Overexpression of the p53 protein and allele loss at 17p13 in ovarian carcinoma

Eccles, Diana M.; Brett, L; Lessells, A M; Gruber, Lucinda; Lane, David P.; Steel, C. M.; Leonard, Robert

doi:10.1038/bjc.1992.8

Cited by 92 publications

(43 citation statements)

References 25 publications

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“…[4][5][6] Throughout chromosome 17 frequent genetic deletions have been identified, suggesting that multiple tumour-suppressor genes may exist on this chromosome. [26][27][28][29] Our data therefore implicate miR-195 and miR-497 as potential tumour-suppressor genes. Since its first description by Swerdlow in 1959, primary peritoneal carcinoma has been treated similarly to ovarian serous carcinoma by surgery and chemotherapy.…”

Section: Discussionmentioning

confidence: 96%

Potentially important microRNA cluster on chromosome 17p13.1 in primary peritoneal carcinoma

et al. 2009

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MicroRNAs are a group of small non-coding RNAs approximately 22 nucleotides in length. Recent work has shown differential expression of mature microRNAs in human cancers. We characterized the alteration in expression of a select group of microRNAs in primary peritoneal carcinoma relative to matched cases of ovarian serous carcinoma. MicroRNA expression was analysed using semi-quantitative stem-loop RT-PCR on a set of 34 formalin-fixed paraffin-embedded samples. Protein expression of p53 and bcl-2 was quantified in the corresponding tissue microarray. We provide definitive evidence that there is downregulation of a select group of microRNAs in tumours meeting Gynaecological Oncology Group criteria for primary peritoneal carcinoma relative to ovarian serous carcinoma. Specifically, we show decreased p53 expression and downregulation of miR-195 and miR-497 from the microRNA cluster site at chromosome 17p13.1 in primary peritoneal carcinoma relative to ovarian serous carcinoma. miR-195 and miR-497 may have potential roles as tumour-suppressor genes in primary peritoneal tumourigenesis.

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Section: Discussionmentioning

confidence: 96%

Potentially important microRNA cluster on chromosome 17p13.1 in primary peritoneal carcinoma

et al. 2009

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“…These genes include the TP53 tumor suppressor at 17p13 (Marks et al, 1991;Okamoto et al, 1991;Tsao et al, 1991;Eccles et al, 1992;Milner et al, 1993), the HER2/neu oncogene at 17q12 (Slamon et al, 1989), the BRCA1 breast-ovarian cancer susceptibility gene at 17q12 (Miki et al, 1994;Merajver et al, 1995), and the NME1 tumor metastasis marker on 17q21-23 (Viel et al, 1995;Scambia et al, 1996;Schneider et al, 1996). Somatic mutations and increased expression of TP53 have been more often reported in high grade and later stage tumors (Berchuck et al, 1994;Kupryjanczyk et al, 1993).…”

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confidence: 99%

Allelotyping defines minimal imbalance at chromosomal region 17q25 in non-serous epithelial ovarian cancers

et al. 2000

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Allelic deletions of multiple chromosome 17q loci in sporadic ovarian cancer of epithelial origin suggest that inactivation of tumor suppressor gene(s) in these regions may be important for ovarian tumorigenesis. To further de®ne the pattern of allelic imbalance in epithelial ovarian tumors of di erent histologies, a PCR-based assay was used to assess loss of heterozygosity (LOH) of polymorphic markers representative of TP53, BRCA1, NME1 and GH1, and region 17q23-25. LOH was observed for at least one marker in 68% of malignant tumors (n=60) and in 18% tumors of borderline malignancy (n=11), but not in benign tumors (n=5). The highest frequency of LOH in malignant tumors (64%) was observed with D17S801 on 17q25. Ten of 39 malignant ovarian tumors displaying LOH of at least one 17q marker, displayed a LOH pattern enabling the determination of a minimal region of overlapping deletion de®ned by D17S795 and D17S801. One borderline tumor also displayed an interstitial LOH pattern that overlapped this 17q25 minimal region of deletion. The histologies of malignant tumors displaying a pattern indicative of interstitial 17q deletions were of the endometrioid, clear cell and mucinous epithelial types. As the minimal region of overlap de®ned by these tumors overlap regions deleted in malignant tumors of all histologic types, and in a tumor of borderline malignancy, the 17q25-tumor suppressor may be implicated in the development of all types of epithelial ovarian tumors.

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“…The TP53 tumor-suppressor gene (TSG) at 17p13.1 is one of the most frequently mutated genes in EOC (Okamoto et al, 1991). However, LOH analysis suggests the location of novel TSGs on the short arm of chromosome 17 at or close to the TP53 locus (Okamoto et al, 1991;Tsao et al, 1991;Eccles et al, 1992;Cliby et al, 1993;Foulkes et al, 1993;Yang-Feng et al, 1993) and at a more telomeric region, 17p13.3 (Phillips et al, 1993;Konishi et al, 1998;Phelan et al, 1998;Hoff et al, 2000). A number of genes on the long arm of chromosome 17 also have been shown to be implicated in EOC: the ERBB2 oncogene at 17q21.1 (Slamon et al, 1989), the hereditary breast/ ovarian cancer TSG BRCA1 at 17q21.1 (Miki et al, 1994;Merajver et al, 1995) and the NME1 tumor metastasis marker gene at 17q21.3 (Mandai et al, 1994;Leary et al, 1995;Schneider et al, 1996Schneider et al, , 2000.…”

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confidence: 99%

Patterns of expression of chromosome 17 genes in primary cultures of normal ovarian surface epithelia and epithelial ovarian cancer cell lines

Presneau

Mes-Masson

et al. 2003

Oncogene

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Overexpression of the p53 protein and allele loss at 17p13 in ovarian carcinoma

Cited by 92 publications

References 25 publications

Potentially important microRNA cluster on chromosome 17p13.1 in primary peritoneal carcinoma

Potentially important microRNA cluster on chromosome 17p13.1 in primary peritoneal carcinoma

Allelotyping defines minimal imbalance at chromosomal region 17q25 in non-serous epithelial ovarian cancers

Patterns of expression of chromosome 17 genes in primary cultures of normal ovarian surface epithelia and epithelial ovarian cancer cell lines

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