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Biophysical Journal 85:1560-1575 (2003)
© 2003 The Biophysical Society

Enlargement and Contracture of C2-Ceramide Channels

Leah J. Siskind, Amirparviz Davoody, Naomi Lewin, Stephanie Marshall and Marco Colombini

Department of Biology, University of Maryland, College Park, Maryland 20742 USA

Correspondence: Address reprint requests to Marco Colombini, Tel.: 301-405-6925; Fax: 301-314-9358; E-mail: mc34{at}umail.umd.edu.

Ceramides are known to play a major regulatory role in apoptosis by inducing cytochrome c release from mitochondria. We have previously reported that ceramide, but not dihydroceramide, forms large and stable channels in phospholipid membranes and outer membranes of isolated mitochondria. C2-ceramide channel formation is characterized by conductance increments ranging from <1 to >200 nS. These conductance increments often represent the enlargement and contracture of channels rather than the opening and closure of independent channels. Enlargement is supported by the observation that many small conductance increments can lead to a large decrement. Also the initial conductances favor cations, but this selectivity drops dramatically with increasing total conductance. La+3 causes rapid ceramide channel disassembly in a manner indicative of large conducting structures. These channels have a propensity to contract by a defined size (often multiples of 4 nS) indicating the formation of cylindrical channels with preferred diameters rather than a continuum of sizes. The results are consistent with ceramides forming barrel-stave channels whose size can change by loss or insertion of multiple ceramide columns.




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