The double minimum E(3)1Σu+ state in Cs2.

The double minimum E1Σu+ state in caesium dimer was investigated by analysing spectra of the E1Σu+← X1Σg+ band system, simplified by polarisation labelling. A total of 6727 rotationally resolved transitions to levels situated in the inner well and above the internal barrier were identified and a potential energy curve allowing to reproduce their energies was constructed using the Fourier grid Hamiltonian and inverted perturbation approach methods. The unambiguity of the potential curve in view of lack of data related to levels located in the outer well is discussed.

Observation and modeling of bound-free transitions to the X1Σ+ and a3Σ+ states of KCs.

The oscillation continuum in laser-induced fluorescence spectra of bound-free c3Σ+ → a3Σ+ and (4)1Σ+ → X1Σ+ transitions of the KCs molecule was recorded by a Fourier-transform spectrometer and modeled under the adiabatic approximation. The required interatomic potentials for ground a3Σ+ and X1Σ+ states were reconstructed in an analytical Chebyshev-polynomial-expansion form in the framework of the regularization direct-potential-fit procedure based on the simultaneous consideration of experimental line positions from Ferber et al. [Phys. Rev. A 80, 062501 (2009)] and the present ab initio calculation of short-range repulsive potential data. It was proved that the repulsive part over the dissociation limit of the derived a3Σ+ potential reproduces the experiment better than the potentials reported in the literature. It is also shown that all empirical and semi-empirical potentials available for the X1Σ+ state reproduce the bound-free (4)1Σ+ → X1Σ+ spectrum with equal quality in the range of observations.

In silico calculated affinity of FVIII-derived peptides for HLA class II alleles predicts inhibitor development in haemophilia A patients with missense mutations in the F8 gene.

Forty per cent of haemophilia A (HA) patients have missense mutations in the F8 gene. Yet, all patients with identical mutations are not at the same risk of developing factor VIII (FVIII) inhibitors. In severe HA patients, human leucocyte antigen (HLA) haplotype was identified as a risk factor for onset of FVIII inhibitors. We hypothesized that missense mutations in endogenous FVIII alter the affinity of the mutated peptides for HLA class II, thus skewing FVIII-specific T-cell tolerance and increasing the risk that the corresponding wild-type FVIII-derived peptides induce an anti-FVIII immune response during replacement therapy. Here, we investigated whether affinity for HLA class II of wild-type FVIII-derived peptides that correspond to missense mutations described in the Haemophilia A Mutation, Structure, Test and Resource database is associated with inhibitor development. We predicted the mean affinity for 10 major HLA class II alleles of wild-type FVIII-derived peptides that corresponded to 1456 reported cases of missense mutations. Linear regression analysis confirmed a significant association between the predicted mean peptide affinity and the mutation inhibitory status (P = 0.006). Significance was lost after adjustment on mutation position on FVIII domains. Although analysis of the A1-A2-A3-C1 domains yielded a positive correlation between predicted HLA-binding affinity and inhibitory status (OR = 0.29 [95% CI: 0.14-0.60] for the high affinity tertile, P = 0.002), the C2 domain-restricted analysis indicated an inverse correlation (OR = 3.56 [1.10-11.52], P = 0.03). Our data validate the importance of the affinity of FVIII peptides for HLA alleles to the immunogenicity of therapeutic FVIII in patients with missense mutations.

Discharge tube with coaxial geometry for efficient production of metal hydrides.

The production of metal hydrides in vapour phase is one of the problems which makes their spectroscopic investigation at high resolution difficult. The molecular densities are usually low and the absorption is often increased by the use of multipass cells or intracavity setups. In this contribution a discharge tube with coaxial geometry is investigated, which is able to produce relatively high densities of NiH (≈10(12) cm(-3)). Additional advantage of the present geometry is that the densities are very homogeneous along the discharge length, 250 mm in our case, which can be made in principle arbitrary long. As a result, reliable absorption was detected even in a single pass experiment. We also present the results of a numerical model which explains the general properties of the plasma in the tube. Based on this understanding, we discuss possible improvements and other applications of this discharge geometry.

Lipid peroxidation in erythrocyte membranes of women with benign and malignant neoplasms of the endometrium.

The content of primary and secondary products of membrane peroxidation, total cholesterol concentration, and relative microviscosity of erythrocyte membranes were measured in women with endometrial cancer and uterine leiomyoma. The content of conjugated dienes in erythrocytes was highest in female patients with malignant tumors of the endometrium. The relative microviscosity of erythrocyte membranes in patients with uterine leiomyoma and endometrial cancer was elevated in the zone of lipid--lipid and protein--lipid contacts.

