Your search keyword '"Codon, Nonsense drug effects"' showing total 95 results

1. Investigating therapeutic nonsense suppression in a neurofibromatosis mouse model.

Author

Wu C, Shazeeb MS, Mangkalaphiban K, Han G, Peker A, Rentiya ZS, Gounis MJ, and Jacobson A

Subjects

Animals, Mice, Male, Female, Oxadiazoles pharmacology, Oxadiazoles therapeutic use, Humans, Mice, Inbred C57BL, Mice, Transgenic, Codon, Nonsense drug effects, Disease Models, Animal, Neurofibromatosis 1 genetics, Neurofibromatosis 1 drug therapy, Neurofibromin 1 genetics

Abstract

Neurofibromatosis type 1 (NF1) is a human genetic disorder caused by variants in the NF1 gene. Plexiform neurofibromas, one of many NF1 manifestations, are benign peripheral nerve sheath tumors occurring in up to 50% of NF1 patients. A substantial fraction of NF1 pathogenetic variants are nonsense mutations, which result in the synthesis of truncated non-functional NF1 protein (neurofibromin). To date, no therapeutics have restored neurofibromin expression or addressed the consequences of this protein's absence in NF1 nonsense mutation patients, but nonsense suppression is a potential approach to the problem. Ataluren is a small molecule drug that has been shown to stimulate functional nonsense codon readthrough in several models of nonsense mutation diseases, as well as in Duchenne muscular dystrophy patients. To test ataluren's potential applicability in nonsense mutation NF1 patients, we evaluated its therapeutic effects using three treatment regimens in a previously established NF1 patient-derived (c.2041C > T; p.Arg681X) nonsense mutation mouse model. Collectively, our experiments indicate that: i) ataluren appeared to slow the growth of neurofibromas and alleviate some paralysis phenotypes, ii) female Nf1-nonsense mutation mice manifested more severe paralysis and neurofibroma phenotypes than male mice, iii) ataluren doses with apparent effectiveness were lower in female mice than in male mice, and iv) age factors also influenced ataluren's effectiveness., Competing Interests: Declaration of competing interest A.J. is co-founder, director, consultant and shareholder for PTC Therapeutics Inc. M.J.G. is a consultant for Alembic LLC, Astrocyte Pharmaceuticals, BendIt Technologies, Cerenovus, Imperative Care, Jacob's Institute, Medtronic Neurovascular, Mivi Neurosciences, phenox GMbH, Q'Apel, Route 92 Medical, Scientia, Simcerre, Stryker Neurovascular, Stryker Sustainability Solutions, and Wallaby Medical and shareholder of Imperative Care, InNeuroCo, Galaxy Therapeutics, Kapto, Neurogami and Synchron. M.S.S. is a consultant for Sanofi. All other authors declare no competing interests., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

2. 2-Guanidino-quinazoline promotes the readthrough of nonsense mutations underlying human genetic diseases.

Author

Bidou L, Bugaud O, Merer G, Coupet M, Hatin I, Chirkin E, Karri S, Demais S, François P, Cintrat JC, and Namy O

Subjects

Cell Line, Codon, Terminator drug effects, Codon, Terminator genetics, Drug Evaluation, Preclinical, Genes, Reporter drug effects, Gentamicins pharmacology, High-Throughput Screening Assays, Humans, Muscular Dystrophy, Duchenne drug therapy, Muscular Dystrophy, Duchenne genetics, Codon, Nonsense drug effects, Codon, Nonsense genetics, Genetic Diseases, Inborn drug therapy, Genetic Diseases, Inborn genetics, Guanidines pharmacology, Quinazolines pharmacology

Abstract

Premature termination codons (PTCs) account for 10 to 20% of genetic diseases in humans. The gene inactivation resulting from PTCs can be counteracted by the use of drugs stimulating PTC readthrough, thereby restoring production of the full-length protein. However, a greater chemical variety of readthrough inducers is required to broaden the medical applications of this therapeutic strategy. In this study, we developed a reporter cell line and performed high-throughput screening (HTS) to identify potential readthrough inducers. After three successive assays, we isolated 2-guanidino-quinazoline (TLN468). We assessed the clinical potential of this drug as a potent readthrough inducer on the 40 PTCs most frequently responsible for Duchenne muscular dystrophy (DMD). We found that TLN468 was more efficient than gentamicin, and acted on a broader range of sequences, without inducing the readthrough of normal stop codons (TC).

Published

2022

3. Nonselective TRPC channel inhibition and suppression of aminoglycoside-induced premature termination codon readthrough by the small molecule AC1903.

Author

Baradaran-Heravi A, Bauer CC, Pickles IB, Hosseini-Farahabadi S, Balgi AD, Choi K, Linley DM, Beech DJ, Roberge M, and Bon RS

Subjects

Humans, Protein Synthesis Inhibitors, Aminoglycosides pharmacology, Codon, Nonsense drug effects, Indazoles pharmacology, TRPC Cation Channels antagonists & inhibitors, TRPC Cation Channels genetics, TRPC Cation Channels metabolism

Abstract

Nonsense mutations, which occur in ∼11% of patients with genetic disorders, introduce premature termination codons (PTCs) that lead to truncated proteins and promote nonsense-mediated mRNA decay. Aminoglycosides such as G418 permit PTC readthrough and so may be used to address this problem. However, their effects are variable between patients, making clinical use of aminoglycosides challenging. In this study, we tested whether TRPC nonselective cation channels contribute to the variable PTC readthrough effect of aminoglycosides by controlling their cellular uptake. Indeed, a recently reported selective TRPC5 inhibitor, AC1903, consistently suppressed G418 uptake and G418-induced PTC readthrough in the DMS-114 cancer cell line and junctional epidermolysis bullosa (JEB) patient-derived keratinocytes. Interestingly, the effect of AC1903 in DMS-114 cells was mimicked by nonselective TRPC inhibitors, but not by well-characterized inhibitors of TRPC1/4/5 (Pico145, GFB-8438) or TRPC3/6/7 (SAR7334), suggesting that AC1903 may work through additional or undefined targets. Indeed, in our experiments, AC1903 inhibited multiple TRPC channels including TRPC3, TRPC4, TRPC5, TRPC6, TRPC4-C1, and TRPC5-C1, as well as endogenous TRPC1:C4 channels in A498 renal cancer cells, all with low micromolar IC 50 values (1.8-18 μM). We also show that AC1903 inhibited TRPV4 channels, but had weak or no effects on TRPV1 and no effect on the nonselective cation channel PIEZO1. Our study reveals that AC1903 has previously unrecognized targets, which need to be considered when interpreting results from experiments with this compound. In addition, our data strengthen the hypothesis that nonselective calcium channels are involved in aminoglycoside uptake., Competing Interests: Conflict of interest David J. Beech is an inventor on the following patent applications: (1) PCT/GB2018/050369. TRPC ion channel inhibitors for use in therapy. Filing date: 9th February 2018. Inventors: David J. Beech, Richard J. Foster, Sin Ying Cheung and Baptiste M Rode; (2) 62/529,063. Englerin derivatives for the treatment of cancer. Filing date: 6th July 2017. Inventors: John A. Beutler, Antonio Echavarren, William Chain, David Beech, Zhenhua Wu, Jean-Simon Suppo, Fernando Bravo, and Hussein Rubaiy., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

4. Pharmacological Premature Termination Codon Readthrough of ABCB11 in Bile Salt Export Pump Deficiency: An In Vitro Study.

Author

Amzal R, Thébaut A, Lapalus M, Almes M, Grosse B, Mareux E, Collado-Hilly M, Davit-Spraul A, Bidou L, Namy O, Jacquemin E, and Gonzales E

Subjects

Animals, Cohort Studies, Dogs, Gentamicins pharmacology, HEK293 Cells, Hep G2 Cells, Humans, Madin Darby Canine Kidney Cells, Mice, NIH 3T3 Cells, Oxadiazoles pharmacology, Phenylbutyrates pharmacology, Signal Transduction drug effects, Transfection, Ursodeoxycholic Acid pharmacology, ATP Binding Cassette Transporter, Subfamily B, Member 11 genetics, ATP Binding Cassette Transporter, Subfamily B, Member 11 metabolism, Cholestasis, Intrahepatic genetics, Cholestasis, Intrahepatic metabolism, Codon, Nonsense drug effects

Abstract

Background and Aims: Progressive familial intrahepatic cholestasis type 2 (PFIC2) is a severe hepatocellular cholestasis due to biallelic mutations in ABCB11 encoding the canalicular bile salt export pump (BSEP). Nonsense mutations are responsible for the most severe phenotypes. The aim was to assess the ability of drugs to induce readthrough of six nonsense mutations (p.Y354X, p.R415X, p.R470X, p.R1057X, p.R1090X, and p.E1302X) identified in patients with PFIC2., Approach and Results: The ability of G418, gentamicin, and PTC124 to induce readthrough was studied using a dual gene reporter system in NIH3T3 cells. The ability of gentamicin to induce readthrough and to lead to the expression of a full-length protein was studied in human embryonic kidney 293 (HEK293), HepG2, and Can 10 cells using immunodetection assays. The function of the gentamicin-induced full-length protein was studied by measuring the [ 3 H]-taurocholate transcellular transport in stable Madin-Darby canine kidney clones co-expressing Na+-taurocholate co-transporting polypeptide (Ntcp). Combinations of gentamicin and chaperone drugs (ursodeoxycholic acid, 4-phenylbutyrate [4-PB]) were investigated. In NIH3T3, aminoglycosides significantly increased the readthrough level of all mutations studied, while PTC124 only slightly increased the readthrough of p.E1302X. Gentamicin induced a readthrough of p.R415X, p.R470X, p.R1057X, and p.R1090X in HEK293 cells. The resulting full-length proteins localized within the cytoplasm, except for Bsep R1090X , which was also detected at the plasma membrane of human embryonic kidney HEK293 and at the canalicular membrane of Can 10 and HepG2 cells. Additional treatment with 4-PB and ursodeoxycholic acid significantly increased the canalicular proportion of full-length Bsep R1090X protein in Can 10 cells. In Madin-Darby canine kidney clones, gentamicin induced a 40% increase of the Bsep R1090X [ 3 H]-taurocholate transport, which was further increased with additional 4-PB treatment., Conclusion: This study constitutes a proof of concept for readthrough therapy in selected patients with PFIC2 with nonsense mutations., (© 2021 by the American Association for the Study of Liver Diseases.)

Published

2021

5. Ataluren and aminoglycosides stimulate read-through of nonsense codons by orthogonal mechanisms.

Author

Ng MY, Li H, Ghelfi MD, Goldman YE, and Cooperman BS

Subjects

Aminoglycosides metabolism, Animals, Artemia genetics, Codon, Nonsense metabolism, Codon, Terminator drug effects, Codon, Terminator metabolism, Cystic Fibrosis genetics, Muscular Dystrophy, Duchenne genetics, Oxadiazoles metabolism, Protein Biosynthesis drug effects, Protein Synthesis Inhibitors, RNA, Transfer drug effects, RNA, Transfer genetics, RNA, Transfer metabolism, Ribosomes drug effects, Saccharomyces genetics, Aminoglycosides pharmacology, Codon, Nonsense drug effects, Oxadiazoles pharmacology, Peptide Chain Elongation, Translational drug effects

Abstract

During protein synthesis, nonsense mutations, resulting in premature stop codons (PSCs), produce truncated, inactive protein products. Such defective gene products give rise to many diseases, including cystic fibrosis, Duchenne muscular dystrophy (DMD), and some cancers. Small molecule nonsense suppressors, known as TRIDs (translational read-through-inducing drugs), stimulate stop codon read-through. The best characterized TRIDs are ataluren, which has been approved by the European Medicines Agency for the treatment of DMD, and G418, a structurally dissimilar aminoglycoside. Previously [1], we applied a highly purified in vitro eukaryotic translation system to demonstrate that both aminoglycosides like G418 and more hydrophobic molecules like ataluren stimulate read-through by direct interaction with the cell's protein synthesis machinery. Our results suggested that they might do so by different mechanisms. Here, we pursue this suggestion through a more-detailed investigation of ataluren and G418 effects on read-through. We find that ataluren stimulation of read-through derives exclusively from its ability to inhibit release factor activity. In contrast, G418 increases functional near-cognate tRNA mispairing with a PSC, resulting from binding to its tight site on the ribosome, with little if any effect on release factor activity. The low toxicity of ataluren suggests that development of new TRIDs exclusively directed toward inhibiting termination should be a priority in combatting PSC diseases. Our results also provide rate measurements of some of the elementary steps during the eukaryotic translation elongation cycle, allowing us to determine how these rates are modified when cognate tRNA is replaced by near-cognate tRNA ± TRIDs., Competing Interests: The authors declare no competing interest., (Copyright © 2021 the Author(s). Published by PNAS.)

