University of Surrey
University of Surrey
1,160 Projects, page 1 of 232
assignment_turned_in Project2023 - 2027Partners:University of SurreyUniversity of SurreyFunder: UK Research and Innovation Project Code: 2919525Insects as a novel source of dietary protein: Does it have legs?
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For further information contact us at helpdesk@openaire.euassignment_turned_in Project2022 - 2023Partners:University of SurreyUniversity of SurreyFunder: UK Research and Innovation Project Code: MR/X013588/1Funder Contribution: 171,101 GBPViruses require living cells to multiply. When doing so, viruses cause a complete re-organisation of the infected cell, overall allowing the production of thousands of new viral particles but also suppressing the ability of the host to fight infection. Crucial insights into this complex interplay can be obtained imaging living cells and viruses, which is only possible using microscopes. Most microscopes are, however, able to image a few cells at a time making it very lengthy and laborious to obtain information from a representative number of cells. In addition, cells undergo their own life cycle and variations exist between them even in the same petri dish. A way to overcome this problem is the use of high-throughput microscopes able to image thousands of cells and analyse their properties on an individual basis. This proposal concerns the acquisition of one of such imaging systems for the Section of Virology at the University of Surrey, a unit of research formed by >20 investigators from 6 different groups studying human viruses and their interplay with human cells. The instrument we propose to acquire will enable us to track where viruses go inside a cell and how they manipulate the intracellular environment. We will be able to visualise viral features such as gene expression and replication factories, as well as the cell's response to infection in the form of stress granules, mitochondrial reorganisation and cell and nucleus morphology. More importantly, we will be able to measure these events qualitatively and quantitatively in hundreds of individual cells in specified conditions, generating high quality reproducible data in a short period of time. As examples, we have recently discovered a viral protein expressed in poxviruses (including the emerging monkeypox virus) that induces the clustering of mitochondria (the energy factories of the cell). The kinetics of assembly and disassembly as well as the size and morphology of these clusters in different conditions remains unknown but can be elucidated with a high-throughput multimode microscopy unit. Similarly, we have recently discovered that cells infected with herpes simplex virus fail to export their mRNAs from the nucleus, causing a blockade of cellular functions that allows efficient virus infection. The mechanisms behind this process are unclear but can be researched with an imaging system equipped with a spot counting module. Altogether the requested instrument will not only increase our capacity to deliver ground-breaking research, but also provide novel perspectives on viral infection that are at present not possible with other equipment.
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For further information contact us at helpdesk@openaire.euassignment_turned_in Project2024 - 2027Partners:University of SurreyUniversity of SurreyFunder: UK Research and Innovation Project Code: 2904825The student will work on studying the halo of the magellanic clouds using the DELVE survey of which Dr Noal is the co-PI. They will invoice new substructures and place meaningful constraints on dark matter
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For further information contact us at helpdesk@openaire.euassignment_turned_in Project2023 - 2027Partners:University of SurreyUniversity of SurreyFunder: UK Research and Innovation Project Code: 2896340Quantum thermodynamical framework for understanding off-equilibrium properties of living systems
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For further information contact us at helpdesk@openaire.euassignment_turned_in Project2016 - 2020Partners:University of SurreyUniversity of SurreyFunder: UK Research and Innovation Project Code: 1796992To investigate the short-lived isotopes 26Al and 30P produced in novae and asymptotic giant branch stars. In reactions of these nuclei with a deuteron target they can pick up a neutron and it is these neutron capture rates that control stellar processes. Such transfer reactions require sophisticated theoretical modelling. The PhD student will learn the algebraic and computational tools needed to exploit this opportunity to make a real contribution to our understanding of such transfer reactions, which in turn gives a better understanding of nucleosynthesis and the evolution of stars.
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