Your search keyword '"Sylvie Giroux"' showing total 55 results

1. Investigating the causal role of MRE11A p.E506* in breast and ovarian cancer

Author

Islam E. Elkholi, Massimo Di Iorio, Somayyeh Fahiminiya, Suzanna L. Arcand, HyeRim Han, Clara Nogué, Supriya Behl, Nancy Hamel, Sylvie Giroux, Manon de Ladurantaye, Olga Aleynikova, Walter H. Gotlieb, Jean-François Côté, François Rousseau, Patricia N. Tonin, Diane Provencher, Anne-Marie MesMasson, Mohammad R. Akbari, Barbara Rivera, and William D. Foulkes

Subjects

Medicine, Science

Abstract

Abstract The nuclease MRE11A is often included in genetic test panels for hereditary breast and ovarian cancer (HBOC) due to its BRCA1-related molecular function in the DNA repair pathway. However, whether MRE11A is a true predisposition gene for HBOC is still questionable. We determined to investigate this notion by dissecting the molecular genetics of the c.1516G > T;p.E506* truncating MRE11A variant, that we pinpointed in two unrelated French-Canadian (FC) HBOC patients. We performed a case–control study for the variant in ~ 2500 breast, ovarian, and endometrial cancer patients from the founder FC population of Quebec. Furthermore, we looked for the presence of second somatic alterations in the MRE11A gene in the tumors of the carriers. In summary, these investigations suggested that the identified variant is not associated with an increased risk of developing breast or ovarian cancer. We finally performed a systematic review for all the previously reported MRE11A variants in breast and ovarian cancer. We found that MRE11A germline variants annotated as pathogenic on ClinVar often lacked evidence for such classification, hence misleading the clinical management for affected patients. In summary, our report suggests the lack of clinical utility of MRE11A testing in HBOC, at least in the White/Caucasian populations.

Published

2021

2. Improving Fetal Fraction of Noninvasive Prenatal Screening Samples Collected in EDTA-Gel Tubes Using Gel Size Selection

Author

Seyedeh S. Daryabari, Sylvie Giroux, André Caron, Briana Chau, Sylvie Langlois, and François Rousseau

Subjects

Molecular Medicine, Pathology and Forensic Medicine

Published

2022

3. Supplementary Table 2 from Functionally Null RAD51D Missense Mutation Associates Strongly with Ovarian Carcinoma

Author

William D. Foulkes, Alexandre Orthwein, Patricia N. Tonin, Christopher J. Lord, Mohammad R. Akbari, Steven A. Narod, Reiner Siebert, Susanne Bens, Jacek Majewski, Anne-Marie Mes-Masson, Jacques L. Michaud, Guy A. Rouleau, Diane Provencher, Albert M. Berghuis, Francois Rousseau, George Zogopoulos, Alexandre Dionne-Laporte, Fadi F. Hamdan, Sylvie Giroux, Olga Aleynikova, Rabea Wagener, Nancy Hamel, Valerie Hastings, Eva Tomiak, Damien Grapton, David L. Burk, Suzanna L. Arcand, Somayyeh Fahiminiya, Javad Nadaf, Jessica Frankum, Massimo Di Iorio, and Barbara Rivera

Abstract

'Supplementary Table S2- Somatic mutations identified in the tumors from individuals III.6; III.7 and III.8 in family 1 and individual III.1 in family 2 among 193 DNA repair genes.'

Published

2023

4. Supplementary Tables and Figures from Functionally Null RAD51D Missense Mutation Associates Strongly with Ovarian Carcinoma

Author

William D. Foulkes, Alexandre Orthwein, Patricia N. Tonin, Christopher J. Lord, Mohammad R. Akbari, Steven A. Narod, Reiner Siebert, Susanne Bens, Jacek Majewski, Anne-Marie Mes-Masson, Jacques L. Michaud, Guy A. Rouleau, Diane Provencher, Albert M. Berghuis, Francois Rousseau, George Zogopoulos, Alexandre Dionne-Laporte, Fadi F. Hamdan, Sylvie Giroux, Olga Aleynikova, Rabea Wagener, Nancy Hamel, Valerie Hastings, Eva Tomiak, Damien Grapton, David L. Burk, Suzanna L. Arcand, Somayyeh Fahiminiya, Javad Nadaf, Jessica Frankum, Massimo Di Iorio, and Barbara Rivera

Abstract

This file includes supplementary Figure S1, Supplementary Figure S2 and Supplementary Figure S3. It also includes Supplementary Table S1 - RAD51D c.620C

Published

2023

5. Supplementary Table 3 from Functionally Null RAD51D Missense Mutation Associates Strongly with Ovarian Carcinoma

Author

William D. Foulkes, Alexandre Orthwein, Patricia N. Tonin, Christopher J. Lord, Mohammad R. Akbari, Steven A. Narod, Reiner Siebert, Susanne Bens, Jacek Majewski, Anne-Marie Mes-Masson, Jacques L. Michaud, Guy A. Rouleau, Diane Provencher, Albert M. Berghuis, Francois Rousseau, George Zogopoulos, Alexandre Dionne-Laporte, Fadi F. Hamdan, Sylvie Giroux, Olga Aleynikova, Rabea Wagener, Nancy Hamel, Valerie Hastings, Eva Tomiak, Damien Grapton, David L. Burk, Suzanna L. Arcand, Somayyeh Fahiminiya, Javad Nadaf, Jessica Frankum, Massimo Di Iorio, and Barbara Rivera

Abstract

'Supplementary Table3 -Presence of allelic imbalanced alleles in RAD51D and TP53 somatic mutations in RAD51D c.620C>T;p.S207L HGSC carriers.'

Published

2023

6. Data from Functionally Null RAD51D Missense Mutation Associates Strongly with Ovarian Carcinoma

Author

William D. Foulkes, Alexandre Orthwein, Patricia N. Tonin, Christopher J. Lord, Mohammad R. Akbari, Steven A. Narod, Reiner Siebert, Susanne Bens, Jacek Majewski, Anne-Marie Mes-Masson, Jacques L. Michaud, Guy A. Rouleau, Diane Provencher, Albert M. Berghuis, Francois Rousseau, George Zogopoulos, Alexandre Dionne-Laporte, Fadi F. Hamdan, Sylvie Giroux, Olga Aleynikova, Rabea Wagener, Nancy Hamel, Valerie Hastings, Eva Tomiak, Damien Grapton, David L. Burk, Suzanna L. Arcand, Somayyeh Fahiminiya, Javad Nadaf, Jessica Frankum, Massimo Di Iorio, and Barbara Rivera

Abstract

RAD51D is a key player in DNA repair by homologous recombination (HR), and RAD51D truncating variant carriers have an increased risk for ovarian cancer. However, the contribution of nontruncating RAD51D variants to cancer predisposition remains uncertain. Using deep sequencing and case–control genotyping studies, we show that in French Canadians, the missense RAD51D variant c.620C>T;p.S207L is highly prevalent and is associated with a significantly increased risk for ovarian high-grade serous carcinoma (HGSC; 3.8% cases vs. 0.2% controls). The frequency of the p.S207L variant did not significantly differ from that of controls in breast, endometrial, pancreas, or colorectal adenocarcinomas. Functionally, we show that this mutation impairs HR by disrupting the RAD51D–XRCC2 interaction and confers PARP inhibitor sensitivity. These results highlight the importance of a functional RAD51D–XRCC2 interaction to promote HR and prevent the development of HGSC. This study identifies c.620C>T;p.S207L as the first bona fide pathogenic RAD51D missense cancer susceptibility allele and supports the use of targeted PARP-inhibitor therapies in ovarian cancer patients carrying deleterious missense RAD51D variants. Cancer Res; 77(16); 4517–29. ©2017 AACR.

Published

2023

7. Validation of a New Protocol to Collect and Isolate Plasma from Pregnant Women for Noninvasive Prenatal Testing (NIPT)

Author

André Caron, Joël Girouard, Sylvie Giroux, Julie Jeuken, Mylène Badeau, and François Rousseau

Subjects

0301 basic medicine, Materials science, Noninvasive Prenatal Testing, law.invention, 03 medical and health sciences, 0302 clinical medicine, Pregnancy, law, Humans, Centrifugation, Filtration, Syringe, Blood Specimen Collection, 030219 obstetrics & reproductive medicine, Chromatography, Significant difference, Pipette, High-Throughput Nucleotide Sequencing, General Medicine, CELL DEBRIS, 030104 developmental biology, Female, Pregnant Women, Sample collection, Cell-Free Nucleic Acids, Blood sampling

Abstract

Background Most laboratories use specialized tubes (e.g., Streck) to recover circulating cell-free DNA (ccfDNA) for noninvasive prenatal testing (NIPT). We validated a low cost, simple procedure for collecting NIPT samples in remote laboratories that avoids highspeed centrifugation. EDTA gel blood sampling tube allows simple separation of plasma from blood cells. Decanted plasma is filtered to remove cell debris. The procedure can be performed within a few minutes after the blood centrifugation step, and ccfDNA-grade plasma can be frozen for transportation. Methods We recruited 51 pregnant women and collected blood in one EDTA-gel Greiner tube and two Streck tubes. All tubes were centrifuged at 1600 g x 10 min within 6 h of sample collection. Plasma from EDTA tubes was poured into a syringe cylinder and filtered through a 0.45 µm Millipore filter. Plasma from Streck tubes was recovered with a pipette and one was filtered as above while the second was centrifuged at 16 000 g. The ccfDNA was isolated and NGS sequencing libraries were prepared and sequenced on an Illumina system. Fetal fractions were estimated using SeqFF. This study had a power of 79% to detect a decrease of 1% in fetal fractions with the new method. Results We did not observe any significant difference between the three procedures for the fetal fraction nor for the quality or quantity of libraries produced. Conclusion EDTA-gel tubes with filtration provide high quality plasma for ccfDNA analysis and can be sent frozen to the NIPT laboratory. This is economical and it frees the laboratory of time-consuming steps.

Published

2020

8. Effect of preexamination conditions in a centralized-testing model of non-invasive prenatal screening

Author

Aly Karsan, François Rousseau, Guy A. Rouleau, André Caron, Lucas Swanson, Sylvie Langlois, Chad Fibke, Sylvie Giroux, Elizabeth Starks, Jeremy Parker, and Loubna Jouan

Subjects

Male, medicine.medical_specialty, Clinical Biochemistry, Aneuploidy, Trisomy, Pregnancy, Prenatal Diagnosis, Linear regression, medicine, Humans, Mass index, Imputation (statistics), Fetus, business.industry, Obstetrics, Biochemistry (medical), Confounding, Gestational age, General Medicine, medicine.disease, Female, Down Syndrome, business, Cell-Free Nucleic Acids, Trisomy 18 Syndrome

Abstract

Objectives Non-invasive prenatal testing requires the presence of fetal DNA in maternal plasma. Understanding how preexamination conditions affect the integrity of cell-free DNA (cfDNA) and fetal fraction (FF) are a prerequisite for test implementation. Therefore, we examined the adjusted effect that EDTA and Streck tubes have on the cfDNA quantity and FF. Methods A total of 3,568 maternal blood samples across Canada were collected in either EDTA, or Streck tubes, and processing metrics, maternal body mass index (BMI), gestational age and fetal karyotype and sex were recorded. Plasma samples were sequenced using two different sequencing platforms in separate laboratories. Sequencing data were processed with SeqFF to estimate FF. Linear regression and multivariate imputation by chained equations were used to estimate the adjusted effect of tube type on cfDNA and FF. Results We found a positive association between cfDNA quantity and blood shipment time in EDTA tubes, which is significantly reduced with the use of Streck tubes. Furthermore, we show the storage of plasma at −80 °C is associated with a 4.4% annual relative decrease in cfDNA levels. FF was not associated with collection tube type when controlling for confounding variables. However, FF was positively associated with gestational age and trisomy 21, while negatively associated with BMI, male fetus, trisomy 18, Turners syndrome and triploidy. Conclusions Preexamination, maternal and fetal variables are associated with cfDNA quantity and FF. The consideration of these variables in future studies may help to reduce the number of pregnant women with inconclusive tests as a result of low FF.

Published

2021

9. Development of Reference Materials for Noninvasive Prenatal Aneuploidy Testing by Massively Parallel Sequencing: A Proof-of-Concept Study

Author

André Caron, Sylvie Giroux, Valérie Clément, Jonatan Blais, and François Rousseau

Subjects

Adult, 0301 basic medicine, Noninvasive Prenatal Testing, Aneuploidy, Computational biology, Biology, Cell Line, Fragment size, 03 medical and health sciences, Fetus, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, medicine, Humans, Multiplex, Volume concentration, 030219 obstetrics & reproductive medicine, Massive parallel sequencing, High-Throughput Nucleotide Sequencing, DNA, General Medicine, medicine.disease, 030104 developmental biology, Feasibility Studies, Female, Down Syndrome

Abstract

Background Noninvasive prenatal aneuploidy testing (NIPT) represents the first large-scale clinical application of massively parallel sequencing technology. However, no NIPT reference material (RM) has yet been widely adopted, impeding the development of quality management systems and standardization. Developing an NIPT RM from a biological sample is complicated by the low concentration of cell-free DNA (cfDNA), which implies pooling specimens and frequent resampling. Methods We tested the feasibility of using DNA from immortalized cell lines of a woman and her aneuploid offspring to spike an artificial plasma matrix. Enzymatic fragmentation of extracted DNA was optimized to achieve fragment size profiles with a mode of 150 to 200 bp, similar to biological cfDNA. This synthetic material was compared with routine biological samples from pregnant women by a targeted NIPT assay in a multiplex sequencing run on a Proton platform. Results Sequencing statistics were similar between artificially prepared material and routine biological samples, as well as relative chromosomal representation, and no matrix effects could be detected. Estimate of fetal fraction (FF) was within the range of expected value, and aneuploidy detection statistic (z-score) was also comparable between both types of samples. Conclusions Artificial plasma spiked with DNA from cell lines of mother and offspring is a promising strategy for developing NIPT RM. This type of material would offer the advantage of a constant and stable composition, allowing for greater standardization of NIPT assays. Moreover, it preserves the parental relatedness used by targeted assay to estimate FF by identification of paternal alleles in single-nucleotide polymorphisms or other variable regions.

