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Sodium Entry into Amiloride-Sensitive Epithelia

$362,500R56FY2009DKNIH

University Of Alabama At Birmingham, Birmingham AL

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Abstract

Abstract Sodium transporting epithelia, such as renal distal and collecting tubules, function to control whole-body sodium homeostasis. Epithelial sodium channels (ENaC) have been found in other sodium transporting epithelia, e.g., salivary glands, colon, bronchial and tracheal epithelia, as well as in many non-epithelial cells, like lymphocytes, neurons, and astrocytes. Amiloride inhibition is a hallmark of these particular channels, regardless of the system in which they are found. Yet, when macroscopic and single channel properties are examined using the patch clamp technique, a myriad of biophysical characteristics emerge. The central hypothesis of this application is that the observed functional diversity of amiloride- sensitive sodium channels results, in part, from different combinations of subunits of the Degenerin (DEG)/ENaC superfamily of ion channels. There are three specific aims. In the first specific aim, we will determine the biochemical composition of an amiloride-sensitive cation channel found in epithelial cells that exhibit biophysical properties different from ENaC. We present preliminary data using RT-PCR profiling showing that message for a variety of DEG/ENaC members are present in these cells. Thus, we will use these cells as model systems to determine the biochemical composition of this channel. In addition, we will employ surface biotinylation and co-immunoprecipitation analysis to verify subunit interactions. We will also use cellular protein knockout approaches (and MTS reagent susceptibility studies) to establish subunit interaction. The second specific aim is to: a.) determine the biophysical characteristics of hybrid ENaC/ASIC, b.) identify ENaC/ASIC interaction using MTS reagent susceptibility. The third specific aim will determine the identify high resolution crystal structure of [unreadable]-ENaC. These results will offer new insights into the nature and ultimately the regulation of amiloride-sensitive sodium channels, and the ways that these hybrid channels can be modulated by inserting or deleting specific subunits of this DEG/ENaC superfamily. Thus, understanding the molecular basis for ENaC diversity will provide unique opportunities for therapeutic interventions in an ever-increasing plethora of ENaC-related diseases.

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