Correctors and Potentiators Rescue Function of the Truncated W1282X-Cystic Fibrosis Transmembrane Regulator (CFTR) Translation Product

Haggie, Peter M.; Phuan, Puay‐Wah; Tan, Joseph-Anthony; Xu, Haijin; Avramescu, Radu G.; Perdomo, Doranda; Zlock, Lorna; Nielson, Dennis W.; Finkbeiner, Walter E.; Lukacs, Gergely L.; Verkman, A. S.

doi:10.1074/jbc.m116.764720

Cited by 78 publications

(124 citation statements)

References 52 publications

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“…However, the expression of this shorter CFTR can be increased by incubation with VX-809 ( Fig. 1C), as reported previously (Haggie et al 2017). Although the full-length read-through protein was not detected, even with G418 treatment (Fig.…”

Section: Chloride Currents Carried By a Mixture Of C-terminus Truncatsupporting

confidence: 88%

“…; Haggie et al . ; Mutyam et al . ; ClinicalTrials.gov Identifier: NCT03624101 (https://clinicaltrials.gov/ct2/show/NCT03624101)).…”

Section: Discussionmentioning

confidence: 99%

“…Lumacaftor and Tezacaftor) to enhance the function of the truncated protein. However, it is unclear if these CFTR modulators, which are now clinical medicines, can be universally applied to PTCs since the relationship between the position of the PTC and the function of the truncated protein has yet to be established (Wang et al 2007;Haggie et al 2017;Mutyam et al 2017;Xue et al 2017;Yeh et al 2019b; ClinicalTrials.gov Identifier: NCT03624101 (https://clinicaltrials.gov/ct2/show/NCT03624101)). In theory, reagents that can promote read-through have the greatest potential for overcoming PTCs, and indeed compounds such as Ataluren and G418 have been shown to increase the expression of read-through CFTR in vitro (Howard et al 1996;Roy et al 2016) and in vivo (Wilschanski et al 2003;Du et al 2008).…”

Section: Discussionmentioning

confidence: 99%

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Positional effects of premature termination codons on the biochemical and biophysical properties of CFTR

Yeh

Hwang

2019

The Journal of Physiology

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Key points Biochemical and biophysical characterizations of three nonsense mutations of cystic fibrosis transmembrane conductance regulator (CFTR) associated with a severe form of cystic fibrosis (CF) reveal the importance and heterogenous effects of the position of the premature termination codon (PTC) on the CFTR protein function. Electrophysiological studies of W1282X‐CFTR, whose PTC is closer to the C‐terminus of CFTR, suggest the presence of both C‐terminus truncated CFTR proteins that are poorly functional and read‐through, full‐length products. For G542X‐ and E60X‐CFTR, the only mechanism capable of generating functional proteins is the read‐through, but the outcome of read‐through products is highly variable depending on the interplay between the missense mutation caused by the read‐through and the structural context of the protein. Pharmacological studies of these three PTCs with various CFTR modulators suggest position‐dependent therapeutic strategies for these disease‐inflicting mutations. Abstract About one‐third of genetic diseases and cancers are caused by the introduction of premature termination codons (PTCs). In theory, the location of the PTC in a gene determines the alternative mechanisms of translation, including premature cessation or reinitiation of translation, and read‐through, resulting in differential effects on protein integrity. In this study, we used CFTR as a model system to investigate the positional effect of the PTC because of its well‐understood structure‐function relationship and pathophysiology. The characterization of three PTC mutations, E60X‐, G542X‐ and W1282X‐CFTR revealed heterogenous effects of these PTCs on CFTR function. The W1282X mutation results in both C‐terminus truncated and read‐through proteins that are partially or fully functional. In contrast, only the read‐through protein is functional with E60X‐ and G542X‐CFTR, although abundant N‐terminus truncated proteins due to reinitiation of translation were detected in E60X‐CFTR. Single‐channel studies of the read‐through proteins of E60X‐ and G542X‐CFTR demonstrated that both mutations have a single‐channel amplitude similar to wild type (WT), and good responses to high‐affinity ATP analogues, suggesting intact ion permeation pathways and nucleotide binding domains (NBDs), albeit with reduced open probability (Po). The comparison of the Po of these mutations with the proposed missense mutations revealed potential identities of the read‐through products. Importantly, a majority of the functional protein studied responds to CFTR modulators like GLPG1837 and Lumacaftor. These results not only expand current understanding of the molecular (patho)physiology of CFTR, but also infer therapeutic strategies for different PTC mutations at large.

