| Literature DB >> 29531036 |
Alice E Parnell1, Silja Mordhorst2, Florian Kemper3, Mariacarmela Giurrandino1, Josh P Prince1, Nikola J Schwarzer3, Alexandre Hofer4, Daniel Wohlwend3, Henning J Jessen4,5, Stefan Gerhardt3, Oliver Einsle3,6, Petra C F Oyston7,8, Jennifer N Andexer9, Peter L Roach10,7.
Abstract
Inorganic polyphosphate is a ubiquitous, linear biopolymer built of up to thousands of phosphate residues that are linked by energy-rich phosphoanhydride bonds. Polyphosphate kinases of the family 2 (PPK2) use polyphosphate to catalyze the reversible phosphorylation of nucleotide phosphates and are highly relevant as targets for new pharmaceutical compounds and as biocatalysts for cofactor regeneration. PPK2s can be classified based on their preference for nucleoside mono- or diphosphates or both. The detailed mechanism of PPK2s and the molecular basis for their substrate preference is unclear, which is mainly due to the lack of high-resolution structures with substrates or substrate analogs. Here, we report the structural analysis and comparison of a class I PPK2 (ADP-phosphorylating) and a class III PPK2 (AMP- and ADP-phosphorylating), both complexed with polyphosphate and/or nucleotide substrates. Together with complementary biochemical analyses, these define the molecular basis of nucleotide specificity and are consistent with a Mg2+ catalyzed in-line phosphoryl transfer mechanism. This mechanistic insight will guide the development of PPK2 inhibitors as potential antibacterials or genetically modified PPK2s that phosphorylate alternative substrates.Entities:
Keywords: enzyme structure; kinase; kinetics; polyphosphate
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Year: 2018 PMID: 29531036 PMCID: PMC5879653 DOI: 10.1073/pnas.1710741115
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205