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1. Genetically encoded redox sensor identifies the role of ROS in degenerative and mitochondrial disease pathogenesis

2. Modes of metabolic compensation during mitochondrial disease using the drosophila model of ATP6 dysfunction

3. Protein coding mitochondrial-targeted RNAs rescue mitochondrial disease in vivo.

4. A conserved polybasic domain mediates plasma membrane targeting of Lgl and its regulation by hypoxia.

5. Small mitochondrial-targeted RNAs modulate endogenous mitochondrial protein expression in vivo.

6. Evidence of a triosephosphate isomerase non-catalytic function crucial to behavior and longevity.

7. A novel Drosophila SOD2 mutant demonstrates a role for mitochondrial ROS in neurodevelopment and disease.

8. Genetically encoded redox sensor identifies the role of ROS in degenerative and mitochondrial disease pathogenesis.

9. Modes of metabolic compensation during mitochondrial disease using the Drosophila model of ATP6 dysfunction.

10. Degradation of functional triose phosphate isomerase protein underlies sugarkill pathology.

11. Drosophila model of human inherited triosephosphate isomerase deficiency glycolytic enzymopathy.

12. Mitochondrial encephalomyopathy in Drosophila.

13. Drosophila: a "model" model system to study neurodegeneration.

15. Identification of alternative splicing regulators by RNA interference in Drosophila.

16. Using single-strand conformational polymorphism gel electrophoresis to analyze mutually exclusive alternative splicing.

17. RNA interference of mRNA processing factors in Drosophila S2 cells.

18. Arginine/serine repeats are sufficient to constitute a splicing activation domain.

19. Exon-specific RNAi: a tool for dissecting the functional relevance of alternative splicing.

20. Alternative splicing of the Drosophila Dscam pre-mRNA is both temporally and spatially regulated.

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