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Section: Chloride Currents Carried By a Mixture Of C-terminus Truncatsupporting

confidence: 88%

“…; Haggie et al . ; Mutyam et al . ; ClinicalTrials.gov Identifier: NCT03624101 (https://clinicaltrials.gov/ct2/show/NCT03624101)).…”

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Positional effects of premature termination codons on the biochemical and biophysical properties of CFTR

Yeh

Hwang

2019

The Journal of Physiology

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“…Also, a panel of known CFTR modulators was tested, including correctors VX-809, VX-661, C3, and C18, which target the NBD1-MSD interface, 9 C4, which targets NBD2, 16 CoPo-22, a CFTR modulator with dual corrector and potentiator function, 12 and W1282X corr -A23, which corrects CFTR 1281 , the protein product generated by the W1282X-CFTR nonsense mutation. 17 None of these correctors increased ΔF508-NBD1 cell surface expression; nor did previously described potentiators VX-770 and PG-01.…”

Section: Resultsmentioning

confidence: 92%

ΔF508-CFTR Modulator Screen Based on Cell Surface Targeting of a Chimeric Nucleotide Binding Domain 1 Reporter

et al. 2018

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The most common cystic fibrosis–causing mutation in the cystic fibrosis transmembrane conductance regulator (CFTR) is deletion of phenylalanine at residue 508 (ΔF508). The ΔF508 mutation impairs folding of nucleotide binding domain 1 (NBD1) and interfacial interactions of NBD1 and the membrane spanning domains. Here, we report a domain-targeted screen to identify ΔF508-CFTR modulators that act on NBD1. A biochemical screen for ΔF508-NBD1 cell surface expression was done in Madin–Darby canine kidney cells expressing a chimeric reporter consisting of ΔF508-NBD1, the CD4 transmembrane domain, and an extracellular horseradish peroxidase (HRP) reporter. Using a luminescence readout of HRP activity, the screen was robust with a Z′ factor of 0.7. The screening of ~20,000 synthetic small molecules allowed the identification of compounds from four chemical classes that increased ΔF508-NBD1 cell surface expression by up to 4-fold; for comparison, a 12-fold increased cell surface expression was found for a wild-type NBD1 chimera. While the compounds were inactive as correctors of full-length ΔF508-CFTR, several carboxamide-benzothiophenes had potentiator activity with low micromolar EC50. Interestingly, the potentiators did not activate G551D or wild-type CFTR. Our results provide a proof of concept for a cell-based NBD1 domain screen to identify ΔF508-CFTR modulators that target the NBD1 domain.

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“…A recent study showed that VX-770 acts additively with VX-809 to restore CFTR function in chronically treated R117H/ ΔF508 cells [52]. Surprisingly however, increased chloride conductance was not seen in W1282X cells despite the presence of adequate transcript levels when treated with both VX-770 and VX-809 [53]. As the combination of VX-770 and VX-809 (i.e., Orkambi) is now used clinically for treating patients carrying the ΔF508 mutation, it seems fitting to rigorously examine its effects on other CF mutations to potentially extend its application.…”

Section: Ongoing Challenges and Future Perspectivesmentioning

confidence: 99%

CFTR potentiators: from bench to bedside

Jih

Lin²,

Saito

et al. 2017

Current Opinion in Pharmacology

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One major breakthrough in cystic fibrosis research in the past decade is the development of drugs that target the root cause of the disease—dysfunctional CFTR protein. One of the compounds, Ivacaftor or Kalydeco, which has been approved for clinical use since 2012, acts by promoting the gating function of CFTR. Our recent studies have led to a gating model that features an energetic coupling between NBD dimerization and gate opening/closing in CFTR’s TMDs. Based on this model, we showed that ATP analogs can enhance CFTR gating by facilitating NBD dimerization, whereas Ivacaftor works by stabilizing the open channel conformation of the TMDs. This latter idea also explains the near omnipotence of Ivacaftor. Furthermore, this model marks multiple approaches to synergistically boost the open probability of CFTR by influencing distinct molecular events that control gating conformational changes.

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Correctors and Potentiators Rescue Function of the Truncated W1282X-Cystic Fibrosis Transmembrane Regulator (CFTR) Translation Product

Cited by 78 publications

References 52 publications

Positional effects of premature termination codons on the biochemical and biophysical properties of CFTR

Positional effects of premature termination codons on the biochemical and biophysical properties of CFTR

ΔF508-CFTR Modulator Screen Based on Cell Surface Targeting of a Chimeric Nucleotide Binding Domain 1 Reporter

CFTR potentiators: from bench to bedside

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