AI Article Synopsis

  • Recent research has identified a second cytosolic hexosaminidase in mammals, called hexosaminidase D, which was previously not well understood.
  • This study successfully characterized the human and murine forms of hexosaminidase D, revealing its substrate specificity, pH dependence, and temperature stability.
  • Additionally, hexosaminidase D shows a nucleocytoplasmic location and is expressed in various mouse tissues, making it a significant addition to the known glycosidases in mammals.

Article Abstract

Some thirty years ago, work on mammalian tissues suggested the presence of two cytosolic hexosaminidases in mammalian cells; one of these has been more recently characterized in a recombinant form and has an important role in cellular function due to its ability to cleave beta-N-acetylglucosamine residues from a variety of nuclear and cytoplasmic proteins. However, the molecular nature of the second cytosolic hexosaminidase, named hexosaminidase D, has remained obscure. In the present study, we molecularly characterize for the first time the human and murine recombinant forms of enzymes, encoded by HEXDC genes, which appear to correspond to hexosaminidase D in terms of substrate specificity, pH dependency and temperature stability. Furthermore, a Myc-tagged form of this novel hexosaminidase displays a nucleocytoplasmic localization. Transcripts of the corresponding gene are expressed in a number of murine tissues. On the basis of its sequence, this enzyme represents, along with the lysosomal hexosaminidase subunits encoded by the HEXA and HEXB genes, the third class 20 glycosidase to be identified from mammalian sources.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2850170PMC
http://dx.doi.org/10.1042/BJ20081630DOI Listing

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