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151. A method to assess the clinical significance of unclassified variants in the BRCA1 and BRCA2 genes based on cancer family history

Author

Garcia, EBG, Oosterwijk, JC, Timmermans, M, van Asperen, CJ, Hogervorst, FBL, Hoogerbrugge, N, Oldenburg, Rogier, Verhoef, S, Dommering, CJ, Ausems, MGEM, van Os, TAM, van der Hout, AH, Ligtenberg, M, van den Ouweland, Ans, van der Luijt, RB, Wijnen, JT, Gille, JJP, Lindsey, PJ, Devilee, P, Blok, MJ, Vreeswijk, MPG, Garcia, EBG, Oosterwijk, JC, Timmermans, M, van Asperen, CJ, Hogervorst, FBL, Hoogerbrugge, N, Oldenburg, Rogier, Verhoef, S, Dommering, CJ, Ausems, MGEM, van Os, TAM, van der Hout, AH, Ligtenberg, M, van den Ouweland, Ans, van der Luijt, RB, Wijnen, JT, Gille, JJP, Lindsey, PJ, Devilee, P, Blok, MJ, and Vreeswijk, MPG

Abstract

Introduction Unclassified variants (UVs) in the BRCA1/BRCA2 genes are a frequent problem in counseling breast cancer and/or ovarian cancer families. Information about cancer family history is usually available, but has rarely been used to evaluate UVs. The aim of the present study was to identify which is the best combination of clinical parameters that can predict whether a UV is deleterious, to be used for the classification of UVs. Methods We developed logistic regression models with the best combination of clinical features that distinguished a positive control of BRCA pathogenic variants (115 families) from a negative control population of BRCA variants initially classified as UVs and later considered neutral (38 families). Results The models included a combination of BRCAPRO scores, Myriad scores, number of ovarian cancers in the family, the age at diagnosis, and the number of persons with ovarian tumors and/ or breast tumors. The areas under the receiver operating characteristic curves were respectively 0.935 and 0.836 for the BRCA1 and BRCA2 models. For each model, the minimum receiver operating characteristic distance (respectively 90% and 78% specificity for BRCA1 and BRCA2) was chosen as the cutoff value to predict which UVs are deleterious from a study population of 12 UVs, present in 59 Dutch families. The p. S1655F, p. R1699W, and p. R1699Q variants in BRCA1 and the p. Y2660D, p. R2784Q, and p. R3052W variants in BRCA2 are classified as deleterious according to our models. The predictions of the p. L246V variant in BRCA1 and of the p. Y42C, p. E462G, p. R2888C, and p. R3052Q variants in BRCA2 are in agreement with published information of them being neutral. The p. R2784W variant in BRCA2 remains uncertain. Conclusions The present study shows that these developed models are useful to classify UVs in clinical genetic practice.

Published
2009

152. Attitude towards pre-implantation genetic diagnosis for hereditary cancer

Author

Lammens, C, Bleiker, E, Aaronson, N, Vriends, A, Ausems, M, Jansweijer, M, Wagner, Anja, Sijmons, R, van den Ouweland, Ans, van der Luijt, R, Spruijt, L, Garcia, EG, Ruijs, M, Verhoef, S, Lammens, C, Bleiker, E, Aaronson, N, Vriends, A, Ausems, M, Jansweijer, M, Wagner, Anja, Sijmons, R, van den Ouweland, Ans, van der Luijt, R, Spruijt, L, Garcia, EG, Ruijs, M, and Verhoef, S

Abstract

The use of pre-implantation genetic diagnosis (PGD) for hereditary cancer is subject to on-going debate, particularly among professionals. This study evaluates the attitude towards PGD and attitude-associated characteristics of those concerned: family members with a hereditary cancer predisposition. Forty-eight Von Hippel-Lindau and 18 Li-Fraumeni Syndrome families were identified via the 9 family cancer clinics in the Netherlands. In total, 216 high risk family members and partners were approached, of whom 179 (83%) completed a self-report questionnaire. Of the high risk family members, 35% expressed a positive attitude towards PGD. Those with a current desire to have children were significantly more likely to have a positive attitude: 48% would consider the use of PGD. No other sociodemographic, medical or psychosocial variables were associated significantly with a positive attitude. The most frequently reported advantage of PGD is the avoidance of a possible pregnancy termination. Uncertainty about late effects was the most frequently reported disadvantage. These results indicate that approximately half of those contemplating a future pregnancy would consider the use of PGD. The actual uptake, however, is expected to be lower. There is no indication that psychosocial factors affect interest in PGD.

Published
2009

153. A simple method for co-segregation analysis to evaluate the pathogenicity of unclassified variants; BRCA1 and BRCA2 as an example

Author

Mohammadi, L, Vreeswijk, MP, Oldenburg, Rogier, van den Ouweland, Ans, Oosterwijk, JC, van der Hout, AH, Hoogerbrugge, N, Ligtenberg, M, Ausems, MG, van der Luijt, RB, Dommering, CJ, Gille, JJ, Verhoef, S, Hogervorst, FB, van Os, TA, Garcia, EG, Blok, MJ, Wijnen, JT, Helmer, Q, Devilee, P, van Asperen, CJ, van Houwelingen, HC, Mohammadi, L, Vreeswijk, MP, Oldenburg, Rogier, van den Ouweland, Ans, Oosterwijk, JC, van der Hout, AH, Hoogerbrugge, N, Ligtenberg, M, Ausems, MG, van der Luijt, RB, Dommering, CJ, Gille, JJ, Verhoef, S, Hogervorst, FB, van Os, TA, Garcia, EG, Blok, MJ, Wijnen, JT, Helmer, Q, Devilee, P, van Asperen, CJ, and van Houwelingen, HC

