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      Genetically targeted 3D visualisation ofDrosophilaneurons under Electron Microscopy and X-Ray Microscopy using miniSOG

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      bioRxiv

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          Abstract

          Large dimension, high-resolution imaging is important for neural circuit visualisation as neurons have both long- and short-range patterns: from axons and dendrites to the numerous synapses at their endings. Electron Microscopy (EM) is the favoured approach for synaptic resolution imaging but how such structures can be segmented from high-density images within large volume datasets remains challenging. Fluorescent probes are widely used to localise synapses, identify cell-types and in tracing studies. The equivalent EM approach would benefit visualising such labelled structures from within sub-cellular, cellular, tissue and neuroanatomical contexts. Here we developed genetically-encoded, electron-dense markers using miniSOG. We demonstrate their ability in 1) labelling cellular sub-compartments of genetically-targeted neurons, 2) generating contrast under different EM modalities, and 3) segmenting labelled structures from EM volumes using computer-assisted strategies. We also tested non-destructive X-ray imaging on whole Drosophilabrains to evaluate contrast staining. This enables us to target specific regions for EM volume acquisition.

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          Author and article information

          Journal
          bioRxiv
          August 22 2016
          Article
          10.1101/070755
          ebe5f231-aaf2-4e2b-a654-f550b5cf15f6
          © 2016
          History

          Molecular medicine,Neurosciences
          Molecular medicine, Neurosciences

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