酶
核酸酶
核酸外切酶
磷脂酶
水解酶
生物化学
生物
磷脂酶D
磷脂酶A2
化学
细胞生物学
DNA聚合酶
作者
Kenta Ishii,S.J. Hermans,Maria Eleni Georgopoulou,Tracy L. Nero,Nancy C. Hancock,Gabriela A. N. Crespi,Michael A. Gorman,Jonathan H. Gooi,Michael W. Parker
摘要
Human 5′‐3′ exonuclease PLD3, a member of the phospholipase D family of enzymes, has been validated as a therapeutic target for treating Alzheimer's disease. Here, we have determined the crystal structure of the luminal domain of the enzyme at 2.3 Å resolution, revealing a bilobal structure with a catalytic site located between the lobes. We then compared the structure with published crystal structures of other human PLD family members which revealed that a number of catalytic and lipid recognition residues, previously shown to be key for phospholipase activity, are not conserved or, are absent. This led us to test whether the enzyme is actually a phospholipase. We could not measure any phospholipase activity but the enzyme shows robust nuclease activity. Finally, we have mapped key single nucleotide polymorphisms onto the structure which reveals plausible reasons as to why they have an impact on Alzheimer's disease.
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