Your search keyword '"Linda Popplewell"' showing total 84 results

1. Expression of the Pro-Fibrotic Marker Periostin in a Mouse Model of Duchenne Muscular Dystrophy

Author

Jessica Trundle, Viktorija Cernisova, Alexis Boulinguiez, Ngoc Lu-Nguyen, Alberto Malerba, and Linda Popplewell

Subjects

Duchenne muscular dystrophy, muscle pathology, periostin, fibrosis, Biology (General), QH301-705.5

Abstract

Duchenne muscular dystrophy (DMD) is characterised by fibrotic tissue deposition in skeletal muscle. We assessed the role of periostin in fibrosis using mdx mice, an established DMD murine model, for which we conducted a thorough examination of periostin expression over a year. RNA and protein levels in diaphragm (DIA) muscles were assessed and complemented by a detailed histological analysis at 5 months of age. In dystrophic DIAs, periostin (Postn) mRNA expression significantly exceeded that seen in wildtype controls at all timepoints analysed, with the highest expression at 5 months of age (p < 0.05). We found Postn to be more consistently highly expressed at the earlier timepoints compared to established markers of fibrosis like transforming growth factor-beta 1 (Tgf-β1) and connective tissue growth factor (Ctgf). Immunohistochemistry confirmed a significantly higher periostin protein expression in 5-month-old mdx mice compared to age-matched healthy controls (p < 0.01), coinciding with a significant fibrotic area percentage (p < 0.0001). RT-qPCR also indicated an elevated expression of Tgf-β1, Col1α1 (collagen type 1 alpha 1) and Ctgf in mdx DIAs compared to wild type controls (p < 0.05) at 8- and 12-month timepoints. Accordingly, immunoblot quantification demonstrated elevated periostin (3, 5 and 8 months, p < 0.01) and Tgf-β1 (8 and 12 months, p < 0.001) proteins in the mdx muscle. These findings collectively suggest that periostin expression is a valuable marker of fibrosis in this relevant model of DMD. They also suggest periostin as a potential contributor to fibrosis development, with an early onset of expression, thereby offering the potential for timely therapeutic intervention and its use as a biomarker in muscular dystrophies.

Published

2024

2. Targeted exon skipping of NF1 exon 17 as a therapeutic for neurofibromatosis type I

Author

André Leier, Marc Moore, Hui Liu, Michael Daniel, Alexis M. Hyde, Ludwine Messiaen, Bruce R. Korf, Jamuna Selvakumaran, Lukasz Ciszewski, Laura Lambert, Jeremy Foote, Margaret R. Wallace, Robert A. Kesterson, George Dickson, Linda Popplewell, and Deeann Wallis

Subjects

MT: Oligonucletides: Therapies and Applications, neurofibromatosis type I, Ras/Raf/MAPK pathway, exon skipping, antisense oligo therapeutics, animal models, Therapeutics. Pharmacology, RM1-950

Abstract

We investigated the feasibility of utilizing an exon-skipping approach as a genotype-dependent therapeutic for neurofibromatosis type 1 (NF1) by determining which NF1 exons might be skipped while maintaining neurofibromin protein expression and GTPase activating protein (GAP)-related domain (GRD) function. Initial in silico analysis predicted exons that can be skipped with minimal loss of neurofibromin function, which was confirmed by in vitro assessments utilizing an Nf1 cDNA-based functional screening system. Skipping of exons 17 or 52 fit our criteria, as minimal effects on protein expression and GRD activity were noted. Antisense phosphorodiamidate morpholino oligomers (PMOs) were utilized to skip exon 17 in human cell lines with patient-specific pathogenic variants in exon 17, c.1885G>A, and c.1929delG. PMOs restored functional neurofibromin expression. To determine the in vivo significance of exon 17 skipping, we generated a homozygous deletion of exon 17 in a novel mouse model. Mice were viable and exhibited a normal lifespan. Initial studies did not reveal the presence of tumor development; however, altered nesting behavior and systemic lymphoid hyperplasia was noted in peripheral lymphoid organs. Alterations in T and B cell frequencies in the thymus and spleen were identified. Hence, exon skipping should be further investigated as a therapeutic approach for NF1 patients with pathogenic variants in exon 17, as homozygous deletion of exon 17 is consistent with at least partial function of neurofibromin.

Published

2022

3. Optimized lentiviral vector to restore full-length dystrophin via a cell-mediated approach in a mouse model of Duchenne muscular dystrophy

Author

Jinhong Meng, Marc Moore, John Counsell, Francesco Muntoni, Linda Popplewell, and Jennifer Morgan

Subjects

lentivirus, Duchenne muscular dystrophy, native full-length dystrophin, sequence-optimized full-length dystrophin, myoblasts, muscle-specific promoter, Genetics, QH426-470, Cytology, QH573-671

Abstract

Duchenne muscular dystrophy (DMD) is a muscle wasting disorder caused by mutations in the DMD gene. Restoration of full-length dystrophin protein in skeletal muscle would have therapeutic benefit, but lentivirally mediated delivery of such a large gene in vivo has been hindered by lack of tissue specificity, limited transduction, and insufficient transgene expression. To address these problems, we developed a lentiviral vector, which contains a muscle-specific promoter and sequence-optimized full-length dystrophin, to constrain dystrophin expression to differentiated myotubes/myofibers and enhance the transgene expression. We further explored the efficiency of restoration of full-length dystrophin in vivo, by grafting DMD myoblasts that had been corrected by this optimized lentiviral vector intramuscularly into an immunodeficient DMD mouse model. We show that these lentivirally corrected DMD myoblasts effectively reconstituted full-length dystrophin expression in 93.58% ± 2.17% of the myotubes in vitro. Moreover, dystrophin was restored in 64.4% ± 2.87% of the donor-derived regenerated muscle fibers in vivo, which were able to recruit members of the dystrophin-glycoprotein complex at the sarcolemma. This study represents a significant advance over existing cell-mediated gene therapy strategies for DMD that aim to restore full-length dystrophin expression in skeletal muscle.

Published

2022

4. Novel Metabolomic Approach for Identifying Pathology-Specific Biomarkers in Rare Diseases: A Case Study in Oculopharyngeal Muscular Dystrophy (OPMD)

Author

Pradeep Harish, Alberto Malerba, Rosemarie H. M. J. M. Kroon, Milad Shademan, Baziel van Engelan, Vered Raz, Linda Popplewell, and Stuart G. Snowden

Subjects

biomarker, metabolomics, LC-MS, random forest, oculopharyngeal muscular dystrophy, Microbiology, QR1-502

Abstract

The identification of metabolomic biomarkers relies on the analysis of large cohorts of patients compared to healthy controls followed by the validation of markers in an independent sample set. Indeed, circulating biomarkers should be causally linked to pathology to ensure that changes in the marker precede changes in the disease. However, this approach becomes unfeasible in rare diseases due to the paucity of samples, necessitating the development of new methods for biomarker identification. The present study describes a novel approach that combines samples from both mouse models and human patients to identify biomarkers of OPMD. We initially identified a pathology-specific metabolic fingerprint in murine dystrophic muscle. This metabolic fingerprint was then translated into (paired) murine serum samples and then to human plasma samples. This study identified a panel of nine candidate biomarkers that could predict muscle pathology with a sensitivity of 74.3% and specificity of 100% in a random forest model. These findings demonstrate that the proposed approach can identify biomarkers with good predictive performance and a higher degree of confidence in their relevance to pathology than markers identified in a small cohort of human samples alone. Therefore, this approach has a high potential utility for identifying circulating biomarkers in rare diseases.

Published

2023

5. RAC1B modulates intestinal tumourigenesis via modulation of WNT and EGFR signalling pathways

Author

Victoria Gudiño, Sebastian Öther-Gee Pohl, Caroline V. Billard, Patrizia Cammareri, Alfonso Bolado, Stuart Aitken, David Stevenson, Adam E. Hall, Mark Agostino, John Cassidy, Colin Nixon, Alex von Kriegsheim, Paz Freile, Linda Popplewell, George Dickson, Laura Murphy, Ann Wheeler, Malcolm Dunlop, Farhat Din, Douglas Strathdee, Owen J. Sansom, and Kevin B. Myant

Subjects

Science

Abstract

RAC1 is a downstream target of the Wnt signaling that promotes intestinal stem cell expansion and tumorigenesis. Here, the authors identify the specific splice variant RAC1B as an important mediator of colorectal tumourigenesis and a potential target for enhancing the efficacy of EGFR inhibitor treatment.

Published

2021

6. The administration of antisense oligonucleotide golodirsen reduces pathological regeneration in patients with Duchenne muscular dystrophy

Author

Dominic Scaglioni, Francesco Catapano, Matthew Ellis, Silvia Torelli, Darren Chambers, Lucy Feng, Matthew Beck, Caroline Sewry, Mauro Monforte, Shawn Harriman, Erica Koenig, Jyoti Malhotra, Linda Popplewell, Michela Guglieri, Volker Straub, Eugenio Mercuri, Laurent Servais, Rahul Phadke, Jennifer Morgan, and Francesco Muntoni

Subjects

Dystrophin, Muscular dystrophy, Immunofluorescence, Genetic therapies, Golodirsen, Clinical trial, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract During the last decade, multiple clinical trials for Duchenne muscular dystrophy (DMD) have focused on the induction of dystrophin expression using different strategies. Many of these trials have reported a clear increase in dystrophin protein following treatment. However, the low levels of the induced dystrophin protein have raised questions on its functionality. In our present study, using an unbiased, high-throughput digital image analysis platform, we assessed markers of regeneration and levels of dystrophin associated protein via immunofluorescent analysis of whole muscle sections in 25 DMD boys who received 48-weeks treatment with exon 53 skipping morpholino antisense oligonucleotide (PMO) golodirsen. We demonstrate that the de novo dystrophin induced by exon skipping with PMO golodirsen is capable of conferring a histological benefit in treated patients with an increase in dystrophin associated proteins at the dystrophin positive regions of the sarcolemma in post-treatment biopsies. Although 48 weeks treatment with golodirsen did not result in a significant change in the levels of fetal/developmental myosins for the entire cohort, there was a significant negative correlation between the amount of dystrophin and levels of regeneration observed in different biopsy samples. Our results provide, for the first time, evidence of functionality of induced dystrophin following successful therapeutic intervention in the human.

Published

2021

7. Mutation-Directed Therapeutics for Neurofibromatosis Type I

Author

Andre Leier, David M. Bedwell, Ann T. Chen, George Dickson, Kim M. Keeling, Robert A. Kesterson, Bruce R. Korf, Tatiana T. Marquez Lago, Ulrich F. Müller, Linda Popplewell, Jiangbing Zhou, and Deeann Wallis

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Significant advances in biotechnology have led to the development of a number of different mutation-directed therapies. Some of these techniques have matured to a level that has allowed testing in clinical trials, but few have made it to approval by drug-regulatory bodies for the treatment of specific diseases. While there are still various hurdles to be overcome, recent success stories have proven the potential power of mutation-directed therapies and have fueled the hope of finding therapeutics for other genetic disorders. In this review, we summarize the state-of-the-art of various therapeutic approaches and assess their applicability to the genetic disorder neurofibromatosis type I (NF1). NF1 is caused by the loss of function of neurofibromin, a tumor suppressor and downregulator of the Ras signaling pathway. The condition is characterized by a variety of phenotypes and includes symptoms such as skin spots, nervous system tumors, skeletal dysplasia, and others. Hence, depending on the patient, therapeutics may need to target different tissues and cell types. While we also discuss the delivery of therapeutics, in particular via viral vectors and nanoparticles, our main focus is on therapeutic techniques that reconstitute functional neurofibromin, most notably cDNA replacement, CRISPR-based DNA repair, RNA repair, antisense oligonucleotide therapeutics including exon skipping, and nonsense suppression.