Abstract

Background: Assessment of the clinical significance of unclassified variants (UVs) identified in BRCA1 and BRCA2 is very important for genetic counselling. The analysis of co-segregation of the variant with the disease in families is a powerful tool for the classification of these variants. Statistical methods have been described in literature but these methods are not always easy to apply in a diagnostic setting. Methods: We have developed an easy to use method which calculates the likelihood ratio (LR) of an UV being deleterious, with penetrance as a function of age of onset, thereby avoiding the use of liability classes. The application of this algorithm is publicly available http://www.msbi.nl/cosegregation. It can easily be used in a diagnostic setting since it requires only information on gender, genotype, present age and/or age of onset for breast and/or ovarian cancer. Results: We have used the algorithm to calculate the likelihood ratio in favour of causality for 3 UVs in BRCA1 (p.M18T, p.S1655F and p.R1699Q) and 5 in BRCA2 (p.E462G p.Y2660D, p.R2784Q, p.R3052W and p.R3052Q). Likelihood ratios varied from 0.097 (BRCA2, p.E462G) to 230.69 (BRCA2, p.Y2660D). Typing distantly related individuals with extreme phenotypes (i.e. very early onset cancer or old healthy individuals) are most informative and give the strongest likelihood ratios for or against causality. Conclusion: Although co-segregation analysis on itself is in most cases insufficient to prove pathogenicity of an UV, this method simplifies the use of co-segregation as one of the key features in a multifactorial approach considerably.

Published
2009

154. The contribution of CHEK2 to the TP53-negative Li-Fraumeni phenotype

Author

Ruijs, MWG, Broeks, A, Menko, FH, Ausems, MGEM, Wagner, Anja, Oldenburg, Rogier, Meijers-Heijboer, EJ, van 't Veer, LJ (Laura), Verhoef, S, Ruijs, MWG, Broeks, A, Menko, FH, Ausems, MGEM, Wagner, Anja, Oldenburg, Rogier, Meijers-Heijboer, EJ, van 't Veer, LJ (Laura), and Verhoef, S

Abstract

Background: CHEK2 has previously been excluded as a major cause of Li-Fraumeni syndrome (LFS). One particular CHEK2 germline mutation, c.1100delC, has been shown to be associated with elevated breast cancer risk. The prevalence of CHEK2*1100delC differs between populations and has been found to be relatively high in the Netherlands. The question remains nevertheless whether CHEK2 germline mutations contribute to the Li-Fraumeni phenotype. Methods: We have screened 65 Dutch TP53-negative LFS/LFL candidate patients for CHEK2 germline mutations to determine their contribution to the LFS/LFL phenotype. Results: We identified six index patients with a CHEK2 sequence variant, four with the c.1100delC variant and two sequence variants of unknown significance, p.Phe328Ser and c.1096-?_1629+? del. Conclusion: Our data show that CHEK2 is not a major LFS susceptibility gene in the Dutch population. However, CHEK2 might be a factor contributing to individual tumour development in TP53-negative cancer-prone families.

Published
2009

158. Colorectal cancer risk variants at 8q23.3 and 11q23.1 are associated with disease phenotype in APC mutation carriers.

Author

Ghorbanoghli, Z., Nieuwenhuis, M., Houwing-Duistermaat, J., Jagmohan-Changur, S., Hes, F., Tops, C., Wagner, A., Aalfs, C., Verhoef, S., Gómez García, E., Sijmons, R., Menko, F., Letteboer, T., Hoogerbrugge, N., Wezel, T., Vasen, H., and Wijnen, J.

Abstract

Familial adenomatous polyposis (FAP) is a dominantly inherited syndrome caused by germline mutations in the APC gene and characterized by the development of multiple colorectal adenomas and a high risk of developing colorectal cancer (CRC). The severity of polyposis is correlated with the site of the APC mutation. However, there is also phenotypic variability within families with the same underlying APC mutation, suggesting that additional factors influence the severity of polyposis. Genome-wide association studies identified several single nucleotide polymorphisms (SNPs) that are associated with CRC. We assessed whether these SNPs are associated with polyp multiplicity in proven APC mutation carriers. Sixteen CRC-associated SNPs were analysed in a cohort of 419 APC germline mutation carriers from 182 families. Clinical data were retrieved from the Dutch Polyposis Registry. Allele frequencies of the SNPs were compared for patients with <100 colorectal adenomas versus patients with ≥100 adenomas, using generalized estimating equations with the APC genotype as a covariate. We found a trend of association of two of the tested SNPs with the ≥100 adenoma phenotype: the C alleles of rs16892766 at 8q23.3 (OR 1.71, 95 % CI 1.05-2.76, p = 0.03, dominant model) and rs3802842 at 11q23.1 (OR 1.51, 95 % CI 1.03-2.22, p = 0.04, dominant model). We identified two risk variants that are associated with a more severe phenotype in APC mutation carriers. These risk variants may partly explain the phenotypic variability in families with the same APC gene defect. Further studies with a larger sample size are recommended to evaluate and confirm the phenotypic effect of these SNPs in FAP. [ABSTRACT FROM AUTHOR]

Published
2016
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159. Low prevalence of HER2 positivity amongst BRCA1 and BRCA2 mutation carriers and in primary BRCA screens.

Author

Evans, D., Lalloo, F., Howell, S., Verhoef, S., Woodward, E., and Howell, A.

Abstract

The aim of this study is to delineate more clearly the prevalence of HER2+ breast cancer in women with germline BRCA1/2 mutations. For this purpose, we analysed primary mutation screens on women with breast cancer with unequivocal HER2 amplification and assessed the proportion of BRCA1 and BRCA2 breast cancers that were HER2+ comparing this with the existing literature. The results are that 1063 primary BRCA screens had confirmed tumour HER2 status. If HER2+ only 2.5 % (4/156) and 3.2 % (5/156) of women had a BRCA1 or BRCA2 mutation identified respectively; compared to 27.7 % (115/415) and 8.2 % (34/415) with triple negative tumours. Only 2.1 % (4/195) women with BRCA1-related breast cancer had HER2 amplified breast cancers rising to 6.8 % ( n = 12, p = 0.04) in BRCA2. These rates are in keeping with most of the existing literature except a recent large multicenter report which documented higher rates but with no control group. The study concluded that true HER2-amplified breast cancers are rare amongst BRCA1 mutation carriers and are less common in BRCA2 than background rates. [ABSTRACT FROM AUTHOR]

Published
2016
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161. A DGGE system for comprehensive mutation screening of BRCA1 and BRCA2: application in a Dutch cancer clinic setting.

