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12 results on '"Bruggenwirth, H.T."'

1. P348: De novo missense variants in ZBTB47 cause a neurodevelopmental phenotype of developmental delays, seizures, and possible movement abnormalities

Author

Ward, Scott, primary, Burrage, Lindsay, additional, Rosenfeld, Jill, additional, Bacino, Carlos, additional, Lee, Brendan, additional, Craigen, William, additional, Emrick, Lisa, additional, Fisher, Kristen, additional, Wadley, Alexandrea, additional, Tsai, Chun-Hui, additional, Benke, Paul, additional, Sacoto, Maria Guillen, additional, Glaser, Kimberly, additional, Murdock, David, additional, Rohena, Luis, additional, Diderich, K.E.M., additional, Bruggenwirth, H.T., additional, and Houck, Kimberly, additional

Published
2023
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2. HLA frequencies and associations in cystic fibrosis

Author

Adriaanse, M.P., Vreugdenhil, A.C., Groeneweg, M., Bruggenwirth, H.T., Castelijns, S.J., van der Ent, C.K., Voorter, C.E., Tilanus, M G., Kindergeneeskunde, RS: NUTRIM - R2 - Gut-liver homeostasis, RS: GROW - Oncology, and RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy

Subjects
musculoskeletal diseases, HLA-DRB1 chains, cystic fibrosis transmembrane conductance regulator, ADULTS, HLA-DQ alpha-chains, ALLELES, GUIDELINES, DIAGNOSIS, DISEASE, cystic fibrosis, HLA antigens, skin and connective tissue diseases, HLA-DQ beta-chains, POPULATION
Abstract

Cystic fibrosis (CF) is classically attributed to the dysfunction of the single CF transmembrane conductance regulator gene. The incidence of human leukocyte antigen (HLA) polymorphisms in different CF-associated diseases raises the question of an unequal distribution of HLA genotypes in CF. This study aimed to evaluate HLA gene frequencies and possible associations in CF patients compared with a control population. Frequencies of HLA-DRB1, HLA-DQA1 and HLA-DQB1, performed by intermediate resolution typing using Luminex sequence-specific oligonucleotide, and epitope counts were similar in 340 CF patients when compared with 400 control subjects. In conclusion, HLA-DRB1, -DQA1 and -DQB1 do not seem to influence susceptibility to CF. Whether HLA plays a role in the severity of CF disease needs to be investigated.

Published
2014

3. Mutations in a TGF-β Ligand, TGFB3, Cause Syndromic Aortic Aneurysms and Dissections

Author

Bertoli-Avella, A.M., Gillis, E., Morisaki, H., Verhagen, J.M.A., de Graaf, B.M., van de Beek, G., Gallo, E., Kruithof, B.P.T., Venselaar, H., Myers, L.A., Laga, S., Doyle, A.J., Oswald, G., van Cappellen, G.W.A., Yamanaka, I., van der Helm, R.M., Beverloo, B., de Klein, A., Pardo, L., Lammens, M., Evers, C., Devriendt, K., Dumoulein, M., Timmermans, J., Bruggenwirth, H.T., Verheijen, F., Rodrigus, I., Baynam, G., Kempers, M., Saenen, J., Van Craenenbroeck, E.M., Minatoya, K., Matsukawa, R., Tsukube, T., Kubo, N., Hofstra, R., Goumans, M.J., Bekkers, J.A., Roos-Hesselink, J.W., van de Laar, I.M.B.H., Dietz, H.C., Van Laer, L., Morisaki, T., Wessels, M.W., Loeys, B.L., Bertoli-Avella, A.M., Gillis, E., Morisaki, H., Verhagen, J.M.A., de Graaf, B.M., van de Beek, G., Gallo, E., Kruithof, B.P.T., Venselaar, H., Myers, L.A., Laga, S., Doyle, A.J., Oswald, G., van Cappellen, G.W.A., Yamanaka, I., van der Helm, R.M., Beverloo, B., de Klein, A., Pardo, L., Lammens, M., Evers, C., Devriendt, K., Dumoulein, M., Timmermans, J., Bruggenwirth, H.T., Verheijen, F., Rodrigus, I., Baynam, G., Kempers, M., Saenen, J., Van Craenenbroeck, E.M., Minatoya, K., Matsukawa, R., Tsukube, T., Kubo, N., Hofstra, R., Goumans, M.J., Bekkers, J.A., Roos-Hesselink, J.W., van de Laar, I.M.B.H., Dietz, H.C., Van Laer, L., Morisaki, T., Wessels, M.W., and Loeys, B.L.