Published

2019

10. Investigating the causal role of MRE11A p.E506* in breast and ovarian cancer

Author

Somayyeh Fahiminiya, Olga Aleynikova, Anne-Marie Mes-Masson, Diane Provencher, Barbara Rivera, HyeRim Han, Nancy Hamel, Supriya Behl, Suzanna L. Arcand, Sylvie Giroux, Massimo Di Iorio, Jean-François Côté, François Rousseau, Manon de Ladurantaye, Clara Nogué, Walter H. Gotlieb, Islam E. Elkholi, Patricia N. Tonin, Mohammad R. Akbari, and William D. Foulkes

Subjects

Adult, Oncology, medicine.medical_specialty, Somatic cell, Science, DNA Mutational Analysis, Population, Càncer d'ovari, Breast Neoplasms, Article, Germline, Càncer de mama, Breast cancer, Endometrial cancer, Ovarian cancer, Molecular genetics, Internal medicine, Exome Sequencing, medicine, Humans, Genetic Predisposition to Disease, Clinical genetics, education, Gene, Alleles, Germ-Line Mutation, Ovarian Neoplasms, Gynaecological cancer, MRE11 Homologue Protein, education.field_of_study, Multidisciplinary, business.industry, Quebec, medicine.disease, Pedigree, MRE11A, Càncer d'endometri, Mutation, Medicine, Hereditary Breast and Ovarian Cancer Syndrome, Female, business

Abstract

The nuclease MRE11A is often included in genetic test panels for hereditary breast and ovarian cancer (HBOC) due to its BRCA1-related molecular function in the DNA repair pathway. However, whether MRE11A is a true predisposition gene for HBOC is still questionable. We determined to investigate this notion by dissecting the molecular genetics of the c.1516G > T;p.E506* truncating MRE11A variant, that we pinpointed in two unrelated French-Canadian (FC) HBOC patients. We performed a case–control study for the variant in ~ 2500 breast, ovarian, and endometrial cancer patients from the founder FC population of Quebec. Furthermore, we looked for the presence of second somatic alterations in the MRE11A gene in the tumors of the carriers. In summary, these investigations suggested that the identified variant is not associated with an increased risk of developing breast or ovarian cancer. We finally performed a systematic review for all the previously reported MRE11A variants in breast and ovarian cancer. We found that MRE11A germline variants annotated as pathogenic on ClinVar often lacked evidence for such classification, hence misleading the clinical management for affected patients. In summary, our report suggests the lack of clinical utility of MRE11A testing in HBOC, at least in the White/Caucasian populations.

Published

2021

11. Visibilité des labels et garantie de qualité des sites

Author

Sylvie Giroux, Dominique Masson, and Philippe Orain

Published

2020

12. Non-invasive prenatal aneuploidy testing: Critical diagnostic performance parameters predict sample z-score values

Author

Valérie Clément, Sylvie Giroux, André Caron, Lucas Swanson, Guy A. Rouleau, Tina MacLeod, Richard A. Moore, Sylvie Langlois, François Rousseau, Yongjun Zhao, Aly Karsan, Jonatan Blais, Alexandre Dionne-Laporte, Loubna Jouan, Julie Gauthier, and Jeremy Parker

Subjects

Adult, 0301 basic medicine, Coefficient of variation, Clinical Biochemistry, Population, Aneuploidy, Chromosome Disorders, Prenatal diagnosis, 030105 genetics & heredity, Standard score, 03 medical and health sciences, 0302 clinical medicine, Predictive Value of Tests, Pregnancy, Prenatal Diagnosis, Statistics, medicine, Humans, Genetic Testing, education, Mathematics, Genetic testing, education.field_of_study, 030219 obstetrics & reproductive medicine, medicine.diagnostic_test, High-Throughput Nucleotide Sequencing, Reproducibility of Results, General Medicine, Models, Theoretical, medicine.disease, 3. Good health, Cell-free fetal DNA, Predictive value of tests, Female

Abstract

Non-invasive prenatal aneuploidy testing (NIPT) by next-generation sequencing of circulating cell-free DNA in maternal plasma relies on chromosomal ratio (chrratio) measurements to detect aneuploid values that depart from euploid ratios. Diagnostic performances are known to depend on the fraction of fetal DNA (FF) present in maternal plasma, although how this translates into specific quantitative changes in specificity/positive predictive values and which other variables might also be important is not well understood.To explore this issue, theoretical relationships between FF and various measures of diagnostic performances were assessed for a range of parameter values. Empirical data from three NIPT assays were then used to validate theoretical calculations.For a given positivity threshold, dramatic changes in specificity and positive predictive values (PPV) as a function of both FF and the coefficient of variation (CV) of the chrratio measurement were observed. Theoretically predicted and observed chrratio z-scores agreed closely, confirming the determinant impact of small changes in both FF and chrratio CV.Evaluation of NIPT assay performances therefore requires knowledge of the FF distribution in the population in which the test is intended to be used and, in particular, of the precise value of the assay chrratio CV for each chromosome or genomic region of interest. Laboratories offering NIPT testing should carefully measure these parameters to ensure test reliability and clinical usefulness in interpreting individual patients' results.

Published

2018

13. Functionally Null RAD51D Missense Mutation Associates Strongly with Ovarian Carcinoma

Author

Jacek Majewski, Rabea Wagener, Jacques L. Michaud, Guy A. Rouleau, Patricia N. Tonin, Mohammad R. Akbari, William D. Foulkes, Diane Provencher, Christopher J. Lord, Somayyeh Fahiminiya, Nancy Hamel, Barbara Rivera, Damien Grapton, David L. Burk, Susanne Bens, George Zogopoulos, Massimo Di Iorio, Alexandre Dionne-Laporte, Jessica Frankum, Anne-Marie Mes-Masson, Sylvie Giroux, Steven A. Narod, Suzanna L. Arcand, Olga Aleynikova, Valerie Hastings, Javad Nadaf, François Rousseau, Eva Tomiak, Alexandre Orthwein, Fadi F. Hamdan, Albert M. Berghuis, and Reiner Siebert

Subjects

0301 basic medicine, Cancer Research, education.field_of_study, Serous carcinoma, Population, Cancer, Biology, medicine.disease, Bioinformatics, 03 medical and health sciences, 030104 developmental biology, Germline mutation, Oncology, Ovarian carcinoma, PARP inhibitor, medicine, Cancer research, Missense mutation, Ovarian cancer, education

Abstract

RAD51D is a key player in DNA repair by homologous recombination (HR), and RAD51D truncating variant carriers have an increased risk for ovarian cancer. However, the contribution of nontruncating RAD51D variants to cancer predisposition remains uncertain. Using deep sequencing and case–control genotyping studies, we show that in French Canadians, the missense RAD51D variant c.620C>T;p.S207L is highly prevalent and is associated with a significantly increased risk for ovarian high-grade serous carcinoma (HGSC; 3.8% cases vs. 0.2% controls). The frequency of the p.S207L variant did not significantly differ from that of controls in breast, endometrial, pancreas, or colorectal adenocarcinomas. Functionally, we show that this mutation impairs HR by disrupting the RAD51D–XRCC2 interaction and confers PARP inhibitor sensitivity. These results highlight the importance of a functional RAD51D–XRCC2 interaction to promote HR and prevent the development of HGSC. This study identifies c.620C>T;p.S207L as the first bona fide pathogenic RAD51D missense cancer susceptibility allele and supports the use of targeted PARP-inhibitor therapies in ovarian cancer patients carrying deleterious missense RAD51D variants. Cancer Res; 77(16); 4517–29. ©2017 AACR.

Published

2017

14. Risk of Misdiagnosis Due to Allele Dropout and False-Positive PCR Artifacts in Molecular Diagnostics

Author

Carmen Lindsay, François Rousseau, Sylvie Giroux, Johanne Bussières, Sébastien B. Lavoie, Mélissa Laroche, Yves Giguère, Jonatan Blais, and Jacqueline Dionne

Subjects

Genetics, Biology, Bioinformatics, Molecular diagnostics, 3. Good health, Pathology and Forensic Medicine, Loss of heterozygosity, Polymorphism (computer science), Genotype, Molecular Medicine, Allele, Primer (molecular biology), Genotyping, Dropout (neural networks)

Abstract

Quality control is a complex issue for clinical molecular diagnostic applications. In the case of genotyping assays, artifacts such as allele dropout represent a risk of misdiagnosis for amplification-based methods. However, its frequency of occurrence in PCR-based diagnostic assays remains unknown. To maximize the likelihood of detecting allele dropout, our clinical genotyping PCR-based assays are designed with two independent assays for each allele (nonoverlapping primers on each DNA strand). To estimate the incidence of allelic dropout, we took advantage of the capacity of our clinical assays to detect such events. We retrospectively studied their occurrence in the initial PCR assay for 30,769 patient reports for mutations involved in four diseases produced over 8 years. Ninety-three allele dropout events were detected and all were solved before reporting. In addition, 42 cases of artifacts caused by amplification of an allele ultimately confirmed to not be part of the genotype (drop-in events) were detected and solved. These artifacts affected 1:227 genotypes, 94% of which were due to nonreproducible PCR failures rather than sequence variants interfering with the assay, suggesting that careful primer design cannot prevent most of these errors. This provides a quantitative estimate for clinical laboratories to take this phenomenon into account in quality management and to favor assay designs that can detect (and minimize) occurrence of these artifacts in routine clinical use.

Published

2015

15. Functionally Null

Author

Barbara, Rivera, Massimo, Di Iorio, Jessica, Frankum, Javad, Nadaf, Somayyeh, Fahiminiya, Suzanna L, Arcand, David L, Burk, Damien, Grapton, Eva, Tomiak, Valerie, Hastings, Nancy, Hamel, Rabea, Wagener, Olga, Aleynikova, Sylvie, Giroux, Fadi F, Hamdan, Alexandre, Dionne-Laporte, George, Zogopoulos, Francois, Rousseau, Albert M, Berghuis, Diane, Provencher, Guy A, Rouleau, Jacques L, Michaud, Anne-Marie, Mes-Masson, Jacek, Majewski, Susanne, Bens, Reiner, Siebert, Steven A, Narod, Mohammad R, Akbari, Christopher J, Lord, Patricia N, Tonin, Alexandre, Orthwein, and William D, Foulkes

Subjects

Adult, DNA-Binding Proteins, Ovarian Neoplasms, Genotype, Case-Control Studies, Mutation, Mutation, Missense, Humans, Female, Middle Aged, Polymorphism, Single Nucleotide, Aged, Pedigree

Abstract

RAD51D is a key player in DNA repair by homologous recombination (HR), and

Published

2017

16. Characterization of a novel founderMSH6mutation causing Lynch syndrome in the French Canadian population

Author

A. Roussel-Jobin, Celia M. T. Greenwood, Jean Latreille, Rachel Laframboise, Olga Aleynikova, George Chong, D. Provencher, Lidia Kasprzak, Serge Nolet, Z. El-Haffaf, A. Volenik, Bruno Maranda, Adrian Gologan, K. Oros-Klein, M. Breguet, Marc Tischkowitz, Laura Palma, Victoria Marcus, Anne Marie Mes-Masson, Sylvie Giroux, R. Gagne, K. Australie, William D. Foulkes, François Rousseau, J. Liu, and Ester Castellsagué

Subjects

Proband, Genetics, education.field_of_study, Endometrial cancer, Population, Haplotype, Odds ratio, Biology, medicine.disease, Lynch syndrome, 3. Good health, MSH6, Mutation (genetic algorithm), medicine, education, Genetics (clinical)

Abstract

We identified an MSH6 mutation (c.10C>T, p.Gln4*) causing Lynch syndrome (LS) in 11 French Canadian (FC) families from the Canadian province of Quebec. We aimed to investigate the molecular and clinical implications of this mutation among FC carriers and to assess its putative founder origin. We studied 11 probands and 27 family members. Additionally 6433 newborns, 187 colorectal cancer (CRC) cases, 381 endometrial cancer (EC) cases and 179 additional controls, all of them from Quebec, were used. Found in approximately 1 of 400 newborns, the mutation is one of the most common LS mutations described. We have found that this mutation confers a greater risk for EC than for CRC, both in the 11 studied families and in the unselected cases: EC [odds ratio (OR) = 7.5, p < 0.0001] and CRC (OR = 2.2, p = 0.46). Haplotype analyses showed that the mutation arose in a common ancestor, probably around 430-656 years ago, coinciding with the arrival of the first French settlers. Application of the results of this study could significantly improve the molecular testing and clinical management of LS families in Quebec.

Published

2014

17. Meta-analysis of genome-wide studies identifies WNT16 and ESR1 SNPs associated with bone mineral density in premenopausal women

Author

Kristina Åkesson, Fiona E. McGuigan, John Blangero, Melanie A. Carless, Ching-Ti Liu, Candace M. Kammerer, François Rousseau, Dongbing Lai, Munro Peacock, Audrey C. Choh, Sylvie Giroux, David Karasik, Tatiana Foroud, Beate St Pourcain, Bradford Towne, David M. Evans, Howard J. Edenberg, Jonathan H Tobias, John P. Kemp, Braxton D. Mitchell, Daniel L. Koller, Debbie A Lawlor, J. Brent Richards, Tim D. Spector, George McMahon, David Goltzman, Laura M. Yerges-Armstrong, Jerilynn C. Prior, Christopher S. Kovacs, Stefan A. Czerwinski, Douglas P. Kiel, Michael J. Econs, Nicholas J. Timpson, and Hou-Feng Zheng

Subjects

Oncology, Peak bone mass, musculoskeletal diseases, medicine.medical_specialty, Bone density, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Genome-wide association study, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, Article, 03 medical and health sciences, 0302 clinical medicine, Bone Density, Internal medicine, medicine, SNP, Humans, Orthopedics and Sports Medicine, 030304 developmental biology, Femoral neck, Genetic association, Bone mineral, 0303 health sciences, business.industry, Estrogen Receptor alpha, Wnt Proteins, Endocrinology, medicine.anatomical_structure, Premenopause, Female, business, Genome-Wide Association Study

Abstract

Previous genome-wide association studies (GWAS) have identified common variants in genes associated with variation in bone mineral density (BMD), although most have been carried out in combined samples of older women and men. Meta-analyses of these results have identified numerous single-nucleotide polymorphisms (SNPs) of modest effect at genome-wide significance levels in genes involved in both bone formation and resorption, as well as other pathways. We performed a meta-analysis restricted to premenopausal white women from four cohorts (n=4061 women, aged 20 to 45 years) to identify genes influencing peak bone mass at the lumbar spine and femoral neck. After imputation, age- and weight-adjusted bone-mineral density (BMD) values were tested for association with each SNP. Association of an SNP in the WNT16 gene (rs3801387; p=1.7x109) and multiple SNPs in the ESR1/C6orf97 region (rs4870044; p=1.3x108) achieved genome-wide significance levels for lumbar spine BMD. These SNPs, along with others demonstrating suggestive evidence of association, were then tested for association in seven replication cohorts that included premenopausal women of European, Hispanic-American, and African-American descent (combined n=5597 for femoral neck; n=4744 for lumbar spine). When the data from the discovery and replication cohorts were analyzed jointly, the evidence was more significant (WNT16 joint p=1.3x1011; ESR1/C6orf97 joint p=1.4x1010). Multiple independent association signals were observed with spine BMD at the ESR1 region after conditioning on the primary signal. Analyses of femoral neck BMD also supported association with SNPs in WNT16 and ESR1/C6orf97 (p

Published

2013

18. UGT2B17 gene deletion associated with an increase in bone mineral density similar to the effect of hormone replacement in postmenopausal women

Author

François Rousseau, Alexandre Bureau, Sylvie Giroux, and Johanne Bussières

Subjects

Adult, medicine.medical_specialty, Adolescent, Genotype, Endocrinology, Diabetes and Metabolism, medicine.medical_treatment, Population, Polymerase Chain Reaction, Minor Histocompatibility Antigens, Young Adult, Bone Density, Internal medicine, medicine, Humans, Glucuronosyltransferase, Allele, education, Gene, Aged, Femoral neck, Aged, 80 and over, Bone mineral, education.field_of_study, Lumbar Vertebrae, Femur Neck, business.industry, Estrogen Replacement Therapy, Middle Aged, Postmenopause, Cross-Sectional Studies, medicine.anatomical_structure, Endocrinology, Premenopause, Transgender hormone therapy, Hip bone, Female, Hormone therapy, business, Gene Deletion

Abstract

UGT2B17 is one of the most important enzymes for androgen metabolism. In addition, the UGT2B17 gene is one of the most commonly deleted regions of the human genome. The deletion was previously found associated with higher femoral bone density in men and women, and we replicated this association in a sample of postmenopausal who never used hormone therapy. Deletion of the UGT2B17 gene was previously shown to be associated with a higher hip bone mineral density (BMD). Using a PCR assay, we tried to replicate the association among a large group of 2,379 women. We examined the effect of the deletion on femoral neck BMD and lumbar spine BMD according to the menopausal status and hormone replacement therapy (HRT). We used a high-throughput PCR assay to identify the gene and the deletion in a population of well-characterized women. Two additional polymorphisms, UGT2B28 deletion and UGT2B15 rs1902023 G > T were also investigated. Only UGT2B17 deletion was associated with LS and FN BMD. Furthermore, the association was seen only among postmenopausal women who had never used hormone replacement as in the first reported association. We confirmed the association between UGT2B17 deletion and a higher LS and FN BMD. In addition, we show that the association is observed among postmenopausal women who never used HRT consistent with the enzymatic function of UGT2B17. The analysis shows that those having one or two UGT2B17 alleles benefit from HRT, which is not the case for null carriers.

