Downregulation of Zebrafish Cytosolic Sialidase Neu3.2 Affects Skeletal Muscle Development.

Int J Mol Sci

Unit of Biotechnology, Department of Molecular and Translational Medicine, University of Brescia, Viale Europa 11, 25123 Brescia, Italy.

Published: September 2023

AI Article Synopsis

  • Sialidases are enzymes that remove sialic acid from glycoconjugates, playing a key role in their turnover across different cellular compartments.
  • Four types of mammalian sialidases (NEU1-4) exhibit distinct properties, while zebrafish have seven sialidases, with Zebrafish Neu3.2 closely related to human NEU2, relevant for muscle differentiation.
  • Research showed that injecting morpholino in zebrafish embryos caused significant developmental defects and impaired muscle formation, but co-injecting mouse mRNA rescued these issues, highlighting the importance of cytosolic sialidase in muscle pathology research.

Article Abstract

Sialidases remove terminal sialic acids residues from the non-reducing ends of glycoconjugates. They have been recognized as catabolic enzymes that work within different subcellular compartments and can ensure the proper turn-over of glycoconjugates. Four mammalian sialidases (NEU1-4) exist, with different subcellular localization, pH optimum and substrate specificity. In zebrafish, seven different sialidases, with high homology to mammalian counterparts, have been identified. Zebrafish Neu3.2 is similar to the human cytosolic sialidase NEU2, which is involved in skeletal muscle differentiation and exhibits a broad substrate specificity toward gangliosides and glycoproteins. In zebrafish , mRNA is expressed during somite development, and its enzymatic activity has been detected in the skeletal muscle and heart of adult animals. In this paper, 1-4-cell-stage embryos injected with splice-blocking morpholino showed severe embryonic defects, mainly in somites, heart and anterior-posterior axis formation. and expressions were altered in morphants, and impaired musculature formation was associated with a defective locomotor behavior. Finally, the co-injection of mouse mRNA in morphants rescued the phenotype. These data are consistent with the involvement of cytosolic sialidase in pathologies related to muscle formation and support the validity of the model to investigate the pathogenesis of the diseases.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10487903PMC
http://dx.doi.org/10.3390/ijms241713578DOI Listing

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