Abstract

Background Aneurysms affecting the aorta are a common condition associated with high mortality as a result of aortic dissection or rupture. Investigations of the pathogenic mechanisms involved in syndromic types of thoracic aortic aneurysms, such as Marfan and Loeys-Dietz syndromes, have revealed an important contribution of disturbed transforming growth factor (TGF)-β signaling. Objectives This study sought to discover a novel gene causing syndromic aortic aneurysms in order to unravel the underlying pathogenesis. Methods We combined genome-wide linkage analysis, exome sequencing, and candidate gene Sanger sequencing in a total of 470 index cases with thoracic aortic aneurysms. Extensive cardiological examination, including physical examination, electrocardiography, and transthoracic echocardiography was performed. In adults, imaging of the entire aorta using computed tomography or magnetic resonance imaging was done. Results Here, we report on 43 patients from 11 families with syndromic presentations of aortic aneurysms caused by TGFB3 mutations. We demonstrate that TGFB3 mutations are associated with significant cardiovascular involvement, including thoracic/abdominal aortic aneurysm and dissection, and mitral valve disease. Other systemic features overlap clinically with Loeys-Dietz, Shprintzen-Goldberg, and Marfan syndromes, including cleft palate, bifid uvula, skeletal overgrowth, cervical spine instability and clubfoot deformity. In line with previous observations in aortic wall tissues of patients with mutations in effectors of TGF-β signaling (TGFBR1/2, SMAD3, and TGFB2), we confirm a paradoxical up-regulation of both canonical and noncanonical TGF-β signaling in association with up-regulation of the expression of TGF-β ligands. Conclusions Our findings emphasize the broad clinical variability associated with TGFB3 mutations and highlight the importance of early recognition of the disease because of high cardiovascular risk.

Published
2015

4. Mutations in a TGF-beta ligand, TGFB3, cause syndromic aortic aneurysms and dissections

Author

Bertoli-Avella, A.M., Gillis, E., Morisaki, H., Verhagen, J.M.A., Graaf, B.M. de, Beek, G. van de, Gallo, E., Kruithof, B.P., Venselaar, H., Myers, L.A., Laga, S., Doyle, A.J., Oswald, G., Cappellen, G.W. van, Yamanaka, I., Helm, R.M. van der, Beverloo, B., Klein, A., Pardo, L., Lammens, M., Evers, C., Devriendt, K., Dumoulein, M., Timmermans, J., Bruggenwirth, H.T., Verheijen, F., Rodrigus, I., Baynam, G., Kempers, M., Saenen, J., Craenenbroeck, E.M. Van, Minatoya, K., Matsukawa, R., Tsukube, T., Kubo, N., Hofstra, R., Goumans, M.J., Bekkers, J.A., Roos-Hesselink, J.W., Laar, I.M. van de, Dietz, H.C., Laer, L. Van, Morisaki, T., Wessels, M.W., Loeys, B.L., Bertoli-Avella, A.M., Gillis, E., Morisaki, H., Verhagen, J.M.A., Graaf, B.M. de, Beek, G. van de, Gallo, E., Kruithof, B.P., Venselaar, H., Myers, L.A., Laga, S., Doyle, A.J., Oswald, G., Cappellen, G.W. van, Yamanaka, I., Helm, R.M. van der, Beverloo, B., Klein, A., Pardo, L., Lammens, M., Evers, C., Devriendt, K., Dumoulein, M., Timmermans, J., Bruggenwirth, H.T., Verheijen, F., Rodrigus, I., Baynam, G., Kempers, M., Saenen, J., Craenenbroeck, E.M. Van, Minatoya, K., Matsukawa, R., Tsukube, T., Kubo, N., Hofstra, R., Goumans, M.J., Bekkers, J.A., Roos-Hesselink, J.W., Laar, I.M. van de, Dietz, H.C., Laer, L. Van, Morisaki, T., Wessels, M.W., and Loeys, B.L.

