Your search keyword '"Patricia N. Tonin"' showing total 211 results

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

Author

D. Provencher, F. Dion, R. J. Seymour, Patricia N. Tonin, and Anne Marie Mes-Masson

Subjects

Genetic Markers, Cancer Research, endocrine system diseases, Loss of Heterozygosity, Biology, Cystadenocarcinoma, Mucinous, medicine.disease_cause, Bioinformatics, Loss of heterozygosity, Tumor Cells, Cultured, Genetics, medicine, Carcinoma, Humans, Molecular Biology, Alleles, Neoplasm Staging, Ovarian Neoplasms, Cancer, Cell Differentiation, medicine.disease, Cystadenocarcinoma, Serous, Serous fluid, Chromosomal region, Cancer research, Female, Ovarian cancer, Carcinogenesis, Carcinoma, Endometrioid, Clear cell, Chromosomes, Human, Pair 17

Abstract

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 define the pattern of allelic imbalance in epithelial ovarian tumors of different 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 defined 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 defined 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.

Published

2000

102. Founder BRCA1 and BRCA2 mutations in French Canadian ovarian cancer cases unselected for family history

Author

Diane Provencher, Anne-Marie Mes-Masson, Patricia N. Tonin, Parviz Ghadirian, and Steven A. Narod

Subjects

Oncology, medicine.medical_specialty, Mutation, endocrine system diseases, Ovary, Biology, BRCA2 Protein, medicine.disease_cause, medicine.disease, female genital diseases and pregnancy complications, medicine.anatomical_structure, Germline mutation, Breast cancer, Internal medicine, Genetics, medicine, Cancer research, Family history, skin and connective tissue diseases, Ovarian cancer, Genetics (clinical), Founder effect

Abstract

The breast cancer susceptibility genes, BRCA1 and BRCA2, differ in their contribution to ovarian cancer. Recently, founder mutations in each of these genes were identified in Canadian breast cancer and breast ovarian cancer families of French ancestry. We have examined the prevalence of the founder mutations in a series of 113 French Canadian women with ovarian cancer unselected for family history. Germline mutations were found in eight of 99 invasive carcinomas and in none of the 14 tumors of borderline malignancy. Five cases carried the BRCA1 C4446T mutation and two cases carried the BRCA2 8765delAG mutation which are the most common mutations that have been described in French Canadian breast cancer and breast ovarian cancer families. All of these cases reported a family history of at least one first-degree relative with breast cancer, diagnosed below age 60 years, or with ovarian cancer. The identification of founder BRCA1 and BRCA2 mutations in ovarian cancer cases unselected for family history can facilitate carrier detection when the expected yield of a comprehensive screen may be low.

Published

1999

103. Expression of FHIT in primary cultures of human epithelial ovarian tumors and malignant ovarian ascites

Author

Anne-Marie Mes-Masson, Andrew P. Manning, Patricia N. Tonin, Melanie Tetrault, Diane Provencher, and Robert J. Seymour

Subjects

Cancer Research, Biology, medicine.disease, medicine.disease_cause, Loss of heterozygosity, Chromosome 3, FHIT, Cell culture, medicine, Cancer research, Northern blot, Ovarian cancer, Carcinogenesis, neoplasms, Molecular Biology, Immortalised cell line

Abstract

Abnormal FHIT gene expression has been reported in a variety of epithelial tumors shown to harbor deletions of chromosome 3p14, the chromosomal assignment of this gene. Recently, we described loss of heterozygosity of 3p in a subset of epithelial ovarian cancers. To investigate a potential role of the FHIT gene in ovarian cancer, we examined primary cell cultures derived from normal ovarian surface epithelium, ovarian tumors, and the cellular fraction of malignant ascites to determine the expression of FHIT by using reverse transcription-polymerase chain reaction. Included in this analysis were four spontaneously immortalized cell lines: three derived from malignant epithelial ovarian tumors (TOV21G, TOV112D, and TOV81D) and one from malignant ovarian ascites (OV90). OV90 was previously shown to harbor a deletion of the whole p arm of chromosome 3. The FHIT transcript was not detectable in two of 11 primary cultures derived from normal ovarian surface epithelium or in a primary culture derived from malignant ovarian ascites, whereas the remaining samples (34 malignant, eight borderline, and three benign specimens), exhibited identical expression patterns. In each case, this pattern was consistent with the co-expression of a normal FHIT transcript and a smaller transcript. DNA sequencing revealed that the abnormal-sized message lacked exons 4-7 (inclusive), which were deleted at their exact intron-exon splice sites. The aberrant-sized transcript was detectable by Northern blot analysis. There was no concordance between FHIT expression and loss of heterozygosity at the FHIT locus. Northern blot analysis also revealed that FHIT was differentially expressed, and the spontaneously immortalized cell lines TOV21G and TOV112D showed the highest level of expression. Because the same reverse transcription-polymerase chain reaction expression pattern was observed in both normal and tumor-derived primary cell cultures, these results argue against a significant role for FHIT in epithelial ovarian tumorigenesis.

Published

1999

104. Founder BRCA1 and BRCA2 Mutations in French Canadian Breast and Ovarian Cancer Families

Author

Kenneth Morgan, P. Andrew Futreal, Steven A. Narod, Patricia N. Tonin, William D. Foulkes, David E. C. Cole, Anne-Marie Mes-Masson, Parviz Ghadirian, Diane Provencher, and Michelle Mahon

Subjects

Genetic Markers, Canada, endocrine system diseases, Genetic counseling, Genes, BRCA1, Breast Neoplasms, Biology, medicine.disease_cause, Polymerase Chain Reaction, Breast cancer, Ovarian cancer, medicine, Genetics, Humans, Point Mutation, Family, Genes, Tumor Suppressor, Genetics(clinical), skin and connective tissue diseases, Genetics (clinical), DNA Primers, Sequence Deletion, BRCA2 Protein, Ovarian Neoplasms, Mutation, BRCA1 Protein, Point mutation, Cancer, Neoplasms, Second Primary, Middle Aged, Founder effect, BRCA1, medicine.disease, BRCA2, Neoplasm Proteins, French Canadians, Female, France, Research Article, Transcription Factors

Abstract

SummaryWe have identified four mutations in each of the breast cancer–susceptibility genes, BRCA1 and BRCA2, in French Canadian breast cancer and breast/ovarian cancer families from Quebec. To identify founder effects, we examined independently ascertained French Canadian cancer families for the distribution of these eight mutations. Mutations were found in 41 of 97 families. Six of eight mutations were observed at least twice. The BRCA1 C4446T mutation was the most common mutation found, followed by the BRCA2 8765delAG mutation. Together, these mutations were found in 28 of 41 families identified to have a mutation. The odds of detection of any of the four BRCA1 mutations was 18.7× greater if one or more cases of ovarian cancer were also present in the family. The odds of detection of any of the four BRCA2 mutations was 5.3× greater if there were at least five cases of breast cancer in the family. Interestingly, the presence of a breast cancer case

Published

1998

105. A high proportion of mutations in the BRCA1 gene in German breast/ovarian cancer families with clustering of mutations in the 3′ third of the gene

Author

Jenny Chang-Claude, Yixin Wu, Juan Dong, Irmgard Debatin, Patricia N. Tonin, Valérie Schumacher, and B. Royer-Pokora

Subjects

Male, Breast Neoplasms, Biology, medicine.disease_cause, Frameshift mutation, Breast cancer, Germany, Genotype, Genetics, medicine, Humans, Missense mutation, skin and connective tissue diseases, Genetics (clinical), Ovarian Neoplasms, Mutation, Polymorphism, Genetic, BRCA1 Protein, Haplotype, Single-strand conformation polymorphism, Middle Aged, medicine.disease, Pedigree, Multigene Family, Female, Ovarian cancer

Abstract

We have analyzed 61 German breast and breast/ovarian cancer families for BRCA1 mutations using single-strand conformation polymorphism analysis (SSCP) followed by sequencing. Forty-seven of the families had at least three cases (at least two under 60 years) and 14 families had only two cases of breast/ovarian cancer (at least one under 50 years). Twenty-eight families were breast/ovarian and 33 were breast cancer-only families. Eighteen mutations in BRCA1 were detected in 11/28 breast/ovarian cancer families and 7/33 breast cancer families and none in the families with only two cases. We identified 17 truncation mutations (8 frameshift, 7 nonsense and 2 splice variants) and one missense mutation. Seven of these are novel and two, the 5382insC and 5622C--T mutations, occurred in two apparently unrelated families. The genotype of the two families with the 5382insC mutation is compatible with the rare haplotype segregating with the 5382insC mutation in different populations, further supporting its European origin. One unclassified missense alteration, R841W, was found in one family but did not segregate with the disease, suggesting that it is more likely a polymorphism. We also report and discuss the sequence of several new unclassified single-nucleotide changes first identified by SSCP. Of the 18 mutations, 13 occurred in the 3' third of the gene (end of exon 11-24) and ovarian cancers were found in eight of these families.

Published

1998

106. Risk factors for familial and sporadic ovarian cancer among French Canadians: A case-control study

Author

Diane Provencher, Anne-Marie Mes-Masson, Patricia N. Tonin, William D. Foulkes, Steven A. Narod, Béatrice Godard, Parviz Ghadirian, and Jean-Sébastien Brunet

Subjects

Adult, Male, medicine.medical_specialty, Sterilization, Tubal, Ovary, Logistic regression, Risk Factors, Epidemiology, medicine, Humans, Childbirth, Risk factor, Family history, Aged, Aged, 80 and over, Ovarian Neoplasms, Gynecology, Ethanol, Obstetrics, business.industry, Case-control study, Obstetrics and Gynecology, Middle Aged, medicine.disease, medicine.anatomical_structure, Talc, Case-Control Studies, Multivariate Analysis, Female, Ovarian cancer, business, Contraceptives, Oral

Abstract

OBJECTIVE: The objective was to compare risk factors between familial and sporadic ovarian cancer by means of a case-control approach. STUDY DESIGN: We conducted a case-control study among French Canadian women in Montreal during 1995-1996. One hundred seventy women 20 to 84 years old with histologically confirmed diagnoses of primary ovarian carcinomas or borderline tumors were interviewed concerning their reproductive, family, and medical histories. During the same period 170 randomly selected population control subjects, frequency-matched to the case patients according to age and ethnic group, were also interviewed. Unconditional logistic regression methods were used for data analysis. RESULTS: The major factors influencing the risk of development of ovarian cancer were as follows: (1) family history of breast or ovarian cancer, (2) a late age at use of oral contraceptives (a protective effect), and (3) a late age at last childbirth (a protective effect for familial case patients only). CONCLUSION: These factors had equally great impacts in familial and sporadic cases, implying that the underlying mechanisms of carcinogenesis in sporadic and familial ovarian cancer may be similar and that hereditary ovarian cancer may be preventable. (Am J Obstet Gynecol 1998;179:403-10.)

Published

1998

107. Genetic Heterogeneity and Penetrance Analysis of the BRCA1 and BRCA2 Genes in Breast Cancer Families

Author

J.M. Birch, Siegfried Scherneck, Y. J. Bignon, Hagay Sobol, Åke Borg, Henry T. Lynch, Jenny Chang-Claude, Bruce A.J. Ponder, Patricia N. Tonin, Michael R. Stratton, Barbara L. Weber, David E. Goldgar, Neva E. Haites, D Ford, M D Teare, Steven A. Narod, Jeffery P. Struewing, Dominique Stoppa-Lyonnet, Adalgeir Arason, Susanne Seitz, Jorunn E. Eyfjord, Rosa B. Barkardottir, Rodney J. Scott, U Hamann, Timothy R. Rebbeck, Annika Lindblom, Julian Peto, Hans F. A. Vasen, Susan L. Neuhausen, Simon A. Gayther, Lisa A. Cannon-Albright, Andrew Craig Schofield, Douglas F. Easton, D. T. Bishop, Christine Maugard, Peter Devilee, Gilbert M. Lenoir, and Moraima Zelada-Hedman

Subjects

medicine.medical_specialty, Cancer, breast, endocrine system diseases, Biology, Lower risk, 03 medical and health sciences, Breast cancer, 0302 clinical medicine, Ovarian cancer, Internal medicine, Genetics, medicine, Genetics(clinical), Risk factor, skin and connective tissue diseases, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Hereditary breast–ovarian cancer syndrome, BRCA mutation, Cancer, BRCA1, medicine.disease, BRCA2, Penetrance, 3. Good health, Mutation analysis, Endocrinology, 030220 oncology & carcinogenesis, Cancer, ovarian, Breast Cancer Genetics, Linkage analysis

Abstract

SummaryThe contribution of BRCA1 and BRCA2 to inherited breast cancer was assessed by linkage and mutation analysis in 237 families, each with at least four cases of breast cancer, collected by the Breast Cancer Linkage Consortium. Families were included without regard to the occurrence of ovarian or other cancers. Overall, disease was linked to BRCA1 in an estimated 52% of families, to BRCA2 in 32% of families, and to neither gene in 16% (95% confidence interval [CI] 6%–28%), suggesting other predisposition genes. The majority (81%) of the breast-ovarian cancer families were due to BRCA1, with most others (14%) due to BRCA2. Conversely, the majority of families with male and female breast cancer were due to BRCA2 (76%). The largest proportion (67%) of families due to other genes was found in families with four or five cases of female breast cancer only. These estimates were not substantially affected either by changing the assumed penetrance model for BRCA1 or by including or excluding BRCA1 mutation data. Among those families with disease due to BRCA1 that were tested by one of the standard screening methods, mutations were detected in the coding sequence or splice sites in an estimated 63% (95% CI 51%–77%). The estimated sensitivity was identical for direct sequencing and other techniques. The penetrance of BRCA2 was estimated by maximizing the LOD score in BRCA2-mutation families, over all possible penetrance functions. The estimated cumulative risk of breast cancer reached 28% (95% CI 9%–44%) by age 50 years and 84% (95% CI 43%–95%) by age 70 years. The corresponding ovarian cancer risks were 0.4% (95% CI 0%–1%) by age 50 years and 27% (95% CI 0%–47%) by age 70 years. The lifetime risk of breast cancer appears similar to the risk in BRCA1 carriers, but there was some suggestion of a lower risk in BRCA2 carriers

Published

1998

108. Is hereditary site-specific ovarian cancer a distinct genetic condition?

Author

William D. Foulkes, Alexander Liede, Mary B. Daly, Corinne Serruya, Steven A. Narod, Chia Chia Sun, and Patricia N. Tonin

Subjects

Genetics, Oncology, endocrine system, medicine.medical_specialty, endocrine system diseases, Genetic counseling, Haplotype, Biology, medicine.disease, female genital diseases and pregnancy complications, Genetic determinism, Cancer syndrome, Breast cancer, Ovarian carcinoma, Internal medicine, Carcinoma, medicine, skin and connective tissue diseases, Ovarian cancer, Genetics (clinical)

Abstract

It is not clear if hereditary site-specific ovarian cancer exists as a genetic entity distinct from the hereditary breast-ovarian cancer syndrome. We have identified a large Ashkenazi Jewish kindred with 8 cases of ovarian carcinoma and no cases of breast cancer. Initially, linkage analysis for this kindred generated a negative LOD score to BRCA1, but subsequent mutation and haplotype analysis of key individuals demonstrated a BRCA1 185delAG mutation segregating with all but 1 of the ovarian cancer cases. This observation has important implications for genetic counselling of families with site-specific ovarian cancer. Hereditary site-specific ovarian cancer is likely to be a variant of the hereditary breast-ovarian cancer syndrome, attributable to either BRCA1 or BRCA2. We consider women from these families to be at increased risk of breast cancer and counsel them accordingly.