Published

2011

19. The contribution of founder mutations to early-onset breast cancer in French-Canadian women

Author

Phil Zhang, C Potvin, E. Nassif, Robert Royer, Erica Patocskai, François Rousseau, Ginette Martin, Sylvie Giroux, Parviz Ghadirian, Steven A. Narod, André Robidoux, Shiyu Zhang, Eve Fafard, N Larouche, Rami Younan, M. Costa, Mohammad R. Akbari, and William D. Foulkes

Subjects

Adult, Oncology, medicine.medical_specialty, Population, Breast Neoplasms, Protein Serine-Threonine Kinases, Breast cancer, Internal medicine, Genetics, medicine, Humans, Genetic Predisposition to Disease, Genetic Testing, Age of Onset, skin and connective tissue diseases, education, CHEK2, Genetics (clinical), BRCA2 Protein, education.field_of_study, BRCA1 Protein, business.industry, Tumor Suppressor Proteins, Quebec, Nuclear Proteins, Cancer, Odds ratio, Middle Aged, medicine.disease, Founder Effect, Checkpoint Kinase 2, Mutation, Female, France, Breast disease, Age of onset, Fanconi Anemia Complementation Group N Protein, business, Founder effect

Abstract

In an ethnically-homogeneous population, it is valuable to identify founder mutations in cancer-predisposing genes. Founder mutations have been found in four breast-cancer-predisposing genes in French-Canadian breast cancer families. The frequencies of the mutant alleles have been measured neither in a large series of unselected breast cancer patients from Quebec, nor in healthy controls. These estimates are necessary to measure their contribution to the hereditary burden of breast cancer in Quebec and to help develop genetic screening policies which are appropriate for the province. We studied 564 French-Canadian women with early-onset invasive breast cancer who were treated at a single Montreal hospital. Patients had been diagnosed at age 50 or less, and were ascertained between 2004 and 2008. We screened all 564 patients for nine founder mutations: four in BRCA1, three in BRCA2 and one each in PALB2 and CHEK2. We also studied 6433 DNA samples from newborn infants from the Quebec City area to estimate the frequency of the nine variant alleles in the French-Canadian population. We identified a mutation in 36 of the 564 breast cancer cases (6.4%) and in 35 of 6443 controls (0.5%). In the breast cancer patients, the majority of mutations were in BRCA2 (54%). However, in the general population (newborn infants), the majority of mutations were in CHEK2 (54%). The odds ratio for breast cancer to age 50, given a BRCA1 mutation, was 10.1 (95% CI: 3.7-28) and given a BRCA2 mutation was 29.5 (95% CI: 12.9-67). The odds ratio for breast cancer to age 50, given a CHEK2 mutation, was 3.6 (95% CI: 1.4-9.1). One-half of the women with a mutation had a first- or second-degree relative diagnosed with breast or ovarian cancer. Thus, it can be concluded that a predisposing mutation in BRCA1, BRCA2, CHEK2 or PALB2 is present in approximately 6% of French-Canadian women with early-onset breast cancer. It is reasonable to offer screening for founder mutations to all French-Canadian women with breast cancer before age 50. The frequency of these mutations in the general population (0.5%) is too low to advocate population-based screening.

Published

2009

20. Genes and osteoporosis: time for a change in strategy

Author

Sylvie Giroux and François Rousseau

Subjects

Bone mineral, Peak bone mass, medicine.medical_specialty, education.field_of_study, Bone density, business.industry, Population, Osteoporosis, Physiology, Heritability, medicine.disease, Twin study, Menopause, Endocrinology, Rheumatology, Internal medicine, Medicine, business, education

Abstract

Osteoporosis is characterized by a decrease in bone mass as well as a deterioration of bone architecture, resulting in an increased risk of fracture. Although the disease is multifactorial, twin studies have shown that genetic factors account for up to 80% of the variance in bone mineral density, the best-known predictor of the risk of fractures. These studies have also shown that this high heritability is observed especially in young women (peak bone mass), before bone starts to be lost due to menopause and age. However, studies conducted so far to identify genetic variants modulating bone mass in the general population have focused mainly on women around menopause or older. This approach has likely impeded the discovery of gene variants with effects of small magnitude, which are expected to be numerous. Therefore, the search for gene variants should probably focus on women close to their peak bone mass.

Published

2009

21. Replication of associations between LRP5 and ESRRA variants and bone density in premenopausal women

Author

David E. C. Cole, Latifa Elfassihi, François Rousseau, and Sylvie Giroux

Subjects

Adult, DNA Replication, musculoskeletal diseases, medicine.medical_specialty, Adolescent, Genotype, Bone density, Endocrinology, Diabetes and Metabolism, Osteoporosis, Young Adult, Bone Density, Polymorphism (computer science), Internal medicine, medicine, Humans, LDL-Receptor Related Proteins, Femoral neck, Genetic association, Ontario, Bone mineral, Lumbar Vertebrae, Polymorphism, Genetic, business.industry, Genetic Variation, medicine.disease, Rheumatology, Low Density Lipoprotein Receptor-Related Protein-5, Endocrinology, medicine.anatomical_structure, Premenopause, Receptors, Estrogen, Female, business

Abstract

Replication is a critical step to validate positive genetic associations. In this study, we tested two previously reported positive associations. The low density lipoprotein receptor-related protein 5 (LRP5) Val667Met and lumbar spine bone density are replicated. This result is in line with results from large consortiums such as Genomos. However, the estrogen-related receptor alpha (ESRRA) repeat in the promoter is not replicated although the polymorphism studied was functional and could have been a causative variant. We sought to validate associations previously reported between LRP5 V667M polymorphism and lumbar spine (LS, p = 0.013) and femoral neck (FN, p = 0.0002) bone mineral density (BMD), and between ESRRA 23 base pair repeat polymorphism and LS BMD (p = 0.0036) in a sample of premenopausal Caucasian women using an independent sample. For the replication sample, we recruited 673 premenopausal women from the Toronto metropolitan area. All women were Caucasian and had BMD measured. LRP5 V667M was genotyped by allele-specific PCR and ESRRA repeats by sizing of PCR products on agarose gels. We reproduced the same association as we reported previously between LRP5 V667M and LS BMD (p = 0.015) but not with FN BMD (p = 0.254). The combined data from the two populations indicate an effect size of 0.28SD for LS BMD (p = 0.00048) and an effect size of 0.26 SD for FN BMD (p = 0.00037). In contrast, the association we reported earlier between ESRRA repeats and LS BMD was not replicated in the sample from Toronto (p = 0.645). The association between LRP5 V667M and LS BMD is confirmed but not that between ESRRA repeats and LS BMD. This result indicates that it is imperative to validate any positive association in an independent sample.

Published

2008

22. Assessment of the prevalence of the 985A>G MCAD mutation in the French-Canadian population using allele-specific PCR

Author

Sylvie Giroux, Y Labelle, Nathalie Laflamme, Yves Giguère, A Dubé-Linteau, François Rousseau, and G Cardinal

Subjects

Genotype, Concordance, DNA Mutational Analysis, Population, Biology, Polymerase Chain Reaction, Acyl-CoA Dehydrogenase, Lipid Metabolism, Inborn Errors, law.invention, Gene Frequency, law, Genetics, Humans, Point Mutation, Genetic Testing, Allele, education, Genotyping, Allele frequency, Alleles, Genetics (clinical), Polymerase chain reaction, education.field_of_study, Newborn screening, Infant, Newborn, Quebec, Reproducibility of Results, Mutation (genetic algorithm), France

Abstract

Inherited deficiency of medium-chain acyl-CoA dehydrogenase (MCAD) is a severe, sometimes fatal disorder. A single mutation in the MCAD gene, 985A>G, is involved in approximately 90% of cases. To evaluate the relevance of implementing a systematic population-based screening program in the province of Quebec using a biochemical test, we measured the prevalence of this mutation in a set of anonymous newborn samples from the Quebec City area, a region where the majority of its inhabitants are French-Canadians. An allele-specific polymerase chain reaction assay was designed and used to detect the mutation in 7143 DNA samples obtained from consecutive anonymous newborns. Pools of eight DNA samples were genotyped in parallel for the same mutation to validate this pooling strategy. The allelic frequency of the MCAD 985A>G mutation was found to be 0.71% and the carrier frequency 1:71 (95% confidence interval 1:55 to 1:98). This estimate predicts a homozygous frequency of 1:19,837. Ninety-nine heterozygous carriers and one homozygous individual were identified out of 7143 samples. There was 100% concordance between the individual and pooled analyses, and the pooling strategy reduced the total genotyping costs by approximately 70%. The carrier frequency estimated for this population is similar to other northwestern European populations and would support implementation of systematic newborn screening (such as tandem mass spectrometry screening) for this disease. Pooling DNA samples followed by genotyping appears to be cost-effective for estimating prevalence of rare mutations.

Published

2007

23. A Polymorphic Autoregulatory Hormone Response Element in the Human Estrogen-related Receptor α (ERRα) Promoter Dictates Peroxisome Proliferator-activated Receptor γ Coactivator-1α Control of ERRα Expression

Author

Sylvie Giroux, Vincent Giguère, François Rousseau, Josée Laganière, Gilles Tremblay, and Catherine R. Dufour

Subjects

Canada, DNA Mutational Analysis, Population, Response element, Gene Dosage, Receptors, Cytoplasmic and Nuclear, Peroxisome proliferator-activated receptor, Biology, Response Elements, Biochemistry, Estrogen-related receptor, Estrogen-related receptor alpha, Coactivator, Humans, Genetic Testing, Promoter Regions, Genetic, education, Molecular Biology, Heat-Shock Proteins, Feedback, Physiological, Hormone response element, chemistry.chemical_classification, education.field_of_study, Polymorphism, Genetic, Cell Biology, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Molecular biology, Hormones, Receptors, Estrogen, chemistry, Nuclear receptor, Female, Transcription Factors

Abstract

The orphan nuclear estrogen-related receptor alpha (ERRalpha) and transcriptional cofactor peroxisome proliferator-activated receptor gamma coactivator-1alpha (PGC-1alpha) are involved in the regulation of energy metabolism. Recently, extensive cross-talk between PGC-1alpha and ERRalpha has been demonstrated. The presence of PGC-1alpha is associated with an elevated expression of ERRalpha, and the two proteins can influence the transcriptional activities of one another. Using a candidate gene approach to detect regulatory variants within genes encoding nuclear receptors, we have identified a 23-bp sequence (ESRRA23) containing two nuclear receptor recognition half-site motifs that is present in 1-4 copies within the promoter of the human ESRRA gene encoding ERRalpha. The ESRRA23 sequence contains a functional ERR response element that is specifically bound by ERRalpha, and chromatin immunoprecipitation shows that endogenous ERRalpha occupies its own promoter in vivo. Strikingly, introduction of PGC-1alpha in HeLa cells by transient transfection induces the activity of the ESRRA promoter in a manner that is dependent on the presence of the ESRRA23 element and on its dosage. Coexpression of ERRalpha and PGC-1alpha results in a synergistic activation of the ESRRA promoter. In experiments using ERRalpha null fibroblasts, the ability of PGC-1alpha to stimulate the ESRRA promoter is considerably reduced but can be restored by addition of ERRalpha. Taken together, these results demonstrate that an interdependent ERRalpha/PGC-1alpha-based transcriptional pathway targets the ESRRA23 element to dictate the level of ERRalpha expression. This study further suggests that this regulatory polymorphism may provide differential responses to ERRalpha/PGC-1alpha-mediated metabolic cues in the human population.