Abstract

Contains fulltext : 153458.pdf (publisher's version ) (Open Access), BACKGROUND: Aneurysms affecting the aorta are a common condition associated with high mortality as a result of aortic dissection or rupture. Investigations of the pathogenic mechanisms involved in syndromic types of thoracic aortic aneurysms, such as Marfan and Loeys-Dietz syndromes, have revealed an important contribution of disturbed transforming growth factor (TGF)-beta signaling. OBJECTIVES: This study sought to discover a novel gene causing syndromic aortic aneurysms in order to unravel the underlying pathogenesis. METHODS: We combined genome-wide linkage analysis, exome sequencing, and candidate gene Sanger sequencing in a total of 470 index cases with thoracic aortic aneurysms. Extensive cardiological examination, including physical examination, electrocardiography, and transthoracic echocardiography was performed. In adults, imaging of the entire aorta using computed tomography or magnetic resonance imaging was done. RESULTS: Here, we report on 43 patients from 11 families with syndromic presentations of aortic aneurysms caused by TGFB3 mutations. We demonstrate that TGFB3 mutations are associated with significant cardiovascular involvement, including thoracic/abdominal aortic aneurysm and dissection, and mitral valve disease. Other systemic features overlap clinically with Loeys-Dietz, Shprintzen-Goldberg, and Marfan syndromes, including cleft palate, bifid uvula, skeletal overgrowth, cervical spine instability and clubfoot deformity. In line with previous observations in aortic wall tissues of patients with mutations in effectors of TGF-beta signaling (TGFBR1/2, SMAD3, and TGFB2), we confirm a paradoxical up-regulation of both canonical and noncanonical TGF-beta signaling in association with up-regulation of the expression of TGF-beta ligands. CONCLUSIONS: Our findings emphasize the broad clinical variability associated with TGFB3 mutations and highlight the importance of early recognition of the disease because of high cardiovascular risk.

Published
2015

5. Familial gigantism caused by an NSD1 mutation

Author

Haelst, M.M. van, Hoogeboom, J.J., Baujat, G., Bruggenwirth, H.T., Laar, I. van de, Coleman, K., Rahman, N., Niermeijer, M.F., Drop, S.L., and Scambler, P.J.

Subjects
Genomic disorders and inherited multi-system disorders [IGMD 3], Genetic defects of metabolism [UMCN 5.1]
Abstract

Contains fulltext : 47843.pdf (Publisher’s version ) (Closed access) A three-generation family with autosomal dominant segregation of a novel NSD1 mutation (6605G --> A, resulting in Cys2202Tyr) is reported. Haploinsufficiency of NSD1 has been identified as the major cause of Sotos syndrome. The overgrowth condition (MIM 117550) is characterized by facial anomalies, macrocephaly, advanced bone age, and learning disabilities. Manifestations in the present family include dramatically increased height, weight, and head circumference together with a long face, large mandible, and large ears, but mental deficiency was absent.

Published
2005

7. Genotype versus phenotype in families with androgen insensitivity syndrome

Author

Boehmer, A.L., Brinkmann, A.O., Bruggenwirth, H.T., Assendelft, C. van, Otten, B.J., Verleun-Mooijman, M.C.T., Niermeijer, M.F., Brunner, H.G., Rouwé, C.W., Waelkens, J.J., Oostdijk, W., Kleijer, W.J., Kwast, T.H. van der, Vroede, M.A. de, and Drop, S.L.

Subjects
Elucidation of hereditary disorders and their molecular diagnosis, Opheldering van erfelijke ziekten en hun moleculaire diagnostiek
Abstract

Item does not contain fulltext Androgen insensitivity syndrome encompasses a wide range of phenotypes, which are caused by numerous different mutations in the AR gene. Detailed information on the genotype/phenotype relationship in androgen insensitivity syndrome is important for sex assignment, treatment of androgen insensitivity syndrome patients, genetic counseling of their families, and insight into the functional domains of the AR. The commonly accepted concept of dependence on fetal androgens of the development of Wolffian ducts was studied in complete androgen insensitivity syndrome (CAIS) patients. In a nationwide survey in The Netherlands, all cases (n = 49) with the presumptive diagnosis androgen insensitivity syndrome known to pediatric endocrinologists and clinical geneticists were studied. After studying the clinical phenotype, mutation analysis and functional analysis of mutant receptors were performed using genital skin fibroblasts and in vitro expression studies. Here we report the findings in families with multiple affected cases. Fifty-nine percent of androgen insensitivity syndrome patients had other affected relatives. A total of 17 families were studied, seven families with CAIS (18 patients), nine families with partial androgen insensitivity (24 patients), and one family with female prepubertal phenotypes (two patients). No phenotypic variation was observed in families with CAIS. However, phenotypic variation was observed in one-third of families with partial androgen insensitivity resulting in different sex of rearing and differences in requirement of reconstructive surgery. Intrafamilial phenotypic variation was observed for mutations R846H, M771I, and deletion of amino acid N682. Four newly identified mutations were found. Follow-up in families with different AR gene mutations provided information on residual androgen action in vivo and the development of the prepubertal and adult phenotype. Patients with a functional complete defective AR had some pubic hair, Tanner stage P2, and vestigial Wolffian duct derivatives despite absence of AR expression. Vaginal length was functional in most but not all CAIS patients. The minimal incidence of androgen insensitivity syndrome in The Netherlands, based on patients with molecular proof of the diagnosis is 1:99,000. Phenotypic variation was absent in families with CAIS, but distinct phenotypic variation was observed relatively frequent in families with partial androgen insensitivity. Molecular observations suggest that phenotypic variation had different etiologies among these families. Sex assignment of patients with partial androgen insensitivity cannot be based on a specific identified AR gene mutation because distinct phenotypic variation in partial androgen insensitivity families is relatively frequent. In genetic counseling of partial androgen insensitivity families, this frequent occurrence of variable expression resulting in differences in sex of rearing and/or requirement of reconstructive surgery is important information. During puberty or normal dose androgen therapy, no or only minimal virilization may occur even in patients with significant (but still deficient) prenatal virilization. Wolffian duct remnants remain detectable but differentiation does not occur in the absence of a functional AR. In many CAIS patients, surgical elongation of the vagina is not indicated.

