Abstract

During the past year we have published a detailed analysis of the B cell response in HCV-infected patients with and without mixed cryoglobulinemia (MC), and the impact of rituximab treatment on B cell function in these patients. MC, the most common of the B-cell abnormalities in HCV-infected patients, is characterized by clonal proliferation of B-cells and the formation of cold-precipitable cryoglobulin complexes composed of IgM antibodies with rheumatoid factor activity. Despite activation and clonal expansion of B-cells in chronic HCV infection we observed a reduction in the total number of B cells and in the size of the naive B cell subset in patients with MC compared to HCV-infected patients without MC and healthy controls. The reduced frequency of naive B cells in HCV-infected patients with MC was associated with decreased ex vivo expression of the antiapoptotic protein Bcl-2 compared to HCV-infected patients without MC and healthy controls, and with an increased in vitro sensitivity of naive B-cells to apoptosis. These results provide mechanistic data on the death of naive B-cells to a previous study by Cacoub et al. who reported a decreased naive B-cell frequency in untreated MC patients but did not examine the underlying mechanism (Blood 2008;111:5334-5341). As naive B-cells comprise approximately 70% of all B-cells, their rapid turnover may trigger the release of immature B-cells from the bone marrow. Indeed, we observed four-fold expansion and skewing (lower T1/T2-ratio) of the immature B-cell subset in HCV-infected patients with MC. This immature subset is important following treatment with rituximab as during the initial stages of B cell reconstitution these cells comprised the majority of B-cells. Based on the observed reduction of CD19+ B-cell percentages and numbers, and the increased apoptosis susceptibility of their main fraction, the naive B-cell population, we propose that the increased size of the immature B-cell subset is due to a secondary egress from the bone marrow to compensate for the B-cell loss in the periphery. This process may be mediated by BAFF, a B-cell growth factor that is elevated in the plasma of HCV patients (J Immunol 2010;185:3019-3027;Ann Rheum Dis 2009;68:337-344).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Investigator-Initiated Intramural Research Projects (ZIA)
Project #
1ZIADK054515-06
Application #
8553537
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
6
Fiscal Year
2012
Total Cost
$129,591
Indirect Cost

  Institution

Name
National Institute of Diabetes and Digestive and Kidney Diseases
Department
Type
DUNS #
City
State
Country
Zip Code

  Publications

Holz, Lauren E; Yoon, Joo Chun; Raghuraman, Sukanya et al. (2013) Reply: b-cell frequency in HCV-related mixed cryoglobulinemia. Hepatology 58:448-9
Holz, Lauren E; Yoon, Joo Chun; Raghuraman, Sukanya et al. (2012) B cell homeostasis in chronic hepatitis C virus-related mixed cryoglobulinemia is maintained through naive B cell apoptosis. Hepatology 56:1602-10
Yoon, Joo Chun; Rehermann, Barbara (2009) Determination of HCV-specific T-cell activity. Methods Mol Biol 510:403-13
Shiina, Masaaki; Rehermann, Barbara (2009) Analysis of HCV-specific T cells by flow cytometry. Methods Mol Biol 510:415-26
Rehermann, Barbara (2009) Hepatitis C virus versus innate and adaptive immune responses: a tale of coevolution and coexistence. J Clin Invest 119:1745-54
Mix, Heiko; Weiler-Normann, Christina; Thimme, Robert et al. (2008) Identification of CD4 T-cell epitopes in soluble liver antigen/liver pancreas autoantigen in autoimmune hepatitis. Gastroenterology 135:2107-18