Search

Your search keyword '"Vos Y.J."' showing total 21 results
Start Over Author "Vos Y.J."
21 results on '"Vos Y.J."'

3. Diagnostic yield of targeted next generation sequencing in 2002 Dutch cardiomyopathy patients

Author

Alimohamed, M.Z., Johansson, L.F., Posafalvi, A., Boven, L.G., Dijk, K.K. van, Walters, L., Vos, Y.J., Westers, H., Hoedemaekers, Y.M., Sinke, R.J., Sijmons, R.H., Sikkema-Raddatz, B., Jongbloed, J.D., Zwaag, Paul A. van der, Alimohamed, M.Z., Johansson, L.F., Posafalvi, A., Boven, L.G., Dijk, K.K. van, Walters, L., Vos, Y.J., Westers, H., Hoedemaekers, Y.M., Sinke, R.J., Sijmons, R.H., Sikkema-Raddatz, B., Jongbloed, J.D., and Zwaag, Paul A. van der

Abstract

Item does not contain fulltext

Published
2021

4. De novo variants in CAMTA1 cause a syndrome variably associated with spasticity, ataxia, and intellectual disability

Author

Wijnen, I.G.M., Veenstra-Knol, Hermine E., Vansenne, F., Gerkes, E.H., Koning, T. de, Vos, Y.J., Tijssen, Marina A. J., Sival, D., Darin, N., Vanhoutte, E.K., Oosterloo, M., Pennings, M., Warrenburg, B.P.C. van de, Kamsteeg, E.J., Wijnen, I.G.M., Veenstra-Knol, Hermine E., Vansenne, F., Gerkes, E.H., Koning, T. de, Vos, Y.J., Tijssen, Marina A. J., Sival, D., Darin, N., Vanhoutte, E.K., Oosterloo, M., Pennings, M., Warrenburg, B.P.C. van de, and Kamsteeg, E.J.

Abstract

Contains fulltext : 220425.pdf (Publisher’s version ) (Closed access), Previously, intragenic CAMTA1 copy number variants (CNVs) have been shown to cause non-progressive, congenital ataxia with or without intellectual disability (OMIM#614756). However, ataxia, intellectual disability, and dysmorphic features were all incompletely penetrant, even within families. Here, we describe four patients with de novo nonsense, frameshift or missense CAMTA1 variants. All four patients predominantly manifested features of ataxia and/or spasticity. Borderline intellectual disability and dysmorphic features were both present in one patient only, and other neurological and behavioural symptoms were variably present. Neurodevelopmental delay was found to be mild. Our findings indicate that also nonsense, frameshift and missense variants in CAMTA1 can cause a spastic ataxia syndrome as the main phenotype.

Published
2020

5. Description and functional analysis of a novel in frame mutation linked to hereditary non-polyposis colorectal cancer. (Letter to JMG)

Author

Raevaara, T.E., Timoharju, T., Lonnqvist, K.E., Kariola, R., Steinhoff, M., Hofstra, R.M.W., Mangold, E., Vos, Y.J., and Nystrom-Lahti, M.

Subjects
Research, Genetic aspects, Medical genetics -- Research, Endometrial cancer -- Genetic aspects -- Research, Gene mutation -- Research -- Genetic aspects, Colorectal cancer -- Genetic aspects -- Research, DNA mismatch repair -- Research -- Genetic aspects, Gene mutations -- Research -- Genetic aspects
Abstract

Hereditary non-polyposis colorectal cancer (HNPCC) is one of the most common cancer syndromes. The cancer susceptibility is dominantly inherited and associated with germline mutations in mismatch repair (MMR) genes. An [...]

