Antisense oligonucleotide splicing modulation as a novel Cystic Fibrosis therapeutic approach for the W1282X nonsense mutation

被引:27
|
作者
Oren, Yifat S. [1 ]
Avizur-Barchad, Ofra [1 ]
Ozeri-Galai, Efrat [1 ]
Elgrabli, Renana [1 ]
Schirelman, Meital R. [1 ]
Blinder, Tehilla [1 ]
Stampfer, Chava D. [1 ]
Ordan, Merav [1 ]
Laselva, Onofrio [2 ,3 ]
Cohen-Cymberknoh, Malena [4 ,5 ,6 ]
Kerem, Eitan [7 ]
Bear, Christine E. [3 ]
Kerem, Batsheva [1 ,8 ]
机构
[1] Hadassah Kerem, SpliSense Biohouse Labs, Jerusalem, Israel
[2] Univ Foggia, Dept Med & Surg Sci, Foggia, Italy
[3] Hosp Sick Children, Res Inst, Div Mol Med, Toronto, ON M5G 0A4, Canada
[4] Univ Jerusalem, Pediat Pulmonol Unit, Jerusalem, Israel
[5] Univ Jerusalem, Hadassah Med Ctr, CF Ctr, Jerusalem, Israel
[6] Univ Jerusalem, Fac Med, Jerusalem, Israel
[7] Hadassah Hebrew Univ, Med Ctr, CF Ctr, Jerusalem, Israel
[8] Hebrew Univ Jerusalem, Dept Genet, Jerusalem, Israel
来源
JOURNAL OF CYSTIC FIBROSIS | 2022年 / 21卷 / 04期
关键词
Cystic fibrosis; Antisense oligonucleotides; Drug development; Exon skipping; CFTR; MECHANISMS; THERAPIES;
D O I
10.1016/j.jcf.2021.12.012
中图分类号
R56 [呼吸系及胸部疾病];
学科分类号
摘要
Background: Antisense oligonucleotide- based drugs for splicing modulation were recently approved for various genetic diseases with unmet need. Here we aimed to generate skipping over exon 23 of the CFTR transcript, to eliminate the W1282X nonsense mutation and avoid RNA degradation induced by the nonsense mediated mRNA decay mechanism, allowing production of partially active CFTR proteins lacking exon 23. Methods: similar to 80 ASOs were screened in 16HBEge W1282X cells. ASO candidates showing significant exon skipping were assessed for their W1282X allele selectivity and the increase of CFTR protein maturation and function. The effect of a highly potent ASO candidates was further analyzed in well differentiated primary human nasal epithelial cells, derived from a W1282X homozygous patient. Results: ASO screening led to identification of several ASOs that significantly decrease the level of CFTR transcripts including exon 23. These ASOs resulted in significant levels of mature CFTR protein and together with modulators restore the channel function following free uptake into these cells. Importantly, a highly potent lead AS0s, efficiently delivered by free uptake, was able to increase the level of transcripts lacking exon 23 and restore the CFTR function in cells from a W1282X homozygote patient. Conclusion: The highly efficient exon 23 skipping induced by free uptake of the lead ASO and the resulting levels of mature CFTR protein exhibiting channel function in the presence of modulators, demonstrate the ASO therapeutic potential benefit for CF patients carrying the W1282X mutation with the objective to advance the lead candidate SPL23-2 to proof-of-concept clinical study. (C) 2021 The Author(s). Published by Elsevier B.V. on behalf of European Cystic Fibrosis Society.
引用
收藏
页码:630 / 636
页数:7
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