Holography
holography
Dr. Yoav Livneh
We are looking for enthusiastic students and researchers from diverse backgrounds, including (but not limited to) biology, physics, medicine, physiology, psychology, engineering, and more. We have several ERC-funded positions at different levels.
Prof Ian Oldenburg
The Oldenburg lab combines optics, multiphoton optogenetics, calcium imaging, and computation to understand the motor system. The overall goal of the Oldenburg Lab is to understand the causal relationship between neural activity and motor actions. We use advanced optical techniques such as multiphoton holographic optogenetics to control neural activity with an incredible degree of precision, writing complex patterns of activity to distributed groups of cells. Only by writing activity into the brain at the scale in which it naturally occurs (individual neurons firing distinct patterns of action potentials) can we test theories of what population activity means. We read out the effects of these precise manipulations locally with calcium imaging, in neighboring brain regions with electrophysiology, and at the 'whole animal level' through changes in behavior. We are looking for curious motivated, and talented people with a wide range of skill sets to join our group at all levels from Technician to Postdoc.
Swimming in the third domain: archaeal extremophiles
Archaea have evolved to survive in some of the most extreme environments on earth. Life in extreme, nutrient-poor conditions gives the opportunity to probe fundamental energy limitations on movement and response to stimuli, two essential markers of living systems. Here we use three-dimensional holographic microscopy and computer simulations to show that halophilic archaea achieve chemotaxis with power requirements one hundred-fold lower than common eubacterial model systems. Their swimming direction is stabilised by their flagella (archaella), enhancing directional persistence in a manner similar to that displayed by eubacteria, albeit with a different motility apparatus. Our experiments and simulations reveal that the cells are capable of slow but deterministic chemotaxis up a chemical gradient, in a biased random walk at the thermodynamic limit.
Playing the piano with the cortex: role of neuronal ensembles and pattern completion in perception
The design of neural circuits, with large numbers of neurons interconnected in vast networks, strongly suggest that they are specifically build to generate emergent functional properties (1). To explore this hypothesis, we have developed two-photon holographic methods to selective image and manipulate the activity of neuronal populations in 3D in vivo (2). Using them we find that groups of synchronous neurons (neuronal ensembles) dominate the evoked and spontaneous activity of mouse primary visual cortex (3). Ensembles can be optogenetically imprinted for several days and some of their neurons trigger the entire ensemble (4). By activating these pattern completion cells in ensembles involved in visual discrimination paradigms, we can bi-directionally alter behavioural choices (5). Our results demonstrate that ensembles are necessary and sufficient for visual perception and are consistent with the possibility that neuronal ensembles are the functional building blocks of cortical circuits. 1. R. Yuste, From the neuron doctrine to neural networks. Nat Rev Neurosci 16, 487-497 (2015). 2. L. Carrillo-Reid, W. Yang, J. E. Kang Miller, D. S. Peterka, R. Yuste, Imaging and Optically Manipulating Neuronal Ensembles. Annu Rev Biophys, 46: 271-293 (2017). 3. J. E. Miller, I. Ayzenshtat, L. Carrillo-Reid, R. Yuste, Visual stimuli recruit intrinsically generated cortical ensembles. Proceedings of the National Academy of Sciences of the United States of America 111, E4053-4061 (2014). 4. L. Carrillo-Reid, W. Yang, Y. Bando, D. S. Peterka, R. Yuste, Imprinting and recalling cortical ensembles. Science 353, 691-694 (2016). 5. L. Carrillo-Reid, S. Han, W. Yang, A. Akrouh, R. Yuste, (2019). Controlling visually-guided behaviour by holographic recalling of cortical ensembles. Cell 178, 447-457. DOI:https://doi.org/10.1016/j.cell.2019.05.045.