Published
2002

6. PRRT2-related phenotypes in patients with a 16p11.2 deletion

Author

Vlaskamp, D.R.M. (Danique R.M.), Callenbach, P.M.C. (Petra), Rump, P. (Patrick), Giannini, L.A.A. (Lucia A.A.), Brilstra, E.H. (Eva H.), Dijkhuizen, T. (Trijnie), Vos, Y.J. (Yvonne), van der Kevie-Kersemaekers, A.M.F., Knijnenburg, J. (Jeroen), Leeuw, N. (Nicole) de, Thornton, A.S. (Andrew), Ruivenkamp, C.A. (Claudia), Stegmann, A.P.A. (Alexander P.A.), Brouwer, O.F. (Oebele), Ravenswaaij-Arts, C.M.A. (Conny) van, Vlaskamp, D.R.M. (Danique R.M.), Callenbach, P.M.C. (Petra), Rump, P. (Patrick), Giannini, L.A.A. (Lucia A.A.), Brilstra, E.H. (Eva H.), Dijkhuizen, T. (Trijnie), Vos, Y.J. (Yvonne), van der Kevie-Kersemaekers, A.M.F., Knijnenburg, J. (Jeroen), Leeuw, N. (Nicole) de, Thornton, A.S. (Andrew), Ruivenkamp, C.A. (Claudia), Stegmann, A.P.A. (Alexander P.A.), Brouwer, O.F. (Oebele), and Ravenswaaij-Arts, C.M.A. (Conny) van

Abstract

We studied the presence of benign infantile epilepsy (BIE), paroxysmal kinesigenic dyskinesia (PKD), and PKD with infantile convulsions (PKD/IC) in patients with a 16p11.2 deletion including PRRT2 or with a PRRT2 loss-of-function sequence variant. Index patients were recruited from seven Dutch university hospitals. The presence of BIE, PKD and PKD/IC was retrospectively evaluated using questionnaires and medical records. We included 33 patients with a 16p11.2 deletion: three (9%) had BIE, none had PKD or PKD/IC. Twelve patients had a PRRT2 sequence variant: BIE was present in four (p = 0.069), PKD in six (p < 0.001) and PKD/IC in two (p = 0.067). Most patients with a deletion had undergone genetic testing because of developmental problems (87%), whereas all patients with a sequence variant were tested because of a movement disorder (55%) or epilepsy (45%). BIE, PKD and PKD/IC clearly showed incomplete penetrance in patients with 16p11.2 deletions, but were found in all and 95% of patients with a PRRT2 sequence variant in our study and a large literature cohort, respectively. Deletions and sequence variants have the same underlying loss-of-function disease mechanism. Thus, differences in ascertainment have led to overestimating the frequency of BIE, PKD and PKD/IC in patients with a PRRT2 sequence variant. This has important implications for counseling if genome-wide sequencing shows such variants in patients not presenting the PRRT2-related phenotypes.

Published
2018
Full Text
View/download PDF

7. Variable phenotypes in individuals with grin2a sequence variants or deletions

Author

Vlaskamp, D.R.M., Callenbach, P.M.C., Rump, P., Van Pinxteren-Nagler, E., Willemsen, M.H., Gunning, B., de Geus, C., Veenstra, Knol H.E., Lunsing, R.J., Dijkhuizen, T., Vos, Y.J., Brouwer, O.F., Van Ravenswaaij-Arts, C.M.A., and Clinical Cognitive Neuropsychiatry Research Program (CCNP)

Subjects
problem behavior, n methyl dextro aspartic acid receptor 2A, endogenous compound, diagnosis, gene deletion, genotype phenotype correlation, missense mutation, spike, major clinical study, speech disorder, Landau Kleffner syndrome, cognitive defect, motor performance, controlled study, slow wave sleep, human, deletion mutant, ligand gated ion channel, language development
Abstract

