Monosynaptic inputs to new neurons in the dentate gyrus

被引:0
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作者
Carmen Vivar
Michelle C. Potter
Jiwon Choi
Ji-young Lee
Thomas P. Stringer
Edward M. Callaway
Fred H. Gage
Hoonkyo Suh
Henriette van Praag
机构
[1] Neuroplasticity and Behavior Unit,
[2] Laboratory of Neurosciences,undefined
[3] Intramural Research Program,undefined
[4] National Institute on Aging,undefined
[5] National Institutes of Health,undefined
[6] Systems Neurobiology Laboratories,undefined
[7] The Salk Institute for Biological Studies,undefined
[8] Lerner Research Institute,undefined
[9] Cleveland Clinic,undefined
[10] Laboratory of Genetics,undefined
[11] The Salk Institute for Biological Studies,undefined
来源
Nature Communications | / 3卷
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摘要
Adult hippocampal neurogenesis is considered important for cognition. The integration of newborn dentate gyrus granule cells into the existing network is regulated by afferent neuronal activity of unspecified origin. Here we combine rabies virus-mediated retrograde tracing with retroviral labelling of new granule cells (21, 30, 60, 90 days after injection) to selectively identify and quantify their monosynaptic inputs in vivo. Our results show that newborn granule cells receive afferents from intra-hippocampal cells (interneurons, mossy cells, area CA3 and transiently, mature granule cells) and septal cholinergic cells. Input from distal cortex (perirhinal (PRH) and lateral entorhinal cortex (LEC)) is sparse 21 days after injection and increases over time. Patch-clamp recordings support innervation by the LEC rather than from the medial entorhinal cortex. Mice with excitotoxic PRH/LEC lesions exhibit deficits in pattern separation but not in water maze learning. Thus, PRH/LEC input is an important functional component of new dentate gyrus neuron circuitry.
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