Published

1998

109. The familial Wilms' tumour susceptibility gene, FWT1, may not be a tumour suppressor gene

Author

Laura Arbour, Michael R. Stratton, Patricia N. Tonin, Steven A. Narod, Sylvain Baruchel, Kathryn Pritchard-Jones, and Nazneen Rahman

Subjects

Genetic Markers, Heterozygote, Cancer Research, Genes, Wilms Tumor, Tumor suppressor gene, Biology, medicine.disease_cause, Polymerase Chain Reaction, Wilms Tumor, Loss of heterozygosity, Genetics, medicine, Humans, Genes, Tumor Suppressor, Genetic Predisposition to Disease, Allele, Molecular Biology, Gene, Alleles, Mutation, Chromosomes, Human, Pair 11, Wilms' tumor, medicine.disease, Genetic marker, Carcinogenesis

Abstract

A familial Wilms' tumour susceptibility gene, known as FWT1, has recently been localised to chromosome 17q12-q21 by genetic linkage analysis. Four Wilms' tumours from a family showing strong evidence of linkage to FWT1 were examined for allele loss using polymorphic microsatellite markers on chromosome 17q. In three tumours no loss of heterozygosity was observed. In the remaining case, loss of heterozygosity was detected at all markers analysed. However, the alleles lost in this Wilms' tumour were those segregating with the disease in the family. This is in contrast to the usual pattern observed in familial cancer syndromes, where the allele lost in tumours arising in gene carriers is the wild type inherited from the non mutation carrying parent. Taken together with previous data indicating that LOH on chromosome 17q is rare in sporadic Wilms' tumour, the results suggest that FWT1 is not a tumour suppressor gene. Moreover, loss of alleles linked to the disease and the implied absence of the mutated susceptibility gene in one tumour, suggests that a mutation in FWT1 may be necessary for the initiation of some familial Wilms' tumours but subsequently the maintenance of the neoplastic phenotype becomes independent of the FWT1 mutation.

Published

1997

110. A descriptive study of BRCA1 testing and reactions to disclosure of test results

Author

Stephen J. Lemon, Jonathan Surdam, Patrice Watson, Jane F. Lynch, Carolyn Durham, Olga Serova, Sue Slominski-Caster, Patricia N. Tonin, Caryn Lerman, Christopher J. Connolly, Susan T. Tinley, Ernest Orinion, Gilbert M. Lenoir, Steven A. Narod, and Henry T. Lynch

Subjects

Gynecology, Cancer Research, medicine.medical_specialty, medicine.diagnostic_test, business.industry, Genetic counseling, media_common.quotation_subject, Context (language use), Prophylactic Mastectomy, Anger, Gene mutation, Prophylactic Oophorectomy, Oncology, Informed consent, medicine, business, Genetic testing, media_common, Clinical psychology

Abstract

BACKGROUND The identification of the BRCA1 gene is a powerful tool for predicting a patient's lifetime risk for carcinoma of the breast and ovary when she has hereditary breast/ovarian carcinoma (HBOC) syndrome. The process of BRCA1 testing and genetic counseling, and participants' reactions to test results, are described. METHODS Education about the natural history of HBOC syndrome and the pros and cons of genetic testing was provided to 14 HBOC families comprised of 2549 bloodline relatives. Of these, 388 underwent DNA testing. After informed consent was given by participants, formal linkage analysis and gene mutation studies were performed on the families. Qualitative data on intentions and emotional reactions were collected by physicians/counselors during the genetic counseling sessions. RESULTS Of those tested, 181 received their results after further genetic counseling. Seventy-eight of them were positive and 100 were negative for BRCA1 gene mutation. Three had ambiguous findings. The most common reasons given for seeking DNA testing were concern about risk to children and concern about surveillance and prevention. Prophylactic mastectomy was considered by 35% of women who tested positive, whereas prophylactic oophorectomy was considered an important option by 76%. Twenty-five percent of both BRCA1 positive and negative individuals were concerned about discrimination by insurance companies. Eighty percent of those who tested negative reported emotional relief, whereas over one-third of those who tested positive reported sadness, anger, or guilt. CONCLUSIONS DNA testing of patients with HBOC syndrome must be performed in the context of genetic counseling. The authors' results demonstrate the many complex clinical and nonclinical issues that are important in this process. [See editorial counterpoint on pages 2063-5 and reply to counterpoint on pages , this issue.] Cancer 1997; 79:2219-28. © 1997 American Cancer Society.

Published

1997

111. Contribution of the PALB2 c.2323C>T [p.Q775X] Founder mutation in well-defined breast and/or ovarian cancer families and unselected ovarian cancer cases of French Canadian descent

Author

Anne-Marie Mes-Masson, Patricia N. Tonin, William D. Foulkes, Marc Tischkowitz, Nancy Hamel, Nelly Sabbaghian, Diane Provencher, Carly Pouchet, Tischkowitz, Marc [0000-0002-7880-0628], and Apollo - University of Cambridge Repository

Subjects

Oncology, endocrine system diseases, p.Q775, Genes, BRCA2, Genes, BRCA1, Genetics(clinical), skin and connective tissue diseases, Genetics (clinical), Hereditary breast cancer, Genetics, Ovarian Neoplasms, education.field_of_study, Nuclear Proteins, Middle Aged, Founder Effect, Pedigree, Serous fluid, Female, Fanconi Anemia Complementation Group N Protein, Research Article, Adult, medicine.medical_specialty, Canada, Heterozygote, lcsh:Internal medicine, lcsh:QH426-470, PALB2, Population, Breast Neoplasms, Founder mutations, Biology, White People, Breast cancer, Germline mutation, Ovarian cancer, Internal medicine, medicine, p.Q775X, Humans, Family, Genetic Predisposition to Disease, education, lcsh:RC31-1245, Germ-Line Mutation, Aged, Base Sequence, Tumor Suppressor Proteins, Cytogenetics, medicine.disease, lcsh:Genetics, French Canadians, Breast cancer risk, Founder effect

Abstract

Background The PALB2 c.2323C>T [p.Q775X] mutation has been reported in at least three breast cancer families and breast cancer cases of French Canadian descent and this has been attributed to common ancestors. The number of mutation-positive cases reported varied based on criteria of ascertainment of index cases tested. Although inherited PALB2 mutations are associated with increased risks of developing breast cancer, risk to ovarian cancer has not been fully explored in this demographically unique population. Methods We screened the PALB2 p.Q775X variant in 71 families with at least three cases of breast cancer (n=48) or breast and ovarian cancers (n=23) that have previously been found negative for at least the most common BRCA1 and BRCA2 mutations reported in the French Canadian population and in 491 women of French Canadian descent who had invasive ovarian cancer and/or low malignant potential tumors of the major histopathological subtypes. Results We identified a PALB2 p.Q775X carrier in a breast cancer family, who had invasive ductal breast carcinomas at 39 and 42 years of age. We also identified a PALB2 p.Q775X carrier who had papillary serous ovarian cystadenocarcinoma at age 58 among the 238 serous subtype ovarian cancer cases investigated, who also had breast cancer at age 52. Conclusion Our findings, taken together with previous reports, support adding PALB2 c.2323C>T p.Q775X to the list of cancer susceptibility genes for which founder mutations have been identified in the French Canadian population.

Published

2013

112. The Human Mammary-Derived Growth Inhibitor (MDGI) Gene: Genomic Structure and Mutation Analysis in Human Breast Tumors

Author

Kenneth Morgan, P. Andrew Futreal, Catherine M. Phelan, M.H. Ruttledge, Stephen Baird, Huynh Hung, Michael Pollak, Catharina Larsson, Patricia N. Tonin, Steven A. Narod, and Robert G. Korneluk

Subjects

Genetic Markers, Heterozygote, Tumor suppressor gene, Molecular Sequence Data, Breast Neoplasms, DNA, Satellite, Gene mutation, Biology, Fatty Acid-Binding Proteins, medicine.disease_cause, Loss of heterozygosity, Exon, Gene mapping, Genetics, medicine, Humans, Genes, Tumor Suppressor, Cloning, Molecular, Regulation of gene expression, Polymorphism, Genetic, Base Sequence, Exons, Middle Aged, Candidate Tumor Suppressor Gene, Molecular biology, Introns, Chromosomes, Human, Pair 1, Mutation, Cancer research, Female, Carrier Proteins, Carcinogenesis, Fatty Acid Binding Protein 3

Abstract

The mammary-derived growth inhibitor (MDGI) gene is a candidate tumor suppressor gene for human breast cancer. It has been shown to reduce the tumorigenicity of breast cancer cell lines in nude mice, and loss of expression of this gene has been shown in primary breast tumors. Furthermore, the human MDGI gene has been mapped to human chromosome 1p32-p35, a common region of deletion in sporadic breast tumors. We have determined the genomic structure of the human MDGI gene from a cosmid clone mapping to chromosome 1p32-p35 and have more finely mapped the MDGI gene relative to chromosome 1p microsatellite markers. The gene covers approximately 8 kb of genomic DNA and is divided into four exons. In an attempt to identify possible inactivating mutations in the MDGI gene in human breast cancer, we have sequenced all four exons and their surrounding splice junctions in 30 sporadic breast tumors. Ten of these tumors showed loss of heterozygosity (LOH) in the 1p32-p35 regions, with 5 tumors showing LOH in the subregion containing the MDGI gene. No mutations were found in this analysis. A polymorphism was identified in exon 2 in the constitutional DNA of 1/30 cases in this study, which resulted in themore » conversion of a lysine to an arginine residue at codon 53. This variant was present in the constitutional DNA of a further 3/26 women with sporadic breast cancer and 2/90 control individual (P=0.20). Despite experimental evidence that MDGI has tumor suppressor activity, our data suggest that mutations in the coding region are uncommon in human breast tumorigenesis. 29 refs., 3 figs., 2 tabs.« less

Published

1996

113. High allele loss rates at I7q I2-q2I in breast and ovarian tumors fromBRCAI-linked families

Author

Rosa B. Barkardottir, R.S. Cornelis, Åke Borg, Patricia N. Tonin, Siegfried Scherneck, Susan L. Neuhausen, Catharina Larsson, Michel Longy, Adalgeir Arason, Annika Lindblom, Philippe Lalle, Jenny Chang-Claude, O. Johansson, Bruce A.J. Ponder, Hagay Sobol, Edith Olah, Ute Hamann, Nigel K. Spurr, Peter Devilee, Yves-Jean Bignon, Steven A. Narod, and David P. Kelsell

Subjects

Genetics, Cancer Research, Tumor suppressor gene, Haplotype, Biology, medicine.disease, Loss of heterozygosity, Breast cancer, Genetic linkage, Genotype, medicine, Cancer research, Allele, Ovarian cancer

Abstract

Loss of heterozygosity (LOH) was evaluated in 174 breast and ovarian tumors derived from 94 families with at least 3 first-degree relatives affected with either of these cancers. By linkage analysis 26 families were identified as having a high posterior probability of being due to BRCAl (the breast/ovarian cancer susceptibility locus on 17q12-21) with lod scores varying from 0.51 to 9.49. Tumor genotypes were determined at at least 2 constitutionally heterozygous markers flanking BRCAl in a total of 58 tumors from these families. These tumors were derived from 52 patients, the BRCAl mutation carrier status of which was evidenced by DNA sequencing in 20, and inferred by reconstructing haplotypes in the remainder. LOH was detected in 50 (86%) tumors, and invariably involved the wild-type allele. Where informative, this allele was of paternal origin in 33 cases and of maternal origin in 10 cases. These results strongly suggest that BRCAl is a tumor suppressor gene and that LOH is greatly favored to fully inactivate it.

