AI Article Synopsis

  • Researchers discovered a new multiprotease complex that includes both α-secretase and γ-secretase, which are important in cleaving single-transmembrane proteins via a process called regulated intramembrane proteolysis (RIP).
  • Evidence shows that ADAM10 (A10), the main neuronal α-secretase, interacts with γ-secretase in cells and brain tissue, with both proteins working closely together and affecting each other’s activity.
  • The study highlights that certain proteins in the tetraspanin web help connect A10 and γ-secretase, leading to a refined understanding of how these secretases coordinate in processing protein substrates effectively within cells.

Article Abstract

Many single-transmembrane proteins are sequentially cleaved by ectodomain-shedding α-secretases and the γ-secretase complex, a process called regulated intramembrane proteolysis (RIP). These cleavages are thought to be spatially and temporally separate. In contrast, we provide evidence for a hitherto unrecognized multiprotease complex containing both α- and γ-secretase. ADAM10 (A10), the principal neuronal α-secretase, interacted and cofractionated with γ-secretase endogenously in cells and mouse brain. A10 immunoprecipitation yielded γ-secretase proteolytic activity and vice versa. In agreement, superresolution microscopy showed that portions of A10 and γ-secretase colocalize. Moreover, multiple γ-secretase inhibitors significantly increased α-secretase processing (r = -0.86) and decreased β-secretase processing of β-amyloid precursor protein. Select members of the tetraspanin web were important both in the association between A10 and γ-secretase and the γ → α feedback mechanism. Portions of endogenous BACE1 coimmunoprecipitated with γ-secretase but not A10, suggesting that β- and α-secretases can form distinct complexes with γ-secretase. Thus, cells possess large multiprotease complexes capable of sequentially and efficiently processing transmembrane substrates through a spatially coordinated RIP mechanism.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4687875PMC
http://dx.doi.org/10.1083/jcb.201502001DOI Listing

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