Literature DB >> 9748235

The human chitotriosidase gene. Nature of inherited enzyme deficiency.

R G Boot1, G H Renkema, M Verhoek, A Strijland, J Bliek, T M de Meulemeester, M M Mannens, J M Aerts.   

Abstract

The human chitinase, named chitotriosidase, is a member of family 18 of glycosylhydrolases. Following the cloning of the chitotriosidase cDNA (Boot, R. G., Renkema, G. H., Strijland, A., van Zonneveld, A. J., and Aerts, J. M. F. G. (1995) J. Biol. Chem. 270, 26252-26256), the gene and mRNA have been investigated. The chitotriosidase gene is assigned to chromosome 1q31-q32. The gene consists of 12 exons and spans about 20 kilobases. The nature of the common deficiency in chitotriosidase activity is reported. A 24-base pair duplication in exon 10 results in activation of a cryptic 3' splice site, generating a mRNA with an in-frame deletion of 87 nucleotides. All chitotriosidase-deficient individuals tested were homozygous for the duplication. The observed carrier frequency of about 35% indicates that the duplication is the predominant cause of chitotriosidase deficiency. The presence of the duplication in individuals from various ethnic groups suggests that this mutation is relatively old.

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Year:  1998        PMID: 9748235     DOI: 10.1074/jbc.273.40.25680

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  118 in total

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Authors:  B Winchester
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2.  High-resolution structures of a chitinase complexed with natural product cyclopentapeptide inhibitors: mimicry of carbohydrate substrate.

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3.  Chitotriosidase activity in plasma and mononuclear and polymorphonuclear leukocyte populations.

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6.  Human chitotriosidase polymorphisms G354R and A442V associated with reduced enzyme activity.

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7.  Evolution of mammalian chitinase(-like) members of family 18 glycosyl hydrolases.

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Review 9.  Potential role of chitinase 3-like-1 in inflammation-associated carcinogenic changes of epithelial cells.

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10.  Gaucher iPSC-derived macrophages produce elevated levels of inflammatory mediators and serve as a new platform for therapeutic development.

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