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Review
. 2015 Feb;156(2):131-40.
doi: 10.1016/j.clim.2014.12.007. Epub 2014 Dec 27.

Fetal-onset IPEX: report of two families and review of literature

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Review

Fetal-onset IPEX: report of two families and review of literature

Mariana Moraes Xavier-da-Silva et al. Clin Immunol. 2015 Feb.

Abstract

Early-life autoimmunity is an IPEX characteristic, however intrauterine forms had not yet been described. Here, two unrelated families with clear evidence of fetal-onset IPEX are reported. One had 5 miscarriages of males in two generations, and a newborn presenting type-1 diabetes mellitus immediately after birth, diarrhea, thrombocytopenia, eczematous dermatitis, eosinophilia, high IgE levels and autoantibodies to pancreatic islet antigens at 4-days-old. Maternal serology was negative. He presented a FOXP3 mutation, c.1189C>T, p.Arg397Trp, previously described only in another family with IPEX at birth. The second family had several miscarriages of males in three consecutive generations and a novel FOXP3 c.319_320delTC mutation was observed in two miscarried monochorionic twin male fetuses. These twins died at 21weeks of gestation due to hydrops, and CD3+ infiltrating lymphocytes were found in their pancreas. We demonstrate that: i) IPEX may develop in fetal life; and ii) c.1189C>T and c.319_320delTC mutations are associated with early-onset phenotype.

Keywords: FOXP3; Fetal IPEX; Fetal hydrops; Miscarriages; Primary immunodeficiency; Type I diabetes mellitus.

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