De l'Ipex à foxp3 : une nouvelle contribution de la pédiatrie à la compréhension du système immunitaire

A. Marabelle; M. Meyer; F. Demeocq; A. Lachaux

doi:10.1016/j.arcped.2007.10.005

De l'Ipex à foxp3 : une nouvelle contribution de la pédiatrie à la compréhension du système immunitaire

Translated title of the contribution: From Ipex to foxp3: A new contribution of pediatrics to the understanding of the immune system

A. Marabelle, M. Meyer, F. Demeocq, A. Lachaux

Research output: Contribution to journal › Short survey › peer-review

5 Citations (Scopus)

Abstract

In 10 years, the neonatal autoimmune enteropathy has been individualized from other causes of neonatal severe protracted diarrheas as a syndrome called Ipex for Immunodysregulation, Polyendocrinopathy, Enteropathy, X-linked. Thanks to linkage analyses in affected families, this rare paediatric syndrome with fatal outcome has been correlated to mutations of the foxp3 gene. Homozygous loss of function of foxp3 gene results in the absence of development of a crucial subpopulation of lymphocytes with CD4+CD25+ phenotype, called regulatory T-cells. The study of these lymphocytes allows a better understanding of the immune system homeostasis and of the physiopathology of Ipex syndrome, which is a prerequisite for treatment. Achieving ex vivo manipulation of such lymphocytes will end up on promising applications of cell therapy.

Translated title of the contribution	From Ipex to foxp3: A new contribution of pediatrics to the understanding of the immune system
Original language	French
Pages (from-to)	55-63
Number of pages	9
Journal	Archives de Pediatrie
Volume	15
Issue number	1
DOIs	https://doi.org/10.1016/j.arcped.2007.10.005
Publication status	Published - 1 Jan 2008
Externally published	Yes

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abstract = "In 10 years, the neonatal autoimmune enteropathy has been individualized from other causes of neonatal severe protracted diarrheas as a syndrome called Ipex for Immunodysregulation, Polyendocrinopathy, Enteropathy, X-linked. Thanks to linkage analyses in affected families, this rare paediatric syndrome with fatal outcome has been correlated to mutations of the foxp3 gene. Homozygous loss of function of foxp3 gene results in the absence of development of a crucial subpopulation of lymphocytes with CD4+CD25+ phenotype, called regulatory T-cells. The study of these lymphocytes allows a better understanding of the immune system homeostasis and of the physiopathology of Ipex syndrome, which is a prerequisite for treatment. Achieving ex vivo manipulation of such lymphocytes will end up on promising applications of cell therapy.",

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AU - Meyer, M.

AU - Demeocq, F.

AU - Lachaux, A.

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N2 - In 10 years, the neonatal autoimmune enteropathy has been individualized from other causes of neonatal severe protracted diarrheas as a syndrome called Ipex for Immunodysregulation, Polyendocrinopathy, Enteropathy, X-linked. Thanks to linkage analyses in affected families, this rare paediatric syndrome with fatal outcome has been correlated to mutations of the foxp3 gene. Homozygous loss of function of foxp3 gene results in the absence of development of a crucial subpopulation of lymphocytes with CD4+CD25+ phenotype, called regulatory T-cells. The study of these lymphocytes allows a better understanding of the immune system homeostasis and of the physiopathology of Ipex syndrome, which is a prerequisite for treatment. Achieving ex vivo manipulation of such lymphocytes will end up on promising applications of cell therapy.

AB - In 10 years, the neonatal autoimmune enteropathy has been individualized from other causes of neonatal severe protracted diarrheas as a syndrome called Ipex for Immunodysregulation, Polyendocrinopathy, Enteropathy, X-linked. Thanks to linkage analyses in affected families, this rare paediatric syndrome with fatal outcome has been correlated to mutations of the foxp3 gene. Homozygous loss of function of foxp3 gene results in the absence of development of a crucial subpopulation of lymphocytes with CD4+CD25+ phenotype, called regulatory T-cells. The study of these lymphocytes allows a better understanding of the immune system homeostasis and of the physiopathology of Ipex syndrome, which is a prerequisite for treatment. Achieving ex vivo manipulation of such lymphocytes will end up on promising applications of cell therapy.

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De l'Ipex à foxp3 : une nouvelle contribution de la pédiatrie à la compréhension du système immunitaire

Abstract

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