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Hamish W King

Researcher at Queen Mary University of London

Publications -  36
Citations -  3274

Hamish W King is an academic researcher from Queen Mary University of London. The author has contributed to research in topics: Chromatin & Regulation of gene expression. The author has an hindex of 15, co-authored 33 publications receiving 2032 citations. Previous affiliations of Hamish W King include Flinders Medical Centre & Flinders University.

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Hypoxic enhancement of exosome release by breast cancer cells

TL;DR: Evidence is provided that hypoxia promotes the release of exosomes by breast cancer cells, and that this hypoxic response may be mediated by HIF-1 α, and this has significant implications for understanding the hypoxic tumour phenotype.
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Variant PRC1 Complex-Dependent H2A Ubiquitylation Drives PRC2 Recruitment and Polycomb Domain Formation

TL;DR: Using a de novo targeting assay in mouse embryonic stem cells, it is found that PRC1-dependent H2AK119ub1 leads to recruitment of PRC2 and H3K27me3 to effectively initiate a polycomb domain, providing a surprising PRC 1-dependent logic forPRC2 occupancy at target sites in vivo.
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The pioneer factor OCT4 requires the chromatin remodeller BRG1 to support gene regulatory element function in mouse embryonic stem cells

TL;DR: It is discovered that the pluripotency-associated pioneer factor OCT4 binds chromatin to shape accessibility, transcription factor co-binding, and regulatory element function in mouse embryonic stem cells.
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Synergy between Variant PRC1 Complexes Defines Polycomb-Mediated Gene Repression

TL;DR: It is demonstrated that canonical Polycomb repressive complex 1 (PRC1), which mediates higher-order chromatin structures, contributes little to gene repression, and a new variant PRC1-dependent logic for Polycomb-mediated gene repression is revealed.