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287 results on '"Spruijt, L."'

1. Pathogenic neurofibromatosis type 1 (NF1) RNA splicing resolved by targeted RNAseq

Author

Koster, R., Brandão, R. D., Tserpelis, D., van Roozendaal, C. E. P., van Oosterhoud, C. N., Claes, K. B. M., Paulussen, A. D. C., Sinnema, M., Vreeburg, M., van der Schoot, V., Stumpel, C. T. R. M., Broen, M. P. G., Spruijt, L., Jongmans, M. C. J., Lesnik Oberstein, S. A. J., Plomp, A. S., Misra-Isrie, M., Duijkers, F. A., Louwers, M. J., Szklarczyk, R., Derks, K. W. J., Brunner, H. G., van den Wijngaard, A., van Geel, M., and Blok, M. J.

Published
2021
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2. 819 International cohort of 19 patients with CARD14-associated papulosquamous eruption: The quest for a genotype-phenotype correlation and successful therapeutic intervention

Author

Rossel, V., primary, Baniel, A., additional, Wertheim-Tysarowska, K., additional, Seyger, M., additional, Spruijt, L., additional, Bekkenk, M., additional, Vreeburg, M., additional, Sprecher, E., additional, Steijlen, P., additional, van Geel, M., additional, and Gostynski, A., additional

Published
2023
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3. Identification of new TRIP12 variants and detailed clinical evaluation of individuals with non-syndromic intellectual disability with or without autism

Author

Bramswig, Nuria C., Lüdecke, H.-J., Pettersson, M., Albrecht, B., Bernier, R. A., Cremer, K., Eichler, E. E., Falkenstein, D., Gerdts, J., Jansen, S., Kuechler, A., Kvarnung, M., Lindstrand, A., Nilsson, D., Nordgren, A., Pfundt, R., Spruijt, L., Surowy, H. M., de Vries, B. B. A., Wieland, T., Engels, H., Strom, T. M., Kleefstra, T., and Wieczorek, D.

Published
2017
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4. BLU-RAY DISC

Author

van Haaren, J.A.M.M., Kuijper, M., Martynov, Yourii V., Hendriks, Benno H.W., Zijp, Ferry, Aarts, Jan, Baartman, Jan-Peter, van Rosmalen, Gerard, Schleipen, Jean J.H.B., van Houten, Henk, Narahara, Tatsuya, Kobayashi, Shoei, Hattori, Masayuki, Shimpuku, Yoshihide, van den Enden, Gijs J., Kahlman, Joost A.H.M., van Dijk, Marten, van Woudenberg, Roel, Ubbens, I., Spruijt, L., Meulen, J.M. ter, Schep, K., Furumiya, Shigeru, Stek, Bert, Ishibashi, Hiromichi, Yamagami, Tamotsu, Schep, Kees, Neijzen, Jaap H.M., Meinders, Erwin R., van Santen, Helmar, Toolenaar, Frank, editor, Peek, Hans, Bergmans, Jan, Haaren, Jos van, and Stan, Sorin

Published
2009
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5. Neurofibromas in LZTR1 schwannomatosis

Author

Groen, J.L., Moghadasi, S., Spruijt, L., Korpershoek, E., Ierland, Y. van, Wezel, J.T. van, Duinen, S. van, Malessy, M.J., Oberstein, S.A., Groen, J.L., Moghadasi, S., Spruijt, L., Korpershoek, E., Ierland, Y. van, Wezel, J.T. van, Duinen, S. van, Malessy, M.J., and Oberstein, S.A.

Abstract

Item does not contain fulltext

Published
2022

6. Pathogenic neurofibromatosis type 1 (NF1) RNA splicing resolved by targeted RNAseq

Author

Koster, R.W., Brandao, R.D., Tserpelis, D.C.J., Roozendaal, C.E.P. van, Oosterhoud, C.N. van, Claes, K.B.M., Spruijt, L., Brunner, H.G., Geel, M. van, Blok, M.J., Koster, R.W., Brandao, R.D., Tserpelis, D.C.J., Roozendaal, C.E.P. van, Oosterhoud, C.N. van, Claes, K.B.M., Spruijt, L., Brunner, H.G., Geel, M. van, and Blok, M.J.

Abstract

Contains fulltext : 240782.pdf (Publisher’s version ) (Open Access)

Published
2021

7. Pathogenic neurofibromatosis type 1 (NF1) RNA splicing resolved by targeted RNAseq

Author

CMM Groep Cuppen, MS Urologische Oncologie, Cancer, Genetica, Genetica Klinische Genetica, Child Health, Psychosociale zorg patientenzorg, Other research (not in main researchprogram), Koster, R., Brandão, R. D., Tserpelis, D., van Roozendaal, C. E.P., van Oosterhoud, C. N., Claes, K. B.M., Paulussen, A. D.C., Sinnema, M., Vreeburg, M., van der Schoot, V., Stumpel, C. T.R.M., Broen, M. P.G., Spruijt, L., Jongmans, M. C.J., Lesnik Oberstein, S. A.J., Plomp, A. S., Misra-Isrie, M., Duijkers, F. A., Louwers, M. J., Szklarczyk, R., Derks, K. W.J., Brunner, H. G., van den Wijngaard, A., van Geel, M., Blok, M. J., CMM Groep Cuppen, MS Urologische Oncologie, Cancer, Genetica, Genetica Klinische Genetica, Child Health, Psychosociale zorg patientenzorg, Other research (not in main researchprogram), Koster, R., Brandão, R. D., Tserpelis, D., van Roozendaal, C. E.P., van Oosterhoud, C. N., Claes, K. B.M., Paulussen, A. D.C., Sinnema, M., Vreeburg, M., van der Schoot, V., Stumpel, C. T.R.M., Broen, M. P.G., Spruijt, L., Jongmans, M. C.J., Lesnik Oberstein, S. A.J., Plomp, A. S., Misra-Isrie, M., Duijkers, F. A., Louwers, M. J., Szklarczyk, R., Derks, K. W.J., Brunner, H. G., van den Wijngaard, A., van Geel, M., and Blok, M. J.

Published
2021

9. Pathogenic Neurofibromatosis type 1 (NF1) RNA splicing resolved by targeted RNAseq

Author

Koster, R., primary, Brandão, R.D., additional, Tserpelis, D., additional, van Roozendaal, C.E.P., additional, van Oosterhoud, C.N., additional, Claes, K.B.M., additional, Paulussen, A.D.C., additional, Sinnema, M., additional, Vreeburg, M., additional, van der Schoot, V., additional, Stumpel, C.T.R.M., additional, Broen, M.P.G., additional, Spruijt, L., additional, Jongmans, M.C.J., additional, Oberstein, S.A.J. Lesnik, additional, Plomp, A.S., additional, Misra-Isrie, M., additional, Duijkers, F.A., additional, Louwers, M.J., additional, Szklarczyk, R., additional, Derks, K.W.J., additional, Brunner, H.G., additional, van den Wijngaard, A., additional, van Geel, M., additional, and Blok, M.J., additional

Published
2021
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10. TINF2 is a haploinsufficient tumor suppressor that limits telomere length

Author

Schmutz, Isabelle, Mensenkamp, A.R., Takai, Kaori K., Haadsma, M.L., Spruijt, L., Voer, R.M. de, Jongmans, Marjolijn C.J., Lange, Titia de, Schmutz, Isabelle, Mensenkamp, A.R., Takai, Kaori K., Haadsma, M.L., Spruijt, L., Voer, R.M. de, Jongmans, Marjolijn C.J., and Lange, Titia de

Abstract

Contains fulltext : 228576.pdf (publisher's version ) (Open Access)

Published
2020

11. Evaluation of yield and experiences of age-related molecular investigation for heritable and nonheritable causes of mismatch repair deficient colorectal cancer to identify Lynch syndrome

Author

Vos, J.R., Fakkert, I.E., Spruijt, L., Willems, R.W., Langenveld, S., Mensenkamp, A.R., Leter, E.M., Nagtegaal, I.D., Ligtenberg, M.J.L., Hoogerbrugge, N., Vos, J.R., Fakkert, I.E., Spruijt, L., Willems, R.W., Langenveld, S., Mensenkamp, A.R., Leter, E.M., Nagtegaal, I.D., Ligtenberg, M.J.L., and Hoogerbrugge, N.

Abstract

Contains fulltext : 225442pub.pdf (publisher's version ) (Open Access), Universal mismatch repair deficiency (dMMR) testing of colorectal cancer (CRC) is promoted as routine diagnostics to prescreen for Lynch syndrome. We evaluated the yield and experience of age-related molecular investigation for heritable and nonheritable causes of dMMR in CRC below age 70 to identify Lynch Syndrome. In a prospective cohort of 3602 newly diagnosed CRCs below age 70 from 19 hospitals, dMMR, MLH1 promoter hypermethylation, germline MMR gene and somatic MMR gene testing was assessed in daily practice. Yield was evaluated using data from the Dutch Pathology Registry (PALGA) and two regional genetic centers. Experiences of clinicians were evaluated through questionnaires. Participating clinicians were overwhelmingly positive about the clinical workflow. Pathologists routinely applied dMMR-testing in 84% CRCs and determined 10% was dMMR, largely due to somatic MLH1 hypermethylation (66%). Of those, 69% with dMMR CRC below age 70 without hypermethylation were referred for genetic testing, of which 55% was due to Lynch syndrome (hereditary) and 43% to somatic biallelic pathogenic MMR (nonhereditary). The prevalence of Lynch syndrome was 18% in CRC < 40, 1.7% in CRC age 40-64 and 0.7% in CRC age 65-69. Age 65-69 represents most cases with dMMR, in which dMMR due to somatic causes (13%) is 20 times more prevalent than Lynch syndrome. In conclusion, up to age 65 routine diagnostics of (non-)heritable causes of dMMR CRCs effectively identifies Lynch syndrome and reduces Lynch-like diagnoses. Above age 64, the effort to detect one Lynch syndrome patient in dMMR CRC is high and germline testing rarely needed.

