Your search keyword '"Meinecke, P."' showing total 16 results

1. High frequency of H3 K27M mutations in adult midline gliomas.

Author

Ebrahimi A, Skardelly M, Schuhmann MU, Ebinger M, Reuss D, Neumann M, Tabatabai G, Kohlhof-Meinecke P, and Schittenhelm J

Subjects

Adolescent, Adult, Age Factors, Aged, Aged, 80 and over, Brain Neoplasms pathology, Child, Child, Preschool, DNA Methylation, Female, Glioma pathology, Histones genetics, Humans, Male, Middle Aged, Neoplasm Grading, Young Adult, Brain Neoplasms genetics, Glioma genetics, Mutation

Abstract

Purpose: Diffuse midline gliomas, H3 K27M-mutant were introduced as a new grade IV entity in WHO classification of tumors 2016. These tumors occur often in pediatric patients and show an adverse prognosis with a median survival less than a year. Most of the studies on these tumors, previously known as pediatric diffuse intrinsic pontine glioma, are on pediatric patients and its significance in adult patients is likely underestimated., Methods: We studied 165 cases of brain tumors of midline localization initially diagnosed as diffuse astrocytomas, oligodendrogliomas, pilocytic astrocytomas, supependymomas, ependymomas and medulloblastomas in patients with an age range of 2-85., Results: We identified 41 diffuse midline gliomas according WHO 2016, including 12 pediatric and 29 adult cases, among them two cases with histological features of low grade tumors: pilocytic astrocytoma and subependymoma. 49% (20/41) of the patients were above 30 years old by the first tumor manifestation including 29% (11/41) above 54 that signifies a broader age spectrum as previously reported. Our study confirms that H3 K27M mutations are associated with a poorer prognosis in pediatric patients compared to wild-type tumors, while in adult patients these mutations do not influence the survival significantly. The pattern of tumor growth was different in pediatric compared to adult patients; a diffuse growth along the brain axis was more evident in adult compared to pediatric patients (24% vs. 15%)., Conclusion: H3 K27M mutations are frequent in adult midline gliomas and have a prognostic role similar to H3 K27M wild-type high-grade tumors.

Published

2019

2. Microcephalic osteodysplastic primordial dwarfism type I with biallelic mutations in the RNU4ATAC gene.

Author

Nagy R, Wang H, Albrecht B, Wieczorek D, Gillessen-Kaesbach G, Haan E, Meinecke P, de la Chapelle A, and Westman JA

Subjects

Brain pathology, Dwarfism diagnosis, Facies, Female, Fetal Growth Retardation diagnosis, Humans, Infant, Life Expectancy, Magnetic Resonance Imaging, Male, Microcephaly diagnosis, Osteochondrodysplasias diagnosis, Phenotype, Alleles, Dwarfism genetics, Fetal Growth Retardation genetics, Microcephaly genetics, Mutation, Osteochondrodysplasias genetics, RNA, Small Nuclear genetics

Abstract

Microcephalic osteodysplastic primordial dwarfism type I (MOPD I) is a rare autosomal recessive developmental disorder characterized by extreme intrauterine growth retardation, severe microcephaly, central nervous system abnormalities, dysmorphic facial features, skin abnormalities, skeletal changes, limb deformations, and early death. Recently, mutations in the RNU4ATAC gene, which encodes U4atac, a small nuclear RNA that is a crucial component of the minor spliceosome, were found to cause MOPD I. MOPD I is the first disease known to be associated with a defect in small nuclear RNAs. We describe here the clinical and molecular data for 17 cases of MOPD I, including 15 previously unreported cases, all carrying biallelic mutations in the RNU4ATAC gene., (© 2011 John Wiley & Sons A/S.)

Published

2012

3. Identity-by-descent filtering of exome sequence data identifies PIGV mutations in hyperphosphatasia mental retardation syndrome.

Author

Krawitz PM, Schweiger MR, Rödelsperger C, Marcelis C, Kölsch U, Meisel C, Stephani F, Kinoshita T, Murakami Y, Bauer S, Isau M, Fischer A, Dahl A, Kerick M, Hecht J, Köhler S, Jäger M, Grünhagen J, de Condor BJ, Doelken S, Brunner HG, Meinecke P, Passarge E, Thompson MD, Cole DE, Horn D, Roscioli T, Mundlos S, and Robinson PN

Subjects

Adolescent, Animals, CHO Cells, Child, Preschool, Cricetinae, Cricetulus, Databases, Genetic, Family Health, Female, Glycosylphosphatidylinositols metabolism, Humans, Infant, Male, Open Reading Frames genetics, Syndrome, Transfection, Exons genetics, Genetic Predisposition to Disease, Hyperphosphatemia genetics, Intellectual Disability genetics, Mannosyltransferases genetics, Mutation genetics

Abstract

Hyperphosphatasia mental retardation (HPMR) syndrome is an autosomal recessive form of mental retardation with distinct facial features and elevated serum alkaline phosphatase. We performed whole-exome sequencing in three siblings of a nonconsanguineous union with HPMR and performed computational inference of regions identical by descent in all siblings to establish PIGV, encoding a member of the GPI-anchor biosynthesis pathway, as the gene mutated in HPMR. We identified homozygous or compound heterozygous mutations in PIGV in three additional families.