Published

2020

8. Inhibition of myostatin improves muscle atrophy in oculopharyngeal muscular dystrophy (OPMD)

Author

Pradeep Harish, Alberto Malerba, Ngoc Lu‐Nguyen, Leysa Forrest, Ornella Cappellari, Fanny Roth, Capucine Trollet, Linda Popplewell, and George Dickson

Subjects

Anti‐myostatin antibody, RK35, OPMD, Muscle atrophy, Diseases of the musculoskeletal system, RC925-935, Human anatomy, QM1-695

Abstract

Abstract Background Oculopharyngeal muscular dystrophy (OPMD) is a late‐onset muscle disease affecting one per 80 000 of the general population characterized by profound dysphagia and ptosis, and limb weakness at later stages. Affected muscles are characterized by increased fibrosis and atrophy. Myostatin is a negative regulator of muscle mass, and inhibition of myostatin has been demonstrated to ameliorate symptoms in dystrophic muscles. Methods In this study, we performed a systemic delivery of a monoclonal antibody to immunologically block myostatin in the A17 mouse model of OPMD. The mice were administered a weekly dose of 10 mg/kg RK35 intraperitonially for 10 weeks, following which histological analyses were performed on the samples. Results This treatment significantly (P < 0.01) improved body mass (11%) and muscle mass (for the tibialis anterior and extensor digitorum longus by 19% and 41%) in the A17 mice treated with RK35 when compared to saline controls. Similarly, a significantly (P < 0.01) increased muscle strength (18% increase in maximal tetanic force) and myofibre diameter (17% and 44% for the tibialis anterior and extensor digitorum longus), and reduced expression of markers of muscle fibrosis (40% reduction in area of expression), was also observed. No change in the density of intranuclear inclusions (a hallmark of disease progression of OPMD) was however observed. Conclusions Our study supports the clinical translation of such antibody‐mediated inhibition of myostatin as a treatment of OPMD. This strategy has implications to be used as adjuvant therapies with gene therapy based approaches, or to stabilize the muscle prior to myoblast transplantation.

Published

2019

9. Long-Term Systemic Treatment of a Mouse Model Displaying Chronic FSHD-like Pathology with Antisense Therapeutics That Inhibit DUX4 Expression

Author

Ngoc Lu-Nguyen, George Dickson, Alberto Malerba, and Linda Popplewell

Subjects

FSHD, DUX4 inhibition, systemic antisense therapy, ACTA1-MCM/FLExDUX4, Biology (General), QH301-705.5

Abstract

Silencing the expression of the double homeobox 4 (DUX4) gene offers great potential for the treatment of facioscapulohumeral muscular dystrophy (FSHD). Several research groups have recently reported promising results using systemic antisense therapy in a transgenic small animal model of FSHD, the ACTA1-MCM/FLExDUX4 mouse model. However, the treatment was applied in non-DUX4-induced mice or shortly after DUX4 activation, which resulted in conditions that do not correctly represent the situation in a clinic. Here, we generated progressive FSHD-like pathology in ACTA1-MCM/FLExDUX4 mice and then treated the animals with vivoPMO-PACS4, an antisense compound that efficiently downregulates DUX4. To best mimic the translation of this treatment in clinical settings, the systemic antisense oligonucleotide administration was delayed to 3 weeks after the DUX4 activation so that the pathology was established at the time of the treatment. The chronic administration of vivoPMO-PACS4 for 8 weeks downregulated the DUX4 expression by 60%. Consequently, the treated mice showed an increase by 18% in body-wide muscle mass and 32% in muscle strength, and a reduction in both myofiber central nucleation and muscle fibrosis by up to 29% and 37%, respectively. Our results in a more suitable model of FSHD pathology confirm the efficacy of vivoPMO-PACS4 administration, and highlight the significant benefit provided by the long-term treatment of the disease.

Published

2022

10. Inhibition of Myostatin Reduces Collagen Deposition in a Mouse Model of Oculopharyngeal Muscular Dystrophy (OPMD) With Established Disease

Author

Pradeep Harish, Leysa Forrest, Shanti Herath, George Dickson, Alberto Malerba, and Linda Popplewell

Subjects

OPMD, myostatin, antibody, RK35, muscular dystrophy, Physiology, QP1-981

Abstract

BackgroundOculopharyngeal muscular dystrophy (OPMD) is a late-onset muscle disease presented by ptosis, dysphagia, and limb weakness. Affected muscles display increased fibrosis and atrophy, with characteristic inclusion bodies in the nucleus. Myostatin is a negative regulator of muscle mass, and inhibition of myostatin has been demonstrated to improve symptoms in models of muscular dystrophy.MethodsWe systemically administered a monoclonal antibody to block myostatin in the A17 mouse model of OPMD at 42 weeks of age. The mice were administered a weekly dose of 10 mg/kg RK35 intraperitonially for 10 weeks, following which serum and histological analyses were performed on muscle samples.ResultsThe administration of the antibody resulted in a significant decrease in serum myostatin and collagen deposition in muscles. However, minimal effects on body mass, muscle mass and myofiber diameter, or the density of intranuclear inclusions (INIs) (a hallmark of disease progression of OPMD) were observed.ConclusionThis study demonstrates that inhibition of myostatin does not revert muscle atrophy in a mouse model with established OPMD disease, but is effective at reducing observed histological markers of fibrosis in the treated muscles.

Published

2020

11. Reversible immortalisation enables genetic correction of human muscle progenitors and engineering of next‐generation human artificial chromosomes for Duchenne muscular dystrophy

Author

Sara Benedetti, Narumi Uno, Hidetoshi Hoshiya, Martina Ragazzi, Giulia Ferrari, Yasuhiro Kazuki, Louise Anne Moyle, Rossana Tonlorenzi, Angelo Lombardo, Soraya Chaouch, Vincent Mouly, Marc Moore, Linda Popplewell, Kanako Kazuki, Motonobu Katoh, Luigi Naldini, George Dickson, Graziella Messina, Mitsuo Oshimura, Giulio Cossu, and Francesco Saverio Tedesco

Subjects

DMD, gene therapy, human artificial chromosomes, human muscle stem/progenitor cells, immortalisation, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Transferring large or multiple genes into primary human stem/progenitor cells is challenged by restrictions in vector capacity, and this hurdle limits the success of gene therapy. A paradigm is Duchenne muscular dystrophy (DMD), an incurable disorder caused by mutations in the largest human gene: dystrophin. The combination of large‐capacity vectors, such as human artificial chromosomes (HACs), with stem/progenitor cells may overcome this limitation. We previously reported amelioration of the dystrophic phenotype in mice transplanted with murine muscle progenitors containing a HAC with the entire dystrophin locus (DYS‐HAC). However, translation of this strategy to human muscle progenitors requires extension of their proliferative potential to withstand clonal cell expansion after HAC transfer. Here, we show that reversible cell immortalisation mediated by lentivirally delivered excisable hTERT and Bmi1 transgenes extended cell proliferation, enabling transfer of a novel DYS‐HAC into DMD satellite cell‐derived myoblasts and perivascular cell‐derived mesoangioblasts. Genetically corrected cells maintained a stable karyotype, did not undergo tumorigenic transformation and retained their migration ability. Cells remained myogenic in vitro (spontaneously or upon MyoD induction) and engrafted murine skeletal muscle upon transplantation. Finally, we combined the aforementioned functions into a next‐generation HAC capable of delivering reversible immortalisation, complete genetic correction, additional dystrophin expression, inducible differentiation and controllable cell death. This work establishes a novel platform for complex gene transfer into clinically relevant human muscle progenitors for DMD gene therapy.

Published

2017

12. Systemic Antisense Therapeutics for Dystrophin and Myostatin Exon Splice Modulation Improve Muscle Pathology of Adult mdx Mice

Author

Ngoc Lu-Nguyen, Alberto Malerba, Linda Popplewell, Fred Schnell, Gunnar Hanson, and George Dickson

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Antisense-mediated exon skipping is a promising approach for the treatment of Duchenne muscular dystrophy (DMD), a rare life-threatening genetic disease due to dystrophin deficiency. Such an approach can restore the disrupted reading frame of dystrophin pre-mRNA, generating a truncated form of the protein. Alternatively, antisense therapy can be used to induce destructive exon skipping of myostatin pre-mRNA, knocking down myostatin expression to enhance muscle strength and reduce fibrosis. We have reported previously that intramuscular or intraperitoneal antisense administration inducing dual exon skipping of dystrophin and myostatin pre-mRNAs was beneficial in mdx mice, a mouse model of DMD, although therapeutic effects were muscle type restricted, possibly due to the delivery routes used. Here, following systemic intravascular antisense treatment, muscle strength and body activity of treated adult mdx mice increased to the levels of healthy controls. Importantly, hallmarks of muscular dystrophy were greatly improved in mice receiving the combined exon-skipping therapy, as compared to those receiving dystrophin antisense therapy alone. Our results support the translation of antisense therapy for dystrophin restoration and myostatin inhibition into the clinical setting for DMD. Keywords: antisense oligonucleotides, Duchenne muscular dystrophy, dystrophin, exon skipping, myostatin

Published

2017

13. A multicenter comparison of quantification methods for antisense oligonucleotide-induced DMD exon 51 skipping in Duchenne muscular dystrophy cell cultures.

Author

Monika Hiller, Maria Sofia Falzarano, Iker Garcia-Jimenez, Valentina Sardone, Ruurd C Verheul, Linda Popplewell, Karen Anthony, Estibaliz Ruiz-Del-Yerro, Hana Osman, Jelle J Goeman, Kamel Mamchaoui, George Dickson, Alessandra Ferlini, Francesco Muntoni, Annemieke Aartsma-Rus, Virginia Arechavala-Gomeza, Nicole A Datson, and Pietro Spitali

Subjects

Medicine, Science

Abstract

BACKGROUND:Duchenne muscular dystrophy is a lethal disease caused by lack of dystrophin. Skipping of exons adjacent to out-of-frame deletions has proven to restore dystrophin expression in Duchenne patients. Exon 51 has been the most studied target in both preclinical and clinical settings and the availability of standardized procedures to quantify exon skipping would be advantageous for the evaluation of preclinical and clinical data. OBJECTIVE:To compare methods currently used to quantify antisense oligonucleotide-induced exon 51 skipping in the DMD transcript and to provide guidance about the method to use. METHODS:Six laboratories shared blinded RNA samples from Duchenne patient-derived muscle cells treated with different amounts of exon 51 targeting antisense oligonucleotide. Exon 51 skipping levels were quantified using five different techniques: digital droplet PCR, single PCR assessed with Agilent bioanalyzer, nested PCR with agarose gel image analysis by either ImageJ or GeneTools software and quantitative real-time PCR. RESULTS:Differences in mean exon skipping levels and dispersion around the mean were observed across the different techniques. Results obtained by digital droplet PCR were reproducible and showed the smallest dispersion. Exon skipping quantification with the other methods showed overestimation of exon skipping or high data variation. CONCLUSIONS:Our results suggest that digital droplet PCR was the most precise and quantitative method. The quantification of exon 51 skipping by Agilent bioanalyzer after a single round of PCR was the second-best choice with a 2.3-fold overestimation of exon 51 skipping levels compared to digital droplet PCR.

