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Abstract

Grant Number: 1R01DA020794-01

Project Title: Calcium channels, newborn neurons, and CNS circuit dynamics

PI Information: Name Email Title

DEISSEROTH, KARL deissero@stanford.edu

Abstract: Adult neural circuits are in a state of constant remodeling. One of most striking mechanisms by which this occurs is the insertion of new neurons, a process that occurs normally in all adult mammals and has been hypothesized to underly aspects of physiological information storage. Abnormal adult neurogenesis, by contrast, has been linked to major neuropsychiatric diseases including drug addiction and depression. We have found that neural activity acts directly on proliferating progenitors to drive adult neurogenesis, and recent years have witnessed many other important new insights into the underlying molecular mechanisms. However, little or no insight has emerged into the impact of adult neurogenesis on neural circuit function. We propose to apply novel ion channel-based probes to study interactions between CMS circuits and calcium channel-dependent neurogenesis. We hypothesize that circuit activity acting through calcium channels is a crucial component of the cellular microenvironment controlling adult neurogenesis. We further hypothesize that this is a bidirectional interaction, as newborn neurons (once functionally inserted into the circuit as a result of local activity patterns) in turn directly modulate these local network activity patterns. Aim 1 will identify mechanisms by which activity and cellular microenvironment interact to drive calcium channel-dependent adult neurogenesis. Aims 2 and 3 will explore mechanisms by which newborn neurons in turn modulate circuit activity dynamics, using novel high-temporal resolution imaging (Aim 2) and stimulation (Aim 3) techniques. Aim 4 describes use of a new genetically-encoded light-responsive stimulation tool to provide physiological activity patterns to proliferating progenitor cells, in order to study molecular mechanisms of environmental control of excitation-neurogenesis coupling. Together, insights garnered from determining the reciprocal relationship between circuit activity and adult neurogenesis may profoundly illuminate core mechanisms of hippocampal neuropsychiatric disease and suggest novel therapeutic strategies, while deepening our understanding of the normal activity-dependent operation and plasticity of progenitor cells in the hippocampal circuit.
Public Health Relevance:
This Public Health Relevance is not available.
Thesaurus Terms:
calcium channel, central nervous system, developmental neurobiology, neuroanatomy, neurogenesis
cell proliferation, hippocampus, intermolecular interaction, nerve stem cell, neural plasticity, stimulus /response
laboratory rat, neuroimaging

Institution: STANFORD UNIVERSITY

STANFORD, CA 94305

Fiscal Year: 2005

Department: BIOENGINEERING

Project Start: 30-SEP-2005

Project End: 31-AUG-2010

ICD: NATIONAL INSTITUTE ON DRUG ABUSE

IRG: NTRC

Grant Number:	1R01DA020794-01
Project Title:	Calcium channels, newborn neurons, and CNS circuit dynamics

PI Information:	Name	Email	Title
	DEISSEROTH, KARL	deissero@stanford.edu

Institution:	STANFORD UNIVERSITY
	STANFORD, CA 94305
Fiscal Year:	2005
Department:	BIOENGINEERING
Project Start:	30-SEP-2005
Project End:	31-AUG-2010
ICD:	NATIONAL INSTITUTE ON DRUG ABUSE
IRG:	NTRC