ERC SOL Synergy PROJECT: ‘Switchable rhodOpsins in Life Sciences'
The project funded by the ERC Synergy Grant “Switchable rhodOpsins in Life Sciences” SOL is based on bistable rhodopsins. Rhodopsins belong to the class of G protein coupled receptors (GPCRs). There are hundreds of different GPCRs activating a variety of different G proteins, and they play an important role in cell signalling in almost every cell type. Not surprisingly, they are the targets of a large variety of pharmaceuticals. Rhodopsins are light-activated GPCRs, best known for their role as light receptors in the retina of the human eye. Upon activation, the vision receptors in our eyes lose their light sensor, the vitamin A derivative retinal, and it must be “reassembled” in order to accept photons (light) again. Bistable rhodopsins, however, keep their retinal and can be activated and deactivated by flashes of different light colours without requiring any assembly, acting as true biological “switches”. They will become revolutionary tools in physiology and neurobiology.
Using light to “switch” a cellular process on and off
"Our consortium pursues three main goals", says Gebhard Schertler. "First, we want to elucidate the structure of the bistable rhodopsins in order to better understand how they function." Second, the researchers will use molecular biological methods to create bistable rhodopsins with novel properties that can be turned on and off by light of different wavelengths and effectively mimic the signalling effect of pharmacologically relevant GPCRs. "This will enable us to turn any G protein-mediated signalling process in any cell type on and off by light of a specific colour", Schertler explains. “Our third goal is to use these switches to study the effect of G protein signalling in animals and to use this knowledge for the development of gene therapeutics against human diseases.”
The second optogenetics revolution
The conception of the first generation of optogenetics introduced a revolutionary idea in modern life sciences and provided an outstanding example of how basic research on molecular properties of proteins can translate into a practical application in cellular and animal systems. Optogenetics has already made an enormous impact in neurosciences. Up to now, however, it has been limited to light-gated ion channels, restricting its application essentially to the stimulation of nerve cells. This has prevented widespread application of this technology in the life sciences. So far, attempts to extend the range of optogenetics tools towards the photo-control of cellular receptors such as GPCR have failed to be efficient. The combined synergistic and interdisciplinary expertise of Gebhard Schertler, an expert in structural characterisation of these receptors, Peter Hegemann, a founding father of the first optogentics tools with an unmatched knowledge in biophysical characterisation of photoreceptors, and Rob Lucas, a world-leading expert on bistable rhodopsins in mammals and an expert in cellular assays and vision restoration, will deliver a toolbox of light-controlled cellular receptors with widespread applications in biology and medicine.
Schertler and Lucas were part of an international “Human Frontier Science Program” funded project, which provided important preliminary data for this ERC Synergy Grant, which is now funded by the European Union over a period of six years. This ERC grant has a realistic chance to become the catalyst for a “second optogenetics revolution” with the ERC SOL consortium playing a pivotal role in extending the boundaries of modern life sciences.
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