Published

2018

14. Dual Myostatin and Dystrophin Exon Skipping by Morpholino Nucleic Acid Oligomers Conjugated to a Cell-penetrating Peptide Is a Promising Therapeutic Strategy for the Treatment of Duchenne Muscular Dystrophy

Author

Alberto Malerba, Jagjeet K Kang, Graham McClorey, Amer F Saleh, Linda Popplewell, Michael J Gait, Matthew JA Wood, and George Dickson

Subjects

antisense oligonucleotides, Duchenne muscular dystrophy, dystrophin, exon skipping, myostatin, Therapeutics. Pharmacology, RM1-950

Abstract

The knockdown of myostatin, a negative regulator of skeletal muscle mass may have important implications in disease conditions accompanied by muscle mass loss like cancer, HIV/AIDS, sarcopenia, muscle atrophy, and Duchenne muscular dystrophy (DMD). In DMD patients, where major muscle loss has occurred due to a lack of dystrophin, the therapeutic restoration of dystrophin expression alone in older patients may not be sufficient to restore the functionality of the muscles. We recently demonstrated that phosphorodiamidate morpholino oligomers (PMOs) can be used to re-direct myostatin splicing and promote the expression of an out-of-frame transcript so reducing the amount of the synthesized myostatin protein. Furthermore, the systemic administration of the same PMO conjugated to an octaguanidine moiety (Vivo-PMO) led to a significant increase in the mass of soleus muscle of treated mice. Here, we have further optimized the use of Vivo-PMO in normal mice and also tested the efficacy of the same PMO conjugated to an arginine-rich cell-penetrating peptide (B-PMO). Similar experiments conducted in mdx dystrophic mice showed that B-PMO targeting myostatin is able to significantly increase the tibialis anterior (TA) muscle weight and when coadministered with a B-PMO targeting the dystrophin exon 23, it does not have a detrimental interaction. This study confirms that myostatin knockdown by exon skipping is a potential therapeutic strategy to counteract muscle wasting conditions and dual myostatin and dystrophin skipping has potential as a therapy for DMD.

Published

2012

15. Novel Metabolomic Approach for Identifying Pathology-Specific Biomarkers in Rare Diseases: A Case Study in Oculopharyngeal Muscular Dystrophy (OPMD)

Author

Snowden, Pradeep Harish, Alberto Malerba, Rosemarie H. M. J. M. Kroon, Milad Shademan, Baziel van Engelan, Vered Raz, Linda Popplewell, and Stuart G.

Subjects

biomarker, metabolomics, LC-MS, random forest, oculopharyngeal muscular dystrophy

Abstract

The identification of metabolomic biomarkers relies on the analysis of large cohorts of patients compared to healthy controls followed by the validation of markers in an independent sample set. Indeed, circulating biomarkers should be causally linked to pathology to ensure that changes in the marker precede changes in the disease. However, this approach becomes unfeasible in rare diseases due to the paucity of samples, necessitating the development of new methods for biomarker identification. The present study describes a novel approach that combines samples from both mouse models and human patients to identify biomarkers of OPMD. We initially identified a pathology-specific metabolic fingerprint in murine dystrophic muscle. This metabolic fingerprint was then translated into (paired) murine serum samples and then to human plasma samples. This study identified a panel of nine candidate biomarkers that could predict muscle pathology with a sensitivity of 74.3% and specificity of 100% in a random forest model. These findings demonstrate that the proposed approach can identify biomarkers with good predictive performance and a higher degree of confidence in their relevance to pathology than markers identified in a small cohort of human samples alone. Therefore, this approach has a high potential utility for identifying circulating biomarkers in rare diseases.

Published

2023

16. Microdystrophin Gene Addition Significantly Improves Muscle Functionality and Diaphragm Muscle Histopathology in a Fibrotic Mouse Model of Duchenne Muscular Dystrophy

Author

Viktorija Cernisova, Ngoc Lu-Nguyen, Jessica Trundle, Shan Herath, Alberto Malerba, and Linda Popplewell

Subjects

Inorganic Chemistry, Organic Chemistry, General Medicine, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Catalysis, Duchenne muscular dystrophy, muscle pathology, AAV8-microdystrophin, fibrosis, Computer Science Applications

Abstract

Duchenne muscular dystrophy (DMD) is a rare neuromuscular disease affecting 1:5000 newborn males. No cure is currently available, but gene addition therapy, based on the adeno-associated viral (AAV) vector-mediated delivery of microdystrophin transgenes, is currently being tested in clinical trials. The muscles of DMD boys present significant fibrotic and adipogenic tissue deposition at the time the treatment starts. The presence of fibrosis not only worsens the disease pathology, but also diminishes the efficacy of gene therapy treatments. To gain an understanding of the efficacy of AAV-based microdystrophin gene addition in a relevant, fibrotic animal model of DMD, we conducted a systemic study in juvenile D2.mdx mice using the single intravenous administration of an AAV8 system expressing a sequence-optimized murine microdystrophin, named MD1 (AAV8-MD1). We mainly focused our study on the diaphragm, a respiratory muscle that is crucial for DMD pathology and that has never been analyzed after treatment with AAV-microdystrophin in this mouse model. We provide strong evidence here that the delivery of AAV8-MD1 provides significant improvement in body-wide muscle function. This is associated with the protection of the hindlimb muscle from contraction-induced damage and the prevention of fibrosis deposition in the diaphragm muscle. Our work corroborates the observation that the administration of gene therapy in DMD is beneficial in preventing muscle fibrosis.

Published

2023

17. Evaluation of the dystrophin carboxy-terminal domain for micro-dystrophin gene therapy in cardiac and skeletal muscles in the DMDmdx rat model

Author

Audrey Bourdon, Virginie François, Liwen Zhang, Aude Lafoux, Bodvael Fraysse, Gilles Toumaniantz, Thibaut Larcher, Tiphaine Girard, Mireille Ledevin, Cyrielle Lebreton, Agnès Hivonnait, Anna Creismeas, Marine Allais, Basile Marie, Justine Guguin, Véronique Blouin, Séverine Remy, Ignacio Anegon, Corinne Huchet, Alberto Malerba, Betty Kao, Anita Le Heron, Philippe Moullier, George Dickson, Linda Popplewell, Oumeya Adjali, Federica Montanaro, and Caroline Le Guiner

Subjects

Genetics, Molecular Medicine, Molecular Biology

Published

2022

18. Knockdown of Muscle-Specific Ribosomal Protein L3-Like Enhances Muscle Function in Healthy and Dystrophic Mice

Author

Linda Popplewell, Ngoc Lu-Nguyen, John J. McCarthy, Pradeep Harish, Betty R Kao, George Dickson, and Alberto Malerba

Subjects

0301 basic medicine, Ribosomal Protein L3, Duchenne muscular dystrophy, Endogeny, Biology, Biochemistry, Dystrophin, Mice, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Ribosomal protein, Drug Discovery, Genetics, medicine, Animals, Myocyte, Muscle, Skeletal, Molecular Biology, Gene knockdown, Cardiac muscle, Skeletal muscle, medicine.disease, Cell biology, Muscular Dystrophy, Duchenne, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Mice, Inbred mdx, Molecular Medicine, Muscle Contraction

Abstract

Ribosomal protein L3-like (RPL3L) is a poorly characterized ribosomal protein that is exclusively expressed in skeletal and cardiac muscle. RPL3L is also downregulated in Duchenne muscular dystrophy (DMD), suggesting that it may play an important role in muscle biology. In this study, we investigated the role of RPL3L in skeletal muscle of healthy C57 and dystrophic mdx mice. We show that RPL3L is developmentally regulated and that intramuscular adeno-associated virus (AAV)-mediated RPL3L knockdown in the tibialis anterior of C57 and mdx mice results in increased specific force with improved resistance to eccentric contraction induced muscle damage in dystrophic muscles. The mechanism by which RPL3L knockdown improves muscle function remains unclear. Histological observations showed a significant increase in muscle length and decrease in muscle cross-sectional area after RPL3L inhibition suggesting that this ribosomal protein may play a role in myofiber morphology. The endogenous downregulation of RPL3L in DMD may be a protective mechanism that attempts to improve skeletal muscle function and counteract the dystrophic phenotype.

Published

2021

19. Dose-Dependent Microdystrophin Expression Enhancement in Cardiac Muscle by a Cardiac-Specific Regulatory Element

Author

Shanthi Herath, HH Abdul-Razak, Susan Jarmin, Marinee Chuah, Linda Popplewell, Chiara Sidoli, Ngoc Lu-Nguyen, Alberto Malerba, George Dickson, Thierry VandenDriessche, Anita Le Heron, Basic (bio-) Medical Sciences, and Division of Gene Therapy & Regenerative Medicine

Subjects

Male, Cardiac failure, Duchenne muscular dystrophy, Genetic enhancement, Genetic Vectors, Bioinformatics, Muscle wasting, Dystrophin, Mice, Genetics, medicine, Animals, Humans, Vector (molecular biology), Respiratory system, Muscle, Skeletal, Molecular Biology, Wasting, Tropism, Medicine(all), business.industry, Myocardium, respiratory failure, Cardiac muscle, Dependovirus, medicine.disease, Muscular Dystrophy, Duchenne, medicine.anatomical_structure, Respiratory failure, Duchenne muscular dystrophy (DMD), Mice, Inbred mdx, Molecular Medicine, medicine.symptom, business

Abstract

Duchenne muscular dystrophy (DMD) is an X-linked recessive disease that affects 1:5,000 live male births and is characterized by muscle wasting. By the age of 13 years, affected individuals are often wheelchair bound and suffer from respiratory and cardiac failure, which results in premature death. Although the administration of corticosteroids and ventilation can relieve the symptoms and extend the patients' lifespan, currently no cure exists for DMD. Among the different approaches under preclinical and clinical testing, gene therapy, using adeno-associated viral (AAV) vectors, is one of the most promising. In this study, we delivered intravenously AAV9 vectors expressing the microdystrophin MD1 (ΔR4-R23/ΔCT) under control of the synthetic muscle-specific promoter Spc5-12 and assessed the effect of adding a cardiac-specific cis-regulatory module (designated as CS-CRM4) on its expression profile in skeletal and cardiac muscles. Results show that Spc5-12 promoter, in combination with an AAV serotype that has high tropism for the heart, drives high MD1 expression levels in cardiac muscle in mdx mice. The additional regulatory element CS-CRM4 can further improve MD1 expression in cardiac muscles, but its effect is dose dependent and enhancement becomes evident only at lower vector doses.

Published

2021

20. Systemic Delivery of a Monoclonal Antibody to Immunologically Block Myostatin in the A17 Mouse Model of OPMD

Author

Alberto Malerba, Pradeep Harish, and Linda Popplewell

Published

2022

21. Systemic Delivery of a Monoclonal Antibody to Immunologically Block Myostatin in the A17 Mouse Model of OPMD

Author

Alberto, Malerba, Pradeep, Harish, and Linda, Popplewell

Subjects

Mice, Disease Models, Animal, Muscular Dystrophy, Oculopharyngeal, Animals, Antibodies, Monoclonal, Immunotherapy, Myostatin

Abstract

Oculopharyngeal muscular dystrophy (OPMD) is a late-onset rare muscle disease affecting approximately 1 in 80,000 individuals worldwide. However, it can affect as much as 1:600 individuals in some populations due to a strong founder effect. The muscle pathology is characterized by progressive eyelid drooping (ptosis), swallowing difficulties (dysphagia), and limb weakness at later stages of disease progression. The genetic defect is associated with significant fibrotic deposition and atrophy in affected muscles. No treatments are available to cure the disease. Only surgical techniques to correct ptosis and swallowing are currently possible, though they carry a risk of recurrence. Myostatin is a negative regulator of muscle growth, and several strategies to downregulate its expression have been developed with the aim of improving muscle mass and strength in muscular pathologies. We recently showed that weekly systemic treatment of the A17 murine model of OPMD with a monoclonal antibody for myostatin improves body and muscle mass, increases muscle strength, and reduces muscle fibrosis. Here, we describe the methodology for repeated intraperitoneal delivery of myostatin antibody in the murine model. Furthermore, we detail the most relevant analyses to assess histopathological and functional improvements of this treatment in this mouse model.

