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Hyper IgM immunodeficiency. A primary dysfunction of B lymphocyte isotype switching.
D Levitt, … , K Rich, M D Cooper
D Levitt, … , K Rich, M D Cooper
Published November 1, 1983
Citation Information: J Clin Invest. 1983;72(5):1650-1657. https://doi.org/10.1172/JCI111124.
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Research Article

Hyper IgM immunodeficiency. A primary dysfunction of B lymphocyte isotype switching.

Abstract

Immunological evaluations (lymphocyte markers, B cell differentiation, T cell function) were performed on peripheral blood mononuclear cells from four individuals with hyper IgM immunodeficiency. Number, proportion, and proliferation of T lymphocytes and T lymphocyte subpopulations were relatively normal in affected individuals. The percentage and number of B cells expressing surface IgM and IgD were either normal or elevated in both blood and lymph nodes. However, surface IgG- and IgA-bearing B lymphocytes were completely absent. In vitro stimulation of blood lymphocytes with both T cell-dependent and T-cell independent polyclonal B cell activators resulted in normal numbers of IgM plasma cells and IgM secretion in cultures, but failed to induce any IgG- or IgA-producing cells. This failure of isotype switching was intrinsic to the B cell population and did not involve aberrant T cell help or suppression. Therefore, individuals with this disorder possess an intrinsic B cell dysfunction that is not related to abnormal T cell regulation.

Authors

D Levitt, P Haber, K Rich, M D Cooper

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