Lipids hexagonal phase-forming

Fig. 8a. Time-resolved small-angle diffraction from a dispersion of a hexagonal-phase forming lipid (l-hexadecyl-2-oleoyl-phosphatidylethanolamine, HOPE) in the presence of excess water (c, p 0.2), during a heating- and cooling experiment. The temperature course are shown in the inserts, b contour-line plots of the intensities. (From Ref. 74, with permission)...

FIG. 15 Cellular entry and intracellular kinetics of the cationic lipid-DNA complexes. Cationic lipid-DOPE liposomes form electrostatic complexes with DNA, and, in this case, also transferrin (Tf) is incorporated. Cellular uptake by endoc5dosis and endosomal acidification can be blocked with cytochaiasin B and bafilomycin Aj, respectively. DNA is proposed to be released at the level of endosomal wall after fusion of the carrier lipids with endosomal bilayer. This process is facilitated by the formation of inverted hexagonal DOPE phase as illustrated in the lower corner on the right. After its release to the C5doplasm DNA may enter the nucleus. (From Ref. 253. By permission of Nature Publishing Group.)... 

Cyclic carbohydrates with two alkyl chains (e.g. 1,2-dialkyl (or 1,2-diacyl) glycerol 8 a (sug=Glcp, Galp) present structural similarities with glycerophospho-lipids. They form complex mesophases such as bicontinuous cubic phases, inverted hexagonal phases or myelin figures [58-61]. Other dialkyl derivatives... 

Generally, lipids forming lamellar phase by themselves, form lamellar lipoplexes in most of these cases, lipids forming Hn phase by themselves tend to form Hn phase lipoplexes. Notable exceptions to this rule are the lipids forming cubic phase. Their lipoplexes do not retain the cubic symmetry and form either lamellar or inverted hexagonal phase [20, 24], The lamellar repeat period of the lipoplexes is typically 1.5 nm higher than that of the pure lipid phases, as a result of DNA intercalation between the lipid bilayers. In addition to the sharp lamellar reflections, a low-intensity diffuse peak is also present in the diffraction patterns (Fig. 23a) [81]. This peak has been ascribed to the in-plane positional correlation of the DNA strands arranged between the lipid lamellae [19, 63, 64, 82], Its position is dependent on the lipid-DNA ratio. The presence of DNA between the bilayers has been verified by the electron density profiles of the lipoplexes [16, 62-64] (Fig. 23b). 

Certain cationic lipids were found to form inverted hexagonal phase lipoplexes [21, 46, 85-87]. The Hn phase lipoplexes consist of DNA coated by lipid monolayers and arranged on a two-dimensional hexagonal lattice. This arrangement is identified by small-angle X-ray reflections in the ratio 1 3 4 (Fig. 24a). The lower intensity of the (11) and (20) lipoplex diffraction peaks relative to the Hn pattern... 

Fig. 24 Inverted hexagonal phase lipoplexes with cationic PCs forming HII phase (a) and cubic Pn3m phase (b). Lipid/DNA 4 1 w/w, 37 °C [46] (reproduced by permission of the Royal Society of Chemistry)...

Due to its ability to form inverted hexagonal phase, DOPE is believed to impart fusogenicity to lipoplexes, thus facilitating fusion followed by destabilization of the endosomal membrane, lipoplex escape from the endosomes, and eventually the DNA release. Indeed, inclusion of DOPE into lipoplexes was shown to enhance considerably the transfection activity of some of the cationic lipid carriers [35,120, 121]. For example, formulations of oxypropyl quaternary ammonium cationic lipids with 50 mol% DOPE have been reported to exhibit 2-5 times higher transfection activity in COS7 cells than formulations with pure cationic lipid (Fig. 29) [35]. Recently, a triple-bond dialkynoyl analog of DOPE has been... 

CL-DNA complexes form spontaneously when solutions of cationic liposomes (typically containing both a cationic lipid and a neutral helper lipid) are combined. We have discovered several distinct nanoscale structures of CL-DNA complexes by synchrotron X-ray diffraction, three of which are schematically shown in Fig. 1. These are the prevalent lamellar phase with DNA sandwiched between cationic membranes (Lo,c) [22], the inverted hexagonal phase with DNA encapsulated within inverse lipid tubes (Hnc) [23], and the more recently discovered Hj0 phase with hexagonally arranged rod-like micelles surrounded by DNA chains forming a continuous substructure with honeycomb symmetry [24]. Both the neutral lipid and the cationic lipid can drive the formation of specific structures of CL-DNA complexes. The inverse cone shape of DOPE favors formation of the... 

The above-mentioned physicochemical properties of phospholipids lead to spontaneous formation of bilayers. Depending on the water-lipid ratio, on the type of phospholipids, and the temperature, the bilayer exists in different, defined mesomorphic physical organizations. These are the La high-temperature liquid crystalline form, the Lp gel form with restricted movement of the hydrocarbon chains, and an inverted hexagonal phase, Hn (see Sections 1.3.1 and 1.3.2). 

When temperature is raised, the membrane bilayer not only becomes increasingly fluid due to enhanced motions of acyl chain, but it also tends to shift increasingly towards forming lipid aggregates in the inverted hexagonal phase (.hexagonal II, Hn, phase) (Hazel, 1995). The temperature at which this type of phase change... 

The propensity of membranes to fuse correlates with the fraction of inverted phase-forming lipids conversely, membrane fusability is reduced with an increase of the lipid fraction that inhibits inverted phase formation. Substantial evidence suggests that the mechanism of lipid membrane fusion is related to the mechanism of lamellar/inverted phase transitions (23). The intermediates that form in membrane fusion seem to be identical to those that form during the transformations between lamellar, bicontinuous inverted cubic and inverted hexagonal lipid liquid-crystalline phases, and these transitions can be used successfully as a model for studying the lipid membrane fusion mechanism and kinetics. 

Proposed more than 20 years ago, the stalk intermediate—a highly curved lipid stmcture— provides the most plausible description of the initial fusion stage currently available. The related stalk-pore mechanism (23-25) of fusion is viewed favorably by most researchers. It shows the close relation between fusion and the transition from lamellar into bilayer cubic and hexagonal phases (see Fig. 4 in the section entitled Formation of nonlamellar phases in membrane lipids ). Studies on the rhombohedral phase formed in partially dehydrated lipids provide another insight into the possible structure of fusion stalks (26). 

---