Your search keyword '"Harriet P Lo"' showing total 15 results

1. Cavin3 released from caveolae interacts with BRCA1 to regulate the cellular stress response

Author

Kerrie-Ann McMahon, David A Stroud, Yann Gambin, Vikas Tillu, Michele Bastiani, Emma Sierecki, Mark E Polinkovsky, Thomas E Hall, Guillermo A Gomez, Yeping Wu, Marie-Odile Parat, Nick Martel, Harriet P Lo, Kum Kum Khanna, Kirill Alexandrov, Roger Daly, Alpha Yap, Michael T Ryan, and Robert G Parton

Subjects

BRCA1, breast cancer, caveolae, cavin proteins, Medicine, Science, Biology (General), QH301-705.5

Abstract

Caveolae-associated protein 3 (cavin3) is inactivated in most cancers. We characterized how cavin3 affects the cellular proteome using genome-edited cells together with label-free quantitative proteomics. These studies revealed a prominent role for cavin3 in DNA repair, with BRCA1 and BRCA1 A-complex components being downregulated on cavin3 deletion. Cellular and cell-free expression assays revealed a direct interaction between BRCA1 and cavin3 that occurs when cavin3 is released from caveolae that are disassembled in response to UV and mechanical stress. Overexpression and RNAi-depletion revealed that cavin3 sensitized various cancer cells to UV-induced apoptosis. Supporting a role in DNA repair, cavin3-deficient cells were sensitive to PARP inhibition, where concomitant depletion of 53BP1 restored BRCA1-dependent sensitivity to PARP inhibition. We conclude that cavin3 functions together with BRCA1 in multiple cancer-related pathways. The loss of cavin3 function may provide tumor cell survival by attenuating apoptotic sensitivity and hindering DNA repair under chronic stress conditions.

Published

2021

2. In vivo proteomic mapping through GFP-directed proximity-dependent biotin labelling in zebrafish

Author

Zherui Xiong, Harriet P Lo, Kerrie-Ann McMahon, Nick Martel, Alun Jones, Michelle M Hill, Robert G Parton, and Thomas E Hall

Subjects

in vivo proteomics, BioID, GFP-binding nanobody, proximity-dependent biotin labelling, cavins, Medicine, Science, Biology (General), QH301-705.5

Abstract

Protein interaction networks are crucial for complex cellular processes. However, the elucidation of protein interactions occurring within highly specialised cells and tissues is challenging. Here, we describe the development, and application, of a new method for proximity-dependent biotin labelling in whole zebrafish. Using a conditionally stabilised GFP-binding nanobody to target a biotin ligase to GFP-labelled proteins of interest, we show tissue-specific proteomic profiling using existing GFP-tagged transgenic zebrafish lines. We demonstrate the applicability of this approach, termed BLITZ (Biotin Labelling In Tagged Zebrafish), in diverse cell types such as neurons and vascular endothelial cells. We applied this methodology to identify interactors of caveolar coat protein, cavins, in skeletal muscle. Using this system, we defined specific interaction networks within in vivo muscle cells for the closely related but functionally distinct Cavin4 and Cavin1 proteins.

Published

2021

3. MURC/cavin-4 Is Co-Expressed with Caveolin-3 in Rhabdomyosarcoma Tumors and Its Silencing Prevents Myogenic Differentiation in the Human Embryonal RD Cell Line.

Author

Fiorella Faggi, Silvia Codenotti, Pietro Luigi Poliani, Manuela Cominelli, Nicola Chiarelli, Marina Colombi, Marika Vezzoli, Eugenio Monti, Federica Bono, Giovanni Tulipano, Chiara Fiorentini, Alessandra Zanola, Harriet P Lo, Robert G Parton, Charles Keller, and Alessandro Fanzani

Subjects

Medicine, Science

Abstract

The purpose of this study was to investigate whether MURC/cavin-4, a plasma membrane and Z-line associated protein exhibiting an overlapping distribution with Caveolin-3 (Cav-3) in heart and muscle tissues, may be expressed and play a role in rhabdomyosarcoma (RMS), an aggressive myogenic tumor affecting childhood. We found MURC/cavin-4 to be expressed, often concurrently with Cav-3, in mouse and human RMS, as demonstrated through in silico analysis of gene datasets and immunohistochemical analysis of tumor samples. In vitro expression studies carried out using human cell lines and primary mouse tumor cultures showed that expression levels of both MURC/cavin-4 and Cav-3, while being low or undetectable during cell proliferation, became robustly increased during myogenic differentiation, as detected via semi-quantitative RT-PCR and immunoblotting analysis. Furthermore, confocal microscopy analysis performed on human RD and RH30 cell lines confirmed that MURC/cavin-4 mostly marks differentiated cell elements, colocalizing at the cell surface with Cav-3 and labeling myosin heavy chain (MHC) expressing cells. Finally, MURC/cavin-4 silencing prevented the differentiation in the RD cell line, leading to morphological cell impairment characterized by depletion of myogenin, Cav-3 and MHC protein levels. Overall, our data suggest that MURC/cavin-4, especially in combination with Cav-3, may play a consistent role in the differentiation process of RMS.