Published

1995

114. Abstract B54: Single and collective cell dissemination modes in ovarian cancer

Author

Patricia N. Tonin, Sara Al-Habyan, Joseph Szymborski, and Luke McCaffrey

Subjects

Cancer Research, Pathology, medicine.medical_specialty, Cell, Biology, medicine.disease, Malignancy, Metastasis, Peritoneal cavity, medicine.anatomical_structure, Lymphatic system, Oncology, Live cell imaging, Ascites, medicine, Cancer research, medicine.symptom, Ovarian cancer

Abstract

Background: Ovarian cancer (OvCa) results in over 114,000 worldwide deaths annually, and is the most lethal malignancy of the female reproductive system. During its progression, OvCa can shed cells into the peritoneal cavity, which can later metastasize to distant pelvic, abdominal, or extra-peritoneal organs. Disordered tumor blood vessels often allow for lymphatic leakage into the abdomen, causing an accumulation of excess ascites fluid that is abundant in growth factors supporting the survival and growth of disseminated tumour cells (DTCs). DTCs were found to exist in ascites both as single cells and as multicellular spheroids, however it is unknown whether cells disseminate in a single or collective manner. Biological and clinical characteristics of DTC spheroids have been under investigation in a number of cancer subtypes, as cells within spheroids exhibit enhanced resistance to multiple chemotherapeutics, increased invasive properties, and faster tumorigenic potential. Therefore, understanding and targeting cancer spheroids can help improve patient prognosis and limit disease progression. Methods: In this study, we examine the modes of dissemination of ovarian cancer cells as single or multi-cellular units using Ov-90 chemo naïve cells and OVCAR-3 cells, which were each derived from human ascites. We utilize in-vitro 2D monolayer cultures and 3D ‘organoids' to characterize the dissemination of cells in suspension for cellular viability, and protein expression and localization. Live imaging is conducted on free-floating, hanging drop generated clusters to visualize dissemination. To confirm in-vitro experiments, ovarian orthotopic transplants in mice are used as an in-vivo system by injecting fluorescently labelled cells. Results: Our novel live imaging models showed that cells disseminate as both single cells and groups of cells. Disseminated cells in culture are frequently observed as cell clusters with a higher live/dead ratio than cells seeded at single cells in suspension, indicating that clusters may have a survival advantage. In addition, immunofluorescence staining of disseminated cells suggests that the transcription factor Zeb1 may be involved in driving cell dissemination by regulating mosaic E-cadherin expression in the absence of complete EMT. Conclusion: Ovarian cancer cells can disseminate as either single cells or clusters. Many gaps in our understanding exist in the early stages of dissemination of ovarian cancer despite intensive research throughout the later time points in metastasis. We predict that a deeper understanding of the mechanisms of dissemination will provide insights to greatly improve patient prognosis and response to chemotherapeutics. Citation Format: Sara Al-Habyan, Joseph Szymborski, Patricia Tonin, Luke McCaffrey. Single and collective cell dissemination modes in ovarian cancer. [abstract]. In: Proceedings of the AACR Special Conference on Advances in Ovarian Cancer Research: Exploiting Vulnerabilities; Oct 17-20, 2015; Orlando, FL. Philadelphia (PA): AACR; Clin Cancer Res 2016;22(2 Suppl):Abstract nr B54.

Published

2016

115. Small cell ovarian carcinoma: genomic stability and responsiveness to therapeutics

Author

Christopher Davis, Jeremy A. Squire, Karen Gambaro, Lisa F Gamwell, Valerie Bourada, Maria Merziotis, Barbara C. Vanderhyden, Patricia N. Tonin, Colleen Crane, Suzanna L. Arcand, and David G. Huntsman

Subjects

Somatic cell, Antineoplastic Agents, Biology, medicine.disease_cause, Polymorphism, Single Nucleotide, Genomic Instability, Loss of heterozygosity, 03 medical and health sciences, Mice, 0302 clinical medicine, Ovarian carcinoma, medicine, Animals, Humans, Small cell ovarian cancer, Genetics(clinical), Pharmacology (medical), Carcinoma, Small Cell, Genomic anomalies, Genetics (clinical), 030304 developmental biology, Medicine(all), Chromosome Aberrations, Oncolytic Virotherapy, Ovarian Neoplasms, 0303 health sciences, Gene Expression Profiling, Research, General Medicine, medicine.disease, Molecular biology, Xenograft Model Antitumor Assays, Immunohistochemistry, 3. Good health, Oncolytic virus, BIN-67, 030220 oncology & carcinogenesis, Karyotyping, Mutation, Female, KRAS, Chromosome 20, Ovarian cancer, Cell line, SNP array

Abstract

Background The biology of small cell ovarian carcinoma of the hypercalcemic type (SCCOHT), which is a rare and aggressive form of ovarian cancer, is poorly understood. Tumourigenicity, in vitro growth characteristics, genetic and genomic anomalies, and sensitivity to standard and novel chemotherapeutic treatments were investigated in the unique SCCOHT cell line, BIN-67, to provide further insight in the biology of this rare type of ovarian cancer. Method The tumourigenic potential of BIN-67 cells was determined and the tumours formed in a xenograft model was compared to human SCCOHT. DNA sequencing, spectral karyotyping and high density SNP array analysis was performed. The sensitivity of the BIN-67 cells to standard chemotherapeutic agents and to vesicular stomatitis virus (VSV) and the JX-594 vaccinia virus was tested. Results BIN-67 cells were capable of forming spheroids in hanging drop cultures. When xenografted into immunodeficient mice, BIN-67 cells developed into tumours that reflected the hypercalcemia and histology of human SCCOHT, notably intense expression of WT-1 and vimentin, and lack of expression of inhibin. Somatic mutations in TP53 and the most common activating mutations in KRAS and BRAF were not found in BIN-67 cells by DNA sequencing. Spectral karyotyping revealed a largely normal diploid karyotype (in greater than 95% of cells) with a visibly shorter chromosome 20 contig. High density SNP array analysis also revealed few genomic anomalies in BIN-67 cells, which included loss of heterozygosity of an estimated 16.7 Mb interval on chromosome 20. SNP array analyses of four SCCOHT samples also indicated a low frequency of genomic anomalies in the majority of cases. Although resistant to platinum chemotherapeutic drugs, BIN-67 cell viability in vitro was reduced by >75% after infection with oncolytic viruses. Conclusions These results show that SCCOHT differs from high-grade serous carcinomas by exhibiting few chromosomal anomalies and lacking TP53 mutations. Although BIN-67 cells are resistant to standard chemotherapeutic agents, their sensitivity to oncolytic viruses suggests that their therapeutic use in SCCOHT should be considered.

Published

2012

116. FKBP10/FKBP65 expression in high-grade ovarian serous carcinoma and its association with patient outcome

Author

Michael C.J. Quinn, Patricia N. Tonin, Anne-Marie Mes-Masson, Paulina M. Wojnarowicz, Diane Provencher, Elaine C. Davis, and Amy E. Pickett

Subjects

Cancer Research, Stromal cell, Survival, Gene Expression, Biology, Carcinoma, Ovarian Epithelial, Collagen Type I, Tacrolimus Binding Proteins, Cell Line, Tumor, Humans, Neoplasms, Glandular and Epithelial, Ovarian Neoplasms, Tissue microarray, Gene Expression Profiling, Epithelial Cells, Cell cycle, Molecular medicine, Staining, Cystadenocarcinoma, Serous, Chromosome 17 (human), Collagen Type I, alpha 1 Chain, Serous fluid, Treatment Outcome, Oncology, Cancer research, Immunohistochemistry, Female, Chromosome Deletion, Smith-Magenis Syndrome, Tumor Suppressor Protein p53, Chromosomes, Human, Pair 17

Abstract

The frequent loss of chromosome 17 in epithelial ovarian carcinomas (EOC), particularly high-grade serous carcinomas (HGSC), has been attributed to the disruption of TP53 (at 17p13.1) and other chromosome 17 genes suspected to play a role in tumour suppressor pathways. In a transcriptome analysis of HGSC, we showed underexpression of a number of chromosome 17 genes, which included FKBP10 (at 17q21.1) and collagen I α 1 (COL1A1; at 17q21.33). FKBP10 codes for the immunophilin FKBP65 and is suspected to act as a chaperone for COL1A1. We have investigated FKBP10 (gene) and FKBP65 (protein) expression in HGSC samples and EOC cell lines that differ in their tumourigenic potential. COL1A1 expression was also investigated given the purported function of FKBP65. RT-PCR analysis verified underexpression of FKBP10 and COL1A1 in HGSCs (n=14) and six tumourigenic EOC cell lines, relative to normal ovarian surface epithelial cells and a non-tumourigenic EOC cell line. Immunohistochemistry analyses of 196 HGSC samples using tissue microarrays revealed variable staining intensities in the epithelial tumour component where only 7.8% and 1.0% of samples stained intensely for FKBP65 and COL1A1, respectively. Variable staining intensities were also observed for the stromal component where 23.6% and 24.1% stained intensely for FKBP65 and COL1A1, respectively. There was no significant correlation of staining intensity of either protein with disease stage. Staining of FKBP65 was clearly visible in normal epithelial cells of the ovarian surface and fallopian tube. There was a significant correlation between absence of FKBP65 staining in the epithelial cell component of the tumour and prolonged overall survival (p

Published

2012

117. Derivation and characterization of matched cell lines from primary and recurrent serous ovarian cancer

Author

Isabelle Létourneau, Anne-Marie Mes-Masson, Suzanna L. Arcand, Liliane Meunier, Nathalie Delvoye, Patricia N. Tonin, Diane Provencher, Lu-Lin Wang, Michael C.J. Quinn, Katia Caceres, Zhen Shen, Lise Portelance, Manon de Ladurantaye, and Louis Cyr

Subjects

Oncology, Cancer Research, endocrine system diseases, Mice, SCID, Deoxycytidine, Carboplatin, chemistry.chemical_compound, Mice, 0302 clinical medicine, Antineoplastic Combined Chemotherapy Protocols, Ovarian Neoplasms, 0303 health sciences, Ascites, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immunohistochemistry, Cell line model, 3. Good health, Serous fluid, 030220 oncology & carcinogenesis, Female, medicine.drug, Research Article, Adult, medicine.medical_specialty, Paclitaxel, Blotting, Western, lcsh:RC254-282, 03 medical and health sciences, Ovarian cancer, Internal medicine, Cell Line, Tumor, medicine, Genetics, Animals, Humans, Chemotherapy, Clonogenic assay, 030304 developmental biology, Aged, Cisplatin, Cell growth, business.industry, medicine.disease, Xenograft Model Antitumor Assays, Gemcitabine, Cystadenocarcinoma, Serous, chemistry, Doxorubicin, Topotecan, business

Abstract

Background Cell line models have proven to be effective tools to investigate a variety of ovarian cancer features. Due to the limited number of cell lines, particularly of the serous subtype, the heterogeneity of the disease, and the lack of cell lines that model disease progression, there is a need to further develop cell line resources available for research. This study describes nine cell lines derived from three ovarian cancer cases that were established at initial diagnosis and at subsequent relapse after chemotherapy. Methods The cell lines from three women diagnosed with high-grade serous ovarian cancer (1369, 2295 and 3133) were derived from solid tumor (TOV) and ascites (OV), at specific time points at diagnosis and relapse (R). Primary treatment was a combination of paclitaxel/carboplatin (1369, 3133), or cisplatin/topotecan (2295). Second line treatment included doxorubicin, gemcitabine and topotecan. In addition to molecular characterization (p53, HER2), the cell lines were characterized based on cell growth characteristics including spheroid growth, migration potential, and anchorage independence. The in vivo tumorigenicity potential of the cell lines was measured. Response to paclitaxel and carboplatin was assessed using a clonogenic assay. Results All cell lines had either a nonsense or missense TP53 mutations. The ability to form compact spheroids or aggregates was observed in six of nine cell lines. Limited ability for migration and anchorage independence was observed. The OV3133(R) cell line, formed tumors at subcutaneous sites in SCID mice. Based on IC50 values and dose response curves, there was clear evidence of acquired resistance to carboplatin for TOV2295(R) and OV2295(R2) cell lines. Conclusion The study identified nine new high-grade serous ovarian cancer cell lines, derived before and after chemotherapy that provides a unique resource for investigating the evolution of this common histopathological subtype of ovarian cancer.

Published

2012

118. Allelic transcripts dosage effect in morphologically normal ovarian cells from heterozygous carriers of a BRCA1/2 French Canadian founder mutation

Author

Enrique Escobar, Diala Abd-Rabbo, Anne-Marie Mes-Masson, Christine Maugard, Caroline Arous, Patricia N. Tonin, Sophie Cloutier, Guillaume B Cardin, Diane Provencher, Christine Abaji, Abdelali Filali-Mouhim, and Lise Portelance

Subjects

Adult, Cancer Research, Canada, Heterozygote, endocrine system diseases, DNA Mutational Analysis, Genes, BRCA2, Gene Dosage, Genes, BRCA1, Penetrance, Biology, Validation Studies as Topic, medicine.disease_cause, Transcriptome, Ovarian tumor, medicine, Humans, RNA, Messenger, Allele, skin and connective tissue diseases, Gene, Alleles, Cells, Cultured, Aged, Mutation, Ovary, Quebec, Heterozygote advantage, Middle Aged, Molecular biology, female genital diseases and pregnancy complications, Founder Effect, Oncology, Female, Founder effect

Abstract

We hypothesized that the transcriptome of primary cultures of morphologically normal ovarian surface epithelial cells could be altered by the presence of a heterozygous BRCA1 or BRCA2 mutation. We aimed to discover early events associated with ovarian carcinogenesis, which could represent putative targets for preventive strategies of this silent killer tumor. We identified the first molecular signature associated with French Canadian BRCA1 or BRCA2 founder mutations in morphologically normal ovarian epithelial cells. We discovered that wild-type and mutated BRCA2 allelic transcripts were expressed not only in morphologically normal but also in tumor cells from BRCA2-8765delAG carriers. Further analysis of morphologically normal ovarian and tumor cells from BRCA1-4446C>T carriers lead to the same observation. Our data support the idea that one single hit in BRCA1 or BRCA2 is sufficient to alter the transcriptome of phenotypically normal ovarian epithelial cells. The highest level of BRCA2-mutated allele transcript expression was measured in cells originating from the most aggressive ovarian tumor. The penetrance of the mutation and the aggressiveness of the related tumor could depend on a dosage effect of the mutated allele transcript. Cancer Prev Res; 5(5); 765–77. ©2012 AACR.

