Abstract

Over the past 26 months our laboratory has investigated G-protein expression and AC activity in alcoholics, nonalcoholics and the nonalcoholic family members of both groups. Our 'work in progress' demonstrates differential expression of Gsalpha levels in nonalcoholic individuals with a family history of alcoholism [family history positive (FHP) compared to nonalcoholic individuals without a family history of alcoholism (family history negative (FHN)]. These data suggest an intrinsic abnormality in the AC system of alcoholics and those biologically vulnerable to this disorder. In our renewal, we shall confirm our important observation that FHP nonalcoholic subjects have enhanced expression of Gsalpha in erythrocyte and lymphocyte membranes by increasing the sample size and including female subjects. We will examine cell lines from control, alcoholic, and unaffected children of alcoholic subjects. From the promising elements, we shall examine the particularly informative stage IV families for appropriate linkage analysis. We shall investigate the potential significance of differential expression of Gsalpha in FHP and FHN nonalcoholic subjects by correlating membrane G-protein expression/function (conducted at JHU) with sophisticated studies of tolerance/activation. The significance of membrane Gsalpha levels in the development of tolerance will be pursued utilizing two manipulatable models of G-protein expression. In the first model, we will employ several stable cell lines created from S49 cells which were designed to have varying degrees of Gsalpha expression. These cell lines recapitulate the spectrum of G-protein expression in humans. We shall test the hypothesis that the degree of ethanol-induced activation/tolerance in the AC system is proportional to amount of Gsalpha expression. We will also utilize a transgenic mouse model of enhanced Gsalpha expression to determine the effects of varying amounts of cellular Gsalpha on the acquisition of tolerance on the whole animal level. Lastly, we shall continue our studies determining if genetic linkage exists between the inheritance of the alcoholism phenotype and specific Gsalpha gene alleles. To date, our analysis has allowed us to detect several polymorphisms in the Gsalpha. We shall obtain DNA from cell lines of control, alcoholic, and unaffected children of alcoholic subjects. From the promising elements, we shall examine the particularly informative stage IV families for appropriate linkage analysis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Alcohol Abuse and Alcoholism (NIAAA)
Type
Research Project (R01)
Project #
5R01AA009000-05
Application #
2045025
Study Section
Biochemistry, Physiology and Medicine Subcommittee (ALCB)
Project Start
1991-08-01
Project End
1999-07-31
Budget Start
1995-08-01
Budget End
1996-07-31
Support Year
5
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Kelly, M P; Stein, J M; Vecsey, C G et al. (2009) Developmental etiology for neuroanatomical and cognitive deficits in mice overexpressing Galphas, a G-protein subunit genetically linked to schizophrenia. Mol Psychiatry 14:398-415, 347
Kelly, Michele P; Cheung, York-Fong; Favilla, Christopher et al. (2008) Constitutive activation of the G-protein subunit Galphas within forebrain neurons causes PKA-dependent alterations in fear conditioning and cortical Arc mRNA expression. Learn Mem 15:75-83
Yang, Xiaoju; Wang, Shelun; Rice, Kenner C et al. (2008) Restraint stress and ethanol consumption in two mouse strains. Alcohol Clin Exp Res 32:840-52
Kelly, Michele P; Isiegas, Carolina; Cheung, York-Fong et al. (2007) Constitutive activation of Galphas within forebrain neurons causes deficits in sensorimotor gating because of PKA-dependent decreases in cAMP. Neuropsychopharmacology 32:577-88
Germain-Lee, Emily L; Schwindinger, William; Crane, Janet L et al. (2005) A mouse model of albright hereditary osteodystrophy generated by targeted disruption of exon 1 of the Gnas gene. Endocrinology 146:4697-709
Chandler, L Judson; Bonci, Antonello; Wand, Gary S et al. (2004) Recent advances in cyclic-adenosine monophosphate/protein kinase A signaling in ethanol-induced synaptic and behavioral alterations. Alcohol Clin Exp Res 28:1129-36
Yang, Xioaju; Oswald, Lynn; Wand, Gary (2003) The cyclic AMP/protein kinase A signal transduction pathway modulates tolerance to sedative and hypothermic effects of ethanol. Alcohol Clin Exp Res 27:1220-5
Wand, G; Levine, M; Zweifel, L et al. (2001) The cAMP-protein kinase A signal transduction pathway modulates ethanol consumption and sedative effects of ethanol. J Neurosci 21:5297-303
Yang, X; Wand, G (2000) Ethanol uses cAMP-independent signal transduction mechanisms to activate proenkephalin promoter activity in rat C6 glioma cells. Alcohol Clin Exp Res 24:952-7
Yang, X; Horn, K; Baraban, J M et al. (1998) Chronic ethanol administration decreases phosphorylation of cyclic AMP response element-binding protein in granule cells of rat cerebellum. J Neurochem 70:224-32

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