Author

Hout, A.H. van der, Ouweland, A.M.W. van den, Luijt, R.B. van der, Gille, H.J., Bodmer, D., Bruggenwirth, H.T., Mulder, I.M., Vlies, P., Elfferich, P., Huisman, M., Berge, A.M. ten, Kromosoeto, J., Jansen, R.P., Zon, P.H. van, Vriesman, T., Arts, N., Lange, M.B., Oosterwijk-Wakka, J.C., Meijers-Heijboer, H., Ausems, M.G.E.M., Hoogerbrugge-van der Linden, N., Verhoef, S., Halley, D.J., Vos, Y.J., Hogervorst, F.B.L., Ligtenberg, M.J.L., Hofstra, R.M., Hout, A.H. van der, Ouweland, A.M.W. van den, Luijt, R.B. van der, Gille, H.J., Bodmer, D., Bruggenwirth, H.T., Mulder, I.M., Vlies, P., Elfferich, P., Huisman, M., Berge, A.M. ten, Kromosoeto, J., Jansen, R.P., Zon, P.H. van, Vriesman, T., Arts, N., Lange, M.B., Oosterwijk-Wakka, J.C., Meijers-Heijboer, H., Ausems, M.G.E.M., Hoogerbrugge-van der Linden, N., Verhoef, S., Halley, D.J., Vos, Y.J., Hogervorst, F.B.L., Ligtenberg, M.J.L., and Hofstra, R.M.

Abstract

Contains fulltext : 51002.pdf (publisher's version ) (Closed access), Rapid and reliable identification of deleterious changes in the breast cancer genes BRCA1 and BRCA2 has become one of the major issues in most DNA services laboratories. To rapidly detect all possible changes within the coding and splice site determining sequences of the breast cancer genes, we established a semiautomated denaturing gradient gel electrophoresis (DGGE) mutation scanning system. All exons of both genes are covered by the DGGE scan, comprising 120 amplicons. We use a semiautomated approach, amplifying all individual amplicons with the same PCR program, after which the amplicons are pooled. DGGE is performed using three slightly different gel conditions. Validation was performed using DNA samples with known sequence variants in 107 of the 120 amplicons; all variants were detected. This DGGE mutation scanning, in combination with a PCR test for two Dutch founder deletions in BRCA1 was then applied in 431 families in which 52 deleterious changes and 70 unclassified variants were found. Fifteen unclassified variants were not reported before. The system was easily adopted by five other laboratories, where in another 3,593 families both exons 11 were analyzed by the protein truncation test (PTT) and the remaining exons by DGGE. In total, a deleterious change (nonsense, frameshift, splice-site mutation, or large deletion) was found in 661 families (16.4%), 462 in BRCA1 (11.5%), 197 in BRCA2 (4.9%), and in two index cases a deleterious change in both BRCA1 and BRCA2 was identified. Eleven deleterious changes in BRCA1 and 36 in BRCA2 had not been reported before. In conclusion, this DGGE mutation screening method for BRCA1 and BRCA2 is proven to be highly sensitive and is easy to adopt, which makes screening of large numbers of patients feasible. The results of screening of BRCA1 and BRCA2 in more than 4,000 families present a valuable overview of mutations in the Dutch population.

Published
2006

162. A multiplex PCR predictor for aCGH success of FFPE samples.

Author

Beers, E.H. van, Joosse, S.A., Ligtenberg, M.J.L., Fles, R., Hogervorst, F.B.L., Verhoef, S., Nederlof, P.M., Beers, E.H. van, Joosse, S.A., Ligtenberg, M.J.L., Fles, R., Hogervorst, F.B.L., Verhoef, S., and Nederlof, P.M.

Abstract

Contains fulltext : 50223.pdf (publisher's version ) (Closed access), Formalin-fixed, paraffin-embedded (FFPE) tissue archives are the largest and longest time-spanning collections of patient material in pathology archives. Methods to disclose information with molecular techniques, such as array comparative genomic hybridisation (aCGH) have rapidly developed but are still not optimal. Array comparative genomic hybridisation is one efficient method for finding tumour suppressors and oncogenes in solid tumours, and also for classification of tumours. The fastest way of analysing large numbers of tumours is through the use of archival tissue samples with first, the huge advantage of larger median follow-up time of patients studied and second, the advantage of being able to locate and analyse multiple tumours, even across generations, from related individuals (families). Unfortunately, DNA from archival tissues is not always suitable for molecular analysis due to insufficient quality. Until now, this quality remained undefined. We report the optimisation of a genomic-DNA isolation procedure from FFPE pathology archives in combination with a subsequent multiplex PCR-based quality-control that simply identified all samples refractory to further DNA-based analyses.

Published
2006

163. Fatale hartritmestoornis na toediening van suxamethonium aan een kraamvrouw die achteraf dystrophia myotonica bleek te hebben

Author

Wildschut, H.I.J., Verhoef, S., Schilder, J.L.A.M., and Hamel, B.C.J.

Subjects
Clinical description and delineation of genetic syndromes, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries), Klinische beschrijving en moleculaire definiëring van genetische syndromen
Abstract

Contains fulltext : 23890___.PDF (Publisher’s version ) (Open Access)

Published
1996

164. Multiplicity in polyp count and extracolonic manifestations in 40 Dutch patients with MYH associated polyposis coli (MAP).