Photoassociation spectroscopy of the B 1Pi state of LiCs.

We present an accurate potential energy curve of the B (1)Pi state in the LiCs molecule for which vibrational levels between v(') = 0 and v(') = 35 (bound by 11.4 GHz) were measured by photoassociation spectroscopy in an ultracold ensemble of (7)Li and (133)Cs atoms. By the combination of conventional spectroscopic data of the B-X system and the new photoassociation measurements a very precise value of the dissociation energy of the ground state X (1)Sigma(+) of LiCs was determined to be D(0) = 5783.495(5) cm(-1).

The potential energy barrier of the 2(1)Pi state in KLi.

The polarisation labelling spectroscopy technique has provided detailed information about the shape of the potential barrier to dissociation of the 2(1)Pi state in KLi. The potential curve of the 2(1)Pi state is constructed using the Inverted Perturbation Approach method. Our analysis shows that the barrier height is DeltaE=20.8+/-1.0 cm(-1) relative to the dissociation limit and the barrier maximum is located at Rbar=8.2+/-0.1 A.

The ground electronic state of KCs studied by Fourier transform spectroscopy.

We present here the first analysis of laser induced fluorescence (LIF) of the KCs molecule obtaining highly accurate data and perform a direct potential construction for the X (1)Sigma(+) ground state in a wide range of internuclear distances. KCs molecules were produced by heating a mixture of K and Cs metals in a heat pipe at a temperature of about 270 degrees C. KCs fluorescence was induced by different laser sources: the 454.5, 457.9, 465.8, and 472.7 nm lines of an Ar(+) laser, a dye laser with Rhodamine 6G dye (excitation at around 16 870 cm(-1)), and 850 and 980 nm diode lasers (11 500-11 900 and 10 200-10 450 cm(-1) tuning ranges, respectively). The LIF to the ground state was recorded by a Bruker IFS-125HR Fourier transform spectrometer with a spectral resolution of 0.03 cm(-1). Particularly, by applying the 850 nm laser diode we were able to observe LIF progressions to very high vibrational levels of the ground state close to the dissociation limit. The present data field contains 7226 term values for the ground state X (1)Sigma(+) and covers a range from v(")=0 to 97 with J(") varying from 12 to 209. More than 10 000 fluorescence lines were used to fit the ground state potential energy curve via the inverted perturbation approach procedure. The present empirical potential extends up to approximately 12.6 A and covers more than 99% of the potential well depth, it describes most of the spectral lines with an accuracy of about 0.003 cm(-1) and yields a dissociation energy of 4069.3+/-1.5 cm(-1) for the ground state X (1)Sigma(+). First observations of the triplet ground state a (3)Sigma(+) of KCs are presented, and preliminary values of few main molecular constants could be derived.

The B 1Pi state of NaCs: high resolution laser induced fluorescence spectroscopy and potential construction.

The lowest (1)Pi state of the NaCs molecule, the B(1)(1)Pi state, was studied using a dye laser for inducing fluorescence that was resolved by a high resolution Fourier-transform spectrometer. The presence of argon buffer gas yielded rich rotational relaxation spectra allowing to enlarge the data set for the B(1)(1)Pi state, to obtain Lambda-splittings and to reveal numerous local perturbations. 543 weakly perturbed energy levels for rotational quantum numbers from J(')=5 to 168 and vibrational quantum numbers from v(')=0 to 25, which cover about 87% of the potential well depth, were used for a direct pointwise fit of the potential energy curve applying the inverted perturbation approach method. The resulting potential reproduces the term values for v(')=0-7 with an experimental accuracy of about 0.01-0.02 cm(-1), whereas for v(')=8-25 the deviations increase due to the perturbations, going to the order of 1 cm(-1); an extrapolation is made to the dissociation asymptote.

Experimental long range potential of the B 1Pi state in NaRb.

The long range potential of the B 1Pi state in NaRb has been investigated by observation of rovibrational levels that it supports, including the high lying ones, with the technique of polarization labeling spectroscopy. This has allowed us to characterize the potential energy curve up to 1.9 cm(-1) from the dissociation limit. The highest observed rovibrational level v=49, J=10 has the outer turning point at R=16.48 A.

High resolution spectroscopy and potential determination of the (3)1Pi state of NaCs.

