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Gi Fay Mok

Researcher at University of East Anglia

Publications -  19
Citations -  380

Gi Fay Mok is an academic researcher from University of East Anglia. The author has contributed to research in topics: Somite & Paraxial mesoderm. The author has an hindex of 8, co-authored 16 publications receiving 300 citations. Previous affiliations of Gi Fay Mok include University of Nottingham.

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Many routes to the same destination: lessons from skeletal muscle development

TL;DR: This review will highlight how cells from multiple distinct starting points can converge on a common set of regulators to generate skeletal muscle.
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microRNAs in skeletal muscle development

TL;DR: The role of non-coding RNAs, in particular microRNAs (miRNAs), in embryonic muscle development and differentiation, and in satellite cells of adult muscle, which are essential for muscle growth and regeneration are reviewed.
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myomiR-dependent switching of BAF60 variant incorporation into Brg1 chromatin remodeling complexes during embryo myogenesis

TL;DR: It is revealed that interactions between tissue-specific non-coding RNAs and chromatin remodeling factors confer robustness to mesodermal lineage determination and suggests that myomiRs contribute to select BAF60c for incorporation into the Brg1 complex by specifically targeting the alternative variants BAF50a and BAF 60b during embryo myogenesis.
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Smad1 transcription factor integrates BMP2 and Wnt3a signals in migrating cardiac progenitor cells

TL;DR: A role for bone morphogenetic proteins (BMPs) in the control of cardiac progenitor cell migration is uncovered and an interaction of BMP and Wnt/glycogen synthase kinase 3 beta (GSK3β) pathways via the differential phosphorylation of Smad1 is identified.
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miR-133-mediated regulation of the Hedgehog pathway orchestrates embryo myogenesis.

TL;DR: It is shown that post-transcriptional silencing of the Gli3 repressor by miR-133 is required to stably establish the myogenic programme in early somites, and a novel Shh/myogenic regulatory factor/miR- 133/Gli3 axis that connects epithelial morphogenesis with myogenic fate specification is identified.