Antigenic heterogeneity of the hepatitis C virus NS4 protein as modeled with synthetic peptides

The effect of sequence heterogeneity on the immunologic properties of two strong antigenic regions of the hepatitis C virus (HCV) NS4 protein was studied by using a set of 443 overlapping 20-mer synthetic peptides. One antigenic region comprising the cleavage site between NS4a and NS4b (region 5-1-1) was modeled with peptides derived from 73 different known sequences, representing HCV genotypes 1-6. The other antigenic region, designated region 59 and located at the C-terminus of the NS4b protein, was modeled with peptides from 7 known sequences representing genotypes 1-3. All peptides were tested for antigenic reactivity by enzyme immunoassay with a panel of anti-HCV-positive serum specimens representing genotypes 1-5. The data demonstrated that immunoreactive peptides fell into two groups. One group, represented by N-terminal peptides, demonstrated genotype-independent immunoreactivity; the other group, from the central part of region 5-1-1, showed strict genotype specificity. Nineteen peptides from the genotype-independent group strongly immunoreacted with a wide range of serum samples containing antibodies to all 5 HCV genotypes. Twenty-five peptides from the genotype-specific group were found to strongly react with serum containing antibodies only to the genotype from which the peptides were derived. Similar to the N-terminal part of region 5-1-1, peptides derived from region 59 did not show genotype-specific immunoreactivity. Some peptides derived from the central part of region 59 showed very strong and broad antigenic reactivity. Thus, after examining two antigenic regions of the NS4 protein, we identified short sequences that can be used for the efficient detection of either genotype-independent or genotype-specific HCV antibodies.     

Estimating and comparing univariate associations with application to the prediction of adult obesity

Studies examining the association between an outcome variable and multiple predictors are common in medical research. Examples include epidemiologic studies of risk factors for disease and clinical studies of prognostic indicators for diseased subjects. This paper is concerned with the assessment of the associations between the outcome and each predictor separately, the so-called univariate associations. Comparisons between predictors in regards to the strengths of their association with the outcome are considered. We show that though such comparisons cannot be made with standard techniques, they can be made using an algorithm which performs all of the univariate analyses simultaneously. This is accomplished with a non-standard application of generalized estimating equation methods. Comparisons of univariate associations are shown to be the key analyses of interest in a retrospective longitudinal study of childhood predictors of adult obesity. We illustrate the methodology on data from this study.     

Proceedings of the Symposium ‘Angiotensin AT1 Receptors: From Molecular Physiology to Therapeutics’: PHYSIOLOGICAL ACTIONS OF ANGIOTENSIN II MEDIATED BY AT1 AND AT2 RECEPTORS IN THE BRAIN

• 1 Autoradiographic binding studies have shown that the AT₁ receptor is the predominant angiotensin II (AngII) receptor subtype in the central nervous system (CNS). Major sites of AT₁ receptors are the lamina terminalis, hypothalamic paraventricular nucleus, the lateral parabrachial nucleus, rostral and caudal ventrolateral medulla, nucleus of the solitary tract and the intermediolateral cell column of the thoraco-lumbar spinal cord.
• 2 While there are differences between species, AT₂ receptors are found mainly in the cerebellum, inferior olive and locus coeruleus of the rat.
• 3 Circulating AngII acts on AT₁ receptors in the subfornical organ and organum vasculosum of the lamina terminalis (OVLT) to stimulate neurons that may have a role in initiating water drinking.
• 4 Centrally administered AngII may act on AT₁ receptors in the median preoptic nucleus and elsewhere to induce drinking, sodium appetite, a sympathetic vasoconstrictor response and vasopressin secretion.
• 5 Recent evidence shows that centrally administered AT₁ antagonists inhibit dipsogenic, natriuretic, pressor and vasopressin secretory responses to intracerebroventricular infusion of hypertonic saline. This suggests that an angiotensinergic neural pathway has a role in osmoregulatory responses.
• 6 Central angiotensinergic pathways which include neural inputs to the rostral ventrolateral medulla may use AT₁ receptors and play a role in the function of sympathetic pathways maintaining arterial pressure.

     

Studies of the binding of diolepoxide metabolites of polycyclic aromatic hydrocarbons to DNA using electrofluorescence polarization spectroscopy

In the electrofluorescence method, a solution of DNA with covalentlybound polycyclic hydrocarbons is placed in an electric field,and changes in the intensity of polarized fluorescence are observed.Under the correct conditions, these changes can be used to determinea value for the angle between the long axis of the hydrocarbonmolecule and the axis of the DNA helix. For DNA or poly(dA-dT)treated with each stereoisomer of anti-benzo[c]phenanthrenediolepoxide, ranged from 55° to 61°, consistent witha mixture of quasi-intercalated adenine adducts and externallybound guanine adducts. Similar results were obtained with anotherset of ‘fjord-region’ diolepoxides, derived frombenzo[c]chrysene. Adducts in DNA treated with diolepoxides derivedfrom chrysene, 5-methylchrysene or 6-methylchrysene gave of53°, so the predominant adducts are externally bound, probablyin the minor groove of DNA.     