Published
2020

17. The Apparent Genetic Anticipation in PMS2-Associated Lynch Syndrome Families Is Explained by Birth-cohort Effect

Author

Broeke, S.W. ten, Rodriguez-Girondo, M., Suerink, M., Aretz, S., Bernstein, I., Capella, G., Engel, C., Gomez-Garcia, E.B., Hest, L.P. van, Doeberitz, M. von Knebel, Lagerstedt-Robinson, K., Letteboer, T.G., Moller, P., Os, T.A. van, Pineda, M., Rahner, N., Olderode-Berends, M.J., Salome, J. von, Schackert, H.K., Spruijt, L., Steinke-Lange, V., Wagner, A., Tops, C.M., Nielsen, M., Broeke, S.W. ten, Rodriguez-Girondo, M., Suerink, M., Aretz, S., Bernstein, I., Capella, G., Engel, C., Gomez-Garcia, E.B., Hest, L.P. van, Doeberitz, M. von Knebel, Lagerstedt-Robinson, K., Letteboer, T.G., Moller, P., Os, T.A. van, Pineda, M., Rahner, N., Olderode-Berends, M.J., Salome, J. von, Schackert, H.K., Spruijt, L., Steinke-Lange, V., Wagner, A., Tops, C.M., and Nielsen, M.

Abstract

Contains fulltext : 206727.pdf (publisher's version ) (Closed access), BACKGROUND: PMS2-associated Lynch syndrome is characterized by a relatively low colorectal cancer penetrance compared with other Lynch syndromes. However, age at colorectal cancer diagnosis varies widely, and a strong genetic anticipation effect has been suggested for PMS2 families. In this study, we examined proposed genetic anticipation in a sample of 152 European PMS2 families. METHODS: The 152 families (637 family members) that were eligible for analysis were mainly clinically ascertained via clinical genetics centers. We used weighted Cox-type random effects model, adjusted by birth cohort and sex, to estimate the generational effect on the age of onset of colorectal cancer. Probands and young birth cohorts were excluded from the analyses. Weights represented mutation probabilities based on kinship coefficients, thus avoiding testing bias. RESULTS: Family data across three generations, including 123 colorectal cancers, were analyzed. When compared with the first generation, the crude HR for anticipation was 2.242 [95% confidence interval (CI), 1.162-4.328] for the second generation and 2.644 (95% CI, 1.082-6.464) for the third generation. However, after correction for birth cohort and sex, the effect vanished [HR = 1.302 (95% CI, 0.648-2.619) and HR = 1.074 (95% CI, 0.406-2.842) for second and third generations, respectively]. CONCLUSIONS: Our study did not confirm previous reports of genetic anticipation in PMS2-associated Lynch syndrome. Birth-cohort effect seems the most likely explanation for observed younger colorectal cancer diagnosis in subsequent generations, particularly because there is currently no commonly accepted biological mechanism that could explain genetic anticipation in Lynch syndrome. IMPACT: This new model for studying genetic anticipation provides a standard for rigorous analysis of families with dominantly inherited cancer predisposition.

Published
2019

18. Cancer Risks for PMS2-Associated Lynch Syndrome (vol 29, pg 2961, 2018)

Author

ten Broeke, SW, van der Klift, HM, Tops, CMJ, Aretz, S, Bernstein, I, Buchanan, DD, de la Chapelle, A, Capella, G, Clendenning, M, Engel, C, Gallinger, S, Garcia, EG, Figueiredo, JC, Haile, R, Hampel, HL, van Hest, L, Hopper, JL, Hoogerbrugge, N, Doeberitz, MVK, Le Marchand, L, Letteboer, TGW, Jenkins, MA, Lindblom, A, Lindor, NM, Mensenkamp, AR, Moller, P, Newcomb, PA, van Os, TAM, Pearlman, R, Pineda, M, Rahner, N, Redeker, EJW, Olderode-Berends, MJW, Rosty, C, Schackert, HK, Scott, R, Senter, L, Spruijt, L, Steinke-Lange, V, Suerink, M, Thibodeau, S, Vos, YJ, Wagner, A, Winship, I, Hes, FJ, Vasen, HFA, Wijnen, JT, Nielsen, M, Win, AK, ten Broeke, SW, van der Klift, HM, Tops, CMJ, Aretz, S, Bernstein, I, Buchanan, DD, de la Chapelle, A, Capella, G, Clendenning, M, Engel, C, Gallinger, S, Garcia, EG, Figueiredo, JC, Haile, R, Hampel, HL, van Hest, L, Hopper, JL, Hoogerbrugge, N, Doeberitz, MVK, Le Marchand, L, Letteboer, TGW, Jenkins, MA, Lindblom, A, Lindor, NM, Mensenkamp, AR, Moller, P, Newcomb, PA, van Os, TAM, Pearlman, R, Pineda, M, Rahner, N, Redeker, EJW, Olderode-Berends, MJW, Rosty, C, Schackert, HK, Scott, R, Senter, L, Spruijt, L, Steinke-Lange, V, Suerink, M, Thibodeau, S, Vos, YJ, Wagner, A, Winship, I, Hes, FJ, Vasen, HFA, Wijnen, JT, Nielsen, M, and Win, AK

Abstract

This corrects the article "Cancer Risks for PMS2-Associated Lynch Syndrome" in volume 36 on page 2961.

Published
2019

20. Molecular Background of Colorectal Tumors From Patients With Lynch Syndrome Associated With Germline Variants in PMS2

Author

Broeke, Sanne W. ten, Bavel, Tom C. van, Jansen, A.M.L, Gomez-Garcia, Encarnca, Hes, Frederik J., Hest, Liselot P. van, Spruijt, L., Wezel, Tom van, Nielsen, Maartje, Broeke, Sanne W. ten, Bavel, Tom C. van, Jansen, A.M.L, Gomez-Garcia, Encarnca, Hes, Frederik J., Hest, Liselot P. van, Spruijt, L., Wezel, Tom van, and Nielsen, Maartje

Abstract

Item does not contain fulltext

Published
2018

21. Clinical Aspects of SDHA-Related Pheochromocytoma and Paraganglioma: A Nationwide Study

Author

Tuin, Karin van der, Mensenkamp, A.R., Tops, Carli M.J., Corssmit, Eleonora P.M., Dinjens, Winand N., Horst-Schrivers, Anouk N. van de, Kunst, H.P.M., Kusters, B., Spruijt, L., Hes, Frederik J., Timmers, H.J.L.M., Tuin, Karin van der, Mensenkamp, A.R., Tops, Carli M.J., Corssmit, Eleonora P.M., Dinjens, Winand N., Horst-Schrivers, Anouk N. van de, Kunst, H.P.M., Kusters, B., Spruijt, L., Hes, Frederik J., and Timmers, H.J.L.M.

Abstract

Item does not contain fulltext

Published
2018

22. Cancer Risks for PMS2-Associated Lynch Syndrome

Author

Broeke, S.W. ten, Klift, H.M. van der, Tops, Carli M.J., Aretz, Stefan, Bernstein, I., Buchanan, Daniel D., Hoogerbrugge, N., Mensenkamp, A.R., Spruijt, L., Nielsen, M., Win, Aung Ko, Broeke, S.W. ten, Klift, H.M. van der, Tops, Carli M.J., Aretz, Stefan, Bernstein, I., Buchanan, Daniel D., Hoogerbrugge, N., Mensenkamp, A.R., Spruijt, L., Nielsen, M., and Win, Aung Ko

Abstract

Item does not contain fulltext

Published
2018

23. CM-Score: a validated scoring system to predict CDKN2A germline mutations in melanoma families from Northern Europe

Author

Potjer, T.P., Helgadottir, H., Leenheer, M., Stoep, N. van der, Gruis, N.A., Hoiom, V., Olsson, H., Doorn, R. van, Vasen, H.F., Asperen, C.J. van, Spruijt, L., Dekkers, O.M., Hes, F.J., Potjer, T.P., Helgadottir, H., Leenheer, M., Stoep, N. van der, Gruis, N.A., Hoiom, V., Olsson, H., Doorn, R. van, Vasen, H.F., Asperen, C.J. van, Spruijt, L., Dekkers, O.M., and Hes, F.J.