Published

2010

4. Mutations in the pericentrin (PCNT) gene cause primordial dwarfism.

Author

Rauch A, Thiel CT, Schindler D, Wick U, Crow YJ, Ekici AB, van Essen AJ, Goecke TO, Al-Gazali L, Chrzanowska KH, Zweier C, Brunner HG, Becker K, Curry CJ, Dallapiccola B, Devriendt K, Dörfler A, Kinning E, Megarbane A, Meinecke P, Semple RK, Spranger S, Toutain A, Trembath RC, Voss E, Wilson L, Hennekam R, de Zegher F, Dörr HG, and Reis A

Subjects

Antigens metabolism, Apoptosis, Cell Line, Centrosome physiology, Dwarfism pathology, Dwarfism physiopathology, Female, Fibroblasts cytology, Humans, Lod Score, Lymphocytes metabolism, Male, Microcephaly pathology, Microcephaly physiopathology, Mitosis, Pedigree, RNA, Messenger genetics, RNA, Messenger metabolism, Spindle Apparatus physiology, Spindle Apparatus ultrastructure, Syndrome, Antigens genetics, Antigens physiology, Dwarfism genetics, Microcephaly genetics, Mutation

Abstract

Fundamental processes influencing human growth can be revealed by studying extreme short stature. Using genetic linkage analysis, we find that biallelic loss-of-function mutations in the centrosomal pericentrin (PCNT) gene on chromosome 21q22.3 cause microcephalic osteodysplastic primordial dwarfism type II (MOPD II) in 25 patients. Adults with this rare inherited condition have an average height of 100 centimeters and a brain size comparable to that of a 3-month-old baby, but are of near-normal intelligence. Absence of PCNT results in disorganized mitotic spindles and missegregation of chromosomes. Mutations in related genes are known to cause primary microcephaly (MCPH1, CDK5RAP2, ASPM, and CENPJ).

Published

2008

5. Mutation and phenotypic spectrum in patients with cardio-facio-cutaneous and Costello syndrome.

Author

Schulz AL, Albrecht B, Arici C, van der Burgt I, Buske A, Gillessen-Kaesbach G, Heller R, Horn D, Hübner CA, Korenke GC, König R, Kress W, Krüger G, Meinecke P, Mücke J, Plecko B, Rossier E, Schinzel A, Schulze A, Seemanova E, Seidel H, Spranger S, Tuysuz B, Uhrig S, Wieczorek D, Kutsche K, and Zenker M

Subjects

Adult, Child, DNA Mutational Analysis, Developmental Disabilities, Humans, Intellectual Disability, MAP Kinase Kinase 1 genetics, MAP Kinase Kinase 2 genetics, Phenotype, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins B-raf genetics, Proto-Oncogene Proteins p21(ras), Syndrome, ras Proteins genetics, Abnormalities, Multiple genetics, Facies, Heart Defects, Congenital genetics, Mutation, Skin Abnormalities genetics

Abstract

Cardio-facio-cutaneous (CFC) and Costello syndrome (CS) are congenital disorders with a significant clinical overlap. The recent discovery of heterozygous mutations in genes encoding components of the RAS-RAF-MAPK pathway in both CFC and CS suggested a similar underlying pathogenesis of these two disorders. While CFC is heterogeneous with mutations in BRAF, MAP2K1, MAP2K2 and KRAS, HRAS alterations are almost exclusively associated with CS. We carried out a comprehensive mutation analysis in 51 CFC-affected patients and 31 individuals with CS. Twelve different BRAF alterations were found in twenty-four patients with CFC (47.0%), two MAP2K1 mutations in five (9.8%) and two MAP2K2 sequence variations in three CFC-affected individuals (5.9%), whereas three patients had a KRAS alteration (5.9%). We identified four different missense mutations of HRAS in twenty-eight cases with CS (90.3%), while KRAS mutations were detected in two infants with a phenotype meeting criteria for CS (6.5%). In 14 informative families, we traced the parental origin of HRAS alterations and demonstrated inheritance of the mutated allele exclusively from the father, further confirming a paternal bias in the parental origin of HRAS mutations in CS. Careful clinical evaluation of patients with BRAF and MAP2K1/2 alterations revealed the presence of slight phenotypic differences regarding craniofacial features in MAP2K1- and MAP2K2-mutation positive individuals, suggesting possible genotype-phenotype correlations.

