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Designing lipids for selective partitioning into liquid ordered membrane domains

Year: 2015

Journal: SOFT MATTER, Vol. 11, p 3241-3250, 20170208

Authors: Momin, Noor; Lee, Stacey; Gadok, Avinash K.; Busch, David J.; Bachand, George D.; Hayden, Carl C.; Stachowiak, Jeanne C.; Sasaki, Darryl Y.

Organizations: Sandia Natl Labs, Biotechnol & Bioengn Dept, Livermore, CA 94550 USA; Sandia Natl Labs, Combust Chem Dept, Livermore, CA USA; Sandia Natl Labs, Nanosyst Synth Anal Dept, Albuquerque, NM 87185 USA; Univ Texas Austin, Dept Biomed Engn, Austin, TX 78712 USA

Self-organization of lipid molecules into specific membrane phases is key to the development of hierarchical molecular assemblies that mimic cellular structures. While the packing interaction of the lipid tails should provide the major driving force to direct lipid partitioning to ordered or disordered membrane domains, numerous examples show that the headgroup and spacer play important but undefined roles. We report here the development of several new biotinylated lipids that examine the role of spacer chemistry and structure on membrane phase partitioning. The new lipids were prepared with varying lengths of low molecular weight polyethylene glycol (EGn) spacers to examine how spacer hydrophilicity and length influence their partitioning behavior following binding with FITC-labeled streptavidin in liquid ordered (L-o) and liquid disordered (L-d) phase coexisting membranes. Partitioning coefficients (K-p L-o/L-d) of the biotinylated lipids were determined using fluorescence measurements in studies with giant unilamellar vesicles (GUVs). Compared against DPPE-biotin, DPPE-cap-biotin, and DSPE-PEG2000-biotin lipids, the new dipalmityl-EGn-biotin lipids exhibited markedly enhanced partitioning into liquid ordered domains, achieving K-p of up to 7.3 with a decaethylene glycol spacer (DP-EG10-biotin). We further demonstrated biological relevance of the lipids with selective partitioning to lipid raft-like domains observed in giant plasma membrane vesicles (GPMVs) derived from mammalian cells. Our results found that the spacer group not only plays a pivotal role for designing lipids with phase selectivity but may also influence the structural order of the domain assemblies.