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
Neuropilin-2 is required in vivo for selective axon guidance responses to secreted semaphorins.
Authors: Authors: Giger RJ, Cloutier JF, Sahay A, Prinjha RK, Levengood DV, Moore SE, Pickering S, Simmons D, Rastan S, Walsh FS, Kolodkin AL, Ginty DD, Geppert M.
Neuron
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Mediation by a CREB family transcription factor of NGF-dependent survival of sympathetic neurons.
Authors: Authors: Riccio A, Ahn S, Davenport CM, Blendy JA, Ginty DD.
Science
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Characterization of an NGF-P-TrkA retrograde-signaling complex and age-dependent regulation of TrkA phosphorylation in sympathetic neurons.
Authors: Authors: Tsui-Pierchala BA, Ginty DD.
J Neurosci
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A late phase of cerebellar long-term depression requires activation of CaMKIV and CREB.
Authors: Authors: Ahn S, Ginty DD, Linden DJ.
Neuron
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Patterning of cortical efferent projections by semaphorin-neuropilin interactions.
Authors: Authors: Polleux F, Giger RJ, Ginty DD, Kolodkin AL, Ghosh A.
Science
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Neuropilin-2 is a receptor for semaphorin IV: insight into the structural basis of receptor function and specificity.
Authors: Authors: Giger RJ, Urquhart ER, Gillespie SK, Levengood DV, Ginty DD, Kolodkin AL.
Neuron
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Identification and characterization of novel substrates of Trk receptors in developing neurons.
Authors: Authors: Qian X, Riccio A, Zhang Y, Ginty DD.
Neuron
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Effects of PS1 deficiency on membrane protein trafficking in neurons.
Authors: Authors: Naruse S, Thinakaran G, Luo JJ, Kusiak JW, Tomita T, Iwatsubo T, Qian X, Ginty DD, Price DL, Borchelt DR, Wong PC, Sisodia SS.
Neuron
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A dominant-negative inhibitor of CREB reveals that it is a general mediator of stimulus-dependent transcription of c-fos.
Authors: Authors: Ahn S, Olive M, Aggarwal S, Krylov D, Ginty DD, Vinson C.
Mol Cell Biol
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Steering clear of semaphorins: neuropilins sound the retreat.
Authors: Authors: Kolodkin AL, Ginty DD.
Neuron
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