Your search keyword '"Brunner, H. G."' showing total 227 results

201. Deafness, sensory neuropathy, and ovarian dysgenesis: a new syndrome or a broader spectrum of Perrault syndrome?

Author

Linssen WH, Van den Bent MJ, Brunner HG, and Poels PJ

Subjects

Family Health, Female, Humans, Infant, Male, Ovary abnormalities, Syndrome, Abnormalities, Multiple classification, Amelogenesis Imperfecta, Deafness, Hereditary Sensory and Autonomic Neuropathies

Abstract

We report on 3 sibs (2 males and one female) with sensorineural deafness. The presence of ovarian dysgenesis in the girl suggested a diagnosis of Perrault syndrome. In addition our patients have a sensory polyneuropathy and amelogenesis imperfecta. Two of the patients have mild mental retardation, fine choreatic movements, and dyspraxia. It is discussed whether these findings are part of a separate clinical entity or should be included within the spectrum of the Perrault syndrome.

Published

1994

202. Aberrant splicing of the COL4A5 gene in patients with Alport syndrome.

Author

Lemmink HH, Kluijtmans LA, Brunner HG, Schröder CH, Knebelmann B, Jelínková E, van Oost BA, Monnens LA, and Smeets HJ

Subjects

Base Sequence, Collagen biosynthesis, Collagen chemistry, Collagen classification, Exons, Female, Frameshift Mutation, Gene Expression Regulation, Heterozygote, Humans, Introns, Male, Molecular Sequence Data, Polymerase Chain Reaction, X Chromosome, Collagen genetics, Mutation, Nephritis, Hereditary genetics, RNA Splicing

Abstract

A variety of mutations have been identified in the X-linked type IV collagen alpha 5 chain (COL4A5) gene in patients with Alport syndrome. A substantial number of these mutations were predicted to have an effect on RNA splicing. For 4 such mutations in our group of patients the effect of the DNA mutation on the COL4A5 mRNA structure and stability was analysed. An alteration of the invariant splice acceptor site of intron 41 resulted in a shift of the actual splicing to either a cryptic splice site within exon 42 or the normal splice site in the next intron. A single base substitution of the final nucleotide of exon 48 resulted in the removal of the entire exon. Two frameshift mutations, a 10 basepair duplication in exon 49 and a single base deletion in exon 41, were incorporated in the mRNA as such and resulted in a stretch of missense codons terminated by a premature stop codon. Exon skipping was occasionally observed in these samples, but not reproducibly in every experiment. In healthy controls exon skipping was never detected. Analysis of female carriers revealed that in only one case was the stability of the mutated mRNA reduced in comparison with the normal transcript. The extent to which the non-collagenous domain was predicted to be deleted correlated with the severeness of the disease.

Published

1994

203. Biogenic amine metabolite patterns in the urine of monoamine oxidase A-deficient patients. A possible tool for diagnosis.

Author

Abeling NG, van Gennip AH, Overmars H, van Oost BA, and Brunner HG

Subjects

Adult, Female, Genetic Linkage, Heterozygote, Humans, Intellectual Disability etiology, Male, Monoamine Oxidase genetics, Netherlands, Pedigree, X Chromosome, Biogenic Amines urine, Monoamine Oxidase deficiency

Published

1994

204. [An unstable mutation as cause of myotonic dystrophy].

Author

Brunner HG, Höweler CJ, Smeets HJ, and Wieringa B

Subjects

Adolescent, Adult, Aged, Child, Child, Preschool, Female, Humans, Infant, Male, Middle Aged, Myotonic Dystrophy classification, Myotonic Dystrophy diagnosis, Pedigree, Sex Factors, Mutation, Myotonic Dystrophy genetics

Published

1993

205. Influence of sex of the transmitting parent as well as of parental allele size on the CTG expansion in myotonic dystrophy (DM).

Author

Brunner HG, Brüggenwirth HT, Nillesen W, Jansen G, Hamel BC, Hoppe RL, de Die CE, Höweler CJ, van Oost BA, and Wieringa B

Subjects

Adult, Alleles, Female, Heterozygote, Humans, Male, Middle Aged, Parents, Pedigree, Phenotype, Myotonic Dystrophy genetics, Repetitive Sequences, Nucleic Acid, Sex Characteristics

Abstract

In patients with myotonic dystrophy (DM), the severity of clinical signs is correlated with the length of a (CTG)n trinucleotide repeat sequence. This sequence tends to expand in subsequent generations. In order to examine the kinetics of this process and, in particular, the influence of the mutant-allele size and the sex of the transmitting parent, we have studied (CTG)n repeat lengths in the offspring of 38 healthy carriers with small mutations (less than 100 CTG trinucleotides, mean length [CTG]67). In these studies, we found a weakly positive correlation between the size of the mutation in the carrier parents and that in their offspring. Furthermore, we observed that, in the offspring of male transmitters, repeat lengths exceeding 100 CTG trinucleotides were much more frequent than in the offspring of carrier females (48 [92%] of 52 vs. 7 [44%] of 16, P = .0002). Similarly, in genealogical studies performed in 38 Dutch DM kindreds, an excess of nonmanifesting male transmitters was noted, which was most conspicuous in the generation immediately preceding that with phenotypic expression of DM. Thus, two separate lines of evidence suggest that the sex of the transmitting parent is an important factor that determines DM allele size in the offspring. On the basis of our data, we estimate that when both parents are asymptomatic, the odds are approximately 2:1 that the father carries the DM mutation. Because expansion of the CTG repeat is more rapid with male transmission, negative selection during spermatogenesis may be required to explain the exclusive maternal inheritance of severe congenital onset DM.