Published

2008

6. Location and type of mutation in the LIS1 gene do not predict phenotypic severity.

Author

Uyanik G, Morris-Rosendahl DJ, Stiegler J, Klapecki J, Gross C, Berman Y, Martin P, Dey L, Spranger S, Korenke GC, Schreyer I, Hertzberg C, Neumann TE, Burkart P, Spaich C, Meng M, Holthausen H, Adès L, Seidel J, Mangold E, Buyse G, Meinecke P, Schara U, Zeschnigk C, Muller D, Helland G, Schulze B, Wright ML, Kortge-Jung S, Hehr A, Bogdahn U, Schuierer G, Kohlhase J, Aigner L, Wolff G, Hehr U, and Winkler J

Subjects

Adolescent, Adult, Cell Movement genetics, Cerebellum abnormalities, Cerebral Cortex metabolism, Cerebral Cortex physiopathology, Child, Child, Preschool, Choristoma genetics, Choristoma metabolism, DNA Mutational Analysis, Female, Genetic Markers genetics, Genetic Testing, Genotype, Humans, Infant, Male, Nervous System Malformations metabolism, Nervous System Malformations physiopathology, Penetrance, Phenotype, 1-Alkyl-2-acetylglycerophosphocholine Esterase genetics, Cerebral Cortex abnormalities, Genetic Predisposition to Disease genetics, Microtubule-Associated Proteins genetics, Mutation genetics, Nervous System Malformations genetics

Abstract

Background: Lissencephaly is a neuronal migration disorder leading to absent or reduced gyration and a broadened but poorly organized cortex. The most common form of lissencephaly is isolated, referred as classic or type 1 lissencephaly. Type 1 lissencephaly is mostly associated with a heterozygous deletion of the entire LIS1 gene, whereas intragenic heterozygous LIS1 mutations or hemizygous DCX mutations in males are less common., Methods: Eighteen unrelated patients with type 1 lissencephaly were clinically and genetically assessed. In addition, patients with subcortical band heterotopia (n = 1) or lissencephaly with cerebellar hypoplasia (n = 2) were included., Results: Fourteen new and seven previously described LIS1 mutations were identified. We observed nine truncating mutations (nonsense, n = 2; frameshift, n = 7), six splice site mutations, five missense mutations, and one in-frame deletion. Somatic mosaicism was assumed in three patients with partial subcortical band heterotopia in the occipital-parietal lobes or mild pachygyria. We report three mutations in exon 11, including a frameshift which extends the LIS1 protein, leading to type 1 lissencephaly and illustrating the functional importance of the WD domains at the C terminus. Furthermore, we present two patients with novel LIS1 mutations in exon 10 associated with lissencephaly with cerebellar hypoplasia type a., Conclusion: In contrast to previous reports, our data suggest that neither type nor position of intragenic mutations in the LIS1 gene allows an unambiguous prediction of the phenotypic severity. Furthermore, patients presenting with mild cerebral malformations such as subcortical band heterotopia or cerebellar hypoplasia should be considered for genetic analysis of the LIS1 gene.

Published

2007

7. Mutations in STRA6 cause a broad spectrum of malformations including anophthalmia, congenital heart defects, diaphragmatic hernia, alveolar capillary dysplasia, lung hypoplasia, and mental retardation.

Author

Pasutto F, Sticht H, Hammersen G, Gillessen-Kaesbach G, Fitzpatrick DR, Nürnberg G, Brasch F, Schirmer-Zimmermann H, Tolmie JL, Chitayat D, Houge G, Fernández-Martínez L, Keating S, Mortier G, Hennekam RC, von der Wense A, Slavotinek A, Meinecke P, Bitoun P, Becker C, Nürnberg P, Reis A, and Rauch A

Subjects

Adolescent, Adult, Amino Acid Sequence, Anophthalmos genetics, Capillaries abnormalities, Consanguinity, Female, Heart Defects, Congenital genetics, Hernia, Diaphragmatic genetics, Humans, Infant, Infant, Newborn, Intellectual Disability genetics, Lung pathology, Male, Membrane Proteins metabolism, Molecular Sequence Data, Pedigree, Phosphorylation, Pulmonary Alveoli blood supply, Sequence Homology, Amino Acid, Abnormalities, Multiple genetics, Lung abnormalities, Membrane Proteins genetics, Mutation genetics, Receptors, Cell Surface genetics