Abstract

Contains fulltext : 199963.pdf (Publisher’s version ) (Open Access), BACKGROUND: Several factors have been reported that influence the probability of a germline CDKN2A mutation in a melanoma family. Our goal was to create a scoring system to estimate this probability, based on a set of clinical features present in the patient and his or her family. METHODS: Five clinical features and their association with CDKN2A mutations were investigated in a training cohort of 1227 Dutch melanoma families (13.7% with CDKN2A mutation) using multivariate logistic regression. Predefined features included number of family members with melanoma and with multiple primary melanomas, median age at diagnosis and presence of pancreatic cancer or upper airway cancer in a family member. Based on these five features, a scoring system (CDKN2A Mutation(CM)-Score) was developed and subsequently validated in a combined Swedish and Dutch familial melanoma cohort (n=421 families; 9.0% with CDKN2A mutation). RESULTS: All five features were significantly associated (p<0.05) with a CDKN2A mutation. At a CM-Score of 16 out of 49 possible points, the threshold of 10% mutation probability is approximated (9.9%; 95% CI 9.8 to 10.1). This probability further increased to >90% for families with >/=36 points. A CM-Score under 16 points was associated with a low mutation probability (/=16 points.

Published
2018

24. Role of germline aberrations affecting CTNNA1, MAP3K6 and MYD88 in gastric cancer susceptibility

Author

Weren, R.D.A. (Robbert D. A.), Van Der Post, R.S. (Rachel S.), Vogelaar, I.P. (Ingrid P.), Van Krieken, J.H. (J. Han), Spruijt, L. (Liesbeth), Lubinski, J. (Jan), Jakubowska, A. (Anna), Teodorczyk, U. (Urszula), Aalfs, C.M. (Cora), Hest, L.P. (Liselotte) van, Oliveira, C. (Carla), Kamping, E. (Eveline), Schackert, H.K. (Hans), Ranzani, G.N. (Guglielmina N.), Gómez García, E.B. (Encarna), Hes, F.J. (Frederik), Holinski-Feder, E. (Elke), Genuardi, M. (Maurizio), Ausems, M.G.E.M. (Margreet), Sijmons, R.H. (Rolf), Wagner, A. (Anja), Kolk, L.E. (Lizet) van der, Cats, A. (Annemieke), Bjørnevoll, I. (Inga), Hoogerbrugge, N. (Nicoline), Ligtenberg, M.J. (Marjolijn), Weren, R.D.A. (Robbert D. A.), Van Der Post, R.S. (Rachel S.), Vogelaar, I.P. (Ingrid P.), Van Krieken, J.H. (J. Han), Spruijt, L. (Liesbeth), Lubinski, J. (Jan), Jakubowska, A. (Anna), Teodorczyk, U. (Urszula), Aalfs, C.M. (Cora), Hest, L.P. (Liselotte) van, Oliveira, C. (Carla), Kamping, E. (Eveline), Schackert, H.K. (Hans), Ranzani, G.N. (Guglielmina N.), Gómez García, E.B. (Encarna), Hes, F.J. (Frederik), Holinski-Feder, E. (Elke), Genuardi, M. (Maurizio), Ausems, M.G.E.M. (Margreet), Sijmons, R.H. (Rolf), Wagner, A. (Anja), Kolk, L.E. (Lizet) van der, Cats, A. (Annemieke), Bjørnevoll, I. (Inga), Hoogerbrugge, N. (Nicoline), and Ligtenberg, M.J. (Marjolijn)

Abstract

Background: In approximately 10% of all gastric cancer (GC) cases, a heritable cause is suspected. A subset of these cases have a causative germline CDH1 mutation; however, in most cases the cause remains unknown. Our objective was to assess to what extent these remaining cases may be explained by germline mutations in the novel candidate GC predisposing genes CTNNA1, MAP3K6 or MYD88. Methods: We sequenced a large cohort of unexplained young and/or familial patients with GC (n=286) without a CDH1germline mutation for germline variants affecting CTNNA1, MAP3K6 and MYD88 using a targeted next-generation sequencing approach based on single-molecule molecular inversion probes. Results: Predicted deleterious germline variants were not encountered in MYD88, but recurrently observed in CTNNA1 (n=2) and MAP3K6 (n=3) in our cohort of patients with GC. In contrast to deleterious variants in CTNNA1, deleterious variants in MAP3K6 also occur frequently in the general population. Conclusions: Based on our results MAP3K6 should no longer be considered a GC predisposition gene, whereas deleterious CTNNA1 variants are confirmed as an infrequent cause of GC susceptibility. Biallelic MYD88 germline mutations are at most a very rare cause of GC susceptibility as no additional cases were identified.

Published
2018
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25. Role of germline aberrations affecting CTNNA1, MAP3K6 and MYD88 in gastric cancer susceptibility

Author

Weren, R.D.A., Post, R.S. van der, Vogelaar, I.P., Krieken, J.H.J.M. van, Spruijt, L., Lubinski, J., Jakubowska, A., Teodorczyk, U., Aalfs, C.M., Hest, L.P. van, Oliveira, C. de, Kamping, E.J., Schackert, H.K., Ranzani, G.N., Garcia, E.B., Hes, F.J., Holinski-Feder, E., Genuardi, M., Ausems, M.G.E.M., Sijmons, R.H., Wagner, A., Kolk, L.E. van der, Cats, A., Bjornevoll, I., Hoogerbrugge, N., Ligtenberg, M.J.L., Weren, R.D.A., Post, R.S. van der, Vogelaar, I.P., Krieken, J.H.J.M. van, Spruijt, L., Lubinski, J., Jakubowska, A., Teodorczyk, U., Aalfs, C.M., Hest, L.P. van, Oliveira, C. de, Kamping, E.J., Schackert, H.K., Ranzani, G.N., Garcia, E.B., Hes, F.J., Holinski-Feder, E., Genuardi, M., Ausems, M.G.E.M., Sijmons, R.H., Wagner, A., Kolk, L.E. van der, Cats, A., Bjornevoll, I., Hoogerbrugge, N., and Ligtenberg, M.J.L.

Abstract

Contains fulltext : 196812.pdf (publisher's version ) (Open Access), BACKGROUND: In approximately 10% of all gastric cancer (GC) cases, a heritable cause is suspected. A subset of these cases have a causative germline CDH1 mutation; however, in most cases the cause remains unknown. Our objective was to assess to what extent these remaining cases may be explained by germline mutations in the novel candidate GC predisposing genes CTNNA1, MAP3K6 or MYD88. METHODS: We sequenced a large cohort of unexplained young and/or familial patients with GC (n=286) without a CDH1germline mutation for germline variants affecting CTNNA1, MAP3K6 and MYD88 using a targeted next-generation sequencing approach based on single-molecule molecular inversion probes. RESULTS: Predicted deleterious germline variants were not encountered in MYD88, but recurrently observed in CTNNA1 (n=2) and MAP3K6 (n=3) in our cohort of patients with GC. In contrast to deleterious variants in CTNNA1, deleterious variants in MAP3K6 also occur frequently in the general population. CONCLUSIONS: Based on our results MAP3K6 should no longer be considered a GC predisposition gene, whereas deleterious CTNNA1 variants are confirmed as an infrequent cause of GC susceptibility. Biallelic MYD88 germline mutations are at most a very rare cause of GC susceptibility as no additional cases were identified.

Published
2018

26. SNP association study in PMS2-associated Lynch syndrome

Author

Broeke, S.W. ten, Elsayed, F.A., Pagan, Lisa, Olderode-Berends, M.J., Garcia, E.G., Gille, H.J., Mensenkamp, A.R., Spruijt, L., Wezel, T. van, Nielsen, M., Broeke, S.W. ten, Elsayed, F.A., Pagan, Lisa, Olderode-Berends, M.J., Garcia, E.G., Gille, H.J., Mensenkamp, A.R., Spruijt, L., Wezel, T. van, and Nielsen, M.

Abstract

Contains fulltext : 196139.pdf (publisher's version ) (Open Access)

Published
2018

27. Cancer Risks for PMS2-Associated Lynch Syndrome

Author

ten Broeke, SW, van der Klift, HM, Tops, CMJ, Aretz, S, Bernstein, I, Buchanan, DD, de la Chapelle, A, Capella, G, Clendenning, M, Engel, C, Gallinger, S, Gomez Garcia, E, Figueiredo, JC, Haile, R, Hampel, HL, Hopper, JL, Hoogerbrugge, N, Doeberitz, MVK, Le Marchand, L, Letteboer, TGW, Jenkins, MA, Lindblom, A, Lindor, NM, Mensenkamp, AR, Moller, P, Newcomb, PA, van Os, TAM, Pearlman, R, Pineda, M, Rahner, N, Redeker, EJW, Olderode-Berends, MJW, Rosty, C, Schackert, HK, Scott, R, Senter, L, Spruijt, L, Steinke-Lange, V, Suerink, M, Thibodeau, S, Vos, YJ, Wagner, A, Winship, I, Hes, FJ, Vasen, HFA, Wijnen, JT, Nielsen, M, Win, AK, ten Broeke, SW, van der Klift, HM, Tops, CMJ, Aretz, S, Bernstein, I, Buchanan, DD, de la Chapelle, A, Capella, G, Clendenning, M, Engel, C, Gallinger, S, Gomez Garcia, E, Figueiredo, JC, Haile, R, Hampel, HL, Hopper, JL, Hoogerbrugge, N, Doeberitz, MVK, Le Marchand, L, Letteboer, TGW, Jenkins, MA, Lindblom, A, Lindor, NM, Mensenkamp, AR, Moller, P, Newcomb, PA, van Os, TAM, Pearlman, R, Pineda, M, Rahner, N, Redeker, EJW, Olderode-Berends, MJW, Rosty, C, Schackert, HK, Scott, R, Senter, L, Spruijt, L, Steinke-Lange, V, Suerink, M, Thibodeau, S, Vos, YJ, Wagner, A, Winship, I, Hes, FJ, Vasen, HFA, Wijnen, JT, Nielsen, M, and Win, AK