Published

2004

24. Abstract 2479: A functionally null RAD51D missense mutation is strongly associated with ovarian carcinoma

Author

Barbara Rivera, Somayyeh Fahiminiya, François Rousseau, Mohammad Esmaeil Akbari, Damien Grapton, Alexandre Orthwein, Massimo Di Iorio, Olga Aleynikova, Valerie Hastings, Anne-Marie Mes-Masson, Guy A. Rouleau, Jacques L. Michaud, Sylvie Giroux, Jessica Frankum, Patricia N. Tonin, George Zogopoulos, William D. Foulkes, Suzanna L. Arcand, Diane Provencher, Christopher J. Lord, David L. Burk, Alexandre Dionne-Laporte, Nancy Hamel, Susanne Bens, Jacek Majewski, Rabea Wagener, Javad Nadaf, Eva Tomiak, Fadi F. Hamdan, Albert M. Berghuis, Reiner Siebert, and Steven A. Narod

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Internal medicine, Ovarian carcinoma, Mutation (genetic algorithm), medicine, Biology

Abstract

Background and goal: RAD51D is a key player in DNA repair by homologous recombination (HR) and carriers of truncating RAD51D mutations have an increased risk for ovarian cancer (OC). However, the contribution of non-truncating RAD51D variants to cancer predisposition remains uncertain. We sought to fully characterize the previously described missense RAD51D variant c.620C>T;p.S207L in order to elucidate its role in OC. Methods: A clinical panel screening was used to identify the RAD51D variant c.620C>T;p.S207L in two French Canadian (FC) kindred affected with familial High Grade Serous Cancer (HGSC) of the ovary or endometrium. High resolution melting, TaqMan genotyping and Sanger sequencing were used to genotype the p.S207L variant in a series of unselected cases of HGSC of the ovary and endometrium, breast, pancreas and colorectal cancer and healthy controls, all of a FC origin. Whole exome sequencing (WES) was performed to study the genetic signature characterizing RAD51D associated tumors. RAD51 foci formation and CRISPR-Cas9-stimulated and HR-mediated gene targeting assays were used to assess HR activity of RAD51D-S207L mutated CHO cells. HR activity in RAD51D-S207L mutated human cells was tested by a DR-GFP assay. The effect of RAD51D p.S207L on RAD51D-XRCC2 interactions was analyzed by co-immunoprecipitation and quantified in-vivo in a single cell colocalization assay. Sensitivity to PARP inhibitors (PARPi) was evaluated in a cell survival assay. Results: Using deep sequencing and case-control genotyping studies, we showed that the missense RAD51D variant c.620C>T;p.S207L is over-represented in the French Canadian population affected by HGSC of the ovary (3.8% cases vs 0.002% controls; p < 0.0001).The frequency of the p.S207L variant did not differ from that of controls in breast, endometrial, pancreas and colorectal adenocarcinomas. A common haplotype shared by all the carriers suggested a founder origin for c.620C>T;p.S207L mutation. WES analysis of RAD51D tumor profiles revealed the presence of signature 3 which is known to be associated with HR defects. Functionally, we show that this mutation impairs HR by disrupting the RAD51D-XRCC2 interaction and confers PARP-inhibitor sensitivity to CHO cells. Conclusions: This work identifies RAD51D p.S207L as the first bona fide pathogenic missense susceptibility allele for HGSC of the ovary and supports the use of targeted PARPi therapies in OC patients carrying missense RAD51D mutations. Citation Format: Barbara Rivera, Massimo R. Di Iorio, Jessica Frankum, Javad Nadaf, Somayyeh Fahiminiya, Suzanna L. Arcand, David Burk, Damien Grapton, Eva Tomiak, Valerie Hastings, Nancy Hamel, Rabea Wagener, Olga Aleynikova, Sylvie Giroux, Fadi F. Hamdan, Alexandre Orthwein, George Zogopoulos, Francois Rousseau, Albert Berghuis, Diane M. Provencher, Guy A. Rouleau, Jacques L. Michaud, Anne-Marie Mes-Masson, Jacek Majewski, Susanne Bens, Reiner Siebert, Steven Narod, Mohammad Akbari, Chris J. Lord, Patricia N. Tonin, Alexandre Dionne-Laporte, William D. Foulkes. A functionally null RAD51D missense mutation is strongly associated with ovarian carcinoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2017; 2017 Apr 1-5; Washington, DC. Philadelphia (PA): AACR; Cancer Res 2017;77(13 Suppl):Abstract nr 2479. doi:10.1158/1538-7445.AM2017-2479

Published

2017

25. Germline RECQL mutations are associated with breast cancer susceptibility

Author

Javad Nadaf, Jacek Gronwald, Marek Szwiec, Nancy Hamel, Tomasz Huzarski, Bartłomiej Masojć, Helena Rudnicka, Aniruddh Kashyap, Tadeusz Dębniak, Anna Jakubowska, Jan Lubinski, François Rousseau, Mohammad R. Akbari, William D. Foulkes, Wojciech Kluźniak, Jacek Majewski, Marcin Lener, Bohdan Górski, Cezary Cybulski, Dominika Wokołorczyk, Tomasz Byrski, Jian Carrot-Zhang, Patrica N Tonin, Sylvie Giroux, Steven A. Narod, Barbara Rivera, and Shiyu Zhang

Subjects

Population, DNA Mutational Analysis, Molecular Sequence Data, Breast Neoplasms, Biology, Germline, DNA sequencing, Germline mutation, Breast cancer, Gene Frequency, Genetics, medicine, Humans, Genetic Predisposition to Disease, skin and connective tissue diseases, education, Allele frequency, Genetic Association Studies, Germ-Line Mutation, education.field_of_study, Base Sequence, RecQ Helicases, DNA replication, Case-control study, medicine.disease, Pedigree, Case-Control Studies, Cancer research, Female

Abstract

Several moderate- and high-risk breast cancer susceptibility genes have been discovered, but more are likely to exist. To discover new breast cancer susceptibility genes, we used 2 populations (from Poland and Quebec, Canada) and applied whole-exome sequencing in a discovery phase (n = 195), followed by validation. We identified rare recurrent RECQL mutations in each population. In Quebec, 7 of 1,013 higher-risk breast cancer cases and 1 of 7,136 newborns carried the c.634C>T (p.Arg215*) variant (P = 0.00004). In Poland, 30 of 13,136 unselected breast cancer cases and 2 of 4,702 controls carried the c.1667_1667+3delAGTA (p.K555delinsMYKLIHYSFR) variant (P = 0.008). RECQL is implicated in resolving stalled DNA replication forks to prevent double-stranded DNA (dsDNA) breaks. This function is related to that of other known breast cancer susceptibility genes, many of which are involved in repairing dsDNA breaks. We conclude that RECQL is a breast cancer susceptibility gene.

Published

2014

26. Risk of Misdiagnosis Due to Allele Dropout and False-Positive PCR Artifacts in Molecular Diagnostics: Analysis of 30,769 Genotypes

Author

Jonatan, Blais, Sébastien B, Lavoie, Sylvie, Giroux, Johanne, Bussières, Carmen, Lindsay, Jacqueline, Dionne, Mélissa, Laroche, Yves, Giguère, and François, Rousseau

Subjects

Genotype, Genotyping Techniques, Molecular Diagnostic Techniques, Risk Factors, Cystic Fibrosis Transmembrane Conductance Regulator, Humans, Loss of Heterozygosity, False Positive Reactions, Diagnostic Errors, Artifacts, Polymerase Chain Reaction, Polymorphism, Single Nucleotide, Alleles

Abstract

Quality control is a complex issue for clinical molecular diagnostic applications. In the case of genotyping assays, artifacts such as allele dropout represent a risk of misdiagnosis for amplification-based methods. However, its frequency of occurrence in PCR-based diagnostic assays remains unknown. To maximize the likelihood of detecting allele dropout, our clinical genotyping PCR-based assays are designed with two independent assays for each allele (nonoverlapping primers on each DNA strand). To estimate the incidence of allelic dropout, we took advantage of the capacity of our clinical assays to detect such events. We retrospectively studied their occurrence in the initial PCR assay for 30,769 patient reports for mutations involved in four diseases produced over 8 years. Ninety-three allele dropout events were detected and all were solved before reporting. In addition, 42 cases of artifacts caused by amplification of an allele ultimately confirmed to not be part of the genotype (drop-in events) were detected and solved. These artifacts affected 1:227 genotypes, 94% of which were due to nonreproducible PCR failures rather than sequence variants interfering with the assay, suggesting that careful primer design cannot prevent most of these errors. This provides a quantitative estimate for clinical laboratories to take this phenomenon into account in quality management and to favor assay designs that can detect (and minimize) occurrence of these artifacts in routine clinical use.

Published

2014

27. Genetic determinants of heel bone properties: genome-wide association meta-analysis and replication in the GEFOS/GENOMOS consortium

Author

Henry Völzke, Jonathan Reeve, Maciej Jaworski, Ozren Polasek, Kristina Åkesson, Marcin Kruk, Wilmar Igl, Peter P. Pramstaller, Matthew A. Brown, Rodney J. Scott, Uwe Völker, Karol Estrada, Mika Kähönen, Hou-Feng Zheng, Su-Mei Xiao, Frances M K Williams, Scott Wilson, Harri Sievänen, Steven Boonen, Doug C. Bauer, Ian R. Reid, Nicholas C. Harvey, Östen Ljunggren, Harry Campbell, Frederick C. W. Wu, Gregory J. Tranah, Douglas P. Kiel, Andrew A. Hicks, Melissa Garcia, Priya Srikanth, Caroline Hayward, Rosalie A. M. Dhonukshe-Rutten, Annie W.C. Kung, Yongmei Liu, Leo-Pekka Lyytikäinen, Cyrus Cooper, Stephen R Pye, Geoffrey C. Nicholson, Elaine M. Dennison, Carrie M. Nielson, Steven R. Cummings, Graeme Jones, Yi-Hsiang Hsu, Georg Homuth, Alireza Moayyeri, Fabiola Del Greco M, Nicole Soranzo, Fiona E. McGuigan, Henri Wallaschofski, John Attia, Alexander Teumer, Mark McEvoy, Tamara B. Harris, Albert Hofman, Pak C. Sham, Markku Alen, Dirk Vanderschueren, Suzanne J. Brown, Christopher Oldmeadow, Elizabeth G. Holliday, George Dedoussis, Maria Luisa Brandi, Anke Hannemann, Ulf Gyllensten, Richard L. Prince, Yoon Shin Cho, Marika Laaksonen, Jorma Viikari, Carolina Medina-Gomez, Johanna Jakobsdottir, Kay-Tee Khaw, Tim D. Spector, Min Jin Go, Stephen Kaptoge, Paweł Płudowski, Kristin Siggeirsdottir, Nathalie van der Velde, Karin M. A. Swart, Eugene V. McCloskey, Sulin Cheng, Robin Haring, André G. Uitterlinden, José L. Hernández, Sylvie Giroux, Emma L. Duncan, Terho Lehtimäki, J. Brent Richards, Paul Leo, John A. Eisman, Albert V. Smith, Thor Aspelund, Eric S. Orwoll, Paul Lips, Robert Luben, Kate L. Holliday, Olli T. Raitakari, Jong-Young Lee, Dan Mellström, Efi Grigoriou, Claes Ohlsson, Laura Masi, Roman S. Lorenc, David Karasik, Yanhua Zhou, Natasja M. van Schoor, Ryan L. Minster, John D. Wark, Joshua R. Lewis, Joo-Yeon Hwang, Vilmundur Gudnason, Nicholas J. Wareham, Olivia Trummer, Joseph M. Zmuda, Ling Oei, Jesús González-Macías, Barbara Obermayer-Pietsch, Richard Eastell, Terence W O'Neill, Åsa Johansson, Lisette C. P. G. M. de Groot, Roseanne Peel, Magnus Karlsson, A.W. Enneman, José M. Olmos, Matthias Nauck, Kun Zhu, Ching-Ti Liu, Fernando Rivadeneira, José A. Riancho, François Rousseau, Erasmus MC other, Internal Medicine, Epidemiology, Luben, Robert [0000-0002-5088-6343], Soranzo, Nicole [0000-0003-1095-3852], Khaw, Kay-Tee [0000-0002-8802-2903], Wareham, Nicholas [0000-0003-1422-2993], Kaptoge, Stephen [0000-0002-1155-4872], Apollo - University of Cambridge Repository, EMGO+ - Musculoskeletal Health, Epidemiology and Data Science, Internal medicine, EMGO - Musculoskeletal health, Universidad de Cantabria, Amsterdam Public Health, Amsterdam Movement Sciences, and Geriatrics

Subjects

Male, Oncology, Heel, Bone density, Osteoporosis, Genome-wide association study, Cohort Studies, Fractures, Bone, quantitative ultrasound, Bone Density, Genetics (clinical), risk, Ultrasonography, Aged, 80 and over, Genetics, medicine.diagnostic_test, Association Studies Articles, phenotypes, ta3141, General Medicine, Middle Aged, 3. Good health, medicine.anatomical_structure, osteoporosis diagnostic radiologic examination roentgen rays ultrasonography bone mineral density fractures calcaneus chromosomes genes genome heel longevity single nucleotide polymorphism sound genetics chromosome 7q31 genotype determination genome-wide association study attenuation osteoporotic fracture risk, Female, women, Adult, musculoskeletal diseases, medicine.medical_specialty, x-ray absorptiometry, Single-nucleotide polymorphism, densitometry, Biology, Polymorphism, Single Nucleotide, calcaneus, Young Adult, SDG 3 - Good Health and Well-being, Internal medicine, medicine, Humans, Genetic Predisposition to Disease, Molecular Biology, Dual-energy X-ray absorptiometry, VLAG, Aged, Global Nutrition, Wereldvoeding, ta1184, ta3121, medicine.disease, osteoporosis, Calcaneus, Genetic epidemiology, fracture, mineral density, Genome-Wide Association Study

Abstract

Quantitative ultrasound of the heel captures heel bone properties that independently predict fracture risk and, with bone mineral density (BMD) assessed by X-ray (DXA), may be convenient alternatives for evaluating osteoporosis and fracture risk. We performed a meta-analysis of genome-wide association (GWA) studies to assess the genetic determinants of heel broadband ultrasound attenuation (BUA; n = 14 260), velocity of sound (VOS; n = 15 514) and BMD (n = 4566) in 13 discovery cohorts. Independent replication involved seven cohorts with GWA data (in silico n = 11 452) and new genotyping in 15 cohorts (de novo n = 24 902). In combined random effects, meta-analysis of the discovery and replication cohorts, nine single nucleotide polymorphisms (SNPs) had genome-wide significant (P < 5 x 10(-8)) associations with heel bone properties. Alongside SNPs within or near previously identified osteoporosis susceptibility genes including ESR1 (6q25.1: rs4869739, rs3020331, rs2982552), SPTBN1 (2p16.2: rs11898505), RSPO3 (6q22.33: rs7741021), WNT16 (7q31.31: rs2908007), DKK1 (10q21.1: rs7902708) and GPATCH1 (19q13.11: rs10416265), we identified a new locus on chromosome 11q14.2 (rs597319 close to TMEM135, a gene recently linked to osteoblastogenesis and longevity) significantly associated with both BUA and VOS (P < 8.23 x 10(-14)). In meta-analyses involving 25 cohorts with up to 14 985 fracture cases, six of 10 SNPs associated with heel bone properties at P < 5 x 10(-6) also had the expected direction of association with any fracture (P < 0.05), including three SNPs with P < 0.005: 6q22.33 (rs7741021), 7q31.31 (rs2908007) and 10q21.1 (rs7902708). In conclusion, this GWA study reveals the effect of several genes common to central DXA-derived BMD and heel ultrasound/DXA measures and points to a new genetic locus with potential implications for better understanding of osteoporosis pathophysiology.

