N. Sigmund scite author profile

To test the hypothesis that a Th2 response to Helicobacter pylori is necessary for protection and to address the possibility that humoral and Th2 cellular responses may compensate for each other, we generated mice deficient in both interleukin-4 (IL-4) and antibodies. The immunized double-knockout mice were protected from H. pylori challenge, as were the parental strains and wild-type C57BL/6 mice. Neutralization of IL-4 in B-cell-deficient mice did not prevent protection. Immunized IL-5-deficient mice were also protected. Thus, IL-4 and IL-5 are not essential for protection.

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T cell cytokines determine the severity of experimental IgA nephropathy by regulating IgA glycosylation

Chintalacharuvu

Nagy

Sigmund

et al. 2001

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Hyperfunction of Th2 cells and aberrant glycosylation of IgA have been proposed independently as factors in the pathogenesis of IgA nephropathy (IgAN), the most common form of glomerulonephritis. To investigate the relationship between Th2 cytokines and IgA glycosylation in the genesis of IgAN, we induced IgAN in C3HeB and BALB/c mice by oral immunization and intranasal challenge with Sendai virus. Although both strains of mice developed microhaematuria and glomerular IgA immune deposits to similar degrees, only BALB/c mice developed significant renal insufficiency. More profound reductions of terminal galactosylation and sialylation occurred in Sendai virus‐specific IgA from BALB/c versus C3HeB mice, and splenocytes from immunized BALB/c mice produced more Th2 and less Th1 cytokines compared to C3HeB mice when stimulated with antigen in vitro. Furthermore, the decreased glycosylation of IgA elicited by Th2 cytokines in vitro was blunted by the addition of IFN‐γ. We conclude that increased production of Th2 cytokines can lead to abnormalities in IgA glycosylation, which in turn promote heightened phlogistic responses to IgA immune complexes lodging in the glomerulus. We suggest that a relative or absolute increase in Th2 cytokine production in response to mucosal infection is a significant pathogenic factor in human IgAN.

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The role of nasal tolerance in a model of IgA nephropathy induced in mice by Sendai virus

Amore

Coppo

Nedrud

et al. 2004

Clinical Immunology

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Orally immunized μMT antibody-deficient mice are protected against H. felis infection

Nedrud¹,

Blanchard²,

Redline³

et al. 1998

Gastroenterology

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N. Sigmund

Antibody-Independent Protective Mucosal Immunity to Gastric Helicobacter Infection in Mice

Vaccine-Induced Protection againstHelicobacter pyloriin Mice Lacking Both Antibodies and Interleukin-4

T cell cytokines determine the severity of experimental IgA nephropathy by regulating IgA glycosylation

The role of nasal tolerance in a model of IgA nephropathy induced in mice by Sendai virus

Orally immunized μMT antibody-deficient mice are protected against H. felis infection

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