Monica Fava scite author profile

Monica Fava

4Publications

81Citation Statements Received

78Citation Statements Given

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Istituti di Ricovero e Cura a Carattere Scientifico, Istituto Giannina Gaslini, University of Genoa

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The TLX2 homeobox gene is a transcriptional target of PHOX2B in neural-crest-derived cells

Borghini

Bachetti

Fava

et al. 2006

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The TLX2 (HOX11L1, Ncx, Enx) and PHOX2B genes encode transcription factors crucial in the development of neural-crest-derived cells, leading to ANS (autonomic nervous system) specific neuronal lineages. Moreover, they share a similar expression pattern and are both involved in downstream steps of BMP (bone morphogenetic protein) signalling. In an attempt to reconstruct the gene network sustaining the correct development of the ANS, we have undertaken an in vitro experimental strategy to identify direct upstream regulators of the TLX2 gene. After characterizing a sequence displaying enhancer property in its 5' flanking region, we confirmed the functional link between the human PHOX2B and TLX2 genes. Transient transfections and electrophoretic-mobility-shift assays suggested that PHOX2B is able to bind the cell-specific element in the 5' regulatory region of the TLX2 gene, determining its transactivation in neuroblastoma cells. Such interaction was also confirmed in vivo by means of chromatin immunoprecipitation assay and, in addition, up-regulation of endogenous TLX2 mRNA level was demonstrated following PHOX2B over-expression, by quantitative real-time PCR. Finally, PHOX2B proteins carrying mutations responsible for CCHS (congenital central hypoventilation syndrome) development showed a severe impairment in activating TLX2 expression, both in vitro and in vivo. Taken together, these results support the PHOX2B-TLX2 promoter interaction, suggesting a physiological role in the transcription-factor cascade underlying the differentiation of neuronal lineages of the ANS during human embryogenesis.

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HOX11L1: a promoter study to evaluate possible expression defects in intestinal motility disorders

Fava

Borghini²,

Cinti³

et al. 2002

Int J Mol Med

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Assignment<footref rid="foot01"><sup>1</sup></footref> of the HOX11L2 gene to human chromosome band 5q35.1 and of its murine homolog to mouse chromosome bands 11A4–A5 by in situ hybridization

Cinti

Fava

Sancandi

et al. 2001

Cytogenet Genome Res

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Functional characterization of a minimal sequence essential for the expression of human TLX2 gene

et al. 2009

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TLX2 is an orphan homeodomain transcription factor whose expression is mainly associated with tissues derived from neural crest cells. Recently, we have demonstrated that PHOX2A and PHOX2B are able to enhance the neural cell-type specific expression of human TLX2 by binding distally the 5'-flanking region. In the present work, to deepen into the TLX2 transcription regulation, we have focused on the proximal 5'-flanking region of the gene, mapping the transcription start site and identifying a minimal promoter necessary and sufficient for the basal transcription in cell lines from different origin. Site-directed mutagenesis has allowed to demonstrate that the integrity of this sequence is crucial for gene expression, while electrophoretic mobility shift assays and chromatin immunoprecipitation experiments have revealed that such an activity is dependent on the binding of a PBX factor. Consistent with these findings, such a basal promoter activity has resulted to be enhanced by the previously reported PHOX2-responding sequence.[BMB reports 2009; 42(12): 788-793]

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Monica Fava

The TLX2 homeobox gene is a transcriptional target of PHOX2B in neural-crest-derived cells

HOX11L1: a promoter study to evaluate possible expression defects in intestinal motility disorders

Assignment<footref rid="foot01"><sup>1</sup></footref> of the HOX11L2 gene to human chromosome band 5q35.1 and of its murine homolog to mouse chromosome bands 11A4–A5 by in situ hybridization

Functional characterization of a minimal sequence essential for the expression of human TLX2 gene

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