AI Article Synopsis

  • Glaucoma-associated myocilin is a protein linked to neuronal development and diseases, displaying a unique tripartite structure comprised of a Y-shaped parallel dimer-of-dimers.
  • Research reveals that the C-terminal region has a surprising repeat pattern that stabilizes the structure through interactions between oppositely charged residues.
  • This study enhances our understanding of protein structure and misfolding mechanisms in the context of myocilin-associated glaucoma, suggesting that certain variants can change its structure without affecting its stability.

Article Abstract

Glaucoma-associated myocilin is a member of the olfactomedins, a protein family involved in neuronal development and human diseases. Molecular studies of the myocilin N-terminal coiled coil demonstrate a unique tripartite architecture: a Y-shaped parallel dimer-of-dimers with distinct tetramer and dimer regions. The structure of the dimeric C-terminal 7-heptad repeats elucidates an unexpected repeat pattern involving inter-strand stabilization by oppositely charged residues. Molecular dynamics simulations reveal an alternate accessible conformation in which the terminal inter-strand disulfide limits the extent of unfolding and results in a kinked configuration. By inference, full-length myocilin is also branched, with two pairs of C-terminal olfactomedin domains. Selected variants within the N-terminal region alter the apparent quaternary structure of myocilin but do so without compromising stability or causing aggregation. In addition to increasing our structural knowledge of naturally occurring extracellular coiled coils and biomedically important olfactomedins, this work broadens the scope of protein misfolding in the pathogenesis of myocilin-associated glaucoma.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5685557PMC
http://dx.doi.org/10.1016/j.str.2017.09.008DOI Listing

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