22 results on '"Babbs, Arran"'
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2. Micro-utrophin Improves Cardiac and Skeletal Muscle Function of Severely Affected D2/mdx Mice
3. Engineering Multiple U7snRNA Constructs to Induce Single and Multiexon-skipping for Duchenne Muscular Dystrophy
4. The Cellular Processing Capacity Limits the Amounts of Chimeric U7 snRNA Available for Antisense Delivery
5. A Dominant Mutation in Snap25 Causes Impaired Vesicle Trafficking, Sensorimotor Gating, and Ataxia in the Blind-Drunk Mouse
6. Functional correction in mouse models of muscular dystrophy using exon-skipping tricyclo-DNA oligomers
7. Prevention of Dystrophic Pathology in Severely Affected Dystrophin/Utrophin-deficient Mice by Morpholino-oligomer-mediated Exon-skipping
8. Second-generation compound for the modulation of utrophin in the therapy of DMD
9. Rescue of severely affected dystrophin/utrophin-deficient mice through scAAV-U7snRNA-mediated exon skipping
10. Diaphragm rescue alone prevents heart dysfunction in dystrophic mice
11. From diagnosis to therapy in Duchenne muscular dystrophy
12. 2-Arylbenzo[d]oxazole Phosphinate Esters as Second-Generation Modulators of Utrophin for the Treatment of Duchenne Muscular Dystrophy
13. The potential of utrophin and dystrophin combination therapies for Duchenne muscular dystrophy
14. Embryonic myosin is a regeneration marker to monitor utrophin-based therapies for DMD
15. potential of utrophin and dystrophin combination therapies for Duchenne muscular dystrophy.
16. Identification of serum protein biomarkers for utrophin based DMD therapy
17. Embryonic myosin is a regeneration marker to monitor utrophin-based therapies for DMD.
18. Temporal transcriptomics suggest that twin-peaking genes reset the clock
19. Author response: Temporal transcriptomics suggest that twin-peaking genes reset the clock
20. Diaphragm rescue alone prevents heart dysfunction in dystrophic mice
21. Enhanced Exon-skipping Induced by U7 snRNA Carrying a Splicing Silencer Sequence: Promising Tool for DMD Therapy
22. 2-Arylbenzo[ d ]oxazole Phosphinate Esters as Second-Generation Modulators of Utrophin for the Treatment of Duchenne Muscular Dystrophy.
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