Your search keyword '"Broliden, P.-A."' showing total 4 results

1. Fine specificity of IgG subclass response to group antigens in HIV-1-infected patients.

Author

Broliden, P. A., Morfeldt-Månsson, L., Rosen, J., Jondal, M., and Wahren, B.

Subjects

*HIV infections, *LENTIVIRUS diseases, *IMMUNOGLOBULINS, *AIDS, *ENZYME-linked immunosorbent assay, *PEPTIDES

Abstract

There is an association between the clinical stage of HIV-1 infection and the presence of antibodies against viral gag proteins (p17 and p24). The IgG subclass (G1 and G3) pattern against these antigens was analysed in stable patients and HIV patients progressing to AIDS. Antibodies were analysed with whole viral or peptide ELISA (using sequentially overlapping peptides) and Western Blots. IgG1 was found to be the dominant anti-HIV-1 IgG subclass and IgG1 antibodies declined in progressing patients against all HIV antigens evaluated in Western blot, including p17, p24, p31, gp41, p64, gp120 and gp160. In contrast IgG antibodies, which were found to be predominantly directed against gag proteins, and which could be detected in almost all patients, remained in the circulation during disease progression. By peptide assays distinct immunogenic regions were found in p17 in contrast to more events distributed epitopes in p24. A decreased divergence of antibody reactivity to both p17 and p24 peptides in the group of patients who developed AIDS was seen. No reaction to any single gag epitope related to disease progression. The difference between IgG1 and IgG3 anti-gag antibodies in relation lo clearance during disease progression may depend on different properties of immune complexes formed by these two IgG subclasses. [ABSTRACT FROM AUTHOR]

Published

1989

2. IgG subclass response to HIV in relation to antibody-dependent cellular cytotoxicity at different clinical stages.

Author

Ljunggren, Kristina, Broliden, P. A., Morfeldt-Manson, L., Jondal, M., and Wahren, B.

Subjects

*HIV, *ANTIBODY-dependent cell cytotoxicity, *IMMUNOGLOBULIN G, *SERUM, *ANTIGENS, *AIDS patients

Abstract

The anti-HIV IgG subclass response was analysed in sera from different clinical stages and related to virus specific antibody-dependent cellular cytotoxicity (ADCC). IgG1 was found to be the dominant subclass, present in all sera and with similar mean titres at different stages. The number of anti-HIV IgG3 positive sera, measured on whole viral lysate antigen plates, decreased during disease progression from 38% in symptom-free to 7% in AIDS patients. IgG2 and IgG4 subclasses were less prevalent although a slight increase of IgG4 frequency was found in AIDS patients. High IgGl titres correlated with a positive ADCC reaction but there was no correlation between anti-HIV IgG1 and ADCC titres. Some sera which contained HIV IgG1 as the only subclass were able to mediate an ADCC reaction. In addition, when anti-HIV IgG3 was isolated, by protein A chromatography, no ADCC killing was induced by these antibodies. It is concluded that IgG1 is the major ADCC-active IgG subclass in HIV infected individuals. The lack of correlation between IgG1 and ADCC titres may be explained by a relatively small fraction of IgG1 antibodies mediating ADCC. [ABSTRACT FROM AUTHOR]

Published

1988

3. Antibody--dependent cellular cytotoxicity and neutralizing activity in sera of HIV--1-infected mothers and their children.

Author

Broliden, K., Sievers, E., Tovo, P. A., Moschese, V., Scarlatti, G., Broliden, P. A., Fundaro, C., and Rossi, P.

Subjects

ANTIBODY-dependent cell cytotoxicity, IMMUNOGLOBULINS, HIV infections, AIDS patients, AUTOIMMUNITY -- Molecular aspects, IMMUNOREGULATION

Abstract

The prognostic and protective role of antibodies mediating cellular cytotoxicity (ADCC) and neutralization was evaluated in sera of HIV-1-infected mothers and their consecutively followed children. The presence and titres of ADCC mediating and/or neutralizing antibodies in maternal sera did not predict HIV-1 infection in their respective children. No significant difference in the sera from the children was seen when comparing the presence of neutralizing antibodies between the uninfected and infected children. Stratification of the infected group according to clinical status revealed differences. Only one of 24 AIDS patients had a high neutralizing titre against IIIB. Four patients had a very low titre and the remaining had no detectable neutralizing antibodies at all. In contrast, 10/17 infected non-AIDS children had neutralizing antibodies. Similarly, no significant difference was seen when comparing the presence of ADCC-mediating antibodies between the uninfected and the infected group of children. However, a significantly higher frequency of ADCC was seen in the seropositive non-AIDS children compared with the AIDS children, This study clearly shows that the presence of antibodies mediating ADCC and neutralization in infected children, 0-2 years old, is associated with a better clinical status and delayed disease progression. [ABSTRACT FROM AUTHOR]

Published

1993

4. Human MoAbs produced from normal, HIV-1-negative donors and specific for glycoprotein gp120 of the HIV-1 envelope.

Author

Ohlin, M., Hinkula, J., Broliden, P.-A., Grunow, R., Borrebaeck, C. A. K., and Wahren, B.

Subjects

IMMUNOGLOBULIN M, HIV, LYMPHOCYTES, RECOMBINANT proteins, IMMUNOGLOBULINS, AMINO acids, CD4 antigen, GLYCOPROTEINS

Abstract

Human MoAbs of IgM class were developed against three regions of the HIV-1 envelope. Uninfected donor lymphocytes were immunized in vitro with recombinant protein pB1. Four out of five antibodies were directed to different parts of the V3 region, which contains a major neutralizing site. Two out of these antibodies were directed to more than one amino acid sequence, indicating reactivity to discontinuous sites. Two of the human MoAbs inhibited viral spread between cells in tissue culture, interpreted as reactivities to conserved amino acid sequences exposed during viral maturation. No MoAb neutralized virus, which may be explained by the relatively low avidity of the antibodies. One MoAb was directed to a region containing amino acids participating in CD4 binding. This technique appears to allow formation of antibodies with fine specificities other than those obtained in infected hosts. [ABSTRACT FROM AUTHOR]

Published

1992