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Applying the pro-drug approach to afford highly bioavailable antagonists of P2Y(14) |
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| Authors: | Robichaud Joël Fournier Jean-François Gagné Sébastien Gauthier Jacques Yves Hamel Martine Han Yongxin Hénault Martin Kargman Stacia Levesque Jean-François Mamane Yaël Mancini Joseph Morin Nicolas Mulrooney Erin Wu Jin Black W Cameron |
| Institution: | Merck Frosst Centre for Therapeutic Research, 16711 TransCanada Hwy., Kirkland, Quebec, Canada H9H 3L1 |
| Abstract: | Our series of competitive antagonists against the G-protein coupled receptor P2Y14 were found to be highly shifted in the presence of serum (>99% protein bound). A binding assay using 2% human serum albumin (HSA) was developed to guide further SAR studies and led to the identification of the zwitterion 2, which is substantially less shifted (18-fold) than our previous lead compound 1 (323-fold). However, as the bioavailability of 2 was low, a library of ester pro-drugs was prepared (7a-7j) and assessed in vitro. The most interesting candidates were then profiled in vivo and led to the identification of the pro-drug 7j, which possesses a substantially improved pharmacokinetic profile. |
| Keywords: | P2Y14 GPR-105 Antagonist Pro-drug Protein binding |
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