Author

Nielsen, M., Franken, P.F., Reinards, T.H., Weiss, M.M., Wagner, A., Klift, H. van der, Kloosterman, S., Houwing-Duistermaat, J.J., Aalfs, C.M., Ausems, M.G.E.M., Brocker-Vriends, A.H., Gomez Garcia, E.B., Hoogerbrugge-van der Linden, N., Menko, F.H., Sijmons, R.H., Verhoef, S., Kuipers, E.J., Morreau, H., Breuning, M.H., Tops, C.M., Wijnen, J.T., Vasen, H.F., Fodde, R., Hes, F.J., Nielsen, M., Franken, P.F., Reinards, T.H., Weiss, M.M., Wagner, A., Klift, H. van der, Kloosterman, S., Houwing-Duistermaat, J.J., Aalfs, C.M., Ausems, M.G.E.M., Brocker-Vriends, A.H., Gomez Garcia, E.B., Hoogerbrugge-van der Linden, N., Menko, F.H., Sijmons, R.H., Verhoef, S., Kuipers, E.J., Morreau, H., Breuning, M.H., Tops, C.M., Wijnen, J.T., Vasen, H.F., Fodde, R., and Hes, F.J.

Abstract

Contains fulltext : 48879.pdf (publisher's version ) (Closed access), OBJECTIVE: To investigate the contribution of MYH associated polyposis coli (MAP) among polyposis families in the Netherlands, and the prevalence of colonic and extracolonic manifestations in MAP patients. METHODS: 170 patients with polyposis coli, who previously tested negative for APC mutations, were screened by denaturing gradient gel electrophoresis and direct sequencing to identify MYH germline mutations. RESULTS: Homozygous and compound heterozygous MYH mutations were identified in 40 patients (24%). No difference was found in the percentage of biallelic mutation carriers between patients with 10-99 polyps or 100-1000 polyps (29% in both groups). Colorectal cancer was found in 26 of the 40 patients with MAP (65%) within the age range 21 to 67 years (median 45). Complete endoscopic reports were available for 16 MAP patients and revealed five cases with gastro-duodenal polyps (31%), one of whom also presented with a duodenal carcinoma. Breast cancer occurred in 18% of female MAP patients, significantly more than expected from national statistics (standardised morbidity ratio = 3.75). CONCLUSIONS: Polyp numbers in MAP patients were equally associated with the attenuated and classical polyposis coli phenotypes. Two thirds of the MAP patients had colorectal cancer, 95% of whom were older than 35 years, and one third of a subset of patients had upper gastrointestinal lesions. Endoscopic screening of the whole intestine should be carried out every two years for all MAP patients, starting from age 25-30 years. The frequent occurrence of additional extraintestinal manifestations, such as breast cancer among female MAP patients, should be thoroughly investigated.

Published
2005

165. Cancer risks in BRCA2 families: estimates for sites other than breast and ovary.

Author

Asperen, C.J. van, Brohet, R.M., Meijers-Heijboer, E.J., Hoogerbrugge-van der Linden, N., Verhoef, S., Vasen, H.F., Ausems, M.G.E.M., Menko, F.H., Gomez Garcia, E.B., Klijn, J.G.M., Hogervorst, F.B.L., Houwelingen, J.C. van, Veer, L.J. van 't, Rookus, M.A., Leeuwen, F.E. van, Asperen, C.J. van, Brohet, R.M., Meijers-Heijboer, E.J., Hoogerbrugge-van der Linden, N., Verhoef, S., Vasen, H.F., Ausems, M.G.E.M., Menko, F.H., Gomez Garcia, E.B., Klijn, J.G.M., Hogervorst, F.B.L., Houwelingen, J.C. van, Veer, L.J. van 't, Rookus, M.A., and Leeuwen, F.E. van

Abstract

Contains fulltext : 48352.pdf (publisher's version ) (Closed access), BACKGROUND: In BRCA2 mutation carriers, increased risks have been reported for several cancer sites besides breast and ovary. As most of the families included in earlier reports were selected on the basis of multiple breast/ovarian cancer cases, it is possible that risk estimates may differ in mutation carriers with a less striking family history. METHODS: In the Netherlands, 139 BRCA2 families with 66 different pathogenic mutations were included in a nationwide study. To avoid testing bias, we chose not to estimate risk in typed carriers, but rather in male and female family members with a 50% prior probability of being a carrier (n = 1811). The relative risk (RR) for each cancer site with the exception of breast and ovarian cancer was determined by comparing observed numbers with those expected, based on Dutch cancer incidence rates. RESULTS: We observed an excess risk for four cancer sites: pancreas (RR 5.9; 95% confidence interval (CI) 3.2 to 10.0), prostate (2.5; 1.6 to 3.8), bone (14.4; 2.9 to 42.1) and pharynx (7.3; 2.0 to 18.6). A small increase was observed for cancer of the digestive tract (1.5; 1.1 to 1.9). Histological verification was available for 46% of the tumours. Nearly all increased risks reached statistical significance for men only. Cancer risks tended to be higher for people before the age of 65 years. Moreover, families with mutations outside the previously defined ovarian cancer cluster region tended to have a higher cancer risk. CONCLUSIONS: We found that BRCA2 carriers are at increased risk for cancers of the prostate and pancreas, and possibly bone and pharynx. Larger databases with extended follow up are needed to provide insight into mutation specific risks of selected carriers in BRCA2 families.

