AI Article Synopsis

  • Sgt2 is a small protein that serves as the initial docking point for newly synthesized tail-anchored (TA) proteins, guiding them to the endoplasmic reticulum via the GET pathway.
  • The first step in this process involves the interaction between Sgt2 and the Get4/Get5 complex, specifically through the N-terminal domain of Sgt2 binding to the ubiquitin-like domain of Get5.
  • Researchers characterized this interaction by solving structures of both Sgt2 and Get5, as well as their complex, using various experimental methods to validate their findings and understand how these proteins work together in TA protein delivery.

Article Abstract

Small, glutamine-rich, tetratricopeptide repeat protein 2 (Sgt2) is the first known port of call for many newly synthesized tail-anchored (TA) proteins released from the ribosome and destined for the GET (Guided Entry of TA proteins) pathway. This leads them to the residential membrane of the endoplasmic reticulum via an alternative to the cotranslational, signal recognition particle-dependent mechanism that their topology denies them. In yeast, the first stage of the GET pathway involves Sgt2 passing TA proteins on to the Get4/Get5 complex through a direct interaction between the N-terminal (NT) domain of Sgt2 and the ubiquitin-like (UBL) domain of Get5. Here we characterize this interaction at a molecular level by solving both a solution structure of Sgt2_NT, which adopts a unique helical fold, and a crystal structure of the Get5_UBL. Furthermore, using reciprocal chemical shift perturbation data and experimental restraints, we solve a structure of the Sgt2_NT/Get5_UBL complex, validate it via site-directed mutagenesis, and empirically determine its stoichiometry using relaxation experiments and isothermal titration calorimetry. Taken together, these data provide detailed structural information about the interaction between two key players in the coordinated delivery of TA protein substrates into the GET pathway.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3557055PMC
http://dx.doi.org/10.1073/pnas.1207518110DOI Listing

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