Chaperones rescue the energetic landscape of mutant CFTR at single molecule and in cell.
Miklos BagdanyGuido VeitRyosuke FukudaRadu G AvramescuTsukasa OkiyonedaImad BaakliniJay SinghGuy SovakHaijin XuPirjo M ApajaSara SattinLenore K BeitelAriel RoldanGiorgio ColomboWilliam BalchJason C YoungGergely L LukacsPublished in: Nature communications (2017)
Molecular chaperones are pivotal in folding and degradation of the cellular proteome but their impact on the conformational dynamics of near-native membrane proteins with disease relevance remains unknown. Here we report the effect of chaperone activity on the functional conformation of the temperature-sensitive mutant cystic fibrosis channel (∆F508-CFTR) at the plasma membrane and after reconstitution into phospholipid bilayer. Thermally induced unfolding at 37 °C and concomitant functional inactivation of ∆F508-CFTR are partially suppressed by constitutive activity of Hsc70 and Hsp90 chaperone/co-chaperone at the plasma membrane and post-endoplasmic reticulum compartments in vivo, and at single-molecule level in vitro, indicated by kinetic and thermodynamic remodeling of the mutant gating energetics toward its wild-type counterpart. Thus, molecular chaperones can contribute to functional maintenance of ∆F508-CFTR by reshaping the conformational energetics of its final fold, a mechanism with implication in the regulation of metastable ABC transporters and other plasma membrane proteins activity in health and diseases.The F508 deletion (F508del) in the cystic fibrosis transmembrane conductance regulator (CFTR) is the most common CF causing mutation. Here the authors show that cytosolic chaperones shift the F508del channel conformation to the native fold by kinetic and thermodynamic remodelling of the gating energetics towards that of wild-type CTFR.
Keyphrases
- cystic fibrosis
- single molecule
- wild type
- heat shock
- endoplasmic reticulum
- pseudomonas aeruginosa
- heat shock protein
- lung function
- atomic force microscopy
- living cells
- heat stress
- single cell
- molecular dynamics simulations
- oxidative stress
- cell therapy
- public health
- healthcare
- mental health
- chronic obstructive pulmonary disease
- transcription factor
- crystal structure
- high glucose
- molecular dynamics
- aqueous solution
- stress induced
- endothelial cells