Structure-function relationship of new anthralin derivatives assayed for growth inhibition and cytotoxicity in human keratinocyte cultures.

HaCaT keratinocyte cultures were exposed to twelve hydrophilic anthralin derivatives 1 to 12 with substituents at C-1 and C-8 of the anthrone skeleton, of one H at C-10 and of both H's at C-10 by lacton rings. After 3 microM treatment growth was determined by cellular protein content, 3H-thymidine- and 14C-amino-acid-uptake and cytotoxicity by the release of cytoplasmic LDH into the culture medium. In comparison to acetone control (100%) anthralin suppressed mean protein content, as well as DNA- and protein-synthesis to 33, 28, and 21%, respectively, and the drug revealed an enzyme release of 660%. In relation to the parent drug we found similar cell growth inhibitory effects of compounds 4, 6, 8, 9, 10, and 12. Deriv. 4, 8, and 10 were, however, to some extent less cytotoxic than anthralin, whereas deriv. 6, 9, and 12 were in the same range. An extreme suppression of growth parameters which differed from the anthralin effect by a factor 0.5-0.8 was caused by deriv. 11, showing the same cytotoxicity. Deriv. 1, 2, 3, 5, and 7 did not demonstrate any cytotoxicity. Concerning growth parameters, deriv. 2 induced a slight stimulation, deriv. 3 and 7 were completely ineffective, deriv. 1 and 5 induced slightly to moderately inhibited proliferation but both being much less effective than anthralin. These data indicate that the "minimum structure" concept by Krebs and Schaltegger--claiming 1-hydroxy-9-anthrone as a precondition for clinical antipsoriatic potency--is not valid at least in cell-biological tests and point toward possible usefulness of some experimental model compounds as alternative antipsoriatics.     

Anthralin derivatives--inhibition of 5-lipoxygenase--antipsoriatic efficacy.

Inhibition of 5-lipoxygenase by anthralin (1) and 41 derivatives is determined: the acids 38 and 39, the lactones 40-42 and 9-anthrone (8) are the most potent inhibitors, the lactone 41 reaching the efficacy of nordihydroguaiaretic acid (NDGA). The results were correlated with the hydrophilic/lipophilic balance of the test compounds and their clinical efficacy as far as known. There is no correlation between the "minimum structure" of Krebs and Schaltegger concerning antipsoriatic activity and the inhibitory effects against 5-lipoxygenase.     

Beitrag zur Frage periartikulärer Verkalkungen nach totalendoprothetischem Hüftgelenksersatz

Zusammenfassung Aufgrund von gaschromatografischen Methylmethacrylatbestimmungen im Gelenkpunktat (N=31) nach totalendoprothetischem Hüftgelenksersatz unter Anwendung von Acrylzement wird gezeigt, daß Restmonomer aus dem Knochenzement nicht die Ursache periartikulärer Verkalkungen ist. Nur in den ersten Tagen nach der TEP-Operation ließen sich bis zu 200 g/ml MMA-Monomer nachweisen. Dabei handelt es sich um MMA-Monomer, das nach beendeter Polymerisation mit einem Gehalt von 1% bis 4% im Knochenzement vorliegt und in die Umgebung diffundiert. Sämtliche gefundenen Monomerkonzentrationen im Gelenkpunktat liegen unter den in der Literatur angegebenen gewebstoxischen Konzentrationen.

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Additional information regarding periarticular ossifications after total hip replacement

Summary Residual monomer originating from acrylic bone cement is not the origin of periarticular calcifications after hip joint replacement. This has been demonstrated by gaschromatografic detection of monomeric methylmethacrylate in the liquid of the joint space. Up to 200 g/ml monomeric MMA could be demonstrated in the first days after the operation only. The concentration of residual monomeric MMA in the bone cement is 1% to 4%. It is deminished time dependently by diffusion of the molecule in the surrounding tissue. All determined concentrations of monomeric MMA in the joint liquid are below the toxic range for tissue demage.

     

Pharmacokinetics of ascorbic acid in man

Summary The pharmacokinetic characteristics of ascorbic acid have been investigated in normal adult volunteers, using a two-compartment open model. After oral administration in a normal gelatine capsule the bioavailability of ascorbic acid was 69%. It was 98% when a sustained-release preparation was given in an identical capsule. During daily oral intake of ascorbic acid 1 g in the sustained-release form blood levels reached the equilibrium state within 3 days. Daily doses of ascorbic acid 1 g resulted in tissue saturation in 7 days, with a profound change in the pharmacokinetics of the vitamin. The binding of ascorbic acid to plasma proteins was low (24%). Its significance for the pharmacokinetic behaviour of the drug is discussed.