Published

2015

4. Endocytic crosstalk: cavins, caveolins, and caveolae regulate clathrin-independent endocytosis.

Author

Natasha Chaudhary, Guillermo A Gomez, Mark T Howes, Harriet P Lo, Kerrie-Ann McMahon, James A Rae, Nicole L Schieber, Michelle M Hill, Katharina Gaus, Alpha S Yap, and Robert G Parton

Subjects

Biology (General), QH301-705.5

Abstract

Several studies have suggested crosstalk between different clathrin-independent endocytic pathways. However, the molecular mechanisms and functional relevance of these interactions are unclear. Caveolins and cavins are crucial components of caveolae, specialized microdomains that also constitute an endocytic route. Here we show that specific caveolar proteins are independently acting negative regulators of clathrin-independent endocytosis. Cavin-1 and Cavin-3, but not Cavin-2 or Cavin-4, are potent inhibitors of the clathrin-independent carriers/GPI-AP enriched early endosomal compartment (CLIC/GEEC) endocytic pathway, in a process independent of caveola formation. Caveolin-1 (CAV1) and CAV3 also inhibit the CLIC/GEEC pathway upon over-expression. Expression of caveolar protein leads to reduction in formation of early CLIC/GEEC carriers, as detected by quantitative electron microscopy analysis. Furthermore, the CLIC/GEEC pathway is upregulated in cells lacking CAV1/Cavin-1 or with reduced expression of Cavin-1 and Cavin-3. Inhibition by caveolins can be mimicked by the isolated caveolin scaffolding domain and is associated with perturbed diffusion of lipid microdomain components, as revealed by fluorescence recovery after photobleaching (FRAP) studies. In the absence of cavins (and caveolae) CAV1 is itself endocytosed preferentially through the CLIC/GEEC pathway, but the pathway loses polarization and sorting attributes with consequences for membrane dynamics and endocytic polarization in migrating cells and adult muscle tissue. We also found that noncaveolar Cavin-1 can act as a modulator for the activity of the key regulator of the CLIC/GEEC pathway, Cdc42. This work provides new insights into the regulation of noncaveolar clathrin-independent endocytosis by specific caveolar proteins, illustrating multiple levels of crosstalk between these pathways. We show for the first time a role for specific cavins in regulating the CLIC/GEEC pathway, provide a new tool to study this pathway, identify caveola-independent functions of the cavins and propose a novel mechanism for inhibition of the CLIC/GEEC pathway by caveolin.

Published

2014

5. High-throughput screening of Australian marine organism extracts for bioactive molecules affecting the cellular storage of neutral lipids.

Author

James Rae, Frank Fontaine, Angela A Salim, Harriet P Lo, Robert J Capon, Robert G Parton, and Sally Martin

Subjects

Medicine, Science

Abstract

Mammalian cells store excess fatty acids as neutral lipids in specialised organelles called lipid droplets (LDs). Using a simple cell-based assay and open-source software we established a high throughput screen for LD formation in A431 cells in order to identify small bioactive molecules affecting lipid storage. Screening an n-butanol extract library from Australian marine organisms we identified 114 extracts that produced either an increase or a decrease in LD formation in fatty acid-treated A431 cells with varying degrees of cytotoxicity. We selected for further analysis a non-cytotoxic extract derived from the genus Spongia (Heterofibria). Solvent partitioning, HPLC fractionation and spectroscopic analysis (NMR, MS) identified a family of related molecules within this extract with unique structural features, a subset of which reduced LD formation. We selected one of these molecules, heterofibrin A1, for more detailed cellular analysis. Inhibition of LD biogenesis by heterofibrin A1 was observed in both A431 cells and AML12 hepatocytes. The activity of heterofibrin A1 was dose dependent with 20 µM inhibiting LD formation and triglyceride accumulation by ∼50% in the presence of 50 µM oleic acid. Using a fluorescent fatty acid analogue we found that heterofibrin A1 significantly reduces the intracellular accumulation of fatty acids and results in the formation of distinct fatty acid metabolites in both cultured cells and in embryos of the zebrafish Danio rerio. In summary we have shown using readily accessible software and a relatively simple assay system that we can identify and isolate bioactive molecules from marine extracts, which affect the formation of LDs and the metabolism of fatty acids both in vitro and in vivo.

