Michael Greenberg

Michael Greenberg, PhD

Nathan Marsh Pusey Professor of Neurobiology

How Experience Shapes Gene Expression & Connectivity in the Brain

Our interactions with the outside world trigger changes in neurons that are critical for proper brain development and higher cognitive function. Experience-driven neuronal activity shapes gene expression in ways that promote the maturation and refinement of neural circuits.

The Greenberg lab studies precisely how, at a molecular level, neuronal activity controls gene expression and connectivity in the brain. A number of human brain developmental disorders, including autism and Rett syndrome, have now been linked to abnormalities in experience-driven brain pathways. Our lab studies the underlying basis of such neurological disorders.

Beginning in the mid-1980s, with the appreciation that growth factors trigger rapid transcription of an important activity-responsive gene called Fos, we have focused on elucidating the nature and role of neuronal transcriptional programs triggered by extracellular stimuli. In this effort, we have discovered various signaling pathways that convey neurotrophin and calcium-dependent signals from distal synapses (far from the cell body) to the nucleus of neurons, where transcription occurs. We have also studied the role of these activity-regulated transcriptional programs in modulating the plasticity of brain circuits.

Given the strong links between these processes and various human disorders of cognitive function, we continually seek to exploit our molecular insights to advance understanding of clinically relevant neurological conditions. Current projects in the lab include studies of sensory-driven circuit development, the role of enhancer elements in activity-dependent transcriptional responses, human-specific molecular neurobiology and the function of MeCP2, the gene mutated in Rett syndrome.

Publications View
Mapping the cis-regulatory architecture of the human retina reveals noncoding genetic variation in disease.
Authors: Authors: Cherry TJ, Yang MG, Harmin DA, Tao P, Timms AE, Bauwens M, Allikmets R, Jones EM, Chen R, De Baere E, Greenberg ME.
Proc Natl Acad Sci U S A
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MeCP2 Represses the Rate of Transcriptional Initiation of Highly Methylated Long Genes.
Authors: Authors: Boxer LD, Renthal W, Greben AW, Whitwam T, Silberfeld A, Stroud H, Li E, Yang MG, Kinde B, Griffith EC, Bonev B, Greenberg ME.
Mol Cell
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Editorial: Neural epigenetics.
Authors: Authors: Greenberg ME, Lomvardas S.
Curr Opin Neurobiol
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Chromatin Environment and Cellular Context Specify Compensatory Activity of Paralogous MEF2 Transcription Factors.
Authors: Authors: Majidi SP, Reddy NC, Moore MJ, Chen H, Yamada T, Andzelm MM, Cherry TJ, Hu LS, Greenberg ME, Bonni A.
Cell Rep
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A scalable platform for the development of cell-type-specific viral drivers.
Authors: Authors: Hrvatin S, Tzeng CP, Nagy MA, Stroud H, Koutsioumpa C, Wilcox OF, Assad EG, Green J, Harvey CD, Griffith EC, Greenberg ME.
Elife
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Sensory lesioning induces microglial synapse elimination via ADAM10 and fractalkine signaling.
Authors: Authors: Gunner G, Cheadle L, Johnson KM, Ayata P, Badimon A, Mondo E, Nagy MA, Liu L, Bemiller SM, Kim KW, Lira SA, Lamb BT, Tapper AR, Ransohoff RM, Greenberg ME, Schaefer A, Schafer DP.
Nat Neurosci
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Loss of Adaptive Myelination Contributes to Methotrexate Chemotherapy-Related Cognitive Impairment.
Authors: Authors: Geraghty AC, Gibson EM, Ghanem RA, Greene JJ, Ocampo A, Goldstein AK, Ni L, Yang T, Marton RM, Pasca SP, Greenberg ME, Longo FM, Monje M.
Neuron
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ARNT2 Tunes Activity-Dependent Gene Expression through NCoR2-Mediated Repression and NPAS4-Mediated Activation.
Authors: Authors: Sharma N, Pollina EA, Nagy MA, Yap EL, DiBiase FA, Hrvatin S, Hu L, Lin C, Greenberg ME.
Neuron
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A Late Phase of Long-Term Synaptic Depression in Cerebellar Purkinje Cells Requires Activation of MEF2.
Authors: Authors: Andzelm MM, Vanness D, Greenberg ME, Linden DJ.
Cell Rep
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Characterization of human mosaic Rett syndrome brain tissue by single-nucleus RNA sequencing.
Authors: Authors: Renthal W, Boxer LD, Hrvatin S, Li E, Silberfeld A, Nagy MA, Griffith EC, Vierbuchen T, Greenberg ME.
Nat Neurosci
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