Discovery, structure-activity relationship, and biological evaluation of noninhibitory small molecule chaperones of glucocerebrosidase

非抑制性葡萄糖脑苷脂酶小分子伴侣的发现、构效关系及生物学评价

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作者:Samarjit Patnaik, Wei Zheng, Jae H Choi, Omid Motabar, Noel Southall, Wendy Westbroek, Wendy A Lea, Arash Velayati, Ehud Goldin, Ellen Sidransky, William Leister, Juan J Marugan

Abstract

A major challenge in the field of Gaucher disease has been the development of new therapeutic strategies including molecular chaperones. All previously described chaperones of glucocerebrosidase are enzyme inhibitors, which complicates their clinical development because their chaperone activity must be balanced against the functional inhibition of the enzyme. Using a novel high throughput screening methodology, we identified a chemical series that does not inhibit the enzyme but can still facilitate its translocation to the lysosome as measured by immunostaining of glucocerebrosidase in patient fibroblasts. These compounds provide the basis for the development of a novel approach toward small molecule treatment for patients with Gaucher disease.

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