Published
2001

8. Phenotypic spectrum of the SMAD3-related aneurysms-osteoarthritis syndrome.

Author

Laar, I.M. van de, Linde, D. van der, Oei, E.H., Bos, P.K., Bessems, J.H., Bierma-Zeinstra, S.M., Meer, B.L. van, Pals, G., Oldenburg, R.A., Bekkers, J.A., Moelker, A., Graaf, B.M. de, Matyas, G., Frohn-Mulder, I.M., Timmermans, J., Hilhorst-Hofstee, Y., Cobben, J.M., Bruggenwirth, H.T., Laer, L. van, Loeys, B.L., Backer, J. de, Coucke, P.J., Dietz, H.C., Willems, P.J., Oostra, B.A., Paepe, A. de, Roos-Hesselink, J.W., Bertoli-Avella, A.M., Wessels, M.W., Laar, I.M. van de, Linde, D. van der, Oei, E.H., Bos, P.K., Bessems, J.H., Bierma-Zeinstra, S.M., Meer, B.L. van, Pals, G., Oldenburg, R.A., Bekkers, J.A., Moelker, A., Graaf, B.M. de, Matyas, G., Frohn-Mulder, I.M., Timmermans, J., Hilhorst-Hofstee, Y., Cobben, J.M., Bruggenwirth, H.T., Laer, L. van, Loeys, B.L., Backer, J. de, Coucke, P.J., Dietz, H.C., Willems, P.J., Oostra, B.A., Paepe, A. de, Roos-Hesselink, J.W., Bertoli-Avella, A.M., and Wessels, M.W.

Abstract

1 januari 2012, Item does not contain fulltext, BACKGROUND: Aneurysms-osteoarthritis syndrome (AOS) is a new autosomal dominant syndromic form of thoracic aortic aneurysms and dissections characterised by the presence of arterial aneurysms and tortuosity, mild craniofacial, skeletal and cutaneous anomalies, and early-onset osteoarthritis. AOS is caused by mutations in the SMAD3 gene. METHODS: A cohort of 393 patients with aneurysms without mutation in FBN1, TGFBR1 and TGFBR2 was screened for mutations in SMAD3. The patients originated from The Netherlands, Belgium, Switzerland and USA. The clinical phenotype in a total of 45 patients from eight different AOS families with eight different SMAD3 mutations is described. In all patients with a SMAD3 mutation, clinical records were reviewed and extensive genetic, cardiovascular and orthopaedic examinations were performed. RESULTS: Five novel SMAD3 mutations (one nonsense, two missense and two frame-shift mutations) were identified in five new AOS families. A follow-up description of the three families with a SMAD3 mutation previously described by the authors was included. In the majority of patients, early-onset joint abnormalities, including osteoarthritis and osteochondritis dissecans, were the initial symptom for which medical advice was sought. Cardiovascular abnormalities were present in almost 90% of patients, and involved mainly aortic aneurysms and dissections. Aneurysms and tortuosity were found in the aorta and other arteries throughout the body, including intracranial arteries. Of the patients who first presented with joint abnormalities, 20% died suddenly from aortic dissection. The presence of mild craniofacial abnormalities including hypertelorism and abnormal uvula may aid the recognition of this syndrome. CONCLUSION: The authors provide further insight into the phenotype of AOS with SMAD3 mutations, and present recommendations for a clinical work-up.