Published

2014

28. Relationships between individual behavioural traits and post-weaning growth in segregated early-weaned piglets

Author

S. Robert, G P Martineau, and Sylvie Giroux

Subjects

Early weaning, Ontogeny, Biology, Positive correlation, Body weight, Developmental psychology, Animal science, Food Animals, Weaned piglets, medicine, Post weaning, Weaning, Animal Science and Zoology, medicine.symptom, Weight gain

Abstract

Piglets' individual behavioural traits have been studied in the last decade but no report has linked these traits with growth. This experiment was conducted to determine if behavioural traits of segregated early-weaned piglets could be good predictors of their post-weaning growth and, thus, help to predict their adaptation to early weaning. Following segregated early weaning at 17+/-1 days old, 252 piglets were submitted to three tests between 20 and 25 days of age: open-field, reaction to humans and rank order based on competition for a restricted-access feeder. The body weight of each piglet was measured the day before weaning and once a week for the next 4 weeks. A principal component analysis yielded five factors with an Eigenvalue higher than 0.90 that accounted for 81% of the total variation between individuals: reaction to humans (25%), active response to stress (21%), passive response to stress (14%), feeding behaviour (10%) and rank order (9%). Passive reaction to stress was associated with better weight gain during the first week post-weaning (r=0.18; P=0.01), and a positive correlation was found between social status and weight gain during the 4 weeks following weaning (-0.15

Published

2000

29. Novel isoforms of the fragile X related protein FXR1P are expressed during myogenesis

Author

Annie Sittler, D. Heitz, Barbara Bardoni, Sylvie Giroux, Jean-Louis Mandel, Sandra Tremblay, C. Pinset, Edouard W. Khandjian, François Rousseau, D. Montarras, and François Corbin

Subjects

Gene isoform, congenital, hereditary, and neonatal diseases and abnormalities, Immunoblotting, Molecular Sequence Data, Nerve Tissue Proteins, Chemical Fractionation, Biology, Muscle Development, Cell Line, Gene product, Fragile X Mental Retardation Protein, Mice, Gene expression, Genetics, Animals, Humans, Myocyte, Molecular Biology, Genetics (clinical), Base Sequence, Sequence Homology, Amino Acid, Myogenesis, Muscles, Alternative splicing, Brain, Gene Expression Regulation, Developmental, RNA-Binding Proteins, 3T3 Cells, General Medicine, Immunohistochemistry, Molecular biology, nervous system diseases, Alternative Splicing, Ribonucleoproteins, Cell culture, Cytoplasm, Fragile X Syndrome, Polyribosomes, COS Cells, RNA, HeLa Cells

Abstract

The fragile X syndrome results from transcriptional silencing of the FMR1 gene and the absence of its encoded FMRP protein. Two autosomal homologues of the FMR1 gene, FXR1 and FXR2, have been identified and the overall structures of the corresponding proteins are very similar to that of FMRP. Using antibodies raised against FXR1P, we observed that two major protein isoforms of relative MW of 78 and 70 kDa are expressed in different mammalian cell lines and in the majority of mouse tissues. In mammalian cells grown in culture as well as in brain extracts, both P78 and P70 isoforms are associated with mRNPs within translating polyribosomes, similarly to their closely related FMRP homologues. In muscle tissues as well as in murine myoblastic cell lines induced to differentiate into myotubes, FXR1P78 and P70 isoforms are replaced by novel unpredicted isoforms of 81‐84 kDa and a novel FXR1 exon splice variant was detected in muscle RNA. While P81‐84 isoforms expressed after fusion into myotubes in murine myoblast cell lines grown in culture are associated with polyribosomes, this is not the case when isolated from muscle tissues since they sediment with lower S values. Immunohistochemical studies showed coexpression of FMRP and FXR1P70 and P78 in the cytoplasm of brain neurons, while in muscle no FMRP was detected and FXR1P81‐84 were mainly localized to structures within the muscle contractile bands. The complex expression pattern of FXR1P suggests tissue-specific expression for the various isoforms of FXR1 and the differential expression of FMRP and FXR1Ps suggests that in certain types of cells and tissues, complementary functions may be fulfilled by the various FMRP family members.

Published

1998

30. Defective Development of the Embryonic Liver in N-myc-Deficient Mice

Author

Jean Charron and Sylvie Giroux

Subjects

Mutant, Genes, myc, Apoptosis, Organogenesis, Biology, Andrology, Embryonic and Fetal Development, Mice, Proto-Oncogene Proteins c-myb, Proto-Oncogene Proteins, Proto-Oncogenes, medicine, Animals, RNA, Messenger, Molecular Biology, Gene Expression Regulation, Developmental, Cell Differentiation, Embryo, Cell Biology, Hematopoietic Stem Cells, Embryonic stem cell, Molecular biology, Mice, Mutant Strains, Haematopoiesis, medicine.anatomical_structure, Liver, Hepatocyte, Trans-Activators, N-Myc, Developmental Biology

Abstract

The mechanisms involved in the formation and the differentiation of the liver remain unclear despite extensive studies. To investigate these events in mouse hepatic development, we have taken advantage of the N-myc mutant mouse line which exhibits abnormal liver development. N-myc mutant embryos die between 11.5 and 12.5 days postcoitum most probably from heart failure. In the present study, we report that at 11.5 days of gestation, extensive apoptosis restricted to the hepatocytes occurred in N-myc mutant liver when compared to wild-type samples. Moreover, the number of hematopoietic cells is reduced in the mutant liver. During early liver organogenesis, the N-myc gene is expressed in tissues involved in the induction and the differentiation of the hepatocytes. At 11.5 days postcoitum, both c-myc and N-myc genes are expressed in the liver. While c-myc is expressed at a high level in the organ per se, N-myc expression is mostly confined to the peripheral layer of the liver which will generate the Glisson's capsule. Taken together, the expression pattern of N-myc in the liver and the specific apoptosis of hepatocytes observed in N-myc mutants indicate that N-myc is required for hepatocyte survival and suggest that it is involved in the genetic cascade leading to normal liver development.

Published

1998

31. Prevalence of selected genomic deletions and duplications in a French-Canadian population-based sample of newborns

Author

François Rousseau, Tracy Tucker, Sylvie Giroux, Jan M. Friedman, Valérie Clément, and Sylvie Langlois

Subjects

Genetic counseling, Population, 22q11.2, 03 medical and health sciences, Intellectual disability, Gene duplication, Genetics, medicine, education, Molecular Biology, normal population, Genetics (clinical), 030304 developmental biology, 0303 health sciences, education.field_of_study, Microarray analysis techniques, business.industry, screening, 030305 genetics & heredity, Original Articles, medicine.disease, 16p11.2, 3. Good health, Schizophrenia, French canadian, Autism, business

Abstract

Chromosomal microarray analysis has identified many novel microdeletions or microduplications that produce neurodevelopmental disorders with a recognizable clinical phenotype and that are not observed in normal individuals. However, imbalance of other genomic regions is associated with a variable phenotype with intellectual disability (ID) or autism in some individuals but are also observed in completely normal individuals. Several large studies have reported the prevalence of copy number (CN) variants in people with particular features (e.g., ID, autism, schizophrenia, or epilepsy); few studies have investigated the prevalence of genomic CN changes in the general population. We used a high-throughput method to screen 6813 consecutive cord blood samples from a predominantly French–Canadian population to assess genomic CN in five genomic regions: 1p36, 15q11-q13, 16p11.2, 16p11.2-p12.2, and 22q11.2. We identified one deletion and one duplication within 1p36, two deletions of 15q11-q13, eight deletions of 16p11.2-p12.2, two deletions and five duplications of 16p11.2, and six duplications of 22q11.2. This study provides estimates of the frequency of CN variants in an unselected population. Our findings have important implications for genetic counseling.

Published

2013

32. Factors affecting the stability of the renal sodium/phosphate symporter during its solubilization and reconstitution

Author

Marie-Claude Delisle, Sylvie Giroux, Raynald Laprade, Vincent Vachon, and Richard Béliveau

Subjects

Glycerol, Proteolipids, Sodium, chemistry.chemical_element, Kidney, Biochemistry, Phosphates, Membrane Lipids, chemistry.chemical_compound, Potassium phosphate, Animals, Chromatography, Microvilli, Symporters, biology, Chemistry, Membrane transport protein, Osmolar Concentration, Temperature, Cholic Acids, Sodium-Phosphate Cotransporter Proteins, Biological activity, Cell Biology, Hydrogen-Ion Concentration, Phosphate, Dithiothreitol, Cholesterol, Ionic strength, Symporter, biology.protein, Cattle, Carrier Proteins

Abstract

Phosphate is reabsorbed across the brush-border membrane of the proximal tubule by a specific sodium-dependent symporter. Like the other brush-border membrane transport proteins of the kidney, the phosphate carrier remains to be isolated in a functional state. To establish a set of parameters that allow to preserve its biological activity, the phosphate carrier was solubilized under systematically varied conditions and reconstituted into proteoliposomes. Successful reconstitution was achieved only when the extraction buffer contained lipids extracted from the renal brush-border membrane. Glycerol, an osmolyte which reduces the water activity of the solution, was also required. It could however be replaced by 150 mM sodium or potassium phosphate. Below this concentration and in the presence of glycerol, the ionic strength of the solution had little effect on the stability of the transporter, but sodium phosphate could not be replaced by sodium chloride. Phosphate transport in reconstituted vesicles depended on the concentration of detergent and pH of the extraction buffer. Finally, transport activity was increased when solubilization was carried out in the presence of a reducing agent, dithiothreitol. These results should be helpful during the purification and further characterization of the renal phosphate symporter.

Published

1995

33. Erratum: Corrigendum: Germline RECQL mutations are associated with breast cancer susceptibility

Author

Jian Carrot-Zhang, Wojciech Kluźniak, Cezary Cybulski, Tomasz Byrski, Bartłomiej Masojć, Patrica N Tonin, Tadeusz Dębniak, François Rousseau, Barbara Rivera, Anna Jakubowska, Jacek Gronwald, Shiyu Zhang, Mohammad R. Akbari, William D. Foulkes, Tomasz Huzarski, Jacek Majewski, Marek Szwiec, Marcin Lener, Aniruddh Kashyap, Helena Rudnicka, Nancy Hamel, Sylvie Giroux, Steven A. Narod, Jan Lubinski, Dominika Wokołorczyk, Javad Nadaf, and Bohdan Górski

Subjects

0301 basic medicine, Genetics, 03 medical and health sciences, 030104 developmental biology, Breast cancer, Published Erratum, MEDLINE, medicine, Biology, medicine.disease, Germline

Abstract

Nat. Genet. 47, 643–646 (2015); published online 27 April 2015; corrected after print 12 January 2016 In the version of this article initially published, one of the variants was incorrectly reported as c.634C>T. The correct nomenclature for this variant is c.643C>T. The error has been corrected in the HTML and PDF versions of the article.

Published

2016

34. Assessment of gene-by-sex interaction effect on bone mineral density

Author

Evangelos Evangelou, Melanie A. Carless, Jane A. Cauley, Elizabeth A. Streeten, Hou-Feng Zheng, Ching-Ti Liu, Nerea Alonso, J. Brent Richards, Dan Mellström, Ben A. Oostra, Stuart H. Ralston, Pak C. Sham, Annie W.C. Kung, M. Carola Zillikens, Kun Zhu, Simona Mencej-Bedrač, Serkalem Demissie, Martha C. Castaño-Betancourt, Elza Khusnutdinova, Fernando Rivadeneira, Najaf Amin, Frances A. Tylavsky, Guo Li, John P. A. Ioannidis, Magnus Karlsson, Carolina Medina-Gomez, Unnur Styrkarsdottir, David Karasik, Jerome I. Rotter, Östen Ljunggren, María T. Zarrabeitia, Douglas P. Kiel, Claes Ohlsson, John A Robbins, Cornelia M. vanDuijn, John Blangero, Braxton D. Mitchell, Millan S. Patel, José A. Riancho, Yongmei Liu, Joel Eriksson, Natalia Garcia-Giralt, Tomi Pastinen, Lise B. Husted, Wim Van Hul, Tamara B. Harris, Laura Masi, Ryan L. Minster, Su-Mei Xiao, Zoe H. Dailiana, Karol Estrada, Tony Kwan, Panagoula Kollia, Joshua R. Lewis, Roser Urreizti, José M. Olmos, Susana Balcells, L. Adrienne Cupples, David Goltzman, Ling Oei, Mattias Lorentzon, Sylvie Giroux, Laura M. Yerges-Armstrong, Gunnar Sigurdsson, Joyce B.J. vanMeurs, Tim D. Spector, Jeffrey R. O'Connell, Theodora Koromila, Bente L. Langdahl, Xavier Nogués, François Rousseau, Janez Prezelj, Kari Stefansson, Jesús González-Macías, Yi-Hsiang Hsu, Gudmar Thorleifsson, Albert Hofman, Rita Khusainova, André G. Uitterlinden, Elin Grundberg, Bruce M. Psaty, Candace M. Kammerer, Janja Marc, Morten Frost, Lizbeth Herrera, Unnur Thorsteinsdottir, Maria Luisa Brandi, Liesbeth Vandenput, Richard L. Prince, Yanhua Zhou, Epidemiology, Erasmus School of Social and Behavioural Sciences, Internal Medicine, and Clinical Genetics

Subjects

Male, Bone density, Endocrinology, Diabetes and Metabolism, Quantitative Trait Loci, 030209 endocrinology & metabolism, Locus (genetics), Single-nucleotide polymorphism, Genome-wide association study, DETERMINANTS, SUSCEPTIBILITY, MASS, Biology, Quantitative trait locus, GENOTYPE IMPUTATION, OSTEOPOROSIS, Polymorphism, Single Nucleotide, Article, AGING, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Meta-Analysis as Topic, BMD, Bone Density, Humans, Orthopedics and Sports Medicine, GENOME-WIDE ASSOCIATION, 030304 developmental biology, Bone mineral, Genetics, QUANTITATIVE TRAIT LOCI, 0303 health sciences, Sex Characteristics, GENE-BY-SEX INTERACTION, Reproducibility of Results, ASSOCIATION, Genes, CELLS, Expression quantitative trait loci, Female, GENDER, Human medicine, Sex characteristics, Genome-Wide Association Study

Abstract

Sexual dimorphism in various bone phenotypes, including bone mineral density (BMD), is widely observed; however, the extent to which genes explain these sex differences is unclear. To identify variants with different effects by sex, we examined gene-by-sex autosomal interactions genome-wide, and performed expression quantitative trait loci (eQTL) analysis and bioinformatics network analysis. We conducted an autosomal genome-wide meta-analysis of gene-by-sex interaction on lumbar spine (LS) and femoral neck (FN) BMD in 25,353 individuals from 8 cohorts. In a second stage, we followed up the 12 top single-nucleotide polymorphisms (SNPs; p −5) in an additional set of 24,763 individuals. Gene-by-sex interaction and sex-specific effects were examined in these 12 SNPs. We detected one novel genome-wide significant interaction associated with LS-BMD at the Chr3p26.1-p25.1 locus, near the GRM7 gene (male effect = 0.02 and p = 3.0 × 10−5; female effect = −0.007 and p = 3.3 × 10−2), and 11 suggestive loci associated with either FN- or LS-BMD in discovery cohorts. However, there was no evidence for genome-wide significant (p −8) gene-by-sex interaction in the joint analysis of discovery and replication cohorts. Despite the large collaborative effort, no genome-wide significant evidence for gene-by-sex interaction was found to influence BMD variation in this screen of autosomal markers. If they exist, gene-by-sex interactions for BMD probably have weak effects, accounting for less than 0.08% of the variation in these traits per implicated SNP.