Purpose: The GRIN2A gene has been associated with epilepsies ranging from benign focal childhood epilepsies to severe epileptic encephalopathies. The aim of this study was to evaluate genotypes and phenotypes in individuals with GRIN2A deletions or variants. Method: We compared genotypes and phenotypes in six newly identified patients with GRIN2A variants with those of 149 individuals with GRIN2A variants from the literature. Results: Six new patients with epilepsy, developmental and/or behavioral problems and GRIN2A deletions (n = 3), missense (n = 2) or splice-site variants (n = 1) are presented. In 125 (84%) of the 149 individuals with GRIN2A variants previously reported, a specific epilepsy syndrome was diagnosed, most often classified as Benign Epilepsy with Centro-Temporal Spikes (BECTS; n = 44) or Landau-Kleffner syndrome/ Continuous Spike-And-Waves during Slow-wave sleep (LKS/ CSWS; n = 42). Problems of speech and language development (81%), cognition (68%), motor skills (50%) or behavior (42%) were common. Missense variants were seen in 52% of the patients reported earlier, more often in individuals with BECTS (71%) compared to those with LKS/ CSWS (48%). Certain missense variants in or close to the ligand-gated ion channel domain were associated with a severe phenotype, as was also observed in two of our patients with severe epilepsy and cognitive impairment. Conclusion: Individuals with GRIN2A gene variants or deletions have an extremely variable phenotype without a clear genotype-phenotype correlation. Variants in or close to the ligand-gated ion channel can be associated with a severe phenotype.

Published
2016

8. Genotype-phenotype correlations in patients with GRIN2A variants

Author

Vlaskamp, D.R.M., Callenbach, P.M.C., Rump, P., Vos, Y.J., Dijkhuizen, T., Van Ravenswaaij-Arts, C.M.A., Brouwer, O.F., and Clinical Cognitive Neuropsychiatry Research Program (CCNP)

Subjects
focal epilepsy, cognition, language, phenotype, neurology, genotype phenotype correlation, genotype, spike, protein function, European, aphasia, speech and language, society, Landau Kleffner syndrome, motor performance, epilepsy, slow wave sleep, patient, human, benign childhood epilepsy, codon, protein structure, gene, protein expression, brain disease
Abstract

Objective: The GRIN2A gene has been associated with both benign childhood epilepsies and severe epileptic encephalopathies. This study evaluates the genotype-phenotype correlations in patients with GRIN2A variants. Methods: A systematic literature search was performed, identifying all patients reported before May 2014 with GRIN2A variants. Patients were classified in two groups based on their GRIN2A genotype. Group I genotypes had an expected detrimental effect on protein expression: nonsense, frameshift, splice site, or initiation codon sequence variants, translocations with breakpoints within GRIN2A, or deletions comprising GRIN2A. Group II genotypes were expected to result in an altered protein structure or function: missense or in-frame sequence variants. Results: Of 136 patients, 74 were included in group I and 62 in group II. Epilepsy was diagnosed in 86% of patients in both groups, with focal seizures being most common (82%). Benign epilepsy with centrotemporal spikes (BECTS) was significantly more often diagnosed in group II than in group I (51% versus 27%, p=0.03). Continuous spikes and waves during slow-wave sleep (CSWS) and Landau-Kleffner syndrome (LKS) occurred more often in group I than in group II (50% versus 37%), although not statistically significant (p=0.29). Mild to severe developmental problems related to speech and language (80%), cognition (66%), and motor skills (48%), and behavioural problems (61%) were present in both groups. Speech and language problems were significantly more often reported in group I than in group II (90% versus 69%, p=0.02), also in patients with no LKS/CSWS (94% versus 50%, p=0.01). Conclusion: GRIN2A variants are associated with a spectrum of epilepsies, mainly accompanied by language developmental problems. This epilepsy-aphasia syndrome spectrum ranges from relatively mild BECTS to more severe LKS/CSWS. This study shows that GRIN2A genotypes with an expected milder effect on protein function are associated with a relatively more benign phenotype including BECTS without language problems.

