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Design and development of a series of borocycles as selective,covalent kallikrein 5 inhibitors |
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| Authors: | Ann L. Walker Alexis Denis Ryan P. Bingham Anne Bouillot Emma V. Edgar Alan Ferrie Duncan S. Holmes Alain Laroze John Liddle Marie-Helene Fouchet Alexandre Moquette Pam Nassau Andrew C. Pearce Oxana Polyakova Kathrine J. Smith Pamela Thomas James H. Thorpe Lionel Trottet Alain Hovnanian |
| Affiliation: | 1. GlaxoSmithKline R&D, Medicines Research Centre, Gunnels Wood Road, Stevenage, Hertfordshire SG1 2NY, UK;2. INSERM UMR1163 Laboratory of Genetic Skin Diseases, Imagine Institute and Université Paris Descarte-Sorbonne Paris Cité, Paris, France |
| Abstract: | The connection between Netherton syndrome and overactivation of epidermal/dermal proteases, particularly Kallikrein 5 (KLK5) has been well established and it is expected that a KLK5 inhibitor would improve the dermal barrier and also reduce the pain and itch that afflict Netherton syndrome patients. One of the challenges of covalent protease inhibitors has been achieving selectivity over closely related targets. In this paper we describe the use of structural insight to design and develop a selective and highly potent reversibly covalent KLK5 inhibitor from an initial weakly binding fragment. |
| Keywords: | Corresponding author. KLK1 kallikrein 1 KLKB1 kallikrein B1 KLK5 kallikrein 5 KLK7 kallikrein 7 KLK8 kallikrein 8 KLK14 kallikrein 14 LCMS liquid chromatography-mass spectrometry LEKTI lympho-epithelial kazal-type-related inhibitor NS Netherton Syndrome NMR nuclear magnetic resonance serine protease inhibitor kazal-type 5 gene KLK1 KLK5 KLKB1 LEKTI Netherton syndrome |
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