Forkhead L2 Is Expressed in the Ovary and Represses the Promoter Activity of the Steroidogenic Acute Regulatory Gene

Pisarska, Margareta D.; Bae, Jang–Ho; Klein, Cynthia; Hsueh, Aaron J. W.

doi:10.1210/en.2003-1141

Cited by 182 publications

(174 citation statements)

References 77 publications

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“…Knockout mice present a blockage in ovarian development secondary to failure in granulosa cell differentiation. 14,15 It has been recently reported that wild-type FOXL2 and its mutant may have differential regulatory activities of the apoptosis. According to Kim et al,17 FOXL2 mutant induces a lower number of apoptotic cells due to deregulation of the caspase activation.…”

Section: Discussionmentioning

confidence: 99%

“…12 FOXL2 overexpression induces apoptosis in ovarian granulosa cells, whereas its alteration induces premature ovarian failure due to the abnormal granulosa cell differentiation. [13][14][15] The missense point mutation (C402G) induces an amino-acid change in FOXL2 (C134W) but neither altered function nor mislocalization of the protein have been reported. 10 Previous studies have shown that this mutation is specific for the adult type granulosa cell tumors and is present in up to 95-97% of these tumors.…”

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confidence: 99%

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Prognostic significance of FOXL2 mutation and mRNA expression in adult and juvenile granulosa cell tumors of the ovary

et al. 2011

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Recently, mutation of the FOXL2 gene has been consistently identified in adult granulosa cell tumors of the ovary. The purpose of this study is to investigate whether the FOXL2 mutation and mRNA expression have a role in the pathogenesis of juvenile and adult granulosa cell tumors and influence tumor progression. Thirty-four adult granulosa cell tumors and 20 juvenile granulosa cell tumors were examined for the presence of the FOXL2 (C402G) mutation. Expression levels were studied by quantitative PCR and immunohistochemistry. We found that FOXL2 (C402G) mutation was present in 19/27 (70%) of the adult type tumors but in none of the juvenile granulosa cell tumors (0/18). No correlation was encountered between the presence of FOXL2 mutation and various clinicopathologic parameters except for the presence of a different sex-cord component, which was more frequently found in the subgroup of wild-type adult granulosa cell tumors than in the mutated tumors. Patients with tumors harboring the FOXL2 (C402G) mutation had a worse disease-free survival than those with the wild-type gene. Expression levels of FOXL2 mRNA had an impact on disease-free survival in both adult and juvenile granulosa cell tumors. We also found that the mutated tumors had a higher immunohistochemical expression of the FOXL2 protein, and there was a linear correlation between mRNA and immunohistochemical FOXL2 expression in both adult and juvenile granulosa cell tumors. Patients with juvenile granulosa cell tumors and higher FOXL2 protein expression had worse overall survival and disease-free survival than those with negative or weakly immunoreactive tumors. Our data suggest that FOXL2 mutation and mRNA expression are of prognostic importance in both adult and juvenile granulosa cell tumors.

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Section: Discussionmentioning

confidence: 99%

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confidence: 99%

Prognostic significance of FOXL2 mutation and mRNA expression in adult and juvenile granulosa cell tumors of the ovary

et al. 2011

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“…We found that PPARGC1A and NR5A2, both involved in cholesterol homoeostasis (35), are stimulated by FOXL2. Previous works (13) have shown that FOXL2 represses expression of Star, a protein that controls cholesterol transport from the outer to the inner mitochondrial membranes. In agreement with this finding, FOXL2 up-regulated the cholesterol 25-hydroxylase whose product is a potent inhibitor of sterol synthesis (42).…”

Section: Analysis Of the Promoters Responding To Foxl2 In Terms Of Trmentioning

confidence: 98%

“…Only three of them, namely the genes encoding the gonadotropin-releasing hormone receptor (GnRHr), the alpha subunit of the gonadotropins (Cga), and the steroidogenic acute regulatory protein (StAR) have been reported so far (11)(12)(13). We have recently suggested that the aromatase gene (CYP19A1) is transcriptionally activated by FOXL2 (14,15).…”

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confidence: 99%

Potential targets of FOXL2, a transcription factor involved in craniofacial and follicular development, identified by transcriptomics