Published

2012

119. Common origins of BRCA1 mutations in Canadian breast and ovarian cancer families

Author

Donna M Shattuck-Eidens, Carole Bélanger, David E. Goldgar, J.-F. Leblanc, Patricia N. Tonin, Johanna M. Rommens, Steven A. Narod, Qingyun Liu, Francine Durocher, Sebastien Gingras, Mark H. Skolnick, Chantal Samson, F. Dion, Fernand Labrie, Kenneth Morgan, and Jacques Simard

Subjects

Male, Canada, Molecular Sequence Data, Breast Neoplasms, Biology, medicine.disease_cause, Frameshift mutation, Breast cancer, Genetics, medicine, Humans, Amino Acid Sequence, Insertion, Allele, Frameshift Mutation, DNA Primers, Ovarian Neoplasms, Mutation, Base Sequence, BRCA1 Protein, Haplotype, Chromosome, medicine.disease, Neoplasm Proteins, Pedigree, Haplotypes, Female, Ovarian cancer, Transcription Factors

Abstract

Women who carry mutations in the BRCA1 gene on chromosome 17q have an 85% lifetime risk of breast cancer, and a 60% risk of ovarian cancer. We have identified BRCA1 mutations in 12 of 30 (40%) Canadian families with breast and/or ovarian cancer, including six of the eight families (75%) that contained two cases of early-onset breast cancer and two cases of ovarian cancer. Six frameshift mutations account for all 12 mutant alleles, including nucleotide insertions (two mutations) and deletions (four mutations). Four independent families carried the same 1 basepair (bp) insertion mutation in codon 1755 and four other families shared a 2 bp deletion mutation in codons 22-23. These families were not known to be related, but haplotype analysis suggests that the carriers of each of these mutations have common ancestors.

Published

1994

120. Hereditary and familial ovarian cancer in southern ontario

Author

David E. C. Cole, Barry P. Rosen, Lisa Madlensky, Patricia N. Tonin, Harvey A. Risch, Steven A. Narod, and Linda Bradley

Subjects

Oncology, Cancer Research, medicine.medical_specialty, education.field_of_study, endocrine system diseases, business.industry, Genetic counseling, Population, Cancer, medicine.disease, Cancer syndrome, Breast cancer, Internal medicine, Epidemiology of cancer, medicine, Family history, Ovarian cancer, business, education

Abstract

Background. Hereditary ovarian cancer may be site specific or may appear in combination with breast cancer or other cancers in a family. The most common hereditary form is the breast-ovarian cancer syndrome. It is estimated that in 100% of these families, there is linkage to a cancer susceptibility gene on chromosome 17q, BRCAl. Methods. A positive family history of breast or ovarian cancer was reported for 71 of 450 unselected cases of ovarian cancer identified in Southern Ontario. Detailed pedigrees were completed by telephone interview for 48 of the 71 subjects. Results.Nine families were identified with five or more cases of breast or ovarian cancer, 14 families with four cases of cancer, and eight families with three cases. Breast cancer appeared in 80% of the ovarian cancer families. There were 81 healthy first-degree female relatives of the cancer cases considered to be at high risk for ovarian cancer. Conclusions. It is feasible to use a simple questionnaire on all incident cases of ovarian cancer in a population to identify families with potential hereditary breastovarian cancer. Two point nine percent to 6.9% of cases of ovarian cancer appear to be inherited; the majority of the families also will have an excess number of cases of breast cancer.

Published

1994

121. Chromosome 17q25 genes, RHBDF2 and CYGB, in ovarian cancer

Author

Anne-Marie Mes-Masson, Patricia N. Tonin, Diane Provencher, and Paulina M. Wojnarowicz

Subjects

Cancer Research, endocrine system diseases, Transcription, Genetic, Molecular Sequence Data, Mutation, Missense, Loss of Heterozygosity, Locus (genetics), Biology, Carcinoma, Ovarian Epithelial, medicine.disease_cause, Loss of heterozygosity, Cell Line, Tumor, medicine, Humans, Genes, Tumor Suppressor, Amino Acid Sequence, Neoplasms, Glandular and Epithelial, Promoter Regions, Genetic, Conserved Sequence, Genetic Association Studies, Sequence Deletion, Ovarian Neoplasms, Gene Expression Profiling, Cytoglobin, Sequence Analysis, DNA, DNA Methylation, medicine.disease, Globins, Gene expression profiling, Chromosome 17 (human), Gene Expression Regulation, Neoplastic, Oncology, DNA methylation, Cancer research, Female, Ovarian cancer, Carcinogenesis, Chromosomes, Human, Pair 17

Abstract

It has been proposed that the frequent loss of heterozygosity (LOH) of an entire chromosome 17 contig in epithelial ovarian cancers (EOC) is the consequence of the inactivation of multiple tumour suppressor genes on this chromosome. We report the characterization of a 453 Kb 17q25 locus shown previously to exhibit a high frequency of LOH in EOC samples. LOH analysis further defined the minimal region of deletion to a 65 Kb interval flanked by D17S2239 and D17S2244, which contains RHBDF2, CYGB and PRCD as tumour suppressor gene candidates. Tissue specific expression excluded PRCD as a candidate. RHBDF2 was expressed at low levels in the majority of benign and low malignant potential (LMP) tumours, and in a subset of malignant ovarian tumour samples, as compared with primary cultures of normal ovarian surface epithelial cell (NOSE) samples. CYGB was expressed at low levels in the majority of LMP and malignant samples compared with benign and NOSE samples. In contrast to CYGB expression, RHBDF2 was expressed at low or undetectable levels in EOC cell lines exhibiting tumourigenic characteristics and up-regulated in a genetically modified EOC cell line rendered non-tumourigenic. DNA sequence analysis identified variants but no apparent deleterious mutations in either gene. Methylation-specific PCR analysis suggested that promoter methylation of CYGB but not RHBDF2 occurred in 6 of 31 malignant samples. The results combined suggest that RHBDF2 and CYGB may play distinctive roles in ovarian cancer and could be added to the growing roster of chromosome 17 genes implicated in this disease.

Published

2011

122. The BRCA2 c.9004GA (E2002K) [corrected] variant is likely pathogenic and recurs in breast and/or ovarian cancer families of French Canadian descent

Author

Stephanie, Cote, Suzanna L, Arcand, Robert, Royer, Serge, Nolet, Anne-Marie, Mes-Masson, Parviz, Ghadirian, William D, Foulkes, Marc, Tischkowitz, Steven A, Narod, Diane, Provencher, and Patricia N, Tonin

Subjects

Adult, Aged, 80 and over, BRCA2 Protein, Ovarian Neoplasms, Canada, DNA Mutational Analysis, Breast Neoplasms, Middle Aged, Polymorphism, Single Nucleotide, Founder Effect, White People, Pedigree, Amino Acid Substitution, Humans, Female, Genetic Predisposition to Disease, Breast, Sequence Alignment, Germ-Line Mutation, Aged

Abstract

Specific BRCA1 and BRCA2 mutations recur in French Canadian breast and/or ovarian cancer families because of common ancestors, facilitating carrier detection in this population. We recently reported a BRCA2 c.9004GA variant of unknown clinical significance in two French Canadian breast cancer families. It confers a E3002K alteration in the conserved C-terminus domain of BRCA2, and has been reported in non-French Canadian cancer families. Seven variant positive French Canadian families have since been identified by mutation screening of referrals to hereditary cancer clinics. In this article, we describe the cancer phenotypes of these families and further assess the contribution of this variant in the French Canadian population. We screened index breast cancer cases from 58 cancer families with at least three confirmed cases of breast and/or ovarian cancer and 960 breast cancer cases (48 years mean age) not selected for family history of cancer that were previously found not to carry the most common BRCA1 and BRCA2 mutations reported in this population. The index variant-positive cases from each family had breast cancer between the ages of 35-55 years (43 years mean age); and reported close relatives with breast cancer diagnoses between the ages of 28-84 years (57 years mean age). Three families had ovarian or peritoneal cancers. BRCA2-associated cancers, such as bladder, esophagus, pancreas, prostate, and thyroid cancers also occurred in these families. One c.9004GA carrier also harbored the PALB2 c.2323CT (Q775X) mutation found to recur in French Canadian breast cancer cases. No new BRCA2 variant carriers were identified in mutation screens. The absence of BRCA2 c.9004GA carriers in the breast cancer cases not selected for family history contrasts with familial cases, supporting a pathogenic status for this variant and addition to the existing common BRCA1 and BRCA2 mutation-screening panel for French Canadian breast and/or ovarian cancer families.

Published

2011

123. Chromosome 3 anomalies investigated by genome wide SNP analysis of benign, low malignant potential and low grade ovarian serous tumours

Author

Kurosh Rahimi, Ashley H. Birch, Anne-Marie Mes-Masson, Suzanna L. Arcand, Patricia N. Tonin, A. Kevin Watters, Diane Provencher, Kathleen Klein Oros, and Celia M. T. Greenwood

Subjects

Pathology, endocrine system diseases, lcsh:Medicine, Genome-wide association study, medicine.disease_cause, Fusion gene, 0302 clinical medicine, Neoplasm Metastasis, lcsh:Science, Ovarian Neoplasms, 0303 health sciences, Multidisciplinary, Gene Ontologies, Homozygote, Obstetrics and Gynecology, Genomics, Genome Scans, female genital diseases and pregnancy complications, Ovarian Cancer, 3. Good health, Gene Expression Regulation, Neoplastic, Serous fluid, Oncology, 030220 oncology & carcinogenesis, Disease Progression, Medicine, Female, Chromosomes, Human, Pair 3, KRAS, Cancer Screening, Research Article, SNP array, medicine.medical_specialty, Histology, Genotype, Biology, Genome Complexity, Polymorphism, Single Nucleotide, Ovarian disease, 03 medical and health sciences, Genome Analysis Tools, Genetic Mutation, Molecular genetics, Genome-Wide Association Studies, Genetics, Cancer Genetics, Cancer Detection and Diagnosis, Early Detection, medicine, Humans, 030304 developmental biology, Chromosome Aberrations, Gene Expression Profiling, Ovary, lcsh:R, Gynecologic Cancers, Computational Biology, Cancers and Neoplasms, Human Genetics, Genetic Maps, medicine.disease, Genes, ras, Chromosome 3, Mutagenesis, Mutation, lcsh:Q, Gynecological Tumors, Genome-Wide Association Study

Abstract

Ovarian carcinomas exhibit extensive heterogeneity, and their etiology remains unknown. Histological and genetic evidence has led to the proposal that low grade ovarian serous carcinomas (LGOSC) have a different etiology than high grade carcinomas (HGOSC), arising from serous tumours of low malignant potential (LMP). Common regions of chromosome (chr) 3 loss have been observed in all types of serous ovarian tumours, including benign, suggesting that these regions contain genes important in the development of all ovarian serous carcinomas. A high-density genome-wide genotyping bead array technology, which assayed >600,000 markers, was applied to a panel of serous benign and LMP tumours and a small set of LGOSC, to characterize somatic events associated with the most indolent forms of ovarian disease. The genomic patterns inferred were related to TP53, KRAS and BRAF mutations. An increasing frequency of genomic anomalies was observed with pathology of disease: 3/22 (13.6%) benign cases, 40/53 (75.5%) LMP cases and 10/11 (90.9%) LGOSC cases. Low frequencies of chr3 anomalies occurred in all tumour types. Runs of homozygosity were most commonly observed on chr3, with the 3p12-p11 candidate tumour suppressor region the most frequently homozygous region in the genome. An LMP harboured a homozygous deletion on chr6 which created a GOPC-ROS1 fusion gene, previously reported as oncogenic in other cancer types. Somatic TP53, KRAS and BRAF mutations were not observed in benign tumours. KRAS-mutation positive LMP cases displayed significantly more chromosomal aberrations than BRAF-mutation positive or KRAS and BRAF mutation negative cases. Gain of 12p, which harbours the KRAS gene, was particularly evident. A pathology review reclassified all TP53-mutation positive LGOSC cases, some of which acquired a HGOSC status. Taken together, our results support the view that LGOSC could arise from serous benign and LMP tumours, but does not exclude the possibility that HGOSC may derive from LMP tumours.

Published

2011

124. RAD51C germline mutations in breast and ovarian cancer patients

Author

Mohammad R. Akbari, William D. Foulkes, Marc Tischkowitz, Patricia N. Tonin, Parviz Ghadirian, and Steven A. Narod

Subjects

Ovarian Neoplasms, Oncology, Mutation, medicine.medical_specialty, Letter, Breast Neoplasms, Biology, medicine.disease_cause, medicine.disease, Germline, DNA-Binding Proteins, Germline mutation, Breast cancer, Surgical oncology, Internal medicine, medicine, Cancer research, Humans, RAD51C, Missense mutation, Female, Ovarian cancer, Germ-Line Mutation

Abstract

Recently, RAD51C reported as a breast cancer susceptibility gene. A germline mutation was seen in 1.3% of breast/ovarian cancer families from Germany. In order to confirm this report, we sequenced coding exons of RAD51C in the germline DNA of 454 patients with familial breast/ovarian cancer. We found no deleterious RAD51C mutation among the 454 patients. Based on the prevalence of mutations in the initial report, we expected to identify approximately five families with a deleterious germline RAD51C mutation. Our result indicates that perhaps RAD51C mutations are not as common as the initial report suggests.

