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1. Zmym4 is required for early cranial gene expression and craniofacial cartilage formation

2. Time-resolved quantitative proteomic analysis of the developing Xenopus otic vesicle reveals putative congenital hearing loss candidates

3. Retinoic Acid is Required for Normal Morphogenetic Movements During Gastrulation

4. Repressive Interactions Between Transcription Factors Separate Different Embryonic Ectodermal Domains

5. Selective disruption of trigeminal sensory neurogenesis and differentiation in a mouse model of 22q11.2 deletion syndrome

7. Six1 proteins with human branchio-oto-renal mutations differentially affect cranial gene expression and otic development

8. Mutations in SIX1 Associated with Branchio-oto-Renal Syndrome (BOR) Differentially Affect Otic Expression of Putative Target Genes

9. Dysphagia and disrupted cranial nerve development in a mouse model of DiGeorge (22q11) deletion syndrome

10. Neural Induction, Neural Fate Stabilization, and Neural Stem Cells

12. Mcrs1 is required for branchial arch and cranial cartilage development

13. Duplicated zebrafish (Danio rerio) inositol phosphatases inpp5ka and inpp5kb diverged in expression pattern and function

15. Duplicated zebrafish (Danio rerio) inositol phosphatases inpp5ka and inpp5kb diverged in expression pattern and function

18. Xenopus

20. Human Molecular Genetics

21. Natural size variation among embryos leads to the corresponding scaling in gene expression

22. The Society for Craniofacial Genetics and Developmental Biology 42nd Annual Meeting

23. Human Molecular Genetics

24. Normal Table of Xenopus development: a new graphical resource

25. iXenopus/iExplants and Transplants

26. Generation of a new six1 ‐null line in Xenopus tropicalis for study of development and congenital disease

28. Repressive Interactions Between Transcription Factors Separate Different Embryonic Ectodermal Domains

29. Sobp modulates the transcriptional activation of Six1 target genes and is required during craniofacial development

30. Disease Models & Mechanisms

33. Sobp is a novel Six1 co‐factor during inner ear development

34. Altering metabolite distribution at Xenopus cleavage stages affects left–right gene expression asymmetries

35. Sobp modulates Six1 transcriptional activation and is required during craniofacial development

36. In the line-up: deleted genes associated with DiGeorge/22q11.2 deletion syndrome: are they all suspects?

37. Microsampling Capillary Electrophoresis Mass Spectrometry Enables Single-Cell Proteomics in Complex Tissues: Developing Cell Clones in Live Xenopus laevis and Zebrafish Embryos

39. Mcrs1 interacts with Six1 to influence early craniofacial and otic development

40. Suckling, Feeding, and Swallowing: Behaviors, Circuits, and Targets for Neurodevelopmental Pathology

41. Six1 proteins with human branchio-oto-renal mutations differentially affect cranial gene expression and otic development

43. Xenopus : From Basic Biology to Disease Models in the Genomic Era

44. In Situ Microprobe Single-Cell Capillary Electrophoresis Mass Spectrometry: Metabolic Reorganization in Single Differentiating Cells in the Live Vertebrate (Xenopus laevis) Embryo

45. Metabolic comparison of dorsal versus ventral cells directly in the live 8-cell frog embryo by microprobe single-cell CE-ESI-MS

46. Pa2G4 is a novel Six1 co-factor that is required for neural crest and otic development

47. A cellular and molecular mosaic establishes growth and differentiation states for cranial sensory neurons

48. Neural transcription factors bias cleavage stage blastomeres to give rise to neural ectoderm

49. Single‐Cell Mass Spectrometry for Discovery Proteomics: Quantifying Translational Cell Heterogeneity in the 16‐Cell Frog ( Xenopus ) Embryo

50. Using Xenopus to discover new genes involved in branchiootorenal spectrum disorders

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