Literature DB >> 31570587

How internal cavities destabilize a protein.

Mengjun Xue1,2, Takuro Wakamoto3, Camilla Kejlberg1,2, Yuichi Yoshimura1,2, Tania Aaquist Nielsen1,2, Michael Wulff Risør1,4, Kristian Wejse Sanggaard4, Ryo Kitahara5,6, Frans A A Mulder7,2.   

Abstract

Although many proteins possess a distinct folded structure lying at a minimum in a funneled free energy landscape, thermal energy causes any protein to continuously access lowly populated excited states. The existence of excited states is an integral part of biological function. Although transitions into the excited states may lead to protein misfolding and aggregation, little structural information is currently available for them. Here, we show how NMR spectroscopy, coupled with pressure perturbation, brings these elusive species to light. As pressure acts to favor states with lower partial molar volume, NMR follows the ensuing change in the equilibrium spectroscopically, with residue-specific resolution. For T4 lysozyme L99A, relaxation dispersion NMR was used to follow the increase in population of a previously identified "invisible" folded state with pressure, as this is driven by the reduction in cavity volume by the flipping-in of a surface aromatic group. Furthermore, multiple partly disordered excited states were detected at equilibrium using pressure-dependent H/D exchange NMR spectroscopy. Here, unfolding reduced partial molar volume by the removal of empty internal cavities and packing imperfections through subglobal and global unfolding. A close correspondence was found for the distinct pressure sensitivities of various parts of the protein and the amount of internal cavity volume that was lost in each unfolding event. The free energies and populations of excited states allowed us to determine the energetic penalty of empty internal protein cavities to be 36 cal⋅Å-3.

Entities:  

Keywords:  high-pressure NMR; protein folding and cooperativity; protein stability; unfolded state

Year:  2019        PMID: 31570587      PMCID: PMC6800337          DOI: 10.1073/pnas.1911181116

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  66 in total

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