2‐ and N6‐functionalized adenosine‐5′‐diphosphate analogs for the inhibition of mortalin
2‐ and N6‐functionalized adenosine‐5′‐diphosphate analogs for the inhibition of mortalin
Our early efforts to find a covalent inhibitor of mortalin, a member of the 70 kDheat shock protein (Hsp70) family, led us to solve the structure of the mortalin nucleotide‐binding domain (NBD) in complex with N6‐propargyladenosine‐5′‐diphosphate. The acquired structure emphasizes the ability of the nucleotide‐binding pocket to accommodate modifiedADPcompounds. A library ofADPanalogs modified at either the 2‐ or N6‐positions of adenosine was screened against the mortalin‐NBD. Competitive inhibition and binding assays of the analogs demonstrate that modifications at the 2‐ or N6‐positions have potential to bind and inhibit mortalin uniquely compared to other Hsp70 homologs, and that modifications at the 2‐position confer the greatest selectivity in binding and inhibition of the mortalin‐NBD.
- Lawrence Berkeley National Laboratory United States
- Miami University United States
Adenosine Diphosphate, Mitochondrial Proteins, Small Molecule Libraries, Binding Sites, Humans, HSP70 Heat-Shock Proteins, Cloning, Molecular, Protein Binding
Adenosine Diphosphate, Mitochondrial Proteins, Small Molecule Libraries, Binding Sites, Humans, HSP70 Heat-Shock Proteins, Cloning, Molecular, Protein Binding
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