AI Article Synopsis

  • 2A oligopeptide sequences can be used to link multiple protein coding sequences within a single Open Reading Frame (ORF) while allowing each protein to be translated separately.
  • The study indicates that proteins downstream of a 2A sequence, even without signal sequences, can still be directed into the endoplasmic reticulum (ER) due to a process called 'slipstream translocation.'
  • Strategies to improve this translocation efficiency include using longer 2A sequences or reorganizing the order of proteins in the polyprotein construct.

Article Abstract

Where 2A oligopeptide sequences occur within ORFs, the formation of the glycyl-prolyl peptide bond at the C-terminus of (each) 2A does not occur. This property can be used to concatenate sequences encoding several proteins into a single ORF: each component of such an artificial polyprotein is generated as a discrete translation product. 2A and '2A-like' sequences have become widely utilised in biotechnology and biomedicine. Individual proteins may also be co- and post-translationally targeted to a variety of sub-cellular sites. In the case of polyproteins bearing N-terminal signal sequences we observed, however, that the protein downstream of 2A (no signal) was translocated into the endoplasmic reticulum (ER). We interpreted these data as a form of 'slipstream' translocation: downstream proteins, without signals, were translocated through a translocon pore already formed by the signal sequence at the N-terminus of the polyprotein. Here we show this effect is, in fact, due to inhibition of the 2A reaction (formation of fusion protein) by the C-terminal region (immediately upstream of 2A) of some proteins when translocated into the ER. Solutions to this problem include the use of longer 2As (with a favourable upstream context) or modifying the order of proteins comprising polyproteins.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2978324PMC
http://dx.doi.org/10.1002/biot.200900134DOI Listing

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