Published

2022

22. Systemic antisense therapeutics inhibiting DUX4 expression ameliorates FSHD-like pathology in an FSHD mouse model

Author

Alberto Malerba, Linda Popplewell, Ngoc Lu-Nguyen, George Dickson, and Shan Herath

Subjects

AcademicSubjects/SCI01140, 0301 basic medicine, Muscle Fibers, Skeletal, Mice, Transgenic, Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, DUX4, In vivo, Genetics, medicine, Animals, Humans, Facioscapulohumeral muscular dystrophy, Myocyte, RNA, Messenger, Muscle, Skeletal, Molecular Biology, Genetics (clinical), Homeodomain Proteins, Messenger RNA, Genes, Homeobox, Skeletal muscle, Translation (biology), General Medicine, medicine.disease, Muscular Dystrophy, Facioscapulohumeral, Muscle atrophy, Disease Models, Animal, Muscular Atrophy, 030104 developmental biology, medicine.anatomical_structure, Cancer research, General Article, medicine.symptom, 030217 neurology & neurosurgery

Abstract

Aberrant expression of the double homeobox 4 (DUX4) gene in skeletal muscle causes muscle deterioration and weakness in Facioscapulohumeral muscular dystrophy (FSHD). Since the presence of a permissive pLAM1 polyadenylation signal is essential for stabilization of DUX4 mRNA and translation of DUX4 protein, disrupting the function of this structure can prevent expression of DUX4. We and others have shown promising results using antisense approaches to reduce DUX4 expression in vitro and in vivo following local intramuscular administration. Here we demonstrate that further development of the antisense chemistries enhances in vitro antisense efficacy. The optimal chemistry was conjugated to a cell-penetrating moiety and was systemically administered into the tamoxifen-inducible Cre-driver FLExDUX4 double-transgenic mouse model of FSHD. After four weekly treatments, mRNA quantities of DUX4 and target genes were reduced by 50% that led to 12% amelioration in muscle atrophy, 52% improvement in in situ muscle strength, 17% reduction in muscle fibrosis and prevention of shift in the myofiber type profile. Systemic DUX4 inhibition also significantly improved the locomotor activity and reduced the fatigue level by 22%. Our data demonstrate that the optimized antisense approach has potential of being further developed as a therapeutic strategy for FSHD.

Published

2021

23. Mutation-Directed Therapeutics for Neurofibromatosis Type I

Author

Ulrich Müller, Linda Popplewell, Tatiana T. Marquez Lago, Deeann Wallis, Ann T. Chen, Bruce R. Korf, André Leier, Robert A. Kesterson, David M. Bedwell, Kim M. Keeling, George Dickson, and Jiangbing Zhou

Subjects

0301 basic medicine, Bioinformatics, medicine.disease_cause, Article, Viral vector, 03 medical and health sciences, 0302 clinical medicine, Drug Discovery, medicine, CRISPR, Loss function, Neurofibromatosis type I, Mutation, biology, business.industry, lcsh:RM1-950, Genetic disorder, medicine.disease, Neurofibromin 1, Exon skipping, 030104 developmental biology, lcsh:Therapeutics. Pharmacology, 030220 oncology & carcinogenesis, biology.protein, Molecular Medicine, business

Abstract

Significant advances in biotechnology have led to the development of a number of different mutation-directed therapies. Some of these techniques have matured to a level that has allowed testing in clinical trials, but few have made it to approval by drug-regulatory bodies for the treatment of specific diseases. While there are still various hurdles to be overcome, recent success stories have proven the potential power of mutation-directed therapies and have fueled the hope of finding therapeutics for other genetic disorders. In this review, we summarize the state-of-the-art of various therapeutic approaches and assess their applicability to the genetic disorder neurofibromatosis type I (NF1). NF1 is caused by the loss of function of neurofibromin, a tumor suppressor and downregulator of the Ras signaling pathway. The condition is characterized by a variety of phenotypes and includes symptoms such as skin spots, nervous system tumors, skeletal dysplasia, and others. Hence, depending on the patient, therapeutics may need to target different tissues and cell types. While we also discuss the delivery of therapeutics, in particular via viral vectors and nanoparticles, our main focus is on therapeutic techniques that reconstitute functional neurofibromin, most notably cDNA replacement, CRISPR-based DNA repair, RNA repair, antisense oligonucleotide therapeutics including exon skipping, and nonsense suppression., Graphical Abstract, We present a comprehensive review that addresses therapeutic approaches to treating specific genetic defects that cause neurofibromatosis type I, including nanoparticle delivery, exon skipping, gene editing, mRNA trans-splicing ribozymes, and non-sense suppression therapeutics. Our multi-faceted approach can be utilized for virtually any rare disease to affect personalized medicine.

Published

2020

24. G-quadruplex ligands mediate downregulation of DUX4 expression

Author

Alex Slater, Mark S. Searle, Lukasz Ciszewski, Linda Popplewell, Ngoc Lu-Nguyen, Andrew Brennan, Huw E. L. Williams, and George Dickson

Subjects

Male, Berberine, AcademicSubjects/SCI00010, Down-Regulation, Biology, Ligands, Cell Fusion, Myoblasts, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, DUX4, Downregulation and upregulation, Cell Line, Tumor, Genetics, medicine, Animals, Myocyte, Facioscapulohumeral muscular dystrophy, RNA, Messenger, Nucleotide Motifs, Muscle, Skeletal, Promoter Regions, Genetic, Enhancer, Gene, 030304 developmental biology, Homeodomain Proteins, 0303 health sciences, Gene regulation, Chromatin and Epigenetics, Ligand (biochemistry), medicine.disease, Fibrosis, Muscular Dystrophy, Facioscapulohumeral, Clone Cells, Cell biology, G-Quadruplexes, Mice, Inbred C57BL, Enhancer Elements, Genetic, chemistry, 030217 neurology & neurosurgery

Abstract

Abnormal DUX4 expression in skeletal muscles plays a key role in facioscapulohumeral muscular dystrophy (FSHD) pathogenesis, although the molecular mechanisms regulating DUX4 expression are not fully defined. Using bioinformatic analysis of the genomic DUX4 locus, we have identified a number of putative G-quadruplexes (GQs) forming sequences. Their presence was confirmed in synthetic oligonucleotiode sequences derived from the enhancer, promoter and transcript of DUX4 through circular dichroism and nuclear magnetic resonance analysis. We further examined the binding affinity of a naturally occurring GQ stabilizing compound, berberine, to these non-canonical genetic structures using UV–Vis and fluorescence spectroscopy. Subsequent in vitro study in FSHD patient myoblasts indicated that berberine treatment reduced DUX4 expression and also expression of genes normally switched on by DUX4. Further investigation in a mouse model overexpressing exogenous DUX4 confirmed the therapeutic effects of berberine in downregulating DUX4 protein expression, inhibiting muscle fibrosis, and consequently rescuing muscle function. Our data demonstrate for the first time that GQs are present in the DUX4 locus and that the GQ interactive ligand reduces DUX4 expression suggesting potential role of GQs in FSHD pathogenesis. Our work provides the basis of a novel therapeutic strategy for the treatment of FSHD.

Published

2020

25. Improving Molecular and Histopathology in Diaphragm Muscle of the Double Transgenic ACTA1-MCM/FLExDUX4 Mouse Model of FSHD with Systemic Antisense Therapy

Author

Ngoc Lu-Nguyen, Alberto Malerba, Marina Antoni Pineda, George Dickson, and Linda Popplewell

Subjects

Homeodomain Proteins, Disease Models, Animal, Mice, Diaphragm, Genetics, Molecular Medicine, Animals, Mice, Transgenic, Muscle, Skeletal, Molecular Biology, Muscular Dystrophy, Facioscapulohumeral

Abstract

Facioscapulohumeral muscular dystrophy (FSHD) is a rare muscle dystrophy causing muscle weakness initially in the face, shoulders, and upper arms, and extends to lower body muscles as the disease progresses. Respiratory restriction in FSHD is increasingly reported to be more common and severe than previously thought, with the involvement of diaphragm weakness in pulmonary insufficiency being under debate. As aberrant expression of the double homeobox 4 (iDUX4/i) gene is the prime cause of FSHD, we and others have developed numerous strategies and reported promising results on downregulatingiDUX4/iexpression in both cellular and animal models of FSHD. However, the effect of DUX4 and anti-DUX4 approaches on diaphragm muscle has not been elucidated. In this study, we show that toxiciDUX4/iexpression causes pathology that affects the diaphragm of ACTA1-MCM/FLExDUX4 mouse model of FSHD at both molecular and histological levels. Of importance, a systemic antisense treatment that suppressesiDUX4/iand target genes expression by 50% significantly improves muscle regeneration and muscle fibrosis, and prevents modification in myofiber type composition, supporting its development as a treatment for FSHD.

Published

2022

26. Targeted Therapeutics for Rare Disorders

Author

Kim M. Keeling, Andre Leier, David M. Bedwell, Ann T. Chen, Robert A. Kesterson, Tatiana T. Marquez Lago, Ulrich F. Müller, Jiangbing Zhou, Linda Popplewell, and Deeann Wallis

Published

2022

27. Use of Small Animal Models for Duchenne and Parameters to Assess Efficiency upon Antisense Treatment

Author

Ngoc Lu-Nguyen, Alberto Malerba, and Linda Popplewell

Subjects

musculoskeletal diseases, Dystrophin, Muscular Dystrophy, Duchenne, congenital, hereditary, and neonatal diseases and abnormalities, Disease Models, Animal, Mice, Mice, Inbred mdx, Animals, Humans, Exons, Oligonucleotides, Antisense, Research Article

Abstract

Duchenne muscular dystrophy (DMD) is a rare genetic disease affecting 1 in 5000 newborn boys. It is caused by mutations in the DMD gene with a consequent lack of dystrophin protein that leads to deterioration of myofibers and their replacement with fibro-adipogenic tissue. Using antisense oligonucleotides (AONs) to modify out-of-frame mutations in the DMD gene, named exon skipping, is currently considered among the most promising treatments for DMD patients. The development of this strategy is rapidly moving forward, and AONs designed to skip exons 51 and 53 have received accelerated approval in the USA. In preclinical setting, the mdx mouse model, carrying a point mutation in exon 23 of the murine Dmd gene that prevents production of dystrophin protein, has emerged as a valuable tool, and it is widely used to study in vivo therapeutic approaches for DMD. Here we describe the methodology for intravenous delivery of AONs targeting dystrophin through tail vein of mdx mice. Furthermore, the most relevant functional analyses to be performed in living mice, and the most informative histopathological and molecular assays to evaluate the effect of this treatment are detailed.

Published

2022

28. Restoration of Normal NF1 Function with Antisense Morpholino Treatment of Recurrent Pathogenic Patient-Specific Variant c.1466A>G; p.Y489C

Author

Elias K. Awad, Marc Moore, Hui Liu, Lukasz Ciszewski, Laura Lambert, Bruce R. Korf, Linda Popplewell, Robert A. Kesterson, and Deeann Wallis

Subjects

Medicine, Medicine (miscellaneous), neurofibromatosis type 1, cryptic splice, antisense oligo therapeutics, Article

Abstract

Neurofibromatosis type 1 (NF1) is an autosomal dominant genetic disorder with almost 3000 different disease-causing variants within the NF1 gene identified. Up to 44% of these variants cause splicing errors to occur within pre-mRNA. A recurrent variant in exon 13, c.1466A>G; p.Y489C (Y489C) results in the creation of an intragenic cryptic splice site, aberrant splicing, a 62 base pair deletion from the mRNA, and subsequent frameshift. We investigated the ability of phosphorodiamidate morpholino oligomers (PMOs) to mask this variant on the RNA level, thus restoring normal splicing. To model this variant, we have developed a human iPS cell line homozygous for the variant using CRISPR/Cas9. PMOs were designed to be 25 base pairs long, and to cover the mutation site so it could not be read by splicing machinery. Results from our in vitro testing showed restoration of normal splicing in the RNA and restoration of full length neurofibromin protein. In addition, we observe the restoration of neurofibromin functionality through GTP-Ras and pERK/ERK testing. The results from this study demonstrate the ability of a PMO to correct splicing errors in NF1 variants at the RNA level, which could open the door for splicing corrections for other variants in this and a variety of diseases.