Published

2011

6. In vivo cell biological screening identifies an endocytic capture mechanism for T-tubule formation

Author

Thomas E. Hall, Nick Martel, Nicholas Ariotti, Zherui Xiong, Harriet P. Lo, Charles Ferguson, James Rae, Ye-Wheen Lim, and Robert G. Parton

Subjects

Science

Abstract

It is unclear how the T-tubule structure of skeletal muscle, which regulates coordinated muscle contraction, forms. Here, the authors develop a four-dimensional quantitative model for T-tubule formation in zebrafish, based on live imaging, proposing a dynamic endocytic capture model.

Published

2020

7. Caveolin-1 Is Necessary for Hepatic Oxidative Lipid Metabolism: Evidence for Crosstalk between Caveolin-1 and Bile Acid Signaling

Author

Manuel A. Fernández-Rojo, Milena Gongora, Rebecca L. Fitzsimmons, Nick Martel, Sheree D. Martin, Susan J. Nixon, Andrew J. Brooks, Maria P. Ikonomopoulou, Sally Martin, Harriet P. Lo, Stephen A. Myers, Christina Restall, Charles Ferguson, Paul F. Pilch, Sean L. McGee, Robin L. Anderson, Michael J. Waters, John F. Hancock, Sean M. Grimmond, George E.O. Muscat, and Robert G. Parton

Subjects

Biology (General), QH301-705.5

Abstract

Caveolae and caveolin-1 (CAV1) have been linked to several cellular functions. However, a model explaining their roles in mammalian tissues in vivo is lacking. Unbiased expression profiling in several tissues and cell types identified lipid metabolism as the main target affected by CAV1 deficiency. CAV1−/− mice exhibited impaired hepatic peroxisome proliferator-activated receptor α (PPARα)-dependent oxidative fatty acid metabolism and ketogenesis. Similar results were recapitulated in CAV1-deficient AML12 hepatocytes, suggesting at least a partial cell-autonomous role of hepatocyte CAV1 in metabolic adaptation to fasting. Finally, our experiments suggest that the hepatic phenotypes observed in CAV1−/− mice involve impaired PPARα ligand signaling and attenuated bile acid and FXRα signaling. These results demonstrate the significance of CAV1 in (1) hepatic lipid homeostasis and (2) nuclear hormone receptor (PPARα, FXRα, and SHP) and bile acid signaling.

Published

2013

8. Caveolae sense oxidative stress through membrane lipid peroxidation and cytosolic release of CAVIN1 to regulate NRF2

Author

Yeping Wu, Ye-Wheen Lim, David A. Stroud, Nick Martel, Thomas E. Hall, Harriet P. Lo, Charles Ferguson, Michael T. Ryan, Kerrie-Ann McMahon, and Robert G. Parton

Subjects

Cell Biology, Molecular Biology, General Biochemistry, Genetics and Molecular Biology, Developmental Biology

Published

2023

9. Mechanoprotection by skeletal muscle caveolae

Author

Robert G. Parton, Harriet P. Lo, and Thomas E. Hall

Subjects

0301 basic medicine, Cell type, Sarcolemma, Skeletal muscle, Cell Biology, General Medicine, Biology, biology.organism_classification, Cell biology, T-tubule, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Membrane, Structural Biology, Caveolae, medicine, Membrane activity, Zebrafish, 030217 neurology & neurosurgery

Abstract

Caveolae, small bulb-like pits, are the most abundant surface feature of many vertebrate cell types. The relationship of the structure of caveolae to their function has been a subject of considerable scientific interest in view of the association of caveolar dysfunction with human disease. In a recent study Lo et al.1 investigated the organization and function of caveolae in skeletal muscle. Using quantitative 3D electron microscopy caveolae were shown to be predominantly organized into multilobed structures which provide a large reservoir of surface-connected membrane underlying the sarcolemma. These structures were preferentially disassembled in response to changes in membrane tension. Perturbation or loss of caveolae in mouse and zebrafish models suggested that caveolae can protect the muscle sarcolemma against damage in response to excessive membrane activity. Flattening of caveolae to release membrane into the bulk plasma membrane in response to increased membrane tension can allow cell shape...

