Point mutation and homozygous deletion of PTEN/MMAC1 in primary bladder cancers

Cairns, Paul; Evron, Ella; Okami, Kenji; Halachmi, Naomi; Esteller, Manel; Herman, James G.; Bose, Shikha; Wang, Steven I.; Parsons, Ramon; Sidransky, David

doi:10.1038/sj.onc.1201855

Cited by 195 publications

(186 citation statements)

References 12 publications

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“…While Steck et al (11) reported mutations in one of four primary renal carcinomas, later, larger studies have found no, or very few, PTEN/MMAC1 mutations in RCC (13)(14)(15)(16)(17). Furthermore, observations in other human tumor types have also shown few PTEN/MMAC1 mutations despite high LOH rates at the gene locus (22,23).…”

Section: Discussionmentioning

confidence: 99%

“…Initial screens of 9 RCCs seemed to support this hypothesis, showing loss of heterozygosity (LOH) in 40% of tumors and mutations in 15% of tumors (11,12). However, two subsequent larger studies failed to detect any mutations (13,14). Recently, Alimov et al (15) reported a 34% LOH rate at 10q23-25 but found only three mutations when they screened the subset of tumors that displayed LOH for mutations; Kondo et al (16) detected only five mutations, some of which were heterozygote, in a series of 68 sporadic renal cell carcinomas; and Sukosd et al (17) found high rates of 10q23.3 LOH in chRCC, but only in 2 of 50 cRCC, and detected no PTEN/MMAC1 mutations in the tumors with LOH.…”

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confidence: 98%

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Intragenic PTEN/MMAC1 Loss of Heterozygosity in Conventional (Clear-Cell) Renal Cell Carcinoma is Associated with Poor Patient Prognosis

Velickovic¹,

Delahunt²,

McIver

et al. 2002

Modern Pathology

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As a group, renal epithelial malignancies are frequently encountered in clinical practice. It is now appreciated that rather than being a single tumor type, they consist of a variety of morphotypes that show differing clinical behavior (1-3). The most frequently encountered subtype is conventional (clear cell) renal cell carcinoma (cRCC), representing 70% of all adult malignant primary renal tumors, whereas papillary renal cell carcinoma (pRCC) account for 10 -15%, and chromophobe renal cell carcinoma (chRCC), for approximately 5%. The remainder is made up of collecting-duct carcinomas and unclassifiable tumors (2-5).

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 98%

Intragenic PTEN/MMAC1 Loss of Heterozygosity in Conventional (Clear-Cell) Renal Cell Carcinoma is Associated with Poor Patient Prognosis

Velickovic¹,

Delahunt²,

McIver

et al. 2002

Modern Pathology

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“…In particular, the mutation of PTEN appears with a frequency of up to 50% in endometrial cancer (Tashiro et al, 1997) compared with other cancers, including glioblastoma (28%), prostate cancer (30%), and melanoma (15%) (Dahia, 2000). Abnormalities in the expression of the PTEN gene have been shown in esophageal cancer, melanoma, and prostate cancer (Cairns et al, 1997;Whang et al, 1998). Gene silencing by promoter methylation of PTEN has been reported in endometrial and prostate cancer (Salvesen et al, 2001).…”