Published

2010

125. Authors' Reply

Author

Jason Madore, Martin Köbel, Patricia N Tonin, David Huntsman, Diane M Provencher, and Anne-Marie Mes-Masson

Subjects

Pathology and Forensic Medicine

Published

2010

126. The gene for a novel protein, a member of the protein disulphide isomerase/form I phosphoinositide-specific phospholipase C family, is amplified in hydroxyurea-resistant cells

Author

P. R. Srinivasan, Patricia N. Tonin, Murari M. Chaudhuri, and William H. Lewis

Subjects

Molecular Sequence Data, Drug Resistance, Protein Disulfide-Isomerases, Biology, Ornithine Decarboxylase, Biochemistry, Cell Line, Deoxyribonuclease EcoRI, Rapid amplification of cDNA ends, Cricetinae, Sequence Homology, Nucleic Acid, Complementary DNA, Ribonucleotide Reductases, Protein biosynthesis, Animals, Hydroxyurea, Amino Acid Sequence, RNA, Messenger, Isomerases, Molecular Biology, Peptide sequence, Binding Sites, Base Sequence, Phosphoric Diester Hydrolases, cDNA library, Phosphatidylinositol Diacylglycerol-Lyase, Gene Amplification, Nucleic acid sequence, Proteins, RNA, DNA, Cell Biology, Molecular biology, Molecular Weight, genomic DNA, Protein Biosynthesis, Research Article

Abstract

Cell lines selected in multiple steps for increasing resistance to hydroxyurea have been shown to have corresponding increases in ribonucleotide reductase activity. We have isolated a number of cDNA clones from a cDNA library constructed from a highly hydroxyurea-resistant hamster cell line, 600H, in which the activity of ribonucleotide reductase is elevated more than 80-fold. These clones correspond to genomic DNA sequences amplified in the 600H cell line compared with the V79 parental line. One of these cDNA clones, termed P5, codes for a 50 kDa protein detected by in vitro translation of poly(A)+ RNA isolated by hybridization/selection. The cDNA sequence contains a single open reading frame of 1317 nucleotides which encodes a polypeptide of 439 amino acids. The amino acid sequence deduced from the cDNA insert contains two copies of the 11-amino-acid sequence Val-Glu-Phe-Tyr-Ala-Pro-Trp-Cys-Gly-His-Cys. Duplicate copies of this sequence also occur in the active site of rat and human protein disulphide isomerase (also known as the beta-subunit of human prolyl 4-hydroxylase, tri-iodothyronine-binding protein) and in Form I phosphoinositide-specific phospholipase C, indicating that P5 falls into this newly defined superfamily of proteins. Genomic sequences similar to the cDNA clone are amplified 10-20-fold in hamster cells selected for resistance to increasing concentrations of hydroxyurea, a phenomenon observed earlier with cDNA clones for the M2 subunit of ribonucleotide reductase and ornithine decarboxylase. RNA blots probed with P5 cDNA show two poly(A)+ RNA species which are elevated in hydroxyurea-resistant cells.

Published

1992

127. Mutations in a 10-bp polyadenine repeat of transforming growth factor β-receptor type II gene is an infrequent event in human epithelial ovarian cancer

Author

Emily N. Manderson, Patricia N. Tonin, Anne Marie Mes-Masson, and D. Provencher

Subjects

medicine.medical_specialty, biology, Tumor cells, Transforming growth factor beta, Receptor type, Gene deletion, Frameshift mutation, Endocrinology, Internal medicine, Genetics, medicine, biology.protein, Cancer research, Epithelial ovarian cancer, Receptor, Gene, Genetics (clinical)

Published

2000

128. Characterization of the molecular differences between ovarian endometrioid carcinoma and ovarian serous carcinoma

Author

Jason, Madore, Fengge, Ren, Ali, Filali-Mouhim, Lilia, Sanchez, Martin, Köbel, Patricia N, Tonin, David, Huntsman, Diane M, Provencher, and Anne-Marie, Mes-Masson

Subjects

Ovarian Neoplasms, Gene Expression Profiling, PTEN Phosphohydrolase, Prognosis, Survival Analysis, Cystadenocarcinoma, Serous, Neoplasm Proteins, Cohort Studies, Biomarkers, Tumor, Humans, Female, Tumor Suppressor Protein p53, WT1 Proteins, Carcinoma, Endometrioid, beta Catenin, Oligonucleotide Array Sequence Analysis

Abstract

The histopathological diagnosis of high-grade endometrioid and serous carcinoma of the ovary is poorly reproducible under the current morphology based classification system, especially for anaplastic, high-grade tumours. The transcription factor Wilms' tumour-1 (WT1) is differentially expressed among the gynaecological epithelia from which epithelial ovarian cancers (EOCs) are believed to originate. In EOCs, WT1 protein is observed in the majority of serous carcinomas and in up to 30% of endometrioid carcinomas. It is unclear whether the latter is a reflection of the actual incidence of WT1 protein expression in endometrioid carcinomas, or whether a significant number of high-grade serous carcinomas have been misclassified as endometrioid carcinoma. Several genetic aberrations are reported to occur in EOCs. These include mutation of the TP53 gene, aberrant activation of beta-catenin signalling and loss of PTEN protein expression, among others. It is unclear whether these aberrations are histotype-specific. The aim of this study was to better define the molecular characteristics of serous and endometrioid carcinomas in an attempt to address the problems with the current histopathological classification methods. Gene expression profiles were analysed to identify reproducible gene expression phenotypes for endometrioid and serous carcinomas. Tissue microarrays (TMA) were used to assess the incidence of TP53, beta-catenin and PTEN aberrations in order to correlate their occurrence with WT1 as an immunohistochemistry based biomarker of serous histotype. It was found that nuclear WT1 protein expression can identify misclassified high-grade endometrioid carcinomas and these tumours should be reassigned to serous histotype. Although low-grade endometrioid carcinomas rarely progress to high-grade carcinomas, a combined WT1-negative, TP53-positive immunophenotype may identify an uncommon high-grade subtype of ovarian endometrioid carcinoma. GEO database: array data accession number GSE6008.

Published

2009

129. Protease inhibitor SERPINA1 expression in epithelial ovarian cancer

Author

Cécile Le Page, Veronique Ouellet, Karine Normandin, Benjamin Péant, Manon de Ladurantaye, Patricia N. Tonin, Diane Provencher, and Anne-Marie Mes-Masson

Subjects

Ovarian Neoplasms, Cancer Research, Proteases, Protease, medicine.medical_treatment, General Medicine, Mice, SCID, Serpin, Biology, medicine.disease, Molecular biology, Metastasis, Mice, Oncology, Tumor progression, Surgical oncology, Tissue Array Analysis, Cell Line, Tumor, alpha 1-Antitrypsin, medicine, Animals, Humans, Female, Ovarian cancer, Survival rate

Abstract

Epithelial ovarian cancer is the most lethal gynecologic cancer with a 5 years survival rate of 30-40% in patients diagnosed with high-grade invasive disease (TOV). This is in stark contrast to the 95% 5 years survival rate in ovarian cancer patients diagnosed with low malignant potential (LMP) disease. The progression from localized tumor to invasive metastasis involves matrix proteolysis. Protease inhibitors are thought to play a key role by limiting this process. Using the Affymetrix HG-U133A GeneChip array, we have studied all serine protease inhibitors and found several serpin family members that are differentially expressed between LMP and TOV serous tumors. SERPINA1 was selected for further study due to its high expression in the majority of LMP tumors and its low expression in TOV tumors; observations that were also validated by quantitative-PCR (Q-PCR). To study the effects of its over expression on different tumorigenic parameters, SERPINA1 was cloned in the pcDNA3.1+ plasmid which was subsequently used to derive stable clones from two invasive ovarian cancer cell lines, TOV-112D and TOV-1946. We found no effect of SERPINA1 over expression on tumor growth in SCID mice although cell migration and invasion were affected in in vitro assays. There was also no association between patient survival and SERPINA1 immunostaining, however, SERPINA1 localization was different in LMP (nuclear) and TOV (cytoplasmic) tumors. SERPINA1 remains an interesting candidate since protein homeostasis, regulated by proteases and their inhibitors, should be studied holistically in order to assess their full impact in tumor progression.

Published

2009

130. The chemiluminescence based Ziplex® automated workstation focus array reproduces ovarian cancer Affymetrix GeneChip® expression profiles

Author

Ashley H. Birch, Diane Provencher, Anne-Marie Mes-Masson, Suzanna L. Arcand, David Englert, Patricia N. Tonin, Fiona Young, Paulina M. Wojnarowicz, Adam A Dempsey, Michael C.J. Quinn, and Daniel J Wilson

Subjects

Untranslated region, Luminescence, lcsh:Medicine, Gene Expression, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Gene expression, Biomarkers, Tumor, medicine, Humans, Gene, Oligonucleotide Array Sequence Analysis, 030304 developmental biology, Medicine(all), Ovarian Neoplasms, 0303 health sciences, Reproducibility, Biochemistry, Genetics and Molecular Biology(all), Gene Expression Profiling, Hybridization probe, lcsh:R, Methodology, Reproducibility of Results, General Medicine, medicine.disease, Molecular biology, Fold change, Gene expression profiling, Data Interpretation, Statistical, 030220 oncology & carcinogenesis, Luminescent Measurements, Female, DNA Probes, Ovarian cancer

Abstract

Background As gene expression signatures may serve as biomarkers, there is a need to develop technologies based on mRNA expression patterns that are adaptable for translational research. Xceed Molecular has recently developed a Ziplex® technology, that can assay for gene expression of a discrete number of genes as a focused array. The present study has evaluated the reproducibility of the Ziplex system as applied to ovarian cancer research of genes shown to exhibit distinct expression profiles initially assessed by Affymetrix GeneChip® analyses. Methods The new chemiluminescence-based Ziplex® gene expression array technology was evaluated for the expression of 93 genes selected based on their Affymetrix GeneChip® profiles as applied to ovarian cancer research. Probe design was based on the Affymetrix target sequence that favors the 3' UTR of transcripts in order to maximize reproducibility across platforms. Gene expression analysis was performed using the Ziplex Automated Workstation. Statistical analyses were performed to evaluate reproducibility of both the magnitude of expression and differences between normal and tumor samples by correlation analyses, fold change differences and statistical significance testing. Results Expressions of 82 of 93 (88.2%) genes were highly correlated (p < 0.01) in a comparison of the two platforms. Overall, 75 of 93 (80.6%) genes exhibited consistent results in normal versus tumor tissue comparisons for both platforms (p < 0.001). The fold change differences were concordant for 87 of 93 (94%) genes, where there was agreement between the platforms regarding statistical significance for 71 (76%) of 87 genes. There was a strong agreement between the two platforms as shown by comparisons of log2 fold differences of gene expression between tumor versus normal samples (R = 0.93) and by Bland-Altman analysis, where greater than 90% of expression values fell within the 95% limits of agreement. Conclusion Overall concordance of gene expression patterns based on correlations, statistical significance between tumor and normal ovary data, and fold changes was consistent between the Ziplex and Affymetrix platforms. The reproducibility and ease-of-use of the technology suggests that the Ziplex array is a suitable platform for translational research.

Published

2009

131. Characterization of the 3p12.3-pcen region associated with tumor suppression in a novel ovarian cancer cell line model genetically modified by chromosome 3 fragment transfer

Author

Neal A L, Cody, Zhen, Shen, Jean-Sebastien, Ripeau, Diane M, Provencher, Anne-Marie, Mes-Masson, Mario, Chevrette, and Patricia N, Tonin

Subjects

Ovarian Neoplasms, Ovary, Loss of Heterozygosity, DNA Methylation, Cystadenocarcinoma, Serous, Alternative Splicing, Case-Control Studies, Cell Line, Tumor, Humans, Female, Genes, Tumor Suppressor, Chromosomes, Human, Pair 3, DNA Primers, Microsatellite Repeats

Abstract

The genetic analysis of nontumorigenic radiation hybrids generated by transfer of chromosome 3 fragments into the tumorigenic OV-90 ovarian cancer cell line identified the 3p12.3-pcen region as a candidate tumor suppressor gene (TSG) locus. In the present study, polymorphic microsatellite repeat analysis of the hybrids further defined the 3p12.3-pcen interval to a 16.1 Mb common region containing 12 known or hypothetical genes: 3ptel-ROBO2-ROBO1-GBE1-CADM2-VGLL3-CHMP2B-POU1F1-HTR1F-CGGBP1-ZNF654-C3orf38-EPHA3-3pcen. Seven of these genes, ROBO1, GBE1, VGLL3, CHMP2B, CGGBP1, ZNF654, and C3orf38, exhibited gene expression in the hybrids, placing them as top TSG candidates for further analysis. The expression of all but one (VGLL3) of these genes was also detected in the parental OV-90 cell line. Mutations were not identified in a comparative sequence analysis of the predicted protein coding regions of these candidates in OV-90 and donor normal chromosome 3 contig. However, the nondeleterious sequence variants identified in the transcribed regions distinguished parent of origin alleles for ROBO1, VGLL3, CHMP2B, and CGGBP1 and cDNA sequencing of the hybrids revealed biallelic expression of these genes. Interestingly, underexpression of VGLL3 and ZNF654 were observed in malignant ovarian tumor samples as compared with primary cultures of normal ovarian surface epithelial cells or benign ovarian tumors, and this occurred regardless of allelic content of 3p12.3-pcen. The results taken together suggest that dysregulation of VGLL3 and/or ZNF654 expression may have affected pathways important in ovarian tumorigenesis which was offset by the transfer of chromosome 3 fragments in OV-90, a cell line hemizygous for 3p.

