Downstream Alternate Start Site Allows N-Terminal Nonsense Variants to Escape NMD and Results in Functional Recovery by Readthrough and Modulator Combination

Genetic variants that introduce premature termination codons (PTCs) have remained difficult to therapeutically target due to lack of protein product. Nonsense mediated mRNA decay (NMD) targets PTC-bearing transcripts to reduce the potentially damaging effects of truncated proteins. Readthrough compo...

Descripción completa

Detalles Bibliográficos
Autores principales: Bowling, Alyssa, Eastman, Alice, Merlo, Christian, Lin, Gabrielle, West, Natalie, Patel, Shivani, Cutting, Garry, Sharma, Neeraj
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9504986/
https://www.ncbi.nlm.nih.gov/pubmed/36143233
http://dx.doi.org/10.3390/jpm12091448
_version_ 1784796360219820032
author Bowling, Alyssa
Eastman, Alice
Merlo, Christian
Lin, Gabrielle
West, Natalie
Patel, Shivani
Cutting, Garry
Sharma, Neeraj
author_facet Bowling, Alyssa
Eastman, Alice
Merlo, Christian
Lin, Gabrielle
West, Natalie
Patel, Shivani
Cutting, Garry
Sharma, Neeraj
author_sort Bowling, Alyssa
collection PubMed
description Genetic variants that introduce premature termination codons (PTCs) have remained difficult to therapeutically target due to lack of protein product. Nonsense mediated mRNA decay (NMD) targets PTC-bearing transcripts to reduce the potentially damaging effects of truncated proteins. Readthrough compounds have been tested on PTC-generating variants in attempt to permit translation through a premature stop. However, readthrough compounds have not proved efficacious in a clinical setting due to lack of stable mRNA. Here, we investigate N-terminal variants in the cystic fibrosis transmembrane conductance regulator (CFTR) gene, which have been shown to escape NMD, potentially through a mechanism of alternative translation initiation at downstream AUG codons. We hypothesized that N-terminal variants in CFTR that evade NMD will produce stable transcript, allowing CFTR function to be restored by a combination of readthrough and protein modulator therapy. We investigate this using two cell line models expressing CFTR-expression minigenes (EMG; HEK293s and CFBEs) and primary human nasal epithelial (NE) cells, and we test readthrough compounds G418 and ELX-02 in combination with CFTR protein modulators. HEK293 cells expressing the variants E60X and L88X generate CFTR-specific core glycosylated products that are consistent with downstream translation initiation. Mutation of downstream methionines at codons 150 and 152 does not result in changes in CFTR protein processing in cells expressing L88X-CFTR-EMG. However, mutation of methionine at 265 results in loss of detectable CFTR protein in cells expressing E60X, L88X, and Y122X CFTR-EMGs, indicating that downstream translation initiation is occurring at the AUG codon at position M265. In HEK293 stable cells harboring L88X, treatment with readthrough compounds alone allows for formation of full-length, but misfolded CFTR protein. Upon addition of protein modulators in combination with readthrough, we observe formation of mature, complex-glycosylated CFTR. In CFBE and NE cells, addition of readthrough ELX-02 and modulator therapy results in substantial recovery of CFTR function. Our work indicates that N-terminal variants generate stable CFTR transcript due to translation initiation at a downstream AUG codon. Thus, individuals with CF bearing 5′ nonsense variants that evade NMD are ideal candidates for treatment with clinically safe readthrough compounds and modulator therapy.
format Online
Article
Text
id pubmed-9504986
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-95049862022-09-24 Downstream Alternate Start Site Allows N-Terminal Nonsense Variants to Escape NMD and Results in Functional Recovery by Readthrough and Modulator Combination Bowling, Alyssa Eastman, Alice Merlo, Christian Lin, Gabrielle West, Natalie Patel, Shivani Cutting, Garry Sharma, Neeraj J Pers Med Article Genetic variants that introduce premature termination codons (PTCs) have remained difficult to therapeutically target due to lack of protein product. Nonsense mediated mRNA decay (NMD) targets PTC-bearing transcripts to reduce the potentially damaging effects of truncated proteins. Readthrough compounds have been tested on PTC-generating variants in attempt to permit translation through a premature stop. However, readthrough compounds have not proved efficacious in a clinical setting due to lack of stable mRNA. Here, we investigate N-terminal variants in the cystic fibrosis transmembrane conductance regulator (CFTR) gene, which have been