Section: Discussionmentioning

confidence: 99%

Promoter Methylation and Silencing of PTEN in Gastric Carcinoma

Kang

Lee

Kim

2002

Laboratory Investigation

220

158

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SUMMARY:The PTEN/MMAC1/TEP1 gene (phosphatase and tensin homolog deleted on chromosome 10/mutated in multiple advanced cancers/TGF-␤ regulated and epithelial cell enriched phosphatase 1), which regulates the signaling pathways of Akt, is a novel tumor suppressor gene implicated in multiple cancers. Because a number of tumor suppressor genes are known to be silenced by aberrant promoter methylation, we examined the methylation status of the 5' CpG islands of PTEN using methylation-specific PCR. The altered expression of PTEN in 310 gastric carcinomas was analyzed by immunohistochemical staining using tissue-array and clinicopathologic profiles related to PTEN expression were characterized. Of 310 consecutive gastric carcinomas, 62 cases (20%) showed expression loss of PTEN. Altered PTEN expression was significantly associated with tumor depth and size, lymphatic invasion, advanced stage, pTNM stage, and patient survival (p Ͻ 0.001). The promoter methylation frequency of PTEN was found to be present in 26 (39%) of 66 cases examined, and 19 (73%) of 26 gastric cancer tissues showing promoter methylation exhibited the loss of PTEN expression. Abnormalities in the expression of PTEN significantly correlated with promoter methylation (p Ͻ 0.001). In conclusion, silencing of the PTEN gene occurs frequently in gastric carcinoma and aberrant promoter methylation is a major mechanism of silencing of the PTEN gene. The abnormalities of the PTEN gene are associated with tumor progression, metastasis, and survival. (Lab Invest 2002, 82:285-291).

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“…Among these mutations are structural rearrangements within the PTEN gene (intragenic inversions, insertions, deletions and duplications known as gross PTEN mutations) that occur in BRCA1-associated basal-like breast cancer (Saal et al, 2008). PTEN mutation frequencies affecting both alleles in various cancers are: endometrial (B50%), glioblastoma (B30%), prostate (B10%), and breast (B5%) (Cairns et al, , 1998Steck et al, 1997;Tashiro et al, 1997;Wang et al, 1997;Chiariello et al, 1998;Duerr et al, 1998;Lin et al, 1998;Shao et al, 1998;Ali et al, 1999;Zhou et al, 2002;Saal et al, 2005). The monoalleleic loss of PTEN is regularly observed in a considerable fraction of malignancies at the following frequencies: glioma (B75%), breast (B40-50%), colon (B20%), lung (B37%), prostate (B42%) (Teng et al, 1997;Bose et al, 1998;Feilotter et al, 1998;Lin et al, 1998;Rubin et al, 2000).…”

Section: Perturbations Of Pten Signaling In Cancermentioning

confidence: 99%

“…Sequencing of the PTEN gene in tumors found it to be one of the most commonly mutated tumor suppressors in human malignancies Rasheed et al, 1997;Tashiro et al, 1997;Wang et al, 1997Wang et al, , 1998Cairns et al, 1998;Duerr et al, 1998;Shao et al, 1998). The hereditary loss of PTEN leads to numerous autosomal dominant disorders: Cowden syndrome, Bannayan-Riley-Ruvalcaba syndrome, Lhermitte-Duclos disease, Proteus syndrome and Proteuslike syndrome, which are characterized by the presence of developmental defects, benign hamartomas and an increased risk of cancer Marsh et al, 1997;Zhou et al, 2000Zhou et al, , 2001.…”

Section: Introductionmentioning

confidence: 99%

The role of PTEN signaling perturbations in cancer and in targeted therapy

2008

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The PTEN tumor suppressor was discovered by its homozygous deletion and other mutations in cancer. Since then, PTEN has been shown to be a non-redundant, evolutionarily conserved phosphatase whose function affects diverse cellular progresses such as cell cycle progression, cell proliferation, chemotaxis, apoptosis, aging, muscle contractility, DNA damage response, angiogenesis and cell polarity. In accordance with its ability to influence multiple crucial cellular processes, PTEN has a major role in the pathogenesis of numerous diseases such as diabetes, autism and almost every cancer examined. This review will discuss the diverse ways in which PTEN signaling is modified in cancer, and how these changes correlate with and might possibly affect the action of targeted chemotherapy.

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Point mutation and homozygous deletion of PTEN/MMAC1 in primary bladder cancers

Cited by 195 publications

References 12 publications

Intragenic PTEN/MMAC1 Loss of Heterozygosity in Conventional (Clear-Cell) Renal Cell Carcinoma is Associated with Poor Patient Prognosis

Intragenic PTEN/MMAC1 Loss of Heterozygosity in Conventional (Clear-Cell) Renal Cell Carcinoma is Associated with Poor Patient Prognosis

Promoter Methylation and Silencing of PTEN in Gastric Carcinoma

The role of PTEN signaling perturbations in cancer and in targeted therapy

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