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(Journal of Leukocyte Biology. 2001;69:81-88.)
© 2001 by Society for Leukocyte Biology

CpG DNA increases primary malignant B cell expression of costimulatory molecules and target antigens

Bernd Jahrsdörfer*, Gunther Hartmann*, Emil Racila{dagger}, Wallen Jackson{ddagger}, Lars Mühlenhoff*, Gerold Meinhardt§, Stefan Endres*, Brian K. Link{dagger},{ddagger},||, Arthur M. Krieg{dagger},{ddagger},|| and George J. Weiner{dagger},{ddagger}

* Division of Clinical Pharmacology
§ Division of Hematology, Department of Internal Medicine, University of Munich, Germany
{ddagger} Department of Internal Medicine
{dagger} the Holden Cancer Center at the University of Iowa, Iowa City, Iowa
|| Coley Pharmaceutical Group Inc., Wellesley, Massachusetts

Correspondence: George J. Weiner, M.D., University of Iowa Cancer Center, 5970Z JPP, University of Iowa, Iowa City, IA 52242. E-mail: george-weiner{at}uiowa.edu

Multiple factors, including expression of costimulatory molecules, antigen-presenting molecules, and target antigens, likely impact the efficacy of antibody therapy and other approaches to the immunotherapy of B cell malignancy. Unmethylated CpG-dinucleotides in select base contexts ("CpG motifs") that resemble sequences found in bacterial DNA are potent immunostimulatory agents capable of inducing a complex immune response, including a strong B cell stimulus. We examined the effect of a potent human CpG oligonucleotide (CpG ODN 2006) on different types of primary human malignant B cells and reactive follicular hyperplasia. CpG oligodeoxynucleotide (CpG ODN), but not control (non-CpG ODN), increased the expression of costimulatory molecules (CD40, CD80, CD86, CD54) on malignant B cells without altering the phenotype of B cells obtained from reactive follicular hyperplasia. CpG ODN also enhanced expression of class I and class II MHC in most samples. CD20 expression was increased in response to CpG ODN, most notably in B-CLL and marginal zone lymphoma. An inverse correlation was found between baseline expression of CD20 and CD40 and their expression after exposure to CpG ODN, thus the most significant increase in expression of these molecules was found in those samples that had the lowest baseline levels. In conclusion, CpG ODN can lead to increasing expression of molecules involved in costimulation, antigen presentation, and as targets for antibody-based therapy and deserve further evaluation as potential immunotherapeutic agents for B cell malignancy.

Key Words: ODN • follicular hyperplasia • B cell activation • non-Hodgkin lymphoma • CLL • monoclonal antibodies




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