Published
2012

9. Mucopolysaccharidosis type IIIA: clinical spectrum and genotype-phenotype correlations.

Author

Valstar, M.J., Neijs, S., Bruggenwirth, H.T., Olmer, R., Ruijter, G.J., Wevers, R.A., Diggelen, O.P. van, Poorthuis, B.J.H.M., Halley, D.J., Wijburg, F.A., Valstar, M.J., Neijs, S., Bruggenwirth, H.T., Olmer, R., Ruijter, G.J., Wevers, R.A., Diggelen, O.P. van, Poorthuis, B.J.H.M., Halley, D.J., and Wijburg, F.A.

Abstract

1 december 2010, Contains fulltext : 89261.pdf (publisher's version ) (Closed access), OBJECTIVE: Mucopolysaccharidosis (MPS) IIIA (Sanfilippo syndrome type A) is a lysosomal storage disorder caused by deficiency of the enzyme sulfamidase. Information on the natural course of MPS IIIA is scarce, but is much needed in view of emerging therapies. METHODS: Clinical history and molecular defects of all 110 MPS IIIA patients identified by enzymatic studies in the Netherlands were collected and included in this study. RESULTS: First clinical signs, mainly consisting of delayed speech development and behavioral problems, were noted between the ages of 1 and 6 years. Other symptoms included sleeping and hearing problems, recurrent upper airway infections, diarrhea, and epilepsy. The clinical course varied remarkably and could be correlated with the molecular defects. The frequent pathogenic mutations p.R245H, p.Q380R, p.S66W, and c.1080delC were associated with the classical severe phenotype. Patients compound heterozygous for the p.S298P mutation in combination with 1 of the mutations associated with the classical severe phenotype had a significantly longer preservation of psychomotor functions and a longer survival. Two patients homozygous for the p.S298P mutation, and 4 patients from 3 families heterozygous for 3 missense variants not reported previously (p.T421R, p.P180L, and p.L12Q), showed a remarkably attenuated phenotype. INTERPRETATION: We report the natural history and mutational analysis in a large unbiased cohort of MPS IIIA patients. We demonstrate that the clinical spectrum of MPS IIIA is much broader than previously reported. A significant genotype-phenotype correlation was established in this cohort.

Published
2010

10. Mucopolysaccharidosis type IIIB may predominantly present with an attenuated clinical phenotype.

Author

Valstar, M.J., Bruggenwirth, H.T., Olmer, R., Wevers, R.A., Verheijen, F.W., Poorthuis, B.J.H.M., Halley, D.J., Wijburg, F.A., Valstar, M.J., Bruggenwirth, H.T., Olmer, R., Wevers, R.A., Verheijen, F.W., Poorthuis, B.J.H.M., Halley, D.J., and Wijburg, F.A.

Abstract

01 december 2010, Contains fulltext : 89262.pdf (publisher's version ) (Closed access), Mucopolysaccharidosis type IIIB (MPS IIIB, Sanfilippo syndrome type B) is a lysosomal storage disorder caused by deficiency of the enzyme N-acetyl-alpha-D-glucosaminidase (NAGLU). Information on the natural course of MPS IIIB is scarce but much needed in view of emerging therapies. To improve knowledge on the natural course, data on all 52 MPS IIIB patients ever identified by enzymatic studies in the Netherlands were gathered. Clinical data on 44 patients could be retrieved. Only a small number (n = 9; 21%) presented with a classical MPS III phenotype; all other patients showed a much more attenuated course of the disease characterized by a significantly slower regression of intellectual and motor abilities. The majority of patients lived well into adulthood. First signs of the disease, usually mild developmental delay, were observed at a median age of 4 years. Subsequently, patients showed a slowing and eventually a stagnation of development. Patients with the attenuated phenotype had a stable intellectual disability for many years. Molecular analysis was performed in 24 index patients. The missense changes p.R643C, p.S612G, p.E634K, and p.L497V were exclusively found in patients with the attenuated phenotype. MPS IIIB comprises a remarkably wide spectrum of disease severity, and an unselected cohort including all Dutch patients showed a large proportion (79%) with an attenuated phenotype. MPS IIIB must be considered in patients with a developmental delay, even in the absence of a progressive decline in intellectual abilities. A key feature, necessitating metabolic studies, is the coexistence of behavioral problems.

Published
2010

11. 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

12. Molecular basis of androgen insensivity

Author

Bruggenwirth, H.T., Boehmer, A.L., Verleun-Mooijman, M.C.T., Hoogenboezem, T., Kleijer, W.J., Otten, B.J., Trapman, J., and Brinkmann, A.O.

Subjects
Overig onderzoek afdeling Paediatrics
Abstract

Item does not contain fulltext 7 p.

Published
1996

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