| Literature DB >> 32795398 |
Matthew B Veldman1, Chang Sin Park1, Charles M Eyermann1, Jason Y Zhang1, Elizabeth Zuniga-Sanchez2, Arlene A Hirano3, Tanya L Daigle4, Nicholas N Foster5, Muye Zhu5, Peter Langfelder1, Ivan A Lopez6, Nicholas C Brecha7, S Lawrence Zipursky2, Hongkui Zeng4, Hong-Wei Dong8, X William Yang9.
Abstract
Cajal recognized that the elaborate shape of neurons is fundamental to their function in the brain. However, there are no simple and generalizable genetic methods to study neuronal or glial cell morphology in the mammalian brain. Here, we describe four mouse lines conferring Cre-dependent sparse cell labeling based on mononucleotide repeat frameshift (MORF) as a stochastic translational switch. Notably, the optimized MORF3 mice, with a membrane-bound multivalent immunoreporter, confer Cre-dependent sparse and bright labeling of thousands of neurons, astrocytes, or microglia in each brain, revealing their intricate morphologies. MORF3 mice are compatible with imaging in tissue-cleared thick brain sections and with immuno-EM. An analysis of 151 MORF3-labeled developing retinal horizontal cells reveals novel morphological cell clusters and axonal maturation patterns. Our study demonstrates a conceptually novel, simple, generalizable, and scalable mouse genetic solution to sparsely label and illuminate the morphology of genetically defined neurons and glia in the mammalian brain.Entities:
Keywords: Cre; MORF; astrocyte; imaging; microglia; morphology; neuron; reconstruction; spaghetti monster; sparse labeling
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Year: 2020 PMID: 32795398 PMCID: PMC7572760 DOI: 10.1016/j.neuron.2020.07.019
Source DB: PubMed Journal: Neuron ISSN: 0896-6273 Impact factor: 17.173