Published

2021

29. Targeted exon skipping of

Author

André, Leier, Marc, Moore, Hui, Liu, Michael, Daniel, Alexis M, Hyde, Ludwine, Messiaen, Bruce R, Korf, Jamuna, Selvakumaran, Lukasz, Ciszewski, Laura, Lambert, Jeremy, Foote, Margaret R, Wallace, Robert A, Kesterson, George, Dickson, Linda, Popplewell, and Deeann, Wallis

Abstract

We investigated the feasibility of utilizing an exon-skipping approach as a genotype-dependent therapeutic for neurofibromatosis type 1 (NF1) by determining which

Published

2021

30. Exon Skipping as a Therapeutic for Neurofibromatosis Type I

Author

Linda Popplewell, Jeremy Foote, Alexis Hyde, Ludwine Messiaen, André Leier, Jamuna Selvakumaran, Marc Moore, Lukasz Ciszewski, Deeann Wallis, Hui Liu, Robert A. Kesterson, Laura J. Lambert, Michael Daniel, Bruce R. Korf, and George Dickson

Subjects

Neurofibromatosis type I, congenital, hereditary, and neonatal diseases and abnormalities, business.industry, Cancer research, medicine, medicine.disease, business, Exon skipping, nervous system diseases

Abstract

We investigated the feasibility of utilizing an exon skipping approach as a genotype-dependent therapeutic for neurofibromatosis type 1 (NF1) by determining which NF1 exons might be skipped while maintaining neurofibromin function. Human neurofibromin is well-known as a GTPase activating protein (GAP), but outside of its GAP-related domain (GRD), it is unclear how critical other regions are for function. Initial in silico analysis predicted exons that can be skipped with minimal loss of neurofibromin function. Utilizing a novel Nf1 cDNA system, we performed a functional screen to determine the effects of exon skipping on in vitro neurofibromin expression and GRD function. Loss of single exons 12, 17, 25, 41, 47, or 52 maintained significant GRD function in at least two Ras activity assays. Exons 18/19, 20 and 28 are critical for GRD function; deletion of exons 20, 41, or 47 led to significantly lower levels of neurofibromin. As suggested by in silico analysis, skipping of exons 17 or 52 resulted in both the highest neurofibromin levels and the greatest suppression of Ras activity. Assessment of NF1 patient databases indicates that pathogenic variants resulting in deletion or skipping of exons 17, 25, and 52 have not been reported; and truncating pathogenic variants in each exon account for ~0.91, 0.94, and 0.25% of unrelated NF1 cases, respectively. Hence, we designed antisense phosphodiamitate morpholino oligos (PMOs) to skip exon 17 and evaluated them in human cell lines that we generated via CRISPR/Cas9 with a patient-specific truncating pathogenic variant, c.1885G>A. We down-selected oligos that efficiently caused skipping of exon 17 and restored NF1 expression and function. Further, homozygous deletion of exon 17 in a novel mouse model is compatible with viable and grossly healthy animals with normal lifespan and no tumor development, providing proof-of-concept that exon 17 is not essential for murine neurofibromin function. Mild phenotypes observed include abnormal nesting behavior and lymphoid hyperplasia with increased numbers of both B- and T-cells. Hence, exon skipping should be further investigated as a therapeutic approach for NF1 patients with treatment of individuals with pathogenic variants in exon 17.

Published

2021

31. RAC1B modulates intestinal tumourigenesis via modulation of WNT and EGFR signalling pathways

Author

George Dickson, Linda Popplewell, Farhat V N Din, Adam E. Hall, Kevin Myant, Malcolm G. Dunlop, Paz Freile, Alfonso Bolado, Caroline V. Billard, Victoria Gudiño, Stuart Aitken, Mark Agostino, David A. Stevenson, Douglas Strathdee, Laura Murphy, Owen J. Sansom, Alex von Kriegsheim, Sebastian Öther-Gee Pohl, John W. Cassidy, Patrizia Cammareri, Colin Nixon, Ann P. Wheeler, Pohl, Sebastian Öther-Gee [0000-0002-4294-9498], Aitken, Stuart [0000-0003-4867-4568], Agostino, Mark [0000-0002-1799-0392], Nixon, Colin [0000-0002-8085-2160], von Kriegsheim, Alex [0000-0002-4952-8573], Wheeler, Ann [0000-0001-8617-827X], Strathdee, Douglas [0000-0003-2959-4327], Sansom, Owen J [0000-0001-9540-3010], Myant, Kevin B [0000-0001-8017-1093], and Apollo - University of Cambridge Repository

Subjects

Male, rac1 GTP-Binding Protein, 0301 basic medicine, Cancer therapy, Carcinogenesis, Colorectal cancer, Cetuximab, General Physics and Astronomy, Mice, Antineoplastic Agents, Immunological, 0302 clinical medicine, Clinical efficacy, Cancer genetics, Wnt Signaling Pathway, EGFR inhibitors, Mice, Knockout, Egfr signalling, Multidisciplinary, Cancer stem cells, Wnt signaling pathway, Up-Regulation, ErbB Receptors, Gene Expression Regulation, Neoplastic, Cancer therapeutic resistance, 030220 oncology & carcinogenesis, Female, Colorectal Neoplasms, Signal Transduction, medicine.drug, Poor prognosis, Science, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Targeted therapies, Mediator, Cell Line, Tumor, medicine, Animals, Humans, business.industry, Neuropeptides, General Chemistry, medicine.disease, Mice, Inbred C57BL, 030104 developmental biology, Drug Resistance, Neoplasm, Cancer research, business

Abstract

Current therapeutic options for treating colorectal cancer have little clinical efficacy and acquired resistance during treatment is common, even following patient stratification. Understanding the mechanisms that promote therapy resistance may lead to the development of novel therapeutic options that complement existing treatments and improve patient outcome. Here, we identify RAC1B as an important mediator of colorectal tumourigenesis and a potential target for enhancing the efficacy of EGFR inhibitor treatment. We find that high RAC1B expression in human colorectal cancer is associated with aggressive disease and poor prognosis and deletion of Rac1b in a mouse colorectal cancer model reduces tumourigenesis. We demonstrate that RAC1B interacts with, and is required for efficient activation of the EGFR signalling pathway. Moreover, RAC1B inhibition sensitises cetuximab resistant human tumour organoids to the effects of EGFR inhibition, outlining a potential therapeutic target for improving the clinical efficacy of EGFR inhibitors in colorectal cancer., RAC1 is a downstream target of the Wnt signaling that promotes intestinal stem cell expansion and tumorigenesis. Here, the authors identify the specific splice variant RAC1B as an important mediator of colorectal tumourigenesis and a potential target for enhancing the efficacy of EGFR inhibitor treatment.

Published

2021

32. Evaluation of the dystrophin carboxy-terminal domain for micro-dystrophin gene therapy in cardiac and skeletal muscles in the DMDsupmdx/suprat model

Author

Audrey, Bourdon, Virginie, François, Liwen, Zhang, Aude, Lafoux, Bodvael, Fraysse, Gilles, Toumaniantz, Thibaut, Larcher, Tiphaine, Girard, Mireille, Ledevin, Cyrielle, Lebreton, Agnès, Hivonnait, Anna, Creismeas, Marine, Allais, Basile, Marie, Justine, Guguin, Véronique, Blouin, Séverine, Remy, Ignacio, Anegon, Corinne, Huchet, Alberto, Malerba, Betty, Kao, Anita, Le Heron, Philippe, Moullier, George, Dickson, Linda, Popplewell, Oumeya, Adjali, Federica, Montanaro, and Caroline, Le Guiner

Subjects

Dystrophin, Muscular Dystrophy, Duchenne, Tandem Mass Spectrometry, Animals, Genetic Therapy, Muscle, Skeletal, Chromatography, Liquid, Dystrophin-Associated Protein Complex, Rats

Abstract

Duchenne muscular dystrophy (DMD) is a muscle wasting disorder caused by mutations in the gene encoding dystrophin. Gene therapy using micro-dystrophin (MD) transgenes and recombinant adeno-associated virus (rAAV) vectors hold great promise. To overcome the limited packaging capacity of rAAV vectors, most MD do not include dystrophin carboxy-terminal (CT) domain. Yet, the CT domain is known to recruit α1- and β1-syntrophins and α-dystrobrevin, a part of the dystrophin-associated protein complex (DAPC), which is a signaling and structural mediator of muscle cells. In this study, we explored the impact of inclusion of the dystrophin CT domain on ΔR4-23/ΔCT MD (MD1), in DMDsupmdx/suprats, which allows for relevant evaluations at muscular and cardiac levels. We showed by LC-MS/MS that MD1 expression is sufficient to restore the interactions at a physiological level of most DAPC partners in skeletal and cardiac muscles, and that inclusion of the CT domain increases the recruitment of some DAPC partners at supra-physiological levels. In parallel, we demonstrated that inclusion of the CT domain does not improve MD1 therapeutic efficacy on DMD muscle and cardiac pathologies. Our work highlights new evidences of the therapeutic potential of MD1 and strengthens the relevance of this candidate for gene therapy of DMD.

Published

2021

33. Systemic antisense therapeutics inhibiting DUX4 expression improves muscle function in an FSHD mouse model

Author

Ngoc Lu-Nguyen, Alberto Malerba, Linda Popplewell, and George Dickson

Subjects

Messenger RNA, Polyadenylation, business.industry, Skeletal muscle, Translation (biology), medicine.disease, In vitro, medicine.anatomical_structure, DUX4, In vivo, medicine, Cancer research, Facioscapulohumeral muscular dystrophy, business

Abstract

Aberrant expression of the double homeobox 4 (DUX4) gene in skeletal muscle causes muscle deterioration and weakness in Facioscapulohumeral Muscular Dystrophy (FSHD). Since the presence of a permissive pLAM1 polyadenylation signal is essential for stabilization of DUX4 mRNA and translation of DUX4 protein, disrupting the function of this structure can prevent expression of DUX4. We and others have shown promising results using antisense approaches to reduce DUX4 expression in vitro and in vivo following local intramuscular administration. Our group has developed further the antisense chemistries, and demonstrate here enhanced in vitro antisense efficacy. The optimal chemistry was conjugated to a cell-penetrating moiety, and for the first time in FSHD research has been systemically administered into a double-transgenic mouse model of FSHD. After four weekly treatments, mRNA quantities of DUX4 and target genes were reduced by 50% that led to a 5% increase in muscle mass, a 52% improvement in in situ muscle strength, and reduction of muscle fibrosis by 17%. Systemic DUX4 inhibition also improved the locomotor activity significantly and reduced the fatigue level by 22%. Our data overall demonstrate that the optimized antisense approach can contribute to future development of a therapeutic strategy for FSHD.

