Seminars in Hematology
Volume 41, Issue 3 , Pages 207-223, July 2004

Recent advances in the molecular biology and immunobiology of chronic lymphocytic leukemia

  • Manlio Ferrarini

      Affiliations

    • Division of Medical Oncology C, Istituto Nazionale per la Ricerca sul Cancro, Genova, and Dipartmento di Oncologia Clinica e Sperimentale, Universitá di Genova, Genova, Italy
    • ,
  • Nicholas Chiorazzi

      Affiliations

    • North Shore-LIJ Research Institute and Departments of Medicine, North Shore University Hospital and NYU School of Medicine, Manhasset, NY, USA
    • Corresponding Author InformationAddress correspondence to Manlio Ferrarini, Istituto Nazionale per la Ricerca sul Cancro, IST Largo Rosanna Benzi, n. 10, 16132 Genova, Italy

Abstract 

B-cell chronic lymphocytic leukemia (B-CLL) has long been viewed as a relatively homogeneous disease caused by the accumulation of monoclonal immature, immunoincompetent B cells with faulty apoptotic capacities. However, recent evidence, reviewed here, demonstrates that at least two different B-CLL subgroups exist with different clinical courses and outcomes. The malignant cells from both B-CLL subgroups are antigen-experienced cells that have a normal apoptotic apparatus and turnover continually. The leukemic cells of the two B-CLL subgroups have engaged antigen before transformation, although primarily the cells of patients in the poor outcome subgroup can respond to antigens following transformation. The difference in the ability to respond to antigen as a full-fledged B-CLL probably accounts for the different biological features and clinical outcomes of the patients in these subgroups.

To access this article, please choose from the options below

Login to an existing account or Register a new account.

  • Purchase this article for 31.50 USD (You must login/register to purchase this article)

    Online access for 24 hours. The PDF version can be downloaded as your permanent record.

  • Subscribe to this title

    Get unlimited online access to this article and all other articles in this title 24/7 for one year.

  • Claim access now

    For current subscribers with Society Membership or Account Number.

  • Visit SciVerse ScienceDirect to see if you have access via your institution.
 

 Supported in part by RO1 Grants No. CA 81554 and CA 87956 from the National Cancer Institute and a General Clinical Research Center Grant (M01 RR018535) from the National Center for Research Resources, the Associazione Italian Ricerca sul Cancro (AIRC), and MURST. The Peter J. Sharp Foundation, The Marks Family Foundation, the Jean Walton Fund for Lymphoma & Myeloma Research, and the Joseph Eletto Leukemia Research Fund also provided support for these studies.

PII: S0037-1963(04)00090-3

doi:10.1053/j.seminhematol.2004.05.003

Seminars in Hematology
Volume 41, Issue 3 , Pages 207-223, July 2004

Article Tools

* Image Usage & Resolution