Withdraw
Loading…
Actin's role in signaling light-induced phase shifts in the mammalian circadian clock
Arnold, Jennifer
Loading…
Permalink
https://hdl.handle.net/2142/42146
Description
- Title
- Actin's role in signaling light-induced phase shifts in the mammalian circadian clock
- Author(s)
- Arnold, Jennifer
- Issue Date
- 2013-02-03T19:17:20Z
- Director of Research (if dissertation) or Advisor (if thesis)
- Gillette, Martha U.
- Doctoral Committee Chair(s)
- Gillette, Martha U.
- Committee Member(s)
- Gillette, Rhanor
- Roy, Edward J.
- Raetzman, Lori T.
- Brieher, William M.
- Department of Study
- Molecular & Integrative Physl
- Discipline
- Molecular & Integrative Physi
- Degree Granting Institution
- University of Illinois at Urbana-Champaign
- Degree Name
- Ph.D.
- Degree Level
- Dissertation
- Keyword(s)
- circadian
- Actin
- light
- Abstract
- The actin cytoskeleton is a critical part of intracellular structure, responsible for the general shape and integrity of all cells. New insights into the dynamic nature of the cytoskeleton describe additional roles for actin, including synaptic plasticity in the hippocampus, regulation of hormone release in endocrine cells, and as a signaling component involved in transcription. My research focused on the hypothesis that changes in actin state contribute to light-induced changes in the state of the circadian clock in the mammalian brain. In early night, the cells of the mammalian circadian clock, in the SCN, initiate a series of signaling events to translate environmental light into transcriptional changes which induce a delay of clock state. This signaling pathway, mediated by glutamate, involves activation of NMDA receptors, nitric oxide synthesis, and opening of ryanodine receptors with subsequent influx of calcium from intracellular stores. Activation of this cascade results in up-regulation of the clock genes, Period 1 and Period 2. This induction is mediated in part via CRE elements, through activation of the transcription factor, CREB. Connecting upstream signaling processes with the end result of transcriptional changes was a target of this study. Based on responses to glutamate in vitro, I hypothesized that activation of the early night light signaling pathway results in a rapid and transient decrease in actin polymerization, which is required for the phase delay to occur. I first characterized actin state around a day-night cycle, in order to determine whether sensitivity to actin depolymerization changes over this period. To this end, I showed that polymerized actin peaks in early night, but this oscillation in actin state is abolished in mice rendered genetically arrhythmic, the BMAL1 -/- mice. Secondly, I measured actin state after light exposure, and found that brief light pulses induced a breakdown of polymerized actin. By injecting the actin-stabilizing chemical jasplakinolide directly into the mouse SCN, I demonstrated a requirement for actin breakdown in mediating the phase delay, while conversely I induced a delay by injecting the actin depolymerzing agent latrunculin A. Thirdly, I measured induction of potential downstream effectors upon actin depolymerization, to analyze the effect of actin dynamics on transcription. Breaking down the cytoskeleton with latrunculin A resulted in activation of the MAP kinase component PERK, as well as a potential activation of PCREB. The importance of actin dynamics on CRE-mediated transcription was demonstrated using electrophysiological recordings, in which inhibition of CRE-mediated transcription abolished the effects of latrunculin A on clock state. Finally, I showed that actin depolymerization induced the clock gene Period 2, providing a potential link between cytoplasmic signaling events that facilitate actin remodeling and nuclear mechanisms of transcription. This work, together with previous in vitro studies, places actin dynamics firmly within the light signaling pathway. This not only contributes to knowledge about circadian cell signaling, but provides a new important role for actin in mediating cellular physiological processes.
- Graduation Semester
- 2012-12
- Permalink
- http://hdl.handle.net/2142/42146
- Copyright and License Information
- Copyright 2012 Jennifer Arnold
Owning Collections
Graduate Dissertations and Theses at Illinois PRIMARY
Graduate Theses and Dissertations at IllinoisManage Files
Loading…
Edit Collection Membership
Loading…
Edit Metadata
Loading…
Edit Properties
Loading…
Embargoes
Loading…