Germline mutations in the PTEN/MMAC1 gene in patients with Cowden disease

Nelen, Marcel; Staveren, Wilma C.G. van; Peeters, Els; Hassel, Mohammed Ben; Gorlin, Robert J.; Hamm, Henning; Lindboe, Christian Fredrik; Fryns, Jean‐Pierre; Sijmons, Rolf H.; Woods, Deontra; Mariman, E.C.M.; Padberg, G.W.A.M.; Kremer, Hannie

doi:10.1093/hmg/6.8.1383

Cited by 407 publications

(258 citation statements)

References 21 publications

(26 reference statements)

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“…Furthermore, previous studies have reported frequent loss of heterozygosity at chromosome 10q23 in endometrial and thyroid cancers (Simpkins et al, 1998). This gene is considered to act as a tumour suppressor gene in the pathogenesis of multiple cancers for several reasons: (i) This gene is frequently mutated in tumours arising in patients with Cowden disease and the Bannayan-Zonana syndrome, which are both characterized as hereditary syndromes leading to multiple hamartomas in the case of Cowden disease and both exhibit an increased risk of developing breast, thyroid and skin cancer Lynch et al, 1997;Marsh et al, 1997;Nelen et al, 1997). (ii) PTEN has been shown to act against phosphatidylinositol phosphates, pointing to a role of PTEN as a mediator of the phosphatidylinositol kinase pathway (Myers et al, 1997;Maehama and Dixon, 1998).…”

Section: Discussionmentioning

confidence: 99%

“…Thus, the reduced expression of PTEN may result from hypermethylation of the PTEN promotor, the enhanced degradation of the transcript or the transcriptional inactivation of the gene (Lynch et al, 1997;Whang et al, 1998). For instance, in Cowden disease, nonsense-mediated degradation of the gene was reported Lynch et al, 1997;Nelen et al, 1997). In addition, in a study using prostate cancer tissues and cell lines, the treatment of the cells with the demethylating agent 5-azadeoxycytidine led to the restoration of PTEN mRNA levels, which reflects a possible role of hypermethylation of the promotor in the regulation of PTEN transcription (Whang et al, 1998).…”

Section: Molecular and Cellular Pathologymentioning

confidence: 99%

“…In addition, recent studies indicate that PTEN may function as a mediator of the phosphatidylinositol (PI3') kinase pathway (Maehama and Dixon, 1998). These findings, along with the description of germline mutations and deletions of PTEN in two hereditary cancer predisposition diseases Marsh et al, 1997;Nelen et al, 1997), i.e. Cowden Disease and the Bannayan-Zonana-syndrome, point to a role of PTEN as a tumour suppressor gene in the pathogenesis of malignant tumours.…”

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confidence: 97%

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Reduced PTEN expression in the pancreas overexpressing transforming growth factor-beta 1

et al. 2002

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PTEN is a candidate tumour suppressor gene and frequently mutated in multiple cancers, however, not in pancreatic cancer.Recently, it has been demonstrated that PTEN expression is regulated by TGF-b1. Using TGF-b1 transgenic mice (n=7) and wildtype littermates (n=6), as well as pancreatic tissues obtained from organ donors (n=10) and patients with pancreatic cancer (n=10), we assessed the expression of PTEN by means of immunohistochemistry and semiquantitative PCR analysis. In addition, PANC-1 cells were treated with TGF-b1 in vitro and the levels of PTEN mRNA were determined in these cells. In human pancreatic cancers PTEN mRNA levels were significantly decreased (P50.05). In addition, in the pancreas of TGF-b1 transgenic mice the expression of PTEN was significantly reduced (P50.01), as compared to wildtype littermates and incubation of PANC-1 cells with TGF-b1 decreased PTEN mRNA levels after 24 h. Inasmuch as TGF-b1 decreases PTEN expression in human pancreatic cancer cells and human pancreatic cancers overexpress TGF-b1, the reduced expression of PTEN in pancreatic cancer may be mediated by TGF-b1 overexpression. Thus, although PTEN is not mutated in pancreatic cancers, the reduction of its expression may give pancreatic cancer cells an additional growth advantage.

