Immunomodulatory effects of Toll-like receptor-7 activation on chronic lymphocytic leukemia cells (original) (raw)

• Original Article
• Published: 08 December 2005

Chronic Lymphocytic Leukemia

• Y Shi1,
• D White1,
• J Mena1,
• C Hammond1,4,
• J Tomic1,4,
• L He5,
• M A Tomai6,
• R L Miller6,
• J Booth1 &
• …
• L Radvanyi5 nAff7

Leukemia volume 20, pages 286–295 (2006)Cite this article

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Abstract

Weak immunogenicity of chronic lymphocytic leukemia (CLL) cells may contribute to disease progression and inhibit effective immunotherapy. Accordingly, agents that enhance the immunogenicity of CLL cells may be useful in immunotherapeutic approaches to this disease. Since Toll-like receptors (TLRs) are major regulators of innate immunity and initiation of adaptive immunity, we studied the effects of viral pathogen associated molecular pattern agonists (that are recognized by TLRs) on the costimulatory phenotype and function of CLL cells. CLL cells (especially those with high endogenous expression of CD38) responded to TLR7-activating imidazoquinolines and guanosine analogs by increasing costimulatory molecule expression, producing inflammatory cytokines, and becoming more sensitive to killing by cytotoxic effectors. Additional activation of protein kinase C pathways increased the ability to stimulate T-cell proliferation, blocked phosphorylation of the transcription factor, signal transducer and activator of transcription (STAT)3, and resulted in the acquisition of a dendritic cell surface phenotype by TLR7-activated CLL cells. Normal B cells also responded to TLR7 activation by increasing costimulatory molecule expression and cytokine production. These findings suggest a potential role for TLR7 agonists in CLL immunotherapy.

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References

1. Spaner DE, Hammond C, Mena J, Foden C, Deabreu A . A phase I/II trial of oxidized autologous tumor vaccines during the ‘watch and wait’ phase of chronic lymphocytic leukemia. Cancer Immunol Immunother 2005; 54: 635–646.
   Article Google Scholar
2. Zinkernagel RM . Immunity against solid tumors? Int J Cancer 2001; 93: 1–5.
   Article CAS Google Scholar
3. Spaner D . Amplifying cancer vaccine responses by modifying pathogenic gene programs in tumor cells. J Leukoc Biol 2004; 76: 338–351.
   Article CAS Google Scholar
4. Kawai T, Akira S . Pathogen recognition with Toll-like receptors. Curr Opin Immunol 2005; 17: 338–344.
   Article CAS Google Scholar
5. Decker T, Schneller F, Sparwasser T, Tretter T, Lipford GB, Wagner H et al. Immunostimulatory CpG-oligonucleotides cause proliferation, cytokine production, and an immunogenic phenotype in CLL B cells. Blood 2000; 95: 999–1006.
   CAS PubMed Google Scholar
6. Hemmi H, Kaisho T, Takeuchi O, Sato S, Tomizawa H, Takeda K et al. Small anti-viral compounds activate immune cells via the TLR7-signaling pathway. Nat Immunol 2002; 3: 196–200.
   Article CAS Google Scholar
7. Lee J, Chuang TH, Redecke V, She L, Pitha PM, Carson DA et al. Molecular basis for the immunostimulatory activity of guanine nucleoside analogs: activation of TLR7. Proc Natl Acad Sci USA 2003; 100: 6646–6651.
   Article CAS Google Scholar
8. Shanafelt TD, Geyer SM, Kay NE . Prognosis at diagnosis: integrating molecular biologic insights into clinical practice for CLL patients. Blood 2004; 103: 1202–1210.
   Article CAS Google Scholar
9. Spaner D, Miller R, Mena J, Grossman L, Sorrenti V, Shi Y . Regression of skin deposits in a CLL patient treated with the TLR7/8 agonist, Imiquimod. Leuk Lymphoma 2005; 46: 935–939.
   Article Google Scholar
10. Darlak K, Miller RB, Stack MS, Spatola AF, Gray RD . Thiol-based inhibitors of mammalian collagenase. J Biol Chem 1990; 265: 5199–5205.
    CAS PubMed Google Scholar
11. Bueno C, Rodriguez-Caballero A, Garcia-Montero A, Orfao A . A new method for detecting TNF_α_-secreting cells using direct-immunofluorescence. J Immunol Methods 2002; 264: 77–87.
    Article CAS Google Scholar
12. Hammond C, Shi Y, Mena J, Tomic J, Cervi D, He L et al. Effect of serum and antioxidants on the immunogenicity of PKC-activated CLL cells. J Immunother 2005; 28: 28–39.
    Article CAS Google Scholar
13. Wallgren A, Festin R, Gidlof C, Dohlsten M, Kalland T, Totterman TH . Efficient killing of B-CLL cells by superantigen-directed T cells. Blood 1993; 82: 1230–1238.
    CAS PubMed Google Scholar
14. Gitelson E, Hammond C, Mena J, Lorenzo M, Berinstein N, Spaner D . CLL-reactive T cells during tumor progression and after autologous tumor vaccines. Clin Cancer Res 2003; 9: 1656–1665.
    CAS PubMed Google Scholar
15. Auphan N, DiDonato JA, Helmberg A, Karin M . Immunosuppression by glucocorticoids: inhibition of NF_κ_B activity through induction of I_κ_B synthesis. Science 1995; 270: 286–290.
    Article CAS Google Scholar
16. Lee JC, Kassis S, Kumar S, Badger A, Adams JL . p38 mitogen-activated protein kinase inhibitors – mechanisms and therapeutic potentials. Pharmacol Ther 1999; 82: 389–397.
    Article CAS Google Scholar
17. Li L, Cousart S, Hu J, McCall CE . Characterization of interleukin-1 receptor-associated kinase in normal and endotoxin-tolerant cells. J Biol Chem 2000; 275: 23340–23345.
    Article CAS Google Scholar
18. Gamero AM, Young HA, Wiltrout RH . Inactivation of Stat3 in tumor cells: releasing a brake on immune responses against cancer? Cancer Cell 2004; 5: 111–112.
    Article CAS Google Scholar
19. Sengupta TK, Talbot ES, Scherle PA, Ivashkiv LB . Rapid inhibition of IL6 signaling and Stat3 activation mediated by MAP kinases. Proc Natl Acad Sci USA 1998; 95: 11107–11112.
    Article CAS Google Scholar
20. Gorden KB, Gorski KS, Gibson SJ, Kedl RM, Tomai MA, Alkan SS et al. Synthetic agonists reveal differences between human TLR7 and TLR8. J Immunol 2005; 174: 1259–1268.
    Article CAS Google Scholar
21. Lecoeur H, Fevrier M, Garcia S, Riviere Y, Gougeon ML . A novel flow cytometric assay for characterization of cell-mediated cytotoxicity. J Immunol Methods 2001; 253: 177–187.
    Article CAS Google Scholar
22. Bekeredjian-Ding IB, Wagner M, Schnurr M, Endres S, Hartmann G . Plasmacytoid DCs control TLR7 sensitivity of naive B cells via type I IFN. J Immunol 2005; 174: 4043–4050.
    Article Google Scholar
23. Fan H, Cook JA . Mechanisms of endotoxin tolerance. J Endotoxin Res 2004; 10: 71–84.
    Article CAS Google Scholar
24. Tosi P, Zinzani PL, Pellacani A, Ottaviani E, Magagnoli M, Tura S . Loxoribine affects fludarabine activity on freshly isolated B-CLL cells. Leuk Lymphoma 1997; 26: 343–348.
    Article CAS Google Scholar