Published

2021

6. Translational Read-Through Therapy of RPGR Nonsense Mutations.

Author

Vössing C, Owczarek-Lipska M, Nagel-Wolfrum K, Reiff C, Jüschke C, and Neidhardt J

Subjects

Case-Control Studies, Cells, Cultured, Cilia metabolism, Eye Proteins biosynthesis, Genetic Diseases, X-Linked metabolism, HEK293 Cells, Hemizygote, Humans, Mutant Proteins biosynthesis, Proof of Concept Study, Protein Biosynthesis drug effects, RNA Stability, Retinitis Pigmentosa metabolism, Codon, Nonsense drug effects, Eye Proteins genetics, Genetic Diseases, X-Linked drug therapy, Genetic Diseases, X-Linked genetics, Mutant Proteins genetics, Oxadiazoles therapeutic use, Retinitis Pigmentosa drug therapy, Retinitis Pigmentosa genetics

Abstract

X-chromosomal retinitis pigmentosa (RP) frequently is caused by mutations in the retinitis pigmentosa GTPase regulator ( RPGR ) gene. We evaluated the potential of PTC124 (Ataluren, Translama TM ) treatment to promote ribosomal read-through of premature termination codons (PTC) in RPGR . Expression constructs in HEK293T cells showed that the efficacy of read-through reagents is higher for UGA than UAA PTCs. We identified the novel hemizygous nonsense mutation c.1154T > A, p.Leu385* (NM_000328.3) causing a UAA PTC in RPGR and generated patient-derived fibroblasts. Immunocytochemistry of serum-starved control fibroblasts showed the RPGR protein in a dot-like expression pattern along the primary cilium. In contrast, RPGR was no longer detectable at the primary cilium in patient-derived cells. Applying PTC124 restored RPGR at the cilium in approximately 8% of patient-derived cells. RT-PCR and Western blot assays verified the pathogenic mechanisms underlying the nonsense variant. Immunofluorescence stainings confirmed the successful PTC124 treatment. Our results showed for the first time that PTC124 induces read-through of PTCs in RPGR and restores the localization of the RPGR protein at the primary cilium in patient-derived cells. These results may provide a promising new treatment option for patients suffering from nonsense mutations in RPGR or other genetic diseases.

Published

2020

7. A no-nonsense approach to hereditary kidney disease.

Author

Tokhmafshan F, Dickinson K, Akpa MM, Brasell E, Huertas P, and Goodyer PR

Subjects

Aminoglycosides pharmacokinetics, Anti-Bacterial Agents pharmacokinetics, Codon, Nonsense drug effects, Humans, Kidney Diseases genetics, Aminoglycosides therapeutic use, Anti-Bacterial Agents therapeutic use, Kidney Diseases drug therapy

Abstract

The advent of a new class of aminoglycosides with increased translational readthrough of nonsense mutations and reduced toxicity offers a new therapeutic strategy for a subset of patients with hereditary kidney disease. The renal uptake and retention of aminoglycosides at a high intracellular concentration makes the kidney an ideal target for this approach. In this review, we explore the potential of aminoglycoside readthrough therapy in a number of hereditary kidney diseases and discuss the therapeutic window of opportunity for subclasses of each disease, when caused by nonsense mutations.

Published

2020

8. Aminoglycosides can be a better choice over macrolides in COVID-19 regimen: Plausible mechanism for repurposing strategy.

Author

Chalichem NSS, Bethapudi B, and Mundkinajeddu D

Subjects

Aminoglycosides pharmacology, Antiviral Agents pharmacology, COVID-19 epidemiology, COVID-19 immunology, Codon, Nonsense drug effects, Defensins biosynthesis, Defensins physiology, Humans, Immunologic Factors pharmacology, Models, Genetic, Pandemics, SARS-CoV-2 physiology, Transcription, Genetic drug effects, Virus Internalization, Aminoglycosides therapeutic use, Antiviral Agents therapeutic use, Defensins genetics, Drug Repositioning, Immunity, Innate drug effects, Immunologic Factors therapeutic use, Macrolides therapeutic use, COVID-19 Drug Treatment

Abstract

In the current COVID-19 pandemic, prioritizing the immunity enhancers is equally important to anti-virals. Defensins are the forgotten molecules that enhance the innate immunity against various microbes. Although macrolides like azithromycin and clarithromycin etc., have been reported to act against respiratory infections but they lack the ability of immunity enhancement through defensins. The aminoglycosides were proved to have defensin mediated antiviral activity, that could enhance the immunity. So, Consideration of aminoglycosides can be a double edge sword viz., against respiratory infection as well as Immunity enhancer (along with anti-virals) for COVID-19 regimen., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

9. Targeting Nonsense: Optimization of 1,2,4-Oxadiazole TRIDs to Rescue CFTR Expression and Functionality in Cystic Fibrosis Cell Model Systems.

Author

Pibiri I, Melfi R, Tutone M, Di Leonardo A, Pace A, and Lentini L

Subjects

Cells, Cultured, Codon, Nonsense drug effects, Cystic Fibrosis genetics, Cystic Fibrosis metabolism, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Humans, Mutation, RNA, Messenger genetics, Codon, Nonsense genetics, Cystic Fibrosis drug therapy, Cystic Fibrosis Transmembrane Conductance Regulator metabolism, Gene Expression Regulation drug effects, Oxadiazoles pharmacology, Protein Biosynthesis, RNA, Messenger metabolism

Abstract

Cystic fibrosis (CF) patients develop a severe form of the disease when the cystic fibrosis transmembrane conductance regulator (CFTR) gene is affected by nonsense mutations. Nonsense mutations are responsible for the presence of a premature termination codon (PTC) in the mRNA, creating a lack of functional protein. In this context, translational readthrough-inducing drugs (TRIDs) represent a promising approach to correct the basic defect caused by PTCs. By using computational optimization and biological screening, we identified three new small molecules showing high readthrough activity. The activity of these compounds has been verified by evaluating CFTR expression and functionality after treatment with the selected molecules in cells expressing nonsense-CFTR-mRNA. Additionally, the channel functionality was measured by the halide sensitive yellow fluorescent protein (YFP) quenching assay. All three of the new TRIDs displayed high readthrough activity and low toxicity and can be considered for further evaluation as a therapeutic approach toward the second major cause of CF.

Published

2020

10. Functional rescue of c.3846G>A (W1282X) in patient-derived nasal cultures achieved by inhibition of nonsense mediated decay and protein modulators with complementary mechanisms of action.

Author

Laselva O, Eckford PD, Bartlett C, Ouyang H, Gunawardena TN, Gonska T, Moraes TJ, and Bear CE

Subjects

Cell Culture Techniques, Cystic Fibrosis genetics, Cystic Fibrosis Transmembrane Conductance Regulator metabolism, Humans, RNA, Messenger metabolism, Codon, Nonsense drug effects, Cystic Fibrosis pathology, Cystic Fibrosis Transmembrane Conductance Regulator drug effects, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Epithelial Cells drug effects, Nonsense Mediated mRNA Decay drug effects

Abstract

Background: The nonsense mutation, c.3846G>A (aka: W1282X-CFTR) leads to a truncated transcript that is susceptible to nonsense-mediated decay (NMD) and produces a shorter protein that is unstable and lacks normal channel activity in patient-derived tissues. However, if overexpressed in a heterologous expression system, the truncated mutant protein has been shown to mediate CFTR channel function following the addition of potentiators. In this study, we asked if a quadruple combination of small molecules that together inhibit nonsense mediated decay, stabilize both halves of the mutant protein and potentiate CFTR channel activity could rescue the functional expression of W1282X-CFTR in patient derived nasal cultures., Methods: We identified the CFTR domains stabilized by corrector compounds supplied from AbbVie using a fragment based, biochemical approach. Rescue of the channel function of W1282X.-CFTR protein by NMD inhibition and small molecule protein modulators was studied using a bronchial cell line engineered to express W1282X and in primary nasal epithelial cultures derived from four patients homozygous for this mutation., Results: We confirmed previous studies showing that inhibition of NMD using the inhibitor: SMG1i, led to an increased abundance of the shorter transcript in a bronchial cell line. Interestingly, on top of SMG1i, treatment with a combination of two new correctors developed by Galapagos/AbbVie (AC1 and AC2-2, separately targeting either the first or second half of CFTR and promoting assembly, significantly increased the potentiated channel activity by the mutant in the bronchial epithelial cell line and in patient-derived nasal epithelial cultures. The average rescue effect in primary cultures was approximately 50% of the regulated chloride conductance measured in non-CF cultures., Conclusions: These studies provide the first in-vitro evidence in patient derived airway cultures that the functional defects incurred by W1282X, has the potential to be effectively repaired pharmacologically., Competing Interests: Declaration of Competing Interest The authors declare no competing interests., (Copyright © 2019. Published by Elsevier B.V.)

Published

2020

11. Pharmacological approaches for targeting cystic fibrosis nonsense mutations.

Author

Sharma J, Keeling KM, and Rowe SM

Subjects

Animals, Codon, Nonsense genetics, Cystic Fibrosis genetics, Dose-Response Relationship, Drug, Humans, Molecular Structure, Mutation, Structure-Activity Relationship, Aminophenols pharmacology, Aminopyridines pharmacology, Benzodioxoles pharmacology, Codon, Nonsense drug effects, Cystic Fibrosis drug therapy, Indoles pharmacology, Pyrazoles pharmacology, Pyridines pharmacology, Pyrrolidines pharmacology, Quinolones pharmacology

Abstract

Cystic fibrosis (CF) is a monogenic autosomal recessive disorder. The clinical manifestations of the disease are caused by ∼2,000 mutations in the cystic fibrosis transmembrane conductance regulator (CFTR) protein. It is unlikely that any one approach will be efficient in correcting all defects. The recent approvals of ivacaftor, lumacaftor/ivacaftor and elexacaftor/tezacaftor/ivacaftor represent the genesis of a new era of precision combination medicine for the CF patient population. In this review, we discuss targeted translational readthrough approaches as mono and combination therapies for CFTR nonsense mutations. We examine the current status of efficacy of translational readthrough/nonsense suppression therapies and their limitations, including non-native amino acid incorporation at PTCs and nonsense-mediated mRNA decay (NMD), along with approaches to tackle these limitations. We further elaborate on combining various therapies such as readthrough agents, NMD inhibitors, and corrector/potentiators to improve the efficacy and safety of suppression therapy. These mutation specific strategies that are directed towards the basic CF defects should positively impact CF patients bearing nonsense mutations., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Masson SAS. All rights reserved.)

Published

2020

12. Aminoglycosides are efficient reagents to induce readthrough of premature termination codon in mutant B4GALNT1 genes found in families of hereditary spastic paraplegia.

Author

Yesmin F, Bhuiyan RH, Ohmi Y, Ohkawa Y, Tajima O, Okajima T, Furukawa K, and Furukawa K

Subjects

Animals, CHO Cells, Cells, Cultured, Codon, Nonsense genetics, Codon, Terminator genetics, Cricetulus, Mice, Mutation, Aminoglycosides pharmacology, Codon, Nonsense drug effects, Codon, Terminator drug effects, N-Acetylgalactosaminyltransferases genetics, Spastic Paraplegia, Hereditary genetics

Abstract

The readthrough of premature termination codon (PTC) by ribosome sometimes produces full-length proteins. We previously reported a readthrough of PTC of glycosyltransferase gene B4GALNT1 with hereditary spastic paraplegia (HSP). Here we featured the readthrough of B4GALNT1 of two mutants, M4 and M2 with PTC by immunoblotting and flow cytometry after transfection of B4GALNT1 cDNAs into cells. Immunoblotting showed a faint band of full-length mutant protein of M4 but not M2 at a similar position with that of wild-type B4GALNT1. AGC sequences at immediately before and after the PTC in M4 were critical for the readthrough. Treatment of cells transfected with mutant M4 cDNA with aminoglycosides resulted in increased readthrough of PTC. Furthermore, treatment of transfectants of mutant M2 cDNA with G418 also resulted in the induction of readthrough of PTC. Both M4 and M2 cDNA transfectants showed increased/induced bands in immunoblotting and GM2 expression in a dose-dependent manner of aminoglycosides. Results of mass spectrometry supported this effect. Here, we showed for the first time the induction and/or enhancement of the readthrough of PTCs of B4GALNT1 by aminoglycoside treatment, suggesting that aminoglycosides are efficient for patients with HSP caused by PTC of B4GALNT1, in which gradual neurological disorders emerged with aging., (© The Author(s) 2020. Published by Oxford University Press on behalf of the Japanese Biochemical Society. All rights reserved.)

