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Transgenic mice expressing a dual, CRE-inducible reporter for the analysis of axon guidance and synaptogenesis
Authors:Badaloni Aurora  Bonanomi Dario  Albieri Ilaria  Givogri Irene  Bongarzone Ernesto  Valtorta Flavia  Consalez G Giacomo
Affiliation:San Raffaele Scientific Institute and Università Vita-Salute San Raffaele, Milano, Italy.
Abstract:
Improved and modular tools are needed for the neuroanatomical dissection of CNS axonal tracts, and to study the cell-intrinsic and cell-extrinsic cues that govern their assembly and plasticity. Here we describe a general purpose transgenic tracer that can be used to visualize axonal tracts and synaptic terminals in any region of the embryonic neural tube or postnatal CNS, on any wild type or mutant genetic background. The construct permits CRE-inducible expression of a dicistronic axonal marker encoding two surface reporter proteins: a farnesylated GFP and the human Placental Alkaline Phosphatase (PLAP). Both proteins localize alongside the neuronal surface, permitting the concomitant detection of cell body, neurites, and presynaptic and postsynaptic sites in the same neuron. This provides a CRE-inducible dual system for imaging neural circuits in vivo, and to study their assembly and remodeling in cultured neurons, neural stem cells, and tissue explants derived from the reporter line. Unlike existing lines, this reporter does not encode a ubiquitously expressed, floxable LacZ gene, permitting the simultaneous analysis of beta galactosidase activity in mutant lines.
Keywords:axon  axon guidance  process outgrowth  growth cone  sprouting  dendrite  filopodia  growth cone  dendritic spines  synapses  GFP  CNS  PNS  neural networks  transgenic mice  stem cells  neural stem cells  graft, neuron  oligodendrocyte  lipid rafts  CRE recombinase  tracer
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