Litcius/Paper detail

Cotranslational folding cooperativity of contiguous domains of α-spectrin

Grant Kemp, Ola B. Nilsson, Pengfei Tian, Robert B. Best, Gunnar von Heijne

2020Proceedings of the National Academy of Sciences32 citationsDOIOpen Access PDF

Abstract

Proteins synthesized in the cell can begin to fold during translation before the entire polypeptide has been produced, which may be particularly relevant to the folding of multidomain proteins. Here, we study the cotranslational folding of adjacent domains from the cytoskeletal protein α-spectrin using force profile analysis (FPA). Specifically, we investigate how the cotranslational folding behavior of the R15 and R16 domains are affected by their neighboring R14 and R16, and R15 and R17 domains, respectively. Our results show that the domains impact each other's folding in distinct ways that may be important for the efficient assembly of α-spectrin, and may reduce its dependence on chaperones. Furthermore, we directly relate the experimentally observed yield of full-length protein in the FPA assay to the force exerted by the folding protein in piconewtons. By combining pulse-chase experiments to measure the rate at which the arrested protein is converted into full-length protein with a Bell model of force-induced rupture, we estimate that the R16 domain exerts a maximal force on the nascent chain of ∼15 pN during cotranslational folding.

Topics & Concepts

Protein foldingRibosomeTransloconSpectrinCooperativityFolding (DSP implementation)Polypeptide chainTranslation (biology)BiophysicsChemistryBiologyComputational biologyCell biologyMembrane proteinBiochemistryGeneMessenger RNACellRNACytoskeletonAmino acidElectrical engineeringEngineeringMembraneProtein Structure and DynamicsEnzyme Structure and FunctionRNA and protein synthesis mechanisms