AI Article Synopsis

  • Annexin A13 is a key protein in vertebrates that plays a role in calcium-dependent membrane binding and is primarily expressed in intestinal and kidney epithelial cells.
  • Alternative splicing produces two variants, A13a and A13b, with A13a showing unique structural properties and different thermal stability compared to A13b.
  • A13a binds more efficiently to acidic phospholipids in a calcium-dependent manner, which may influence its location within cells and highlight the functional differences between the two isoforms.

Article Abstract

Annexin A13 is the founder member of the vertebrate family of annexins, which are comprised of a tetrad of unique conserved domains responsible for calcium-dependent binding to membranes. Its expression is restricted to epithelial intestinal and kidney cells. Alternative splicing in the N-terminal region generates two isoforms, A13a and A13b, differing in a deletion of 41 residues in the former. We have confirmed the expression of both isoforms in human colon adenocarcinoma cells at the mRNA and protein levels. We have cloned, expressed, and purified human annexin A13a for the first time to analyze its structural characteristics. Its secondary structure and thermal stability differs greatly from the A13b isoform. The only tryptophan residue (Trp186) is buried in the protein core in the absence of calcium but is exposed to the solvent after calcium binding even though circular dichroism spectra are quite similar. Non-myristoylated annexin A13a binds in a calcium-dependent manner to acidic phospholipids but not to neutral or raft-like liposomes. Calcium requirements for binding to phosphatidylserine are around 6-fold lower than those required by the A13b isoform. This fact could account for the different subcellular localization of both annexins as binding to basolateral membranes seems to be calcium-dependent and myristoylation-independent.

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Source
http://dx.doi.org/10.1515/hsz-2016-0242DOI Listing

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