Published
2015

9. SNP association study in PMS2-associated Lynch syndrome

Author

Ten Broeke, S.W. (Sanne W.), Elsayed, F.A. (Fadwa A.), Pagan, L. (Lisa), Olderode-Berends, M. (Maran), Garcia, E.B.G., Gille, H.J.P. (Hans), Hest, L.P. (Liselotte) van, Letteboer, T.G.W. (Tom), Kolk, L.E. (Lizet) van der, Mensenkamp, A.R. (Arjen R.), Os, T.A.M. (Theo) van, Spruijt, L. (Liesbeth), Redeker, B. (Bert), Suerink, M. (Manon), Vos, Y.J. (Yvonne), Wagner, A. (Anja), Wijnen, J.T. (Juul), Steyerberg, E.W. (Ewout), Tops, C. (Carli), Wezel, T. (Tom) van, Nielsen, M. (Maartje), Ten Broeke, S.W. (Sanne W.), Elsayed, F.A. (Fadwa A.), Pagan, L. (Lisa), Olderode-Berends, M. (Maran), Garcia, E.B.G., Gille, H.J.P. (Hans), Hest, L.P. (Liselotte) van, Letteboer, T.G.W. (Tom), Kolk, L.E. (Lizet) van der, Mensenkamp, A.R. (Arjen R.), Os, T.A.M. (Theo) van, Spruijt, L. (Liesbeth), Redeker, B. (Bert), Suerink, M. (Manon), Vos, Y.J. (Yvonne), Wagner, A. (Anja), Wijnen, J.T. (Juul), Steyerberg, E.W. (Ewout), Tops, C. (Carli), Wezel, T. (Tom) van, and Nielsen, M. (Maartje)

Abstract

Lynch syndrome (LS) patients are at high risk of developing colorectal cancer (CRC). Phenotypic variability might in part be explained by common susceptibility loci identified in Genome Wide Association Studies (GWAS). Previous studies focused mostly on MLH1, MSH2 and MSH6 carriers, with conflicting results. We aimed to determine the role of GWAS SNPs in PMS2 mutation carriers. A cohort study was performed in 507 PMS2 carriers (124 CRC cases), genotyped for 24 GWAS SNPs, including SNPs at 11q23.1 and 8q23.3. Hazard ratios (HRs) were calculated using a weighted Cox regression analysis to correct for ascertainment bias. Discrimination was assessed with a concordance statistic in a bootstrap cross-validation procedure. Individual SNPs only had non-significant associations with CRC occurrence with HRs lower than 2, although male carriers of allele A at rs1321311 (6p21.31) may have increased risk of CRC (HR = 2.1, 95% CI 1.2–3.0). A polygenic risk score (PRS) based on 24 HRs had an HR of 2.6 (95% CI 1.5–4.6) for the highest compared to the lowest quartile, but had no discriminative ability (c statistic 0.52). Previously suggested SNPs do not modify CRC risk in PMS2 carriers. Future large studies are needed for improved risk stratification among Lynch syndrome patients.

Published
2017
Full Text
View/download PDF

10. The effect of genotypes and parent of origin on cancer risk and age of cancer development in PMS2 mutation carriers

Author

Suerink, M., Klift, H.M. van der, Broeke, S.W. ten, Dekkers, O.M., Bernstein, I., Capella Munar, G., Garcia, E., Hoogerbrugge, N., Letteboer, T.G., Menko, F.H., Lindblom, A., Mensenkamp, A., Moller, P., Os, T.A. van, Rahner, N., Redeker, B.J., Olderode-Berends, M.J., Spruijt, L., Vos, Y.J., Wagner, A., Morreau, H., Hes, F.J., Vasen, H.F.A., Tops, C.M., Wijnen, J.T., Nielsen, M., Suerink, M., Klift, H.M. van der, Broeke, S.W. ten, Dekkers, O.M., Bernstein, I., Capella Munar, G., Garcia, E., Hoogerbrugge, N., Letteboer, T.G., Menko, F.H., Lindblom, A., Mensenkamp, A., Moller, P., Os, T.A. van, Rahner, N., Redeker, B.J., Olderode-Berends, M.J., Spruijt, L., Vos, Y.J., Wagner, A., Morreau, H., Hes, F.J., Vasen, H.F.A., Tops, C.M., Wijnen, J.T., and Nielsen, M.

