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Kathryn M. Murphy

Researcher at McMaster University

Publications -  61
Citations -  1839

Kathryn M. Murphy is an academic researcher from McMaster University. The author has contributed to research in topics: Visual cortex & Monocular deprivation. The author has an hindex of 24, co-authored 60 publications receiving 1718 citations. Previous affiliations of Kathryn M. Murphy include Dalhousie University & University of California, Berkeley.

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D1-dopamine receptor agonists selectively activate striatal c-fos independent of rotational behaviour.

TL;DR: A mechanism by which D1-dopamine receptor mechanisms may regulate long-term changes in dopaminergic systems is suggested, which is mediated by dopamine receptors in the striatum.
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Peripheral-type benzodiazepine receptors in the central nervous system: localization to olfactory nerves

TL;DR: Binding levels of [3H]Ro5–4864, a ligand selective for peripheral-type benzodiazepine receptors, are substantially higher in homogenates of the olfactory bulb than in the rest of the brain, suggesting that these binding sites appear in large part to be localized to Olfactory nerves which originate in the nasal epithelium.
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Developmental changes in GABAergic mechanisms in human visual cortex across the lifespan.

TL;DR: This study shows for the first time how GABAergic mechanisms develop in the human visual cortex across the lifespan, and provides key information for translating therapies developed in animal models into effective treatments for amblyopia in humans.
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Development of human visual cortex: a balance between excitatory and inhibitory plasticity mechanisms.

TL;DR: In this paper, the expression of the major glutamatergic receptors, GABAA receptors, and glutamic acid decarboxylase (GAD) isoforms during the first 6 years of postnatal development of human visual cortex was studied.
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The development of human visual cortex and clinical implications.

TL;DR: Five stages of development for human V1 that start in infancy and continue across the life span are described, compared with visual and anatomical milestones, and implications for translating treatments for visual disorders that depend on neuroplasticity of V1 function are discussed.