Abstract

PURPOSE: Lynch syndrome due to pathogenic variants in the DNA mismatch repair genes MLH1, MSH2, and MSH6 is predominantly associated with colorectal and endometrial cancer, although extracolonic cancers have been described within the Lynch tumor spectrum. However, the age-specific cumulative risk (penetrance) of these cancers is still poorly defined for PMS2-associated Lynch syndrome. Using a large data set from a worldwide collaboration, our aim was to determine accurate penetrance measures of cancers for carriers of heterozygous pathogenic PMS2 variants. METHODS: A modified segregation analysis was conducted that incorporated both genotyped and nongenotyped relatives, with conditioning for ascertainment to estimates corrected for bias. Hazard ratios (HRs) and corresponding 95% CIs were estimated for each cancer site for mutation carriers compared with the general population, followed by estimation of penetrance. RESULTS: In total, 284 families consisting of 4,878 first- and second-degree family members were included in the analysis. PMS2 mutation carriers were at increased risk for colorectal cancer (cumulative risk to age 80 years of 13% [95% CI, 7.9% to 22%] for males and 12% [95% CI, 6.7% to 21%] for females) and endometrial cancer (13% [95% CI, 7.0%-24%]), compared with the general population (6.6%, 4.7%, and 2.4%, respectively). There was no clear evidence of an increased risk of ovarian, gastric, hepatobiliary, bladder, renal, brain, breast, prostate, or small bowel cancer. CONCLUSION: Heterozygous PMS2 mutation carriers were at small increased risk for colorectal and endometrial cancer but not for any other Lynch syndrome-associated cancer. This finding justifies that PMS2-specific screening protocols could be restricted to colonoscopies. The role of risk-reducing hysterectomy and bilateral salpingo-oophorectomy for PMS2 mutation carriers needs further discussion.

Published
2018

28. SNP association study in PMS2-associated Lynch syndrome

Author

ten Broeke, SW, Elsayed, FA, Pagan, L, Olderode-Berends, M J W, Garcia, EG, Gille, HJP, Hest, LP, Letteboer, TGW, van der Kolk, LE, Mensenkamp, AR, van Os, TA, Spruijt, L, Redeker, BJW, Suerink, M, Vos, YJ, Wagner, Anja, Wijnen, JT, Steyerberg, EW, Tops, CMJ, van Wezel, T, Nielsen, M, ten Broeke, SW, Elsayed, FA, Pagan, L, Olderode-Berends, M J W, Garcia, EG, Gille, HJP, Hest, LP, Letteboer, TGW, van der Kolk, LE, Mensenkamp, AR, van Os, TA, Spruijt, L, Redeker, BJW, Suerink, M, Vos, YJ, Wagner, Anja, Wijnen, JT, Steyerberg, EW, Tops, CMJ, van Wezel, T, and Nielsen, M

Published
2018

29. Role of germline aberrations affecting CTNNA1, MAP3K6 and MYD88 in gastric cancer susceptibility

Author

Weren, RDA, van der Post, RS, Vogelaar, IP, Van Krieken, JH, Spruijt, L, Lubinski, J, Jakubowska, A, Teodorczyk, U, Aalfs, CM, Hest, LP, Oliveira, C, Kamping, EJ, Schackert, HK, Ranzani, GN, Garcia, EBG, Hes, FJ, Holinski-Feder, E, Genuardi, M, Ausems, M, Sijmons, RH, Wagner, Anja, van der Kolk, LE, Cats, A, Bjornevoll, I, Hoogerbrugge, N, Ligtenberg, MJL, Weren, RDA, van der Post, RS, Vogelaar, IP, Van Krieken, JH, Spruijt, L, Lubinski, J, Jakubowska, A, Teodorczyk, U, Aalfs, CM, Hest, LP, Oliveira, C, Kamping, EJ, Schackert, HK, Ranzani, GN, Garcia, EBG, Hes, FJ, Holinski-Feder, E, Genuardi, M, Ausems, M, Sijmons, RH, Wagner, Anja, van der Kolk, LE, Cats, A, Bjornevoll, I, Hoogerbrugge, N, and Ligtenberg, MJL

Published
2018

30. Identification of new TRIP12 variants and detailed clinical evaluation of individuals with non-syndromic intellectual disability with or without autism

Author

Bramswig, N.C., Ludecke, H.J., Pettersson, M., Albrecht, B., Bernier, R.A., Cremer, K., Eichler, E.E., Falkenstein, D., Gerdts, J., Jansen, S, Kuechler, A., Kvarnung, M., Lindstrand, A., Nilsson, D., Nordgren, A., Pfundt, R.P., Spruijt, L., Surowy, H.M., Vries, B.B. de, Wieland, T., Engels, H., Strom, T.M., Kleefstra, T., Wieczorek, D., Bramswig, N.C., Ludecke, H.J., Pettersson, M., Albrecht, B., Bernier, R.A., Cremer, K., Eichler, E.E., Falkenstein, D., Gerdts, J., Jansen, S, Kuechler, A., Kvarnung, M., Lindstrand, A., Nilsson, D., Nordgren, A., Pfundt, R.P., Spruijt, L., Surowy, H.M., Vries, B.B. de, Wieland, T., Engels, H., Strom, T.M., Kleefstra, T., and Wieczorek, D.

Abstract

Contains fulltext : 169702.pdf (publisher's version ) (Closed access), The ubiquitin pathway is an enzymatic cascade including activating E1, conjugating E2, and ligating E3 enzymes, which governs protein degradation and sorting. It is crucial for many physiological processes. Compromised function of members of the ubiquitin pathway leads to a wide range of human diseases, such as cancer, neurodegenerative diseases, and neurodevelopmental disorders. Mutations in the thyroid hormone receptor interactor 12 (TRIP12) gene (OMIM 604506), which encodes an E3 ligase in the ubiquitin pathway, have been associated with autism spectrum disorder (ASD). In addition to autistic features, TRIP12 mutation carriers showed intellectual disability (ID). More recently, TRIP12 was postulated as a novel candidate gene for intellectual disability in a meta-analysis of published ID cohorts. However, detailed clinical information characterizing the phenotype of these individuals was not provided. In this study, we present seven novel individuals with private TRIP12 mutations including two splice site mutations, one nonsense mutation, three missense mutations, and one translocation case with a breakpoint in intron 1 of the TRIP12 gene and clinically review four previously published cases. The TRIP12 mutation-positive individuals presented with mild to moderate ID (10/11) or learning disability [intelligence quotient (IQ) 76 in one individual], ASD (8/11) and some of them with unspecific craniofacial dysmorphism and other anomalies. In this study, we provide detailed clinical information of 11 TRIP12 mutation-positive individuals and thereby expand the clinical spectrum of the TRIP12 gene in non-syndromic intellectual disability with or without ASD.

Published
2017

31. Unraveling genetic predisposition to familial or early onset gastric cancer using germline whole-exome sequencing

Author

Vogelaar, I.P., Post, R.S. van der, Krieken, J.H. van, Spruijt, L., Zelst-Stams, W.A.G. van, Kets, C.M., Lubinski, J., Jakubowska, A., Teodorczyk, U., Aalfs, C.M., Hest, L.P. van, Pinheiro, H., Oliveira, C. de, Jhangiani, S.N., Muzny, D.M., Gibbs, R.A., Lupski, J.R., Ligt, J. de, Vissers, L.E.L.M., Hoischen, A., Gilissen, C., Vorst, J.M. van de, Goeman, J.J., Schackert, H.K., Ranzani, G.N., Molinaro, V., Garcia, E.B., Hes, F.J., Holinski-Feder, E., Genuardi, M., Ausems, M., Sijmons, R.H., Wagner, A., Kolk, L.E. van der, Bjornevoll, I., Hoberg-Vetti, H., Geurts van Kessel, A.H.M., Kuiper, R.P., Ligtenberg, M.J.L., Hoogerbrugge, N., Vogelaar, I.P., Post, R.S. van der, Krieken, J.H. van, Spruijt, L., Zelst-Stams, W.A.G. van, Kets, C.M., Lubinski, J., Jakubowska, A., Teodorczyk, U., Aalfs, C.M., Hest, L.P. van, Pinheiro, H., Oliveira, C. de, Jhangiani, S.N., Muzny, D.M., Gibbs, R.A., Lupski, J.R., Ligt, J. de, Vissers, L.E.L.M., Hoischen, A., Gilissen, C., Vorst, J.M. van de, Goeman, J.J., Schackert, H.K., Ranzani, G.N., Molinaro, V., Garcia, E.B., Hes, F.J., Holinski-Feder, E., Genuardi, M., Ausems, M., Sijmons, R.H., Wagner, A., Kolk, L.E. van der, Bjornevoll, I., Hoberg-Vetti, H., Geurts van Kessel, A.H.M., Kuiper, R.P., Ligtenberg, M.J.L., and Hoogerbrugge, N.