Abstract

Item does not contain fulltext, PURPOSE: Lynch syndrome (LS), a heritable disorder with an increased risk of primarily colorectal cancer (CRC) and endometrial cancer (EC), can be caused by mutations in the PMS2 gene. We wished to establish whether genotype and/or parent-of-origin effects (POE) explain (part of) the reported variability in severity of the phenotype. METHODS: European PMS2 mutation carriers (n = 381) were grouped and compared based on RNA expression and whether the mutation was inherited paternally or maternally. RESULTS: Mutation carriers with loss of RNA expression (group 1) had a significantly lower age at CRC diagnosis (51.1 years vs. 60.0 years, P = 0.035) and a lower age at EC diagnosis (55.8 years vs. 61.0 years, P = 0.2, nonsignificant) compared with group 2 (retention of RNA expression). Furthermore, group 1 showed slightly higher, but nonsignificant, hazard ratios (HRs) for both CRC (HR: 1.31, P = 0.38) and EC (HR: 1.22, P = 0.72). No evidence for a significant parent-of-origin effect was found for either CRC or EC. CONCLUSIONS: PMS2 mutation carriers with retention of RNA expression developed CRC 9 years later than those with loss of RNA expression. If confirmed, this finding would justify a delay in surveillance for these cases. Cancer risk was not influenced by a parent-of-origin effect.Genet Med 18 4, 405-409.

Published
2016

11. Comprehensive Mutation Analysis of PMS2 in a Large Cohort of Probands Suspected of Lynch Syndrome or Constitutional Mismatch Repair Deficiency Syndrome

Author

Klift, H.M. van der, Mensenkamp, A.R., Drost, M., Bik, E.C., Vos, Y.J., Gille, H.J., Redeker, B.E., Tiersma, Y., Zonneveld, J.B., Garcia, E.G., Letteboer, T.G., Olderode-Berends, M.J., Hest, L.P. van, Os, T.A. van, Verhoef, S., Wagner, A., Asperen, C.J. van, Broeke, S.W. ten, Hes, F.J., Wind, N. de, Nielsen, M., Devilee, P., Ligtenberg, M.J.L., Wijnen, J.T., Tops, C.M., Klift, H.M. van der, Mensenkamp, A.R., Drost, M., Bik, E.C., Vos, Y.J., Gille, H.J., Redeker, B.E., Tiersma, Y., Zonneveld, J.B., Garcia, E.G., Letteboer, T.G., Olderode-Berends, M.J., Hest, L.P. van, Os, T.A. van, Verhoef, S., Wagner, A., Asperen, C.J. van, Broeke, S.W. ten, Hes, F.J., Wind, N. de, Nielsen, M., Devilee, P., Ligtenberg, M.J.L., Wijnen, J.T., and Tops, C.M.

Abstract

Item does not contain fulltext, Monoallelic PMS2 germline mutations cause 5%-15% of Lynch syndrome, a midlife cancer predisposition, whereas biallelic PMS2 mutations cause approximately 60% of constitutional mismatch repair deficiency (CMMRD), a rare childhood cancer syndrome. Recently improved DNA- and RNA-based strategies are applied to overcome problematic PMS2 mutation analysis due to the presence of pseudogenes and frequent gene conversion events. Here, we determined PMS2 mutation detection yield and mutation spectrum in a nationwide cohort of 396 probands. Furthermore, we studied concordance between tumor IHC/MSI (immunohistochemistry/microsatellite instability) profile and mutation carrier state. Overall, we found 52 different pathogenic PMS2 variants explaining 121 Lynch syndrome and nine CMMRD patients. In vitro mismatch repair assays suggested pathogenicity for three missense variants. Ninety-one PMS2 mutation carriers (70%) showed isolated loss of PMS2 in their tumors, for 31 (24%) no or inconclusive IHC was available, and eight carriers (6%) showed discordant IHC (presence of PMS2 or loss of both MLH1 and PMS2). Ten cases with isolated PMS2 loss (10%; 10/97) harbored MLH1 mutations. We confirmed that recently improved mutation analysis provides a high yield of PMS2 mutations in patients with isolated loss of PMS2 expression. Application of universal tumor prescreening methods will however miss some PMS2 germline mutation carriers.

