Selection of a respiratory syncytial virus fusion inhibitor clinical candidate, part 1: Improving the pharmacokinetic profile using the structure-property relationship

被引:40
作者
Bonfanti, Jean-Francois
Doublet, Frederic
Fortin, Jerome
Lacrampe, Jean
Guillemont, Jerome
Muller, Philippe
Queguiner, Laurence
Arnoult, Eric
Gevers, Tom
Janssens, Peggy
Szel, Heidi
Willebrords, Rudy
Timmerman, Philip
Wuyts, Koen
Janssens, Frans
Sommen, Cois
Wigerinck, Piet
Andries, Koen
机构
[1] Johnson & Johnson Pharmaceut Res & Dev, Dept Med Chem, F-27106 Val De Reuil, France
[2] Johnson & Johnson Pharmaceut Res & Dev, Antimicrobial Res Dept, B-2340 Beerse, Belgium
[3] Johnson & Johnson Pharmaceut Res & Dev, ADME Tox & Bioanal Dept, B-2340 Beerse, Belgium
[4] Johnson & Johnson Pharmaceut Res & Dev, Dept Med Chem, B-2340 Beerse, Belgium
[5] Tibotec BVBA, B-2800 Mechelen, Belgium
关键词
D O I
10.1021/jm070143x
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
We previously reported the discovery of substituted benzimidazole fusion inhibitors with nanomolar activity against respiratory syncytial virus (Andries, K.; et al. Antiviral Res. 2003, 60, 209-219). A lead compound of the series was selected for preclinical evaluation. This drug candidate, JNJ-2408068 (formerly R 17059 1, 1), showed long tissue retention times in several species (rat, dog, and monkey), creating cause for concern. We herein describe the optimization program to develop compounds with improved properties in terms of tissue retention. We have identified the aminoethyl-piperidine moiety as being responsible for the long tissue retention time of 1. We have investigated the replacement or the modification of this group, and we suggest that the pK(a) of this part of the molecules influences both the antiviral activity and the pharmacokinetic profile. We were able to identify new respiratory syncytial virus inhibitors with shorter half-lives in lung tissue.
引用
收藏
页码:4572 / 4584
页数:13
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