Published

2020

13. Nonsense Suppression Therapy: New Hypothesis for the Treatment of Inherited Bone Marrow Failure Syndromes.

Author

Bezzerri V, Api M, Allegri M, Fabrizzi B, Corey SJ, and Cipolli M

Subjects

Aminoglycosides pharmacology, Congenital Bone Marrow Failure Syndromes genetics, Humans, Oxadiazoles pharmacology, Aminoglycosides therapeutic use, Codon, Nonsense drug effects, Congenital Bone Marrow Failure Syndromes therapy, Nonsense Mediated mRNA Decay drug effects, Oxadiazoles therapeutic use

Abstract

Inherited bone marrow failure syndromes (IBMFS) are a group of cancer-prone genetic diseases characterized by hypocellular bone marrow with impairment in one or more hematopoietic lineages. The pathogenesis of IBMFS involves mutations in several genes which encode for proteins involved in DNA repair, telomere biology and ribosome biogenesis. The classical IBMFS include Shwachman-Diamond syndrome (SDS), Diamond-Blackfan anemia (DBA), Fanconi anemia (FA), dyskeratosis congenita (DC), and severe congenital neutropenia (SCN). IBMFS are associated with high risk of myelodysplastic syndrome (MDS), acute myeloid leukemia (AML), and solid tumors. Unfortunately, no specific pharmacological therapies have been highly effective for IBMFS. Hematopoietic stem cell transplantation provides a cure for aplastic or myeloid neoplastic complications. However, it does not affect the risk of solid tumors. Since approximately 28% of FA, 24% of SCN, 21% of DBA, 20% of SDS, and 17% of DC patients harbor nonsense mutations in the respective IBMFS-related genes, we discuss the use of the nonsense suppression therapy in these diseases. We recently described the beneficial effect of ataluren, a nonsense suppressor drug, in SDS bone marrow hematopoietic cells ex vivo. A similar approach could be therefore designed for treating other IBMFS. In this review we explain in detail the new generation of nonsense suppressor molecules and their mechanistic roles. Furthermore, we will discuss strengths and limitations of these molecules which are emerging from preclinical and clinical studies. Finally we discuss the state-of-the-art of preclinical and clinical therapeutic studies carried out for IBMFS.

Published

2020

14. Suppression of Nonsense Mutations by New Emerging Technologies.

Author

Morais P, Adachi H, and Yu YT

Subjects

Clinical Trials as Topic, Genetic Predisposition to Disease, Humans, Nonsense Mediated mRNA Decay drug effects, Polymorphism, Single Nucleotide, Precision Medicine, RNA, Messenger drug effects, Small Molecule Libraries pharmacology, Codon, Nonsense drug effects, RNA, Messenger chemistry, Small Molecule Libraries therapeutic use

Abstract

Nonsense mutations often result from single nucleotide substitutions that change a sense codon (coding for an amino acid) to a nonsense or premature termination codon (PTC) within the coding region of a gene. The impact of nonsense mutations is two-fold: (1) the PTC-containing mRNA is degraded by a surveillance pathway called nonsense-mediated mRNA decay (NMD) and (2) protein translation stops prematurely at the PTC codon, and thus no functional full-length protein is produced. As such, nonsense mutations result in a large number of human diseases. Nonsense suppression is a strategy that aims to correct the defects of hundreds of genetic disorders and reverse disease phenotypes and conditions. While most clinical trials have been performed with small molecules, there is an increasing need for sequence-specific repair approaches that are safer and adaptable to personalized medicine. Here, we discuss recent advances in both conventional strategies as well as new technologies. Several of these will soon be tested in clinical trials as nonsense therapies, even if they still have some limitations and challenges to overcome.

Published

2020

15. 2,6-Diaminopurine as a highly potent corrector of UGA nonsense mutations.

Author

Trzaska C, Amand S, Bailly C, Leroy C, Marchand V, Duvernois-Berthet E, Saliou JM, Benhabiles H, Werkmeister E, Chassat T, Guilbert R, Hannebique D, Mouray A, Copin MC, Moreau PA, Adriaenssens E, Kulozik A, Westhof E, Tulasne D, Motorin Y, Rebuffat S, and Lejeune F

Subjects

Animals, Disease Models, Animal, Gene Expression Regulation, Neoplastic drug effects, Genes, p53 genetics, HEK293 Cells, HeLa Cells, Humans, Lepisma chemistry, Mice, Mice, Nude, RNA, Transfer genetics, tRNA Methyltransferases metabolism, 2-Aminopurine analogs & derivatives, 2-Aminopurine pharmacology, Codon, Nonsense drug effects, Drug Discovery, Drug Screening Assays, Antitumor, Mutation drug effects

Abstract

Nonsense mutations cause about 10% of genetic disease cases, and no treatments are available. Nonsense mutations can be corrected by molecules with nonsense mutation readthrough activity. An extract of the mushroom Lepista inversa has recently shown high-efficiency correction of UGA and UAA nonsense mutations. One active constituent of this extract is 2,6-diaminopurine (DAP). In Calu-6 cancer cells, in which TP53 gene has a UGA nonsense mutation, DAP treatment increases p53 level. It also decreases the growth of tumors arising from Calu-6 cells injected into immunodeficient nude mice. DAP acts by interfering with the activity of a tRNA-specific 2'-O-methyltransferase (FTSJ1) responsible for cytosine 34 modification in tRNA Trp . Low-toxicity and high-efficiency UGA nonsense mutation correction make DAP a good candidate for the development of treatments for genetic diseases caused by nonsense mutations.

Published

2020

16. Gentamicin induces COL17A1 nonsense mutation readthrough in junctional epidermolysis bullosa.

Author

Li Y, Shen J, Liang J, Zheng L, Chen F, Yao Z, and Li M

Subjects

Gentamicins pharmacology, Humans, Infant, Male, Protein Synthesis Inhibitors pharmacology, Collagen Type XVII, Autoantigens genetics, Codon, Nonsense drug effects, Epidermolysis Bullosa, Junctional genetics, Gentamicins therapeutic use, Non-Fibrillar Collagens genetics, Protein Synthesis Inhibitors therapeutic use

Published

2020

17. Use of PTC124 for nonsense suppression therapy targeting BMP4 nonsense variants in vitro and the bmp4st72 allele in zebrafish.

Author

Krall M, Htun S, and Slavotinek A

Subjects

Alleles, Animals, Genetic Therapy, HEK293 Cells, Humans, Suppression, Genetic drug effects, Transfection, Bone Morphogenetic Protein 4 genetics, Codon, Nonsense drug effects, Oxadiazoles pharmacology, Zebrafish genetics, Zebrafish Proteins genetics

Abstract

Nonsense suppression therapy (NST) utilizes compounds such as PTC124 (Ataluren) to induce translational read-through of stop variants by promoting the insertion of near cognate, aminoacyl tRNAs that yield functional proteins. We used NST with PTC124 to determine if we could successfully rescue nonsense variants in human Bone Morphogenetic Protein 4 (BMP4) in vitro and in a zebrafish bmp4 allele with a stop variant in vivo. We transfected 293T/17 cells with wildtype or mutant human BMP4 cDNA containing p.Arg198* and p.Glu213* and exposed cells to 0-20 μM PTC124. Treatment with 20 μM PTC124 produced a small, non-significant increase in BMP4 when targeting the p.Arg198* allele, but not the p.Glu213* allele, as measured with an In-cell ELISA assay. We then examined the ability of PTC124 to rescue the ventral tail fin defects associated with homozygosity for the p.Glu209* allele of bmp4 (bmp4st72/st72) in Danio rerio. We in-crossed bmp4st72/+ heterozygous fish and found a statistically significant increase in homozygous larvae without tail fin and ventroposterior defects, consistent with phenotypic rescue, after treatment of dechorionated larvae with 0.5 μM PTC124. We conclude that treatment with PTC124 can rescue bmp4 nonsense variants, but that the degree of rescue may depend on sequence specific factors and the amount of RNA transcript available for rescue. Our work also confirms that zebrafish show promise as a useful animal model for assessing the efficacy of PTC124 treatment on nonsense variants., Competing Interests: The authors have declared that no competing interests exist.

Published

2019

18. A mini-review and implementation model for using ataluren to treat nonsense mutation Duchenne muscular dystrophy.

Author

Landfeldt E, Sejersen T, and Tulinius M

Subjects

Clinical Trials as Topic, Codon, Nonsense drug effects, Cost-Benefit Analysis, Humans, Muscular Dystrophy, Duchenne genetics, Orphan Drug Production, Oxadiazoles economics, Oxadiazoles pharmacology, Sweden, Muscular Dystrophy, Duchenne drug therapy, Oxadiazoles therapeutic use

Abstract

Aim: Ataluren has been approved for treating nonsense mutation Duchenne muscular dystrophy (nmDMD), and there are currently discussions concerning drug access and applications beyond the development programme. This study provides an overview of nmDMD and ataluren, stipulates clinical rules for treatment initiation and discontinuation and proposes a model for the implementation of orphan drugs in clinical practice in Sweden., Methods: This was a targeted mini-review of the literature from 1995 to 2018, which included cohort studies, guidelines, randomised clinical trials, clinical commentaries and reviews. The review covered the pathophysiology, epidemiology and burden of nmDMD and the clinical programme for ataluren., Results: Based on the current evidence, and our experiences, we recommend that patients with nmDMD should be given ataluren as soon as possible after diagnosis and this treatment should continue until they reach a forced vital capacity of <30%, and, or, a score of at least six on the Brooke upper extremity scale. We propose an implementation model that comprises a coordinating specialist physician and a national expert committee responsible for providing clinical intelligence to ensure appropriate use., Conclusion: Our clinical recommendations and proposed implementation model will inform the optimum medical management of nmDMD in Sweden and help ensure timely, equal access to ataluren and similar orphan drugs., (©2018 Foundation Acta Paediatrica. Published by John Wiley & Sons Ltd.)

Published

2019

19. Carbamazepine reduces disease severity in a mouse model of metaphyseal chondrodysplasia type Schmid caused by a premature stop codon (Y632X) in the Col10a1 gene.

Author

Forouhan M, Sonntag S, and Boot-Handford RP

Subjects

Animals, Chondrocytes drug effects, Chondrocytes pathology, Codon, Nonsense drug effects, Disease Models, Animal, Endoplasmic Reticulum Stress drug effects, Growth Plate drug effects, Growth Plate growth & development, Growth Plate physiopathology, Heterozygote, Humans, Mice, Mutation, Osteochondrodysplasias genetics, Osteochondrodysplasias physiopathology, Severity of Illness Index, Unfolded Protein Response genetics, Carbamazepine administration & dosage, Codon, Nonsense genetics, Collagen Type X genetics, Osteochondrodysplasias drug therapy

Abstract

Mutations, mostly in the region of the COL10A1 gene encoding the C-terminal non-collagenous domain, cause the dwarfism metaphyseal chondrodysplasia type Schmid (MCDS). In most cases, the disease mechanism involves the misfolding of the mutant protein causing increased endoplasmic reticulum (ER) stress and an unfolded protein response (UPR). However, in an iliac crest biopsy, the COL10A1 p.Y632X mutation was found to produce instability of the mutant mRNA such that little mutant protein may be produced. To investigate the disease mechanism further, a gene-targeted mouse model of the Col10a1 p.Y632X mutation was generated. In this model, the mutant mRNA showed no instability, and in mice heterozygous for the mutation, mutant and wild-type mRNAs were present at equal concentrations. The protein was translated from the mutant allele and retained within the cell, triggering increased ER stress and a UPR. The mutation produced a relatively severe form of MCDS. Nevertheless, treatment of the mice with carbamazepine (CBZ), a drug which stimulates intracellular proteolysis and alleviates ER stress, effectively reduced the disease severity in this model of MCDS caused by a premature stop codon in the Col10a1 gene. Specifically, the drug reduced ER stress in the growth plate, restored growth plate architecture toward the wild-type state, significantly increased bone growth and within 2 weeks of treatment corrected the MCDS-induced hip distortion. These results indicate that CBZ is likely to be effective in ongoing clinical trials against all forms of MCDS whether caused by premature stop codons or substitutions.

Published

2018

20. Ataluren-driven restoration of Shwachman-Bodian-Diamond syndrome protein function in Shwachman-Diamond syndrome bone marrow cells.