Published

2012

35. Genome-wide meta-analysis identifies 56 bone mineral density loci and reveals 14 loci associated with risk of fracture

Author

Barbara Obermayer-Pietsch, Nerea Alonso, Su-Mei Xiao, Zoe H. Dailiana, Daniel I. Chasman, Andrew R. Wood, Ghi Su Kim, P. Eline Slagboom, Stephen Kaptoge, Sjur Reppe, L. B. Husted, André G. Uitterlinden, Jonathan Reeve, Emma L. Duncan, Annie W.C. Kung, Tomi Pastinen, Paul Leo, George Dedoussis, Paul Lips, Mattias Lorentzon, David M. Evans, Ling Oei, John A. Eisman, Nelson Ls Tang, Marcin Kruk, Hou-Feng Zheng, Brendan M. Buckley, Kun Zhu, Simona Mencej-Bedrač, James F. Wilson, Geoffrey C. Nicholson, Seung-Hun Lee, Elaine M. Dennison, Charles Kooperberg, Matthew A. Brown, Karol Estrada, Aaron K. Aragaki, Martha C. Castaño-Betancourt, Laura Masi, Ryan L. Minster, Gunnar Sigurdsson, John P. A. Ioannidis, Göran Hallmans, J. Wouter Jukema, Tony Kwan, John P. Kemp, Rebecca D. Jackson, Alireza Moayyeri, José A. Riancho, Dominique J. Verlaan, Joshua R. Lewis, Janez Prezelj, Claus Christiansen, Paul M. Ridker, Elza Khusnutdinova, Khusainova Ri, Roman S. Lorenc, David M. Reid, Yi-Hsiang Hsu, Claes Ohlsson, Ching-Ti Liu, Kannabiran Nandakumar, Nicholas J. Wareham, Lynda M. Rose, Albert V. Smith, Carolina Medina-Gomez, Evangelia E. Ntzani, Cornelia M. van Duijn, Kay-Tee Khaw, Gudmar Thorleifsson, Tamara B. Harris, P. C. Leung, Millan S. Patel, Laura M. Yerges-Armstrong, Yanhua Zhou, Lynne J. Hocking, Dan Mellström, Yongmei Liu, Frances M K Williams, Alan R. Shuldiner, Janja Marc, Omar M. E. Albagha, Theodora Koromila, Elizabeth A. Streeten, Fernando Rivadeneira, Braxton D. Mitchell, Karen A. Jameson, Hrefna Johannsdottir, L. Adrienne Cupples, Douglas P. Kiel, Tim D. Spector, Sulin Cheng, Kristin Siggeirsdottir, Stuart H. Ralston, Rui Jian Li, Ian Ford, J. Brent Richards, Serena Scollen, Scott Wilson, Guo Shuai Li, Mika Kähönen, Jean Woo, Munro Peacock, María T. Zarrabeitia, Soumya Raychaudhuri, Huibert A. P. Pols, John A Robbins, Morten Frost, Wim Van Hul, Andrea Z. LaCroix, David Karasik, Natasja M. van Schoor, Yurii S. Aulchenko, Jorma Viikari, Bente L. Langdahl, Xavier Nogués, Marika Laaksonen, Jung-Min Koh, Ian R. Reid, Dana Willner, Stefan T Palsson, Olle Svensson, Robert Luben, Markku Alen, Richard L. Prince, David Goltzman, Lizbeth Herrera, Thorvaldur Ingvarsson, Olli T. Raitakari, Sylvie Giroux, Kari Stefansson, Patrick Danoy, Susana Balcells, Eugene V. McCloskey, Pak C. Sham, Liesbeth Vandenput, Evangelos Evangelou, François Rousseau, Unnur Styrkarsdottir, Jesús González-Macías, Albert Hofman, Graeme R. Clark, M. Carola Zillikens, Steven R. Cummings, Magnus Karlsson, Panagoula Kollia, Thor Aspelund, Graeme Jones, William D. Leslie, Ben A. Oostra, Unnur Thorsteinsdottir, Maria Luisa Brandi, Stella Trompet, Michael J. Econs, Olivia Trummer, Ulrika Pettersson-Kymmer, José M. Olmos, Jane A. Cauley, Natalia Garcia-Giralt, Najaf Amin, Philip N. Sambrook, Terho Lehtimäki, Daniel L. Koller, David Duggan, Joyce B. J. van Meurs, Ville Aalto, Joel Eriksson, Roser Urreizti, Vilmundur Gudnason, Kaare M. Gautvik, Richard Eastell, Elin Grundberg, Bruce M. Psaty, Candace M. Kammerer, Jerome I. Rotter, Östen Ljunggren, Melissa Nolan Garcia, Cyrus Cooper, Tuan V. Nguyen, Frances A. Tylavsky, Epidemiology and Data Science, Internal medicine, EMGO - Musculoskeletal health, Internal Medicine, Epidemiology, Erasmus School of Social and Behavioural Sciences, Erasmus MC other, Pediatric Surgery, Clinical Genetics, EMGO+ - Musculoskeletal Health, and Universitat de Barcelona

Subjects

Male, Bone density, Osteoporosis, Genome-wide association study, Mitochondrial Membrane Transport Proteins, Bone densitometry, Fractures, Bone, 0302 clinical medicine, Bone Density, Risk Factors, Femur, Genetics, Bone mineral, 0303 health sciences, education.field_of_study, Extracellular Matrix Proteins, Lumbar Vertebrae, Femur Neck, ta3141, medicine.anatomical_structure, Low Density Lipoprotein Receptor-Related Protein-5, Intercellular Signaling Peptides and Proteins, Female, Gens, musculoskeletal diseases, Genotype, Population, European Continental Ancestry Group, Quantitative Trait Loci, 030209 endocrinology & metabolism, Vèrtebres lumbars, Biology, Fèmur, Polymorphism, Single Nucleotide, Article, White People, 03 medical and health sciences, SDG 3 - Good Health and Well-being, Densitometria òssia, medicine, Humans, Genetic Predisposition to Disease, education, 030304 developmental biology, Femoral neck, Genetic association, Glycoproteins, Gene Expression Profiling, Computational Biology, Spectrin, ta3121, medicine.disease, Phosphoproteins, Genes, Mesenchymal stem cell differentiation, Human medicine, Fractures, Genome-Wide Association Study

Abstract

Bone mineral density (BMD) is the most widely used predictor of fracture risk. We performed the largest meta-analysis to date on lumbar spine and femoral neck BMD, including 17 genome-wide association studies and 32,961 individuals of European and east Asian ancestry. We tested the top BMD-associated markers for replication in 50,933 independent subjects and for association with risk of low-trauma fracture in 31,016 individuals with a history of fracture (cases) and 102,444 controls. We identified 56 loci (32 new) associated with BMD at genome-wide significance (P < 5 × 10 -8). Several of these factors cluster within the RANK-RANKL-OPG, mesenchymal stem cell differentiation, endochondral ossification and Wnt signaling pathways. However, we also discovered loci that were localized to genes not known to have a role in bone biology. Fourteen BMD-associated loci were also associated with fracture risk (P < 5 × 10 -4, Bonferroni corrected), of which six reached P < 5 × 10 -8, including at 18p11.21 (FAM210A), 7q21.3 (SLC25A13), 11q13.2 (LRP5), 4q22.1 (MEPE), 2p16.2 (SPTBN1) and 10q21.1 (DKK1). These findings shed light on the genetic architecture and pathophysiological mechanisms underlying BMD variation and fracture susceptibility. © 2012 Nature America, Inc. All rights reserved.

Published

2012

36. Molecular Size of the Functional Complex and Protein Subunits of the Renal Phosphate Symporter

Author

Richard Béliveau, Michel Potier, Vincent Vachon, Marie-Claude Delisle, Christian J. C. Boyer, and Sylvie Giroux

Subjects

Male, Macromolecular Substances, Protein subunit, Immunoblotting, Kidney, Biochemistry, Rats, Sprague-Dawley, Animals, Peptide sequence, Gel electrophoresis, chemistry.chemical_classification, Microvilli, Symporters, Molecular mass, Dose-Response Relationship, Radiation, Sodium-Phosphate Cotransporter Proteins, Rats, Amino acid, Molecular Weight, chemistry, Symporter, Electrophoresis, Polyacrylamide Gel, Rabbits, Carrier Proteins, Cotransporter, Homotetramer

Abstract

The oligomeric structure of the rabbit renal brush-border membrane sodium/phosphate cotransporter was examined with the radiation inactivation and fragmentation technique. The size of its functional complex (its "radiation inactivation size") was estimated from the rate of decay of its sodium-dependent transport activity as a function of the radiation dose. A radiation inactivation size of 223 +/- 42 kDa was obtained. The polypeptide constituting the monomeric unit of the Na1+/Pi symporter was detected by immunoblotting with polyclonal anti-peptide antibodies directed against the 14 amino acid C-terminal portion of the symporter molecule. Its apparent molecular size estimated by comparison with standards following SDS-polyacrylamide gel electrophoresis was 64,000. This value is in good agreement with its known molecular mass of 51,797 Da calculated from the amino acid sequence deducted from the nucleotide sequence of its gene since this protein is probably glycosylated. The loss of labeling intensity of the polypeptide of M(r) = 64,000 was also measured as a function of radiation dose. The molecular size calculated from these data (its "target size") was 165 +/- 20 kDa. The target size estimated for the rat phosphate cotransporter was 184 +/- 46 kDa, and its previously reported radiation inactivation size was 234 +/- 14 kDa. These results strongly suggest that the renal Na1+/Pi cotransporter exists as an oligomeric protein, probably a homotetramer. The fact that the values obtained for the target size are about 3/4 those obtained for the radiation inactivation size of these cotransport proteins indicates that their subunits are closely associated since most of their subunits appear to be fragmented by a single ionizing radiation hit.

Published

1994

37. Immunodetection and characterization of proteins implicated in renal sodium/phosphate cotransport

Author

Christian J. C. Boyer, Richard Béliveau, Vincent Vachon, Sylvie Giroux, and Marie-Claude Delisle

Subjects

Male, Peptide Biosynthesis, Kidney Cortex, Molecular Sequence Data, Biophysics, Biochemistry, Phosphates, Rats, Sprague-Dawley, Western blot, Antibody Specificity, medicine, Animals, Amino Acid Sequence, Epithelial polarity, Kidney, Symporters, medicine.diagnostic_test, biology, Chemistry, Sodium, Membrane Proteins, Sodium-Phosphate Cotransporter Proteins, Cell Biology, Membrane transport, Rats, Cytosol, medicine.anatomical_structure, Membrane protein, Polyclonal antibodies, biology.protein, Cattle, Rabbits, Carrier Proteins, Peptides, Cotransporter, Subcellular Fractions

Abstract

Polyclonal antibodies raised against the 14-amino acid C-terminal portion of the rabbit renal brush-border membrane Na+/Pi cotransporter, as deduced from the nucleotide sequence of the cloned NaPi-1 gene, were used for Western blot analysis of renal brush-border membrane proteins from rat, rabbit and beef. Proteins of 65 kDa from the rat, 64 kDa from the rabbit, and 38, 66, 77, 92, 110, 176 and 222 kDa from the beef were specifically labelled. The affinity of the antibodies was much greater, however, for the proteins of the rat and rabbit than for those of the beef. The rat 65-kDa antigen was readily detected in brush-border membranes isolated from kidney cortex, but was absent from the basolateral membrane and the cytosolic and microsomal fractions of this tissue, in agreement with the subcellular localization of the Na+/Pi cotransporter. This antigen was however several-fold more abundant in the juxtamedullary portion of the cortex than in the outer portion. Despite a strong stimulation in phosphate transport, a low-phosphate diet had little influence on the amount of antigen detected. An additional peptide-displaceable band corresponding to a protein of 250 kDa appeared when β-mercaptoethanol was omitted during electrophoresis, in agreement with the possibility that disulfide bonds may be involved in the regulation of renal phosphate transport activity.

Published

1994

38. High-density polymorphisms analysis of 23 candidate genes for association with bone mineral density

Author

David E. C. Cole, Alexandre Bureau, Sylvie Giroux, Johanne Bussières, Latifa Elfassihi, François Rousseau, and Valérie Clément

Subjects

Peak bone mass, Adult, medicine.medical_specialty, Candidate gene, Histology, Bone density, Bone disease, Adolescent, Physiology, Endocrinology, Diabetes and Metabolism, Osteoporosis, Biology, Polymorphism, Single Nucleotide, Young Adult, Absorptiometry, Photon, Bone Density, Internal medicine, Receptors, Colony-Stimulating Factor, medicine, Humans, Aged, Bone mineral, Aged, 80 and over, Heritability, Middle Aged, medicine.disease, Menopause, Postmenopause, Endocrinology, Premenopause, Female

Abstract

Osteoporosis is a bone disease characterized by low bone mineral density (BMD), a highly heritable and polygenic trait. Women are more prone than men to develop osteoporosis due to a lower peak bone mass and accelerated bone loss at menopause. Peak bone mass has been convincingly shown to be due to genetic factors with heritability up to 80%. Menopausal bone loss has been shown to have around 38% to 49% heritability depending on the site studied. To have more statistical power to detect small genetic effects we focused on premenopausal women. We studied 23 candidate genes, some involved in calcium and vitamin-D regulation and others because estrogens strongly induced their gene expression in mice where it was correlated with humerus trabecular bone density. High-density polymorphisms were selected to cover the entire gene variability and 231 polymorphisms were genotyped in a first sample of 709 premenopausal women. Positive associations were retested in a second, independent, sample of 673 premenopausal women. Ten polymorphisms remained associated with BMD in the combined samples and one was further associated in a large sample of postmenopausal women (1401 women). This associated polymorphism was located in the gene CSF3R (granulocyte colony stimulating factor receptor) that had never been associated with BMD before. The results reported in this study suggest a role for CSF3R in the determination of bone density in women.

Published

2010

39. Characterization of essential arginine residues implicated in the renal transport of phosphate and glucose

Author

Sylvie Giroux, Bruno Beaumier, Johanne Strévey, Richard Béliveau, and Vincent Vachon

Subjects

Phenylglyoxal, Kidney Cortex, Arginine, Sodium, Kinetics, Biophysics, Alkalinity, chemistry.chemical_element, In Vitro Techniques, Biochemistry, Phosphates, chemistry.chemical_compound, Animals, Microvilli, Cell Membrane, Glucose transporter, Biological Transport, Cell Biology, Hydrogen-Ion Concentration, Phosphate, Rats, Glucose, chemistry, Reagent

Abstract

We have characterized the reaction of arginine-specific reagents with the phosphate and glucose carriers of the kidney brush-border membrane. The inhibition of phosphate and glucose transport by phenylglyoxal follows pseudo-first-order kinetics. The rate of inactivation of phosphate transport by 50 mM phenylglyoxal was about 3-fold higher than that for glucose transport (kapp was 0.052 s−1 for the uptake of phosphate and 0.019 s−1 for the uptake of glucose). The order of the reaction, n, with respect to phenylglyoxal was 1.25 and 1.31 for the inactivation of phosphate and glucose transport, respectively. The inactivation of phosphate flux by p-hydroxyphenylglyoxal also follows pseudo-first-order kinetics, but the inhibition rate (kapp = 0.0012 s−1) was slower than with phenylglyoxal. The inactivation increased with the alkalinity of the preincubation medium for both phosphate and glucose fluxes and was maximal at pH 9.0. The inactivation of phosphate flux by phenylglyoxal depends upon the presence of an alkaline intravesicular pH. Extravesicular pH does not affect the reaction. Phenylglyoxal does not interfere with the recycling of the protonated carrier since phosphate uptake is inhibited independently of the pH used for transport measurements. Moreover, phenylglyoxal completely abolished trans stimulation by phosphate. Trans sodium inhibited phosphate uptake and abolished the pH profile of phosphate uptake.

