The discovery of a potent series of carboxamide TRPA1 antagonists

被引:7
作者
Pryde, D. C. [1 ,6 ]
Marron, B. [2 ]
West, C. G. [2 ]
Reister, S. [2 ]
Amato, G. [2 ]
Yoger, K. [2 ]
Padilla, K. [2 ]
Turner, J. [3 ]
Swain, N. A. [1 ]
Cox, P. J. [3 ]
Skerratt, S. E. [1 ]
Ryckmans, T. [4 ]
Blakemore, D. C. [1 ]
Warmus, J. [5 ]
Gerlach, A. C. [2 ]
机构
[1] Pfizer Worldwide Med Chem, Neurosci & Pain Res Unit, Portway Bldg,Granta Pk, Great Abington CB21 6GS, Cambs, England
[2] Icagen Inc, 4222 Emperor Blvd,Suite 350, Durham, NC 27703 USA
[3] Neurosci & Pain Res Unit, Portway Bldg,Granta Pk, Great Abington CB21 6GS, Cambs, England
[4] Pfizer Worldwide Med Chem, Ramsgate Rd, Sandwich CT13 9NJ, Kent, England
[5] Pfizer Worldwide Med Chem, Neurosci & Pain Res Unit, Groton, CT USA
[6] Curadev UK, Innovat House,Discovery Pk, Sandwich CT14 9FF, Kent, England
关键词
BIOLOGICAL EVALUATION; CHANNEL TRPA1; DRUG TARGETS; RECEPTOR; PAIN; INFLAMMATION; ACTIVATE; NEURONS; TRPV1; COLD;
D O I
10.1039/c6md00387g
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
A series of potent and selective carboxamide TRPA1 antagonists were identified by a high throughput screen. Structure-activity relationship studies around this series are described, resulting in a highly potent example of the series. Pharmacokinetic and skin flux data are presented for this compound. Efficacy was observed in a topical cinnamaldehyde flare study, providing a topical proof of pharmacology for this mechanism. These data suggest TRPA1 antagonism could be a viable mechanism to treat topical conditions such as atopic dermatitis.
引用
收藏
页码:2145 / 2158
页数:14
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