Abstract

We observed two unrelated consanguineous families with malformation syndromes sharing anophthalmia and distinct eyebrows as common signs, but differing for alveolar capillary dysplasia or complex congenital heart defect in one and diaphragmatic hernia in the other family. Homozygosity mapping revealed linkage to a common locus on chromosome 15, and pathogenic homozygous mutations were identified in STRA6, a member of a large group of "stimulated by retinoic acid" genes encoding novel transmembrane proteins, transcription factors, and secreted signaling molecules or proteins of largely unknown function. Subsequently, homozygous STRA6 mutations were also demonstrated in 3 of 13 patients chosen on the basis of significant phenotypic overlap to the original cases. While a homozygous deletion generating a premature stop codon (p.G50AfsX22) led to absence of the immunoreactive protein in patient's fibroblast culture, structural analysis of three missense mutations (P90L, P293L, and T321P) suggested significant effects on the geometry of the loops connecting the transmembrane helices of STRA6. Two further variations in the C-terminus (T644M and R655C) alter specific functional sites, an SH2-binding motif and a phosphorylation site, respectively. STRA6 mutations thus define a pleiotropic malformation syndrome representing the first human phenotype associated with mutations in a gene from the "STRA" group.

Published

2007

8. Clinical and mutational spectrum of Mowat-Wilson syndrome.

Author

Zweier C, Thiel CT, Dufke A, Crow YJ, Meinecke P, Suri M, Ala-Mello S, Beemer F, Bernasconi S, Bianchi P, Bier A, Devriendt K, Dimitrov B, Firth H, Gallagher RC, Garavelli L, Gillessen-Kaesbach G, Hudgins L, Kääriäinen H, Karstens S, Krantz I, Mannhardt A, Medne L, Mücke J, Kibaek M, Krogh LN, Peippo M, Rittinger O, Schulz S, Schelley SL, Temple IK, Dennis NR, Van der Knaap MS, Wheeler P, Yerushalmi B, Zenker M, Seidel H, Lachmeijer A, Prescott T, Kraus C, Lowry RB, and Rauch A

Subjects

Adolescent, Adult, Base Sequence, Child, Child, Preschool, Codon, Terminator genetics, DNA genetics, DNA Mutational Analysis, Female, Genotype, Humans, Infant, Male, Molecular Sequence Data, Phenotype, RNA Splicing, Reverse Transcriptase Polymerase Chain Reaction, Sequence Deletion, Syndrome, Zinc Finger E-box Binding Homeobox 2, Abnormalities, Multiple genetics, Homeodomain Proteins genetics, Intellectual Disability genetics, Mutation, Repressor Proteins genetics

Abstract

Mowat-Wilson Syndrome is a recently delineated mental retardation syndrome usually associated with multiple malformations and a recognizable facial phenotype caused by defects of the transcriptional repressor ZFHX1B. To address the question of clinical and mutational variability, we analysed a large number of patients with suspected Mowat-Wilson Syndrome (MWS). Without prior knowledge of their mutational status, 70 patients were classified into "typical MWS", "ambiguous" and "atypical" groups according to their facial phenotype. Using FISH, qPCR and sequencing, ZFHX1B deletions, splice site or truncating mutations were detected in all 28 patients classified as typical MWS. No ZFHX1B defect was apparent in the remaining 15 cases with ambiguous facial features or in the 27 atypical patients. Genotype-phenotype analysis confirmed that ZFHX1B deletions and stop mutations result in a recognizable facial dysmorphism with associated severe mental retardation and variable malformations such as Hirschsprung disease and congenital heart defects. Our findings indicate that structural eye anomalies such as microphthalmia should be considered as part of the MWS spectrum. We also show that agenesis of the corpus callosum and urogenital anomalies (especially hypospadias) are significant positive predictors of a ZFHX1B defect. Based on our observation of affected siblings and the number of MWS cases previously reported, we suggest a recurrence risk of around 1%. The lack of missense mutations in MWS and MWS-like patients suggests there may be other, as yet unrecognized phenotypes, associated with missense mutations of this transcription factor.