Published

2016

10. The caveolin–cavin system plays a conserved and critical role in mechanoprotection of skeletal muscle

Author

Thomas E. Hall, Matthias Floetenmeyer, Michele Bastiani, Charles Ferguson, Nicole L. Schieber, Nick Martel, Paul F. Pilch, Jocelyn Laporte, Garry Morgan, Susan J. Nixon, Harriet P. Lo, Belinda S. Cowling, Manuel A. Fernandez-Rojo, and Robert G. Parton

Subjects

Electron Microscope Tomography, endocrine system, animal structures, Immunology, Molecular Sequence Data, Muscle Fibers, Skeletal, Biology, Motor Activity, Caveolins, Mechanotransduction, Cellular, Muscular Dystrophies, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Sarcolemma, Caveolae, Caveolin, medicine, Immunology and Allergy, Animals, Muscular dystrophy, Myopathy, Zebrafish, Research Articles, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Skeletal muscle, Membrane Proteins, RNA-Binding Proteins, Cell Biology, medicine.disease, Molecular biology, Cell biology, Mice, Inbred C57BL, medicine.anatomical_structure, Membrane protein, Commentary, Stress, Mechanical, medicine.symptom, 030217 neurology & neurosurgery, Cavin

Abstract

The caveolar membrane microdomain plays an integral role in stabilizing the muscle fiber surface in mice and zebrafish., Dysfunction of caveolae is involved in human muscle disease, although the underlying molecular mechanisms remain unclear. In this paper, we have functionally characterized mouse and zebrafish models of caveolae-associated muscle disease. Using electron tomography, we quantitatively defined the unique three-dimensional membrane architecture of the mature muscle surface. Caveolae occupied around 50% of the sarcolemmal area predominantly assembled into multilobed rosettes. These rosettes were preferentially disassembled in response to increased membrane tension. Caveola-deficient cavin-1−/− muscle fibers showed a striking loss of sarcolemmal organization, aberrant T-tubule structures, and increased sensitivity to membrane tension, which was rescued by muscle-specific Cavin-1 reexpression. In vivo imaging of live zebrafish embryos revealed that loss of muscle-specific Cavin-1 or expression of a dystrophy-associated Caveolin-3 mutant both led to sarcolemmal damage but only in response to vigorous muscle activity. Our findings define a conserved and critical role in mechanoprotection for the unique membrane architecture generated by the caveolin–cavin system.

Published

2015

11. MURC/Cavin-4 and cavin family members form tissue-specific caveolar complexes

Author

Michelle M. Hill, Piers J. Walser, Michele Bastiani, Susan J. Nixon, Paul F. Pilch, Mark P. Jedrychowski, Manuel A. Fernandez-Rojo, John F. Hancock, Kathryn N. North, Daniel Abankwa, Jørgen Vinten, Libin Liu, Harriet P. Lo, Steven P. Gygi, Michael R. Breen, Robert G. Parton, and Robert Luetterforst

Subjects

Multiprotein complex, Recombinant Fusion Proteins, Molecular Sequence Data, Muscle Proteins, Biology, Caveolae, Caveolins, Article, Gene product, Mice, 03 medical and health sciences, Sarcolemma, 0302 clinical medicine, Muscular Diseases, PTRF, 3T3-L1 Cells, Caveolin, Animals, Humans, Protein Isoforms, Amino Acid Sequence, Phylogeny, Research Articles, 030304 developmental biology, Mice, Knockout, 0303 health sciences, Binding protein, Membrane Proteins, RNA-Binding Proteins, Cell Biology, Cell biology, Membrane protein, Biochemistry, Multiprotein Complexes, Sequence Alignment, 030217 neurology & neurosurgery, Cavin

Abstract

Polymerase I and transcript release factor (PTRF)/Cavin is a cytoplasmic protein whose expression is obligatory for caveola formation. Using biochemistry and fluorescence resonance energy transfer–based approaches, we now show that a family of related proteins, PTRF/Cavin-1, serum deprivation response (SDR)/Cavin-2, SDR-related gene product that binds to C kinase (SRBC)/Cavin-3, and muscle-restricted coiled-coil protein (MURC)/Cavin-4, forms a multiprotein complex that associates with caveolae. This complex can constitutively assemble in the cytosol and associate with caveolin at plasma membrane caveolae. Cavin-1, but not other cavins, can induce caveola formation in a heterologous system and is required for the recruitment of the cavin complex to caveolae. The tissue-restricted expression of cavins suggests that caveolae may perform tissue-specific functions regulated by the composition of the cavin complex. Cavin-4 is expressed predominantly in muscle, and its distribution is perturbed in human muscle disease associated with Caveolin-3 dysfunction, identifying Cavin-4 as a novel muscle disease candidate caveolar protein.

