Targeting the BACE1 Active Site Flap Leads to a Potent Inhibitor That Elicits Robust Brain A? Reduction in Rodents [electronic resource]

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Ngôn ngữ: eng

Ký hiệu phân loại: 547 Organic chemistry

Thông tin xuất bản: Washington, D.C. : Oak Ridge, Tenn. : United States. Dept. of Energy. Office of Science ; Distributed by the Office of Scientific and Technical Information, U.S. Dept. of Energy, 2016

Mô tả vật lý: Size: p. 271-276 : , digital, PDF file.

Bộ sưu tập: Metadata

ID: 261020

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By targeting the flap backbone of the BACE1 active site, we discovered 6-dimethylisoxazole-substituted biaryl aminothiazine 18 with 34-fold improved BACE1 inhibitory activity over the lead compound 1. The cocrystal structure of 18 bound to the active site indicated two hydrogen-bond interactions between the dimethylisoxazole and threonine 72 and glutamine 73 of the flap. Incorporation of the dimethylisoxazole substitution onto the related aminothiazine carboxamide series led to pyrazine-carboxamide 26 as a very potent BACE1 inhibitor (IC<
sub>
50<
/sub>
<
1 nM). This compound demonstrated robust brain A? reduction in rat dose?response studies. Thus, compound 26 may be useful in testing the amyloid hypothesis of Alzheimer?s disease.

1. 37 inorganic, organic, physical, and analytical chemistry
2. 60 applied life sciences
3. A?42
4. Alzheimer?s disease
5. Aminothiazine
6. Amyloid hypothesis
7. Bace1
8. Inhibitor

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