Human farnesyl pyrophosphate synthase is allosterically inhibited by its own product.

Human farnesyl pyrophosphate synthase is allosterically inhibited by its own product.

Nature communications (2017-01-18)

Jaeok Park, Michal Zielinski, Alexandr Magder, Youla S Tsantrizos, Albert M Berghuis

摘要

Farnesyl pyrophosphate synthase (FPPS) is an enzyme of the mevalonate pathway and a well-established therapeutic target. Recent research has focused around a newly identified druggable pocket near the enzyme's active site. Pharmacological exploitation of this pocket is deemed promising; however, its natural biological function, if any, is yet unknown. Here we report that the product of FPPS, farnesyl pyrophosphate (FPP), can bind to this pocket and lock the enzyme in an inactive state. The K

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F6892

Sigma-Aldrich

法尼焦磷酸铵盐, methanol:ammonia solution, ≥95% (TLC)

I0503

Sigma-Aldrich

异戊烯焦磷酸盐三铵盐溶液, 1 mg/mL in methanol (:aqueous 10 mM NH₄OH (7:3)), ≥95% (TLC)

G6772

Sigma-Aldrich

香叶基焦磷酸盐铵盐, 1 mg/mL in methanol (:aqueous 10 mM NH₄OH (7:3)), ≥95% (TLC)

D4287

Sigma-Aldrich

γ,γ-二甲基烯丙基焦磷酸三铵盐, 1 mg/mL in methanol (:aqueous 10 mM NH₄OH (7:3)), ≥90% (TLC)