David D Ginty

David D Ginty, Ph.D.

Edward R. and Anne G. Lefler Professor of Neurobiology, Harvard Medical School
Head of the Department of Neurobiology, Harvard Medical School

Neurons and Circuits That Mediate Touch

The somatosensory system endows us with a remarkable capacity for recognizing textural differences and shapes of objects held in our hands, and to feel pain, pressure, temperature, position, movement and vibration. Understanding the neurobiological basis of touch perception will help us to determine why touch can be painful or aversive under certain pathological states.

The Ginty lab uses mouse molecular genetics, in vitro signaling approaches, circuit mapping, electrophysiological and behavioral analyses to gain understanding of the development, organization, and function of neural circuits that underlie the sense of touch. Mouse molecular genetic approaches are used to identify, visualize, and functionally manipulate physiologically defined classes of low-threshold mechanosensory neurons (LTMRs) and nociceptors, the primary cutaneous sensory neurons that mediate the sense of touch and pain. We also strive to gain genetic access to spinal cord interneurons and projection neurons to reveal the organizational logic and functions of touch and pain circuits in the spinal cord and brainstem.

Our current goals are to discover: 1) the unique functions and properties of LTMR and nociceptor subtypes; 2) the organization of synaptic connections between LTMR subtypes and nociceptors, spinal cord dorsal horn interneurons and projection neurons, and dorsal column nuclei neurons; 3) the neural circuits that underlie the perception of touch; 4) molecular and developmental mechanisms by which primary somatosensory neurons and touch and pain circuit organization are established; and 5) mechanisms of touch circuit dysfunction in mouse models of autism spectrum disorders and neuropathic pain.

Publications View
Growth and survival signals controlling sympathetic nervous system development.
Authors: Authors: Glebova NO, Ginty DD.
Annu Rev Neurosci
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Restricted inactivation of serum response factor to the cardiovascular system.
Authors: Authors: Miano JM, Ramanan N, Georger MA, de Mesy Bentley KL, Emerson RL, Balza RO, Xiao Q, Weiler H, Ginty DD, Misra RP.
Proc Natl Acad Sci U S A
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Vascular endothelial growth factor controls neuronal migration and cooperates with Sema3A to pattern distinct compartments of the facial nerve.
Authors: Authors: Schwarz Q, Gu C, Fujisawa H, Sabelko K, Gertsenstein M, Nagy A, Taniguchi M, Kolodkin AL, Ginty DD, Shima DT, Ruhrberg C.
Genes Dev
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Differential requirements for semaphorin 3F and Slit-1 in axonal targeting, fasciculation, and segregation of olfactory sensory neuron projections.
Authors: Authors: Cloutier JF, Sahay A, Chang EC, Tessier-Lavigne M, Dulac C, Kolodkin AL, Ginty DD.
J Neurosci
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A neurotrophin signaling cascade coordinates sympathetic neuron development through differential control of TrkA trafficking and retrograde signaling.
Authors: Authors: Kuruvilla R, Zweifel LS, Glebova NO, Lonze BE, Valdez G, Ye H, Ginty DD.
Cell
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Heterogeneous requirement of NGF for sympathetic target innervation in vivo.
Authors: Authors: Glebova NO, Ginty DD.
J Neurosci
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Semaphorin 3F is critical for development of limbic system circuitry and is required in neurons for selective CNS axon guidance events.
Authors: Authors: Sahay A, Molliver ME, Ginty DD, Kolodkin AL.
J Neurosci
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Evidence in support of signaling endosome-based retrograde survival of sympathetic neurons.
Authors: Authors: Ye H, Kuruvilla R, Zweifel LS, Ginty DD.
Neuron
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Neuropilin-1 conveys semaphorin and VEGF signaling during neural and cardiovascular development.
Authors: Authors: Gu C, Rodriguez ER, Reimert DV, Shu T, Fritzsch B, Richards LJ, Kolodkin AL, Ginty DD.
Dev Cell
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Signaling at the growth cone: ligand-receptor complexes and the control of axon growth and guidance.
Authors: Authors: Huber AB, Kolodkin AL, Ginty DD, Cloutier JF.
Annu Rev Neurosci
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