Published

2005

9. Mild phenotypes in a series of patients with Opitz GBBB syndrome with MID1 mutations.

Author

So J, Suckow V, Kijas Z, Kalscheuer V, Moser B, Winter J, Baars M, Firth H, Lunt P, Hamel B, Meinecke P, Moraine C, Odent S, Schinzel A, van der Smagt JJ, Devriendt K, Albrecht B, Gillessen-Kaesbach G, van der Burgt I, Petrij F, Faivre L, McGaughran J, McKenzie F, Opitz JM, Cox T, and Schweiger S

Subjects

Exons genetics, Family Health, Female, Genetic Diseases, X-Linked genetics, Humans, Male, Pedigree, Phenotype, Smith-Lemli-Opitz Syndrome pathology, Ubiquitin-Protein Ligases, Microtubule Proteins genetics, Mutation, Nuclear Proteins genetics, Smith-Lemli-Opitz Syndrome genetics, Transcription Factors genetics

Abstract

Opitz syndrome (OS; MIM 145410 and MIM 300000) is a congenital midline malformation syndrome characterized by hypertelorism, hypospadias, cleft lip/palate, laryngotracheoesophageal (LTE) abnormalities, imperforate anus, developmental delay, and cardiac defects. The X-linked form (XLOS) is caused by mutations in the MID1 gene, which encodes a microtubule-associated RBCC protein. In this study, phenotypic manifestations of patients with and without MID1 mutations were compared to determine genotype-phenotype correlations. We detected 10 novel mutations, 5 in familial cases, 2 in sporadic cases, and 3 in families for whom it was not clear if they were familial or sporadic. The genotype and phenotype was compared for these 10 families, clinically diagnosed OS patients found not to have MID1 mutations, and 4 families in whom we have previously reported MID1 mutations. This combined data set includes clinical and mutation data on 70 patients. The XLOS patients with MID1 mutations were less severely affected than patients with MID1 mutations reported in previous studies, particularly in functionally significant neurologic, LTE, anal, and cardiac abnormalities. Minor anomalies were more prevalent in patients with MID1 mutations compared to those without mutations in this study. Female MID1 mutation carriers had milder phenotypes compared to male MID1 mutation carriers, with the most common manifestation being hypertelorism in both sexes. Most of the anomalies found in the patients of the present study do not correlate with the MID1 mutation type, with the possible exception of LTE malformations. This study demonstrates the wide spectrum of severity and manifestations of OS. It also shows that XLOS patients with MID1 mutations may be less severely affected than indicated in prior reports., ((c) 2004 Wiley-Liss, Inc.)

Published

2005

10. Mutations in NSD1 are responsible for Sotos syndrome, but are not a frequent finding in other overgrowth phenotypes.

Author

Türkmen S, Gillessen-Kaesbach G, Meinecke P, Albrecht B, Neumann LM, Hesse V, Palanduz S, Balg S, Majewski F, Fuchs S, Zschieschang P, Greiwe M, Mennicke K, Kreuz FR, Dehmel HJ, Rodeck B, Kunze J, Tinschert S, Mundlos S, and Horn D

Subjects

Adult, Child, Child, Preschool, Chromosome Deletion, DNA Mutational Analysis, Female, Histone Methyltransferases, Histone-Lysine N-Methyltransferase, Humans, Infant, Infant, Newborn, Male, Pedigree, Phenotype, Polymorphism, Genetic, Syndrome, Carrier Proteins genetics, Craniofacial Abnormalities genetics, Developmental Disabilities genetics, Growth Disorders genetics, Intellectual Disability genetics, Intracellular Signaling Peptides and Proteins, Mutation, Nuclear Proteins genetics

Abstract

Recently, deletions encompassing the nuclear receptor binding SET-Domain 1 (NSD1) gene have been described as the major cause of Japanese patients with the Sotos syndrome, whereas point mutations have been identified in the majority of European Sotos syndrome patients. In order to investigate a possible phenotype-genotype correlation and to further define the predictive value of NSD1 mutations, we performed mutational analysis of the NSD1 gene in 20 patients and one familial case with Sotos syndrome, five patients with Weaver syndrome, six patients with unclassified overgrowth/mental retardation, and six patients with macrocephaly/mental retardation. We were able to identify mutations within the NSD1 gene in 18 patients and the familial case with Sotos syndrome (90%). The mutations (six nonsense, eight frame shifts, three splice site, one missense, one in-frame deletion) are expected to result in an impairment of NSD1 function. The best correlation between clinical assessment and molecular results was obtained for the Sotos facial gestalt in conjunction with overgrowth, macrocephaly, and developmental delay. In contrast to the high mutation detection rate in Sotos syndrome, none of the patients with Weaver syndrome, unclassified overgrowth/mental retardation and macrocephaly/mental retardation, harbored NSD1 mutations. We tested for large deletions by FISH analysis but were not able to identify any deletion cases. The results indicate that the great majority of patients with Sotos syndrome are caused by mutations in NSD1. Deletions covering the NSD1 locus were not found in the patients analyzed here.

