Understanding and optimizing microemulsions with magnetic room temperature ionic liquids (MRTILs).

Nonaqueous microemulsions containing the magnetic room temperature ionic liquid (MRTIL) bmimFeCl4 as polar phase were studied with respect to their macroscopic phase behavior and structure by means of small angle neutron scattering (SANS). The phase behavior was studied in detail for different alcohols as cosurfactant and different oils as nonpolar phase and mainly by varying the chain length of the used ionic surfactant (CnmimCl with n = 14, 16, 18). In general, phase behavior and structural ordering in the mesophases were found to be comparable to water systems where with increasing content of MRTIL the microemulsions seems to become less and less structured leading to a rough and softer interface with less long-range ordering. The extent of structuring increases with increasing chain length of the surfactant. However, the pure surfactant is not able to form microemulsions and a rather large amount of alcohol is required for stabilization, where the effectiveness of the alcohol increases with increasing chain length of the alcohol. From this comprehensive investigation systematic trends can be deduced in order to formulate correspondingly structured microemulsions with MRTIL as polar phase.

Self-assembly of imidazolium-based surfactants in magnetic room-temperature ionic liquids: binary mixtures.

The phase behaviour of binary mixtures of ionic surfactants (1-alkyl-3-imidazolium chloride, C(n)mimCl with n=14, 16 and 18) and imidazolium-based ionic liquids (1-alkyl-3-methylimidazolium tetrachloroferrate, C(n)mimFeCl4, with n=2 and 4) over a broad temperature range and the complete range of compositions is described. By using many complementary methods including differential scanning calorimetry (DSC), polarised microscopy, small-angle neutron and X-ray scattering (SANS/SAXS), and surface tension, the ability of this model system to support self-assembly is described quantitatively and this behaviour is compared with common water systems. The existence of micelles swollen by the solvent can be deduced from SANS experiments and represent a possible model for aggregates, which has barely been considered for ionic-liquid systems until now, and can be ascribed to the rather low solvophobicity of the surfactants. Our investigation shows that, in general, C(n)mimCl is a rather weak amphiphile in these ionic liquids. The amphiphilic strength increases systematically with the length of the alkyl chain, as seen from the phase behaviour, the critical micelle concentration, and also the level of definition of the aggregates formed.

Magnetic microemulsions based on magnetic ionic liquids.

Microemulsions with magnetic properties were formed by employing a magnetic room temperature ionic liquid (MRTIL) as polar phase, cyclohexane as oil, and an appropriate mixture of ionic surfactant and decanol as a cosurfactant. By means of small-angle neutron scattering (SANS) and electric conductivity the microemulsion structure could be confirmed, where the classical structural sequence of oil-continuous-bicontinuous-polar phase continuous is observed with increasing ratio [polar phase]/[oil]. Accordingly a maximum of the structural size is observed at about equal volumes of oil and MRTIL contained. Therefore this system is structurally the same as normal microemulsions but with the magnetic properties added to it by the incorporation into the systems formulation.

Influence of architecture on the interaction of negatively charged multisensitive poly(N-isopropylacrylamide)-co-methacrylic acid microgels with oppositely charged polyelectrolyte: absorption vs adsorption.