Published

1992

40. Molecular size of the renal sodium/phosphate symporter in native and reconstituted systems

Author

Sylvie Giroux, Michel Potier, Marie-Claude Delisle, Vincent Vachon, Raynald Laprade, and Richard Béliveau

Subjects

Brush border, Proteolipids, Sodium, Tetramisole, Biophysics, Synthetic membrane, chemistry.chemical_element, Kidney, Biochemistry, chemistry.chemical_compound, Animals, chemistry.chemical_classification, Microvilli, Symporters, Vesicle, Sodium-Phosphate Cotransporter Proteins, Cell Biology, Phosphate, Kinetics, Enzyme, chemistry, Symporter, Alkaline phosphatase, Cattle, Carrier Proteins

Abstract

The size of the renal sodium/phosphate symporter was estimated with the radiation inactivation technique in isolated bovine brush border membrane vesicles and after reconstitution in proteoliposomes. The functional unit of the native phosphate carrier had a radiation inactivation size of 172 ± 17kDa. Identical values were obtained for the reconstituted carrier whether it was irradiated before or after the formation of the proteoliposomes (161 ± 9 and 159 ± 11kDa, respectively). The sodium-independent uptake of phosphate was not affected significantly by radiation doses up to 10 Mrad. This activity is therefore not due to the reconstitution of a large phosphate-binding protein such as alkaline phosphatase. Furthermore, bromotetramisole, a specific inhibitor of phosphate binding to this enzyme, had no significant effect on the uptake of phosphate by the proteoliposomes.

Published

1992

41. Identification of a novel truncating PALB2mutation and analysis of its contribution to early-onset breast cancer in French-Canadian women

Author

Eve Fafard, Ginette Martin, Mohammed Reza Akbari, Steven A. Narod, Tarek A. Bismar, Parviz Ghadirian, Marc Tischkowitz, Nancy Hamel, André Robidoux, Aletta Poll, François Rousseau, William D. Foulkes, Robert Royer, Sylvie Giroux, Nelly Sabbaghian, and Andrew Darnel

Subjects

Adult, Oncology, medicine.medical_specialty, Glutamine, PALB2, Population, Breast Neoplasms, Single-nucleotide polymorphism, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Surgical oncology, Internal medicine, Humans, Medicine, Genetic Predisposition to Disease, Age of Onset, skin and connective tissue diseases, education, 030304 developmental biology, Medicine(all), Gynecology, 0303 health sciences, education.field_of_study, business.industry, Tumor Suppressor Proteins, Infant, Newborn, Quebec, Nuclear Proteins, Middle Aged, medicine.disease, Founder Effect, 3. Good health, 030220 oncology & carcinogenesis, Mutation, Mutation (genetic algorithm), Female, France, Age of onset, Fanconi Anemia Complementation Group N Protein, business, Research Article, Founder effect

Abstract

Background PALB2 has recently been identified as a breast cancer susceptibility gene. PALB2 mutations are rare causes of hereditary breast cancer but may be important in countries such as Finland where a founder mutation is present. We sought to estimate the contribution of PALB2 mutations to the burden of breast cancer in French Canadians from Quebec. Methods We screened all coding exons of PALB2 in a sample of 50 French-Canadian women diagnosed with either early-onset breast cancer or familial breast cancer at a single Montreal hospital. The genetic variants identified in this sample were then studied in 356 additional women with breast cancer diagnosed before age 50 and in 6,448 newborn controls. Results We identified a single protein-truncating mutation in PALB2 (c.2323 C>T, resulting in Q775X) in 1 of the 50 high-risk women. This variant was present in 2 of 356 breast cancer cases and in none of 6,440 newborn French-Canadian controls (P = 0.003). We also identified two novel new non-synonymous single nucleotide polymorphisms in exon 4 of PALB2 (c.5038 A>G [I76V] and c.5156 G>T [G115V]). G115V was found in 1 of 356 cases and in 15 of 6,442 controls (P = 0.6). The I76V variant was not identified in either the extended case series or the controls. Conclusion We have identified a novel truncating mutation in PALB2. The mutation was found in approximately 0.5% of unselected French-Canadian women with early-onset breast cancer and appears to have a single origin. Although mutations are infrequent, PALB2 can be added to the list of breast cancer susceptibility genes for which founder mutations have been identified in the French-Canadian population.

Published

2007

42. Whole-genome sequencing identifies EN1 as a determinant of bone density and fracture

Author

Daniel I. Chasman, Tamara B. Harris, Rui Li, Natasja M. van Schoor, Klaudia Walter, Charles R. Farber, Josée Dostie, Chia-Ho Cheng, Angela Xuereb-Anastasi, Katie Cremin, Denis Paquette, José A. Riancho, Joyce B. J. van Meurs, Yasin Memari, André G. Uitterlinden, Mila Jhamai, Stephen R. Williams, Douglas P. Kiel, Elin Grundberg, J L Min, Charles Kooperberg, Melina Claussnitzer, Nicole Soranzo, Pascal P. Arp, Shu Huang Chen, Emma L. Duncan, Melissa M. Formosa, Nicholas J. Timpson, Paul L. Auer, Liesbeth Vandenput, Gaurav Garg, Matthew A. Hibbs, Hou-Feng Zheng, Cynthia A. Loomis, Dominique Gauguier, Susan M. Ring, James Fraser, Daniel Grinberg, Bente L. Langdahl, Xavier Nogués, Paul Leo, Alberto Roselló-Díez, Wen-Chi Chou, Warren A. Cheung, Kyung-Hyun Park-Min, Joyce Y. Tung, John A. Eisman, John P. Kemp, Lauren E. Mokry, Beatrice Melin, David M. Evans, Ling Oei, François Rousseau, Lenore Launer, Joshua R. Lewis, Jens Erik Beck Jensen, Nerea Alonso, Christopher S. Carlson, Dan Mellström, Andrea Z. LaCroix, Olle Svensson, Yanhua Zhou, M. Carola Zillikens, Unnur Thorsteinsdottir, Vincenzo Forgetta, Chitra Lekha Dahia, Jeroen van Rooij, Paul M. Ridker, Adrian Sayers, Richard L. Prince, Beth Wilmot, Stephen Kaptoge, Carolina Medina-Gomez, David Karasik, Rebecca D. Jackson, Natalia Garcia-Giralt, David W. Rowe, Kay-Tee Khaw, Evangelia E. Ntzani, Li Hsu, Tuan V. Nguyen, Cornelia M. van Duijn, Jonathan Reeve, Petr Danecek, Celia M. T. Greenwood, Jeffrey Haessler, Ulrike Peters, Magnus Karlsson, David Goltzman, Nathalie van der Velde, George Davey-Smith, Tomi Pastinen, A.W. Enneman, Sylvie Giroux, Daniel S. Evans, Kari Stefansson, Katerina Trajanoska, Lynda M. Rose, Cheryl L. Ackert-Bicknell, Göran Hallmans, David A. Hinds, Kwangbom Choi, Albert V. Smith, Sophie Calderari, Mhairi Marshall, Kristin Siggeirsdottir, Xi Jiang, Matthew A. Brown, Jonathan H Tobias, Stuart H. Ralston, Johanne Bussiere, J. Brent Richards, Tim D. Spector, Najaf Amin, Celia L Gregson, Carrie M. Nielson, L. Adrienne Cupples, Yi-Hsiang Hsu, Albert Hofman, Gudmar Thorleifsson, Gregory J. Tranah, Ulrika Pettersson-Kymmer, José M. Olmos, Bing Ge, Claes Ohlsson, Matthew T. Maurano, Aaron Kleinman, Karol Estrada, Tony Kwan, Ching-Ti Liu, Fernando Rivadeneira, María T. Zarrabeitia, Franco Giulianini, Eric S. Orwoll, Alireza Moayyeri, Fiona E. McGuigan, Lisette C. P. G. M. de Groot, Shane A. McCarthy, Richard Durbin, Joel Eriksson, Carl Wibom, Charlotta Uggla, Robert Kraaij, Claus Christiansen, Soizik Berlivet, Jie Huang, Östen Ljunggren, Scott Wilson, Fjorda Koromani, Alexandra L. Joyner, Kristina Åkesson, Brooke Gardiner, Unnur Styrkarsdottir, V. Gudnason, A. Pernille Hermann, McGill University = Université McGill [Montréal, Canada], Hebrew SeniorLife [Boston], Department of Medicine, Harvard Medical School [Boston] (HMS)-Beth Israel Deaconess Medical Center [Boston] (BIDMC), Harvard Medical School [Boston] (HMS), Broad Institute of MIT and Harvard (BROAD INSTITUTE), Harvard Medical School [Boston] (HMS)-Massachusetts Institute of Technology (MIT)-Massachusetts General Hospital [Boston], Centre de Recherche des Cordeliers (CRC (UMR_S_1138 / U1138)), École pratique des hautes études (EPHE), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Université Paris Diderot - Paris 7 (UPD7)-Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU), ProdInra, Migration, Epidemiology and Data Science, EMGO - Musculoskeletal health, APH - Amsterdam Public Health, AMS - Amsterdam Movement Sciences, Geriatrics, Erasmus MC other, Internal Medicine, Epidemiology, Pediatric Surgery, and Universitat de Barcelona

Subjects

Bone density, [SDV.MHEP.PHY] Life Sciences [q-bio]/Human health and pathology/Tissues and Organs [q-bio.TO], Bioinformatics, Bone densitometry, Fractures, Bone, Mice, 0302 clinical medicine, Gene Frequency, Bone Density, Osteoporosis -- Genetic aspects, Exome, Genetics, 0303 health sciences, education.field_of_study, Multidisciplinary, [SDV.MHEP] Life Sciences [q-bio]/Human health and pathology, Genomics, Europe, Female, Genotype, Population, European Continental Ancestry Group, 030209 endocrinology & metabolism, Locus (genetics), Biology, Bone and Bones, White People, Article, 03 medical and health sciences, Ossos -- Malalties -- Aspectes genètics, Densitometria òssia, [SDV.MHEP.PHY]Life Sciences [q-bio]/Human health and pathology/Tissues and Organs [q-bio.TO], Life Science, Animals, Humans, Genetic Predisposition to Disease, Bones -- Diseases -- Diagnosis, 1000 Genomes Project, Genomes, education, Allele frequency, 030304 developmental biology, VLAG, Whole genome sequencing, Global Nutrition, Homeodomain Proteins, Wereldvoeding, Genome, Human, Genetic Variation, Sequence Analysis, DNA, Minor allele frequency, Wnt Proteins, Disease Models, Animal, Osteoporosis, Fractures, Imputation (genetics), [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology

Abstract

A full list of authors and affiliations appears on page 5 of this article., The extent to which low-frequency (minor allele frequency (MAF) between 1-5%) and rare (MAF ≤ 1%) variants contribute to complex traits and disease in the general population is mainly unknown. Bone mineral density (BMD) is highly heritable, a major predictor of osteoporotic fractures, and has been previously associated with common genetic variants, as well as rare, population-specific, coding variants. Here we identify novel non-coding genetic variants with large effects on BMD (ntotal = 53,236) and fracture (ntotal = 508,253) in individuals of European ancestry from the general population. Associations for BMD were derived from whole-genome sequencing (n = 2,882 from UK10K (ref. 10); a population-based genome sequencing consortium), whole-exome sequencing (n = 3,549), deep imputation of genotyped samples using a combined UK10K/1000 Genomes reference panel (n = 26,534), and de novo replication genotyping (n = 20,271). We identified a low-frequency non-coding variant near a novel locus, EN1, with an effect size fourfold larger than the mean of previously reported common variants for lumbar spine BMD (rs11692564(T), MAF = 1.6%, replication effect size = +0.20 s.d., Pmeta = 2 × 10-14), which was also associated with a decreased risk of fracture (odds ratio = 0.85; P = 2 × 10-11; ncases = 98,742 and ncontrols = 409,511). Using an En1cre/flox mouse model, we observed that conditional loss of En1 results in low bone mass, probably as a consequence of high bone turnover. We also identified a novel low-frequency non-coding variant with large effects on BMD near WNT16 (rs148771817(T), MAF = 1.2%, replication effect size = +0.41 s.d., Pmeta = 1 × 10-11). In general, there was an excess of association signals arising from deleterious coding and conserved non-coding variants. These findings provide evidence that low-frequency non-coding variants have large effects on BMD and fracture, thereby providing rationale for whole-genome sequencing and improved imputation reference panels to study the genetic architecture of complex traits and disease in the general population., peer-reviewed

Published

2015

43. LRP5 coding polymorphisms influence the variation of peak bone mass in a normal population of French-Canadian women

Author

Guy Cardinal, Sylvie Giroux, Latifa Elfassihi, Nathalie Laflamme, and François Rousseau

Subjects

musculoskeletal diseases, Peak bone mass, Adult, Linkage disequilibrium, medicine.medical_specialty, Canada, Histology, Heel, Bone density, Physiology, Endocrinology, Diabetes and Metabolism, Polymorphism (computer science), Bone Density, Internal medicine, medicine, Humans, LDL-Receptor Related Proteins, Femoral neck, Aged, Bone mineral, Aged, 80 and over, Polymorphism, Genetic, business.industry, Haplotype, Middle Aged, Hormones, medicine.anatomical_structure, Endocrinology, Low Density Lipoprotein Receptor-Related Protein-5, Haplotypes, Female, France, Menopause, business

Abstract

Introduction Bone mineral density has a strong genetic component but it is also influenced by environmental factors making it a complex trait to study. LRP5 gene was previously shown to be involved in rare diseases affecting bone mass. Mutations associated with gain-of-function were described as well as loss-of-function mutations. Following this discovery, many frequent LRP5 polymorphisms were tested against the variation of BMD in the normal population. Materials and methods Heel bone parameters (SOS, BUA) were measured by right calcaneal QUS in 5021 healthy French-Canadian women and for 2104 women, BMD evaluated by DXA at two sites was available (femoral neck (FN) and lumbar spine (LS)). Among women with QUS measures and those with DXA measures, 26.5% and 32.8% respectively were premenopausal, 9.2% and 10.7% were perimenopausal and 64.2% and 56.5% were postmenopausal. About a third of the peri- and postmenopausal women never received hormone therapy. Two single nucleotide coding polymorphisms (Val667Met and Ala1330Val) in LRP5 gene were genotyped by allele-specific PCR. All bone measures were tested individually for associations with each polymorphism by analysis of covariance with adjustment for non genetic risk factors. Furthermore, haplotype analysis was performed to take into account the strong linkage disequilibrium between the two polymorphisms. Results and conclusion The two LRP5 polymorphisms were found to be associated with all five bone measures (L2L4 and femoral neck DXA as well as heel SOS, BUA and stiffness index) in the whole sample. Premenopausal women drove the association as expected from the proposed role of LRP5 in peak bone mass. Our results suggest that the Val 667 Met polymorphism is the causative variant but this remains to be functionally proven.