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Acknowledgements

Supported by grants from the Leukemia Research Fund of Canada and the Ontario Cancer Research Network (OCRN) (to DS).RM and MT are employed by a company whose (potential) product was studied in this work.

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Author notes

1. L Radvanyi
   Present address: Department of Melanoma Medical Oncology, University of Texas, MD Anderson Cancer Center, Houston, Texas, 77030, USA

Authors and Affiliations

1. Division of Molecular and Cellular Biology, Research Institute, Sunnybrook and Women's College Health Sciences Center, Toronto, Canada
   D E Spaner, Y Shi, D White, J Mena, C Hammond, J Tomic & J Booth
2. Toronto-Sunnybrook Regional Cancer Center, Toronto, Canada
   D E Spaner
3. Department of Medicine, University of Toronto, Toronto, Canada
   D E Spaner
4. Department of Medical Biophysics, University of Toronto, Toronto, Canada
   D E Spaner, C Hammond & J Tomic
5. Immunology platform, Sanofi-Pasteur, Toronto, Canada
   L He & L Radvanyi
6. Department of Pharmacology, 3M Pharmaceuticals, 3M Center, St Paul, MN, USA
   M A Tomai & R L Miller

Authors

1. D E Spaner
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2. Y Shi
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3. D White
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4. J Mena
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5. C Hammond
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6. J Tomic
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7. L He
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8. M A Tomai
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9. R L Miller
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10. J Booth
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11. L Radvanyi
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Corresponding author

Correspondence toD E Spaner.

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Spaner, D., Shi, Y., White, D. et al. Immunomodulatory effects of Toll-like receptor-7 activation on chronic lymphocytic leukemia cells.Leukemia 20, 286–295 (2006). https://doi.org/10.1038/sj.leu.2404061

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• Received: 26 July 2005
• Revised: 24 October 2005
• Accepted: 03 November 2005
• Published: 08 December 2005
• Issue Date: 01 February 2006
• DOI: https://doi.org/10.1038/sj.leu.2404061

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