Abstract

The Transgenic Core provides all of our Projects with state-of-the-art tools to enable manipulation of specific genes of interest in brain reward regions in the context of animal models of drug abuse and addiction. Centralizing these functions within a single Core derives substantial cost savings and ensures the proper and rigorous use of these approaches. First, numerous lines of transgenic and knockout mice, generated by PPG investigators or obtained from other laboratories, are required for the PPG's research. The Core is responsible for breeding, genotyping, and maintaining the progeny for use by the individual Projects, as well as providing the appropriate control mice. Careful consideration is given to genetic background and we use wildtype littermate controls for all experiments. The Core is also responsible for generating several new lines of transgenic and knockout mice required for the proposed program of research. Prominent among the existing and proposed new mouse lines are those that manipulate the expression of specific genes both temporally and spatially, i.e., inducible and cell-targeted mutations. Our group has substantial experience with these methods, which include use of the tetracycline gene regulation system and the Cre-loxP system. Indeed, Core research has succeeded in developing truly inducible, cell-targeted gene knockouts in brain reward regions. Second, the Core provides Project investigators with vectors for viral-mediated gene transfer, a crucial tool used in our research program. PPG investigators have played a leading role nationally in these efforts, and now routinely use Herpes simplex and Adeno-associated viral vectors. This work includes viral expression of Cre recombinase to induce highly localized knockouts in brain, and the expression of small hairpin RNA's to induce knockdowns of genes via an RNA interference (RNAi) mechanism. We are very proud of the Core's achievements over the past 4 years, and we will work during the next Grant period to introduce further innovations in mouse mutagenesis and viral gene transfer for studies of the molecular basis of drug addiction.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Program Projects (P01)
Project #
3P01DA008227-21S1
Application #
8684705
Study Section
Special Emphasis Panel (ZDA1-RXL-E)
Project Start
Project End
Budget Start
2013-07-01
Budget End
2013-12-30
Support Year
21
Fiscal Year
2013
Total Cost
$183,713
Indirect Cost
$66,553

  Institution

Name
Icahn School of Medicine at Mount Sinai
Department
Type
DUNS #
078861598
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Monteggia, Lisa M; Heimer, Hakon; Nestler, Eric J (2018) Meeting Report: Can We Make Animal Models of Human Mental Illness? Biol Psychiatry 84:542-545
Clark, Christopher R; Maile, Makayla; Blaney, Patrick et al. (2018) Transposon mutagenesis screen in mice identifies TM9SF2 as a novel colorectal cancer oncogene. Sci Rep 8:15327
Cates, Hannah M; Heller, Elizabeth A; Lardner, Casey K et al. (2018) Transcription Factor E2F3a in Nucleus Accumbens Affects Cocaine Action via Transcription and Alternative Splicing. Biol Psychiatry 84:167-179
Cahill, M E; Walker, D M; Gancarz, A M et al. (2018) The dendritic spine morphogenic effects of repeated cocaine use occur through the regulation of serum response factor signaling. Mol Psychiatry 23:1474-1486
Hamilton, Peter J; Burek, Dominika J; Lombroso, Sonia I et al. (2018) Cell-Type-Specific Epigenetic Editing at the Fosb Gene Controls Susceptibility to Social Defeat Stress. Neuropsychopharmacology 43:272-284
Egervari, Gabor; Kozlenkov, Alexey; Dracheva, Stella et al. (2018) Molecular windows into the human brain for psychiatric disorders. Mol Psychiatry :
de la Fuente Revenga, Mario; Ibi, Daisuke; Saunders, Justin M et al. (2018) HDAC2-dependent Antipsychotic-like Effects of Chronic Treatment with the HDAC Inhibitor SAHA in Mice. Neuroscience 388:102-117
Anderson, Ethan M; Sun, Haosheng; Guzman, Daniel et al. (2018) Knockdown of the histone di-methyltransferase G9a in nucleus accumbens shell decreases cocaine self-administration, stress-induced reinstatement, and anxiety. Neuropsychopharmacology :
Hamilton, Peter J; Lim, Carissa J; Nestler, Eric J et al. (2018) Stereotaxic Surgery and Viral Delivery of Zinc-Finger Epigenetic Editing Tools in Rodent Brain. Methods Mol Biol 1867:229-238
Inquimbert, Perrine; Moll, Martin; Latremoliere, Alban et al. (2018) NMDA Receptor Activation Underlies the Loss of Spinal Dorsal Horn Neurons and the Transition to Persistent Pain after Peripheral Nerve Injury. Cell Rep 23:2678-2689

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