Batista

Vaiman

Dausset

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

110

102

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FOXL2 is a gene encoding a forkhead transcription factor, whose mutations are responsible for the blepharophimosis-ptosisepicanthus inversus syndrome that often involves premature ovarian failure. FOXL2 is one of the earliest ovarian markers and it offers, along with its targets, an excellent model to study ovarian development and function in normal and pathological conditions. We have recently shown that the aromatase gene is a target of FOXL2, and only three other targets have been reported so far. To detect potential transcriptional targets of FOXL2, we used DNA chips and quantitative PCR to compare the transcriptomes of granulosa-like cells overexpressing, or not, FOXL2. This analysis showed that mediators of inflammation, apoptotic and transcriptional regulators, genes involved in cholesterol metabolism, and genes encoding enzymes and transcription factors involved in reactive oxygen species detoxification were up-regulated. On the other hand, FOXL2 down-regulated the transcription of several genes involved in proteolysis and signal transduction and in transcription regulation. A bioinformatic analysis was conducted to discriminate between potential target promoters activated and repressed by FOXL2. In addition, the promoters of strongly activated genes were enriched in forkhead recognition sites, suggesting that these genes might be direct FOXL2 targets. Altogether, these results provide insight into the activity of FOXL2 and may help in understanding the mechanisms of pathogenesis of FOXL2 mutations if the targets prove to be the same in the ovary.forkhead ͉ infertility ͉ premature ovarian failure ͉ ovary

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“…Mutations in FOXL2 cause blepharophimosis, ptosis, epicanthus inversus syndrome (OMIM #110100), and blepharophimosis, ptosis, epicanthus inversus syndrome type I is accompanied by premature ovarian failure of the affected female (Crisponi et al, 2001). FOXL2 is mainly expressed in undifferentiated granulosa cells, and blockage of ovarian follicle development because of the failure of granulosa cell differentiation was observed in FoxL2 lacZ homozygous mutant mice (Pisarska et al, 2004;Uda et al, 2004).…”

Section: Introductionmentioning

confidence: 99%

Differential apoptotic activities of wild-type FOXL2 and the adult-type granulosa cell tumor-associated mutant FOXL2 (C134W)

et al. 2010

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Some mutations in FOXL2 result in premature ovarian failure accompanied by blepharophimosis, ptosis, epicanthus inversus syndrome type I disease, and FOXL2-null mice exhibit developmental defects in granulosa cells. Recently, FOXL2 c.402C4G, a new somatic mutation that leads to a p.C134W change, was found in the majority of adult-type ovarian granulosa cell tumors (GCTs). In this study, we investigated the possible mechanisms by which the C134W mutation contributes to the development of GCTs. Wild-type (WT) and mutant FOXL2 displayed differential apoptotic activities. Specifically, WT FOXL2 induced significant granulosa cell death, but the mutant exhibited minimal cell death. The FOXL2-induced apoptotic response was greatly dependent on caspase 8, BID and BAK because the depletion of any of these three proteins inhibited FOXL2 from eliciting the full apoptotic response. Activation of caspase 8 and subsequent increased production of truncated BID, and oligomerization of BAK, and release of cytochrome c were all associated with the apoptosis induced by WT FOXL2 expression. In contrast, the mutant FOXL2 was unable to elicit the full array of apoptotic signaling responses. In addition, we found differential TNF-R1 (tumor necrosis factor-receptor 1) and Fas (CD95/APO-1) upregulation between the WT and the mutant, and the silencing of TNF-R1 or Fas and the blockage of the death signaling mediated by TNF-R1 or Fas using TNF-Fc or Fas-Fc, respectively, resulted in significant attenuations of FOXL2-induced apoptosis. Moreover, granulosa cells that expressed either WT FOXL2 or mutant exhibited distinct cell death sensitivities on activation of death receptors and deprivation of serum. Thus, the differential activities of FOXL2 and its mutant may partially account for the pathophysiology of GCT development.

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Forkhead L2 Is Expressed in the Ovary and Represses the Promoter Activity of the Steroidogenic Acute Regulatory Gene

Cited by 182 publications

References 77 publications

Prognostic significance of FOXL2 mutation and mRNA expression in adult and juvenile granulosa cell tumors of the ovary

Prognostic significance of FOXL2 mutation and mRNA expression in adult and juvenile granulosa cell tumors of the ovary

Potential targets of FOXL2, a transcription factor involved in craniofacial and follicular development, identified by transcriptomics

Differential apoptotic activities of wild-type FOXL2 and the adult-type granulosa cell tumor-associated mutant FOXL2 (C134W)

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