Author

Bezzerri V, Bardelli D, Morini J, Vella A, Cesaro S, Sorio C, Biondi A, Danesino C, Farruggia P, Assael BM, D'amico G, and Cipolli M

Subjects

Apoptosis drug effects, Bone Marrow Diseases pathology, Cells, Cultured, Codon, Nonsense drug effects, Colony-Forming Units Assay, Exocrine Pancreatic Insufficiency pathology, Gene Expression Regulation drug effects, Humans, Lipomatosis pathology, Monocytes cytology, Monocytes drug effects, Phosphorylation drug effects, Protein Processing, Post-Translational drug effects, Shwachman-Diamond Syndrome, TOR Serine-Threonine Kinases metabolism, Bone Marrow Cells metabolism, Bone Marrow Diseases metabolism, Exocrine Pancreatic Insufficiency metabolism, Lipomatosis metabolism, Oxadiazoles pharmacology, Proteins genetics

Abstract

Shwachman-Diamond syndrome (SDS) is a rare inherited recessive disease mainly caused by mutations in the Shwachman-Bodian-Diamond syndrome (SBDS) gene, which encodes for the homonymous protein SBDS, whose function still remains to be fully established. SDS affects several organs causing bone marrow failure, exocrine pancreatic insufficiency, skeletal malformations, and cognitive disorders. About 15% of SDS patients develop myelodysplastic syndrome (MDS) and are at higher risk of developing acute myeloid leukemia (AML). Deficiency in SBDS expression has been associated with increased apoptosis and lack of myeloid differentiation in bone marrow hematopoietic progenitors. Importantly, most SDS patients carry nonsense mutations in SBDS. Since ataluren is a well-characterized small molecule inhibitor that can suppress nonsense mutations, here, we have assessed the efficacy of this drug in restoring SBDS expression in hematopoietic cells obtained from a cohort of SDS patients. Remarkably, we show that ataluren treatment readily restores SBDS protein expression in different cell types, particularly bone marrow stem cells. Furthermore, ataluren promotes myeloid differentiation in hematopoietic progenitors, reduces apoptotic rate in primary PBMCs, and brings mammalian target of rapamycin phosphorylation levels back to normal in both lymphoblasts and bone marrow mesenchymal stromal cells (BM-MSCs). Since a specific therapy against SDS is currently lacking, these results provide the rationale for ataluren repurposing clinical trials., (© 2018 Wiley Periodicals, Inc.)

Published

2018

21. Readthrough of ACTN3 577X nonsense mutation produces full-length α-actinin-3 protein.

Author

Harada N, Hatakeyama A, Okuyama M, Miyatake Y, Nakagawa T, Kuroda M, Masumoto S, Tsutsumi R, Nakaya Y, and Sakaue H

Subjects

Caffeine pharmacology, Gentamicins pharmacology, HEK293 Cells, Humans, Muscle, Skeletal metabolism, Peptide Chain Termination, Translational drug effects, RNA Stability, RNA, Messenger genetics, RNA, Messenger metabolism, Transfection, Actinin biosynthesis, Actinin genetics, Codon, Nonsense drug effects, Mutant Proteins biosynthesis, Mutant Proteins genetics

Abstract

The ACTN3 gene encodes α-actinin-3 protein, which stabilizes the contractile apparatus at the Z-line in skeletal muscle cell fast fibers. A nonsense mutation of the arginine (R) at the codon for amino acid 577 of the ACTN3 gene generates a premature termination codon (PTC) and produces the R577X polymorphism in humans (X specifies translational termination). The ACTN3 577X genotype abolishes α-actinin-3 protein production due to targeted degradation of the mutant transcript by the cellular nonsense-mediated mRNA decay (NMD) system, which requires mRNA splicing. In humans, α-actinin-3 deficiency can decrease sprinting and power performance as well as skeletal muscle mass and strength. Here we investigated whether suppression of the in-frame PTC induced by treatment with the aminoglycosides gentamicin and G418 that promote termination codon readthrough could allow production of full-length α-actinin-3 protein from ACTN3 577X. We constructed expression plasmids encoding mature mRNA that lacks introns or pre-mRNA, which carries introns for the ACTN3 577X gene (X and X pre , respectively) and transfected the constructs into HEK293 cells. Similar constructs for the ACTN3 577R gene were used as controls. HEK293 cells carrying the X gene, but not the X pre gene, expressed exogenous truncated α-actinin-3 protein, indicating NMD-mediated suppression of exogenous X pre expression. Cells treated with aminoglycosides produced exogenous full-length α-actinin-3 protein in X-transfected cells, but not in X pre -transfected cells. The NMD inhibitor caffeine prevented suppression of X pre expression and thereby induced production of full-length α-actinin-3 protein in the presence of aminoglycoside. Together these results indicate that the ACTN3 R577X polymorphism could be a novel target for readthrough therapy, which may affect athletic and muscle performance in humans., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

22. Amlexanox provides a potential therapy for nonsense mutations in the lysosomal storage disorder Aspartylglucosaminuria.

Author

Banning A, Schiff M, and Tikkanen R

Subjects

Amino Acid Substitution, Aminopyridines pharmacology, Cells, Cultured, Child, Female, HEK293 Cells, HeLa Cells, Humans, Lysosomal Storage Diseases drug therapy, Lysosomal Storage Diseases genetics, Mutation, Missense, Aminopyridines therapeutic use, Aspartylglucosaminuria drug therapy, Aspartylglucosaminuria genetics, Aspartylglucosylaminase genetics, Codon, Nonsense drug effects

Abstract

Aspartylglucosaminuria (AGU) is a lysosomal storage disorder caused by mutations in the gene for aspartylglucosaminidase (AGA). This enzyme participates in glycoprotein degradation in lysosomes. AGU results in progressive mental retardation, and no curative therapy is currently available. We have here characterized the consequences of AGA gene mutations in a compound heterozygous patient who exhibits a missense mutation producing a Ser72Pro substitution in one allele, and a nonsense mutation Trp168X in the other. Ser72 is not a catalytic residue, but is required for the stabilization of the active site conformation. Thus, Ser72Pro exchange impairs the autocatalytic activation of the AGA precursor, and results in a considerable reduction of the enzyme activity and in altered AGA precursor processing. Betaine, which can partially rescue the AGA activity in AGU patients carrying certain missense mutations, turned out to be ineffective in the case of Ser72Pro substitution. The Trp168X nonsense allele results in complete lack of AGA polypeptide due to nonsense-mediated decay (NMD) of the mRNA. Amlexanox, which inhibits NMD and causes a translational read-through, facilitated the synthesis of a full-length, functional AGA protein from the nonsense allele. This could be demonstrated as presence of the AGA polypeptide and increased enzyme activity upon Amlexanox treatment. Furthermore, in the Ser72Pro/Trp168X expressing cells, Amlexanox induced a synergistic increase in AGA activity and polypeptide processing due to enhanced processing of the Ser72Pro polypeptide. Our data show for the first time that Amlexanox might provide a valid therapy for AGU., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

23. Chemotherapeutics overcoming nonsense mutation-associated genetic diseases: medicinal chemistry of negamycin.

Author

Taguchi A, Hamada K, and Hayashi Y

Subjects

Amino Acids, Diamino chemical synthesis, Amino Acids, Diamino chemistry, Amino Acids, Diamino therapeutic use, Animals, Humans, Mice, Codon, Nonsense drug effects, Genetic Diseases, Inborn drug therapy, Genetic Diseases, Inborn genetics

Abstract

Nonsense mutations caused by the presence of an in-frame premature termination codon (PTC) account for ~10% of gene lesions that together cause over 1800 inherited human diseases. One approach to treating genetic diseases that stem from PTCs is selective promotion of translational readthrough in a PTC using 'readthrough compounds' that can lead to partial restoration of full-length functional protein expression. (+)-Negamycin, a natural dipeptide-like antibiotic, may restore some dystrophin expression in the skeletal muscles of mice with Duchenne muscular dystrophy, and this compound has been recognized as a potential therapeutic agent for diseases caused by nonsense mutations. In an effort to develop new candidate molecules with improved activities, we established the efficient total synthesis in eight steps of (+)-negamycin using both achiral and chiral starting material. These routes provided a deamino derivative with in vivo readthrough activity with potential for long-term treatment. In a separate approach, we discovered two natural negamycin analogs, 3-epi-deoxynegamycin and its leucine derivative, which are potent readthrough compounds effective against nonsense mutations of eukaryotes but not prokaryotes. These compounds fail to display antimicrobial activity. More potent derivatives, whose structure is derived from 3-epi-deoxynegamycin, were identified and their chemistry is discussed in this review.

Published

2018

24. The nucleoside analog clitocine is a potent and efficacious readthrough agent.

Author

Friesen WJ, Trotta CR, Tomizawa Y, Zhuo J, Johnson B, Sierra J, Roy B, Weetall M, Hedrick J, Sheedy J, Takasugi J, Moon YC, Babu S, Baiazitov R, Leszyk JD, Davis TW, Colacino JM, Peltz SW, and Welch EM

Subjects

Animals, Antimetabolites, Antineoplastic chemical synthesis, Antimetabolites, Antineoplastic metabolism, Apoptosis drug effects, Biomimetic Materials chemical synthesis, Biomimetic Materials metabolism, Cell Line, Tumor, Female, Furans chemical synthesis, Furans metabolism, Genes, Reporter, Humans, Luciferases genetics, Luciferases metabolism, Mice, Mice, Nude, Nucleosides chemical synthesis, Nucleosides metabolism, Ovarian Neoplasms genetics, Ovarian Neoplasms metabolism, Ovarian Neoplasms pathology, Protein Biosynthesis, Pyrimidine Nucleosides chemical synthesis, Pyrimidine Nucleosides metabolism, Signal Transduction, Transcriptional Activation, Tumor Burden drug effects, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Xenograft Model Antitumor Assays, Antimetabolites, Antineoplastic pharmacology, Biomimetic Materials pharmacology, Codon, Nonsense drug effects, Furans pharmacology, Nucleosides pharmacology, Ovarian Neoplasms drug therapy, Pyrimidine Nucleosides pharmacology, Tumor Suppressor Protein p53 agonists

Abstract

Nonsense mutations resulting in a premature stop codon in an open reading frame occur in critical tumor suppressor genes in a large number of the most common forms of cancers and are known to cause or contribute to the progression of disease. Low molecular weight compounds that induce readthrough of nonsense mutations offer a new means of treating patients with genetic disorders or cancers resulting from nonsense mutations. We have identified the nucleoside analog clitocine as a potent and efficacious suppressor of nonsense mutations. We determined that incorporation of clitocine into RNA during transcription is a prerequisite for its readthrough activity; the presence of clitocine in the third position of a premature stop codon directly induces readthrough. We demonstrate that clitocine can induce the production of p53 protein in cells harboring p53 nonsense-mutated alleles. In these cells, clitocine restored production of full-length and functional p53 as evidenced by induced transcriptional activation of downstream p53 target genes, progression of cells into apoptosis, and impeded growth of nonsense-containing human ovarian cancer tumors in xenograft tumor models. Thus, clitocine induces readthrough of nonsense mutations by a previously undescribed mechanism and represents a novel therapeutic modality to treat cancers and genetic diseases caused by nonsense mutations., (© 2017 Friesen et al.; Published by Cold Spring Harbor Laboratory Press for the RNA Society.)

Published

2017

25. Ataluren and similar compounds (specific therapies for premature termination codon class I mutations) for cystic fibrosis.

Author

Aslam AA, Higgins C, Sinha IP, and Southern KW

Subjects

Adolescent, Adult, Anti-Bacterial Agents therapeutic use, Child, Disease Progression, Female, Humans, Male, Middle Aged, Oxadiazoles adverse effects, Quality of Life, Randomized Controlled Trials as Topic, Tobramycin therapeutic use, Codon, Nonsense drug effects, Cystic Fibrosis drug therapy, Cystic Fibrosis genetics, Oxadiazoles therapeutic use