Published

2009

12. Muscular dystrophy associated with α-dystroglycan deficiency in Sphynx and Devon Rex cats

Author

G. Diane Shelton, Eva Engvall, Ling T. Guo, Leslie A. Lyons, Paul T. Martin, Beverly K. Sturges, Rui Xu, Harriet P. Lo, Peter J Dickinson, Richard A Lecouteur, Richard Malik, Kathryn N. North, and Robert A. Grahn

Subjects

Male, musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Glycosylation, animal structures, Biopsy, Immunoblotting, biology.animal_breed, Fluorescent Antibody Technique, Polymerase Chain Reaction, Article, Laminin, Lectins, Internal medicine, medicine, Dystroglycan, Animals, Muscular dystrophy, Dystroglycans, Muscle, Skeletal, Myopathy, Genetics (clinical), Sphynx cat, Muscle Weakness, CATS, biology, Muscle weakness, Muscular Dystrophy, Animal, medicine.disease, Disease Models, Animal, Endocrinology, Neurology, Pediatrics, Perinatology and Child Health, Immunology, Cats, biology.protein, Female, Neurology (clinical), medicine.symptom, Dystrophin

Abstract

Recent studies have identified a number of forms of muscular dystrophy, termed dystroglycanopathies, which are associated with loss of natively glycosylated alpha-dystroglycan. Here we identify a new animal model for this class of disorders in Sphynx and Devon Rex cats. Affected cats displayed a slowly progressive myopathy with clinical and histologic hallmarks of muscular dystrophy including skeletal muscle weakness with no involvement of peripheral nerves or CNS. Skeletal muscles had myopathic features and reduced expression of alpha-dystroglycan, while beta-dystroglycan, sarcoglycans, and dystrophin were expressed at normal levels. In the Sphynx cat, analysis of laminin and lectin binding capacity demonstrated no loss in overall glycosylation or ligand binding for the alpha-dystroglycan protein, only a loss of protein expression. A reduction in laminin-alpha2 expression in the basal lamina surrounding skeletal myofibers was also observed. Sequence analysis of translated regions of the feline dystroglycan gene (DAG1) in affected cats did not identify a causative mutation, and levels of DAG1 mRNA determined by real-time QRT-PCR did not differ significantly from normal controls. Reduction in the levels of glycosylated alpha-dystroglycan by immunoblot was also identified in an affected Devon Rex cat. These data suggest that muscular dystrophy in Sphynx and Devon Rex cats results from a deficiency in alpha-dystroglycan protein expression, and as such may represent a new type of dystroglycanopathy where expression, but not glycosylation, is affected.

Published

2008

13. Changes in skeletal muscle expression of AQP1 and AQP4 in dystrophinopathy and dysferlinopathy patients

Author

Sandra T. Cooper, Kathryn N. North, Harriet P. Lo, Jonathan R. Egan, Tanya L. Butler, Carol G. Au, David S. Winlaw, and Alison G. Compton

Subjects

Adult, Male, musculoskeletal diseases, Dysferlinopathy, Pathology, medicine.medical_specialty, Adolescent, Duchenne muscular dystrophy, Blotting, Western, Down-Regulation, Gene Expression, Muscle Proteins, Pathology and Forensic Medicine, Dystrophin, Dysferlin, Cellular and Molecular Neuroscience, Humans, Medicine, Muscular dystrophy, Child, Muscle, Skeletal, Syntrophin, Aquaporin 4, Aquaporin 1, biology, Reverse Transcriptase Polymerase Chain Reaction, business.industry, Calcium-Binding Proteins, Infant, Membrane Proteins, Middle Aged, medicine.disease, Immunohistochemistry, Molecular biology, Muscular Dystrophy, Duchenne, Muscular Dystrophies, Limb-Girdle, Child, Preschool, biology.protein, Female, sense organs, Neurology (clinical), business, ITGA7, Limb-girdle muscular dystrophy