Published
2005

166. Discovering genetic profiles by array-CGH in familial breast tumors

Author

Nederlof, P.M. (author), Van Beers, E. (author), Joosse, S. (author), Hogervorst, F.B.L. (author), Wessels, L.F.A. (author), Devilee, P. (author), Cornelisse, C. (author), Oldenburg, R. (author), Verhoef, S. (author), Van 't Veer, L.J. (author), Nederlof, P.M. (author), Van Beers, E. (author), Joosse, S. (author), Hogervorst, F.B.L. (author), Wessels, L.F.A. (author), Devilee, P. (author), Cornelisse, C. (author), Oldenburg, R. (author), Verhoef, S. (author), and Van 't Veer, L.J. (author)

Published
2005

167. Abstract P4-11-01: Rapid genetic counseling and testing in newly diagnosed breast cancer patients, findings from an RCT

Author

Wevers, MR, primary, Ausems, MG, additional, Bleiker, EM, additional, Rutgers, EJ, additional, Witkamp, AJ, additional, Hahn, DE, additional, Brouwer, T, additional, Kuenen, MA, additional, van der Sanden-Melis, J, additional, van der Luijt, RB, additional, Hogervorst, FB, additional, van Dalen, T, additional, Theunissen, EB, additional, van Ooijen, B, additional, de Roos, MA, additional, Borgstein, PJ, additional, Vrouenraets, BC, additional, Huisman, JJ, additional, Bouma, WH, additional, Rijna, H, additional, Vente, JP, additional, Valdimarsdottir, H, additional, Verhoef, S, additional, and Aaronson, NK, additional

Published
2012
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168. A non-BRCA1/2 hereditary breast cancer sub-group defined by aCGH profiling of genetically related patients

Author

Didraga, M. A., primary, van Beers, E. H., additional, Joosse, S. A., additional, Brandwijk, K. I. M., additional, Oldenburg, R. A., additional, Wessels, L. F. A., additional, Hogervorst, F. B. L., additional, Ligtenberg, M. J., additional, Hoogerbrugge, N., additional, Verhoef, S., additional, Devilee, P., additional, and Nederlof, P. M., additional

Published
2011
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172. Regular surveillance for Li-fraumeni syndrome: advice, adherence and perceived benefits

Author

Lammens, C. R. M., primary, Bleiker, E. M. A., additional, Aaronson, N. K., additional, Wagner, A., additional, Sijmons, R. H., additional, Ausems, M. G. E. M., additional, Vriends, A. H. J. T., additional, Ruijs, M. W. G., additional, van Os, T. A. M., additional, Spruijt, L., additional, Gómez García, E. B., additional, Cats, A., additional, Nagtegaal, T., additional, and Verhoef, S., additional

Published
2010
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173. TP53 germline mutation testing in 180 families suspected of Li-Fraumeni syndrome: mutation detection rate and relative frequency of cancers in different familial phenotypes

Author

Ruijs, M. W. G., primary, Verhoef, S., additional, Rookus, M. A., additional, Pruntel, R., additional, van der Hout, A. H., additional, Hogervorst, F. B. L., additional, Kluijt, I., additional, Sijmons, R. H., additional, Aalfs, C. M., additional, Wagner, A., additional, Ausems, M. G. E. M., additional, Hoogerbrugge, N., additional, van Asperen, C. J., additional, Gomez Garcia, E. B., additional, Meijers-Heijboer, H., additional, ten Kate, L. P., additional, Menko, F. H., additional, and van 't Veer, L. J., additional

Published
2010
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175. Psychosocial impact of Von Hippel–Lindau disease: levels and sources of distress

Author

Lammens, CRM, primary, Bleiker, EMA, additional, Verhoef, S, additional, Hes, FJ, additional, Ausems, MGEM, additional, Majoor‐Krakauer, D, additional, Sijmons, RH, additional, Van Der Luijt, RB, additional, Van Den Ouweland, AMW, additional, Van Os, Tam, additional, Hoogerbrugge, N, additional, Gómez García, EB, additional, Dommering, CJ, additional, Gundy, CM, additional, and Aaronson, NK, additional

Published
2010
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179. An unbalanced submicroscopic translocation t(8;16)(q24.3;p13.3)pat associated with tuberous sclerosis complex, adult polycystic kidney disease, and hypomelanosis of Ito

Author

Eussen, H.J.F.M.M. (Bert), Verhoef, S., Fois, A., Halley, D.J.J. (Dicky), Bartalini, G. (Gabriella), Bakker, L. (Lida), Balestri, P. (Paolo), Lucca, C. di, Hemel, J.O. van, Dauwerse, H., Ouweland, A.M.W. (Ans) van den, Ris-Stalpers, C. (Carolyn), Eussen, H.J.F.M.M. (Bert), Verhoef, S., Fois, A., Halley, D.J.J. (Dicky), Bartalini, G. (Gabriella), Bakker, L. (Lida), Balestri, P. (Paolo), Lucca, C. di, Hemel, J.O. van, Dauwerse, H., Ouweland, A.M.W. (Ans) van den, and Ris-Stalpers, C. (Carolyn)

Abstract

We report on a familial submicroscopic translocation involving chromosomes 8 and 16. The proband of the family had a clinical picture suggestive of a large deletion in the chromosome 16p13.3 area, as he was affected with tuberous sclerosis complex (TSC) and had alpha thalassaemia trait, and his half brother, who also had TSC, may have suffered additionally from polycystic kidney disease (PKD). FISH studies provided evidence for a familial translocation t(8;16)(q24.3;p13.3) with an unbalanced form in the proband and a balanced form in the father and in a paternal aunt. The unbalanced translocation caused the index patient to be deleted for the chromosome 16p13.3-pter region, with the most proximal breakpoint described to date for terminal 16p deletions. In addition, FISH analysis showed a duplication for the distal 8q region. Since the index patient also had hypomelanosis of Ito (HI), either of the chromosomal areas involved in the translocation may be a candidate region for an HI determining gene. Furthermore, it is noteworthy that both carriers of the balanced translocation showed a nodular goitre, while the proband has hypothyroidism.

Published
2000

180. An unbalanced submicroscopic translocation t(8;16)(q24.3;p13.3) pat associated with tuberous sclerosis complex, adult polycystic kidney disease, and hypomelanosis of Ito

Author

Eussen, HJFMM (Bert), Bartalini, G, Bakker, Ingeborg, Balestri, P, di Lucca, C, Hemel, JO, Dauwerse, H, van den Ouweland, Ans, Ris-Stalpers, C, Verhoef, S, Halley, Dicky, Fois, A, Eussen, HJFMM (Bert), Bartalini, G, Bakker, Ingeborg, Balestri, P, di Lucca, C, Hemel, JO, Dauwerse, H, van den Ouweland, Ans, Ris-Stalpers, C, Verhoef, S, Halley, Dicky, and Fois, A

Published
2000

181. Timing of risk reducing mastectomy in breast cancer patients carrying a BRCA1/2 mutation: retrospective data from the Dutch HEBON study.

