Transcription of platelet-derived growth factor receptor   in Leydig cells involves specificity protein 1 and 3

Bergeron, François; Bagu, Edward T.; Tremblay, Jacques

doi:10.1530/jme-10-0145

Cited by 14 publications

(11 citation statements)

References 69 publications

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“…The increase in activity may have been due to elimination of repressive elements upstream of K1117 bp. The presence of alternating d(TG)n-type purine-pyrimidine di-nucleotide repeats in the deleted region could have suppressed the HAMP promoter activity (Naylor & Clark 1990, Bergeron et al 2011; however, in silico analysis of the deleted region revealed a potential CP-2 transcription factor binding site K1191/K1181 with a WT sequence -GGCCATGCCCT- (Heinemeyer et al 1998). CP-2 is expressed in hepatocytes and acts either as a transcription enhancer or repressor (Veljkovic & Hansen 2004, Jang et al 2010.…”

Section: Discussionmentioning

confidence: 99%

Friend of GATA suppresses the GATA-induced transcription of hepcidin in hepatocytes through a GATA-regulatory element in the HAMP promoter

Bagu

Santos²

2011

Journal of Molecular Endocrinology

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Hepcidin is an antimicrobial peptide hormone involved in the metabolism of iron, encoded for by the HAMP gene mainly in hepatocytes. It's expressed at lower levels in other cells such as the macrophages. The mechanisms that determine tissue-specific expression of hepcidin remain unclear. GATA-and its co-factor Friend of GATA (FOG) modulate the tissue-specific transcription of other genes involved in the metabolism of iron. GATA proteins are group of evolutionary conserved transcriptional regulators that bind to the consensus motif -WGATAR-in the promoter. We characterized a 1 . 3 kb fragment of the 5 0 -flanking sequence of the HAMP gene in Huh7 cells, which express HAMP. Transfection of 5 0 -deletions of the HAMP promoter in Huh7 cells revealed two regions, K932/K878 and K155/K96, that when deleted decreased promoter activity. Using site-directed mutations in the HAMP promoter region K155/K96 we identified two subregions, K138/K125 and K103/K98, which when mutated suppressed promoter activity by 70 and 90% respectively. Site K103/K98 with a sequence -TTATCT-to which endogenous GATA proteins 4 and 6 bind and transactivate HAMP is a GATA-regulatory element (RE). Mutation of the GATA-RE abrogated binding of GATA proteins 4 and 6 to the promoter and blunted the GATA transactivation of HAMP. FOG proteins 1 and 2 suppressed the endogenous and exogenous GATA activation of the HAMP promoter. We concluded that the GATA-RE, -TTATCT-in the HAMP promoter region K103/K98 is crucial for the GATA-4 and GATA-6 driven transcription of hepcidin in Huh7 cells and that FOG proteins moderate the transcription by suppressing the GATA transactivation of HAMP.

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Section: Discussionmentioning

confidence: 99%

Friend of GATA suppresses the GATA-induced transcription of hepcidin in hepatocytes through a GATA-regulatory element in the HAMP promoter

Bagu

Santos²

2011

Journal of Molecular Endocrinology

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“…The expression of PDGFRA is regulated by the transcription factors SP1 and SP3 (Bergeron et al, 2011). The downstream signaling of PDGFRA in regulating the commitment of SLCs into the LC lineage is still unclear.…”

Section: Regulation Of Leydig Cell Developmentmentioning

confidence: 99%

Insights into the Development of the Adult Leydig Cell Lineage from Stem Leydig Cells

et al. 2017

Front. Physiol.

188

166

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Adult Leydig cells (ALCs) are the steroidogenic cells in the testes that produce testosterone. ALCs develop postnatally from a pool of stem cells, referred to as stem Leydig cells (SLCs). SLCs are spindle-shaped cells that lack steroidogenic cell markers, including luteinizing hormone (LH) receptor and 3β-hydroxysteroid dehydrogenase. The commitment of SLCs into the progenitor Leydig cells (PLCs), the first stage in the lineage, requires growth factors, including Dessert Hedgehog (DHH) and platelet-derived growth factor-AA. PLCs are still spindle-shaped, but become steroidogenic and produce mainly androsterone. The next transition in the lineage is from PLC to the immature Leydig cell (ILC). This transition requires LH, DHH, and androgen. ILCs are ovoid cells that are competent for producing a different form of androgen, androstanediol. The final stage in the developmental lineage is ALC. The transition to ALC involves the reduced expression of 5α-reductase 1, a step that is necessary to make the cells to produce testosterone as the final product. The transitions along the Leydig cell lineage are associated with the progressive down-regulation of the proliferative activity, and the up-regulation of steroidogenic capacity, with each step requiring unique regulatory signaling.

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“…The SP family of transcription factors, including Sp3, is highly regulated at the posttranslational level. Although Sp3 is able to up- ( 35,36 ) and down-regulate gene transcription (37)(38)(39), phosphorylation is generally associated with increased DNA binding activity and, consequently, increased transcriptional activation ( 35,40 ). Modifi cations such as acetylation have also been described to activate ( 21 ) and repress ( 41 ) Sp3 transcriptional activity, whereas sumoylated Sp3 signifi cantly represses transcription (42)(43)(44).…”

Section: Downloaded Frommentioning

confidence: 99%

Okadaic acid inhibits the trichostatin A-mediated increase of human CYP46A1 neuronal expression in a ERK1/2-Sp3-dependent pathway

Nunes

Moutinho

Milagre

et al. 2012

Journal of Lipid Research

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Transcription of platelet-derived growth factor receptor in Leydig cells involves specificity protein 1 and 3

Cited by 14 publications

References 69 publications

Friend of GATA suppresses the GATA-induced transcription of hepcidin in hepatocytes through a GATA-regulatory element in the HAMP promoter

Friend of GATA suppresses the GATA-induced transcription of hepcidin in hepatocytes through a GATA-regulatory element in the HAMP promoter

Insights into the Development of the Adult Leydig Cell Lineage from Stem Leydig Cells

Okadaic acid inhibits the trichostatin A-mediated increase of human CYP46A1 neuronal expression in a ERK1/2-Sp3-dependent pathway

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