The development of potent non-peptidic PTP-1B inhibitors.

Claude Dufresne,Patrick Roy,Zhaoyin Wang,Ernest Asante-Appiah,Wanda Cromlish,Yves Boie,Farnaz Forghani,Sylvie Desmarais,Qingping Wang,Kathryn Skorey,Deena Waddleton,Chidambaram Ramachandran,Brian P. Kennedy,Lijing Xu,Robert Gordon,Chi-Chung Chan,Yves Leblanc

The development of potent non-peptidic PTP-1B inhibitors.

2004

Claude Dufresne
Patrick Roy
Zhaoyin Wang
Ernest Asante-Appiah
Wanda Cromlish
Yves Boie
Farnaz Forghani
Sylvie Desmarais
Qingping Wang
Kathryn Skorey
Deena Waddleton
Chidambaram Ramachandran
Brian P. Kennedy
Lijing Xu
Robert Gordon
Chi-Chung Chan
Yves Leblanc

The SAR from our peptide libraries was exploited to design a series of potent deoxybenzoin PTP-1B inhibitors. The introduction of an ortho bromo substituent next to the difluoromethylphosphonate warhead gave up to 20-fold increase in potency compared to the desbromo analogues. In addition, these compounds were orally bioavailable and active in the animal models of non-insulin dependent diabetes mellitus (NIDDM).

Keywords:

Enzyme
Organic chemistry
Potency
Animal model
Biochemistry
Chemistry
Enzyme inhibitor
Peptide
Stereochemistry
In vivo
Substituent
Chemical synthesis
In vitro

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