Author

Wevers, M., Schmidt, M., Engelhardt, E., Verhoef, S., Hooning, M., Kriege, M., Seynaeve, C., Collée, M., Asperen, C., Tollenaar, R., Koppert, L., Witkamp, A., Rutgers, E., Aaronson, N., Rookus, M., and Ausems, M.

Abstract

It is expected that rapid genetic counseling and testing (RGCT) will lead to increasing numbers of breast cancer (BC) patients knowing their BRCA1/2 carrier status before primary surgery. Considering the potential impact of knowing one's status on uptake and timing of risk-reducing contralateral mastectomy (RRCM), we aimed to evaluate trends over time in RRCM, and differences between carriers identified either before (predictively) or after (diagnostically) diagnosis. We collected data from female BRCA1/2 mutation carriers diagnosed with BC between 1995 and 2009 from four Dutch university hospitals. We compared the timing of genetic testing and RRCM in relation to diagnosis in 1995-2000 versus 2001-2009 for all patients, and predictively and diagnostically tested patients separately. Of 287 patients, 219 (76 %) had a diagnostic BRCA1/2 test. In this cohort, the median time from diagnosis to DNA testing decreased from 28 months for those diagnosed between 1995 and 2000 to 14 months for those diagnosed between 2001 and 2009 ( p < 0.001). Similarly, over time women in this cohort underwent RRCM sooner after diagnosis (median of 77 vs. 27 months, p = 0.05). Predictively tested women who subsequently developed BC underwent an immediate RRCM significantly more often than women who had a diagnostic test (21/61, 34 %, vs. 13/170, 7.6 %, p < 0.001). Knowledge of carrying a BRCA1/2 mutation when diagnosed with BC influenced decisions concerning primary surgery. Additionally, in more recent years, women who had not undergone predictive testing were more likely to undergo diagnostic DNA testing and RRCM sooner after diagnosis. This suggests the need for RGCT to guide treatment decisions. [ABSTRACT FROM AUTHOR]

Published
2015
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182. Breast Cancer Risk After Salpingo-Oophorectomy in Healthy BRCA1/2 Mutation Carriers: Revisiting the Evidence for Risk Reduction.

Author

Heemskerk-Gerritsen, B. A. M., Seynaeve, C., van Asperen, C. J., Ausems, M. G. E. M., Collée, J. M., van Doorn, H. C., Gomez Garcia, E. B., Kets, C. M., van Leeuwen, F. E., Meijers-Heijboer, H. E. J., Mourits, M. J. E., van Os, T. A. M., Vasen, H. F. A., Verhoef, S., Rookus, M. A., and Hooning, M. J.

Subjects
OVARIECTOMY, BRCA genes, GENETICS of breast cancer, BREAST cancer risk factors, GENETIC mutation
Abstract

Background: Previous studies have reported a breast cancer (BC) risk reduction of approximately 50% after risk-reducing salpingo-oophorectomy (RRSO) in BRCA1/2 mutation carriers, but may have been subject to several types of bias. The purpose of this nationwide cohort study was to assess potential bias in the estimated BC risk reduction after RRSO. Methods: We selected BRCA1/2 mutation carriers from an ongoing nationwide cohort study on Hereditary Breast and Ovarian Cancer in the Netherlands (HEBON). First, we replicated the analytical methods as previously applied in four major studies on BC risk after RRSO. Cox proportional hazards models were used to calculate hazard ratios and conditional logistic regression to calculate odds ratios. Secondly, we analyzed the data in a revised design in order to further minimize bias using an extended Cox model with RRSO as a time-dependent variable to calculate the hazard ratio. The most important differences between our approach and those of previous studies were the requirement of no history of cancer at the date of DNA diagnosis and the inclusion of person-time preceding RRSO. Results: Applying the four previously described analytical methods and the data of 551 to 934 BRCA1/2 mutation carriers with a median follow-up of 2.7 to 4.6 years, the odds ratio was 0.61 (95% confidence interval [CI] = 0.35 to 1.08), and the hazard ratios were 0.36 (95% CI = 0.25 to 0.53), 0.62 (95% CI = 0.39 to 0.99), and 0.49 (95% CI = 0.33 to 0.71), being similar to earlier findings. For the revised analysis, we included 822 BRCA1/2 mutation carriers. After a median follow-up period of 3.2 years, we obtained a hazard ratio of 1.09 (95% CI = 0.67 to 1.77). Conclusion: In previous studies, BC risk reduction after RRSO in BRCA1/2 mutation carriers may have been overestimated because of bias. Using a design that maximally eliminated bias, we found no evidence for a protective effect. [ABSTRACT FROM AUTHOR]

Published
2015
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183. Malignant pancreatic tumour within the spectrum of tuberous sclerosis complex in childhood

Author

Verhoef, S., Diemen-Steenvoorde, R. (R.) van, Akkersdijk, G.P. (George), Bax, N.M.A. (Klaas), Ariyurek, Y. (Yavuz), Hermans, C.J. (Caroline), Nieuwenhuizen, O. (Onno) van, Nikkels, P.G.J. (Peter), Lindhout, D. (Dick), Halley, D.J.J. (Dicky), Lips, K. (K.), Ouweland, A.M.W. (Ans) van den, Verhoef, S., Diemen-Steenvoorde, R. (R.) van, Akkersdijk, G.P. (George), Bax, N.M.A. (Klaas), Ariyurek, Y. (Yavuz), Hermans, C.J. (Caroline), Nieuwenhuizen, O. (Onno) van, Nikkels, P.G.J. (Peter), Lindhout, D. (Dick), Halley, D.J.J. (Dicky), Lips, K. (K.), and Ouweland, A.M.W. (Ans) van den