Published

2003

11. Genotypic and phenotypic spectrum in tricho-rhino-phalangeal syndrome types I and III.

Author

Lüdecke HJ, Schaper J, Meinecke P, Momeni P, Gross S, von Holtum D, Hirche H, Abramowicz MJ, Albrecht B, Apacik C, Christen HJ, Claussen U, Devriendt K, Fastnacht E, Forderer A, Friedrich U, Goodship TH, Greiwe M, Hamm H, Hennekam RC, Hinkel GK, Hoeltzenbein M, Kayserili H, Majewski F, Mathieu M, McLeod R, Midro AT, Moog U, Nagai T, Niikawa N, Orstavik KH, Plöchl E, Seitz C, Schmidtke J, Tranebjaerg L, Tsukahara M, Wittwer B, Zabel B, Gillessen-Kaesbach G, and Horsthemke B

Subjects

Adolescent, Adult, Amino Acid Sequence, Anthropometry, Base Sequence, Body Height, Child, Child, Preschool, DNA Mutational Analysis, DNA-Binding Proteins metabolism, Erythroid-Specific DNA-Binding Factors, Exons genetics, Female, Genotype, Humans, Infant, Limb Deformities, Congenital diagnostic imaging, Limb Deformities, Congenital physiopathology, Male, Middle Aged, Molecular Sequence Data, Osteochondrodysplasias diagnostic imaging, Osteochondrodysplasias pathology, Pedigree, Phenotype, Polymorphism, Single Nucleotide genetics, Radiography, Syndrome, Transcription Factors metabolism, Zinc Fingers genetics, Chromosomes, Human, Pair 8 genetics, Limb Deformities, Congenital genetics, Limb Deformities, Congenital pathology, Mutation genetics, Osteochondrodysplasias classification, Osteochondrodysplasias genetics

Abstract

Tricho-rhino-phalangeal syndrome (TRPS) is characterized by craniofacial and skeletal abnormalities. Three subtypes have been described: TRPS I, caused by mutations in the TRPS1 gene on chromosome 8; TRPS II, a microdeletion syndrome affecting the TRPS1 and EXT1 genes; and TRPS III, a form with severe brachydactyly, due to short metacarpals, and severe short stature, but without exostoses. To investigate whether TRPS III is caused by TRPS1 mutations and to establish a genotype-phenotype correlation in TRPS, we performed extensive mutation analysis and evaluated the height and degree of brachydactyly in patients with TRPS I or TRPS III. We found 35 different mutations in 44 of 51 unrelated patients. The detection rate (86%) indicates that TRPS1 is the major locus for TRPS I and TRPS III. We did not find any mutation in the parents of sporadic patients or in apparently healthy relatives of familial patients, indicating complete penetrance of TRPS1 mutations. Evaluation of skeletal abnormalities of patients with TRPS1 mutations revealed a wide clinical spectrum. The phenotype was variable in unrelated, age- and sex-matched patients with identical mutations, as well as in families. Four of the five missense mutations alter the GATA DNA-binding zinc finger, and six of the seven unrelated patients with these mutations may be classified as having TRPS III. Our data indicate that TRPS III is at the severe end of the TRPS spectrum and that it is most often caused by a specific class of mutations in the TRPS1 gene.

Published

2001

12. Distinct mutations in the receptor tyrosine kinase gene ROR2 cause brachydactyly type B.

Author

Schwabe GC, Tinschert S, Buschow C, Meinecke P, Wolff G, Gillessen-Kaesbach G, Oldridge M, Wilkie AO, Kömec R, and Mundlos S

Subjects

Amino Acid Sequence, Base Sequence, Codon, Nonsense genetics, Consanguinity, DNA Mutational Analysis, Exons genetics, Female, Fingers physiopathology, Frameshift Mutation genetics, Genotype, Hand Deformities, Congenital classification, Hand Deformities, Congenital physiopathology, Humans, Introns genetics, Male, Molecular Sequence Data, Pedigree, Phenotype, Protein Structure, Tertiary, RNA Splice Sites genetics, Receptor Tyrosine Kinase-like Orphan Receptors, Receptors, Cell Surface chemistry, Syndrome, Fingers abnormalities, Hand Deformities, Congenital genetics, Mutation genetics, Receptor Protein-Tyrosine Kinases genetics, Receptors, Cell Surface genetics