Abstract

Contains fulltext : 182216.pdf (publisher's version ) (Open Access), Recognition of individuals with a genetic predisposition to gastric cancer (GC) enables preventive measures. However, the underlying cause of genetic susceptibility to gastric cancer remains largely unexplained. We performed germline whole-exome sequencing on leukocyte DNA of 54 patients from 53 families with genetically unexplained diffuse-type and intestinal-type GC to identify novel GC-predisposing candidate genes. As young age at diagnosis and familial clustering are hallmarks of genetic tumor susceptibility, we selected patients that were diagnosed below the age of 35, patients from families with two cases of GC at or below age 60 and patients from families with three GC cases at or below age 70. All included individuals were tested negative for germline CDH1 mutations before or during the study. Variants that were possibly deleterious according to in silico predictions were filtered using several independent approaches that were based on gene function and gene mutation burden in controls. Despite a rigorous search, no obvious candidate GC predisposition genes were identified. This negative result stresses the importance of future research studies in large, homogeneous cohorts.

Published
2017

32. 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
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33. Unraveling genetic predisposition to familial or early onset gastric cancer using germline whole-exome sequencing

Author

Vogelaar, I.P. (Ingrid P.), Van Der Post, R.S. (Rachel S.), Van Krieken, J.H. (J. Han), Spruijt, L. (Liesbeth), Zelst-Stams, W.A. van, Kets, C.M. (Marleen), Lubinski, J. (Jan), Jakubowska, A. (Anna), Teodorczyk, U. (Urszula), Aalfs, C.M. (Cora), Hest, L.P. (Liselotte) van, Pinheiro, H. (Hugo), Oliveira, C. (Carla), Jhangiani, S.N. (Shalini N.), Muzny, D. (Donna), Gibbs, R.A. (Richard A.), Lupski, J.R. (James R.), Ligt, J. (Joep) de, Vissers, L.E.L.M., Hoischen, A. (Alex), Gilissen, C. (Christian), Van De Vorst, M. (Maartje), Goeman, J.J. (Jelle), Schackert, H.K. (Hans), Ranzani, G.N. (Guglielmina N.), Molinaro, V. (Valeria), Garcia, E.B.G., Hes, F.J. (Frederik), Holinski-Feder, E. (Elke), Genuardi, M. (Maurizio), Ausems, M.G.E.M. (Margreet), Sijmons, R.H. (Rolf), Wagner, A. (Anja), Kolk, L.E. (Lizet) van der, Bjørnevoll, I. (Inga), Høberg Vetti, H. (Hildegunn), Geurts van Kessel, A.H.M. (Ad), Kuiper, R. (Ruud), Ligtenberg, M.J. (Marjolijn), Hoogerbrugge, N. (Nicoline), Vogelaar, I.P. (Ingrid P.), Van Der Post, R.S. (Rachel S.), Van Krieken, J.H. (J. Han), Spruijt, L. (Liesbeth), Zelst-Stams, W.A. van, Kets, C.M. (Marleen), Lubinski, J. (Jan), Jakubowska, A. (Anna), Teodorczyk, U. (Urszula), Aalfs, C.M. (Cora), Hest, L.P. (Liselotte) van, Pinheiro, H. (Hugo), Oliveira, C. (Carla), Jhangiani, S.N. (Shalini N.), Muzny, D. (Donna), Gibbs, R.A. (Richard A.), Lupski, J.R. (James R.), Ligt, J. (Joep) de, Vissers, L.E.L.M., Hoischen, A. (Alex), Gilissen, C. (Christian), Van De Vorst, M. (Maartje), Goeman, J.J. (Jelle), Schackert, H.K. (Hans), Ranzani, G.N. (Guglielmina N.), Molinaro, V. (Valeria), Garcia, E.B.G., Hes, F.J. (Frederik), Holinski-Feder, E. (Elke), Genuardi, M. (Maurizio), Ausems, M.G.E.M. (Margreet), Sijmons, R.H. (Rolf), Wagner, A. (Anja), Kolk, L.E. (Lizet) van der, Bjørnevoll, I. (Inga), Høberg Vetti, H. (Hildegunn), Geurts van Kessel, A.H.M. (Ad), Kuiper, R. (Ruud), Ligtenberg, M.J. (Marjolijn), and Hoogerbrugge, N. (Nicoline)

Abstract

Recognition of individuals with a genetic predisposition to gastric cancer (GC) enables preventive measures. However, the underlying cause of genetic susceptibility to gastric cancer remains largely unexplained. We performed germline whole-exome sequencing on leukocyte DNA of 54 patients from 53 families with genetically unexplained diffuse-type and intestinal-type GC to identify novel GC-predisposing candidate genes. As young age at diagnosis and familial clustering are hallmarks of genetic tumor susceptibility, we selected patients that were diagnosed below the age of 35, patients from families with two cases of GC at or below age 60 and patients from families with three GC cases at or below age 70. All included individuals were tested negative for germline CDH1 mutations before or during the study. Variants that were possibly deleterious according to in silico predictions were filtered using several independent approaches that were based on gene function and gene mutation burden in controls. Despite a rigorous search, no obvious candidate GC predisposition genes were identified. This negative result stresses the importance of future research studies in large, homogeneous cohorts.

Published
2017
Full Text
View/download PDF

34. Unraveling genetic predisposition to familial or early onset gastric cancer using germline whole-exome sequencing

Author

Vogelaar, IP, van der Post, RS, van Krieken, J, Spruijt, L, van Zelst-Stams, W A G, Kets, CM, Lubinski, J, Jakubowska, A, Teodorczyk, U, Aalfs, CM, van Hest, LP (Liselotte), Pinheiro, H, Oliveira, C, Jhangiani, SN, Muzny, DM, Gibbs, RA, Lupski, JR, de Ligt, J, Vissers, L, Hoischen, A, Gilissen, C, van de Vorst, M, Goeman, JJ, Schackert, HK, Ranzani, GN, Molinaro, V, Garcia, EBG, Hes, FJ, Holinski-Feder, E, Genuardi, M, Ausems, M, Sijmons, RH, Wagner, Anja, van der Kolk, LE, Bjornevoll, I, Hoberg-Vetti, H, van Kessel, AG, Kuiper, RP (Roland), Ligtenberg, MJL, Hoogerbrugge, N, Vogelaar, IP, van der Post, RS, van Krieken, J, Spruijt, L, van Zelst-Stams, W A G, Kets, CM, Lubinski, J, Jakubowska, A, Teodorczyk, U, Aalfs, CM, van Hest, LP (Liselotte), Pinheiro, H, Oliveira, C, Jhangiani, SN, Muzny, DM, Gibbs, RA, Lupski, JR, de Ligt, J, Vissers, L, Hoischen, A, Gilissen, C, van de Vorst, M, Goeman, JJ, Schackert, HK, Ranzani, GN, Molinaro, V, Garcia, EBG, Hes, FJ, Holinski-Feder, E, Genuardi, M, Ausems, M, Sijmons, RH, Wagner, Anja, van der Kolk, LE, Bjornevoll, I, Hoberg-Vetti, H, van Kessel, AG, Kuiper, RP (Roland), Ligtenberg, MJL, and Hoogerbrugge, N

Published
2017

35. 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

36. Pathogenetics of alveolar capillary dysplasia with misalignment of pulmonary veins

Author

Szafranski, P., Gambin, T., Dharmadhikari, A.V., Akdemir, K.C., Jhangiani, S.N., Schuette, J., Godiwala, N., Yatsenko, S.A., Sebastian, J., Madan-Khetarpal, S., Surti, U., Abellar, R.G., Bateman, D.A., Wilson, A.L., Markham, M.H., Slamon, J., Santos-Simarro, F., Palomares, M., Nevado, J., Lapunzina, P., Chung, B.H., Wong, W.L., Chu, Y.W., Mok, G.T., Kerem, E., Reiter, J., Ambalavanan, N., Anderson, S.A., Kelly, D.R., Shieh, J., Rosenthal, T.C., Scheible, K., Steiner, L., Iqbal, M.A., McKinnon, M.L., Hamilton, S.J., Schlade-Bartusiak, K., English, D., Hendson, G., Roeder, E.R., DeNapoli, T.S., Littlejohn, R.O., Wolff, D.J., Wagner, C.L., Yeung, A., Francis, D., Fiorino, E.K., Edelman, M., Fox, J., Hayes, D.A., Janssens, S., Baere, E. De, Menten, B., Loccufier, A., Vanwalleghem, L., Moerman, P., Sznajer, Y., Lay, A.S., Kussmann, J.L., Chawla, J., Payton, D.J., Phillips, G.E., Brosens, E., Tibboel, D., Klein, A., Maystadt, I., Fisher, R., Sebire, N., Male, A., Chopra, M., Pinner, J., Malcolm, G., Peters, G., Arbuckle, S., Lees, M., Mead, Z., Quarrell, O., Sayers, R., Owens, M., Shaw-Smith, C., Lioy, J., McKay, E., Leeuw, N. de, Feenstra, I., Spruijt, L., Elmslie, F., Thiruchelvam, T., Bacino, C.A., Langston, C., Lupski, J.R., Sen, P., Popek, E., Stankiewicz, P., Szafranski, P., Gambin, T., Dharmadhikari, A.V., Akdemir, K.C., Jhangiani, S.N., Schuette, J., Godiwala, N., Yatsenko, S.A., Sebastian, J., Madan-Khetarpal, S., Surti, U., Abellar, R.G., Bateman, D.A., Wilson, A.L., Markham, M.H., Slamon, J., Santos-Simarro, F., Palomares, M., Nevado, J., Lapunzina, P., Chung, B.H., Wong, W.L., Chu, Y.W., Mok, G.T., Kerem, E., Reiter, J., Ambalavanan, N., Anderson, S.A., Kelly, D.R., Shieh, J., Rosenthal, T.C., Scheible, K., Steiner, L., Iqbal, M.A., McKinnon, M.L., Hamilton, S.J., Schlade-Bartusiak, K., English, D., Hendson, G., Roeder, E.R., DeNapoli, T.S., Littlejohn, R.O., Wolff, D.J., Wagner, C.L., Yeung, A., Francis, D., Fiorino, E.K., Edelman, M., Fox, J., Hayes, D.A., Janssens, S., Baere, E. De, Menten, B., Loccufier, A., Vanwalleghem, L., Moerman, P., Sznajer, Y., Lay, A.S., Kussmann, J.L., Chawla, J., Payton, D.J., Phillips, G.E., Brosens, E., Tibboel, D., Klein, A., Maystadt, I., Fisher, R., Sebire, N., Male, A., Chopra, M., Pinner, J., Malcolm, G., Peters, G., Arbuckle, S., Lees, M., Mead, Z., Quarrell, O., Sayers, R., Owens, M., Shaw-Smith, C., Lioy, J., McKay, E., Leeuw, N. de, Feenstra, I., Spruijt, L., Elmslie, F., Thiruchelvam, T., Bacino, C.A., Langston, C., Lupski, J.R., Sen, P., Popek, E., and Stankiewicz, P.

