6 results match your criteria: "ASTAR Institute of Molecular and Cell Biology[Affiliation]"

The COVID-19 pandemic has driven the scientific community to adopt an efficient and reliable model that could keep up with the infectious disease arms race. Coinciding with the pandemic, three dimensional (3D) human organoids technology has also gained traction in the field of infectious disease. An in vitro construct that can closely resemble the in vivo organ, organoid technology could bridge the gap between the traditional two-dimensional (2D) cell culture and animal models.

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Intestinal cells marked by Lgr5 function as tissue-resident stem cells that sustain the homeostatic replenishment of the epithelium. By incorporating a diphtheria toxin receptor (DTR) cassette linked to the Lgr5 coding region, native Lgr5-expressing cells are susceptible to ablation upon DT administration . A similar strategy can be used for Lgr5-expressing cells within organoids established from DTR models.

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Medical research in the recent years has achieved significant progress due to the increasing prominence of organoid technology. Various developed tissue organoids bridge the limitations of conventional 2D cell culture and animal models by recapitulating cellular complexity. Current 3D cardiac organoid cultures have shown their utility in modelling key developmental hallmarks of heart organogenesis, but the complexity of the organ demands a more versatile model that can investigate more fundamental parameters, such as structure, organization and compartmentalization of a functioning heart.

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Chromatin Regulation in Development: Current Understanding and Approaches.

Stem Cells Int

February 2021

Laboratory for Epigenetics, Stem Cells & Cell Therapy, Programme in Stem Cell, Regenerative Medicine and Aging, ASTAR Institute of Molecular and Cell Biology, Singapore 138673.

The regulation of mammalian stem cell fate during differentiation is complex and can be delineated across many levels. At the chromatin level, the replacement of histone variants by chromatin-modifying proteins, enrichment of specific active and repressive histone modifications, long-range gene interactions, and topological changes all play crucial roles in the determination of cell fate. These processes control regulatory elements of critical transcriptional factors, thereby establishing the networks unique to different cell fates and initiate waves of distinctive transcription events.

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The role of Sox6 in zebrafish muscle fiber type specification.

Skelet Muscle

February 2015

ASTAR Institute of Molecular and Cell Biology, Proteos, 61 Biopolis Drive, Singapore, 138673 Republic of Singapore ; Lee Kong Chian School of Medicine, Nanyang Technological University, Proteos, 61 Biopolis Drive, Singapore, 138673 Republic of Singapore ; Department of Medicine, Imperial College, South Kensington Campus, London, SW7 2AZ UK.

Background: The transcription factor Sox6 has been implicated in regulating muscle fiber type-specific gene expression in mammals. In zebrafish, loss of function of the transcription factor Prdm1a results in a slow to fast-twitch fiber type transformation presaged by ectopic expression of sox6 in slow-twitch progenitors. Morpholino-mediated Sox6 knockdown can suppress this transformation but causes ectopic expression of only one of three slow-twitch specific genes assayed.

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