Abstract

Gap junctions are the plasma membrane specializations, present between most types of contacting cells, through which the passive movement of small molecules from one cell to another occurs (direct cell-cell communication). Many studies have indicated that cell growth, development and differentiation may be regulated by the passage of small molecules through these junctions. The long-term objective of this study is to understand the significance of gap junctional communication, how it is established and regulated. The major focus of the proposed studies is to identify the covalent modifications, such as proteolytic processing and covalent derivatization, that the gap junction undergoes along the pathway from initial synthesis of gap junction polypeptides through the assembly and regulation of mature gap junctions. Particular emphasis will be placed on how these modifications function to permit assembly of junctions and regulation of communication. The initial steps in this process will be analyzed by in vitro translation of mRNA, while latter steps will be examined in tissue culture cells, including one in which the terminal steps in assembly can be induced by incubation with cAMP. The interaction of the gap junction protein with other cellular polypeptides, including calmodulin, will be investigated. The proposed experiments capitalize on properties of recently developed antibodies to the 27,000-dalton (27kD) major polypeptide of rat liver gap junctions. These polyclonal, precipitating antibodies recognize 27kD polypeptides with similar characteristics in a wide variety of tissues and cultured cell lines. Additional antibodies, both polyclonal and monoclonal, with different specificities, will also be generated for use in this investigation. Topological studies, using both biochemical and immunochemical approaches, will be undertaken to develop a model for the disposition of the protein in the plasma membrane lipid bilayer. Attempts will be made to reconstitute gap junctional communication in vitro in both planar bilayers and liposomes to develop systems for direct analysis of the regulatory mechanisms of gap junctional communication. Information obtained from these studies ultimately will be applied to analysis of other systems, including many transformed cells in which gap junctional communication is altered or absent.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
7R01GM030667-08
Application #
3278470
Study Section
Cellular Biology and Physiology Subcommittee 1 (CBY)
Project Start
1988-09-01
Project End
1990-04-30
Budget Start
1988-09-01
Budget End
1989-04-30
Support Year
8
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Albert Einstein College of Medicine
Department
Type
Schools of Medicine
DUNS #
009095365
City
Bronx
State
NY
Country
United States
Zip Code
10461

  Publications

Hertzberg, E L; Saez, J C; Corpina, R A et al. (2000) Use of antibodies in the analysis of connexin 43 turnover and phosphorylation. Methods 20:129-39
Minkoff, R; Parker, S B; Rundus, V R et al. (1997) Expression patterns of connexin43 protein during facial development in the chick embryo: associates with outgrowth, attachment, and closure of the midfacial primordia. Anat Rec 248:279-90
Saez, J C; Nairn, A C; Czernik, A J et al. (1997) Phosphorylation of connexin43 and the regulation of neonatal rat cardiac myocyte gap junctions. J Mol Cell Cardiol 29:2131-45
Nagy, J I; Hossain, M Z; Hertzberg, E L et al. (1996) Induction of connexin43 and gap junctional communication in PC12 cells overexpressing the carboxy terminal region of amyloid precursor protein. J Neurosci Res 44:124-32
Hofer, A; Saez, J C; Chang, C C et al. (1996) C-erbB2/neu transfection induces gap junctional communication incompetence in glial cells. J Neurosci 16:4311-21
Nagy, J I; Li, W; Hertzberg, E L et al. (1996) Elevated connexin43 immunoreactivity at sites of amyloid plaques in Alzheimer's disease. Brain Res 717:173-8
Donahue, H J; McLeod, K J; Rubin, C T et al. (1995) Cell-to-cell communication in osteoblastic networks: cell line-dependent hormonal regulation of gap junction function. J Bone Miner Res 10:881-9
Moreno, A P; Saez, J C; Fishman, G I et al. (1994) Human connexin43 gap junction channels. Regulation of unitary conductances by phosphorylation. Circ Res 74:1050-7
Parker, S B; Hertzberg, E L; Minkoff, R (1994) Modulation of gap junction-mediated intercellular communication in embryonic chick mesenchyme during tissue remodeling in vitro. Cell Tissue Res 275:215-24
Minkoff, R; Rundus, V R; Parker, S B et al. (1994) Gap junction proteins exhibit early and specific expression during intramembranous bone formation in the developing chick mandible. Anat Embryol (Berl) 190:231-41

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