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Biophys. J. BioFAST: First Published August 11, 2006. doi:10.1529/biophysj.106.091421
© 2006 by the Biophysical Society.


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MEMBRANES

Transbilayer effects of raft-like lipid domains in asymmetric planar bilayers measured by single molecule tracking

Volker Kiessling 1, Jonathan M. Crane 2 and Lukas K. Tamm 1*

1 University of Virginia
2 University of California San Francisco

* To whom correspondence should be addressed. E-mail: lkt2e{at}virginia.edu.

Submitted on June 15, 2006
Revised on July 12, 2006
Accepted on 24 July 2006


   Abstract
Cell membranes have complex lipid compositions, including an asymmetric distribution of phospholipids between the opposing leaflets of the bilayer. While it has been demonstrated that the lipid composition of the outer leaflet of the plasma membrane is sufficient for the formation of raft-like liquid-ordered (lo) phase domains, the influence that such domains may have on the lipids and proteins of the inner leaflet remains unknown. We used tethered polymer supports and a combined Langmuir-Blodgett/vesicle fusion (LB/VF) technique to build asymmetric planar bilayers that mimic plasma membrane asymmetry in many ways. We show that directly supported LB monolayers containing cholesterol-rich lo phases are inherently unstable when exposed to water or vesicle suspensions. However, tethering the LB monolayer to the solid support with the lipid-anchored polymer 1,2-dimyristoyl phophatidylethanolamine-N-[poly(ethylene glycol)-triethoxysilane] significantly improves stability and allows for the formation of complex planar supported bilayers that retain >90% asymmetry for one to two hours. We developed a single molecule tracking (SPT) system for the study of lipid diffusion in asymmetric bilayers with coexisting liquid phases. SPT allowed us to study in detail the diffusion of individual lipids inside, outside, or directly opposed to lo phase domains. We show here that lo phase domains in one monolayer of an asymmetric bilayer do not induce the formation of domains in the opposite leaflet when this leaflet is composed of palmitoyl-oleoyl phosphatidylcholine and cholesterol, but do induce domains when this leaflet is composed of porcine brain phosphatidylcholine, phosphatidylethanolamine, phosphatidylserine, and cholesterol. The diffusion of lipids is similar in lo and ld phase domains and is not affected by transbilayer coupling indicating that lateral and transverse lipid interactions that give rise to the domain structure are weak in the biological lipid mixtures that were employed in this work.

Key Words: diffusion, lipid, lipid asymmetry, single molecule fluorescence, supported bilayers




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Copyright © 2006 by the Biophysical Society.