Abstract

Background: Cystic fibrosis is a common life-shortening genetic disorder in the Caucasian population (less common in other ethnic groups) caused by the mutation of a single gene that codes for the production of the cystic fibrosis transmembrane conductance regulator protein. This protein coordinates the transport of salt (and bicarbonate) across cell surfaces and the mutation most notably affects the airways. In the lungs of people with cystic fibrosis, defective protein results in a dehydrated surface liquid and compromised mucociliary clearance. The resulting thick mucus makes the airway prone to chronic infection and inflammation, which consequently damages the structure of the airways, eventually leading to respiratory failure. Additionally, abnormalities in the cystic fibrosis transmembrane conductance regulator protein lead to other systemic complications including malnutrition, diabetes and subfertility.Five classes of mutation have been described, depending on the impact of the mutation on the processing of the cystic fibrosis transmembrane conductance regulator protein in the cell. In class I mutations, the presence of premature termination codons prevents the production of any functional protein resulting in a severe cystic fibrosis phenotype. Advances in the understanding of the molecular genetics of cystic fibrosis has led to the development of novel mutation-specific therapies. Therapies targeting class I mutations (premature termination codons) aim to mask the abnormal gene sequence and enable the normal cellular mechanism to read through the mutation, potentially restoring the production of the cystic fibrosis transmembrane conductance regulator protein. This could in turn make salt transport in the cells function more normally and may decrease the chronic infection and inflammation that characterises lung disease in people with cystic fibrosis., Objectives: To evaluate the benefits and harms of ataluren and similar compounds on clinically important outcomes in people with cystic fibrosis with class I mutations (premature termination codons)., Search Methods: We searched the Cochrane Cystic Fibrosis Trials Register which is compiled from electronic database searches and handsearching of journals and conference abstract books. We also searched the reference lists of relevant articles. Last search of Group's register: 24 October 2016.We searched clinical trial registries maintained by the European Medicines Agency, the US National Institutes of Health and the WHO. Last search of clinical trials registries: 28 November 2016., Selection Criteria: Randomised controlled trials of parallel design comparing ataluren and similar compounds (specific therapies for class I mutations) with placebo in people with cystic fibrosis who have at least one class I mutation. Cross-over trials were reviewed individually to evaluate whether data from the first treatment arm could be included. We excluded trials that combined therapies for premature termination codon class I mutations with other mutation-specific therapies., Data Collection and Analysis: The authors independently assessed the risk of bias and extracted data from the included trial; they contacted trial authors for additional data., Main Results: Our searches identified 28 references to eight trials; five trials were excluded (three were cross-over and one was not randomised and one did not have relevant outcomes), one cross-over trial is awaiting classification pending provision of data and one trial is ongoing. The included parallel randomised controlled trial compared ataluren to placebo for a duration of 48 weeks in 238 participants (age range 6 to 53 years) with cystic fibrosis who had at least one nonsense mutation (a type of class I mutation).The quality of evidence and risk of bias assessments for the trial were moderate overall. Random sequence generation, allocation concealment and blinding of trial personnel were well-documented; participant blinding was less clear. Some participant data were excluded from the analysis. The trial was assessed as high risk of bias for selective outcome reporting, especially when reporting on the trial's post hoc subgroup of participants by chronic inhaled antibiotic use.The trial was sponsored by PTC Therapeutics Incorporated with grant support by the Cystic Fibrosis Foundation, the Food and Drug Administration's Office of Orphan Products Development and the National Institutes of Health (NIH).The trial reported no significant difference between treatment groups in quality of life, assessed by the Cystic Fibrosis Questionnaire-Revised respiratory domain score and no improvement in respiratory function measures (mean difference of relative change in forced expiratory volume at one second 2.97% (95% confidence interval -0.58 to 6.52)). Ataluren was associated with a significantly higher rate of episodes of renal impairment, risk ratio 17.70 (99% confidence interval 1.28 to 244.40). The trial reported no significant treatment effect for ataluren for the review's secondary outcomes: pulmonary exacerbation; computerised tomography score; weight; body mass index; and sweat chloride. No deaths were reported in the trial.A post hoc subgroup analysis of participants not receiving chronic inhaled tobramycin (n = 146) demonstrated favourable results for ataluren (n = 72) for relative change in % predicted forced expiratory volume at one second and pulmonary exacerbation rate. Participants receiving chronic inhaled tobramycin appeared to have a reduced rate of pulmonary exacerbation compared to those not receiving chronic inhaled tobramycin. This drug interaction was not anticipated and may affect the interpretation of the trial results., Authors' Conclusions: There is currently insufficient evidence to determine the effect of ataluren as a therapy for people with cystic fibrosis with class I mutations. Future trials should carefully assess for adverse events, notably renal impairment and consider the possibility of drug interactions. Cross-over trials should be avoided given the potential for the treatment to change the natural history of cystic fibrosis.

Published

2017

26. Therapeutic Suppression of Nonsense Mutation: An Emerging Target in Multiple Diseases and Thrombotic Disorders.

Author

Asiful Islam M, Alam F, Kamal MA, Gan SH, Wong KK, and Sasongko TH

Subjects

Humans, Codon, Nonsense drug effects, Codon, Nonsense genetics, Mutation drug effects, Suppression, Genetic drug effects, Thrombosis drug therapy, Thrombosis genetics

Abstract

Nonsense mutations contribute to approximately 10-30% of the total human inherited diseases via disruption of protein translation. If any of the three termination codons (UGA, UAG and UAA) emerges prematurely [known as premature termination codon (PTC)] before the natural canonical stop codon, truncated nonfunctional proteins or proteins with deleterious loss or gain-of-function activities are synthesized, followed by the development of nonsense mutation-mediated diseases. In the past decade, PTC-associated diseases captured much attention in biomedical research, especially as molecular therapeutic targets via nonsense suppression (i.e. translational readthrough) regimens. In this review, we highlighted different treatment strategies of PTC targeting readthrough therapeutics including the use of aminoglycosides, ataluren (formerly known as PTC124), suppressor tRNAs, nonsense-mediated mRNA decay, pseudouridylation and CRISPR/Cas9 system to treat PTC-mediated diseases. In addition, as thrombotic disorders are a group of disease with major burdens worldwide, 19 potential genes containing a total of 705 PTCs that cause 21 thrombotic disorders have been listed based on the data reanalysis from the 'GeneCards® - Human Gene Database' and 'Human Gene Mutation Database' (HGMD®). These PTC-containing genes can be potential targets amenable for different readthrough therapeutic strategies in the future., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.)

Published

2017

27. Discovery of Clinically Approved Agents That Promote Suppression of Cystic Fibrosis Transmembrane Conductance Regulator Nonsense Mutations.

Author

Mutyam V, Du M, Xue X, Keeling KM, White EL, Bostwick JR, Rasmussen L, Liu B, Mazur M, Hong JS, Falk Libby E, Liang F, Shang H, Mense M, Suto MJ, Bedwell DM, and Rowe SM

Subjects

Animals, Cell Line, Codon, Nonsense genetics, Cystic Fibrosis genetics, Cystic Fibrosis Transmembrane Conductance Regulator drug effects, Drug Evaluation, Preclinical methods, Humans, Luciferases metabolism, Rats, Inbred F344, Real-Time Polymerase Chain Reaction, Codon, Nonsense drug effects, Cystic Fibrosis drug therapy, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Drug Discovery methods

Abstract

Rationale: Premature termination codons (PTCs) in the cystic fibrosis transmembrane conductance regulator (CFTR) gene cause cystic fibrosis (CF). Several agents are known to suppress PTCs but are poorly efficacious or toxic., Objectives: To determine whether there are clinically available agents that elicit translational readthrough and improve CFTR function sufficient to confer therapeutic benefit to patients with CF with PTCs., Methods: Two independent screens, firefly luciferase and CFTR-mediated transepithelial chloride conductance assay, were performed on a library of 1,600 clinically approved compounds using fisher rat thyroid cells stably transfected with stop codons. Select agents were further evaluated using secondary screening assays including short circuit current analysis on primary cells from patients with CF. In addition, the effect of CFTR modulators (ivacaftor) was tested in combination with the most efficacious agents., Measurements and Main Results: From the primary screen, 48 agents were selected as potentially active. Following confirmatory tests in the transepithelial chloride conductance assay and prioritizing agents based on favorable pharmacologic properties, eight agents were advanced for secondary screening. Ivacaftor significantly increased short circuit current following forskolin stimulation in cells treated with pyranoradine tetraphosphate, potassium p-aminobenzoate, and escin as compared with vehicle control. Escin, an herbal agent, consistently induced readthrough activity as demonstrated by enhanced CFTR expression and function in vitro., Conclusions: Clinically approved drugs identified as potential readthrough agents, in combination with ivacaftor, may induce nonsense suppression to restore therapeutic levels of CFTR function. One or more agents may be suitable to advance to human testing.

Published

2016

28. Exploring the readthrough of nonsense mutations by non-acidic Ataluren analogues selected by ligand-based virtual screening.

Author

Pibiri I, Lentini L, Tutone M, Melfi R, Pace A, and Di Leonardo A

Subjects

Cystic Fibrosis Transmembrane Conductance Regulator genetics, Drug Evaluation, Preclinical, HeLa Cells, Humans, Molecular Conformation, Molecular Dynamics Simulation, Oxadiazoles chemistry, Oxadiazoles metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Codon, Nonsense drug effects, Oxadiazoles pharmacology

Abstract

Ataluren, also known as PTC124, is a 5-(fluorophenyl)-1,2,4-oxadiazolyl-benzoic acid suggested to suppress nonsense mutations by readthrough of premature stop codons in the mRNA. Potential interaction of PTC124 with mRNA has been recently studied by molecular dynamics simulations highlighting the importance of H-bonding and stacking π-π interactions. A series of non-acidic analogues of PTC124 were selected from a large database via a ligand-based virtual screening approach. Eight of them were synthesized and tested for their readthrough activity using the Fluc reporter harboring the UGA premature stop codon. The most active compound was further tested for suppression of the UGA nonsense mutation in the bronchial epithelial IB3.1 cell line carrying the W1282X mutation in the CFTR gene., (Copyright © 2016 Elsevier Masson SAS. All rights reserved.)

Published

2016

29. The functional mechanisms and clinical application of read-through drugs.

Author

Fu Y, Shu ZY, and Gu MM

Subjects

Aminoglycosides pharmacology, Aminoglycosides therapeutic use, Cystic Fibrosis drug therapy, Genetic Diseases, Inborn genetics, Humans, Muscular Dystrophy, Duchenne drug therapy, Oxadiazoles therapeutic use, Codon, Nonsense drug effects, Codon, Nonsense genetics

Abstract

According to previous reports, nearly one in 10 genetic diseases are caused by nonsense mutations around the world. Nonsense mutations lead to premature transcription terminations in cells, which in turn generate non-functional, truncated proteins. In recent years, read-through drugs are playing increasing prominent roles in the researches related to genetic diseases caused by nonsense mutations. However, due to the fact that the mechanisms lying behind translation termination still remain to be elucidated, the mechanistic research and clinical application of read-through drugs are facing new challenges. This review mainly discusses about the pathogenesis of genetic diseases caused by nonsense mutations, and then introduces the current clinical application of read-through drugs. Finally, we display some problems that remain to be solved and propose some possible coping strategies.

Published

2016

30. Targeting Nonsense Mutations in Diseases with Translational Read-Through-Inducing Drugs (TRIDs).

Author

Nagel-Wolfrum K, Möller F, Penner I, Baasov T, and Wolfrum U

Subjects

Animals, Genetic Diseases, Inborn genetics, Genetic Therapy methods, Genotype, Humans, RNA, Messenger genetics, Codon, Nonsense drug effects, Genetic Diseases, Inborn drug therapy, Pharmaceutical Preparations administration & dosage

Abstract

In recent years, remarkable advances in the ability to diagnose genetic disorders have been made. The identification of disease-causing genes allows the development of gene-specific therapies with the ultimate goal to develop personalized medicines for each patient according to their own specific genetic defect. In-depth genotyping of many different genes has revealed that ~12% of inherited genetic disorders are caused by in-frame nonsense mutations. Nonsense (non-coding) mutations are caused by point mutations, which generate premature termination codons (PTCs) that cause premature translational termination of the mRNA, and subsequently inhibit normal full-length protein expression. Recently, a gene-based therapeutic approach for genetic diseases caused by nonsense mutations has emerged, namely the so-called translational read-through (TR) therapy. Read-through therapy is based on the discovery that small molecules, known as TR-inducing drugs (TRIDs), allow the translation machinery to suppress a nonsense codon, elongate the nascent peptide chain, and consequently result in the synthesis of full-length protein. Several TRIDs are currently under investigation and research has been performed on several genetic disorders caused by nonsense mutations over the years. These findings have raised hope for the usage of TR therapy as a gene-based pharmacogenetic therapy for nonsense mutations in various genes responsible for a variety of genetic diseases.

Published

2016

31. Limited premature termination codon suppression by read-through agents in cystic fibrosis intestinal organoids.

Author

Zomer-van Ommen DD, Vijftigschild LA, Kruisselbrink E, Vonk AM, Dekkers JF, Janssens HM, de Winter-de Groot KM, van der Ent CK, and Beekman JM

Subjects

Cells, Cultured, Coccidiostats therapeutic use, Cystic Fibrosis genetics, Cystic Fibrosis metabolism, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Cystic Fibrosis Transmembrane Conductance Regulator metabolism, Humans, RNA genetics, Codon, Nonsense drug effects, Cystic Fibrosis drug therapy, Cystic Fibrosis Transmembrane Conductance Regulator drug effects, Gentamicins therapeutic use, Organoids cytology, Oxadiazoles therapeutic use

Abstract

Premature termination codon read-through drugs offer opportunities for treatment of multiple rare genetic diseases including cystic fibrosis. We here analyzed the read-through efficacy of PTC124 and G418 using human cystic fibrosis intestinal organoids (E60X/4015delATTT, E60X/F508del, G542X/F508del, R1162X/F508del, W1282X/F508del and F508del/F508del). G418-mediated read-through induced only limited CFTR function, but functional restoration of CFTR by PTC124 could not be confirmed. These studies suggest that better read-through agents are needed for robust treatment of nonsense mutations in cystic fibrosis., (Copyright © 2015 European Cystic Fibrosis Society. Published by Elsevier B.V. All rights reserved.)

Published

2016

32. Evaluation of Aminoglycoside and Non-Aminoglycoside Compounds for Stop-Codon Readthrough Therapy in Four Lysosomal Storage Diseases.

