Literature DB >> 14766013

Human aldolase A natural mutants: relationship between flexibility of the C-terminal region and enzyme function.

Gabriella Esposito1, Luigi Vitagliano, Paola Costanzo, Loredana Borrelli, Rita Barone, Lorenzo Pavone, Paola Izzo, Adriana Zagari, Francesco Salvatore.   

Abstract

We have identified a new mutation in the FBP (fructose 1,6-bisphosphate) aldolase A gene in a child with suspected haemolytic anaemia associated with myopathic symptoms at birth and with a subsequent diagnosis of arthrogryposis multiplex congenita and pituitary ectopia. Sequence analysis of the whole gene, also performed on the patient's full-length cDNA, revealed only a Gly346-->Ser substitution in the heterozygous state. We expressed in a bacterial system the new aldolase A Gly346-->Ser mutant, and the Glu206-->Lys mutant identified by others, in a patient with an aldolase A deficit. Analysis of their functional profiles showed that the Gly346Ser mutant had the same Km as the wild-type enzyme, but a 4-fold lower kcat. The Glu206-->Lys mutant had a Km approx. 2-fold higher than that of both the Gly346-->Ser mutant and the wild-type enzyme, and a kcat value 40% less than the wild-type. The Gly346-->Ser and wild-type enzymes had the same Tm (melting temperature), which was approx. 6-7 degrees C higher than that of the Glu206-->Lys enzyme. An extensive molecular graphic analysis of the mutated enzymes, using human and rabbit aldolase A crystallographic structures, suggests that the Glu206-->Lys mutation destabilizes the aldolase A tetramer at the subunit interface, and highlights the fact that the glycine-to-serine substitution at position 346 limits the flexibility of the C-terminal region. These results also provide the first evidence that Gly346 is crucial for the correct conformation and function of aldolase A, because it governs the entry/release of the substrates into/from the enzyme cleft, and/or allows important C-terminal residues to approach the active site.

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Year:  2004        PMID: 14766013      PMCID: PMC1224144          DOI: 10.1042/BJ20031941

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  26 in total

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Authors:  S MINAKAMI; H YOSHIKAWA
Journal:  Biochem Biophys Res Commun       Date:  1965-02-03       Impact factor: 3.575

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Authors:  E Beutler; S Scott; A Bishop; N Margolis; F Matsumoto; W Kuhl
Journal:  Trans Assoc Am Physicians       Date:  1973

Review 5.  Aldolase gene and protein families: structure, expression and pathophysiology.

Authors:  F Salvatore; P Izzo; G Paolella
Journal:  Horiz Biochem Biophys       Date:  1986

6.  Functional and molecular modelling studies of two hereditary fructose intolerance-causing mutations at arginine 303 in human liver aldolase.

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