Published
2016

13. Lynch syndrome caused by germline PMS2 mutations: delineating the cancer risk

Author

Broeke, S.W. ten, Brohet, R.M., Tops, C.M., Klift, H.M. van der, Velthuizen, M.E., Bernstein, I., Capella Munar, G., Garcia, E., Hoogerbrugge, N., Letteboer, T.G., Menko, F.H., Lindblom, A., Mensenkamp, A.R., Moller, P., Os, T.A. van, Rahner, N., Redeker, B.J., Sijmons, R.H., Spruijt, L., Suerink, M., Vos, Y.J., Wagner, A., Hes, F.J., Vasen, H.F.A., Nielsen, M., Wijnen, J.T., Broeke, S.W. ten, Brohet, R.M., Tops, C.M., Klift, H.M. van der, Velthuizen, M.E., Bernstein, I., Capella Munar, G., Garcia, E., Hoogerbrugge, N., Letteboer, T.G., Menko, F.H., Lindblom, A., Mensenkamp, A.R., Moller, P., Os, T.A. van, Rahner, N., Redeker, B.J., Sijmons, R.H., Spruijt, L., Suerink, M., Vos, Y.J., Wagner, A., Hes, F.J., Vasen, H.F.A., Nielsen, M., and Wijnen, J.T.

Abstract

Item does not contain fulltext, PURPOSE: The clinical consequences of PMS2 germline mutations are poorly understood compared with other Lynch-associated mismatch repair gene (MMR) mutations. The aim of this European cohort study was to define the cancer risk faced by PMS2 mutation carriers. METHODS: Data were collected from 98 PMS2 families ascertained from family cancer clinics that included a total of 2,548 family members and 377 proven mutation carriers. To adjust for potential ascertainment bias, a modified segregation analysis model was used to calculate colorectal cancer (CRC) and endometrial cancer (EC) risks. Standardized incidence ratios (SIRs) were calculated to estimate risks for other Lynch syndrome-associated cancers. RESULTS: The cumulative risk (CR) of CRC for male mutation carriers by age 70 years was 19%. The CR among female carriers was 11% for CRC and 12% for EC. The mean age of CRC development was 52 years, and there was a significant difference in mean age of CRC between the probands (mean, 47 years; range, 26 to 68 years) and other family members with a PMS2 mutation (mean, 58 years; range, 31 to 86 years; P < .001). Significant SIRs were observed for cancers of the small bowel, ovaries, breast, and renal pelvis. CONCLUSION: CRC and EC risks were found to be markedly lower than those previously reported for the other MMR. However, these risks embody the isolated risk of carrying a PMS2 mutation, and it should be noted that we observed a substantial variation in cancer phenotype within and between families, suggesting the influence of genetic modifiers and lifestyle factors on cancer risks.

Published
2015

15. Contribution of bi-allelic germline MUTYH mutations to early-onset and familial colorectal cancer and to low number of adenomatous polyps: case-series and literature review

Author

Knopperts, A.P., Nielsen, M., Niessen, R.C., Tops, C.M., Jorritsma, B., Varkevisser, J., Wijnen, J., Siezen, C.L., Heine-Broring, R.C., Kranen, H.J. van, Vos, Y.J., Westers, H., Kampman, E., Sijmons, R.H., Hes, F.J., Knopperts, A.P., Nielsen, M., Niessen, R.C., Tops, C.M., Jorritsma, B., Varkevisser, J., Wijnen, J., Siezen, C.L., Heine-Broring, R.C., Kranen, H.J. van, Vos, Y.J., Westers, H., Kampman, E., Sijmons, R.H., and Hes, F.J.

Abstract

Item does not contain fulltext, In the absence of a polyposis phenotype, colorectal cancer (CRC) patients referred for genetic testing because of early-onset disease and/or a positive family history, typically undergo testing for molecular signs of Lynch syndrome in their tumors. In the absence of these signs, DNA testing for germline mutations associated with other known tumor syndromes is usually not performed. However, a few studies in large series of CRC patients suggest that in a small percentage of CRC cases, bi-allelic MUTYH germline mutations can be found in the absence of the MUTYH-associated polyposis phenotype. This has not been studied in the Dutch population. Therefore, we analyzed the MUTYH gene for mutations in 89 patients with microsatellite-low or stable CRC cancer diagnosed before the age of 40 years or otherwise meeting the Bethesda criteria, all of them without a polyposis phenotype. In addition, we studied a series of 693 non-CRC patients with 1-13 adenomatous colorectal polyps for the MUTYH hotspot mutations Y179C, G396D and P405L. No bi-allelic MUTYH mutations were observed. Our data suggest that the contribution of bi-allelic MUTYH mutations to the development of CRC in Dutch non-polyposis patients that meet clinical genetic referral criteria, and to the development of low number of colorectal adenomas in non-CRC patients, is likely to be low.