Published

2021

34. A new strategy to increase RNA editing at the Q/R site of GluA2 AMPA receptor subunits by targeting alternative splicing patterns of ADAR2

Author

Linda Popplewell, Philip E. Chen, Helena Chaytow, George Dickson, Ilda Sethw Hassan, and Sara Akbar

Subjects

Gene isoform, chemistry.chemical_classification, Antisense oligonucleotides, AMPARs, Chemistry, Adenosine Deaminase, General Neuroscience, Protein subunit, Short Communication, Alternative splicing, RNA, RNA-Binding Proteins, AMPA receptor, Ribosomal RNA, Amyotrophic lateral sclerosis, Cell biology, Amino acid, Alternative Splicing, RNA editing, ADAR2, Animals, RNA Editing, Receptors, AMPA, Neurodegeneration

Abstract

Background The GluA2 subunit of AMPA receptors (AMPARs) undergoes RNA editing at a specific base mediated by the enzyme ADAR2, changing the coded amino acid from a glutamine to arginine at the so-called Q/R site, which is critical for regulating calcium permeability. ADAR2 exists as multiple alternatively-spliced variants within mammalian cells with differing editing efficiency. New method In this study, phosphorodiamidate morpholino oligomers (PMOs) were used to increase Q/R site editing, by affecting the alternative splicing of ADAR2. Results PMOs targeting the ADAR2 pre-mRNA transcript successfully induced alternative splicing around the AluJ cassette leading to expression of a more active isoform with increased editing of the GluA2 subunit compared to control. Comparison with existing method(s) Previously PMOs have been used to disrupt RNA editing via steric hindrance of the GluA2 RNA duplex. In contrast we report PMOs that can increase the expression of more catalytically active variants of ADAR2, leading to enhanced GluA2 Q/R RNA editing. Conclusions Using PMOs to increase Q/R site editing is presented here as a validated method that would allow investigation of downstream cellular processes implicated in altered ADAR2 activity., Graphical Abstract ga1, Highlights • Aberrant RNA editing has been linked to a number of neurodegenerative diseases. • Phosphorodiamidate morpholino oligomers (PMOs) were targeted to ADAR2 pre-mRNA. • These PMOs increased expression of ADAR2 isoforms with higher editing efficiency. • These PMOs significantly increased Q/R editing in HeLa and SH-SY5Y cell lines.

Published

2021

35. The administration of antisense oligonucleotide golodirsen reduces pathological regeneration in patients with Duchenne muscular dystrophy

Author

F. Catapano, Jennifer E. Morgan, Caroline Sewry, Matthew Ellis, D. Scaglioni, Erica Koenig, Matthew Beck, Mauro Monforte, Lucy Feng, Volker Straub, Francesco Muntoni, Silvia Torelli, Eugenio Mercuri, D. Chambers, Jyoti Malhotra, Linda Popplewell, Shawn Harriman, Laurent Servais, Michela Guglieri, and Rahul Phadke

Subjects

0301 basic medicine, Male, Morpholino, Duchenne muscular dystrophy, Biopsy, Immunofluorescence, Oligonucleotides, lcsh:RC346-429, Dystrophin, Exon, 0302 clinical medicine, Sarcolemma, Genetic therapies, Medicine, Muscular dystrophy, Child, Dystroglycans, biology, medicine.diagnostic_test, musculoskeletal system, Dystrophin-associated protein, Clinical trial, Treatment Outcome, Golodirsen, musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Myosins, Pathology and Forensic Medicine, 03 medical and health sciences, Cellular and Molecular Neuroscience, Sarcoglycans, Humans, Regeneration, Muscle, Skeletal, lcsh:Neurology. Diseases of the nervous system, business.industry, Research, Oligonucleotides, Antisense, medicine.disease, Exon skipping, Muscular Dystrophy, Duchenne, 030104 developmental biology, Cancer research, biology.protein, Neurology (clinical), Laminin, business, 030217 neurology & neurosurgery

Abstract

During the last decade, multiple clinical trials for Duchenne muscular dystrophy (DMD) have focused on the induction of dystrophin expression using different strategies. Many of these trials have reported a clear increase in dystrophin protein following treatment. However, the low levels of the induced dystrophin protein have raised questions on its functionality. In our present study, using an unbiased, high-throughput digital image analysis platform, we assessed markers of regeneration and levels of dystrophin associated protein via immunofluorescent analysis of whole muscle sections in 25 DMD boys who received 48-weeks treatment with exon 53 skipping morpholino antisense oligonucleotide (PMO) golodirsen. We demonstrate that the de novo dystrophin induced by exon skipping with PMO golodirsen is capable of conferring a histological benefit in treated patients with an increase in dystrophin associated proteins at the dystrophin positive regions of the sarcolemma in post-treatment biopsies. Although 48 weeks treatment with golodirsen did not result in a significant change in the levels of fetal/developmental myosins for the entire cohort, there was a significant negative correlation between the amount of dystrophin and levels of regeneration observed in different biopsy samples. Our results provide, for the first time, evidence of functionality of induced dystrophin following successful therapeutic intervention in the human. Electronic supplementary material The online version of this article (10.1186/s40478-020-01106-1) contains supplementary material, which is available to authorized users.

Published

2020

36. Fast Facts: Gene Therapy

Author

Roland Herzog and Linda Popplewell

Published

2020

37. Fast Facts: Gene Therapy A new therapeutic direction?

Author

Roland W. Herzog and Linda Popplewell

Published

2021

38. Systemic Antisense Therapeutics for Dystrophin and Myostatin Exon Splice Modulation Improve Muscle Pathology of Adult mdx Mice

Author

Linda Popplewell, Gunnar J. Hanson, George Dickson, Ngoc Lu-Nguyen, Fred Schnell, and Alberto Malerba

Subjects

0301 basic medicine, musculoskeletal diseases, Duchenne muscular dystrophy, congenital, hereditary, and neonatal diseases and abnormalities, government.form_of_government, Myostatin, dystrophin, 03 medical and health sciences, Exon, Fibrosis, Drug Discovery, Medicine, Muscular dystrophy, Antisense therapy, biology, business.industry, lcsh:RM1-950, medicine.disease, musculoskeletal system, Exon skipping, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, myostatin, biology.protein, government, Cancer research, Molecular Medicine, Original Article, antisense oligonucleotides, business, Dystrophin, exon skipping

Abstract

Antisense-mediated exon skipping is a promising approach for the treatment of Duchenne muscular dystrophy (DMD), a rare life-threatening genetic disease due to dystrophin deficiency. Such an approach can restore the disrupted reading frame of dystrophin pre-mRNA, generating a truncated form of the protein. Alternatively, antisense therapy can be used to induce destructive exon skipping of myostatin pre-mRNA, knocking down myostatin expression to enhance muscle strength and reduce fibrosis. We have reported previously that intramuscular or intraperitoneal antisense administration inducing dual exon skipping of dystrophin and myostatin pre-mRNAs was beneficial in mdx mice, a mouse model of DMD, although therapeutic effects were muscle type restricted, possibly due to the delivery routes used. Here, following systemic intravascular antisense treatment, muscle strength and body activity of treated adult mdx mice increased to the levels of healthy controls. Importantly, hallmarks of muscular dystrophy were greatly improved in mice receiving the combined exon-skipping therapy, as compared to those receiving dystrophin antisense therapy alone. Our results support the translation of antisense therapy for dystrophin restoration and myostatin inhibition into the clinical setting for DMD. Keywords: antisense oligonucleotides, Duchenne muscular dystrophy, dystrophin, exon skipping, myostatin

Published

2016

39. GENETIC THERAPY OF MUSCLE DISEASES: DUCHENNE MUSCULAR DYSTROPHY

Author

Takis Athanasopoulos, Susan Jarmin, Helen Foster, Keith Foster, Jagjeet Kang, Taeyoung Koo, Alberto Malerba, Linda Popplewell, Daniel Scherman, and George Dickson

Published

2019

40. Inhibition of myostatin improves muscle atrophy in oculopharyngeal muscular dystrophy (OPMD)

Author

Leysa Forrest, George Dickson, Pradeep Harish, Linda Popplewell, Fanny Roth, Ornella Cappellari, Capucine Trollet, Ngoc Lu-Nguyen, Alberto Malerba, Royal Holloway, University of London, Royal Veterinary College [London], University of London [London], Centre de recherche en myologie, Université Pierre et Marie Curie - Paris 6 (UPMC)-Association française contre les myopathies (AFM-Téléthon)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Unité de Pharmacologie Chimique et Génétique (UPCG - UMR_S 640/UMR 8151), Centre National de la Recherche Scientifique (CNRS)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Descartes - Paris 5 (UPD5)-Institut des sciences du Médicament -Toxicologie - Chimie - Environnement (IFR71), Institut National de la Santé et de la Recherche Médicale (INSERM)-Ecole Nationale Supérieure de Chimie de Paris - Chimie ParisTech-PSL (ENSCP), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche pour le Développement (IRD)-Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Ecole Nationale Supérieure de Chimie de Paris - Chimie ParisTech-PSL (ENSCP), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche pour le Développement (IRD)-Université Paris Descartes - Paris 5 (UPD5)-Institut de Chimie du CNRS (INC), Royal Holloway, School of Biological Sciences (ROYAL HOLLOWAY), Queen Mary University of London (QMUL), Centre National de la Recherche Scientifique (CNRS)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Association française contre les myopathies (AFM-Téléthon)-Université Pierre et Marie Curie - Paris 6 (UPMC), Ecole Nationale Supérieure de Chimie de Paris- Chimie ParisTech-PSL (ENSCP)-Institut des sciences du Médicament -Toxicologie - Chimie - Environnement (IFR71), and Institut National de la Santé et de la Recherche Médicale (INSERM)-Ecole Nationale Supérieure de Chimie de Paris- Chimie ParisTech-PSL (ENSCP)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche pour le Développement (IRD)-Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche pour le Développement (IRD)-Université Paris Descartes - Paris 5 (UPD5)-Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)

Subjects

0301 basic medicine, muscle atrophy, lcsh:Diseases of the musculoskeletal system, Myostatin, Myoblasts, Mice, 0302 clinical medicine, Ptosis, Myocyte, Orthopedics and Sports Medicine, ComputingMilieux_MISCELLANEOUS, education.field_of_study, biology, Antibodies, Monoclonal, lcsh:Human anatomy, musculoskeletal system, Immunohistochemistry, Muscle atrophy, 3. Good health, Muscular Atrophy, 030220 oncology & carcinogenesis, OPMD, Body Composition, Original Article, medicine.symptom, medicine.medical_specialty, Population, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, lcsh:QM1-695, Oculopharyngeal muscular dystrophy, 03 medical and health sciences, Atrophy, Muscular Dystrophy, Oculopharyngeal, Physiology (medical), Internal medicine, medicine, Animals, Muscle Strength, education, Muscle, Skeletal, RK35, Anti‐myostatin antibody, business.industry, Anti-myostatin antibody, Original Articles, medicine.disease, Transplantation, 030104 developmental biology, Endocrinology, biology.protein, lcsh:RC925-935, business, Biomarkers

Abstract

Copyright © 2019 The Authors. Background: Oculopharyngeal muscular dystrophy (OPMD) is a late-onset muscle disease affecting one per 80 000 of the general population characterized by profound dysphagia and ptosis, and limb weakness at later stages. Affected muscles are characterized by increased fibrosis and atrophy. Myostatin is a negative regulator of muscle mass, and inhibition of myostatin has been demonstrated to ameliorate symptoms in dystrophic muscles. Methods: In this study, we performed a systemic delivery of a monoclonal antibody to immunologically block myostatin in the A17 mouse model of OPMD. The mice were administered a weekly dose of 10 mg/kg RK35 intraperitonially for 10 weeks, following which histological analyses were performed on the samples. Results: This treatment significantly (P < 0.01) improved body mass (11%) and muscle mass (for the tibialis anterior and extensor digitorum longus by 19% and 41%) in the A17 mice treated with RK35 when compared to saline controls. Similarly, a significantly (P < 0.01) increased muscle strength (18% increase in maximal tetanic force) and myofibre diameter (17% and 44% for the tibialis anterior and extensor digitorum longus), and reduced expression of markers of muscle fibrosis (40% reduction in area of expression), was also observed. No change in the density of intranuclear inclusions (a hallmark of disease progression of OPMD) was however observed. Conclusions: Our study supports the clinical translation of such antibody-mediated inhibition of myostatin as a treatment of OPMD. This strategy has implications to be used as adjuvant therapies with gene therapy based approaches, or to stabilize the muscle prior to myoblast transplantation.

