| Literature DB >> 20964868 |
Abstract
The sensory cortex is subject to continuous remodelling during early development and throughout adulthood. This process is important for establishing normal brain function and is dependent on cholinergic modulation via muscarinic receptors. Five muscarinic receptor genes encode five unique receptor subtypes (M1-5). The distributions and functions of each subtype vary in central and peripheral systems. In the brain, the M1 receptor is most abundant in the cerebral cortex, where its immunoreactivity peaks transiently during early development. This likely signifies the importance of M1 receptor in the development and maintenance of normal cortical function. Several lines of study have outlined the roles of M1 receptors in the development and plasticity of the auditory cortex. For example, M1-knockout reduces experience-dependent plasticity and disrupts tonotopic mapping in the adult mouse auditory cortex. Further evidence demonstrates a role for M1 in neurite outgrowth and hence determining the structure of cortical neurons. The disruption of tonotopic maps in M1-knockout mice may be linked to alterations in thalamocortical connectivity, because the targets of thalamocortical afferents (layer IV cortical neurons) appear less mature in M1 knockouts. Herein we review the literature to date concerning M1 receptors in the auditory cortex and consider some future directions that will contribute to our understanding.Entities:
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Year: 2010 PMID: 20964868 PMCID: PMC2972260 DOI: 10.1186/1756-6606-3-29
Source DB: PubMed Journal: Mol Brain ISSN: 1756-6606 Impact factor: 4.041
Figure 1Schematic representation of thalamocortical and cholinergic fiber ingrowth to the auditory cortex of mice. The open circle depicits the arrival of thalamocortical afferent fibers at embryonic day (E)15-16 [1,5], and the line extending from it represents the course of their maturation to completion at postnatal day (P)7 [6]. The closed circle represents the initial invasion to the cortex by cholinergic fibers on E18-19, and the associated line, their maturation through the first 7 weeks of life [7,81]. The dotted lines delineate the boundaries of proposed critical periods of rapid reformation and maturation beginning at P11 [13] and extending to P21 [32], with the grey dotted line marking the end of an purposed early critical period at P13 [13]. The light-grey cloud represents the trends in M1 expression, with a peak represents the maximal adult expression levels at ~P26 and a subsequent gradual decline throughout adult life (conservative average of data from from several articles [32,38,82]). The dark-grey shaded area area represents choline acetyltransferase (ChAT) expression, again with the peak of this curve being maximal expression, rising more slowly and likely sustained longer into adult life than that for M1 (based on data published by Hohmann 1985 [81]).
Acetylcholine Receptors and Function in Brain.
| Nicotinic | Muscarinic | ||||
|---|---|---|---|---|---|
| M1 | M2 | M3 | M4 | M5 | |
| Facilitates thalamocortical transmission[ | Neurite outgrowth[ | ||||
| Unclear roles in plasticity and development | Promotes Cell Survival[ | Promotes Cell Survival[ | Promotes Cell Survival[ | ||
| Impact auditory plasticity[ | Impact auditory plasticity[ | Impact auditory plasticity[ | Impact auditory plasticity[ | Impact auditory plasticity[ | |
| Proposed importance in cortical development[ | |||||