Published

2009

132. Thematic issue on the molecular biology of hereditary ovarian cancer

Author

Patricia N. Tonin

Subjects

Oncology, Cancer Research, medicine.medical_specialty, General Medicine, Computational biology, medicine.disease, Internal medicine, Genetics, medicine, Molecular Medicine, Preface, Ovarian cancer, Psychology

Published

2009

133. Reprogramming of the transcriptome in a novel chromosome 3 transfer tumor suppressor ovarian cancer cell line model affected molecular networks that are characteristic of ovarian cancer

Author

Anne-Marie Mes-Masson, Michael C.J. Quinn, Patricia N. Tonin, Abdelali Filali-Mouhim, and Diane Provencher

Subjects

Genetics, Ovarian Neoplasms, Cancer Research, endocrine system diseases, Tumor suppressor gene, Microarray, Microarray analysis techniques, Reverse Transcriptase Polymerase Chain Reaction, Cancer, Biology, medicine.disease, Transcriptome, Chromosome 3, Cell Line, Tumor, medicine, Cancer research, Humans, Female, Genes, Tumor Suppressor, Chromosomes, Human, Pair 3, RNA, Messenger, Ovarian cancer, Molecular Biology, Gene, Oligonucleotide Array Sequence Analysis

Abstract

Tumor suppression as a consequence of the transfer of chromosome 3p fragments was previously observed in a novel epithelial ovarian cancer (EOC) OV-90 cell line model harboring loss of 3p. Microarray analysis revealed that tumor suppression was associated with a modified transcriptome. To investigate the relevance of the altered transcriptome, the differentially expressed genes identified by Affymetrix analysis in the 3p transfer studies, were integrated with a comparative microarray analysis of normal ovarian surface epithelial (NOSE) cells and malignant ovarian (TOV) cancers. Data from 219 significantly differentially expressed genes exhibited patterns in the direction predicted by the analysis of 3p transfer study. The 30 genes with the highest statistically significant differences (P

Published

2009

134. Immunohistochemical profiling of benign, low malignant potential and low grade serous epithelial ovarian tumors

Author

Diane Provencher, Tak Hay Ling, Christian Lussier, Véronique Barrès, Anne-Marie Mes-Masson, Karine Normandin, Dimcho Bachvarov, Claudine Rancourt, Veronique Ouellet, Patricia N. Tonin, and Jason Madore

Subjects

Cancer Research, Pathology, medicine.medical_specialty, endocrine system diseases, lcsh:RC254-282, Protein expression, Ovarian disease, Surgical oncology, Genetics, medicine, Biomarkers, Tumor, Humans, Epithelial ovarian cancer, Ovarian Neoplasms, business.industry, Cystadenoma, Serous, Serous Cystadenoma, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immunohistochemistry, Serous fluid, Oncology, Tissue Array Analysis, Female, Stem cell, business, Research Article

Abstract

Background Serous epithelial ovarian tumors can be subdivided into benign (BOV), low malignant potential (LMP) or borderline and invasive (TOV) tumors. Although the molecular characteristics of serous BOV, LMP and low grade (LG) TOV tumors has been initiated, definitive immunohistochemical markers to distinguish between these tumor types have not been defined. Methods In the present study, we used a tissue array composed of 27 BOVs, 78 LMPs and 23 LG TOVs to evaluate the protein expression of a subset of selected candidates identified in our previous studies (Ape1, Set, Ran, Ccne1 and Trail) or known to be implicated in epithelial ovarian cancer disease (p21, Ccnb1, Ckd1). Results Statistically significant difference in protein expression was observed for Ccnb1 when BOV tumors were compared to LMP tumors (p = 0.003). When BOV were compared to LG TOV tumors, Trail was significantly expressed at a higher level in malignant tumors (p = 0.01). Expression of p21 was significantly lower in LG tumors when compared with either BOVs (p = 0.03) or LMPs (p = 0.001). We also observed that expression of p21 was higher in LMP tumors with no (p = 0.02) or non-invasive (p = 0.01) implants compared to the LMP associated with invasive implants. Conclusion This study represents an extensive analyse of the benign and highly differentiated ovarian disease from an immunohistochemical perspective.

Published

2008

135. Identification of a novel CHEK2variant and assessment of its contribution to the risk of breast cancer in French Canadian women

Author

Phil Zhang, François Rousseau, David J. Novak, William D. Foulkes, Nancy Hamel, Steven A. Narod, Long Qi Chen, Parviz Ghadirian, Vanessa Rossiny, Patricia N. Tonin, André Robidoux, and Guy Cardinal

Subjects

Adult, Canada, Cancer Research, Genes, BRCA2, Population, Genes, BRCA1, Mutation, Missense, Breast Neoplasms, Protein Serine-Threonine Kinases, lcsh:RC254-282, Breast cancer, Genetics, Humans, Medicine, Genetic Predisposition to Disease, Allele, skin and connective tissue diseases, education, Genotyping, CHEK2, Aged, education.field_of_study, business.industry, Genetic Variation, Middle Aged, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Penetrance, Founder Effect, Gene Expression Regulation, Neoplastic, Checkpoint Kinase 2, Oncology, Female, business, Variants of PCR, Research Article, Founder effect

Abstract

BackgroundBRCA1andBRCA2account for the majority of the known familial breast cancer risk, however, the impact of other cancer susceptibility genes largely remains to be elucidated. Checkpoint Kinase 2 (CHEK2) is an important signal transducer of cellular responses to DNA damage, whose defects have been associated with an increase in breast cancer risk. Previous studies have identified low penetranceCHEK2alleles such as 1100delC and I157T, as well as variants such as S428F in the Ashkenazi Jewish population and IVS2 + 1G>A in the Polish population. No founder allele has been specifically identified in the French Canadian population.MethodsThe 14 coding exons ofCHEK2were fully sequenced for variant alleles in a panel of 25 affected French Canadian women and 25 healthy controls. Two variants were identified of which one novel variant was further screened for in an additional panel of 667 breast cancer patients and 6548 healthy controls. Additional genotyping was conducted using allele specific PCR and a restriction digest assay. Significance of amino acid substitutions were deduced by employing comparative analysis techniques.ResultsTwo variants were identified: the previously reported silent substitution 252A>G (E84E) and the novel missense variant, 1217G>A (R406H). No significant difference in allele distribution between French Canadian women with breast cancer and healthy controls was observed (3/692, 0.43% vs. 22/6573, 0.33%, respectively, P = 0.73).ConclusionThe novel CHEK2 missense variant identified in this study, R406H, is unlikely to contribute to breast cancer risk in French Canadian women.

Published

2008

136. Influence of monolayer, spheroid, and tumor growth conditions on chromosome 3 gene expression in tumorigenic epithelial ovarian cancer cell lines

Author

Neal A.L. Cody, Diane Provencher, A. Filali-Mouhim, Patricia N. Tonin, Magdalena Zietarska, and Anne-Marie Mes-Masson

Subjects

0303 health sciences, lcsh:Internal medicine, Microarray, lcsh:QH426-470, Microarray analysis techniques, Biology, Molecular biology, 03 medical and health sciences, lcsh:Genetics, 0302 clinical medicine, Chromosome 3, Cell culture, 030220 oncology & carcinogenesis, Gene expression, Cancer research, Genetics, Genetics(clinical), Epigenetics, DNA microarray, lcsh:RC31-1245, Gene, Genetics (clinical), 030304 developmental biology, Research Article

Abstract

Background Expression microarray analyses of epithelial ovarian cancer (EOC) cell lines may be exploited to elucidate genetic and epigenetic events important in this disease. A possible variable is the influence of growth conditions on discerning candidates. The present study examined the influence of growth conditions on the expression of chromosome 3 genes in the tumorigenic EOC cell lines, OV-90, TOV-21G and TOV-112D using Affymetrix GeneChip® HG-U133A expression microarray analysis. Methods Chromosome 3 gene expression profiles (n = 1147 probe sets, representing 735 genes) were extracted from U133A expression microarray analyses of the EOC cell lines OV-90, TOV-21G and TOV-112D that were grown as monolayers, spheroids or nude mouse xenografts and monolayers derived from these tumors. Hierarchical cluster analysis was performed to compare chromosome 3 transcriptome patterns of each growth condition. Differentially expressed genes were identified and characterized by two-way comparative analyses of fold-differences in gene expression between monolayer cultures and each of the other growth conditions, and between the maximum and minimum values of expression of all growth conditions for each EOC cell line. Results An overall high degree of similarity (> 90%) in gene expression was observed when expression values of alternative growth conditions were compared within each EOC cell line group. Two-way comparative analysis of each EOC cell line grown in an alternative condition relative to the monolayer culture showed that overall less than 15% of probe sets exhibited at least a 3-fold difference in expression profile. Less than 23% of probe sets exhibited greater than 3-fold differences in gene expression in comparisons of the maximum and minimum value of expression of all growth conditions within each EOC cell line group. The majority of these differences were less than 5-fold. There were 17 genes in common which were differentially expressed in all EOC cell lines. However, the patterns of expression of these genes were not necessarily the same for each growth condition when one cell line was compared with another. Conclusion The various alternative in vivo and in vitro growth conditions of tumorigenic EOC cell lines appeared to modestly influence the global chromosome 3 transcriptome supporting the notion that the in vitro cell line models are a viable option for testing gene candidates.

Published

2008

137. Characterization of three new serous epithelial ovarian cancer cell lines

Author

Anne-Marie Mes-Masson, Julie Lafontaine, Patricia N. Tonin, Lise Portelance, Marie-Line Puiffe, Veronique Ouellet, Suzanna L. Arcand, Diane Provencher, Jason Madore, Zhen Shen, Josée Hébert, and Magdalena Zietarska

Subjects

Cancer Research, Pathology, medicine.medical_specialty, endocrine system diseases, Receptor, ErbB-2, Somatic cell, Transplantation, Heterologous, Population, Cell Growth Processes, Mice, SCID, Biology, medicine.disease_cause, lcsh:RC254-282, Germline, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Genetics, medicine, Animals, Humans, education, 030304 developmental biology, Ovarian Neoplasms, 0303 health sciences, education.field_of_study, Mutation, Ascites, Cancer, Epithelial Cells, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Cystadenocarcinoma, Serous, 3. Good health, Serous fluid, Oncology, Karyotyping, 030220 oncology & carcinogenesis, Cancer research, Keratins, Female, KRAS, Tumor Suppressor Protein p53, Stem cell, Research Article

Abstract

Background Cell lines constitute a powerful model to study cancer, and here we describe three new epithelial ovarian cancer (EOC) cell lines derived from poorly differentiated serous solid tumors (TOV-1946, and TOV-2223G), as well as the matched ascites for one case (OV-1946). Methods In addition to growth parameters, the cell lines were characterized for anchorage independent growth, migration and invasion potential, ability to form spheroids and xenografts in SCID mice. Results While all cell lines were capable of anchorage independent growth, only the TOV-1946 and OV-1946 cell lines were able to form spheroid and produce tumors. Profiling of keratins, p53 and Her2 protein expression was assessed by immunohistochemistry and western blot analyses. Somatic TP53 mutations were found in all cell lines, with TOV-1946 and OV-1946 harboring the same mutation, and none harbored the commonly observed somatic mutations in BRAF, KRAS or germline BRCA1/2 mutations found to recur in the French Canadian population. Conventional cytogenetics and spectral karyotype (SKY) analyses revealed complex karyotypes often observed in ovarian disease. Conclusion This is the first report of the establishment of matched EOC cell lines derived from both solid tumor and ascites of the same patient.

Published

2008

138. Construction of a chromosome 17 transcriptome in serous ovarian cancer identifies differentially expressed genes

Author

A. Breznan, A. Filali-Mouhim, Paulina M. Wojnarowicz, Suzanna L. Arcand, Patricia N. Tonin, D. Provencher, and Anne Marie Mes-Masson

Subjects

Adult, Biology, Transcriptome, medicine, Tumor Cells, Cultured, Humans, RNA, Messenger, Gene, Aged, Regulation of gene expression, Genetics, Ovarian Neoplasms, Gene Expression Profiling, Obstetrics and Gynecology, Middle Aged, medicine.disease, Molecular biology, Chromosome 17 (human), Gene expression profiling, Gene Expression Regulation, Neoplastic, Serous fluid, Oncology, Gene chip analysis, Female, Ovarian cancer, Chromosomes, Human, Pair 17

Abstract

Cytogenetic, molecular genetic, and functional analyses have implicated chromosome 17 genes in epithelial ovarian cancer (EOC). To further characterize the contribution of chromosome 17 genes in EOC, the Affymetrix U133A GeneChip was used to perform transcriptome analyses of 15 primary cultures of normal ovarian surface epithelial (NOSE) cells and 17 malignant ovarian tumor (TOV) samples of the serous histopathologic subtype. A two-way comparative analysis of 776 known genes and expressed sequences identified 253 genes that exhibited at least a threefold difference in expression in at least one TOV sample compared to the mean of NOSE samples. Within this data set, 99 of the 253 (39.1%) genes exhibited similar patterns of expression across all tested samples, suggesting a high degree of concordance in the chromosome 17 transcriptome. This observation was supported by hierarchical clustering analysis that segregated the TOV and NOSE samples into two separate groups. There were 77 genes that were differentially expressed in at least 50% of the TOV samples. Five genes (AdoRA2Bat 17p12,CCL2at 17q12,ACLYat 17q21.2,WIPI1at 17q24.2, andSLC16A3at 17q25.3) were significantly (P< 5.13E−11) differentially expressed at least threefold in all serous TOV samples, and all five genes were underexpressed in these TOV samples as compared to the NOSE samples. Interestingly, several of these differentially expressed genes have been previously associated with response to hypoxia.

