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Merck

A therapeutic approach to pantothenate kinase associated neurodegeneration.

Nature communications (2018-10-26)
Lalit Kumar Sharma, Chitra Subramanian, Mi-Kyung Yun, Matthew W Frank, Stephen W White, Charles O Rock, Richard E Lee, Suzanne Jackowski
ABSTRAKT

Pantothenate kinase (PANK) is a metabolic enzyme that regulates cellular coenzyme A (CoA) levels. There are three human PANK genes, and inactivating mutations in PANK2 lead to pantothenate kinase associated neurodegeneration (PKAN). Here we performed a library screen followed by chemical optimization to produce PZ-2891, an allosteric PANK activator that crosses the blood brain barrier. PZ-2891 occupies the pantothenate pocket and engages the dimer interface to form a PANK•ATP•Mg2+•PZ-2891 complex. The binding of PZ-2891 to one protomer locks the opposite protomer in a catalytically active conformation that is refractory to acetyl-CoA inhibition. Oral administration of PZ-2891 increases CoA levels in mouse liver and brain. A knockout mouse model of brain CoA deficiency exhibited weight loss, severe locomotor impairment and early death. Knockout mice on PZ-2891 therapy gain weight, and have improved locomotor activity and life span establishing pantazines as novel therapeutics for the treatment of PKAN.

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Sigma-Aldrich
Anti-Integrin αV Antibody, clone 13C2, clone 13C2, Chemicon®, from mouse