Transient down-modulation of CD20 by rituximab in patients with chronic lymphocytic leukemia.

@article{Jilani2003TransientDO,
  title={Transient down-modulation of CD20 by rituximab in patients with chronic lymphocytic leukemia.},
  author={Iman B Jilani and Susan O'brien and Taghi Manshuri and Deborah A. Thomas and Vilmos A. Thomazy and Maha Imam and Sana Naeem and Srdan Verstovsek and Hagop M. Kantarjian and Francis J. Giles and Michael J. Keating and Maher Albitar},
  journal={Blood},
  year={2003},
  volume={102 10},
  pages={
          3514-20
        }
}
Lymphoid cells in most patients with chronic lymphocytic leukemia (CLL), when treated with rituximab, become CD20-. This is thought to be due to masking of CD20 by rituximab. We used specific antimouse immunoglobulin antibodies to detect rituximab on the surface of CLL lymphocytes and we demonstrate that rituximab is rarely detectable after therapy. Only 3 of 65 patients with CLL had rituximab detectable on their lymphocytes after rituximab therapy despite the fact that most had no detectable… 
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Modulation of CD20 antigen expression after rituximab treatment: a retrospective study in patients with chronic lymphocytic leukemia.
Analysis of changes in CD20, CD55, and CD59 expression on established rituximab-resistant B-lymphoma cell lines.
Regulation of CD20 in Rituximab-Resistant Cell Lines and B-cell Non-Hodgkin Lymphoma
TLDR
It is shown that, whereas CD20 expression is important for rituximab activity, additional factors likely contribute to ritUXimab sensitivity in B-cell lymphoma.
Antigenic modulation limits the efficacy of anti-CD20 antibodies: implications for antibody selection.
TLDR
It is demonstrated that type II (tositumomab- like) anti-CD20 mAbs are 5 times more potent than type I (rituximab-like) reagents in depleting human CD20 Tg B cells, despite both operating exclusively via activatory Fcgamma receptor-expressing macrophages.
Down-regulation of CD20 expression in B-cell lymphoma cells after treatment with rituximab-containing combination chemotherapies: its prevalence and clinical significance.
TLDR
Interestingly, when CD20-negative cells were treated with 5-aza-2'-deoxycytidine in vitro, the expression of CD20 mRNA was stimulated within 3 days, resulting in the restoration of both cell surface expression of the CD20 protein and rituximab sensitivity, suggesting that some epigenetic mechanisms may be partly related to the down-regulation ofCD20 expression after ritUXimab treatment.
Immunophenotypic Changes and Clinical Outcome in B-Cell Lymphomas Treated with Rituximab
TLDR
Results show that in many cases of B-NHL persisting after rituximab therapy, CD20 expression decreases or is lost, raising the possibility of deletion or expression modulation of the CD20 gene in neoplastic cells.
HuMab-7D8, a monoclonal antibody directed against the membrane-proximal small loop epitope of CD20 can effectively eliminate CD20low expressing tumor cells that resist rituximab-mediated lysis
TLDR
Cells that are insensitive to in vitro and in vivo killing by rituximab as the result of their low CD20-expression profile may be efficiently killed by an antibody against the membrane-proximal epitope on CD20.
Understanding rituximab function and resistance: implications for tailored therapy.
TLDR
The most significant results showing the role of Rituximab as a signal-inducing antibody and as a chemosensitizing agent through negative regulation of major survival pathways are analyzed and may become useful for novel therapeutic strategies in the treatment of patients resistant to standard therapy.
CD40 stimulation sensitizes CLL cells to rituximab-induced cell death
TLDR
By increasing basal ROS production, CD40 stimulation sensitizes CLL cells to rituximab-mediated death, providing a rationale for combination treatment of CLL with cytotoxic drugs and anti-CD20 monoclonal antibodies.
HDAC inhibitors augment cytotoxic activity of rituximab by upregulating CD20 expression on lymphoma cells
TLDR
It is shown that histone deacetylase (HDAC) inhibitors augment the cytotoxic activity of rituximab by enhancing the surface expression of CD20 antigen on lymphoma cells.
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