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| Funder | Medical Research Council |
|---|---|
| Recipient Organization | University of Cambridge |
| Country | United Kingdom |
| Start Date | Feb 01, 2021 |
| End Date | Dec 31, 2024 |
| Duration | 1,429 days |
| Number of Grantees | 2 |
| Roles | Principal Investigator; Award Holder |
| Data Source | UKRI Gateway to Research |
| Grant ID | MR/V009192/1 |
One of the most important events in pregnancy occurs early in the process, when the embryo implants into the uterus of the mother. This event it so crucial for pregnancy success, that implantation failure is estimated to be responsible for around 30% of miscarriages. Repeated issues with this step during assisted reproductive therapy is considered as a condition called recurrent implantation failure and can be devasting for parents hoping to conceive through in vitro fertilisation (IVF).
From the perspective of the embryo, implantation also reflects an important moment in its development. As embryos begin to develop and grow, cells must be come different from one another in a controlled manner so that the full spectrum of different cell types are generated. These different early cell populations must also grow and expand at the correct rate, so that organs are generated of the correct size and proportion.
As developmental biologists, we know a lot about what controls the generation of different cell types, and as this is beginning around the stages of implantation, it is a major focus of many research laboratories across the globe. However, the question of how cells uptake the correct nutrients to expand these early cell populations is relatively understudied.
In fact, we know very little of how these two essential processes: cell differentiation and growth, are coordinated in early development. It is essential to know more, as problems in the provision, uptake and usage of nutrients by the early embryo may be important for our better understanding of early pregnancy loss. In addition, it is likely to provide researchers in IVF clinics improved methods to assess the health of embryos in their selection for embryo transfer to the mother.
How cells uptake and use nutrients is a highly complicated process, that uses multiple overlapping metabolic pathways inside the cell. This research proposal will focus on understanding how cells specifically uptake glucose in a region of the early embryo called the mesoderm. This region later gives rise to many tissues in the adult body including the blood system, skeletal muscle and much of the skeleton.
We will build on some preliminary data showing a surprising result that these cells have transporter proteins on the cell membrane to uptake glucose in a selective manner. We will follow how this glucose is used within the cell to fuel the generation of new cellular components important for regulating the growth of mesoderm progenitors. At the same time, we will look at how glucose is broken down and used in other parts of cellular metabolism linked to the regulation of developmental signalling pathways.
We know these signalling pathways very well, as they are known to be important for the generation of multiple distinct cell types in early development, and in particular the early mesoderm. Therefore, we will uncover a direct link between the regulation of cell differentiation and growth. This will have far reaching consequences, both for an improved understanding of what happens in early pregnancy loss and for improving experimental protocols for the differentiation and expansion of specific cell types from stem cells and their use in regenerative medicine.
University of Cambridge
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