Author

Gómez-Grau M, Garrido E, Cozar M, Rodriguez-Sureda V, Domínguez C, Arenas C, Gatti RA, Cormand B, Grinberg D, and Vilageliu L

Subjects

Animals, COS Cells, Cell Line, Chlorocebus aethiops, Codon, Nonsense drug effects, Codon, Nonsense genetics, Codon, Terminator drug effects, Fibroblasts cytology, Humans, Lysosomes metabolism, Mucopolysaccharidosis III drug therapy, Mucopolysaccharidosis VI drug therapy, Niemann-Pick Disease, Type A drug therapy, Niemann-Pick Disease, Type A genetics, Niemann-Pick Disease, Type B drug therapy, Niemann-Pick Disease, Type B genetics, RNA, Messenger genetics, Codon, Terminator genetics, Gentamicins therapeutic use, Mucopolysaccharidosis III genetics, Mucopolysaccharidosis VI genetics

Abstract

Nonsense mutations are quite prevalent in inherited diseases. Readthrough drugs could provide a therapeutic option for any disease caused by this type of mutation. Geneticin (G418) and gentamicin were among the first to be described. Novel compounds have been generated, but only a few have shown improved results. PTC124 is the only compound to have reached clinical trials. Here we first investigated the readthrough effects of gentamicin on fibroblasts from one patient with Sanfilippo B, one with Sanfilippo C, and one with Maroteaux-Lamy. We found that ARSB activity (Maroteaux-Lamy case) resulted in an increase of 2-3 folds and that the amount of this enzyme within the lysosomes was also increased, after treatment. Since the other two cases (Sanfilippo B and Sanfilippo C) did not respond to gentamicin, the treatments were extended with the use of geneticin and five non-aminoglycoside (PTC124, RTC13, RTC14, BZ6 and BZ16) readthrough compounds (RTCs). No recovery was observed at the enzyme activity level. However, mRNA recovery was observed in both cases, nearly a two-fold increase for Sanfilippo B fibroblasts with G418 and around 1.5 fold increase for Sanfilippo C cells with RTC14 and PTC124. Afterwards, some of the products were assessed through in vitro analyses for seven mutations in genes responsible for those diseases and, also, for Niemann-Pick A/B. Using the coupled transcription/translation system (TNT), the best results were obtained for SMPD1 mutations with G418, reaching a 35% recovery at 0.25 μg/ml, for the p.W168X mutation. The use of COS cells transfected with mutant cDNAs gave positive results for most of the mutations with some of the drugs, although to a different extent. The higher enzyme activity recovery, of around two-fold increase, was found for gentamicin on the ARSB p.W146X mutation. Our results are promising and consistent with those of other groups. Further studies of novel compounds are necessary to find those with more consistent efficacy and fewer toxic effects.

Published

2015

33. [Duchenne muscular dystrophy].

Author

Meißner T

Subjects

Administration, Oral, Child, Preschool, Codon, Nonsense drug effects, Humans, Muscular Dystrophy, Duchenne genetics, Suspensions, Muscular Dystrophy, Duchenne drug therapy, Oxadiazoles therapeutic use

Published

2015

34. Readthrough of stop codons by use of aminoglycosides in cells from xeroderma pigmentosum group C patients.

Author

Kuschal C, Khan SG, Enk B, DiGiovanna JJ, and Kraemer KH

Subjects

Administration, Topical, Aminoglycosides administration & dosage, Cells, Cultured, DNA-Binding Proteins metabolism, Gene Expression drug effects, Gentamicins pharmacology, Humans, Mutant Proteins genetics, Mutant Proteins metabolism, Precision Medicine, RNA, Messenger genetics, RNA, Messenger metabolism, Xeroderma Pigmentosum metabolism, Aminoglycosides pharmacology, Codon, Nonsense drug effects, DNA-Binding Proteins genetics, Xeroderma Pigmentosum drug therapy, Xeroderma Pigmentosum genetics

Abstract

Readthrough of premature termination (stop) codons (PTC) is a new approach to treatment of genetic diseases. We recently reported that readthrough of PTC in cells from some xeroderma pigmentosum complementation group C (XP-C) patients could be achieved with the aminoglycosides geneticin or gentamicin. We found that the response depended on several factors including the PTC sequence, its location within the gene and the aminoglycoside used. Here, we extended these studies to investigate the effects of other aminoglycosides that are already on the market. We reasoned that topical treatment could deliver much higher concentrations of drug to the skin, the therapeutic target, and thus increase the therapeutic effect while reducing renal or ototoxicity in comparison with systemic treatment. Our prior clinical studies indicated that only a few percent of normal XPC expression was associated with mild clinical disease. We found minimal cell toxicity in the XP-C cells with several aminoglycosides. We found increased XPC mRNA expression in PTC-containing XP-C cells with G418, paromomycin, neomycin and kanamycin and increased XPC protein expression with G418. We conclude that in selected patients with XP, topical PTC therapy can be investigated as a method of personalized medicine to alleviate their cutaneous symptoms., (Published 2015. This article is a U.S. Government work and is in the public domain in the USA.)

Published

2015

35. Rapid identification and recovery of ENU-induced mutations with next-generation sequencing and Paired-End Low-Error analysis.

Author

Pan L, Shah AN, Phelps IG, Doherty D, Johnson EA, and Moens CB

Subjects

Animals, Codon, Nonsense drug effects, DNA analysis, DNA isolation & purification, Gene Library, Genomics standards, Male, Mutation drug effects, RNA Splice Sites genetics, Sequence Analysis, DNA, Spermatozoa metabolism, Zebrafish genetics, Zebrafish metabolism, Ethylnitrosourea toxicity, Genome drug effects, Genomics methods, High-Throughput Nucleotide Sequencing standards

Abstract

Background: Targeting Induced Local Lesions IN Genomes (TILLING) is a reverse genetics approach to directly identify point mutations in specific genes of interest in genomic DNA from a large chemically mutagenized population. Classical TILLING processes, based on enzymatic detection of mutations in heteroduplex PCR amplicons, are slow and labor intensive., Results: Here we describe a new TILLING strategy in zebrafish using direct next generation sequencing (NGS) of 250 bp amplicons followed by Paired-End Low-Error (PELE) sequence analysis. By pooling a genomic DNA library made from over 9,000 N-ethyl-N-nitrosourea (ENU) mutagenized F1 fish into 32 equal pools of 288 fish, each with a unique Illumina barcode, we reduce the complexity of the template to a level at which we can detect mutations that occur in a single heterozygous fish in the entire library. MiSeq sequencing generates 250 base-pair overlapping paired-end reads, and PELE analysis aligns the overlapping sequences to each other and filters out any imperfect matches, thereby eliminating variants introduced during the sequencing process. We find that this filtering step reduces the number of false positive calls 50-fold without loss of true variant calls. After PELE we were able to validate 61.5% of the mutant calls that occurred at a frequency between 1 mutant call:100 wildtype calls and 1 mutant call:1000 wildtype calls in a pool of 288 fish. We then use high-resolution melt analysis to identify the single heterozygous mutation carrier in the 288-fish pool in which the mutation was identified., Conclusions: Using this NGS-TILLING protocol we validated 28 nonsense or splice site mutations in 20 genes, at a two-fold higher efficiency than using traditional Cel1 screening. We conclude that this approach significantly increases screening efficiency and accuracy at reduced cost and can be applied in a wide range of organisms.

Published

2015

36. Molecular analysis, pathogenic mechanisms, and readthrough therapy on a large cohort of Kabuki syndrome patients.

Author

Micale L, Augello B, Maffeo C, Selicorni A, Zucchetti F, Fusco C, De Nittis P, Pellico MT, Mandriani B, Fischetto R, Boccone L, Silengo M, Biamino E, Perria C, Sotgiu S, Serra G, Lapi E, Neri M, Ferlini A, Cavaliere ML, Chiurazzi P, Monica MD, Scarano G, Faravelli F, Ferrari P, Mazzanti L, Pilotta A, Patricelli MG, Bedeschi MF, Benedicenti F, Prontera P, Toschi B, Salviati L, Melis D, Di Battista E, Vancini A, Garavelli L, Zelante L, and Merla G

Subjects

Abnormalities, Multiple drug therapy, Cell Line, Codon, Nonsense drug effects, Cohort Studies, DNA Mutational Analysis, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Gene Expression, Gene Expression Regulation drug effects, Genetic Association Studies, Gentamicins pharmacology, Gentamicins therapeutic use, Haploinsufficiency, Hematologic Diseases drug therapy, Histone Demethylases genetics, Homeodomain Proteins genetics, Humans, Mutation, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Nonsense Mediated mRNA Decay, Nuclear Proteins genetics, RNA Splice Sites, Sequence Analysis, DNA, Transcription, Genetic, Vestibular Diseases drug therapy, Abnormalities, Multiple genetics, Face abnormalities, Hematologic Diseases genetics, Vestibular Diseases genetics

Abstract

Kabuki syndrome (KS) is a multiple congenital anomalies syndrome characterized by characteristic facial features and varying degrees of mental retardation, caused by mutations in KMT2D/MLL2 and KDM6A/UTX genes. In this study, we performed a mutational screening on 303 Kabuki patients by direct sequencing, MLPA, and quantitative PCR identifying 133 KMT2D, 62 never described before, and four KDM6A mutations, three of them are novel. We found that a number of KMT2D truncating mutations result in mRNA degradation through the nonsense-mediated mRNA decay, contributing to protein haploinsufficiency. Furthermore, we demonstrated that the reduction of KMT2D protein level in patients' lymphoblastoid and skin fibroblast cell lines carrying KMT2D-truncating mutations affects the expression levels of known KMT2D target genes. Finally, we hypothesized that the KS patients may benefit from a readthrough therapy to restore physiological levels of KMT2D and KDM6A proteins. To assess this, we performed a proof-of-principle study on 14 KMT2D and two KDM6A nonsense mutations using specific compounds that mediate translational readthrough and thereby stimulate the re-expression of full-length functional proteins. Our experimental data showed that both KMT2D and KDM6A nonsense mutations displayed high levels of readthrough in response to gentamicin treatment, paving the way to further studies aimed at eventually treating some Kabuki patients with readthrough inducers., (© 2014 The Authors. *Human Mutation published by Wiley Periodicals, Inc.)

Published

2014

37. Synthetic aminoglycosides efficiently suppress cystic fibrosis transmembrane conductance regulator nonsense mutations and are enhanced by ivacaftor.

Author

Xue X, Mutyam V, Tang L, Biswas S, Du M, Jackson LA, Dai Y, Belakhov V, Shalev M, Chen F, Schacht J, J Bridges R, Baasov T, Hong J, Bedwell DM, and Rowe SM

Subjects

Aminoglycosides chemical synthesis, Aminoglycosides pharmacokinetics, Aminoglycosides toxicity, Aminophenols pharmacokinetics, Animals, Biological Transport, Cell Line, Chlorides metabolism, Cystic Fibrosis genetics, Cystic Fibrosis metabolism, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Cystic Fibrosis Transmembrane Conductance Regulator metabolism, Disease Models, Animal, Drug Synergism, Genes, Reporter, Humans, Luciferases genetics, Luciferases metabolism, Mice, Mice, Inbred CFTR, Mice, Transgenic, Organ of Corti drug effects, Organ of Corti pathology, Quinolones pharmacokinetics, Rats, Rats, Inbred F344, Time Factors, Transfection, Aminoglycosides pharmacology, Aminophenols pharmacology, Codon, Nonsense drug effects, Cystic Fibrosis drug therapy, Cystic Fibrosis Transmembrane Conductance Regulator drug effects, Quinolones pharmacology

Abstract

New drugs are needed to enhance premature termination codon (PTC) suppression to treat the underlying cause of cystic fibrosis (CF) and other diseases caused by nonsense mutations. We tested new synthetic aminoglycoside derivatives expressly developed for PTC suppression in a series of complementary CF models. Using a dual-luciferase reporter system containing the four most prevalent CF transmembrane conductance regulator (CFTR) nonsense mutations (G542X, R553X, R1162X, and W1282X) within their local sequence contexts (the three codons on either side of the PTC), we found that NB124 promoted the most readthrough of G542X, R1162X, and W1282X PTCs. NB124 also restored full-length CFTR expression and chloride transport in Fischer rat thyroid cells stably transduced with a CFTR-G542XcDNA transgene, and was superior to gentamicin and other aminoglycosides tested. NB124 restored CFTR function to roughly 7% of wild-type activity in primary human bronchial epithelial (HBE) CF cells (G542X/delF508), a highly relevant preclinical model with endogenous CFTR expression. Efficacy was further enhanced by addition of the CFTR potentiator, ivacaftor (VX-770), to airway cells expressing CFTR PTCs. NB124 treatment rescued CFTR function in a CF mouse model expressing a human CFTR-G542X transgene; efficacy was superior to gentamicin and exhibited favorable pharmacokinetic properties, suggesting that in vitro results translated to clinical benefit in vivo. NB124 was also less cytotoxic than gentamicin in a tissue-based model for ototoxicity. These results provide evidence that NB124 and other synthetic aminoglycosides provide a 10-fold improvement in therapeutic index over gentamicin and other first-generation aminoglycosides, providing a promising treatment for a wide array of CFTR nonsense mutations.