Abstract

Transmembrane water transport is mediated by aquaporins (AQPs), of which AQP1 and AQP4 are expressed in skeletal muscle. AQP4 expression is reduced in Duchenne muscular dystrophy (DMD) patients, and is reported to correlate with decreased alpha1-syntrophin and altered osmotic permeability. In this study, we assessed the relationship between AQP1, AQP4, dystrophin and alpha1-syntrophin in dystrophinopathy and dysferlinopathy patients. Muscle biopsies of patients with DMD (n = 8) and limb-girdle muscular dystrophy type 2B (LGMD2B; n = 5) were screened for AQP1 and AQP4 expression by real-time quantitative RT-PCR or Western blot and immunohistochemistry. AQP expression was further analyzed in primary myotubes derived from DMD and LGMD2B patients by cell culture and immunohistochemistry. AQP1 transcript and protein expression was significantly elevated in DMD biopsies, and was localized to the sarcolemma of muscle fibers and endothelia of muscle capillaries. AQP4 was significantly reduced despite normal dystrophin and alpha1-syntrophin in dysferlinopathy patients, while expression of AQP1 was variably upregulated. Expression of AQP1 and AQP4 was normal in patient-derived primary myotubes, suggesting that altered AQPs observed in biopsies are likely secondary to the dystrophic process. Our study shows that AQP4 downregulation can occur in muscular dystrophies with either normal or disrupted expression of dystrophin-associated proteins, and that this might be associated with upregulation of AQP1.

Published

2008

14. Dystrophinopathy carrier determination and detection of protein deficiencies in muscular dystrophy using lentiviral MyoD-forced myogenesis

Author

Eddy Kizana, Zhan He Wu, Sandra T. Cooper, Kathryn N. North, Harriet P. Lo, Nan Yang, Ian E. Alexander, and Jonathon D. Yates

Subjects

Male, Time Factors, Duchenne muscular dystrophy, DNA Mutational Analysis, Muscle Development, Muscular Dystrophies, Dystrophin, Dysferlin, Transduction, Genetic, Protein Deficiency, Utrophin, medicine, Humans, Actinin, RNA, Messenger, Muscular dystrophy, Cells, Cultured, Genetics (clinical), MyoD Protein, Genetics, biology, Reverse Transcriptase Polymerase Chain Reaction, Myogenesis, Lentivirus, Cell Differentiation, Fibroblasts, musculoskeletal system, medicine.disease, Cell biology, Neurology, Mutation, Pediatrics, Perinatology and Child Health, biology.protein, Female, Neurology (clinical), Chorionic Villi, ITGA7, Limb-girdle muscular dystrophy

Abstract

The objective of this study is to expand the applications of MyoD-forced myogenesis for research and diagnosis of human muscle disorders using a lentiviral vector (LVhMyoD) for efficient trans-differentiation of patient primary cells. LVhMyoD transduced cells readily formed striated, multinucleate myotubes expressing a wide range of genes associated with muscular dystrophy (dystrophin, dysferlin, sarcoglycans, caveolin-3) and congenital myopathy (nebulin, actin, desmin, tropomyosin, troponin). We demonstrate that MyoD gene-modified fibroblasts reproduce protein deficiencies associated with different forms of muscular dystrophy, and confirm that LVhMyoD gene-modified chorionic villus can be used successfully to determine the dystrophin status of the developing fetus, augmenting prenatal diagnosis of dystrophinopathy patients. Using muscle-specific cDNA derived from LVhMyoD gene-modified patient cells, we identified a female carrier bearing a large dystrophin deletion and a previously unidentified non-coding splice-site mutation within dystrophin in a Becker muscular dystrophy patient. This study highlights the significant potential of lentiviral MyoD-forced myogenesis for study of a wide range of human muscle disorders; a field constrained by the limited availability of human tissue. LVhMyoD gene-modified patient cells provide a renewable source of mutant protein and muscle-specific mRNA, facilitating accelerated mutation screening of large genes, molecular analyses of splicing abnormalities and study of disease-causing mutations.

Published

2007

15. Rippling muscle disease

Author

Bruce Day, Harriet P. Lo, Helene Roberts, Catriona McLean, and Kathryn N. North

Subjects

Pathology, medicine.medical_specialty, Caveolin 3, business.industry, Rippling muscle disease, Point mutation, General Medicine, Middle Aged, Muscle Rigidity, Clinical neurology, Muscular Diseases, Neurology, Physiology (medical), Mutation (genetic algorithm), Humans, Point Mutation, Medicine, Female, Surgery, Neurology (clinical), business

Abstract

A case of rippling muscle disease is presented and features of this rare condition, and its association with caveolin-3 are discussed.

Published

2006