Abstract

Contains fulltext : 168023.pdf (publisher's version ) (Closed access), Alveolar capillary dysplasia with misalignment of pulmonary veins (ACDMPV) is a lethal lung developmental disorder caused by heterozygous point mutations or genomic deletion copy-number variants (CNVs) of FOXF1 or its upstream enhancer involving fetal lung-expressed long noncoding RNA genes LINC01081 and LINC01082. Using custom-designed array comparative genomic hybridization, Sanger sequencing, whole exome sequencing (WES), and bioinformatic analyses, we studied 22 new unrelated families (20 postnatal and two prenatal) with clinically diagnosed ACDMPV. We describe novel deletion CNVs at the FOXF1 locus in 13 unrelated ACDMPV patients. Together with the previously reported cases, all 31 genomic deletions in 16q24.1, pathogenic for ACDMPV, for which parental origin was determined, arose de novo with 30 of them occurring on the maternally inherited chromosome 16, strongly implicating genomic imprinting of the FOXF1 locus in human lungs. Surprisingly, we have also identified four ACDMPV families with the pathogenic variants in the FOXF1 locus that arose on paternal chromosome 16. Interestingly, a combination of the severe cardiac defects, including hypoplastic left heart, and single umbilical artery were observed only in children with deletion CNVs involving FOXF1 and its upstream enhancer. Our data demonstrate that genomic imprinting at 16q24.1 plays an important role in variable ACDMPV manifestation likely through long-range regulation of FOXF1 expression, and may be also responsible for key phenotypic features of maternal uniparental disomy 16. Moreover, in one family, WES revealed a de novo missense variant in ESRP1, potentially implicating FGF signaling in the etiology of ACDMPV.

Published
2016

37. High Satisfaction and Low Distress in Breast Cancer Patients One Year after BRCA-Mutation Testing without Prior Face-to-Face Genetic Counseling

Author

Sie, A.S., Spruijt, L., Zelst-Stams, W.A.G. van, Mensenkamp, A.R., Ligtenberg, M.J.L., Brunner, H.G., Prins, J.B., Hoogerbrugge, N., Sie, A.S., Spruijt, L., Zelst-Stams, W.A.G. van, Mensenkamp, A.R., Ligtenberg, M.J.L., Brunner, H.G., Prins, J.B., and Hoogerbrugge, N.

Abstract

Contains fulltext : 167845.pdf (publisher's version ) (Open Access), According to standard practice following referral to clinical genetics, most high risk breast cancer (BC) patients in many countries receive face-to-face genetic counseling prior to BRCA-mutation testing (DNA-intake). We evaluated a novel format by prospective study: replacing the intake consultation with telephone, written and digital information sent home. Face-to-face counseling then followed BRCA-mutation testing (DNA-direct). One year after BRCA-result disclosure, 108 participants returned long-term follow-up questionnaires, of whom 59 (55 %) had previously chosen DNA-direct (intervention) versus DNA-intake (standard practice i.e., control: 45 %). Questionnaires assessed satisfaction and psychological distress. All participants were satisfied and 85 % of DNA-direct participants would choose this procedure again; 10 % would prefer DNA-intake and 5 % were undecided. In repeated measurements ANOVA, general distress (GHQ-12, p = 0.01) and BC-specific distress (IES-bc, p = 0.03) were lower in DNA-direct than DNA-intake at all time measurements. Heredity-specific distress (IES-her) did not differ significantly between groups. Multivariate regression analyses showed that choice of procedure did not significantly contribute to either general or heredity-specific distress. BC-specific distress (after BC diagnosis) did contribute to both general and heredity-specific distress. This suggests that higher distress scores reflected BC experience, rather than the type of genetic diagnostic procedure. In conclusion, the large majority of BC patients that used DNA-direct reported high satisfaction without increased distress both in the short term, and 1 year after conclusion of genetic testing.

Published
2016

38. Identification of Novel Candidate Genes for Early-Onset Colorectal Cancer Susceptibility

Author

Voer, R.M. de, Hahn, M.M., Weren, R.D.A., Mensenkamp, A.R., Gilissen, C.F., Zelst-Stams, W.A. van, Spruijt, L., Kets, C.M., Zhang, J.Z, Venselaar, H., Vreede, L.A., Schubert, N., Tychon, M.W.J., Derks, R, Schackert, H.K., Geurts van Kessel, A.H., Hoogerbrugge, N., Ligtenberg, M.J., Kuiper, R.P., Voer, R.M. de, Hahn, M.M., Weren, R.D.A., Mensenkamp, A.R., Gilissen, C.F., Zelst-Stams, W.A. van, Spruijt, L., Kets, C.M., Zhang, J.Z, Venselaar, H., Vreede, L.A., Schubert, N., Tychon, M.W.J., Derks, R, Schackert, H.K., Geurts van Kessel, A.H., Hoogerbrugge, N., Ligtenberg, M.J., and Kuiper, R.P.

Abstract

Contains fulltext : 165665.PDF (publisher's version ) (Open Access), Approximately 25-30% of colorectal cancer (CRC) cases are expected to result from a genetic predisposition, but in only 5-10% of these cases highly penetrant germline mutations are found. The remaining CRC heritability is still unexplained, and may be caused by a hitherto-undefined set of rare variants with a moderately penetrant risk. Here we aimed to identify novel risk factors for early-onset CRC using whole-exome sequencing, which was performed on a cohort of CRC individuals (n = 55) with a disease onset before 45 years of age. We searched for genes that were recurrently affected by rare variants (minor allele frequency

Published
2016

40. Hypertrophic left calf and multiple flesh-coloured subcutaneous tumours in a 5-year-old girl: a quiz. Gardner-associated fibroma

Author

Geel, M.J. van, Wijnen, M.H., Hoppenreijs, E.P.A.H., Gierenz, N., Spruijt, L., Koolwijk, M.P. van, Flucke, U.E., Blokx, W.A.M., and Seyger, M.M.B.

Subjects
Tumours of the digestive tract Radboud Institute for Health Sciences [Radboudumc 14], Cancer development and immune defence Radboud Institute for Molecular Life Sciences [Radboudumc 2], Other Research Radboud Institute for Health Sciences [Radboudumc 0], Inflammatory diseases Radboud Institute for Health Sciences [Radboudumc 5], Rare cancers Radboud Institute for Molecular Life Sciences [Radboudumc 9], GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries), Inflammatory diseases Radboud Institute for Molecular Life Sciences [Radboudumc 5]
Abstract

Contains fulltext : 138194.pdf (Publisher’s version ) (Open Access)

Published
2014

41. Identification of new TRIP12 variants and detailed clinical evaluation of individuals with non-syndromic intellectual disability with or without autism

Author

Bramswig, Nuria C., primary, Lüdecke, H.-J., additional, Pettersson, M., additional, Albrecht, B., additional, Bernier, R. A., additional, Cremer, K., additional, Eichler, E. E., additional, Falkenstein, D., additional, Gerdts, J., additional, Jansen, S., additional, Kuechler, A., additional, Kvarnung, M., additional, Lindstrand, A., additional, Nilsson, D., additional, Nordgren, A., additional, Pfundt, R., additional, Spruijt, L., additional, Surowy, H. M., additional, de Vries, B. B. A., additional, Wieland, T., additional, Engels, H., additional, Strom, T. M., additional, Kleefstra, T., additional, and Wieczorek, D., additional

Published
2016
Full Text
View/download PDF

42. A germline homozygous mutation in the base-excision repair gene NTHL1 causes adenomatous polyposis and colorectal cancer

Author

Weren, R.D.A., Ligtenberg, M.J., Kets, C.M., Voer, R.M. de, Verwiel, E.T.P., Spruijt, L., Zelst-Stams, W.A.G. van, Jongmans, M.C.J., Gilissen, C., Hehir, J.Y., Hoischen, A., Shendure, J., Boyle, E.A., Kamping, E.J., Nagtegaal, I.D., Tops, B.B.J., Nagengast, F.M., Geurts van Kessel, A.H.M., Krieken, J.H.J.M. van, Kuiper, R.P., Hoogerbrugge, N., Weren, R.D.A., Ligtenberg, M.J., Kets, C.M., Voer, R.M. de, Verwiel, E.T.P., Spruijt, L., Zelst-Stams, W.A.G. van, Jongmans, M.C.J., Gilissen, C., Hehir, J.Y., Hoischen, A., Shendure, J., Boyle, E.A., Kamping, E.J., Nagtegaal, I.D., Tops, B.B.J., Nagengast, F.M., Geurts van Kessel, A.H.M., Krieken, J.H.J.M. van, Kuiper, R.P., and Hoogerbrugge, N.

