Four synthetic anion transporters (SATs) having the general formula (n-C(18)H(37))2N-COCH(2)OCH,CO-(Gly)(3)Pro-Lys(epsilon-N-R)-(Gly)(2)-O-n-C(7)H(15) were prepared and studied. The group R was Cbz, H (TFA salt), t-Boc, and dansyl in peptides 1, 2, 3, and 4 respectively. The glutamine analog (GGGPQAG sequence) was also included. A dansyl-substituted fluorescent SAT was used to probe peptide insertion; the dansyl sidechain resides in an environment near the bilayer's midpolar regime. When the lysine sidechain was free or protected amine, little effect was noted on final Cl(-) transport rate in DOPC : DOPA (7 : 3) liposomes. This stands in contrast to the significant retardation of transport previously observed when a negative glutamate residue was present in the peptide sequence. It was also found that Cl- release from liposomes depended on the phospholipid composition of the vesicles. Chloride transport diminished significantly for the free lysine containing SAT, 2, when the lipid was altered from DOPC: DOPA to pure DOPC. Amide-sidechained SATs I and 5 showed a relatively small decrease in Cl- transport. The effect of lipid composition on Cl- transport was explained by differences in electrostatic interaction between amino acid sidechain and lipid headgroup, which was modeled by computation.

• 出版日期2008-8-21