Loss of adenylyl cyclase I activity disrupts patterning of mouse somatosensory cortex

被引:0
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作者
Raja M. Abdel-Majid
Wey L. Leong
Leonard C. Schalkwyk
Donald S. Smallman
Scott T. Wong
Daniel R. Storm
Alan Fine
Melanie J. Dobson
Duane L. Guernsey
Paul E. Neumann
机构
[1] Faculty of Medicine,Department of Anatomy & Neurobiology
[2] Dalhousie University,Department of Surgery
[3] Faculty of Medicine,Department of Pathology
[4] Dalhousie University,Department of Physiology & Biophysics
[5] Faculty of Medicine,Department of Biochemistry
[6] Dalhousie University,undefined
[7] Max-Planck-Institut für Molekulare Genetik,undefined
[8] Faculty of Medicine,undefined
[9] Dalhousie University,undefined
[10] Faculty of Medicine,undefined
[11] Dalhousie University,undefined
来源
Nature Genetics | 1998年 / 19卷
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摘要
The somatosensory (SI) cortex of mice displays a patterned, nonuniform distribution of neurons in layer IV called the 'barrelfield' ( ref. 1). Thalamocortical afferents (TCAs) that terminate in layer IV are segregated such that each barrel, a readily visible cylindrical array of neurons surrounding a cell-sparse center, represents a distinct receptive field. TCA arbors are confined to the barrel hollow and synapse on barrel-wall neurons whose dendrites are oriented toward the center of the barrel2. Mice homozygous for the barrelless (brl) mutation, which occurred spontaneously in ICR stock at Université de Lausanne (Switzerland), fail to develop this patterned distribution of neurons, but still display normal topological organization of the SI cortex3. Despite the absence of barrels and the overlapping zones of TCA arborization, the size of individual whisker representations, as judged by 2-deoxyglucose uptake, is similar to that of wild-type mice. We identified adenylyl cyclase type I (Adcy1) as the gene disrupted in brl mutant mice by fine mapping of proximal chromosome 11, enzyme assay, mutation analysis and examination of mice homozygous for a targeted disruption of Adcy1. These results provide the first evidence for involvement of cAMP signalling pathways in pattern formation of the brain.
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页码:289 / 291
页数:2
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