Abstract

Brachydactyly type B (BDB) is an autosomal dominant skeletal disorder characterized by hypoplasia/aplasia of distal phalanges and nails. Recently, heterozygous mutations of the orphan receptor tyrosine kinase (TK) ROR2, located within a distinct segment directly after the TK domain, have been shown to be responsible for BDB. We report four novel mutations in ROR2 (two frameshifts, one splice mutation, and one nonsense mutation) in five families with BDB. The mutations predict truncation of the protein within two distinct regions immediately before and after the TK domain, resulting in a complete or partial loss of the intracellular portion of the protein. Patients affected with the distal mutations have a more severe phenotype than do those with the proximal mutation. Our analysis includes the first description of homozygous BDB in an individual with a 5-bp deletion proximal to the TK domain. His phenotype resembles an extreme form of brachydactyly, with extensive hypoplasia of the phalanges and metacarpals/metatarsals and absence of nails. In addition, he has vertebral anomalies, brachymelia of the arms, and a ventricular septal defect-features that are reminiscent of Robinow syndrome, which has also been shown to be caused by mutations in ROR2. The BDB phenotype, as well as the location and the nature of the BDB mutations, suggests a specific mutational effect that cannot be explained by simple haploinsufficiency and that is distinct from that in Robinow syndrome.

Published

2000

13. SOX9 mutation in a previously published case of campomelic dysplasia without overt campomelia.

Author

Friedrich U, Schaefer E, Meinecke P, and Scherer G

Subjects

Humans, SOX9 Transcription Factor, High Mobility Group Proteins genetics, Mutation, Osteochondrodysplasias genetics, Transcription Factors genetics

Abstract

An SOX9 mutation in a previously published case of campomelic dysplasia is described. This case did not have overt campomelia of the femora or tibiae although campomelic dysplasia has subsequently been confirmed by gene analysis.

Published

2000

14. Mutations in a new gene, encoding a zinc-finger protein, cause tricho-rhino-phalangeal syndrome type I.

Author

Momeni P, Glöckner G, Schmidt O, von Holtum D, Albrecht B, Gillessen-Kaesbach G, Hennekam R, Meinecke P, Zabel B, Rosenthal A, Horsthemke B, and Lüdecke HJ

Subjects

Blotting, Northern, Chromosome Mapping, Chromosomes, Human, Pair 8, DNA, Complementary, Female, Humans, Male, Molecular Sequence Data, Open Reading Frames, Pedigree, Langer-Giedion Syndrome genetics, Mutation, Zinc Fingers genetics

Abstract

Tricho-rhino-phalangeal syndrome type I (TRPS I, MIM 190350) is a malformation syndrome characterized by craniofacial and skeletal abnormalities and is inherited in an autosomal dominant manner. TRPS I patients have sparse scalp hair, a bulbous tip of the nose, a long flat philtrum, a thin upper vermilion border and protruding ears. Skeletal abnormalities include cone-shaped epiphyses at the phalanges, hip malformations and short stature. We assigned TRPS1 to human chromosome 8q24. It maps proximal of EXT1, which is affected in a subgroup of patients with multiple cartilaginous exostoses and deleted in all patients with TRPS type II (TRPS II, or Langer-Giedion syndrome, MIM 150230; ref.2-5). We have positionally cloned a gene that spans the chromosomal breakpoint of two patients with TRPS I and is deleted in five patients with TRPS I and an interstitial deletion. Northern-blot analyses revealed transcripts of 7 and 10.5 kb. TRPS1has seven exons and an ORF of 3,843 bp. The predicted protein sequence has two potential nuclear localization signals and an unusual combination of different zinc-finger motifs, including IKAROS-like and GATA-binding sequences. We identified six different nonsense mutations in ten unrelated patients. Our findings suggest that haploinsufficiency for this putative transcription factor causes TRPS I.

Published

2000

15. Point mutations throughout the GLI3 gene cause Greig cephalopolysyndactyly syndrome.

Author

Kalff-Suske M, Wild A, Topp J, Wessling M, Jacobsen EM, Bornholdt D, Engel H, Heuer H, Aalfs CM, Ausems MG, Barone R, Herzog A, Heutink P, Homfray T, Gillessen-Kaesbach G, König R, Kunze J, Meinecke P, Müller D, Rizzo R, Strenge S, Superti-Furga A, and Grzeschik KH

Subjects

Animals, DNA Mutational Analysis, Drosophila, Humans, Kruppel-Like Transcription Factors, Recombinant Fusion Proteins, Sequence Deletion, Syndrome, Transcriptional Activation, Transfection, Tumor Cells, Cultured, Zinc Finger Protein Gli3, Zinc Fingers genetics, Craniofacial Abnormalities genetics, DNA-Binding Proteins genetics, Limb Deformities, Congenital genetics, Mutation, Nerve Tissue Proteins, Repressor Proteins, Transcription Factors genetics, Xenopus Proteins

