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Citations to this article

Oligonucleotide linked to human gammaglobulin specifically diminishes anti-DNA antibody formation in cultured lymphoid cells from patients with systemic lupus erythematosus.
Y Borel, H Borel
Y Borel, H Borel
Published December 1, 1988
Citation Information: J Clin Invest. 1988;82(6):1901-1907. https://doi.org/10.1172/JCI113808.
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Research Article Article has an altmetric score of 6

Oligonucleotide linked to human gammaglobulin specifically diminishes anti-DNA antibody formation in cultured lymphoid cells from patients with systemic lupus erythematosus.

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Abstract

In vitro studies were undertaken to determine whether the level of anti-DNA antibody can be modulated in humans with systemic lupus erythematosus (SLE). DNA fragments of different sizes, i.e., oligonucleotide (N20-30) or oligonucleotide (N10-100), were covalently linked either to human gammaglobulin (HGG) and used as tolerogens or to keyhole limpet hemocyanin and used as immunogens. Experiments were done to determine whether such tolerogens specifically diminish antibodies to denatured DNA, native DNA, or both. PBL were obtained from 87 patients with SLE, 55 of whom spontaneously produced anti-DNA antibodies in vitro. Furthermore, of these 55 test subjects 23 made anti-DNA antibodies in response to antigen challenge in vitro. Exposure of PBL to tolerogenic oligonucleotide-HGG reduced spontaneous antibody formation in 34 of the 55 patients' PBL and abrogated the in vitro-induced response in all instances. The suppression was tolerogen specific. In some SLE patients lymphoid cells were suppressed by both (N10-100)-HGG and (N20-30)-HGG, while in others lymphoid cells were suppressed by only one. Longitudinal studies of spontaneous antibody production showed that the same tolerogens consistently reduced anti-DNA antibody formation in lymphoid cells of 12 patients on several occasions over a 2-yr interval, but in 8 others the results were either variable or inconsistent. In contrast, tolerogens consistently abrogated the antigen-induced response in all 23 patients' PBL. These results obtained in humans in vitro suggest that the principle of carrier-determined tolerance could be applied as a specific therapy for SLE in vivo.

Authors

Y Borel, H Borel

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Total citations by year

Year: 2013 2005 1995 1994 1991 1990 1989 Total
Citations: 2 1 1 1 1 3 1 10
Citation information
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Citations to this article (10)

Title and authors Publication Year
Dubois' Lupus Erythematosus and Related Syndromes
JC Crispín, GC Tsokos
Dubois' Lupus Erythematosus and Related Syndromes 2013
Fusion Protein Technologies for Biopharmaceuticals: Applications and Challenges
B Mei, SC Low, S Krassova, RT Peters, GF Pierce, JA Dumont
Fusion Protein Technologies for Biopharmaceuticals: Applications and Challenges 2013
SLE: translating lessons from model systems to human disease
RR Singh
Trends in Immunology 2005
Induction of tolerance by administration of hapten-immunoglobulin conjugates is associated with decreased IL-2 and IL-4 production
V Dumas, W Ptak, M Demarchez, , Y Borel, C Hauser
Archives of Dermatological Research 1995
Conjugates or dsDNA Linked to Human Gammaglobulin Inhibit Anti-dsDNA Antibodies In Vitro
N Mikael, M Boguniewicz, Y Manakata, T Sasaki, H Borel, Y Borel
Lupus 1994
Chemisch modifizierte Oligonucleotide als Sonden und Agentien
U Englisch, DH Gauss
Angewandte Chemie 1991
DNA antibody idiotypes an analysis of their role in health and disease
DA Isenberg, NA Staines
Journal of Autoimmunity 1990
A novel technique to link either proteins or peptides to gammaglobulin to construct tolerogens
H Borel, Y Borel
Journal of Immunological Methods 1990
DNA-binding antibodies and parasitic diseases
AO Wozencraft, NA Staines
Parasitology Today 1990
Immunologic tolerance to DNA in B cell lines from both normal and autoimmune mice
M Aldo-Benson, H Borel, L Scheiderer-Pratt, Y Borel
Immunologic Research 1989

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