The (3)(1)Pi state of the NaCs molecule was studied by high resolution Fourier-transform spectroscopy. The (3)(1)Pi-->X (1)Sigma(+) laser induced fluorescence was excited by an Ar(+) ion laser or by a single-mode frequency-doubled cw Nd:YAG laser. The presence of argon buffer gas yielded rich rotational relaxation spectra allowing to enlarge the data set for the (3)(1)Pi state term values, as well as to observe Lambda splittings in a wide range of vibrational (v(')) and rotational (J(')) quantum numbers. The data field includes about 820 energy levels of (3)(1)Pi NaCs in the range from v(')=0 to 37 and from J(')=3 to 190, which corresponds to ca. 95% of the potential well depth. Direct fit of the potential energy curve to the level energies is realized using the inverted perturbation approach method; a set of Dunham coefficients is also presented.

The autoreactivity of therapeutic intravenous immunoglobulin (IVIG) preparations depends on the fractionation methods used.

Natural immunoglobulin G (IgG) autoantibodies are present in the plasma of healthy individuals and, as a result, in pooled therapeutic intravenous immunoglobulin (IVIg) preparations. The production processes of commercial IVIg preparations involve different fractionation and virus-inactivation steps that include in some cases treatments at extreme conditions. Different physical and chemical treatments are known to augment greatly the reactivity of natural autoantibodies to self-antigens. It is not clear to what extent the self-reactivity of IVIg preparations is due to the presence of natural IgG antibodies in the plasma pools used for fractionation, and to what extent it is due to the treatments that the IgG molecules have been subjected to during the fractionation process. We compared the binding of seven different commercial IVIg preparations to human liver antigens. All studied IVIg's could be clearly separated into two distinct groups: those that possess significant self-reactivity and those with low binding to self-antigens. Increased self-binding was seen in the preparations produced using a fractionation step at low pH. The treatment of IVIg at low pH resulted in increasing the inhibitory effect of the pooled IgG on PHA-induced proliferation of human peripheral blood mononuclear cells. IVIg's with high and low self-binding may have different immunomodulating activities when infused to autoimmune patients.

A regularized inverted perturbation approach method: potential energy curve of the 4 (1)Sigma(u) (+) state in Na(2).

We describe a modification of the inverted perturbation approach method allowing to construct physically sensible potential energy curves for electronic states of diatomic molecules even when some parts of the potential are not adequately characterized by the experimental data. The method is based on a simple regularization procedure, imposing an additional constraint on the constructed potential curve. In the present work it is applied to the double minimum 4 (1)Sigma(u) (+) state of Na(2), observed experimentally by polarization labeling spectroscopy technique.

Fucosylated lactosamines participate in adhesion of HIV-1 envelope glycoprotein to dendritic cells.

Carbohydrates expressed on HIV-1 gp160 are purported to bind to several receptor types that affect virus pathophysiology. Here, we define a potential role for fucosylated glycans involved in the adhesion of cells expressing anchored HIV-1 glycoprotein or HIV virions to human dendritic cells (DCs). We observe that a monoclonal antibody (FH6), with reactivity toward an extended dimeric form of a fucosyl lactosamine, binds to gp120 transfectants, blocking adhesion of these cells and virus particles to human DCs. We observe that serum antibodies induced by peptide mimetic of fucosylated carbohydrate core structures emulate the monoclonal antibody reactivity pattern, showing enhanced reactivity to HIV-1 envelope-expressing cell line and blocking the adhesion of these cells to human DCs. These results suggest a potential role for initial adherence of virally infected cells or virions mediated by fucosylated lactosamines expressed on the envelope protein. As these carbohydrates function as adhesion molecules associated with homing and dissemination processes, such interactions may contribute to the HIV infection process.

Spectroscopic study of the E(4)1sigma+ state in NaLi.

Polarization labelling spectroscopy is applied to study the excited E1sigma+ state of NaLi in the energy range 26,500-28,000 cm(-1) above the bottom of the ground state. The potential curve of the E state is constructed using the Inverted Perturbation Approach method. The values of Te, omega(e) and Re are found to be 26,474.82(4), 180.3(2) cm(-1) and 3.343(1) A, respectively.

Lupus-specific kidney deposits of HSP90 are associated with altered IgG idiotypic interactions of anti-HSP90 autoantibodies.

