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Multicenter Study
. 2012 Jan;91(1):49-56.
doi: 10.1097/MD.0b013e3182433d77.

IgG4-related systemic disease: features and treatment response in a French cohort: results of a multicenter registry

Mikael Ebbo  1 Laurent DanielMichel PavicPascal SèveMohamed HamidouEmmanuel AndresStéphane BurteyLaurent ChicheJacques SerratriceMaïté Longy-BoursierMarc RuivardJulien HarocheBertrand GodeauAnne-Bérengère BeucherJean-Marie BerthelotThomas PapoJean-Loup PennaforteAudrey BenyamineNoémie JourdeCédric LandronPascal RoblotOlivier MoranneChristine SilvainBrigitte GranelFanny BernardVeronique VeitKarin MazodierEmmanuelle BernitHugues RoussetJosé BoucrautJean-Jacques BoffaPierre-Jean WeillerGilles KaplanskiPierre AucouturierJean-Robert HarléNicolas Schleinitz
Affiliations
Free article
Multicenter Study

IgG4-related systemic disease: features and treatment response in a French cohort: results of a multicenter registry

Mikael Ebbo et al. Medicine (Baltimore). 2012 Jan.
Free article

Abstract

IgG4-related systemic disease is now recognized as a systemic disease that may affect various organs. The diagnosis is usually made in patients who present with elevated IgG4 in serum and tissue infiltration of diseased organs by numerous IgG4+ plasma cells, in the absence of validated diagnosis criteria. We report the clinical, laboratory, and histologic characteristics of 25 patients from a French nationwide cohort. We also report the treatment outcome and show that despite the efficacy of corticosteroids, a second-line treatment is frequently necessary. The clinical findings in our patients are not different from the results of previous reports from Eastern countries. Our laboratory and histologic findings, however, suggest, at least in some patients, a more broad polyclonal B cell activation than the skewed IgG4 switch previously reported. These observations strongly suggest the implication of a T-cell dependent B-cell polyclonal activation in IgG4-related systemic disease, probably at least in part under the control of T helper follicular cells.

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References

    1. Aalberse RC, Dieges PH, Knul-Bretlova V, Vooren P, Aalbers M, van Leeuwen J. IgG4 as a blocking antibody. Clin Rev Allergy. 1983; 1: 289–302.
    1. Aalberse RC, Stapel SO, Schuurman J, Rispens T. Immunoglobulin G4: an odd antibody. Clin Exp Allergy. 2009; 39: 469–477.
    1. Akitake R, Watanabe T, Zaima C, Uza N, Ida H, Tada S, Nishida N, Chiba T. Possible involvement of T helper type 2 responses to Toll-like receptor ligands in IgG4-related sclerosing disease. Gut. 2010; 59: 542–545.
    1. Boulanger E, Fuentes V, Meignin V, Mougenot B, Labaume S, Gouilleux-Gruart V, Cogne M, Aucouturier P, Clauvel JP, Ronco P, Lassoued K. Polyclonal IgG4 hypergammaglobulinemia associated with plasmacytic lymphadenopathy, anemia and nephropathy. Ann Hematol. 2006; 85: 833–840.
    1. Cheuk W, Yuen HK, Chu SY, Chiu EK, Lam LK, Chan JK. Lymphadenopathy of IgG4-related sclerosing disease. Am J Surg Pathol. 2008; 32: 671–681.

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