Literature DB >> 18978204

Foxn1 is required to maintain the postnatal thymic microenvironment in a dosage-sensitive manner.

Lizhen Chen1, Shiyun Xiao, Nancy R Manley.   

Abstract

The postnatal thymus is the primary source of T cells in vertebrates, and many if not all stages of thymocyte development require interactions with thymic epithelial cells (TECs). The Foxn1 gene is a key regulator of TEC differentiation, and is required for multiple aspects of fetal TEC differentiation. Foxn1 is also expressed in the postnatal thymus, but its function after birth is unknown. We generated a Foxn1 allele with normal fetal expression and thymus development, but decreased expression in the postnatal thymus. This down-regulation causes rapid thymic compartment degeneration and reduced T-cell production. TEC subsets that express higher Foxn1 levels are most sensitive to its down-regulation, in particular MHCII(hi)UEA-1(hi) medullary TECs. The requirement for Foxn1 is extremely dosage sensitive, with small changes in Foxn1 levels having large effects on thymus phenotypes. Our results provide the first evidence that Foxn1 is required to maintain the postnatal thymus. Furthermore, the similarities of this phenotype to accelerated aging-related thymic involution support the possibility that changes in Foxn1 expression in TECs during aging contribute to the mechanism of involution.

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Year:  2008        PMID: 18978204      PMCID: PMC2628364          DOI: 10.1182/blood-2008-05-156265

Source DB:  PubMed          Journal:  Blood        ISSN: 0006-4971            Impact factor:   22.113


  44 in total

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5.  Expression of Dll4 and CCL25 in Foxn1-negative epithelial cells in the post-natal thymus.

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  104 in total

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6.  Postnatal tissue-specific disruption of transcription factor FoxN1 triggers acute thymic atrophy.

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7.  Umbilical cord-derived mesenchymal stem cells regulate thymic epithelial cell development and function in Foxn1(-/-) mice.

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Review 8.  Sex steroid ablation: an immunoregenerative strategy for immunocompromised patients.

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9.  Restoration of Thymus Function with Bioengineered Thymus Organoids.

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10.  Impaired thymic selection and abnormal antigen-specific T cell responses in Foxn1(Δ/Δ) mutant mice.

Authors:  Shiyun Xiao; Nancy R Manley
Journal:  PLoS One       Date:  2010-11-04       Impact factor: 3.240

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