Two sets of core-shell microgels composed of temperature-sensitive poly(N-isopropylacrylamide) (PNiPAM) with different spatial distribution of pH-sensitive methacrylic acid (MAA) groups were prepared. The cores consist of either PNiPAM (neutral core; nc) or PNiPAM-co-MAA (charged core; cc). A charged shell existing of PNiPAM-co-MAA was added to the neutral core (yielding neutral core-charged shell; nccs), on the charged core, on the other hand, a neutral shell of PNiPAM was added (charged core-neutral shell; ccns). Complexes of these microgels with positively charged poly(diallyldimethylammonium chloride) (PDADMAC) of different molar masses were prepared. The amount of bound polyelectrolyte was quantified, and the microgel-polyelectrolyte complexes were characterized with respect to electrophoretic mobility and hydrodynamic radius. The penetration of polyelectrolyte into the microgel was also monitored by means of lifetime analysis of a fluorescent dye covalently bound to poly(L-lysine) providing information on the probe's local environment. The architecture of the microgel has a significant influence on the interaction with oppositely charged polyelectrolyte. Complexes with microgel with the charged shell tend to flocculate at charge ratios of 1 and are thus similar to polyelectrolyte complexes with rigid colloidal particles. Complexes with microgels that consist of a charged core and a neutral shell show very different properties: They are still temperature sensitive and reveal an influence of the polyelectrolyte's chain length. Low molecular weight PDADMAC can penetrate through the neutral shell into the charged core, and thus nearly no charge reversal occurs. The high-MW polyelectrolyte does not penetrate fully and leads to charge reversal. The results demonstrate that microgels are able to absorb or adsorb polyelectrolytes depending on the polyelectrolyte's chain length and the microgels architecture. Complexes with different surface properties and different colloidal stability can be prepared, and polyelectrolytes can be encapsulated in the microgel core. Thus, multisensitive core-shell microgels combine permeability and compartmentalization on a nanometer length scale and provide unique opportunities for applications in controlled uptake and release.

Early detection of decreased soluble HLA-G levels in the maternal circulation predicts the occurrence of preeclampsia and intrauterine growth retardation during further course of pregnancy.

PROBLEM: Soluble (s) HLA-G1/G5 molecules may potentially affect immune homeostasis during pregnancy. The aim of this study was to determine changes of sHLA-G1/G5 plasma levels throughout normal pregnancy and to assess its predictive value for the occurrence of characteristic gestation-associated diseases during further course of pregnancy. METHOD OF STUDY: sHLA-G1/G5 levels were estimated in plasma samples of 40 non-pregnant women, 291 women throughout normal pregnancy and 236 women affected by different complications. RESULTS: In comparison with non-pregnant women sHLA-G1/G5 levels strongly increased during the first trimenon and then decreased continuously toward term. Non-parametric discriminant analysis showed that women with significantly decreased sHLA-G1/G5 levels in the second trimenon had an increased risk of developing preeclampsia and/or intrauterine growth retardation (IUGR) during further course of pregnancy. However, in the third trimenon, sHLA-G1/G5 levels in affected women did not deviate significantly from those of non-affected women. Surprisingly, significantly increased sHLA-G1/G5 levels were detected in third trimenon women with uncontrollable preterm labor, but not in women with prolonged preterm rupture of fetal membranes. CONCLUSION: For the identification of women with an increased risk of IUGR and/or preeclampsia, measurement of sHLA-G1/G5 plasma levels may be a powerful new tool in prenatal diagnostics.

Prolonged preterm rupture of fetal membranes, a consequence of an increased maternal anti-fetal T cell responsiveness.

A fetus, although semi-allogeneic, is usually accepted by the maternal immune system. However, complications, including alloresponsive mechanisms, are thought to be potentially detrimental for a successful pregnancy. Therefore, we compared allogeneic T cell responses of nonpregnant women with the response of healthy pregnant women and pregnant women who have various gestation-associated diseases. Peripheral blood mononuclear cells (PBMCs) of all three groups were stimulated with PBMCs from unrelated volunteers. Pregnant women had significantly reduced stimulation indices (SIs) compared with nonpregnant women. Exposing PBMCs from pregnant women to PBMCs of their own fetus led to a further significant decrease of SIs. Among the two groups of pregnant individuals, SIs of women with prolonged preterm rupture of fetal membranes (PPROM) were significantly higher when the maternal PBMCs were stimulated with PBMCs of their own fetus. This phenomenon could not be observed after stimulation with PBMCs from unrelated volunteers. In addition, an increased humoral immune response was assessed for women with PPROM in comparison with women with uncontrollable preterm labor. Our results revealed a strongly reduced allogeneic T cell response of PBMCs from pregnant women that was further down-regulated when PBMCs from their own fetus were used as stimulators. By contrast, data from women with PPROM suggest an increased maternal T cell response specifically toward the fetal HLA antigens.