Published
2013

16. Genotype-phenotype correlation in L1 syndrome: a guide for genetic counselling and mutation analysis.

Author

Vos, Y.J., Walle, H.E. de, Bos, K.K., Stegeman, J.A., Berge, A.M. ten, Bruining, M., Maarle, M.C. van, Elting, M.W., Hollander, N.S. den, Hamel, B.C.J., Fortuna, A.M., Sunde, L., Stolte-Dijkstra, I., Schrander-Stumpel, C.T.R.M., Hofstra, R.M., Vos, Y.J., Walle, H.E. de, Bos, K.K., Stegeman, J.A., Berge, A.M. ten, Bruining, M., Maarle, M.C. van, Elting, M.W., Hollander, N.S. den, Hamel, B.C.J., Fortuna, A.M., Sunde, L., Stolte-Dijkstra, I., Schrander-Stumpel, C.T.R.M., and Hofstra, R.M.

Abstract

Contains fulltext : 88493.pdf (publisher's version ) (Closed access)

Published
2010

17. Autosomal dominant inheritance of cardiac valves anomalies in two families: extended spectrum of left-ventricular outflow tract obstruction.

Author

Wessels, M.W., Laar, I.M. van de, Roos-Hesselink, J.W., Strikwerda, S., Majoor-Krakauer, D.F., Vries, L.B.A. de, Kerstjens-Frederikse, W.S., Vos, Y.J., Graaf, B.M. de, Bertoli-Avella, A.M., Willems, P.J., Wessels, M.W., Laar, I.M. van de, Roos-Hesselink, J.W., Strikwerda, S., Majoor-Krakauer, D.F., Vries, L.B.A. de, Kerstjens-Frederikse, W.S., Vos, Y.J., Graaf, B.M. de, Bertoli-Avella, A.M., and Willems, P.J.

Abstract

Item does not contain fulltext, Only a limited number of families with clear monogenic inheritance of nonsyndromic forms of congenital valve defects have been described. We describe two multiplex pedigrees with a similar nonsyndromic form of heart valve anomalies that segregate as an autosomal dominant condition. The first family is a three-generation pedigree with 10 family members affected with congenital defects of the cardiac valves, including six patients with aortic stenosis and/or aortic regurgitation. Pulmonary and/or tricuspid valve abnormalities were present in three patients, and ventricular septal defect (VSD) was present in two patients. The second family consists of 11 patients in three generations with aortic valve stenosis in seven patients, defects of the pulmonary valves in two patients, and atrial septal defect (ASD) in two patients. Incomplete penetrance was observed in both families. Although left-ventricular outflow tract obstruction was present in most family members, the co-occurrence with pulmonary valve abnormalities and septal defects in both families is uncommon. These families provide evidence that left-sided obstructive defects and thoracic aortic aneurysm may be accompanied by right-sided defects, and even septal defects. These families might be instrumental in identifying genes involved in cardiac valve morphogenesis and malformation.