Published
1999
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184. High rate of mosaicism in tuberous sclerosis complex

Author

Verhoef, S., Bakker, L. (Lida), Tempelaars, A.M.P. (Anita), Hesseling-Janssen, A.L.W. (Arjenne), Mazurczak, T., Jozwiak, S., Fois, A., Bartalini, G. (Gabriella), Zonnenberg, B.A., Essen, J.A. (Anthonie) van, Lindhout, D. (Dick), Halley, D.J.J. (Dicky), Ouweland, A.M.W. (Ans) van den, Verhoef, S., Bakker, L. (Lida), Tempelaars, A.M.P. (Anita), Hesseling-Janssen, A.L.W. (Arjenne), Mazurczak, T., Jozwiak, S., Fois, A., Bartalini, G. (Gabriella), Zonnenberg, B.A., Essen, J.A. (Anthonie) van, Lindhout, D. (Dick), Halley, D.J.J. (Dicky), and Ouweland, A.M.W. (Ans) van den

Published
1999
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185. Mutational spectrum of the TSC1 gene in a cohort of 225 tuberous sclerosis complex patients: no evidence for genotype-phenotype correlation

Author

Verhoef, S., Tempelaars, A.M.P. (Anita), Bakker, L. (Lida), Wang, Q. (Qing), Wessels, M.W. (Marja), Nellist, M.D. (Mark), Bakker, R. (Remco), Lindhout, D. (Dick), Halley, D.J.J. (Dicky), Ouweland, A.M.W. (Ans) van den, Slegtenhorst, M.A. (Marjon) van, Verhoef, S., Tempelaars, A.M.P. (Anita), Bakker, L. (Lida), Wang, Q. (Qing), Wessels, M.W. (Marja), Nellist, M.D. (Mark), Bakker, R. (Remco), Lindhout, D. (Dick), Halley, D.J.J. (Dicky), Ouweland, A.M.W. (Ans) van den, and Slegtenhorst, M.A. (Marjon) van

Abstract

Tuberous sclerosis complex is an inherited tumour suppressor syndrome, caused by a mutation in either the TSC1 or

Published
1999

186. Malignant pancreatic tumour within the spectrum of tuberous sclerosis complex in childhood

Author

Verhoef, S, van Diemen-Steenvoorde, R, Akkersdijk, WL, Bax, NM, Ariyurek, Y (Yavuz), Hermans, Caroline, van Nieuwenhuizen, O, Nikkels, PGJ (Peter), Halley, Dicky, Lips, K, van den Ouweland, Ans, Verhoef, S, van Diemen-Steenvoorde, R, Akkersdijk, WL, Bax, NM, Ariyurek, Y (Yavuz), Hermans, Caroline, van Nieuwenhuizen, O, Nikkels, PGJ (Peter), Halley, Dicky, Lips, K, and van den Ouweland, Ans

Published
1999

187. Duodenal carcinoma in MUTYH-associated polyposis

Author

Nielsen, M, primary, Poley, J W, additional, Verhoef, S, additional, van Puijenbroek, M, additional, Weiss, M M, additional, Burger, G T, additional, Dommering, C J, additional, Vasen, H F A, additional, Kuipers, E J, additional, Wagner, A, additional, Morreau, H, additional, and Hes, F J, additional

Published
2006
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194. Refined localization of TSC1 by combined analysis of 9q34 and 16pl3 data in 14 tuberous sclerosis families

Author

Janssen, L.A.J. (Bart), Sampson, J. (Julian), Est, M. (Mieke) van der, Deelen, W.H. (Wouter), Verhoef, S., Daniels, I. (Ian), Hesseling, P.G.M. (Pjotr), Brook-Carter, P.T. (Phillip), Nellist, M.D. (Mark), Lindhout, D. (Dick), Sandkuijl, L.A. (Lodewijk), Halley, D.J.J. (Dicky), Janssen, L.A.J. (Bart), Sampson, J. (Julian), Est, M. (Mieke) van der, Deelen, W.H. (Wouter), Verhoef, S., Daniels, I. (Ian), Hesseling, P.G.M. (Pjotr), Brook-Carter, P.T. (Phillip), Nellist, M.D. (Mark), Lindhout, D. (Dick), Sandkuijl, L.A. (Lodewijk), and Halley, D.J.J. (Dicky)

Abstract

Tuberous sclerosis (TSC) is a heterogeneous trait. Since 1990, linkage studies have yielded putative TSC loci on chromosomes 9, 11, 12 and 16. Our current analysis, performed on 14 Dutch and British families, reveals only evidence for loci on chromosome 9q34 (TSC1) and chromosome 16p13 (TSC2). We have found no indication for a third locus for TSC, linked or unlinked to either of these chromosomal regions. The majority of our families shows linkage to chromosome 9. We have refined the candidate region for TSC1 to a region of approximately 5 c M between ABL and ABO.