Published

2019

41. A multicenter comparison of quantification methods for antisense oligonucleotideinduced DMD exon 51 skipping in Duchenne muscular dystrophy cell cultures

Author

Nicole A. Datson, Pietro Spitali, Kamel Mamchaoui, Karen Anthony, Monika Hiller, Alessandra Ferlini, E. Ruiz-Del-Yerro, H. Osman, Linda Popplewell, George Dickson, Maria Sofia Falzarano, Ruurd C. Verheul, Valentina Sardone, Jelle J. Goeman, I. Garcia-Jimenez, Francesco Muntoni, Annemieke Aartsma-Rus, Virginia Arechavala-Gomeza, Leiden University Medical Center (LUMC), Università degli Studi di Ferrara (UniFE), Biocruces Bizkaia Health Research Institute [Baracaldo], Great Ormond Street Institute of Child Health [London, UK] (UCL), University College of London [London] (UCL), Royal Holloway [University of London] (RHUL), University of Northampton, Centre de Recherche en Myologie, Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU), Institut de Myologie, Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Association française contre les myopathies (AFM-Téléthon)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), Centre de recherche en Myologie – U974 SU-INSERM, and Centre National de la Recherche Scientifique (CNRS)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Association française contre les myopathies (AFM-Téléthon)-Sorbonne Université (SU)

Subjects

0301 basic medicine, Heredity, Genetic Linkage, Duchenne muscular dystrophy, lcsh:Medicine, cDNA synthesis, Artificial Gene Amplification and Extension, Biochemistry, Muscular Dystrophies, law.invention, Myoblasts, Dystrophin, Exon, 0302 clinical medicine, law, Medicine and Health Sciences, Computer software, Muscular dystrophy, lcsh:Science, Polymerase chain reaction, Multidisciplinary, biology, Exons, 3. Good health, Nucleic acids, Neurology, X-Linked Traits, Sex Linkage, RNA splicing, Nested polymerase chain reaction, Research Article, musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, RNA Splicing, Nucleic acid synthesis, Research and Analysis Methods, Transfection, NO, Cell Line, Electrophoretic Techniques, 03 medical and health sciences, Genetics, medicine, [SDV.MHEP.AHA]Life Sciences [q-bio]/Human health and pathology/Tissues and Organs [q-bio.TO], Humans, Chemical synthesis, RNA synthesis, Molecular Biology Techniques, Molecular Biology, Clinical Genetics, lcsh:R, Biology and Life Sciences, Proteins, Oligonucleotides, Antisense, medicine.disease, Gel electrophoresis, Molecular biology, Exon skipping, Muscular Dystrophy, Duchenne, Cytoskeletal Proteins, Biosynthetic techniques, 030104 developmental biology, biology.protein, RNA, lcsh:Q, 030217 neurology & neurosurgery

Abstract

Background: Duchenne muscular dystrophy is a lethal disease caused by lack of dystrophin. Skipping of exons adjacent to out-of-frame deletions has proven to restore dystrophin expression in Duchenne patients. Exon 51 has been the most studied target in both preclinical and clinical settings and the availability of standardized procedures to quantify exon skipping would be advantageous for the evaluation of preclinical and clinical data. Objective: To compare methods currently used to quantify antisense oligonucleotide–induced exon 51 skipping in the DMD transcript and to provide guidance about the method to use. Methods: Six laboratories shared blinded RNA samples from Duchenne patient-derived muscle cells treated with different amounts of exon 51 targeting antisense oligonucleotide. Exon 51 skipping levels were quantified using five different techniques: digital droplet PCR, single PCR assessed with Agilent bioanalyzer, nested PCR with agarose gel image analysis by either ImageJ or GeneTools software and quantitative real-time PCR. Results: Differences in mean exon skipping levels and dispersion around the mean were observed across the different techniques. Results obtained by digital droplet PCR were reproducible and showed the smallest dispersion. Exon skipping quantification with the other methods showed overestimation of exon skipping or high data variation. Conclusions: Our results suggest that digital droplet PCR was the most precise and quantitative method. The quantification of exon 51 skipping by Agilent bioanalyzer after a single round of PCR was the second-best choice with a 2.3-fold overestimation of exon 51 skipping levels compared to digital droplet PCR.

Published

2018

42. Antisense Oligonucleotide Targeting of 3'-UTR of mRNA for Expression Knockdown

Author

Golnoush, Golshirazi, Lukasz, Ciszewski, Ngoc, Lu-Nguyen, and Linda, Popplewell

Subjects

Homeodomain Proteins, Binding Sites, Muscle Fibers, Skeletal, Computational Biology, Oligonucleotides, Antisense, Muscle Development, Polyadenylation, Myoblasts, Gene Targeting, Rhabdomyosarcoma, Humans, Nucleic Acid Conformation, Gene Silencing, RNA, Messenger, Poly A, 3' Untranslated Regions, Protein Binding

Abstract

With the recent conditional approval of an antisense oligonucleotide (AON) that restores the reading frame of DMD transcript in a subset of Duchenne muscular dystrophy patients, it has been established that AONs sharing similar chemistry have clear clinical potential. Genetic diseases, such as facioscapulohumeral dystrophy (FSHD), can be the result of gain-of-function mutations. Since mRNA processing in terms of termination of transcription, its transport from the nucleus to the cytoplasm, its stability and translation efficiency are dependent on key 3'UTR elements, it follows that targeting these elements with AONs have the potential to induce gene silencing. Aberrant expression of the Double homeobox 4 (DUX4) transcription factor and the downstream consequences of such expression is the hallmark of FSHD. Here we describe the bioinformatic strategies behind the design of AONs targeting polyadenylation signals and the methodologies relevant to their in vitro screening for efficacy and safety, including analysis of expression at the transcript and protein level of the specific target and downstream genes, and measurement of the effect on the fusion index of myotubes. The targeting of permissive DUX4 and MSTN are used as examples. MSTN encodes for myostatin, a negative regulator of myogenesis; the downregulation of MSTN expression has the potential to address the muscular atrophy associated with muscular dystrophies, sarcopenia, cancer and acquired immunodeficiency syndrome.

Published

2018

43. Editorial of the Special Issue: Antisense Therapies

Author

Linda Popplewell

Subjects

0301 basic medicine, business.industry, MEDLINE, Medicine (miscellaneous), Bioinformatics, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Editorial, n/a, lcsh:Biology (General), 030220 oncology & carcinogenesis, Medicine, business, lcsh:QH301-705.5

Abstract

n/a

Published

2018

44. Targeting TGFβ Signaling to Address Fibrosis Using Antisense Oligonucleotides

Author

Heidi Carr, Linda Popplewell, Viktorija Cernisova, Ngoc Lu-Nguyen, Yee Leong, James T. March, and Golnoush Golshirazi

Subjects

0301 basic medicine, antisense oligonucleotide, Duchenne muscular dystrophy, Medicine (miscellaneous), Review, General Biochemistry, Genetics and Molecular Biology, Extracellular matrix, 03 medical and health sciences, Fibrosis, medicine, lcsh:QH301-705.5, transforming growth factor beta, Gene knockdown, biology, business.industry, fibrosis, Transforming growth factor beta, Spinal muscular atrophy, medicine.disease, Crosstalk (biology), 030104 developmental biology, lcsh:Biology (General), Cancer research, biology.protein, Signal transduction, business

Abstract

Fibrosis results from the excessive accumulation of extracellular matrix in chronically injured tissue. The fibrotic process is governed by crosstalk between many signaling pathways. The search for an effective treatment is further complicated by the fact that there is a degree of tissue-specificity in the pathways involved, although the process is not completely understood for all tissues. A plethora of drugs have shown promise in pre-clinical models, which is not always borne out translationally in clinical trial. With the recent approvals of two antisense oligonucleotides for the treatment of the genetic diseases Duchenne muscular dystrophy and spinal muscular atrophy, we explore here the potential of antisense oligonucleotides to knockdown the expression of pro-fibrotic proteins. We give an overview of the generalized fibrotic process, concentrating on key players and highlight where antisense oligonucleotides have been used effectively in cellular and animal models of different fibrotic conditions. Consideration is given to the advantages antisense oligonucleotides would have as an anti-fibrotic therapy alongside factors that would need to be addressed to improve efficacy. A prospective outlook for the development of antisense oligonucleotides to target fibrosis is outlined.

Published

2018

45. Antisense Oligonucleotide Targeting of 3’-UTR of mRNA for Expression Knockdown

Author

Linda Popplewell, Golnoush Golshirazi, Lukasz Ciszewski, and Ngoc Lu-Nguyen

Subjects

0301 basic medicine, Gene knockdown, biology, Myogenesis, Three prime untranslated region, Duchenne muscular dystrophy, Myostatin, 030105 genetics & heredity, medicine.disease, Cell biology, 03 medical and health sciences, 030104 developmental biology, DUX4, biology.protein, medicine, Gene silencing, Transcription factor

Abstract

With the recent conditional approval of an antisense oligonucleotide (AON) that restores the reading frame of DMD transcript in a subset of Duchenne muscular dystrophy patients, it has been established that AONs sharing similar chemistry have clear clinical potential. Genetic diseases, such as facioscapulohumeral dystrophy (FSHD), can be the result of gain-of-function mutations. Since mRNA processing in terms of termination of transcription, its transport from the nucleus to the cytoplasm, its stability and translation efficiency are dependent on key 3'UTR elements, it follows that targeting these elements with AONs have the potential to induce gene silencing. Aberrant expression of the Double homeobox 4 (DUX4) transcription factor and the downstream consequences of such expression is the hallmark of FSHD. Here we describe the bioinformatic strategies behind the design of AONs targeting polyadenylation signals and the methodologies relevant to their in vitro screening for efficacy and safety, including analysis of expression at the transcript and protein level of the specific target and downstream genes, and measurement of the effect on the fusion index of myotubes. The targeting of permissive DUX4 and MSTN are used as examples. MSTN encodes for myostatin, a negative regulator of myogenesis; the downregulation of MSTN expression has the potential to address the muscular atrophy associated with muscular dystrophies, sarcopenia, cancer and acquired immunodeficiency syndrome.

Published

2018

46. Combination Antisense Treatment for Destructive Exon Skipping of Myostatin and Open Reading Frame Rescue of Dystrophin in Neonatal mdx Mice

Author

Ngoc Lu-Nguyen, Amer F. Saleh, George Dickson, Linda Popplewell, Michael J. Gait, and Susan Jarmin

Subjects

Male, Reading Frames, Duchenne muscular dystrophy, Myostatin, Morpholinos, Muscle hypertrophy, Dystrophin, Mice, Exon, Drug Discovery, biology, Exons, musculoskeletal system, Molecular Medicine, Original Article, medicine.symptom, musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, government.form_of_government, Diaphragm, Arginine, Necrosis, Open Reading Frames, Internal medicine, Genetics, medicine, Animals, Muscle, Skeletal, Molecular Biology, Pharmacology, Antisense therapy, Muscle weakness, Genetic Therapy, Oligonucleotides, Antisense, medicine.disease, Molecular biology, Exon skipping, Mice, Inbred C57BL, Muscular Dystrophy, Duchenne, Alternative Splicing, Disease Models, Animal, Endocrinology, Animals, Newborn, Mice, Inbred mdx, biology.protein, government, Peptides

Abstract

The fatal X-linked Duchenne muscular dystrophy (DMD), characterized by progressive muscle wasting and muscle weakness, is caused by mutations within the DMD gene. The use of antisense oligonucleotides (AOs) modulating pre-mRNA splicing to restore the disrupted dystrophin reading frame, subsequently generating a shortened but functional protein has emerged as a potential strategy in DMD treatment. AO therapy has recently been applied to induce out-of-frame exon skipping of myostatin pre-mRNA, knocking-down expression of myostatin protein, and such an approach is suggested to enhance muscle hypertrophy/hyperplasia and to reduce muscle necrosis. Within this study, we investigated dual exon skipping of dystrophin and myostatin pre-mRNAs using phosphorodiamidate morpholino oligomers conjugated with an arginine-rich peptide (B-PMOs). Intraperitoneal administration of B-PMOs was performed in neonatal mdx males on the day of birth, and at weeks 3 and 6. At week 9, we observed in treated mice (as compared to age-matched, saline-injected controls) normalization of muscle mass, a recovery in dystrophin expression, and a decrease in muscle necrosis, particularly in the diaphragm. Our data provide a proof of concept for antisense therapy combining dystrophin restoration and myostatin inhibition for the treatment of DMD.