Published

2007

139. Transcriptome analysis of serous ovarian cancers identifies differentially expressed chromosome 3 genes

Author

Ashley H. Birch, Diane Provencher, Michael C.J. Quinn, Anne-Marie Mes-Masson, A. Filali-Mouhim, and Patricia N. Tonin

Subjects

Cancer Research, endocrine system diseases, Microarray, Transcription, Genetic, Cell Culture Techniques, Biology, Cell Line, Transcriptome, Loss of heterozygosity, Cell Line, Tumor, Gene expression, medicine, Humans, Molecular Biology, Gene, Chromosome Aberrations, Ovarian Neoplasms, Ovary, Chromosome Mapping, Epithelial Cells, DNA, Neoplasm, medicine.disease, Molecular biology, Gene Expression Regulation, Neoplastic, Serous fluid, Chromosome 3, Female, Chromosomes, Human, Pair 3, Ovarian cancer

Abstract

Cytogenetic, molecular genetic and functional analyses have implicated chromosome 3 genes in epithelial ovarian cancers (EOC). To further characterize their contribution to EOC, the Affymetrix U133A GeneChip® was used to perform transcriptome analyses of chromosome 3 genes in primary cultures of normal ovarian surface epithelial (NOSE) cells (n = 14), malignant serous epithelial ovarian tumors (TOV) (n = 17), and four EOC cell lines (TOV-81D, TOV-112D, TOV-21G, and OV-90). A two-way comparative analysis of 735 known genes and expressed sequences identified 278 differentially expressed genes, where 43 genes were differentially expressed in at least 50% of the TOV samples. Three genes, RIS1 (at 3p21.31), GBE1 (at 3p12.2), and HEG1 (at 3q21.2), were similarly underexpressed in all TOV samples. Deregulation of the expression of these genes was not associated with loss of heterozygosity (LOH) of the genetic loci harboring them. LOH analysis of the RIS1, GBE1, and HEG1 loci was observed at frequencies of 14.3%, 13.7%, and 9.2%, respectively, in a series of 66 malignant TOV samples of the serous subtype. Reduced expression levels of RIS1, GBE1, and HEG1 were observed only in the tumorigenic EOC cell lines (TOV-21G, TOV-112D, and OV-90) and did not correlate with LOH. These results combined suggest that RIS1, GBE1, and HEG1, unlike classical tumor suppressor genes, are not likely to be primary targets of inactivation. This study provides a comprehensive analysis of chromosome 3 gene expression in NOSE and in EOC samples and identifies chromosome 3 gene candidates for further study. © 2007 Wiley-Liss, Inc.

Published

2007

140. An apoptotic molecular network identified by microarray: on the TRAIL to new insights in epithelial ovarian cancer

Author

Patricia N. Tonin, Veronique Ouellet, Véronique Barrès, Marie-Claude Guyot, Cécile Le Page, Diane Provencher, Jason Madore, Christian Lussier, and Anne-Marie Mes-Masson

Subjects

Cancer Research, Candidate gene, Pathology, medicine.medical_specialty, Microarray, medicine.medical_treatment, Apoptosis, Caspase 8, TNF-Related Apoptosis-Inducing Ligand, medicine, Humans, Neoplasms, Glandular and Epithelial, Oligonucleotide Array Sequence Analysis, Ovarian Neoplasms, business.industry, Cancer, medicine.disease, Prognosis, Survival Analysis, Serous fluid, Cytokine, Oncology, Flip, Cancer research, Immunohistochemistry, Female, business

Abstract

BACKGROUND. In a previous microarray expression analysis, the authors identified candidate genes that were expressed differentially between ovarian tumors with low malignant potential and invasive serous epithelial ovarian tumors. Among them, the apoptosis-related candidate genes tumor necrosis factor-related apoptosis-inducing ligand (TRAIL), caspase 8 (CASP8), FLICE-inhibitory protein (FLIP), and cytochrome C (CYC) were identified. METHODS. For the current study, the authors conducted immunohistochemical analyses of a tissue array comprised of 235 serous tumors of different grades and stages to evaluate whether there was differential protein expression for these candidates and for the 4 death cell receptors of Trail: Dr4, Dr5, DcR1, and DcR2. RESULTS. All proteins except DcR1 and DcR2 had significantly differential expression levels between grade 0 tumors (low malignant potential) and grade 2 and 3 tumors. Trail also showed differential expression between grade 0 tumors and grade 1 tumors. When all tumors were compared, the expression levels of Trail, Dr4, Dr5, DcR1, and Flip differed significantly between early-stage and advanced-stage disease. High Dr5 expression was associated with a poor prognosis in patients who had invasive tumors and in the subgroup of patients who had grade 3 tumors. Furthermore, the combinations of 2 proteins (Trail and Dr5, DcR2 and Cyc, Flip and Dr5, Flip and DcR2, DcR1 and Dr5 or Dr4 and Flip) revealed an association with patient prognosis. CONCLUSIONS. The identification of new proteins in the initial diagnosis and prognosis of patients with epithelial ovarian cancer may lead to a better understanding of the disease, highlighting new potential therapeutic targets, and may be useful in patient management. Cancer 2007. © 2007 American Cancer Society.

Published

2007

141. Analysis of PALB2/FANCN-associated breast cancer families

Author

Aletta Poll, Tayma Khalil, Nora Wong, Atilla Omeroglu, Bing Xia, Patricia N. Tonin, Pierre Lepage, Lili Li, Marc Tischkowitz, Steven A. Narod, Erik H. van Beers, Jorge S. Reis-Filho, William D. Foulkes, David M. Livingston, Alan Ashworth, Guilan Li, Nancy Hamel, Nelly Sabbaghian, Petra M. Nederlof, and Louise A. Quenneville

Subjects

Oncology, Adult, Male, medicine.medical_specialty, PALB2, DNA Mutational Analysis, Breast Neoplasms, Biology, medicine.disease_cause, Frameshift mutation, Breast Neoplasms, Male, Loss of heterozygosity, Breast cancer, Internal medicine, medicine, Humans, Point Mutation, Genetic Predisposition to Disease, Family history, skin and connective tissue diseases, Frameshift Mutation, CHEK2, Melanoma, Genetics, Aged, 80 and over, Mutation, Multidisciplinary, Point mutation, Tumor Suppressor Proteins, Nuclear Proteins, Middle Aged, Biological Sciences, medicine.disease, Pedigree, Fanconi Anemia, Female, Fanconi Anemia Complementation Group N Protein

Abstract

No more than ≈30% of hereditary breast cancer has been accounted for by mutations in known genes. Most of these genes, such as BRCA1 , BRCA2 , TP53 , CHEK2 , ATM , and FANCJ/BRIP1 , function in DNA repair, raising the possibility that germ line mutations in other genes that contribute to this process also predispose to breast cancer. Given its close relationship with BRCA2 , PALB2 was sequenced in affected probands from 68 BRCA1/BRCA2 -negative breast cancer families of Ashkenazi Jewish, French Canadian, or mixed ethnic descent. The average BRCAPRO score was 0.58. A truncating mutation (229delT) was identified in one family with a strong history of breast cancer (seven breast cancers in three female mutation carriers). This mutation and its associated breast cancers were characterized with another recently reported but unstudied mutation (2521delA) that is also associated with a strong family history of breast cancer. There was no loss of heterozygosity in tumors with either mutation. Moreover, comparative genomic hybridization analysis showed major similarities to that of BRCA2 tumors but with some notable differences, especially loss of 18q, a change that was previously unknown in BRCA2 tumors and less common in sporadic breast cancer. This study supports recent observations that PALB2 mutations are present, albeit not frequently, in breast cancer families. The apparently high penetrance noted in this study suggests that at least some PALB2 mutations are associated with a substantially increased risk for the disease.

Published

2007

142. Global analysis of chromosome X gene expression in primary cultures of normal ovarian surface epithelial cells and epithelial ovarian cancer cell lines

Author

Anne-Marie Mes-Masson, Suzanna L. Arcand, Thomas J. Hudson, Jeremy A. Squire, Marie-Hélène Benoît, Diane Provencher, Georges Maire, and Patricia N. Tonin

Subjects

Transcriptome, Loss of heterozygosity, Genetics, Cancer Research, Oncology, Barr body, Gene duplication, XIST, Biology, Skewed X-inactivation, Molecular biology, X chromosome, X-inactivation

Abstract

The interpretation of loss of heterozygosity (LOH) in cancers is complicated as genes that map to LOH regions may be transcriptionally active (Xa) or inactive (Xi) due to X chromosome inactivation (XCI). We have analyzed the chromosome X transcriptome in four epithelial ovarian cancer (EOC) cell lines (TOV21G, TOV8 ID, TOV112D, and OV90) and 12 primary cultures of normal ovarian surface epithelial (NOSE) cells in relation to chromosome X integrity. Two-way comparative analysis using HuGeneFL Affymetrix GeneChips® of TOV21G, TOV81D and OV90 relative to the NOSE samples was highly correlated (>89%) in contrast to that of TOV112D (56-69%). TOV112D, followed by TOV21G, exhibited the largest number of up-regulated genes. XIST expression by RT-PCR was not detectable in TOV112D or TOV21G. Allele-specific transcription by cDNA sequence analysis of genes known to be subjected to XCI revealed maintenance of XCI in TOV81D and OV90, but not TOV21G. Biallelic expression could not be assessed in TOV112D due to reduction to hemizygosity of chromosome X. Chromosome X rearrangements were observed in FISH analysis of TOV112D and TOV21G, and both of these EOC cell lines were negative for Barr body analysis. The differentially expressed genes did not appear to map to any particular region of the X chromosome in any EOC cell line. The absence of XIST expression is consistent with Barr body loss in TOV112D and TOV21G. The combined evidence is consistent with two proposed mechanisms to account for absence of Xi in female cancers: Xi loss followed by Xa duplication (exemplified by TOV112D) and transcriptional reactivation of Xi (exemplified by TOV21G). Despite an alteration in XIST expression and differences in allelic content in the EOC cell lines, the chromosome X transcriptome was modified modestly when compared with that of NOSE samples.

Published

2007

143. Abstract POSTER-TECH-1101: Characterization of genomic landscapes of BRCA1 and BRCA2 implicated ovarian cancer specimens from a founder french canadian population

Author

Celia M. T. Greenwood, Eman AlShehri, Patricia N. Tonin, Kathleen Klein Oros, Moria H Belanger, and Suzanna L. Arcand

Subjects

Genetics, Cancer Research, education.field_of_study, endocrine system diseases, Population, Biology, medicine.disease, Genome, Germline, Oncology, Genotype, medicine, Missense mutation, skin and connective tissue diseases, Ovarian cancer, education, TP53 Gene Mutation, Founder effect

Abstract

Although molecular genetic profiling of ovarian cancers harboring germline BRCA1/BRCA2 mutations suggest that pathways in common with sporadic cases are involved in the pathogenesis of the disease, overall survival differs between BRCA1, BRCA2 and sporadic disease. To further dissect molecular pathways involved, which could account for differences in pathogenesis of the disease, we have investigated genomic landscapes in the BRCA1 and BRCA2 mutated ovarian cancers. Chromosomal anomalies were assessed in 28 specimens with BRCA1 (n=15), BRCA2 (n=12) or BRCA1 and BRCA2 (n=1) mutations using high-density Illumina SNP arrays. The majority (22/28) are serous adenocarcinomas while the remaining samples were either endometroid (2/28) or mixed adenocarcinomas (4/28). The cases harbor BRCA1/BRCA2 mutations from a French Canadian population, which exhibit strong founder effects. Allelic imbalance, copy number differences, intrachromosomal breaks and homozygous deletions were inferred visually using the Genome Viewer module of the BeadStudio software followed by ASCAT analysis. A statistical analysis was used to directly compare genotypes of BRCA1 versus BRCA2 positive samples. TP53 gene mutation status was also assessed. All samples were found to harbor a somatic TP53 mutation comprised of missense (19/28), nonsense (2/28), frame-shift (4/28) and (3/28) splice mutations. The results were compared to independently derived data generated previously from our group, which was largely comprised of sporadic cases (Wojnarowicz et al 2012), and to the genomic data from the Cancer Genome Atlas project (TCGA). The genomic landscapes of BRCA1 and BRCA2 mutated cancers overlap those reported in previous studies. However, there were significant differences in the genomic landscapes involving chromosome 6q between BRCA1 and BRCA2 mutation-positive cancers. This genomic distinction between BRCA1 and BRCA2 ovarian cancer samples may point to a region containing genes important in the etiology or progression of hereditary cancer. Citation Format: Eman AlShehri, Moria Belanger, Suzanna Arcand, Kathleen Klein Oros, Celia Greenwood, Patricia N. Tonin. Characterization of genomic landscapes of BRCA1 and BRCA2 implicated ovarian cancer specimens from a founder french canadian population [abstract]. In: Proceedings of the 10th Biennial Ovarian Cancer Research Symposium; Sep 8-9, 2014; Seattle, WA. Philadelphia (PA): AACR; Clin Cancer Res 2015;21(16 Suppl):Abstract nr POSTER-TECH-1101.

Published

2015

144. Global analysis of chromosome X gene expression in primary cultures of normal ovarian surface epithelial cells and epithelial ovarian cancer cell lines

Author

Marie-Hélène, Benoît, Thomas J, Hudson, Georges, Maire, Jeremy A, Squire, Suzanna L, Arcand, Diane, Provencher, Anne-Marie, Mes-Masson, and Patricia N, Tonin

Subjects

Ovarian Neoplasms, Chromosomes, Human, X, Transcription, Genetic, Reverse Transcriptase Polymerase Chain Reaction, Ovary, Chromosome Mapping, Epithelial Cells, Gene Expression Regulation, Neoplastic, Gene Expression Regulation, Cell Line, Tumor, Humans, RNA, Female, RNA, Neoplasm, Cells, Cultured, Oligonucleotide Array Sequence Analysis

Abstract

The interpretation of loss of heterozygosity (LOH) in cancers is complicated as genes that map to LOH regions may be transcriptionally active (Xa) or inactive (Xi) due to X chromosome inactivation (XCI). We have analyzed the chromosome X transcriptome in four epithelial ovarian cancer (EOC) cell lines (TOV21G, TOV81D, TOV112D, and OV90) and 12 primary cultures of normal ovarian surface epithelial (NOSE) cells in relation to chromosome X integrity. Two-way comparative analysis using HuGeneFL Affymetrix GeneChips of TOV21G, TOV81D and OV90 relative to the NOSE samples was highly correlated (89%) in contrast to that of TOV112D (56-69%). TOV112D, followed by TOV21G, exhibited the largest number of up-regulated genes. XIST expression by RT-PCR was not detectable in TOV112D or TOV21G. Allele-specific transcription by cDNA sequence analysis of genes known to be subjected to XCI revealed maintenance of XCI in TOV81D and OV90, but not TOV21G. Biallelic expression could not be assessed in TOV112D due to reduction to hemizygosity of chromosome X. Chromosome X rearrangements were observed in FISH analysis of TOV112D and TOV21G, and both of these EOC cell lines were negative for Barr body analysis. The differentially expressed genes did not appear to map to any particular region of the X chromosome in any EOC cell line. The absence of XIST expression is consistent with Barr body loss in TOV112D and TOV21G. The combined evidence is consistent with two proposed mechanisms to account for absence of Xi in female cancers: Xi loss followed by Xa duplication (exemplified by TOV112D) and transcriptional reactivation of Xi (exemplified by TOV21G). Despite an alteration in XIST expression and differences in allelic content in the EOC cell lines, the chromosome X transcriptome was modified modestly when compared with that of NOSE samples.