Published

2006

44. A frequent regulatory variant of the estrogen-related receptor alpha gene associated with BMD in French-Canadian premenopausal women

Author

Kenneth Morgan, Latifa Elfassihi, Vincent Giguère, Nathalie Laflamme, Sylvie Giroux, Sylvie Dodin, J. Concepción Loredo-Osti, Claudine Blanchet, and François Rousseau

Subjects

musculoskeletal diseases, Adult, medicine.medical_specialty, Canada, Heel, DNA, Complementary, Genotype, Endocrinology, Diabetes and Metabolism, Osteoporosis, Receptors, Cytoplasmic and Nuclear, Biology, Bone and Bones, Bone remodeling, Estrogen-related receptor, Lumbar, Absorptiometry, Photon, Bone Density, Internal medicine, medicine, Humans, Orthopedics and Sports Medicine, Genetic association, Femoral neck, Gene Library, Ultrasonography, Lumbar Vertebrae, Polymorphism, Genetic, Femur Neck, Genetic Variation, Middle Aged, medicine.disease, Endocrinology, medicine.anatomical_structure, Premenopause, Receptors, Estrogen, Multivariate Analysis, Female

Abstract

Genes are important BMD determinants. We studied the association of an ESRRA gene func- tional variant with BMD in 1335 premenopausal women. The ESRRA genotype was an independent predictor of L 2 -L 4 BMD, with an effect similar to smoking and equivalent to a 10-kg difference in weight. Introduction: Several genetic polymorphisms have been associated with osteoporosis or osteoporosis frac- tures, but no functional effect has been shown for most of these gene variants. Because functional studies have implicated estrogen-related receptor (ESRRA) in bone metabolism, we evaluated whether a recently described regulatory variant of the ESRRA gene is associated with lumbar and hip BMD as measured by DXA and with heel bone parameters as measured by quantitative ultrasound (QUS). Materials and Methods: Heel bone parameters were measured by right calcaneal QUS in 1335 healthy French-Canadian premenopausal women, and one-half of these women also had their BMD evaluated at two sites: femoral neck and lumbar spine (L2-L4) by DXA. All bone measures were tested separately for asso- ciation with the ESRRA genotype by analysis of covariance. The significance of the ESRRA contribution to the model was also assessed by two different permutation tests. Results: A statistically significant association between ESRRA genotype and lumbar spine BMD was ob- served: women carrying the long ESRRA genotype had a 3.9% (0.045 g/cm 2 ) higher lumbar spine BMD than those carrying the short ESRRA genotype (p 0.004), independently of other risk factors measured. This effect of ESRRA genotype is similar to the effect of smoking and equivalent to a 10-kg difference in weight. This association was confirmed by permutation tests (p 0.004). The same trend was observed for femoral neck BMD (2.6%, p 0.07). However, no association was observed between ESRRA and QUS heel bone measures. Conclusion: These results support the genetic influence of this ESRRA regulatory variant on BMD. J Bone Miner Res 2005;20:938-944. Published online on February 7, 2005; doi: 10.1359/JBMR.050203

Published

2004

45. Cyclosporin treatment alters protein phosphorylation in kidney membranes

Author

Sylvie Giroux, Richard Béliveau, Gérard F. Murphy, and Michel Demeule

Subjects

Cholera Toxin, Brush border, Biology, Kidney, Biochemistry, Methylation, Rats, Sprague-Dawley, Cyclosporin a, Animals, Protein phosphorylation, Virulence Factors, Bordetella, Phosphorylation, Protein kinase A, Molecular Biology, Protein kinase C, Protein Kinase C, Adenosine Diphosphate Ribose, Microvilli, Cell Membrane, Cell Biology, Protein-Tyrosine Kinases, Phosphoproteins, Molecular biology, Cyclic AMP-Dependent Protein Kinases, Rats, Molecular Weight, Membrane, Pertussis Toxin, Guanosine 5'-O-(3-Thiotriphosphate), Cyclosporine, Tyrosine kinase

Abstract

Phosphorylation, protein carboxyl methylation, and ADP-ribosylation were assayed in renal basolateral membranes and brush border membranes isolated from rats treated by subcutaneous administration of 5 or 10 mg/(kg∙day) of cyclosporin A (CsA) for 10 days to investigate potential alterations in signal transduction in kidney cortex. Protein carboxyl methylation of class II measured in membranes and in cytosolic fraction was not affected by CsA treatment. ADP-ribosylation performed in the presence of pertussis or cholera toxin was also similar in control and treated rats. However, changes in phosphorylation of endogenous substrates were observed in membranes and cytosol isolated from rats treated with 10 mg/(kg∙day) of CsA. Phosphorylation was increased for two brush border membrane proteins (56 and 77 kilodaltons (kDa)) by 47 and 24% and for two basolateral membrane proteins (51 and 80 kDa) by 28 and 29%, respectively. In the cytosolic fraction, phosphorylation of two proteins (31 and 65 kDa) was increased by 37% and that of 25- and 43-kDa proteins was reduced by 29%. Protein kinase A, protein kinase C, and tyrosine protein kinase activities were also determined in membranes. Increases in protein kinase C and tyrosine protein kinase activities were observed in basolateral membranes, but not in brush border membranes after cyclosporin A administration. Endogenous substrates for tyrosine kinase were also detected with an antiphosphotyrosine (PY20) monoclonal antibody. Densitometric analysis indicated that the phosphorylation of three proteins of high molecular masses (61, 132, and 183 kDa) was stimulated by CsA in basolateral membranes. Immunodetection of calcineurin with a monoclonal antibody directed against the β-subunit was similar in control and treated rats. These results suggest that cyclosporin A treatment may bring about changes in covalent modifications as an adaptative response in signal transduction in the kidney proximal tubule.Key words: cyclosporin A, kidney, membranes, carboxyl methylation, ADP-ribosylation, phosphorylation.

Published

1994

46. Phosphate Transport in Capillaries of the Blood-Brain Barrier

Author

Richard Béliveau, Lise Dallaire, and Sylvie Giroux

Subjects

Tight junction, Endothelium, Membrane transport, Phosphate, Blood–brain barrier, chemistry.chemical_compound, medicine.anatomical_structure, Biochemistry, chemistry, Interstitial fluid, Extracellular fluid, medicine, Biophysics, Transcellular

Abstract

Endothelial cells of cerebral capillaries form a continuous barrier between blood and brain interstitium. These endothelial cells, sealed together by tight junctions, do not possess fenestrations or transendothelial channels (1,2). Brain capillaries also contain a large number of mitochondria and are able to metabolize a variety of substrates (3, 4). This specialized endothelium regulates the movement of solutes between blood and brain. This is accomplished through carrier-mediated transport systems for hexoses, monocarboxylic acids, amino acids, nucleosides, purines and amines (5). Active transport pumps in the endothelial cells of brain capillaries appear to maintain the volume and composition of brain’s interstitial fluid (6). This extracellular fluid differs from plasma in that it is almost free of protein and differs from an ultrafiltrate of plasma by maintaining the concentration of various ions at distinct levels. In fact, the concentration of inorganic phosphate in the interstitial fluid of the brain is held between 0.5 and 1.0 mM, and the plasma level is maintained between 1.5 and 1.8 mM (7). Maintenance of this transcellular phosphate concentration gradient could be a result of transport mechanisms at the luminal and anti-luminal sites of the membranes of cerebral capillaries. The relationship of inorganic phosphate to the phosphorylation processes could account for a regulation of the concentration of this ion by a membrane transport mechanism. Furthermore, capillary cells require phosphate for energy demands, as reflected by the large number of mitochondria, and for synthesis of nucleic acids and complex lipids (3). Phosphate transport in brain capillaries was studied with metabolically active capillaries isolated from bovine cortex (8).

Published

1993

47. Regulation of phosphate transport by second messengers in capillaries of the blood-brain barrier

Author

Richard Béliveau, Lise Dallaire, and Sylvie Giroux

Subjects

medicine.medical_specialty, Cholera Toxin, G protein, Vasoactive intestinal peptide, Biophysics, Parathyroid hormone, In Vitro Techniques, medicine.disease_cause, Pertussis toxin, Biochemistry, Second Messenger Systems, Muscle, Smooth, Vascular, Phosphates, chemistry.chemical_compound, Internal medicine, 1-Methyl-3-isobutylxanthine, Phorbol Esters, medicine, Animals, Virulence Factors, Bordetella, Growth Substances, Cerebral Cortex, Cholera toxin, Isoproterenol, Biological Transport, Cell Biology, Phosphate, Angiotensin II, Hormones, Capillaries, Kinetics, Endocrinology, chemistry, Bucladesine, Pertussis Toxin, Blood-Brain Barrier, Parathyroid Hormone, Second messenger system, Cattle

Abstract

Regulation of phosphate uptake by the blood-brain barrier was studied in isolated bvine capillaries. Dibutyryl cAMP, in the presence of 3-isobutylmethylxanthine, resulted in a dose-dependent inhibition of phosphate uptake. Phosphate influx, with or without 3-isobutylmethylxanthine, was not different. Inhibition of phosphate uptake was also observed when capillaries were preincubated with isoproterenol, parathyroid hormone, insulin and acidic or basic fibroblast growth factors. Treatment of capillaries with vasoactive intestinal peptide, prostaglandin E 1 , angiotensin II, epidermal growth factor and phorbol esters did not affect phosphate transport. Endothelin I increased phosphate uptake by 15%. Preincubation with cholera toxin also resulted in a dose-dependent decrease in phosphate uptake. In addition, pertussis toxin inhibited phosphate transport by 29%, but only in the presence of 3-isobutylmethylxanthine. These results demonstrate that generation of second messengers, following receptor stimulation, can induce physiological effects on capillary phosphate influx and suggest that G proteins may modulate this transport.

Published

1992

48. The Contribution of Founder Mutations to Early-Onset Breast Cancer in French-Canadian Women

Author

Parviz Ghadirian, Robert Royer, Sylvie Giroux, Shiyu Zhang, Phil Zhang, Eve Fafard, Ginette Martin, André Robidoux, C Potvin, E. Nassif, Erica Patocskai, Steven A. Narod, Mohammad R. Akbari, William D. Foulkes, N Larouche, Rami Younan, and M. Costa

Subjects

Gynecology, Oncology, Cancer Research, medicine.medical_specialty, Mutation, education.field_of_study, business.industry, PALB2, Population, Cancer, Odds ratio, medicine.disease_cause, medicine.disease, Breast cancer, Internal medicine, medicine, skin and connective tissue diseases, Ovarian cancer, education, business, CHEK2

Abstract

Background: In an ethnically-homogeneous population, it is valuable to identify founder mutations in cancer-predisposing genes. Founder mutations have been found in four breast cancer predisposing genes in French-Canadian breast cancer families. The frequencies of the mutant alleles have not been measured in a large series of unselected breast cancer patients from Quebec, nor in healthy controls. These estimates are necessary to measure their contribution to the hereditary burden of breast cancer in Quebec and to help develop genetic screening policies which are appropriate for the province.Methods: We studied 564 French-Canadian women with early-onset invasive breast cancer who were treated at a single Montreal hospital. Patients had been diagnosed at age 50 or less, and were ascertained between 2004 and 2008. We screened all 564 patients for nine founder mutations; four in BRCA1, three in BRCA2 and one each in PALB2 and CHEK2. We also studied 6433 DNA samples from newborn infants from the Quebec City area to estimate the frequency of the nine variant alleles in the French-Canadian population.Results: We identified a mutation in 36 of the 564 breast cancer cases (6.4%) and in 35 of 6443 controls (0.5%). In the breast cancer patients, the majority of mutations were in BRCA2 (54%). However, in the general population (newborn infants), the majority of mutations were in CHEK2 (54%). The odds ratio for breast cancer to age 50, given a BRCA1 mutation was 10.1 (95% CI: 3.7 to 28) and given a BRCA2 mutation was 29.5 (95% CI: 12.9 – 67). The odds ratio for breast cancer to age 50, given a CHEK2 mutation was 3.6 (95% CI: 1.4 – 9.1). One-half of the women with a mutation had a first or second-degree relative diagnosed with breast or ovarian cancer. Citation Information: Cancer Res 2009;69(24 Suppl):Abstract nr 902.

Published

2009

49. Association With Replication Between Estrogen-Related Receptor Gamma (ESRRG) Polymorphisms and Bone Phenotypes in Women of European Ancestry

Author

François Rousseau, Nathalie Laflamme, Latifa Elfassihi, Alexandre Bureau, Sylvie Giroux, and David E. C. Cole

Subjects

Adult, Peak bone mass, medicine.medical_specialty, Bone density, Bone disease, Endocrinology, Diabetes and Metabolism, Osteoporosis, Estrogen receptor, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, Bone Density, Internal medicine, medicine, Humans, Genetic Predisposition to Disease, Orthopedics and Sports Medicine, Genetic Association Studies, Aged, Ultrasonography, Aged, 80 and over, Ontario, Bone mineral, Lumbar Vertebrae, Polymorphism, Genetic, Femur Neck, business.industry, Estrogen Replacement Therapy, Quebec, Middle Aged, medicine.disease, Phenotype, Endocrinology, Haplotypes, Receptors, Estrogen, Female, Heel, business, Estrogen receptor alpha

Abstract

Osteoporosis is a bone disease characterized by low bone mineral density (BMD), a highly heritable polygenic trait. Women are more prone than men to develop osteoporosis owing to a lower peak bone mass and accelerated bone loss at menopause. Lack of estrogen thus is a major risk factor for osteoporosis. In addition to having strong similarity to the estrogen receptor 1 (ESR1), the orphan nuclear estrogen-related receptor gamma (ESRRgamma) is widely expressed and shows overlap with ESR1 expression in tissues where estrogen has important physiologic functions. For these reasons, we have undertaken a study of ESRRgamma sequence variants in association with bone measurements [heel quantitative ultrasound (QUS) by measurements of broadband ultrasound attenuation (BUA), speed of sound (SOS), and stiffness index (SI) and dual-energy X-ray absorptiometry (DXA) at the femoral neck (FN) and lumbar spine (LS)]. A silent variant was found to be associated with multiple bone measurements (LS, BUA, SOS, and SI), the p values ranging from .006 to .04 in a sample of 5144 Quebec women. The region of this variant was analyzed using the HapMap database and the Gabriel method to define a block of 20 kb. Using the Tagger method, eight TagSNPs were identified and genotyped in a sample of 1335 women. Four of these SNPs capture the five major block haplotypes. One SNP (rs2818964) and one haplotype were significantly associated with multiple bone measures. All SNPs involved in the associations were analyzed in two other sample sets with significant results in the same direction. These results suggest involvement of ESRRgamma in the determination of bone density in women.

Published

2009

50. CYP1A1: Ethnic and Population Differences in Allelic Frequencies and Interpretation of Bone Biology Studies

Author

Latifa Elfassihi, Sylvie Giroux, and François Rousseau

Subjects

Genetics, education.field_of_study, Bone density, Endocrinology, Diabetes and Metabolism, Interpretation (philosophy), Population, Ethnic group, Biology, Genotype frequency, Orthopedics and Sports Medicine, Bone biology, Allele, education, Allele frequency

Published

2006