Abstract

Greig cephalopolysyndactyly syndrome, characterized by craniofacial and limb anomalies (GCPS; MIM 175700), previously has been demonstrated to be associated with translocations as well as point mutations affecting one allele of the zinc finger gene GLI3. In addition to GCPS, Pallister-Hall syndrome (PHS; MIM 146510) and post-axial polydactyly type A (PAP-A; MIM 174200), two other disorders of human development, are caused by GLI3 mutations. In order to gain more insight into the mutational spectrum associated with a single phenotype, we report here the extension of the GLI3 mutation analysis to 24 new GCPS cases. We report the identification of 15 novel mutations present in one of the patient's GLI3 alleles. The mutations map throughout the coding gene regions. The majority are truncating mutations (nine of 15) that engender prematurely terminated protein products mostly but not exclusively N-terminally to or within the central region encoding the DNA-binding domain. Two missense and two splicing mutations mapping within the zinc finger motifs presumably also interfere with DNA binding. The five mutations identified within the protein regions C-terminal to the zinc fingers putatively affect additional functional properties of GLI3. In cell transfection experiments using fusions of the DNA-binding domain of yeast GAL4 to different segments of GLI3, transactivating capacity was assigned to two adjacent independent domains (TA(1)and TA(2)) in the C-terminal third of GLI3. Since these are the only functional domains affected by three C-terminally truncating mutations, we postulate that GCPS may be due either to haploinsufficiency resulting from the complete loss of one gene copy or to functional haploinsufficiency related to compromised properties of this transcription factor such as DNA binding and transactivation.

Published

1999

16. Mutations of the Mitochondrial Holocytochrome c–Type Synthase in X-Linked Dominant Microphthalmia with Linear Skin Defects Syndrome

Author

Isabella Wimplinger, Manuela Morleo, Brunella Franco, Andrea Ballabio, Georg Rosenberger, Daniela Iaconis, Andreas Gal, Ulrike Orth, Israela Lerer, Peter Meinecke, Kerstin Kutsche, Wimplinger, I, Morleo, M, Rosenberger, G, Iaconis, D, Orth, U, Meinecke, P, Lerer, I, Ballabio, Andrea, Gal, A, Franco, Brunella, Kutsche, K., Ballabio, A, Franco, B, and Kutsche, K

Subjects

Male, Nonsense mutation, Mutant, Molecular Sequence Data, Lyases, CHO Cells, Mitochondrion, Biology, medicine.disease_cause, Microphthalmia, Polymorphism, Single Nucleotide, Article, Mutant protein, Genes, X-Linked, X Chromosome Inactivation, Cricetinae, medicine, Genetics, Missense mutation, Animals, Humans, Microphthalmos, Genetics(clinical), Amino Acid Sequence, Child, Genetics (clinical), Genes, Dominant, Sequence Deletion, Mutation, Base Sequence, Genetic Complementation Test, Genetic Diseases, X-Linked, DNA, Syndrome, HCCS, medicine.disease, Molecular biology, Mitochondria, Pedigree, Phenotype, Haplotypes, Child, Preschool, Skin Abnormalities, Female, Holoenzymes

Abstract

The microphthalmia with linear skin defects syndrome (MLS, or MIDAS) is an X-linked dominant male-lethal disorder almost invariably associated with segmental monosomy of the Xp22 region. In two female patients, from two families, with MLS and a normal karyotype, we identified heterozygous de novo point mutations--a missense mutation (p.R217C) and a nonsense mutation (p.R197X)--in the HCCS gene. HCCS encodes the mitochondrial holocytochrome c-type synthase that functions as heme lyase by covalently adding the prosthetic heme group to both apocytochrome c and c(1). We investigated a third family, displaying phenotypic variability, in which the mother and two of her daughters carry an 8.6-kb submicroscopic deletion encompassing part of the HCCS gene. Functional analysis demonstrates that both mutant proteins (R217C and Delta 197-268) were unable to complement a Saccharomyces cerevisiae mutant deficient for the HCCS orthologue Cyc3p, in contrast to wild-type HCCS. Moreover, ectopically expressed HCCS wild-type and the R217C mutant protein are targeted to mitochondria in CHO-K1 cells, whereas the C-terminal-truncated Delta 197-268 mutant failed to be sorted to mitochondria. Cytochrome c, the final product of holocytochrome c-type synthase activity, is implicated in both oxidative phosphorylation (OXPHOS) and apoptosis. We hypothesize that the inability of HCCS-deficient cells to undergo cytochrome c-mediated apoptosis may push cell death toward necrosis that gives rise to severe deterioration of the affected tissues. In summary, we suggest that disturbance of both OXPHOS and the balance between apoptosis and necrosis, as well as the X-inactivation pattern, may contribute to the variable phenotype observed in patients with MLS.

Published

2006