Published

2015

47. Nuclear poly(A)-binding protein aggregates misplace a pre-mRNA outside of SC35 speckle causing its abnormal splicing

Author

Bruno Bastide, Alberto Malerba, Vincent Mouly, George Dickson, Capucine Trollet, Fanny Roth, Sophie Périé, Jean Lacau St Guily, Teresa Gidaro, Linda Popplewell, Gillian Butler-Browne, Valérie Montel, Pierre Klein, Susan Jarmin, Michael Antoniou, Martine Oloko, Pierre de la Grange, Univ. Littoral Côte d’Opale, Univ. Artois, Université de Lille, Université Pierre et Marie Curie - Paris 6 [UPMC], Unité de Recherche Pluridisciplinaire Sport, Santé, Société (URePSSS) - ULR 7369 - ULR 4488 [URePSSS], Royal Holloway [University of London] [RHUL], CHU Pitié-Salpêtrière [AP-HP], Guy's Hospital [London], Centre de recherche en myologie, University of London [London], HAL UPMC, Gestionnaire, Centre de recherche en Myologie – U974 SU-INSERM, Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU), Unité de Recherche Pluridisciplinaire Sport, Santé, Société (URePSSS) - ULR 7369 - ULR 4488 (URePSSS), Université d'Artois (UA)-Université du Littoral Côte d'Opale (ULCO)-Université de Lille, Royal Holloway, School of Biological Sciences (ROYAL HOLLOWAY), Queen Mary University of London (QMUL), Oto-Rhino-Laryngologie Chirurgie cervico-faciale [CHU Tenon], CHU Tenon [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), GenoSplice technology, Incubateur et Pépinière d'Entreprises Paris-Salpêtrière (iPEPS-ICM), Université Pierre et Marie Curie - Paris 6 (UPMC)-Association française contre les myopathies (AFM-Téléthon)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Université d'Artois (UA)-Université de Lille-Université du Littoral Côte d'Opale (ULCO), Service d’ORL et de chirurgie cervico-faciale [CHU Tenon], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-CHU Tenon [AP-HP], Sorbonne Université (SU)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Sorbonne Université (SU), and GenoSplice [Paris]

Subjects

Adult, Male, 0301 basic medicine, Exonic splicing enhancer, Mice, Transgenic, RNA-binding protein, Biology, Splicing, Poly(A)-Binding Protein I, RNA Transport, Mice, Protein Aggregates, 03 medical and health sciences, Splicing factor, Exon, 0302 clinical medicine, SR protein, Muscular Dystrophy, Oculopharyngeal, Troponin T, Protein splicing, RNA Precursors, [SDV.BBM] Life Sciences [q-bio]/Biochemistry, Molecular Biology, Genetics, Animals, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Muscle, Skeletal, Aged, Aged, 80 and over, Aggregate, [SDV.MHEP] Life Sciences [q-bio]/Human health and pathology, Serine-Arginine Splicing Factors, Alternative splicing, Middle Aged, Molecular biology, Cell biology, Alternative Splicing, HEK293 Cells, 030104 developmental biology, Case-Control Studies, OPMD, RNA splicing, RNA, TNNT3, Female, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology, 030217 neurology & neurosurgery, 80 and over, Transgenic, Muscle, Skeletal, Muscular Dystrophy, Oculopharyngeal

Abstract

International audience; A short abnormal polyalanine expansion in the polyadenylate-binding protein nuclear-1 (PABPN1) protein causes oculopharyngeal muscular dystro-phy (OPMD). Mutated PABPN1 proteins accumulate as insoluble intranuclear aggregates in muscles of OPMD patients. While the roles of PABPN1 in nuclear polyadenylation and regulation of alternative poly(A) site choice have been established, the molecular mechanisms which trigger pathological defects in OPMD and the role of aggregates remain to be determined. Using exon array, for the first time we have identified several splicing defects in OPMD. In particular, we have demonstrated a defect in the splicing regulation of the muscle-specific Troponin T3 (TNNT3) mutually exclusive exons 16 and 17 in OPMD samples compared to controls. This splicing defect is directly linked to the SC35 (SRSF2) splicing factor and to the presence of nuclear aggregates. As reported here, PABPN1 aggregates are able to trap TNNT3 pre-mRNA, driving it outside nuclear speck-les, leading to an altered SC35-mediated splicing. This results in a decreased calcium sensitivity of muscle fibers, which could in turn plays a role in muscle pathology. We thus report a novel mechanism of alternative splicing deregulation that may play a role in various other diseases with nuclear inclusions or foci containing an RNA binding protein.

Published

2016

48. New developments in the use of gene therapy to treat Duchenne muscular dystrophy

Author

George Dickson, Linda Popplewell, Susan Jarmin, and Hanna Kymalainen

Subjects

musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, RNA Splicing, Duchenne muscular dystrophy, Genetic enhancement, Genetic Vectors, Clinical Biochemistry, Bioinformatics, Dystrophin, Mice, Open Reading Frames, 03 medical and health sciences, Exon, Clinical Trials, Phase II as Topic, 0302 clinical medicine, Genome editing, Drug Discovery, medicine, Animals, Humans, Transgenes, Muscular dystrophy, Wasting, 030304 developmental biology, Pharmacology, Genetics, 0303 health sciences, business.industry, Gene Transfer Techniques, Exons, Genetic Therapy, Dependovirus, Oligonucleotides, Antisense, medicine.disease, Exon skipping, 3. Good health, Muscular Dystrophy, Duchenne, Clinical trial, Phenotype, Clinical Trials, Phase III as Topic, Mutation, Codon, Terminator, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Duchenne muscular dystrophy (DMD) is a lethal X-linked inherited disorder characterised by progressive muscle weakness, wasting and degeneration. Although the gene affected in DMD was identified over 25 years ago, there is still no effective treatment.Here we review some of the genetic-based strategies aimed at amelioration of the DMD phenotype. A number of Phase II/III clinical trials of antisense oligonucleotide-induced exon skipping for restoration of the open reading frame (ORF) of the DMD gene have recently been completed. The potential strategies for overcoming the hurdles that appear to prevent exon skipping becoming an effective treatment for DMD currently are discussed.The applicability of exon skipping as a therapy to DMD is restricted and the development of alternative strategies that are more encompassing is needed. The rapid pre-clinical advances that are being made in the field of adeno-associated virus (AAV)-based delivery of micro-dystrophin would address this. The obstacles to be faced with gene replacement strategies would include the need for high viral titres, efficient muscle targeting and avoidance of immune response to vector and transgene. The new emerging field of gene editing could potentially provide permanent correction of the DMD gene and the feasibility of such an approach to DMD is discussed.

Published

2013

49. Gene Correction of a Duchenne Muscular Dystrophy Mutation by Meganuclease-Enhanced Exon Knock-In

Author

Frédéric Pâques, Taeyoung Koo, Thomas Voit, Linda Popplewell, Vincent Mouly, Kamel Mamchaoui, Olga Isman, Agnès Gouble, Xavier Leclerc, George Dickson, Frédéric Cédrone, Rafael J. Yáñez-Muñoz, and Aymeric Duclert

Subjects

musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, DNA Repair, Duchenne muscular dystrophy, Genetic enhancement, Blotting, Western, Genetic Vectors, Biology, Myoblasts, Exon, INDEL Mutation, Gene knockin, Genetics, medicine, Humans, Gene Knock-In Techniques, Muscular dystrophy, Molecular Biology, Gene, Deoxyribonucleases, Lentivirus, High-Throughput Nucleotide Sequencing, Exons, Genetic Therapy, Oligonucleotides, Antisense, medicine.disease, Molecular biology, Muscular Dystrophy, Duchenne, Mutation, Meganuclease, Molecular Medicine, Targeted Gene Repair, Minigene

Abstract

Duchenne muscular dystrophy (DMD) is a severe inherited, muscle-wasting disorder caused by mutations in the DMD gene. Gene therapy development for DMD has concentrated on vector-based DMD minigene transfer, cell-based gene therapy using genetically modified adult muscle stem cells or healthy wild-type donor cells, and antisense oligonucleotide-induced exon-skipping therapy to restore the reading frame of the mutated DMD gene. This study is an investigation into DMD gene targeting-mediated correction of deletions in human patient myoblasts using a target-specific meganuclease (MN) and a homologous recombination repair matrix. The MN was designed to cleave within DMD intron 44, upstream of a deletion hotspot, and integration-competent lentiviral vectors expressing the nuclease (LVcMN) were generated. MN western blotting and deep gene sequencing for LVcMN-induced non-homologous end-joining InDels (microdeletions or microinsertions) confirmed efficient MN expression and activity in transduced DMD myoblasts. A homologous repair matrix carrying exons 45-52 (RM45-52) was designed and packaged into integration-deficient lentiviral vectors (IDLVs; LVdRM45-52). After cotransduction of DMD myoblasts harboring a deletion of exons 45 to 52 with LVcMN and LVdRM45-52 vectors, targeted knock-in of the RM45-52 region in the correct location in DMD intron 44, and expression of full-length, correctly spliced wild-type dystrophin mRNA containing exons 45-52 were observed. This work demonstrates that genome surgery on human DMD gene mutations can be achieved by MN-induced locus-specific genome cleavage and homologous recombination knock-in of deleted exons. The feasibility of human DMD gene repair in patient myoblasts has exciting therapeutic potential.

Published

2016

50. Genetic Therapeutic Approaches for Duchenne Muscular Dystrophy

Author

George Dickson, Linda Popplewell, and Helen Foster

Subjects

musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Transgene, Duchenne muscular dystrophy, Genetic Vectors, Nonsense mutation, Bioinformatics, Dystrophin, 03 medical and health sciences, 0302 clinical medicine, Genome editing, Utrophin, Genetics, medicine, Animals, Humans, Muscular dystrophy, Molecular Biology, 030304 developmental biology, Clinical Trials as Topic, 0303 health sciences, biology, Genetic Therapy, Dependovirus, medicine.disease, Exon skipping, 3. Good health, Muscular Dystrophy, Duchenne, Mutation, biology.protein, Cancer research, Molecular Medicine, 030217 neurology & neurosurgery

Abstract

Despite an expansive wealth of research following the discovery of the DMD gene 25 years ago, there is still no curative treatment for Duchenne muscular dystrophy. However, there are currently many promising lines of research, including cell-based therapies and pharmacological reagents to upregulate dystrophin via readthrough of nonsense mutations or by upregulation of the dystrophin homolog utrophin. Here we review genetic-based therapeutic strategies aimed at the amelioration of the DMD phenotype. These include the reintroduction of a copy of the DMD gene into an affected tissue by means of a viral vector; correction of the mutated DMD transcript by antisense oligonucleotide-induced exon skipping to restore the open reading frame; and direct modification of the DMD gene at a chromosomal level through genome editing. All these approaches are discussed in terms of the more recent advances, and the hurdles to be overcome if a comprehensive and effective treatment for DMD is to be found. These hurdles include the need to target all musculature of the body. Therefore any potential treatment would need to be administered systemically. In addition, any treatment needs to have a long-term effect, with the possibility of readministration, while avoiding any potentially detrimental immune response to the vector or transgene.

Published

2012