Abstract

Contains fulltext : 155056.pdf (publisher's version ) (Closed access), The genetic cause underlying the development of multiple colonic adenomas, the premalignant precursors of colorectal cancer (CRC), frequently remains unresolved in patients with adenomatous polyposis. Here we applied whole-exome sequencing to 51 individuals with multiple colonic adenomas from 48 families. In seven affected individuals from three unrelated families, we identified a homozygous germline nonsense mutation in the base-excision repair (BER) gene NTHL1. This mutation was exclusively found in a heterozygous state in controls (minor allele frequency of 0.0036; n = 2,329). All three families showed recessive inheritance of the adenomatous polyposis phenotype and progression to CRC in at least one member. All three affected women developed an endometrial malignancy or premalignancy. Genetic analysis of three carcinomas and five adenomas from different affected individuals showed a non-hypermutated profile enriched for cytosine-to-thymine transitions. We conclude that a homozygous loss-of-function germline mutation in the NTHL1 gene predisposes to a new subtype of BER-associated adenomatous polyposis and CRC.

Published
2015

43. Deleterious Germline BLM Mutations and the Risk for Early-onset Colorectal Cancer

Author

Voer, R.M. de, Hahn, M.M., Mensenkamp, A.R., Hoischen, A., Gilissen, C.F., Henkes, A., Spruijt, L., Zelst-Stams, W.A. van, Kets, C.M., Verwiel, E.T.P., Nagtegaal, I.D., Schackert, H.K., Kessel, A.G. van, Hoogerbrugge, N., Ligtenberg, M.J., Kuiper, R.P., Voer, R.M. de, Hahn, M.M., Mensenkamp, A.R., Hoischen, A., Gilissen, C.F., Henkes, A., Spruijt, L., Zelst-Stams, W.A. van, Kets, C.M., Verwiel, E.T.P., Nagtegaal, I.D., Schackert, H.K., Kessel, A.G. van, Hoogerbrugge, N., Ligtenberg, M.J., and Kuiper, R.P.

Abstract

Contains fulltext : 154952.pdf (publisher's version ) (Open Access), Bloom syndrome is an autosomal recessive disorder characterized by chromosomal instability and increased cancer risk, caused by biallelic mutations in the RECQL-helicase gene BLM. Previous studies have led to conflicting conclusions as to whether carriers of heterozygous BLM mutations have an increased risk to develop colorectal cancer (CRC). We recently identified two carriers of a pathogenic BLM mutation in a cohort of 55 early-onset CRC patients (

Published
2015

44. Allelic Mutations of KITLG, Encoding KIT Ligand, Cause Asymmetric and Unilateral Hearing Loss and Waardenburg Syndrome Type 2

Author

Zazo Seco, C., Castro, L.S. de, Nierop, J.W. van, Morin, M., Jhangiani, S., Verver, E.J., Schraders, M., Maiwald, N., Wesdorp, F.M., Venselaar, H., Spruijt, L., Oostrik, J., Schoots, J., Reeuwijk, J. van, Lelieveld, S.H., Huygen, P.L.M., Insenser, M., Admiraal, R.J.C., Pennings, R.J.E., Hoefsloot, L.H., Arias Vasquez, A., Ligt, J. de, Yntema, H.G., Jansen, J.H., Muzny, D.M., Huls, G.A., Rossum, M.M. van, Lupski, J.R., Moreno-Pelayo, M.A., Kunst, H.P.M., Kremer, H., Zazo Seco, C., Castro, L.S. de, Nierop, J.W. van, Morin, M., Jhangiani, S., Verver, E.J., Schraders, M., Maiwald, N., Wesdorp, F.M., Venselaar, H., Spruijt, L., Oostrik, J., Schoots, J., Reeuwijk, J. van, Lelieveld, S.H., Huygen, P.L.M., Insenser, M., Admiraal, R.J.C., Pennings, R.J.E., Hoefsloot, L.H., Arias Vasquez, A., Ligt, J. de, Yntema, H.G., Jansen, J.H., Muzny, D.M., Huls, G.A., Rossum, M.M. van, Lupski, J.R., Moreno-Pelayo, M.A., Kunst, H.P.M., and Kremer, H.

Abstract

Contains fulltext : 152605.pdf (publisher's version ) (Closed access), Linkage analysis combined with whole-exome sequencing in a large family with congenital and stable non-syndromic unilateral and asymmetric hearing loss (NS-UHL/AHL) revealed a heterozygous truncating mutation, c.286_303delinsT (p.Ser96Ter), in KITLG. This mutation co-segregated with NS-UHL/AHL as a dominant trait with reduced penetrance. By screening a panel of probands with NS-UHL/AHL, we found an additional mutation, c.200_202del (p.His67_Cys68delinsArg). In vitro studies revealed that the p.His67_Cys68delinsArg transmembrane isoform of KITLG is not detectable at the cell membrane, supporting pathogenicity. KITLG encodes a ligand for the KIT receptor. Also, KITLG-KIT signaling and MITF are suggested to mutually interact in melanocyte development. Because mutations in MITF are causative of Waardenburg syndrome type 2 (WS2), we screened KITLG in suspected WS2-affected probands. A heterozygous missense mutation, c.310C>G (p.Leu104Val), that segregated with WS2 was identified in a small family. In vitro studies revealed that the p.Leu104Val transmembrane isoform of KITLG is located at the cell membrane, as is wild-type KITLG. However, in culture media of transfected cells, the p.Leu104Val soluble isoform of KITLG was reduced, and no soluble p.His67_Cys68delinsArg and p.Ser96Ter KITLG could be detected. These data suggest that mutations in KITLG associated with NS-UHL/AHL have a loss-of-function effect. We speculate that the mechanism of the mutation underlying WS2 and leading to membrane incorporation and reduced secretion of KITLG occurs via a dominant-negative or gain-of-function effect. Our study unveils different phenotypes associated with KITLG, previously associated with pigmentation abnormalities, and will thereby improve the genetic counseling given to individuals with KITLG variants.

Published
2015

45. 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

46. Pancreatic cancer-associated gene polymorphisms in a nation-wide cohort of p16-Leiden germline mutation carriers; a case-control study

Author

Potjer, T.P., Stoep, N. van der, Houwing-Duistermaat, J.J., Konings, I.C., Aalfs, C.M., Akker, P.C. van den, Ausems, M.G., Dommering, C.J., Kolk, L.E. van der, Maiburg, M.C., Spruijt, L., Wagner, A., Vasen, H.F.A., Hes, F.J., Potjer, T.P., Stoep, N. van der, Houwing-Duistermaat, J.J., Konings, I.C., Aalfs, C.M., Akker, P.C. van den, Ausems, M.G., Dommering, C.J., Kolk, L.E. van der, Maiburg, M.C., Spruijt, L., Wagner, A., Vasen, H.F.A., and Hes, F.J.

Abstract

Contains fulltext : 153585.pdf (publisher's version ) (Open Access), BACKGROUND: The p16-Leiden founder mutation in the CDKN2A gene is the most common cause of Familial Atypical Multiple Mole Melanoma (FAMMM) syndrome in the Netherlands. Individuals with this mutation are at increased risk for developing melanoma of the skin, as well as pancreatic cancer. However, there is a notable interfamilial variability in the occurrence of pancreatic cancer among p16-Leiden families. We aimed to test whether previously identified genetic risk factors for pancreatic cancer modify the risk for pancreatic cancer in p16-Leiden germline mutation carriers. METHODS: Seven pancreatic cancer-associated SNPs were selected from the literature and were genotyped in a cohort of 185 p16-Leiden germline mutation carriers from 88 families, including 50 cases (median age 55 years) with pancreatic cancer and 135 controls (median age 64 years) without pancreatic cancer. Allelic odds ratios per SNP were calculated. Results : No significant association with pancreatic cancer was found for any of the seven SNPs. CONCLUSIONS: Since genetic modifiers for developing melanoma have already been identified in CDKN2A mutation carriers, this study does not exclude that genetic modifiers do not play a role in the individual pancreatic cancer risk in this cohort of p16-Leiden germline mutation carriers. The search for these modifiers should therefore continue, because they can potentially facilitate more targeted pancreatic surveillance programs.