Published

2006

145. Application of BRCA1 and BRCA2 mutation carrier prediction models in breast and/or ovarian cancer families of French Canadian descent

Author

Anne Marie Mes-Masson, Yosabeth Paredes, Kathleen Klein Oros, Christine Maugard, William D. Foulkes, Chantal Perret, D. Provencher, Patricia N. Tonin, and Parviz Ghadirian

Subjects

Oncology, Male, medicine.medical_specialty, Canada, Genetic counseling, Breast Neoplasms, Breast Neoplasms, Male, Germline mutation, Breast cancer, Mutation Carrier, Internal medicine, Genetics, medicine, Humans, Genetic Predisposition to Disease, skin and connective tissue diseases, Genetics (clinical), Germ-Line Mutation, Genetic testing, Probability, BRCA2 Protein, Ovarian Neoplasms, medicine.diagnostic_test, Models, Genetic, business.industry, BRCA1 Protein, Quebec, Cancer, Middle Aged, medicine.disease, BRCA2 Mutation Carrier, Pedigree, ROC Curve, Male breast cancer, Female, business

Abstract

The BRCAPRO, Couch, Myriad I and II, Ontario Family History Assessment Tool (FHAT), and Manchester models have been used to predict BRCA1 or BRCA2 mutation carrier status of women at high risk for developing the heritable form of breast and ovarian cancers. We have evaluated these models for their accuracy in classifying 224 French Canadian families with at least three cases of breast cancer (diagnosed before the age of 65 years), ovarian cancer, or male breast cancer where mutation status was known for an index affected case used to assess the model. This series includes 44 BRCA1 and 52 BRCA2 mutation-positive families. Using receiver operator characteristics analyses, the C-statistics were found to be 0.81, 0.80, 0.79, and 0.74 for the BRCAPRO, FHAT, Manchester, and Myriad II models, respectively, when incorporating both BRCA1 and BRCA2 mutation carrier predictions. For the BRCAPRO model, 75% scored greater than a 0.43 probability in the mutation-positive group and 75% scored less than 0.50 in the mutation-negative group. Only 38 of 128 (30%) mutation-negative group had a probability greater than 0.43 with the BRCAPRO model. While all models were highly predictive of carrier status, the BRCAPRO model was the most accurate where a cut-off of 10% would have eliminated 60 of 128 (47%) mutation-negative families for genetic testing and only miss 10 of 96 (10%) mutation-positive families. A review of the cancer phenotypes with high BRCAPRO probabilities showed that significantly more metachronous bilateral breast cancer cases occurred in BRCA1/2 mutation carrier families in comparison to mutation-negative families, a feature which is not discriminated in the BRCAPRO model.

Published

2006

146. Transfer of chromosome 3 fragments suppresses tumorigenicity of an ovarian cancer cell line monoallelic for chromosome 3p

Author

Mario Chevrette, Veronique Ouellet, P. Tellis, D. Provencher, Emily N. Manderson, A. Filali-Mouhim, Magdalena Zietarska, Michael C.J. Quinn, Neal A.L. Cody, Anne Marie Mes-Masson, and Patricia N. Tonin

Subjects

Cancer Research, Tumor suppressor gene, Chromosome Transfer, Mice, Nude, Biology, Adenocarcinoma, medicine.disease_cause, Loss of heterozygosity, Transcriptome, Mice, Cell Line, Tumor, Genetics, medicine, Animals, Humans, Genes, Tumor Suppressor, Molecular Biology, Chromosome Aberrations, Ovarian Neoplasms, Microarray analysis techniques, Gene Expression Profiling, Gene Transfer Techniques, medicine.disease, Xenograft Model Antitumor Assays, Chromosome 3, Cancer research, Female, Chromosomes, Human, Pair 3, Ovarian cancer, Carcinogenesis

Abstract

Multiple chromosome 3p tumor suppressor genes (TSG) have been proposed in the pathogenesis of ovarian cancer based on complex patterns of 3p loss. To attain functional evidence in support of TSGs and identify candidate regions, we applied a chromosome transfer method involving cell fusions of the tumorigenic OV90 human ovarian cancer cell line, monoallelic for 3p and an irradiated mouse cell line containing a human chromosome 3 in order to derive OV90 hybrids containing normal 3p fragments. The resulting hybrids showed complete or incomplete suppression of tumorigenicity in nude mouse xenograft assays, and varied in their ability to form colonies in soft agarose and three-dimensional spheroids in a manner consistent with alteration of their in vivo tumorigenic phenotypes. Expression microarray analysis identified a set of common differentially expressed genes, such as SPARC, DAB2 and VEGF, some of which have been shown implicated in ovarian cancer. Genotyping assays revealed that they harbored normal 3p fragments, some of which overlapped candidate TSG regions (3p25-p26, 3p24 and 3p14-pcen) identified previously in loss of heterozygosity analyses of ovarian cancers. However, only the 3p12-pcen region was acquired in common by all hybrids where expression microarray analysis identified differentially expressed genes. The correlation of 3p12-pcen transfer and tumor suppression with a concerted re-programming of the cellular transcriptome suggest that the putative TSG may have affected key underlying events in ovarian cancer.

Published

2006

147. SET complex in serous epithelial ovarian cancer

Author

Véronique, Ouellet, Cécile, Le Page, Marie-Claude, Guyot, Christian, Lussier, Patricia N, Tonin, Diane M, Provencher, and Anne-Marie, Mes-Masson

Subjects

Adult, Male, Ovarian Neoplasms, Chromosomal Proteins, Non-Histone, Carcinoma, Middle Aged, Immunohistochemistry, Survival Analysis, Disease-Free Survival, DNA-Binding Proteins, Humans, Female, Histone Chaperones, Aged, Neoplasm Staging, Transcription Factors

Abstract

With low cure rates but increasing diverse treatment options that provide variable remission times, ovarian cancer is increasingly being recognized as a chronic disease. This reality indicates the need for a better understanding of factors influencing disease progression. In a previous global analysis of gene expression, we identified genes differentially expressed when comparing serous epithelial ovarian tumors of low and high malignant potential (grade 0 vs grade 3). In this analysis, 4 out of 5 members of the SET complex, SET, APE1, NM23 and HMGB2, were highly expressed in invasive grade 3 tumors. To further investigate the expression of these genes and the fifth member of the SET complex (pp32), we performed immunohistochemistry, on a tissue array composed of 235 serous tumors of different grades and disease stages. A significant correlation between expression of all SET complex proteins and the tumor differentiation was observed (p0.05). When combining all tumors, overexpression of Nm23 (p = 0.04), Set (p = 0.004) and Ape1 (p = 0.004) was associated with the clinical stage of the disease. No marker by itself was associated with prognosis. The combination of a high level of Nm23 in the context of a low level of Set compared to all other combinations of these markers did confer a better prognosis (p = 0.03). When combined, high expression of Hmgb2 and low expression of Ape1 was also associated with patient prognosis (p = 0.05). These findings suggest that a strategy that sums the activities of different partners within a pathway may be more appropriate in designing nomograms for patient stratification.

Published

2006

148. [The limited spectrum of pathogenic BRCA1 and BRCA2 mutations in the French Canadian breast and breast-ovarian cancer families, a founder population of Quebec, Canada]

Author

Patricia N, Tonin

Subjects

Ovarian Neoplasms, Genes, BRCA2, Age Factors, Genes, BRCA1, Quebec, Breast Neoplasms, Emigration and Immigration, Founder Effect, Mutation, Humans, Family, Female, Genetic Predisposition to Disease, France, Germ-Line Mutation

Abstract

The unique genetic demography of the French Canadian population of Quebec, Canada, has provided a means to study the contribution of BRCA1 and BRCA2, the breast-ovarian cancer susceptibility genes. Here we review BRCA1 and BRCA2 in the context of French Canadian cancer families, a well-characterized founder population known for its contributions to medical genetics. Pathogenic BRCA1 and BRCA2 mutations contribute to a significant proportion of hereditary breast and/or ovarian cancer families of French Canadian descent. BRCA1 and BRCA2 mutations have been reported in approximately 40 % of families with at least three cases of breast and/or ovarian cancer, where breast cancer diagnosis occurred before age 66 years, and where all cases occurred within first-, second- and/or third-degree relatives to index affected cases tested for mutations. The proportion of mutation-positive families was very similar to that reported in independent studies of families not selected for ethnicity. However, 84 % of mutation-positive families were accounted for by one of eight pathogenic mutations in BRCA1 (2953delGTA + C, 3875delGTCT, and 4446C --T) and BRCA2 (2816insA, 3398delAAAAG, 6085G --T, 6503delTT, and 8765delAG). Haplotype analyses has suggested that carriers of the most common recurring mutations share a related ancestry. This effect has been attributed to common founders in the French Canadian population of Quebec who emigrated from France in between 1608 and 1759. It is possible that novel highly penetrant cancer susceptibility genes account for a fraction of the 60 % of BRCA mutation-negative French Canadian cancer families. The continued genetic analysis and phenotypic characterization of French Canadian cancer families is warranted given the large family structure of these families are amenable for classical genome-wide linkage analysis for novel breast and ovarian cancer susceptibility genes.

Published

2006

149. OGG1 Cys326 variant, allelic imbalance of chromosome band 3p25.3 and TP53 mutations in ovarian cancer

Author

Patricia N. Tonin, Diane Provencher, Suzanna L. Arcand, and Anne-Marie Mes-Masson

Subjects

Genetics, Cancer Research, endocrine system diseases, Tumor suppressor gene, Cancer, Locus (genetics), Biology, medicine.disease, Loss of heterozygosity, Oncology, Allelic Imbalance, Genotype, medicine, Ovarian cancer, Gene

Abstract

A Ser326Cys amino acid variant encoded by OGG1 that removes the highly mutagenic 8-oxo-7,8-dihydroguanine adducts resulting from the oxidative damage produced by reactive oxygen species, has been suggested to reduce activity of the enzyme and result in an increase in G:C --> T:A transversions. Carriers homozygous for the Cys326 variant have been associated with increased risk in some cancers. In this study, we tested the association of this polymorphism with epithelial ovarian cancer (EOC) (n=91 cases) in comparison with women unaffected by the disease (n=57). Although the genotype encoding the homozygous Cys326 variant was found more often in cases (11%) than controls (9%), this was not statistically significant (p=0.297). As OGG1 at chromosome band 3p25.3 overlaps a region exhibiting allelic imbalance (AI) in EOC, we also examined the frequency of AI of the OGG1 locus and its association with somatic mutations in the TP53 tumor suppressor gene, which is frequently mutated in EOC. The frequency of AI and TP53 mutations in EOC was 32 and 37%, respectively. Although the proportion of EOC cases harboring the genotype homozygous for Cys326 was greater in TP53 mutation-positive cases (5 of 34, 15%) than mutation-negative cases (5 of 57, 9%), the distribution of genotypes was not significantly different (p=0.289). Four of the six heterozygous Ser326/Cys326 samples exhibiting AI, displayed loss of the Ser326 variant. About 16% of samples exhibited both AI of the OGG1 locus and a TP53 mutation. Proportionately more EOC samples harbored a mutation in the group of samples exhibiting AI (15 of 29, 52%) in comparison to the group of samples with no AI (19 of 62, 31%) (p=0.036). Although the OGG1 Cys326 variant appears to play a minor role in conferring increased risk of ovarian cancer, the observed AI of the OGG1 locus in association with TP53 somatic mutations warrants further investigation in this disease.

Published

2005

150. From gene profiling to diagnostic markers: IL-18 and FGF-2 complement CA125 as serum-based markers in epithelial ovarian cancer

Author

Jason Madore, Diane Provencher, Cécile Le Page, Anne-Marie Mes-Masson, Veronique Ouellet, Thomas J. Hudson, and Patricia N. Tonin

Subjects

Cancer Research, Pathology, medicine.medical_specialty, endocrine system diseases, medicine.medical_treatment, Enzyme-Linked Immunosorbent Assay, Biology, Polymerase Chain Reaction, Sensitivity and Specificity, Epithelium, Ovarian disease, Predictive Value of Tests, Gene expression, medicine, Biomarkers, Tumor, Humans, Prospective cohort study, Oligonucleotide Array Sequence Analysis, Ovarian Neoplasms, Gene Expression Profiling, Ovary, Interleukin-18, medicine.disease, female genital diseases and pregnancy complications, Real-time polymerase chain reaction, Cytokine, Oncology, CA-125 Antigen, Case-Control Studies, Immunohistochemistry, Interleukin 18, Female, Fibroblast Growth Factor 2, Ovarian cancer

Abstract

We used an oligonucleotide-based DNA microarray to identify potential markers in 39 primary cultures of ovarian cancer specimens compared with 11 primary cultures of normal ovarian epithelia. Differential gene expression of IL-18 and FGF-2 was validated on a subset of samples by quantitative PCR and by IHC, using an independent tissue array of 90 cores of 20 normal ovarian surface epithelia and 70 EOCs representing different grades and pathologies of ovarian disease. We further compared, by ELISA, these two markers with CA125 in sera from 25 cancer-free and 47 ovarian cancer patients. IL-18 and FGF-2 proteins were significantly elevated in tumor tissues (p

Published

2005