Antisense Mediated Splicing Modulation For Inherited Metabolic Diseases: Challenges for Delivery

Pérez, Belén; Vilageliu, Lluı̈sa; Grinberg, Daniel; Desviat, Lourdes R.

doi:10.1089/nat.2013.0453

Cited by 12 publications

(9 citation statements)

References 81 publications

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“…Based on our previous work on antisense therapy for splicing defects [ 27 ], [ 28 ] one of our aims was to investigate the feasibility of correcting the spf/ash mutation and rescuing OTC expression by the use of AONs. The development of oligonucleotide therapeutics is progressing rapidly, with a large number of disease targets residing in the liver [ 29 ].…”

Section: Discussionmentioning

confidence: 99%

Functional Characterization of the spf/ash Splicing Variation in OTC Deficiency of Mice and Man

et al. 2015

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The spf/ash mouse model of ornithine transcarbamylase (OTC) deficiency, a severe urea cycle disorder, is caused by a mutation (c.386G>A; p.R129H) in the last nucleotide of exon 4 of the Otc gene, affecting the 5’ splice site and resulting in partial use of a cryptic splice site 48 bp into the adjacent intron. The equivalent nucleotide change and predicted amino acid change is found in OTC deficient patients. Here we have used liver tissue and minigene assays to dissect the transcriptional profile resulting from the “spf/ash” mutation in mice and man. For the mutant mouse, we confirmed liver transcripts corresponding to partial intron 4 retention by the use of the c.386+48 cryptic site and to normally spliced transcripts, with exon 4 always containing the c.386G>A (p.R129H) variant. In contrast, the OTC patient exhibited exon 4 skipping or c.386G>A (p.R129H)-variant exon 4 retention by using the natural or a cryptic splice site at nucleotide position c.386+4. The corresponding OTC tissue enzyme activities were between 3-6% of normal control in mouse and human liver. The use of the cryptic splice sites was reproduced in minigenes carrying murine or human mutant sequences. Some normally spliced transcripts could be detected in minigenes in both cases. Antisense oligonucleotides designed to block the murine cryptic +48 site were used in minigenes in an attempt to redirect splicing to the natural site. The results highlight the relevance of in depth investigations of the molecular mechanisms of splicing mutations and potential therapeutic approaches. Notably, they emphasize the fact that findings in animal models may not be applicable for human patients due to the different genomic context of the mutations.

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Section: Discussionmentioning

confidence: 99%

Functional Characterization of the spf/ash Splicing Variation in OTC Deficiency of Mice and Man

et al. 2015

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“…The present work also reports the efficacy of antisense oligonucleotide therapy for rescuing normal splicing of the cryptic splice site generated by GFM1 c.689+908G>A in patient fibroblasts. Easy to design and highly specific, antisense oligonucleotides have been used as RNA-modulators in cellular models of several genetic disorders [47] including ISCU myopathy [48]. The challenge is always to achieve the safe and efficient delivery of the therapeutic oligonucleotide to the required tissues.…”

Section: Discussionmentioning

confidence: 99%

Genes and Variants Underlying Human Congenital Lactic Acidosis—From Genetics to Personalized Treatment

Bravo-Alonso

Navarrete

Vega

et al. 2019

JCM

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Congenital lactic acidosis (CLA) is a rare condition in most instances due to a range of inborn errors of metabolism that result in defective mitochondrial function. Even though the implementation of next generation sequencing has been rapid, the diagnosis rate for this highly heterogeneous allelic condition remains low. The present work reports our group’s experience of using a clinical/biochemical analysis system in conjunction with genetic findings that facilitates the taking of timely clinical decisions with minimum need for invasive procedures. The system’s workflow combines different metabolomics datasets and phenotypic information with the results of clinical exome sequencing and/or RNA analysis. The system’s use detected genetic variants in 64% of a cohort of 39 CLA-patients; these variants, 14 of which were novel, were found in 19 different nuclear and two mitochondrial genes. For patients with variants of unknown significance, the genetic analysis was combined with functional genetic and/or bioenergetics analyses in an attempt to detect pathogenicity. Our results warranted subsequent testing of antisense therapy to rescue the abnormal splicing in cultures of fibroblasts from a patient with a defective GFM1 gene. The discussed system facilitates the diagnosis of CLA by avoiding the need to use invasive techniques and increase our knowledge of the causes of this condition.

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“…Our experience suggests that delivery reagents are necessary for the successful use of AON therapeutics in the liver, particularly targeting hepatocytes (e.g. for the treatment of hyperlipidaemia, hepatitis C or inherited metabolic disorders with major hepatic expression) (Disterer et al , ; Yilmaz‐Elis et al , ; Perez et al , ).…”

Section: Delivery Hurdles and How To Make The Most Of Themmentioning

confidence: 99%

Delivery is key: lessons learnt from developing splice‐switching antisense therapies

et al. 2017

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The use of splice‐switching antisense therapy is highly promising, with a wealth of pre‐clinical data and numerous clinical trials ongoing. Nevertheless, its potential to treat a variety of disorders has yet to be realized. The main obstacle impeding the clinical translation of this approach is the relatively poor delivery of antisense oligonucleotides to target tissues after systemic delivery. We are a group of researchers closely involved in the development of these therapies and would like to communicate our discussions concerning the validity of standard methodologies currently used in their pre‐clinical development, the gaps in current knowledge and the pertinent challenges facing the field. We therefore make recommendations in order to focus future research efforts and facilitate a wider application of therapeutic antisense oligonucleotides.

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Antisense Mediated Splicing Modulation For Inherited Metabolic Diseases: Challenges for Delivery

Cited by 12 publications

References 81 publications

Functional Characterization of the spf/ash Splicing Variation in OTC Deficiency of Mice and Man

Functional Characterization of the spf/ash Splicing Variation in OTC Deficiency of Mice and Man

Genes and Variants Underlying Human Congenital Lactic Acidosis—From Genetics to Personalized Treatment

Delivery is key: lessons learnt from developing splice‐switching antisense therapies

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