2019
DOI: 10.1111/febs.14997
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Structural and biochemical consequences of pyridoxine‐dependent epilepsy mutations that target the aldehyde binding site of aldehyde dehydrogenase ALDH7A1

Abstract: In humans, certain mutations in the gene encoding aldehyde dehydrogenase 7A1 are associated with pyridoxine‐dependent epilepsy (PDE). Understanding the impact of PDE‐causing mutations on the structure and activity of ALDH7A1 could allow for the prediction of symptom‐severity and aid the development of patient‐specific medical treatments. Herein, we investigate the biochemical and structural consequences of PDE missense mutations targeting residues in the aldehyde substrate binding site: N167S, P169S, A171V, G1… Show more

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Cited by 8 publications
(17 citation statements)
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“…Here we focus on a complete form of the biological unit (PDB code: 4ZUL), a homotetramer solved with a resolution of 0.170 nm and with the maximal coverage with the sequence P49419, without the mitochondrial target peptide [32]. Recently, important variants of the protein, associated with PDE and hampering its activity, have been also solved with atomic resolution [33]. Finally, the protein, as a major feature, according to the MobiDB database [34], does not have intrinsically disordered regions (IDPs).…”
Section: The Case Study Of Alpha-aminoadipic Semialdehyde Dehydrogenasementioning
confidence: 99%
See 1 more Smart Citation
“…Here we focus on a complete form of the biological unit (PDB code: 4ZUL), a homotetramer solved with a resolution of 0.170 nm and with the maximal coverage with the sequence P49419, without the mitochondrial target peptide [32]. Recently, important variants of the protein, associated with PDE and hampering its activity, have been also solved with atomic resolution [33]. Finally, the protein, as a major feature, according to the MobiDB database [34], does not have intrinsically disordered regions (IDPs).…”
Section: The Case Study Of Alpha-aminoadipic Semialdehyde Dehydrogenasementioning
confidence: 99%
“…This suggests that disease may be also due to an unpaired translocation of the protein to the mitochondrial compartment. For the sake of comparison, in Table S2 (Supplementary Materials), we label, in red, some PDE disease-related variations, known to occur in the aldehyde substrate binding site (N195S, P197S, A199V, G202V, W203G) and recently detailed with atomic resolution on their effect on the protein structure and function [33]. INPS predicts P197S, G202V, W203G as perturbing the protein stability (Table S2).…”
Section: The Case Study Of Alpha-aminoadipic Semialdehyde Dehydrogenasementioning
confidence: 99%
“…The tetramer observed in the crystal has been shown to be the active form of ALDH7A1 . We note this is the same crystal form that has been used to solve structures of wild‐type ALDH7A1 and several PDE mutant variants …”
Section: Resultsmentioning
confidence: 81%
“…We note that the NMN is also disordered in wild‐type ALDH7A1 structures when NAD + is included in the crystallisation at 5 mM (eg, see PDB code 4ZUK) . However, the cofactor is fully resolved by strong electron density when included in the crystallisation in the higher concentration range of 11 to 15 mM (PDB codes 2J6L, 6O4B‐C, 6O4E, 6O4H) . Because 15 mM NAD + was used for crystallisation of E427Q, the lack of electron density for the NMN is meaningful.…”
Section: Resultsmentioning
confidence: 99%
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