Molecular and Cellular Approaches for Diversifying and Extending Optogenetics
Abstract
Optogenetic technologies employ light to control biological processes within targeted cells in vivo with high temporal precision. Here, we show that application of molecular trafficking principles can expand the optogenetic repertoire along several long-sought dimensions. Subcellular and transcellular trafficking strategies now permit (1) optical regulation at the far-red/infrared border and extension of optogenetic control across the entire visible spectrum, (2) increased potency of optical inhibition without increased light power requirement (nanoampere-scale chloride-mediated photocurrents that maintain the light sensitivity and reversible, step-like kinetic stability of earlier tools), and (3) generalizable strategies for targeting cells based not only on genetic identity, but also on morphology and tissue topology, to allow versatile targeting when promoters are not known or in genetically intractable organisms. Together, these results illustrate use of cell-biological principles to enable expansion of the versatile fast optogenetic technologies suitable for intact-systems biology and behavior.
Additional Information
© 2010 Elsevier Inc. Received: October 9, 2009; Revised: January 11, 2010; Accepted: February 18, 2010; Published online: March 18, 2010. V.G. is supported by the Stanford Interdisciplinary Graduate Fellowship, F.Z. by the National Institutes of Health (NIH) and Harvard Society of Fellows, J.M. by the Stanford Medical Scientist Training Program, R.P. by the NIH, I.D. by the German Academic Exchange Service and the Human Frontier Science Program, I.G. by the Machiah Foundation and the Weizmann Institute, K.T. by the National Alliance for Research on Schizophrenia and Depression, and K.D. by the Woo, Keck, Snyder, McKnight, Yu, and Coulter Foundations, as well as by the California Institute of Regenerative Medicine, the National Science Foundation, and the NIH. We thank the entire Deisseroth lab for their support.Attached Files
Accepted Version - nihms-625704.pdf
Supplemental Material - mmc1.pdf
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Additional details
- PMCID
- PMC4160532
- Eprint ID
- 35840
- Resolver ID
- CaltechAUTHORS:20121206-083746393
- Stanford Interdisciplinary Graduate Fellowship
- NIH
- Harvard Society of Fellows
- Stanford Medical Scientist Training Program
- Deutscher Akademischer Austauschdienst (DAAD)
- Machiah Foundation
- Weizmann Institute
- National Alliance for Research on Schizophrenia and Depression
- Woo Foundation
- California Institute of Regenerative Medicine
- NSF
- Human Frontier Science Program
- W. M. Keck Foundation
- McKnight Foundation
- H. L. Snyder Medical Foundation
- Albert Yu and Mary Bechmann Foundation
- Wallace Coulter Foundation
- Created
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2012-12-07Created from EPrint's datestamp field
- Updated
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2021-11-09Created from EPrint's last_modified field