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Section: Discussionmentioning

confidence: 99%

Section: Molecular and Cellular Pathologymentioning

confidence: 99%

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confidence: 97%

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Reduced PTEN expression in the pancreas overexpressing transforming growth factor-beta 1

et al. 2002

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“…Germ-line mutations of PTEN cause three autosomal dominant disorders, Cowden disease, Lhermitte-Duclos disease and Bannayan-Zonana syndrome, all of which form benign tumors in a variety of tissues with increased risk for cancer development Nelen et al, 1997;Marsh et al, 1998). PTEN is also essential for embryonic development: Its inactivation by gene targeted disruption in mouse resulted in early embryonic lethality, and Pten þ /À mice showed hyperplastic-dysplastic changes in many tissues (Di Cristofano et al, 1998).…”

Section: Introductionmentioning

confidence: 99%

GSK3β mediates suppression of cyclin D2 expression by tumor suppressor PTEN

Huang

et al. 2006

Oncogene

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PTEN, encoding a lipid phosphatase, is a tumor suppressor gene and is mutated in various types of cancers. It is reported to regulate G1 to S phase transition of the cell cycle by influencing the expression, protein stability and subcellular location of cyclin D1. Here, we provide evidence that PTEN modulates the transcription and protein stability of cyclin D2. Targeted deletion of Pten in mouse embryonic fibroblasts (MEFs) endowed cells with greater potential to overcome G1 arrest than wild-type MEFs and led to the elevated expression of cyclin D2, which was suppressed by the introduction of PTEN. We further defined a pathway involving GSK3b and b-catenin/TCF in PTEN-mediated suppression of cyclin D2 transcription. LiCl, an inhibitor of GSK3b, abolished inhibitory effect of PTEN on cyclin D2 expression, and TCF members could directly bind to the promoter of cyclin D2 and regulate its transcription in a CREB-dependent manner. Our results indicate that the downregulation of cyclin D2 expression by PTEN is mediated by the GSK3b/b-catenin/TCF pathway in cooperation with CREB, and suggest a convergence from the PI-3 kinase/PTEN pathway and the Wnt pathway in modulation of cyclin D2 expression.

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“…Mutation of PTEN appears to occur early in tumour development in endometrial cancer but late in the development of gliomas. Germline mutations in PTEN have also been found in the dominantly inherited Cowden, LhermitteDuclos, and Bannayan-Zonana syndromes, which are characterised by the formation of multiple benign tumours (Nelen et al, 1997).…”

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A novel germline mutation of PTEN associated with brain tumours of multiple lineages

et al. 2002

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We have identified a novel germline mutation in the PTEN tumour suppressor gene. The mutation was identified in a patient with a glioma, and turned out to be a heterozygous germline mutation of PTEN (Arg234Gln), without loss of heterozygosity in tumour DNA. The biological consequences of this germline mutation were investigated by means of transfection studies of the mutant PTEN molecule compared to wild-type PTEN. In contrast to the wild-type molecule, the mutant PTEN protein is not capable of inducing apoptosis, induces increased cell proliferation and leads to high constitutive PKB/Akt activation, which cannot be increased anymore by stimulation with insulin. The reported patient, in addition to glioma, had suffered from benign meningioma in the past but did not show any clinical signs of Cowden disease or other hereditary diseases typically associated with PTEN germline mutations. The functional consequences of the mutation in transfection studies are consistent with high proliferative activity. Together, these findings suggest that the Arg234Gln missense mutation in PTEN has oncogenic properties and predisposes to brain tumours of multiple lineages.

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Germline mutations in the PTEN/MMAC1 gene in patients with Cowden disease

Cited by 407 publications

References 21 publications

Reduced PTEN expression in the pancreas overexpressing transforming growth factor-beta 1

Reduced PTEN expression in the pancreas overexpressing transforming growth factor-beta 1

GSK3β mediates suppression of cyclin D2 expression by tumor suppressor PTEN

A novel germline mutation of PTEN associated with brain tumours of multiple lineages

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