Published
1994
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195. The polycystic kidney disease 1 gene encodes a 14 kb transcript and lies within a duplicated region on chromosome 16

Author

Ward, C.J. (Christopher), Peral, B. (Belén), Hughes, J. (Jim), Thomas, S. (Siep), Gamble, V. (Vicki), MacCarthy, A.B. (Angela), Sloane-Stanley, J. (Jackie), Buckle, P. (Peter), Kearney, P. (Peter), Higgs, D. (Douglas), Ratcliffe, C., Harris, P.C. (Peter), Roelfsema, J.H. (Jeroen), Spruit, L. (Lia), Saris, J.J. (Jasper), Dauwerse, H.G. (Hans), Peters, D. (Dorien), Breuning, M.H. (Martijn), Nellist, M.D. (Mark), Brook-Carter, P.T. (Phillip), Maheshwar, M.M. (Magitha), Cordeiro, I. (Isabel), Santos, H. (Heloisa), Cabral, P. (Pedro), Sampson, J. (Julian), Janssen, L.A.J. (Bart), Hesseling-Janssen, A.L.W. (Arjenne), Ouweland, A.M.W. (Ans) van den, Eussen, H.J.F.M.M. (Bert), Verhoef, S., Lindhout, D. (Dick), Halley, D.J.J. (Dicky), Ward, C.J. (Christopher), Peral, B. (Belén), Hughes, J. (Jim), Thomas, S. (Siep), Gamble, V. (Vicki), MacCarthy, A.B. (Angela), Sloane-Stanley, J. (Jackie), Buckle, P. (Peter), Kearney, P. (Peter), Higgs, D. (Douglas), Ratcliffe, C., Harris, P.C. (Peter), Roelfsema, J.H. (Jeroen), Spruit, L. (Lia), Saris, J.J. (Jasper), Dauwerse, H.G. (Hans), Peters, D. (Dorien), Breuning, M.H. (Martijn), Nellist, M.D. (Mark), Brook-Carter, P.T. (Phillip), Maheshwar, M.M. (Magitha), Cordeiro, I. (Isabel), Santos, H. (Heloisa), Cabral, P. (Pedro), Sampson, J. (Julian), Janssen, L.A.J. (Bart), Hesseling-Janssen, A.L.W. (Arjenne), Ouweland, A.M.W. (Ans) van den, Eussen, H.J.F.M.M. (Bert), Verhoef, S., Lindhout, D. (Dick), and Halley, D.J.J. (Dicky)

Abstract

Autosomal dominant polycystic kidney disease (ADPKD) is a common genetic disorder that frequently results in renal fallure due to progressive cyst development. The major locus, PKD1, maps to 16p13.3. We identified a chromosome translocation associated with ADPKD that disrupts a gene (PBP) encoding a 14 kb transcript in the PKD1 candidate region. Further mutations of the PBP gene were found in PKD1 patients, two deletions (one a de novo event) and a splicing defect, confirming that PBP is the PKD1 gene. This gene is located adjacent to the TSC2 locus in a genomic region that is reiterated more proximally on 16p. The duplicate area encodes three transcripts substantially homologous to the PKD1 transcript. Partial sequence analysis of the PKD1 transcript shows that it encodes a novel protein whose function is at present unknown.

Published
1994
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196. Validating measures of free-living physical activity in overweight and obese subjects using an accelerometer.

Author

Valenti, G, Camps, S G J A, Verhoef, S P M, Bonomi, A G, and Westerterp, K R

Subjects
PHYSICAL activity, CALORIC expenditure, OBESITY, ACCELEROMETERS, BODY weight
Abstract

Background:Free-living physical activity can be assessed with an accelerometer to estimate energy expenditure but its validity in overweight and obese subjects remains unknown.Objective:Here, we validated published prediction equations derived in a lean population with the TracmorD accelerometer (DirectLife, Philips Consumer Lifestyle) in a population of overweight and obese. We also explored possible improvements of new equations specifically developed in overweight and obese subjects.Design:Subjects were 11 men and 25 women (age: 41±7 years; body mass index: 31.0±2.5 kg m−2). Physical activity was monitored under free-living conditions with TracmorD, whereas total energy expenditure was measured simultaneously with doubly-labeled water. Physical activity level (PAL) and activity energy expenditure (AEE) were calculated from total energy expenditure and sleeping metabolic rate.Results:The published prediction equation explained 47% of the variance of the measured PAL (P<0.001). PAL estimates were unbiased (errors (bias±95% confidence interval): −0.02±0.28). Measured and predicted AEE/body weight were highly correlated (r2=58%, P<0.001); however, the prediction model showed a significant bias of 8 kJ kg−1 per day or 17.4% of the average AEE/body weight. The new prediction equation of AEE/body weight developed in the obese group showed no bias.Conclusions:In conclusion, equations derived with the TracmorD allow valid assessment of PAL and AEE/body weight in overweight and obese subjects. There is evidence that estimates of AEE/body weight could be affected by gender. Equations specifically developed in overweight and obese can improve the accuracy of predictions of AEE/body weight. [ABSTRACT FROM AUTHOR]

Published
2014
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197. Malignant pancreatic tumour within the spectrum of tuberous sclerosis complex in childhood

Author

Verhoef, S., primary, van Diemen-Steenvoorde, R., additional, Akkersdijk, W. L., additional, Bax, N. M. A., additional, Ariyurek, Y., additional, Hermans, C. J., additional, van Nieuwenhuizen, O., additional, Nikkels, P. G. J., additional, Lindhout, D., additional, Halley, D. J. J., additional, Lips, K., additional, and van den Ouweland, A. M. W., additional

Published
1999
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198. Identification of a large insertion and two novel point mutations (3671del8 and S1221X) in tuberous sclerosis complex (TSC) patients

Author

Wang, Q., primary, Verhoef, S., additional, Tempelaars, A.M.P., additional, Bakker, P.L.G., additional, Vrtel, R., additional, Hesseling‐Janssen,, A.L.W., additional, Nellist, M., additional, Oranje, A.P., additional, Stroink, H., additional, Lindhout, D., additional, Halley, D.J.J., additional, and van den Ouweland, A.M.W., additional

Published
1998
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200. Identification of a nonsense mutation at the 5' end of the TSC2 gene in a family with a presumptive diagnosis of tuberous sclerosis complex.

Author

Vrtel, R, primary, Verhoef, S, additional, Bouman, K, additional, Maheshwar, M M, additional, Nellist, M, additional, van Essen, A J, additional, Bakker, P L, additional, Hermans, C J, additional, Bink-Boelkens, M T, additional, van Elburg, R M, additional, Hoff, M, additional, Lindhout, D, additional, Sampson, J, additional, Halley, D J, additional, and van den Ouweland, A M, additional

Published
1996
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