Published

2014

38. Therapeutics based on stop codon readthrough.

Author

Keeling KM, Xue X, Gunn G, and Bedwell DM

Subjects

Codon, Nonsense genetics, Genetic Diseases, Inborn drug therapy, Genetic Diseases, Inborn pathology, Humans, Nonsense Mediated mRNA Decay drug effects, Nonsense Mediated mRNA Decay genetics, Protein Biosynthesis drug effects, Protein Biosynthesis genetics, Codon, Nonsense drug effects, Genetic Diseases, Inborn genetics, Peptide Chain Termination, Translational

Abstract

Nonsense suppression therapy encompasses approaches aimed at suppressing translation termination at in-frame premature termination codons (PTCs, also known as nonsense mutations) to restore deficient protein function. In this review, we examine the current status of PTC suppression as a therapy for genetic diseases caused by nonsense mutations. We discuss what is currently known about the mechanism of PTC suppression as well as therapeutic approaches under development to suppress PTCs. The approaches considered include readthrough drugs, suppressor tRNAs, PTC pseudouridylation, and inhibition of nonsense-mediated mRNA decay. We also discuss the barriers that currently limit the clinical application of nonsense suppression therapy and suggest how some of these difficulties may be overcome. Finally, we consider how PTC suppression may play a role in the clinical treatment of genetic diseases caused by nonsense mutations.

Published

2014

39. Tobramycin is a suppressor of premature termination codons.

Author

Altamura N, Castaldo R, Finotti A, Breveglieri G, Salvatori F, Zuccato C, Gambari R, Panin GC, and Borgatti M

Subjects

Codon, Nonsense drug effects, Codon, Nonsense metabolism, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Genes, Reporter, Gentamicins pharmacology, Models, Genetic, Nonsense Mediated mRNA Decay genetics, Saccharomyces cerevisiae genetics, Suppression, Genetic genetics, Anti-Bacterial Agents pharmacology, Anti-Bacterial Agents therapeutic use, Codon, Nonsense genetics, Cystic Fibrosis drug therapy, Cystic Fibrosis genetics, Nonsense Mediated mRNA Decay drug effects, Suppression, Genetic drug effects, Tobramycin pharmacology, Tobramycin therapeutic use

Abstract

Premature translation terminations (PTCs) constitute the molecular basis of many genetic diseases, including cystic fibrosis, as they lead to the synthesis of truncated non-functional or partially functional protein. Suppression of translation terminations at PTCs (read-through) has been developed as a therapeutic strategy to restore full-length protein in several genetic diseases. Phenotypic consequences of PTCs can be exacerbated by the nonsense-mediated mRNA decay (NMD) pathway that detects and degrades mRNA containing PTC. Modulation of NMD, therefore, is also of interest as a potential target for the suppression therapy. Tobramycin is an aminoglycoside antibiotic, normally used to treat Pseudomonas aeruginosa pulmonary infection in CF patients. In the present study, by using yeast as a genetic system, we have examined the ability of Tobramycin to suppress PTCs as a function of the presence or absence of NMD. Results demonstrate that Tobramycin exhibits read-through ability on PTCs and preferentially in absence of NMD., (Copyright © 2013 European Cystic Fibrosis Society. Published by Elsevier B.V. All rights reserved.)

Published

2013

40. Muscular dystrophy: new challenges and review of the current clinical trials.

Author

Mercuri E and Muntoni F

Subjects

Adolescent, Child, Child, Preschool, Clinical Trials as Topic, Codon, Nonsense genetics, Female, Genetic Predisposition to Disease, Genetic Therapy, Humans, Infant, Male, Oligoribonucleotides, Antisense therapeutic use, Translational Research, Biomedical, Angiotensin-Converting Enzyme Inhibitors therapeutic use, Anti-Inflammatory Agents therapeutic use, Codon, Nonsense drug effects, Muscular Dystrophies drug therapy, Muscular Dystrophies genetics

Abstract

Purpose of Review: We provide a review of recent standards of care and therapeutic development in different forms of muscular dystrophies. This topic is relevant as the improved understanding of these disorders has not only led to a better definition of clinical course and to the development of standards of care for individual types of muscular dystrophies, but also culminated in different therapeutic approaches., Recent Findings: Recent natural history studies have demonstrated the impact of new standards of care in different forms of muscular dystrophies, and identified areas of clinical management in which further developments are needed. The majority of the experimental studies are focused on Duchenne muscular dystrophy. Some of them target patients with specific mutations, such as antisense oligonucleotides, to induce exon skipping of specific mutations or drugs developed to allow read-through of nonsense mutations, whereas other therapies deal with secondary aspects of muscle degeneration, aiming, for example, at reducing inflammation or apoptosis, and may also be suitable for other forms of muscular dystrophies., Summary: The advances in the field of muscular dystrophy have resulted in improved clinical course and survival. The encouraging results of early experimental studies could further improve these outcomes in the future.

Published

2013

41. New approach for fish breeding by chemical mutagenesis: establishment of TILLING method in fugu (Takifugu rubripes) with ENU mutagenesis.

Author

Kuroyanagi M, Katayama T, Imai T, Yamamoto Y, Chisada S, Yoshiura Y, Ushijima T, Matsushita T, Fujita M, Nozawa A, Suzuki Y, Kikuchi K, and Okamoto H

Subjects

Alleles, Animals, Codon, Nonsense drug effects, Codon, Nonsense genetics, Ethylnitrosourea administration & dosage, Female, Genome drug effects, Male, Breeding, Mutagenesis, Reverse Genetics, Takifugu genetics

Abstract

Background: In fish breeding, it is essential to discover and generate fish exhibiting an effective phenotype for the aquaculture industry, but screening for natural mutants by only depending on natural spontaneous mutations is limited. Presently, reverse genetics has become an important tool to generate mutants, which exhibit the phenotype caused by inactivation of a gene. TILLING (Targeting Induced Local Lesions IN Genomes) is a reverse genetics strategy that combines random chemical mutagenesis with high-throughput discovery technologies for screening the induced mutations in target genes. Although the chemical mutagenesis has been used widely in a variety of model species and also genetic breeding of microorganisms and crops, the application of the mutagenesis in fish breeding has been only rarely reported., Results: In this study, we developed the TILLING method in fugu with ENU mutagenesis and high-resolution melting (HRM) analysis to detect base pair changes in target sequences. Fugu males were treated 3 times at weekly intervals with various ENU concentrations, and then the collected sperm after the treatment was used to fertilize normal female for generating the mutagenized population (F1). The fertilization and the hatching ratios were similar to those of the control and did not reveal a dose dependency of ENU. Genomic DNA from the harvested F1 offspring was used for the HRM analysis. To obtain a fish exhibiting a useful phenotype (e.g. high meat production and rapid growth), fugu myostatin (Mstn) gene was examined as a target gene, because it has been clarified that the mstn deficient medaka exhibited double-muscle phenotype in common with MSTN knockout mice and bovine MSTN mutant. As a result, ten types of ENU-induced mutations were identified including a nonsense mutation in the investigated region with HRM analysis. In addition, the average mutation frequency in fugu Mstn gene was 1 mutant per 297 kb, which is similar to values calculated for zebrafish and medaka TILLING libraries., Conclusions: These results demonstrate that the TILLING method in fugu was established. We anticipate that this TILLING approach can be used to generate a wide range of mutant alleles, and be applicable to many farmed fish that can be chemically mutagenized.

Published

2013

42. In vitro read-through of phenylalanine hydroxylase (PAH) nonsense mutations using aminoglycosides: a potential therapy for phenylketonuria.

Author

Ho G, Reichardt J, and Christodoulou J

Subjects

Aminoglycosides genetics, Animals, COS Cells, Chlorocebus aethiops, Drug Evaluation, Preclinical, Genetic Therapy methods, HEK293 Cells, Humans, Phenylketonurias genetics, Phenylketonurias pathology, Aminoglycosides therapeutic use, Codon, Nonsense drug effects, Gentamicins therapeutic use, Oxadiazoles therapeutic use, Phenylalanine Hydroxylase genetics, Phenylketonurias drug therapy

Abstract

Phenylketonuria (PKU, OMIM 261600) is an autosomal recessive inborn error of phenylalanine metabolism, predominantly caused by mutations in the phenylalanine hydroxylase (PAH) gene. Approximately 10% of patients carry a nonsense mutation, which results in an inactive or unstable truncated protein. In some genetic disorders, including cystic fibrosis and Duchenne muscular dystrophy, restoration of full-length protein has been achieved by aminoglycoside antibiotics, such as gentamicin and G-418 (Geneticin). More recently, nonsense read-through has been induced at greater rates using a non-aminoglycoside drug, PTC124 (Ataluren), which has the advantage of being non-toxic in contrast to the antibiotics. The efficacy of read-through induced by three compounds, aminoglycosides G418 and gentamicin, and PTC124 were evaluated for four nonsense mutations of PAH in an in vitro expression system in two mammalian cell lines (COS-7 and HEK293). The production of full-length PAH was investigated using western blotting and the functionality confirmed by enzyme activity. Gentamicin and G-418 induced read-through of nonsense PAH mutations in HEK293 cells. The read-through product partially restored enzymatic activity, which was significantly less than that of wild-type, but comparable to a missense mutation of PAH associated with less severe forms of PKU. Treatment with PTC124 up to 100 μM did not result in full-length PAH polypeptide. Nonsense read-through drugs are a potential form of treatment for PKU, although the high dosage of aminoglycosides used is not appropriate in a clinical setting. In vitro studies with new non-toxic read-through agents as well as in vivo studies would also be essential to determine the extent of read-through required to restore normal phenylalanine levels.

Published

2013

43. Genetic variations in the active efflux pump genes acrA/B and tolC in different drug-induced strains of Escherichia coli CVCC 1547.

Author

Liu JH, Pan YS, Yuan L, Wu H, Hu GZ, and Chen YX

Subjects

Amikacin pharmacology, Ceftriaxone pharmacology, Ciprofloxacin pharmacology, Codon, Nonsense drug effects, Escherichia coli drug effects, Gene Expression Regulation, Bacterial, Mutation, Missense drug effects, Sequence Analysis, DNA, Bacterial Outer Membrane Proteins genetics, Drug Resistance, Multiple, Bacterial genetics, Escherichia coli Proteins genetics, Lipoproteins genetics, Membrane Transport Proteins genetics, Multidrug Resistance-Associated Proteins genetics

Abstract

This study aimed to investigate the properties of mutations of the active efflux pump genes acrA/B and tolC in Escherichia coli CVCC 1547 when induced by different drugs. The mutations were isolated in vitro by exposing E. coli CVCC 1547 to stepwise increases in the concentration of ceftriaxone (CRO), amikacin (AMK), or ciprofloxacin. The results showed that the minimum inhibitory concentrations for the corresponding drugs increased, as did the minimum inhibitory concentrations for other fluoroquinolones and β-lactam drugs that were not inducers. DNA sequence analyses of the acrA/B and tolC genes of the mutants and comparison with the parent strain revealed that genetic variations had occurred. Three point mutations resulted in amino acid changes in the proteins expressed. Specifically, strain CRO10 had a mutation in acrA, A309G, that resulted in a Thr-103 to Ala substitution, and a mutation in tolC, G735A, that changed Ala-245 to Thr; strain AMK20 (and AMK30) had a Val-447 to Ile amino acid change in acrB. In addition to the missense mutations in these strains, we detected 7, 20, and 15 nonsense mutations in acrA, acrB, and tolC, respectively. To sum up, multiple genetic sequence variations and some changes in amino acid sequences were detected when E. coli CVCC 1547 was challenged in vitro with CRO, AMK, or ciprofloxacin. These changes may have given rise to multidrug-resistant strains.

Published

2013

44. Ataluren: a 'no-nonsense' approach for pulmonary diseases.

Author

Loudon JA

Subjects

Genes, p53, Humans, Lung Diseases drug therapy, Lung Neoplasms drug therapy, Lung Neoplasms physiopathology, Oxadiazoles therapeutic use, Phenotype, Codon, Nonsense drug effects, Lung Diseases physiopathology, Oxadiazoles pharmacology

Published

2013

45. Development of generic immunoassay for the detection of a series of aminoglycosides with 6'-OH group for the treatment of genetic diseases in biological samples.

