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1. Have a Little Heart (or Not): Highly Minimized Skeletal Muscle Regulatory Cassettes with Low or No Activity in the Heart.

2. FSHD Therapeutic Strategies: What Will It Take to Get to Clinic?

3. Targeted epigenetic repression by CRISPR/dSaCas9 suppresses pathogenic DUX4-fl expression in FSHD.

4. The Good, The Bad, and The Unexpected: Roles of DUX4 in Health and Disease.

5. The Genetics and Epigenetics of Facioscapulohumeral Muscular Dystrophy.

6. Identification of Epigenetic Regulators of DUX4-fl for Targeted Therapy of Facioscapulohumeral Muscular Dystrophy.

7. Large family cohorts of lymphoblastoid cells provide a new cellular model for investigating facioscapulohumeral muscular dystrophy.

8. Scalpel or Straitjacket: CRISPR/Cas9 Approaches for Muscular Dystrophies.

9. CRISPR/dCas9-mediated Transcriptional Inhibition Ameliorates the Epigenetic Dysregulation at D4Z4 and Represses DUX4-fl in FSH Muscular Dystrophy.

10. Facioscapulohumeral muscular dystrophy as a model for epigenetic regulation and disease.

11. Individual epigenetic status of the pathogenic D4Z4 macrosatellite correlates with disease in facioscapulohumeral muscular dystrophy.

12. Myogenic enhancers regulate expression of the facioscapulohumeral muscular dystrophy-associated DUX4 gene.

13. Pax3 synergizes with Gli2 and Zic1 in transactivating the Myf5 epaxial somite enhancer.

14. Analysis of muscle gene transcription in cultured skeletal muscle cells.

15. Differentiation and fiber type-specific activity of a muscle creatine kinase intronic enhancer.

16. Design and testing of regulatory cassettes for optimal activity in skeletal and cardiac muscles.

17. KLF3 regulates muscle-specific gene expression and synergizes with serum response factor on KLF binding sites.

18. Quantitative proteomic identification of MAZ as a transcriptional regulator of muscle-specific genes in skeletal and cardiac myocytes.

19. Design of tissue-specific regulatory cassettes for high-level rAAV-mediated expression in skeletal and cardiac muscle.

20. Quantitative proteomic identification of six4 as the trex-binding factor in the muscle creatine kinase enhancer.

21. Differences in the function of three conserved E-boxes of the muscle creatine kinase gene in cultured myocytes and in transgenic mouse skeletal and cardiac muscle.

22. Transgenic and tissue culture analyses of the muscle creatine kinase enhancer Trex control element in skeletal and cardiac muscle indicate differences in gene expression between muscle types.

23. Implication of interfering antibody formation and apoptosis as two different mechanisms leading to variable duration of adenovirus-mediated transgene expression in immune-competent mice.

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