Abstract

A growing body of evidence, contributed to significantly by work from the previous funding cycle, has demonstrated that gap junction channels display a surprising level of selectivity for their permeants, dictated by the connexin composition of the channels. The basis of this selectivity is complex, but understanding it will be critical to defining the diverse role these intercellular channels play in normal and pathogenic cell function. It is likely that the principles governing selective permeabilities of these channels will be distinct from the much better studied ion channels, and will require a new generation of tools. The current proposal seeks to develop these tools and to apply them to a mapping of the molecular determinants of permeabilty through these channels. A comparative analysis of gap junction channels comprised of different connexins that display very different permeability properties should define the structural diversity within these pores that may underlie their different properties (Aim #1). Scanning and targetted mutagenic and labeling strategies will then be used in the different connexins to map selectivity determinants for size and charge of permeants, as well as mapping sites of affinity for natural permants (Aim #2). We also propose the first comprehensive comparison of peremability characteristics and pore structure of intercellular gap junction channels and their corresponding hemichannels on the cell surface (Aim #3). Initial evidence suggests that there may be significant differences between these two channel isoforms, and growing evidence for the physiological significance of hemichannels in several processes, including cell death via apoptosis, etc., makes understanding such differences critical. The comparative studies proposed here should also resolve a controversy in the literature over the actual nature of the pore lining. While different members of the gap junction family have been mapped as the genetic causes of a surprising variety of human diseases, from catarracts, skin disease and peripheral nerve paralysis to the most common form of hereditary sensorineural deafness, we still have almost no understanding of how damage to these genes can cause the phenotypes observed. The current work will make a significant stride in resolving this issue by defining the molecular structure of these intercellular pores and how this can regulate what goes through them. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM055437-15
Application #
7387466
Study Section
Membrane Biology and Protein Processing (MBPP)
Program Officer
Shapiro, Bert I
Project Start
1997-01-01
Project End
2010-03-31
Budget Start
2008-04-01
Budget End
2009-03-31
Support Year
15
Fiscal Year
2008
Total Cost
$296,291
Indirect Cost

  Institution

Name
University of Texas Health Science Center San Antonio
Department
Biochemistry
Type
Schools of Medicine
DUNS #
800772162
City
San Antonio
State
TX
Country
United States
Zip Code
78229

  Publications

Polusani, Srikanth R; Kalmykov, Edward A; Chandrasekhar, Anjana et al. (2016) Cell coupling mediated by connexin 26 selectively contributes to reduced adhesivity and increased migration. J Cell Sci 129:4399-4410
Chandrasekhar, Anjana; Kalmykov, Edward A; Polusani, Srikanth R et al. (2013) Intercellular redistribution of cAMP underlies selective suppression of cancer cell growth by connexin26. PLoS One 8:e82335
Xu, Ji; Nicholson, Bruce J (2013) The role of connexins in ear and skin physiology - functional insights from disease-associated mutations. Biochim Biophys Acta 1828:167-78
Liu, Jialu; Xu, Ji; Gu, Sumin et al. (2011) Aquaporin 0 enhances gap junction coupling via its cell adhesion function and interaction with connexin 50. J Cell Sci 124:198-206
Oshima, Atsunori; Tani, Kazutoshi; Toloue, Masoud M et al. (2011) Asymmetric configurations and N-terminal rearrangements in connexin26 gap junction channels. J Mol Biol 405:724-35
Ambrosi, Cinzia; Boassa, Daniela; Pranskevich, Jennifer et al. (2010) Analysis of four connexin26 mutant gap junctions and hemichannels reveals variations in hexamer stability. Biophys J 98:1809-19
Starich, Todd A; Xu, Ji; Skerrett, I Martha et al. (2009) Interactions between innexins UNC-7 and UNC-9 mediate electrical synapse specificity in the Caenorhabditis elegans locomotory nervous system. Neural Dev 4:16
Martínez, Agustín D; Acuña, Rodrigo; Figueroa, Vania et al. (2009) Gap-junction channels dysfunction in deafness and hearing loss. Antioxid Redox Signal 11:309-22
Banks, Eric A; Toloue, Masoud M; Shi, Qian et al. (2009) Connexin mutation that causes dominant congenital cataracts inhibits gap junctions, but not hemichannels, in a dominant negative manner. J Cell Sci 122:378-88
Toloue, M M; Woolwine, Y; Karcz, J A et al. (2008) Site-directed mutagenesis reveals putative regions of protein interaction within the transmembrane domains of connexins. Cell Commun Adhes 15:95-105

Showing the most recent 10 out of 14 publications