Abstract

SUMMARY Immune dysregulation, polyendocrinopathy and enteropathy with X-linked inheritance (IPEX) is a serious disease arising from mutations in FOXP3. This gene codifies for a transcription factor whose dysfunction results in hyperactivation of T cells. It is not clear, however, why an intermediate phenotype is not seen in heterozygous females, who are completely healthy. In order to address this question, we investigated X-chromosome inactivation in peripheral blood lymphocytes from a heterozygous female with a child affected by IPEX. No preferential inactivation was shown in freshly sorted CD4+, CD8+, CD19+ cells or in IL-2 cultured CD4 and CD8 T cells, indicating that peripheral blood lymphocytes in these women are randomly selected. Moreover, only one single FOXP3 transcript was expressed by CD4 T cell clones analysed by RT-PCR, confirming that this gene is subject to X- inactivation. We hypothesize that hyper-activation of T cell in carriers of FOXP3 mutations is regulated by the presence of normal regulatory T cells.

Keywords

FOXP3BiologyX-inactivationCD8CD19X chromosomeImmunologyMutationPhenotypeMolecular biologyTCIRG1Immune dysregulationGeneticsT cellGeneImmune systemInterleukin 21

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Year
2002
Type
article
Volume
130
Issue
1
Pages
127-130
Citations
96
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Alberto Tommasini, Sérgio Ferrari, Daniele Moratto et al. (2002). X-chromosome inactivation analysis in a female carrier of FOXP3 mutation. Clinical & Experimental Immunology , 130 (1) , 127-130. https://doi.org/10.1046/j.1365-2249.2002.01940.x

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DOI
10.1046/j.1365-2249.2002.01940.x