Previous studies have shown that autoantibodies to heat shock protein 90 (HSP90) are elevated in a significant proportion of patients with systemic lupus erythematosus (SLE) who are more likely to have renal disease and a low C3 level. Using samples from 24 patients, we searched for glomerular deposits of HSP90 in renal biopsy specimens from seven patients with lupus nephritis and 17 cases of glomerulonephritis from patients without SLE. Positive glomerular immunofluorescent staining for HSP90 was observed in six of seven cases of SLE and positive tubular staining in two of seven SLE patients. The staining for HSP90 was granular in nature and was located in subepithelial, subendothelial and mesangial areas. None of the non-SLE renal biopsies revealed positive staining for HSP90 deposition. Further we showed the presence of anti-HSP90 IgG autoantibodies in IgG from sera of patients with SLE as well as in normal human IgG (IVIg). In normal IgG this autoreactivity could be adsorbed almost completely on F(ab')2 fragments from the same IgG preparation, coupled to Sepharose and could be inhibited by the effluent obtained after subjecting normal IgG to HSP90 affinity column. These findings indicate that anti-HSP90 natural autoantibodies are blocked by idiotypic interactions within the IgG repertoire. Unlike natural autoantibodies, anti-HSP90 IgG from SLE patients' sera were only moderately adsorbed on F(ab')2 fragments of normal IgG. These results demonstrate that immunopathogenesis of lupus nephritis is associated with HSP90 (as an autoantigen) and that the pathology is associated with altered idiotypic regulation of the anti-HSP90 IgG autoantibodies.

Accurate Potential Curve for the Double Minimum 2(1)Sigma(+)(u) State of Na(2).

The double minimum 2(1)Sigma(+)(u) state of Na(2) was investigated by polarization labeling spectroscopy technique. A total of 1156 transitions to rovibrational levels of the inner well and above the barrier were identified. Using the IPA method, an accurate potential curve of the state was constructed based on a weighted fit of our experimental results and spectroscopic data available in the literature [D. L. Cooper, R. F. Barrow, J. Vergés, C. Effantin, and J. d'Incan, Can. J. Phys. 62, 1543-1558 (1984)]. Copyright 2000 Academic Press.

Natural antibodies to factor VIII.

Anti-factor VIII antibodies represent a unique model to study the relationship between natural autoreactivity (natural antibodies to factor VIII of healthy individuals), disease-associated autoimmunity ("spontaneous" factor VIII inhibitors of patients with anti-factor VIII autoimmune disease) and antigen-driven immune responses (immune inhibitors in multitransfused patients with hemophilia A) to a single human protein antigen. Although natural and disease-associated anti-factor VIII antibodies are not readily distinguished based on the comparison of their isotypic distribution and epitope mapping, available studies of cross-reacting idiotypes suggest that factor VIII inhibitors in patient's plasma encompass two populations of anti-factor VIII antibodies. Some antibodies result from the clonal expansion of B lymphocytes that exist before treatment with factor VIII and secrete anti-factor VIII antibodies with properties similar to those of natural anti-factor VIII antibodies present in healthy individuals; other inhibitors are produced by B cell clones that have undergone affinity maturation and hypermutation of the V regions of the antibodies they produce. The implications for the treatment of patients with anti-factor VIII inhibitors are discussed.

Phosphorylation of Bcl-2 and mitochondrial changes are associated with apoptosis of lymphoblastoid cells induced by normal immunoglobulin G.

Normal human immunoglobulin G induces apoptosis in human lymphoblastoid cells which involves antibody-mediated Fas ligation and the activation of caspases. Here, we show that Bcl-2 is phosphorylated on serine upon treatment of CEM T cells with normal IgG and that the overexpression of Bcl-2 in stable transfectants of CEM T cells prevents IgG-induced cell death. Treatment of CEM cells with normal IgG also results in a reduction in mitochondrial transmembrane potential and in the release of cytochrome c (Cyt c) into cytosol. The findings are concordant with earlier observations that apoptosis induced by IgG is associated with the activation of caspases. Our results demonstrate that Bcl-2 controls apoptosis induced by normal IgG and support a central role for Bcl-2 and mitochondria in antibody-mediated selection of lymphocyte repertoires.

[Immunomodulatory effects of intravenous immunoglobulins in autoimmune diseases]. / Effets immunomodulateurs des immunoglobulines intraveineuses au cours des maladies auto-immunes.

PURPOSE: Intravenous immunoglobulins (IVIg) therapy has been reported to be beneficial in a large number of autoantibody-mediated or self-reactive T cells-associated autoimmune diseases. Thus, the beneficial effect of IVIg is probably due to multiple distinct mechanisms. MAIN POINTS: The immunoregulatory effect of IVIg in autoimmune diseases is dependent on: interaction of the Fc portion of IVIg with Fc receptors on leucocyte surfaces; interaction of infused IgG with complement components; modulation of synthesis and release of cytokines produced by lymphocytes and monocytes: V region-dependent neutralization of circulating autoantibodies by infused IgG; selection of immune repertoires; modulation of cell proliferation, particularly through modulation of Fas-induced apoptosis; interaction of IVIg with numerous other molecules onto the surface of T and B cells. PERSPECTIVES: Better understanding of these mechanisms should allow a better definition of the spectrum of diseases likely to benefit from IVIg treatment.