2 are involved in a number of diseases, including atherosclerosis. Several CCR2 antagonists have been developed as potential therapeutic agents, however their in vivo clinical efficacy was limited. In this report, we aimed to determine whet...
| Autores principales: | , , , , , , , , , , , , |
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| Formato: | Online Artículo Texto |
| Lenguaje: | English |
| Publicado: |
Nature Publishing Group UK
2017
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| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5427923/ https://www.ncbi.nlm.nih.gov/pubmed/28246398 http://dx.doi.org/10.1038/s41598-017-00104-z |
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| author | Bot, Ilze Ortiz Zacarías, Natalia V. de Witte, Wilhelmus E. A. de Vries, Henk van Santbrink, Peter J. van der Velden, Daniël Kröner, Mara J. van der Berg, Dirk-Jan Stamos, Dean de Lange, Elizabeth C. M. Kuiper, Johan IJzerman, Adriaan P. Heitman, Laura H. |
| author_facet | Bot, Ilze Ortiz Zacarías, Natalia V. de Witte, Wilhelmus E. A. de Vries, Henk van Santbrink, Peter J. van der Velden, Daniël Kröner, Mara J. van der Berg, Dirk-Jan Stamos, Dean de Lange, Elizabeth C. M. Kuiper, Johan IJzerman, Adriaan P. Heitman, Laura H. |
| author_sort | Bot, Ilze |
| collection | PubMed |
| description | CC Chemokine Receptor 2 (CCR2) and its endogenous ligand CCL2 are involved in a number of diseases, including atherosclerosis. Several CCR2 antagonists have been developed as potential therapeutic agents, however their in vivo clinical efficacy was limited. In this report, we aimed to determine whether 15a, an antagonist with a long residence time on the human CCR2, is effective in inhibiting the development of atherosclerosis in a mouse disease model. First, radioligand binding assays were performed to determine affinity and binding kinetics of 15a on murine CCR2. To assess the in vivo efficacy, western-type diet fed apoE(−/−) mice were treated daily with 15a or vehicle as control. Treatment with 15a reduced the amount of circulating CCR2(+) monocytes and the size of the atherosclerotic plaques in both the carotid artery and the aortic root. We then showed that the long pharmacokinetic half-life of 15a combined with the high drug concentrations ensured prolonged CCR2 occupancy. These data render 15a a promising compound for drug development and confirms high receptor occupancy as a key parameter when targeting chemokine receptors. |
| format | Online Article Text |
| id | pubmed-5427923 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2017 |
| publisher | Nature Publishing Group UK |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-54279232017-05-12 A novel CCR2 antagonist inhibits atherogenesis in apoE deficient mice by achieving high receptor occupancy Bot, Ilze Ortiz Zacarías, Natalia V. de Witte, Wilhelmus E. A. de Vries, Henk van Santbrink, Peter J. van der Velden, Daniël Kröner, Mara J. van der Berg, Dirk-Jan Stamos, Dean de Lange, Elizabeth C. M. Kuiper, Johan IJzerman, Adriaan P. Heitman, Laura H. Sci Rep Article CC Chemokine Receptor 2 (CCR2) and its endogenous ligand CCL2 are involved in a number of diseases, including atherosclerosis. Several CCR2 antagonists have been developed as potential therapeutic agents, however their in vivo clinical efficacy was limited. In this report, we aimed to determine whether 15a, an antagonist with a long residence time on the human CCR2, is effective in inhibiting the development of atherosclerosis in a mouse disease model. First, radioligand binding assays were performed to determine affinity and binding kinetics of 15a on murine CCR2. To assess the in vivo efficacy, western-type diet fed apoE(−/−) mice were treated daily with 15a or vehicle as control. Treatment with 15a reduced the amount of circulating CCR2(+) monocytes and the size of the atherosclerotic plaques in both the carotid artery and the aortic root. We then showed that the long pharmacokinetic half-life of 15a combined with the high drug concentrations ensured prolonged CCR2 occupancy. These data render 15a a promising compound for drug development and confirms high receptor occupancy as a key parameter when targeting chemokine receptors. Nature Publishing Group UK 2017-03-03 /pmc/articles/PMC5427923/ /pubmed/28246398 http://dx.doi.org/10.1038/s41598-017-00104-z Text en © The Author(s) 2017 This work is licensed under a Creative Commons Attribution 4.0 International License. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ |
| spellingShingle | Article Bot, Ilze Ortiz Zacarías, Natalia V. de Witte, Wilhelmus E. A. de Vries, Henk van Santbrink, Peter J. van der Velden, Daniël Kröner, Mara J. van der Berg, Dirk-Jan Stamos, Dean de Lange, Elizabeth C. M. Kuiper, Johan IJzerman, Adriaan P. Heitman, Laura H. A novel CCR2 antagonist inhibits atherogenesis in apoE deficient mice by achieving high receptor occupancy |
| title | A novel CCR2 antagonist inhibits atherogenesis in apoE deficient mice by achieving high receptor occupancy |
| title_full | A novel CCR2 antagonist inhibits atherogenesis in apoE deficient mice by achieving high receptor occupancy |
| title_fullStr | A novel CCR2 antagonist inhibits atherogenesis in apoE deficient mice by achieving high receptor occupancy |
| title_full_unstemmed | A novel CCR2 antagonist inhibits atherogenesis in apoE deficient mice by achieving high receptor occupancy |
| title_short | A novel CCR2 antagonist inhibits atherogenesis in apoE deficient mice by achieving high receptor occupancy |
| title_sort | novel ccr2 antagonist inhibits atherogenesis in apoe deficient mice by achieving high receptor occupancy |
| topic | Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5427923/ https://www.ncbi.nlm.nih.gov/pubmed/28246398 http://dx.doi.org/10.1038/s41598-017-00104-z |
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