Ometa C. Herman scite author profile

We have studied the role of secreted immunoglobulin (Ig)M in protection from infection with influenza virus and delineated the relative contributions of B-1 versus B-2 cell–derived IgM in this process. Mice deficient in secreted IgM but capable of expressing surface IgM and secreting other Ig classes show significantly reduced virus clearance and survival rates compared with wild-type controls. Irradiation chimeras in which only either B-1 or B-2 cells lack the ability to secrete IgM show mortality rates similar to those of mice in which neither B-1 nor B-2 cells secrete IgM. Dependence on both sources of IgM for survival is partially explained by findings in allotype chimeras that broadly cross-reactive B-1 cell–derived natural IgM is present before infection, whereas virus strain–specific, B-2 cell–derived IgM appears only after infection. Furthermore, lack of IgM secreted from one or both sources significantly impairs the antiviral IgG response. Reconstitution of chimeras lacking B-1 cell–derived IgM only with IgM-containing serum from noninfected mice improved both survival rates and serum levels of virus-specific IgG. Thus, virus-induced IgM must be secreted in the presence of natural IgM for efficient induction of specific IgG and for immune protection, identifying B-1 and B-2 cell–derived IgM antibodies as nonredundant components of the antiviral response.

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Innate and acquired humoral immunities to influenza virus are mediated by distinct arms of the immune system

Baumgarth

Herman

Jager

et al. 1999

Proc. Natl. Acad. Sci. U.S.A.

290

250

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ABSTRACT''Natural'' Igs, mainly IgM, comprise part of the innate immune system present in healthy individuals, including antigen-free mice. These Igs are thought to delay pathogenicity of infecting agents until antigen-induced high affinity Igs of all isotypes are produced. Previous studies suggested that the acquired humoral response arises directly from the innate response, i.e., that B cells expressing natural IgM, upon antigen encounter, differentiate to give rise both to cells that secrete high amounts of IgM and to cells that undergo affinity maturation and isotype switching. However, by using a murine model of inf luenza virus infection, we demonstrate here that the B cells that produce natural antiviral IgM neither increase their IgM production nor undergo isotype switching to IgG2a in response to the infection. These cells are distinct from the B cells that produce the antiviral response after encounter with the pathogen. Our data therefore demonstrate that the innate and the acquired humoral immunities to inf luenza virus are separate effector arms of the immune system and that antigen exposure per se is not sufficient to increase natural antibody production.

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The Role of B-1 and B-2 Cells in Immune Protection from Influenza Virus Infection

Baumgarth¹,

Chen²,

Herman³

et al. 2000

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CD4⁺T cells derived from B cell-deficient mice inhibit the establishment of peripheral B cell pools

Baumgarth

Jager

Herman

et al. 2000

Proc. Natl. Acad. Sci. U.S.A.

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Ometa C. Herman

B-1 and B-2 Cell–Derived Immunoglobulin M Antibodies Are Nonredundant Components of the Protective Response to Influenza Virus Infection

Innate and acquired humoral immunities to influenza virus are mediated by distinct arms of the immune system

The Role of B-1 and B-2 Cells in Immune Protection from Influenza Virus Infection

CD4⁺T cells derived from B cell-deficient mice inhibit the establishment of peripheral B cell pools

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Ometa C. Herman

B-1 and B-2 Cell–Derived Immunoglobulin M Antibodies Are Nonredundant Components of the Protective Response to Influenza Virus Infection

Innate and acquired humoral immunities to influenza virus are mediated by distinct arms of the immune system

The Role of B-1 and B-2 Cells in Immune Protection from Influenza Virus Infection

CD4+T cells derived from B cell-deficient mice inhibit the establishment of peripheral B cell pools

Contact Info

Product

Resources

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CD4⁺T cells derived from B cell-deficient mice inhibit the establishment of peripheral B cell pools