Published

1993

206. Two additional cases of the Ohdo blepharophimosis syndrome.

Author

Maat-Kievit A, Brunner HG, and Maaswinkel-Mooij P

Subjects

Abnormalities, Multiple genetics, Blepharophimosis genetics, Blepharophimosis physiopathology, Child, Preschool, Female, Humans, Male, Syndrome, Blepharophimosis diagnosis

Abstract

Two additional cases of the Ohdo blepharophimosis syndrome are described and compared to the 5 patients previously reported. Blepharophimosis, ptosis, dental hypoplasia, mental retardation, and deafness can be considered as common manifestations of the syndrome. Male patients show cryptorchidism and scrotal hypoplasia.

Published

1993

207. Abnormal behavior associated with a point mutation in the structural gene for monoamine oxidase A.

Author

Brunner HG, Nelen M, Breakefield XO, Ropers HH, and van Oost BA

Subjects

Cell Line, Cells, Cultured, Female, Humans, Intellectual Disability enzymology, Male, Monoamine Oxidase deficiency, Pedigree, Phenotype, Skin enzymology, Syndrome, X Chromosome, Aggression, Genes, Intellectual Disability genetics, Monoamine Oxidase genetics, Point Mutation

Abstract

Genetic and metabolic studies have been done on a large kindred in which several males are affected by a syndrome of borderline mental retardation and abnormal behavior. The types of behavior that occurred include impulsive aggression, arson, attempted rape, and exhibitionism. Analysis of 24-hour urine samples indicated markedly disturbed monoamine metabolism. This syndrome was associated with a complete and selective deficiency of enzymatic activity of monoamine oxidase A (MAOA). In each of five affected males, a point mutation was identified in the eighth exon of the MAOA structural gene, which changes a glutamine to a termination codon. Thus, isolated complete MAOA deficiency in this family is associated with a recognizable behavioral phenotype that includes disturbed regulation of impulsive aggression.

Published

1993

208. Identification of four novel mutations in the COL4A5 gene of patients with Alport syndrome.

Author

Lemmink HH, Schröder CH, Brunner HG, Nelen MR, Zhou J, Tryggvason K, Haagsma-Schouten WA, Roodvoets AP, Rascher W, and van Oost BA

Subjects

Amino Acid Sequence, Animals, Base Sequence, Exons, Female, Humans, Molecular Sequence Data, Oligodeoxyribonucleotides, Phenotype, Polymerase Chain Reaction, Reference Values, Sequence Homology, Amino Acid, Collagen genetics, Nephritis, Hereditary genetics, Point Mutation

Abstract

The type IV collagen alpha 5 chain (COL4A5) genes of patients with Alport syndrome were tested for major gene rearrangements by Southern blot analysis, using COL4A5 cDNA clones as probes. In addition, individual exons were screened for small mutations by single-strand conformation polymorphism (SSCP) analysis. Four new COL4A5 mutations were detected. A duplication of the nine most 3' located nucleotides of exon 49 and the first nucleotide of intron 49 was identified in the COL4A5 gene of one patient. Two patients displayed single base substitutions leading to, respectively, a proline to threonine and an arginine to glutamine substitution in the C-terminal end. Both substitutions involve amino acids conserved through evolution. In COL4A5 intron 41 a mutation changing the splice acceptor site from AG to AA was identified. All mutations cosegregate with the clinical phenotype of Alport syndrome in affected family members. In a control population of 50 individuals tested by PCR-SSCP these mutations were never identified. Together with two mutations reported previously, a total of six mutations were found in 26 patients with Alport syndrome (23%) after systematic screening of about 30% of the COL4A5 coding region. The clinical features of these six patients are described in detail.

Published

1993

209. X-linked borderline mental retardation with prominent behavioral disturbance: phenotype, genetic localization, and evidence for disturbed monoamine metabolism.