shown to escape NMD, potentially through a mechanism of alternative translation initiation at downstream AUG codons. We hypothesized that N-terminal variants in CFTR that evade NMD will produce stable transcript, allowing CFTR function to be restored by a combination of readthrough and protein modulator therapy. We investigate this using two cell line models expressing CFTR-expression minigenes (EMG; HEK293s and CFBEs) and primary human nasal epithelial (NE) cells, and we test readthrough compounds G418 and ELX-02 in combination with CFTR protein modulators. HEK293 cells expressing the variants E60X and L88X generate CFTR-specific core glycosylated products that are consistent with downstream translation initiation. Mutation of downstream methionines at codons 150 and 152 does not result in changes in CFTR protein processing in cells expressing L88X-CFTR-EMG. However, mutation of methionine at 265 results in loss of detectable CFTR protein in cells expressing E60X, L88X, and Y122X CFTR-EMGs, indicating that downstream translation initiation is occurring at the AUG codon at position M265. In HEK293 stable cells harboring L88X, treatment with readthrough compounds alone allows for formation of full-length, but misfolded CFTR protein. Upon addition of protein modulators in combination with readthrough, we observe formation of mature, complex-glycosylated CFTR. In CFBE and NE cells, addition of readthrough ELX-02 and modulator therapy results in substantial recovery of CFTR function. Our work indicates that N-terminal variants generate stable CFTR transcript due to translation initiation at a downstream AUG codon. Thus, individuals with CF bearing 5′ nonsense variants that evade NMD are ideal candidates for treatment with clinically safe readthrough compounds and modulator therapy. MDPI 2022-09-01 /pmc/articles/PMC9504986/ /pubmed/36143233 http://dx.doi.org/10.3390/jpm12091448 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Bowling, Alyssa
Eastman, Alice
Merlo, Christian
Lin, Gabrielle
West, Natalie
Patel, Shivani
Cutting, Garry
Sharma, Neeraj
Downstream Alternate Start Site Allows N-Terminal Nonsense Variants to Escape NMD and Results in Functional Recovery by Readthrough and Modulator Combination
title Downstream Alternate Start Site Allows N-Terminal Nonsense Variants to Escape NMD and Results in Functional Recovery by Readthrough and Modulator Combination
title_full Downstream Alternate Start Site Allows N-Terminal Nonsense Variants to Escape NMD and Results in Functional Recovery by Readthrough and Modulator Combination
title_fullStr Downstream Alternate Start Site Allows N-Terminal Nonsense Variants to Escape NMD and Results in Functional Recovery by Readthrough and Modulator Combination
title_full_unstemmed Downstream Alternate Start Site Allows N-Terminal Nonsense Variants to Escape NMD and Results in Functional Recovery by Readthrough and Modulator Combination
title_short Downstream Alternate Start Site Allows N-Terminal Nonsense Variants to Escape NMD and Results in Functional Recovery by Readthrough and Modulator Combination
title_sort downstream alternate start site allows n-terminal nonsense variants to escape nmd and results in functional recovery by readthrough and modulator combination
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9504986/
https://www.ncbi.nlm.nih.gov/pubmed/36143233
http://dx.doi.org/10.3390/jpm12091448
work_keys_str_mv AT bowlingalyssa downstreamalternatestartsiteallowsnterminalnonsensevariantstoescapenmdandresultsinfunctionalrecoverybyreadthroughandmodulatorcombination
AT eastmanalice downstreamalternatestartsiteallowsnterminalnonsensevariantstoescapenmdandresultsinfunctionalrecoverybyreadthroughandmodulatorcombination
AT merlochristian downstreamalternatestartsiteallowsnterminalnonsensevariantstoescapenmdandresultsinfunctionalrecoverybyreadthroughandmodulatorcombination
AT lingabrielle downstreamalternatestartsiteallowsnterminalnonsensevariantstoescapenmdandresultsinfunctionalrecoverybyreadthroughandmodulatorcombination
AT westnatalie downstreamalternatestartsiteallowsnterminalnonsensevariantstoescapenmdandresultsinfunctionalrecoverybyreadthroughandmodulatorcombination
AT patelshivani downstreamalternatestartsiteallowsnterminalnonsensevariantstoescapenmdandresultsinfunctionalrecoverybyreadthroughandmodulatorcombination
AT cuttinggarry downstreamalternatestartsiteallowsnterminalnonsensevariantstoescapenmdandresultsinfunctionalrecoverybyreadthroughandmodulatorcombination
AT sharmaneeraj downstreamalternatestartsiteallowsnterminalnonsensevariantstoescapenmdandresultsinfunctionalrecoverybyreadthroughandmodulatorcombination

Ejemplares similares