Published
2015

47. Allelic mutations of KITLG, encoding KIT ligand, cause asymmetric and unilateral hearing loss and Waardenburg syndrome type 2

Author

Zazo Seco, C. (Celia), Serrão De Castro, L. (Luciana), Nierop, J.W.I. van, Morín, M. (Matías), Jhangiani, S.N. (Shalini N.), Verver, E.J.J. (Eva J. J.), Schraders, M. (Margit), Maiwald, N. (Nadine), Wesdorp, M. (Mieke), Venselaar, H. (Hanka), Spruijt, L. (Liesbeth), Oostrik, J. (Jaap), Schoots, J. (Jeroen), Reeuwijk, J. (Jeroen) van, Lelieveld, S.H. (Stefan H.), Huygen, P.L.M. (Patrick), Insenser, M. (María), Admiraal, R.J. (Ronald), Pennings, R.J.E. (Ronald J.E.), Hoefsloot, E.H. (Lies), Arias-Vásquez, A. (Alejandro), Ligt, J. (Joep) de, Yntema, H.G., Jansen, J.H. (Joop H.), Muzny, D. (Donna), Huls, G. (Gerwin), Rossum, M.M. (Michelle) van, Lupski, J.R. (James R.), Moreno-Pelayo, M.A. (Miguel Angel), Kunst, H.P.M. (Henricus P.M.), Kremer, H. (Hannie), Zazo Seco, C. (Celia), Serrão De Castro, L. (Luciana), Nierop, J.W.I. van, Morín, M. (Matías), Jhangiani, S.N. (Shalini N.), Verver, E.J.J. (Eva J. J.), Schraders, M. (Margit), Maiwald, N. (Nadine), Wesdorp, M. (Mieke), Venselaar, H. (Hanka), Spruijt, L. (Liesbeth), Oostrik, J. (Jaap), Schoots, J. (Jeroen), Reeuwijk, J. (Jeroen) van, Lelieveld, S.H. (Stefan H.), Huygen, P.L.M. (Patrick), Insenser, M. (María), Admiraal, R.J. (Ronald), Pennings, R.J.E. (Ronald J.E.), Hoefsloot, E.H. (Lies), Arias-Vásquez, A. (Alejandro), Ligt, J. (Joep) de, Yntema, H.G., Jansen, J.H. (Joop H.), Muzny, D. (Donna), Huls, G. (Gerwin), Rossum, M.M. (Michelle) van, Lupski, J.R. (James R.), Moreno-Pelayo, M.A. (Miguel Angel), Kunst, H.P.M. (Henricus P.M.), and Kremer, H. (Hannie)

Abstract

Linkage analysis combined with whole-exome sequencing in a large family with congenital and stable non-syndromic unilateral and asymmetric hearing loss (NS-UHL/AHL) revealed a heterozygous truncating mutation, c.286-303delinsT (p.Ser96Ter), in KITLG. This mutation co-segregated with NS-UHL/AHL as a dominant trait with reduced penetrance. By screening a panel of probands with NS-UHL/AHL, we found an additional mutation, c.200-202del (p.His67-Cys68delinsArg). In vitro studies revealed that the p.His67-Cys68delinsArg transmembrane isoform of KITLG is not detectable at the cell membrane, supporting pathogenicity. KITLG encodes a ligand for the KIT receptor. Also, KITLG-KIT signaling and MITF are suggested to mutually interact in melanocyte development. Because mutations in MITF are causative of Waardenburg syndrome type 2 (WS2), we screened KITLG in suspected WS2-affected probands. A heterozygous missense mutation, c.310C>G (p.Leu104Val), that segregated with WS2 was identified in a small family. In vitro studies revealed that the p.Leu104Val transmembrane isoform of KITLG is located at the cell membrane, as is wild-type KITLG. However, in culture media of transfected cells, the p.Leu104Val soluble isoform of KITLG was reduced, and no soluble p.His67-Cys68delinsArg and p.Ser96Ter KITLG could be detected. These data suggest that mutations in KITLG associated with NS-UHL/AHL have a loss-of-function effect. We speculate that the mechanism of the mutation underlying WS2 and leading to membrane incorporation and reduced secretion of KITLG occurs via a dominant-negative or gain-of-function effect. Our study unveils different phenotypes associated with KITLG, previously associated with pigmentation abnormalities, and will thereby improve the genetic counseling given to individuals with KITLG variants.

Published
2015
Full Text
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48. Pancreatic Cancer-Associated Gene Polymorphisms in a Nation-Wide Cohort of P16-Leiden Germline Mutation Carriers; a Case-Control Study Medical Genetics

Author

Potjer, TP, van der Stoep, N, Houwing-Duistermaat, JJ, Konings, Ingrid, Aalfs, CM, van den Akker, PC, Ausems, MG, Dommering, CJ, van der Kolk, LE, Maiburg, MC, Spruijt, L, Wagner, Anja, Vasen, HFA, Hes, FJ, Potjer, TP, van der Stoep, N, Houwing-Duistermaat, JJ, Konings, Ingrid, Aalfs, CM, van den Akker, PC, Ausems, MG, Dommering, CJ, van der Kolk, LE, Maiburg, MC, Spruijt, L, Wagner, Anja, Vasen, HFA, and Hes, FJ

Published
2015

49. Founder mutations among the Dutch*

Author

Zeegers, M.P.A., van Poppel, F., Vlietinck, R., Spruijt, L., Ostrer, H., Wilde, A.M., Tintelen, Complexe Genetica, Populatie Genetica, and RS: NUTRIM - R4 - Gene-environment interaction

Subjects
General practice, Library science, Sociology
Abstract

Department of Epidemiology, Maastricht University, PO Box 616, 6200 MD, Maastricht, The Netherlands; Academic Centre of General Practice, Catholic University Leuven, Kapucijnenvoer 33Blok J 3000 Leuven, Belgium; Netherlands Interdisciplinary Demographic Institute (NIDI), PO Box 11650, 2502 AR, Denhaag, The Netherlands; Department of Genetics and Cell Biology, Maastricht University, PO Box 616, 6200 MD, Maastricht, The Netherlands; New York University School of Medicine, 550 First Avenue, MSB 136, New York, NY 10016, USA

Published
2013
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50. Mutation and association analyses of the candidate genes ESR1, ESR2, MAX, PCNA, and KAT2A in patients with unexplained MSH2-deficient tumors

Author

Rahner, N., Brockschmidt, F.F., Steinke, V., Kahl, P., Becker, T., Vasen, H.F., Wijnen, J.T., Tops, C.J., Holinski-Feder, E., Ligtenberg, M.J.L., Spruijt, L., Gorgens, H., Stemmler, S., Kloor, M., Dietmaier, W., Schumacher, J., Nothen, Markus, Propping, P., Hoogerbrugge, N., Genetica & Celbiologie, Klinische Genetica, and RS: GROW - School for Oncology and Reproduction

Subjects
Cancer Research, Candidate gene, congenital, hereditary, and neonatal diseases and abnormalities, Hereditary cancer and cancer-related syndromes Genetics and epigenetic pathways of disease [ONCOL 1], HNPCC, Single-nucleotide polymorphism, KAT2A, Biology, MLH1, Immunoenzyme Techniques, Germline mutation, Translational research [ONCOL 3], Proliferating Cell Nuclear Antigen, Genetics, medicine, Estrogen Receptor beta, Humans, PCNA, Genetics and epigenetic pathways of disease Translational research [NCMLS 6], Genetics (clinical), Histone Acetyltransferases, ESR, Hereditary cancer and cancer-related syndromes [ONCOL 1], Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Estrogen Receptor alpha, nutritional and metabolic diseases, medicine.disease, Prognosis, Colorectal Neoplasms, Hereditary Nonpolyposis, Lynch syndrome, digestive system diseases, Association study, MutS Homolog 2 Protein, Mutation analysis, Oncology, MSH2, Case-Control Studies, Mutation, Mutation testing, DNA mismatch repair, Follow-Up Studies, Microsatellite Repeats, MAX
Abstract

Item does not contain fulltext Lynch syndrome (Hereditary non-polyposis colorectal cancer/HNPCC) is a cancer susceptibility syndrome which is caused by germline mutations in DNA mismatch repair (MMR) genes, in particular MLH1 and MSH2. A pathogenic germline mutation in the respective MMR gene is suggested by the finding of a loss of a mismatch repair protein in tumor tissue on immunohistochemical staining combined with an early age of onset and/or the familial occurrence of colorectal cancer. Pathogenic germline mutations are identifiable in around 60% of patients suspected of Lynch syndrome, depending on the familial occurrence. The aim of the present study was to identify novel susceptibility genes for Lynch syndrome. 64 Healthy controls and 64 Lynch syndrome patients with no pathogenic MSH2 mutation but a loss of MSH2 expression in their tumor tissue were screened for rare and disease causing germline mutations in the functional candidate genes ESR1, ESR2, MAX, PCNA, and KAT2A. Thirty variants were identified, and these were then genotyped in an independent sample of 36 mutation negative Lynch syndrome patients and 234 controls. Since a trend towards association was observed for KAT2A, an additional set of 21 tagging SNPs was analyzed at this locus in a final case-control sample of 142 mutation negative Lynch syndrome patients and 298 controls. The mutation analysis failed to reveal any rare disease-causing mutations. No association was found at the single-marker or haplotypic level for any common disease-modifying variant. The present results suggest that neither rare nor common genetic variants in ESR1, ESR2, MAX, PCNA, or KAT2A contribute to the development of Lynch syndrome. 01 maart 2012

Published
2012

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