Author

Shalev M, Kandasamy J, Skalka N, Belakhov V, Rosin-Arbesfeld R, and Baasov T

Subjects

Aminoglycosides administration & dosage, Aminoglycosides blood, Aminoglycosides pharmacokinetics, Animals, Anti-Bacterial Agents administration & dosage, Anti-Bacterial Agents blood, Anti-Bacterial Agents pharmacokinetics, Antibody Affinity, Binding, Competitive, Calibration, Codon, Nonsense drug effects, Codon, Terminator drug effects, Cross Reactions, Enzyme-Linked Immunosorbent Assay, Genetic Diseases, Inborn drug therapy, Genetic Diseases, Inborn genetics, Genetic Diseases, Inborn metabolism, Haptens, Injections, Intraperitoneal, Limit of Detection, Male, Mice, Mice, Inbred C57BL, Reproducibility of Results, Aminoglycosides analysis, Anti-Bacterial Agents analysis, Drug Discovery methods

Abstract

Over the last two decades, a growing number of scientific evidences highlighted the potential therapeutic value of several structures of aminoglycoside antibiotics (including gentamicin and G418) for the treatment of various genetic diseases caused by nonsense mutations. These findings resulted in a fast evolvement of synthetic derivatives of aminoglycosides which were shown to be more target specific and less toxic than the clinically used antibiotics. The emerging progress in drug design and development has necessitated the urge to develop a fast, easy and accurate procedure for the determination of these potential therapeutic agents in various biologically derived matrices. Here we describe the preparation of a generic polyclonal antibody that was used for the development of homologous and heterologous immunoassays for the detection of a wide range of natural and synthetic aminoglycoside derivatives, highlighted today as potential therapeutic agents for the treatment of various genetic diseases. A common two-ring scaffold, NB82, present in the majority of compounds exhibiting potent biological activity, was used as a generic immunization hapten for the immunization of two rabbits. By using a series of chemical steps, NB82 was selectively conjugated via the N-1 position through glutaric acid linker to a carrier protein. Sensitivity (I₅₀) values for the recognition of three representative compounds NB82, NB84 and NB124 were determined to be 10 ± 3 ng mL⁻¹, 0.5 ± 0.04 μg mL⁻¹ and 1 ± 0.12 μg mL⁻¹, respectively. Limits of detection were determined to be 1 ± 0.3 ng mL⁻¹ for NB82, 20 ± 7 ng mL⁻¹ for NB84 and 15 ± 8 ng mL⁻¹ for NB124. The developed assays were further exploited for the in vivo monitoring of the therapeutic compounds in mice serum. Serum experimentations exhibited similar detection limits as observed for the PBS calibration experiments, demonstrating no interference with assays sensitivity, with rather high recovery ratios ranging from 92 to 107% in whole blood samples., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2013

46. Cell models for McArdle disease and aminoglycoside-induced read-through of a premature termination codon.

Author

Birch KE, Quinlivan RM, and Morris GE

Subjects

Animals, CHO Cells, Codon, Nonsense metabolism, Cricetinae, Cricetulus, Cytomegalovirus genetics, Disease Models, Animal, Female, Glycogen Storage Disease Type V metabolism, Green Fluorescent Proteins genetics, Green Fluorescent Proteins metabolism, Mutation, Missense genetics, Ovary cytology, Ovary drug effects, Ovary metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Transfection, Aminoglycosides pharmacology, Codon, Nonsense drug effects, Codon, Nonsense genetics, Glycogen Phosphorylase, Muscle Form genetics, Glycogen Storage Disease Type V genetics, Models, Biological, Models, Genetic, Mutation genetics

Abstract

McArdle disease results from mutations in the gene encoding muscle glycogen phosphorylase (PYGM) protein and the two most common mutations are a premature termination codon (R50X) and a missense mutation (G205S). Myoblasts from patients cannot be used to create a cell model of McArdle disease because even normal myoblasts produce little or no PYGM protein in cell culture. We therefore created cell models by expressing wild-type or mutant (R50X or G205S) PYGM from cDNA integrated into the genome of Chinese hamster ovary cells. These cell lines enable the study of McArdle mutations in the absence of nonsense-mediated decay of mRNA transcripts. Although all cell lines produced stable mRNA, only wild-type produced detectable PYGM protein. Our data suggest that the G205S mutation affects PYGM by causing misfolding and accelerated protein turnover. Using the N-terminal region of PYGM containing the R50X mutation fused to green fluorescent protein, we were able to demonstrate both small amounts of truncated protein production and read-through of the R50X premature termination codon induced by the aminoglycoside, G418., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2013

47. Suppression of hepcidin expression and iron overload mediate Salmonella susceptibility in ankyrin 1 ENU-induced mutant.

Author

Yuki KE, Eva MM, Richer E, Chung D, Paquet M, Cellier M, Canonne-Hergaux F, Vaulont S, Vidal SM, and Malo D

Subjects

Anemia, Hemolytic metabolism, Anemia, Hemolytic microbiology, Anemia, Hemolytic mortality, Animals, Ankyrins metabolism, Antimicrobial Cationic Peptides deficiency, Erythrocytes metabolism, Erythrocytes pathology, Erythropoietin genetics, Erythropoietin metabolism, Gene Expression, Genetic Predisposition to Disease, Growth Differentiation Factor 15 genetics, Growth Differentiation Factor 15 metabolism, Heme Oxygenase-1 genetics, Heme Oxygenase-1 metabolism, Hepcidins, Heterozygote, Homozygote, Iron metabolism, Iron Overload metabolism, Iron Overload microbiology, Iron Overload mortality, Liver metabolism, Liver pathology, Membrane Proteins genetics, Membrane Proteins metabolism, Mice, Salmonella Infections metabolism, Salmonella Infections microbiology, Salmonella Infections mortality, Salmonella typhimurium physiology, Survival Analysis, Anemia, Hemolytic genetics, Ankyrins genetics, Antimicrobial Cationic Peptides genetics, Codon, Nonsense drug effects, Ethylnitrosourea toxicity, Iron Overload genetics, Salmonella Infections genetics

Abstract

Salmonella, a ubiquitous Gram-negative intracellular bacterium, is a food borne pathogen that infects a broad range of hosts. Infection with Salmonella Typhimurium in mice is a broadly recognized experimental model resembling typhoid fever in humans. Using a N-ethyl-N-nitrosurea (ENU) mutagenesis recessive screen, we report the identification of Ity16 (Immunity to Typhimurium locus 16), a locus responsible for increased susceptibility to infection. The position of Ity16 was refined on chromosome 8 and a nonsense mutation was identified in the ankyrin 1 (Ank1) gene. ANK1 plays an important role in the formation and stabilization of the red cell cytoskeleton. The Ank1(Ity16/Ity16) mutation causes severe hemolytic anemia in uninfected mice resulting in splenomegaly, hyperbilirubinemia, jaundice, extramedullary erythropoiesis and iron overload in liver and kidneys. Ank1(Ity16/Ity16) mutant mice demonstrated low levels of hepcidin (Hamp) expression and significant increases in the expression of the growth differentiation factor 15 (Gdf15), erythropoietin (Epo) and heme oxygenase 1 (Hmox1) exacerbating extramedullary erythropoiesis, tissue iron deposition and splenomegaly. As the infection progresses in Ank1(Ity16/Ity16), the anemia worsens and bacterial load were high in liver and kidneys compared to wild type mice. Heterozygous Ank1(+/Ity16) mice were also more susceptible to Salmonella infection although to a lesser extent than Ank1(Ity16/Ity16) and they did not inherently present anemia and splenomegaly. During infection, iron accumulated in the kidneys of Ank1(+/Ity16) mice where bacterial loads were high compared to littermate controls. The critical role of HAMP in the host response to Salmonella infection was validated by showing increased susceptibility to infection in Hamp-deficient mice and significant survival benefits in Ank1(+/Ity16) heterozygous mice treated with HAMP peptide. This study illustrates that the regulation of Hamp and iron balance are crucial in the host response to Salmonella infection in Ank1 mutants.

Published

2013

48. Treatment of a methylmalonyl-CoA mutase stopcodon mutation.

Author

Buck NE, Wood LR, Hamilton NJ, Bennett MJ, and Peters HL

Subjects

Animals, Cell Line, Codon, Nonsense drug effects, Codon, Nonsense genetics, Codon, Terminator genetics, Disease Models, Animal, Fibroblasts drug effects, Fibroblasts enzymology, Humans, Methylmalonyl-CoA Mutase deficiency, Mice, Mice, Transgenic, Amino Acid Metabolism, Inborn Errors genetics, Codon, Terminator drug effects, Gentamicins pharmacology, Methylmalonyl-CoA Mutase genetics, Oxadiazoles pharmacology

Abstract

There are limited treatment options for the metabolic disorder methylmalonic aciduria. The disorder can be caused by nonsense mutations within the methylmalonyl-CoA mutase gene, resulting in the production of a truncated protein with little or no catalytic activity. We used a genomic reporter assay and mouse primary cell lines which carry a stop-codon mutation in the human methylmalonyl-CoA mutase gene to test the effects of gentamicin and PTC124 for stop-codon read-through potential. Fibroblast cell lines were established from methylmalonic aciduria knockout-stop codon mice. Addition of gentamicin to the culture medium caused a 1.5- to 2-fold increase in mRNA expression of the human methylmalonyl-CoA mutase gene. Without treatment the cells contained 19% of the normal levels of methylmalonyl-CoA mutase enzyme activity which increased to 32% with treatment, suggesting a functional improvement. Treatment with PTC124 increased the amount of human methylmalonyl-CoA mutase gene mRNA by 1.6±0.3-fold and a trend suggesting increased enzyme activity. The genomic reporter assay, BAC&#95;MMA(∗)EGFP, expresses enhanced green fluorescent protein when read-through of the stop codon occurs. Using flow cytometry, RT-real-time PCR and enzyme assay, read-through was measured. Treatment with PTC124 at 20μmol/L resulted in a significant increase in enhanced green fluorescent protein, a 2-fold increase in mRNA expression and a trend to a slight increase in enzyme activity. The clinical relevance of these effects may be tested in mouse models of MMA carrying nonsense mutations in the methylmalonyl-CoA mutase gene. Pharmacological approaches have the advantage of providing a broader effect on multiple tissues, which will benefit many different disorders with similar nonsense mutations., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

49. Pharmaceutical therapies to recode nonsense mutations in inherited diseases.

Author

Lee HL and Dougherty JP

Subjects

Aminoglycosides therapeutic use, Animals, Cystic Fibrosis drug therapy, Cystic Fibrosis genetics, Gene Expression Regulation, Genetic Diseases, Inborn genetics, Hemophilia A drug therapy, Hemophilia A genetics, Humans, Muscular Dystrophy, Duchenne drug therapy, Muscular Dystrophy, Duchenne genetics, RNA, Messenger analysis, Rett Syndrome drug therapy, Rett Syndrome genetics, Codon, Nonsense drug effects, Genetic Diseases, Inborn drug therapy

Abstract

Nonsense codons, generated from nonsense mutations or frameshifts, contribute significantly to the spectrum of inherited human diseases such as cystic fibrosis, Duchenne muscular dystrophy, hemophilia, spinal muscular atrophy, and many forms of cancer. The presence of a mutant nonsense codon results in premature termination to preclude the synthesis of a full-length protein and leads to aberrations in gene expression. Suppression therapy to recode a premature termination codon with an amino acid allowing readthrough to rescue the production of a full-length protein presents a promising strategy for treatment of patients suffering from debilitating nonsense-mediated disorders. Suppression therapy using aminoglycosides to promote readthrough in vitro have been known since the sixties. Recent progress in the field of recoding via pharmaceuticals has led to the continuous discovery and development of several pharmacological agents with nonsense suppression activities. Here, we review the mechanisms that are involved in discriminating normal versus premature termination codons, the factors involved in readthrough efficiency, the epidemiology of several well-known nonsense-mediated diseases, and the various pharmacological agents (aminoglycoside and non-aminoglycoside compounds) that are currently being employed in nonsense suppression therapy studies. We also discuss how these therapeutic agents can be used to regulate gene expression for gene therapy applications., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

50. Pharmacological therapies for muscular dystrophies.

Author

Abdel-Hamid H and Clemens PR

Subjects

Adrenal Cortex Hormones therapeutic use, Angiotensin II Type 1 Receptor Blockers therapeutic use, Angiotensin-Converting Enzyme Inhibitors therapeutic use, Animals, Anti-Arrhythmia Agents therapeutic use, Anti-Inflammatory Agents therapeutic use, Bone and Bones pathology, Codon, Nonsense drug effects, Humans, Mexiletine therapeutic use, Muscular Dystrophy, Duchenne drug therapy, Muscular Dystrophy, Facioscapulohumeral drug therapy, Myotonic Dystrophy drug therapy, Utrophin biosynthesis, Utrophin physiology, Muscular Dystrophies drug therapy

Abstract

Purpose of Review: The study reviews recent advances in pharmacological management of muscular dystrophies. Similarities and differences among the pathophysiology of different forms of muscular dystrophy lead to a broad array of approaches to provide new treatments., Recent Findings: In this review, we include only those muscular dystrophies for which advances have been published in the past year. This represents the 'advancing edge' of a large body of research over more than 20 years. This runs the gamut of new discoveries in symptomatic management to mutation-specific strategies that attempt to correct the root cause of the disorder., Summary: The field of pharmacological therapies for the muscular dystrophies continues to steadily advance. It is encouraging that research into new therapies is increasingly exploring pharmacological strategies with the potential to ameliorate disease pathology to a clinically significant degree.

Published

2012