25/03/2022
Key points:
Researchers from the 海角社区论坛鈥檚 Epigenetics research programme have been able to learn more about na茂ve stem cell reprogramming following a genome wide functional screen. Their research, published today in , describes the critical regulators of reprogramming and offers opportunities for a more efficient, faster way to generate human na茂ve pluripotent stem cells.
Human pluripotent stem cells (PSCs) are a useful tool for researchers investigating how cells specialise to make every tissue of our body. They come in two different states, primed and na茂ve. Both types of PSC can self-renew and differentiate into new cell types but they have distinct functions and molecular characteristics.
Group leader Dr Peter Rugg-Gunn explained the importance of these cells: 鈥淗uman PSCs in the na茂ve state replicate the key molecular and cellular characteristics of cells in a pre-implantation stage embryo. Importantly, when na茂ve PSCs are encouraged to self-organise in particular conditions, they form structures that resemble an early blastocyst stage of development. By growing these cells in the lab, we can learn about the key events that happen during human development, and they have potential uses in personalised medicine. But we need to create high-quality, stable stem cell populations to be able to conduct our experiments.鈥
Pluripotent stem cells are formed either from embryos or using Nobel Prize-winning methods to remove cell identity from specialised cells. The majority of reprogramming experiments generate primed PSCs, which are more developmentally advanced than na茂ve PSCs. Na茂ve PSCs can be collected directly from human pre-implantation embryos, or more commonly researchers expose primed PSCs to conditions that induces them to become na茂ve PSCs. Existing methods for reprogramming were inefficient and slow, preventing researchers from quickly producing the numbers of high-quality stem cells they needed.
Adam Bendall, PhD student and a lead researcher on the study, said: 鈥淰ery little was known about what genetic and epigenetic factors are required for na茂ve cell reprogramming, and this knowledge gap limited the design of reprogramming conditions.鈥
The low efficiency of na茂ve reprogramming suggests the presence of barriers that limit cells in reaching the na茂ve state. Adam and his colleagues honed in on these barriers by performing a large-scale genetic screen to identify genes that hinder and help reprogramming. They were able to identify a large number of genes that have a crucial role in na茂ve PSC programming that had not been previously linked to the process.
The team focused on one epigenetic complex in particular, the PRC1.3 complex, that regulates gene expression without altering the underlying DNA sequence, and which they found to be essential for the formation of na茂ve PSCs. Without this complex, the cells undergoing reprogramming become a completely different type of cell rather than na茂ve PSCs. This suggests that the activity of PRC1.3 could encourage more cells to reprogramme properly, in effect lowering the barrier.
After identifying factors that promote reprogramming, the researchers also looked at factors that impede reprogramming, exemplified in their study by an epigenetic protein called HDAC2. Dr Amanda Collier, first author on the paper, explained: 鈥淓xcitingly, when we inhibited one of these factors using selective chemicals, then na茂ve PSC reprogramming occurred more efficiently and rapidly. We鈥檙e able to look at it from both sides; we can remove the barriers and introduce the factors that push cells towards state change.鈥
Not only does this research improve scientists鈥 ability to produce human na茂ve PSCs, it provides details on the molecular events that occur during the cell state transition itself, some of which are conserved in developmental regulation in human embryos.
The Rugg-Gunn lab are putting together the pieces of a bigger puzzle - the best understanding of the formation and control of na茂ve stem cells. Their previous research has identified molecular factors that help to maintain cells in a na茂ve stage. Group leader, Dr Peter Rugg-Gunn said: 鈥淏y building up our tools for manipulating pluripotent stem cells, we can spend more time asking important questions about the pre-implantation embryo. In the longer term, further improvements in working with na茂ve PSCs might open up the possibility for using these cells in personalised disease models or cell therapies, although this will require more research on how to differentiate na茂ve PSCs into specialised cell types.鈥
Publication reference Collier et al., Genome-Wide Screening Identifies Polycomb Repressive Complex 1.3 as an Essential Regulator of Human Na茂ve Pluripotent Cell Reprogramming Science Advances, 2022
Press contact: Honor Pollard, Communications Officer, honor.pollard@babraham.ac.uk
Image description: Immunofluorescent microscopy images show the different morphology of reprogrammed pluripotent stem cells (orange) and cells that were not reprogrammed (purple).
Affiliated authors (in author order): Amanda Collier, former PhD student, Rugg-Gunn lab Adam Bendall, PhD student, Rugg-Gunn lab Charlene Fabian, former PhD student, Rugg-Gunn lab Andrew Malcolm, PhD student, Rugg-Gunn lab Claudia Semprich, postdoctoral researcher, Rugg-Gunn lab Katarzyna Wojdyla, former postdoctoral researcher, Rugg-Gunn lab Paola Nisi, former visiting PhD student, Rugg-Gunn lab Peter Rugg-Gunn, Group leader, Epigenetics research programme
Research funding This research was funded by the BBSRC, the Medical Research Council and the Wellcome Trust.
Additional/related resources: Rugg-Gunn lab page News 1 September 2021, The key to staying na茂ve
About the 海角社区论坛 The 海角社区论坛 undertakes world-class life sciences research to generate new knowledge of biological mechanisms underpinning ageing, development and the maintenance of health. 海角社区论坛 focuses on cellular signalling, gene regulation and the impact of epigenetic regulation at different stages of life. By determining how the body reacts to dietary and environmental stimuli and manages microbial and viral interactions, we aim to improve wellbeing and support healthier ageing. The Institute is strategically funded by the Biotechnology and Biological Sciences Research Council (BBSRC), part of UK Research and Innovation, through Institute Strategic Programme Grants and an Institute Core Capability Grant and also receives funding from other UK research councils, charitable foundations, the EU and medical charities.
About BBSRC The Biotechnology and Biological Sciences Research Council (BBSRC) is part of UK Research and Innovation, a non-departmental public body funded by a grant-in-aid from the UK government.BBSRC invests in world-class bioscience research and training on behalf of the UK public. Our aim is to further scientific knowledge, to promote economic growth, wealth and job creation and to improve quality of life in the UK and beyond.
Funded by government, BBSRC invested 拢451 million in world-class bioscience in 2019-20. We support research and training in universities and strategically funded institutes. BBSRC research and the people we fund are helping society to meet major challenges, including food security, green energy and healthier, longer lives. Our investments underpin important UK economic sectors, such as farming, food, industrial biotechnology and pharmaceuticals.
25 March 2022