Published
2009

18. 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

21. An alternative approach to establishing unbiased colorectal cancer risk estimation in Lynch syndrome

Author

Inbal Kedar, Christi J. van Asperen, Jeanine J. Houwing-Duistermaat, Laurence Brugières, Sergey Nikolaev, Michael Farrell, Anja Wagner, D. Gareth Evans, Lone Sunde, Yael Goldberg, Mar Rodríguez-Girondo, Jessica I. Hoell, Katharina Wimmer, Karl Heinimann, Stefan Aretz, Maartje Nielsen, Heleen M. van der Klift, Maria Grazia Tibiletti, Tim Ripperger, Leigha Senter, Sanne W. ten Broeke, Wenche Sjursen, Encarna B. Gomez-Garcia, Stefanie Y. Zimmermann, Daniel Rueda, Marjolijn C.J. Jongmans, Noémie Lavoine, Ingrid Winship, Christina Therkildsen, Gabriel Capellá Munar, Chrystelle Colas, Alison H. Trainer, Kory Jasperson, Maurizio Genuardi, Theo A. M. van Os, Yvonne J. Vos, Mitul Modi, Hans F. A. Vasen, Manon Suerink, Suerink M., Rodriguez-Girondo M., van der Klift H.M., Colas C., Brugieres L., Lavoine N., Jongmans M., Munar G.C., Evans D.G., Farrell M.P., Genuardi M., Goldberg Y., Gomez-Garcia E., Heinimann K., Hoell J.I., Aretz S., Jasperson K.W., Kedar I., Modi M.B., Nikolaev S., van Os T.A.M., Ripperger T., Rueda D., Senter L., Sjursen W., Sunde L., Therkildsen C., Tibiletti M.G., Trainer A.H., Vos Y.J., Wagner A., Winship I., Wimmer K., Zimmermann S.Y., Vasen H.F., van Asperen C.J., Houwing-Duistermaat J.J., ten Broeke S.W., Nielsen M., Human Genetics, Clinical Genetics, Klinische Genetica, MUMC+: DA KG Polikliniek (9), and RS: GROW - R4 - Reproductive and Perinatal Medicine

Subjects
Male, Oncology, MICROSATELLITE INSTABILITY, Settore MED/03 - GENETICA MEDICA, PHENOTYPE, FAMILIES, Cohort Studies, Risk Factors, PMS2, CRITERIA, Genetics(clinical), Genetics (clinical), Mismatch Repair Endonuclease PMS2, Incidence, Incidence (epidemiology), DNA MISMATCH REPAIR, GERMLINE MUTATIONS, Middle Aged, Lynch syndrome, DNA-Binding Proteins, Cohort, colon cancer risk, Female, Colorectal Neoplasms, bMMRD, Cohort study, Adult, medicine.medical_specialty, HNPCC, colorectal cancer, FREQUENCY, Risk Assessment, BREAST, AGE, SDG 3 - Good Health and Well-being, Internal medicine, SURVEILLANCE, medicine, Humans, Genetic Predisposition to Disease, Germ-Line Mutation, Aged, business.industry, Microsatellite instability, MSH6, medicine.disease, Colorectal Neoplasms, Hereditary Nonpolyposis, Confidence interval, Mutation, business
Abstract

Purpose: Biallelic pathogenic variants in the mismatch repair (MMR) genes cause a recessive childhood cancer predisposition syndrome known as constitutional mismatch repair deficiency (CMMRD). Family members with a heterozygous MMR variant have Lynch syndrome. We aimed at estimating cancer risk in these heterozygous carriers as a novel approach to avoid complicated statistical methods to correct for ascertainment bias.Methods: Cumulative colorectal cancer incidence was estimated in a cohort of PMS2- and MSH6-associated families, ascertained by the CMMRD phenotype of the index, by using mutation probabilities based on kinship coefficients as analytical weights in a proportional hazard regression on the cause-specific hazards. Confidence intervals (CIs) were obtained by bootstrapping at the family level.Results: The estimated cumulative colorectal cancer risk at age 70 years for heterozygous PMS2 variant carriers was 8.7% (95% CI 4.3-12.7%) for both sexes combined, and 9.9% (95% CI 4.9-15.3%) for men and 5.9% (95% CI 1.6-11.1%) for women separately. For heterozygous MSH6 variant carriers these estimates are 11.8% (95% CI 4.5-22.7%) for both sexes combined, 10.0% (95% CI 1.83-24.5%) for men and 11.7% (95% CI 2.10-26.5%) for women.Conclusion: Our findings are consistent with previous reports that used more complex statistical methods to correct for ascertainment bias. These results underline the need for MMR gene-specific surveillance protocols for Lynch syndrome.

Published
2019
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results