Author

Brunner HG, Nelen MR, van Zandvoort P, Abeling NG, van Gennip AH, Wolters EC, Kuiper MA, Ropers HH, and van Oost BA

Subjects

Adult, Biogenic Monoamines urine, Female, Genes, Humans, Intellectual Disability urine, Karyotyping, Male, Monoamine Oxidase blood, Mutation, Pedigree, Polymorphism, Genetic, Dangerous Behavior, Genetic Linkage, Intellectual Disability genetics, Monoamine Oxidase genetics, X Chromosome

Abstract

We have identified a large Dutch kindred with a new form of X-linked nondysmorphic mild mental retardation. All affected males in this family show very characteristic abnormal behavior, in particular aggressive and sometimes violent behavior. Other types of impulsive behavior include arson, attempted rape, and exhibitionism. Attempted suicide has been reported in a single case. The locus for this disorder could be assigned to the Xp11-21 interval between DXS7 and DXS77 by linkage analysis using markers spanning the X chromosome. A maximal multipoint lod score of 3.69 was obtained at the monoamine oxidase type A (MAOA) locus in Xp11.23-11.4. Results of 24-h urine analysis in three affected males indicated a marked disturbance of monoamine metabolism. These data are compatible with a primary defect in the structural gene for MAOA and/or monoamine oxidase type B (MAOB). Normal platelet MAOB activity suggests that the unusual behavior pattern in this family may be caused by isolated MAOA deficiency.

Published

1993

210. Exclusion of the neurofibromatosis 1 locus in a family with inherited café-au-lait spots.

Author

Brunner HG, Hulsebos T, Steijlen PM, der Kinderen DJ, vd Steen A, and Hamel BC

Subjects

Adolescent, Alleles, Child, Chromosome Mapping, Female, Humans, Mutation, Neurofibromatoses pathology, Pedigree, Pigmentation Disorders pathology, Genes, Neurofibromatosis 1, Genetic Linkage, Neurofibromatoses genetics, Pigmentation Disorders genetics

Abstract

We have performed linkage analysis in a small family with autosomal dominant inheritance of multiple café-au-lait spots (CLS) in order to clarify its relationship to classical von Recklinghausen disease (NF 1). We found that an affected woman had transmitted a different haplotype for markers flanking the NF1 gene to both of her affected daughters. These results exclude an allelic mutation of the NF 1 gene on chromosome 17 as the cause for inherited café-au-lait spots in this family.

Published

1993

211. Brief report: reverse mutation in myotonic dystrophy.

Author

Brunner HG, Jansen G, Nillesen W, Nelen MR, de Die CE, Höweler CJ, van Oost BA, Wieringa B, Ropers HH, and Smeets HJ

Subjects

Adult, Alleles, Chromosomes, Human, Pair 19, Female, Genetic Linkage, Humans, Male, Mutation, Pedigree, Peptide Fragments analysis, Repetitive Sequences, Nucleic Acid, Myotonic Dystrophy genetics

Published

1993

212. [The Coffin-Siris syndrome. Description of 4 patients and a literature review].

Author

van Heyst AF, Kollée LA, and Brunner HG

Subjects

Female, Humans, Infant, Infant, Newborn, Joint Instability diagnosis, Male, Syndrome, Abnormalities, Multiple, Growth Disorders diagnosis, Hypertelorism diagnosis, Nails, Malformed

Abstract

Four patients with Coffin-Siris syndrome are described. In addition a 30 cases are reviewed. The most frequent symptoms are dysmorphic features of the facies with sparse scalp hair, nail hypoplasia and mental retardation.

Published

1993

213. [Dystrophia myotonica and pregnancy].

Author

van de Biezenbos JB, Nijhuis JG, and Brunner HG

Subjects

Adult, Clubfoot etiology, Female, Genetic Counseling, Humans, Infant, Newborn, Myotonic Dystrophy congenital, Myotonic Dystrophy genetics, Polyhydramnios etiology, Pregnancy, Myotonic Dystrophy complications, Pregnancy Complications

Abstract

We describe the maternal and neonatal complications of pregnancy in two patients with myotonic dystrophy. The disease leads to an increased spontaneous abortion rate, hydramnios, prolonged first and second stages of labour, retained placenta, postpartum haemorrhages and anaesthetic sensitivity in the mother. The neonatal problems are caused by the congenital form of the disease. The major clinical features of congenital myotonic dystrophy are bilateral facial weakness, hypotonia, neonatal distress, feeding difficulties, talipes, tent-shaped mouth, mental retardation and delayed motor development. Relatives of a known myotonic dystrophy patient should be advised to let themselves be examined for this disease. If the disease is diagnosed, information should be given regarding possibilities for prenatal diagnosis. Pregnancy in myotonic dystrophy patients should be monitored by a gynaecologist. Labour has to take place in a hospital with intensive care facilities for mother and child.

Published

1992

214. Craniofrontonasal dysplasia.

Author

Kapusta L, Brunner HG, and Hamel BC

Subjects

Adult, Child, Child Development, Diagnosis, Differential, Female, Fingers abnormalities, Follow-Up Studies, Growth, Humans, Intellectual Disability, Male, Nails, Malformed, Toes abnormalities, Abnormalities, Multiple diagnosis, Abnormalities, Multiple genetics, Abnormalities, Multiple physiopathology, Facial Bones abnormalities, Skull abnormalities

Abstract

We report on nine patients with craniofrontonasal dysplasia (CFND). Seven classical cases had facial features suggestive of frontonasal dysplasia and coronal craniosynostosis. Extracranial abnormalities such as brittle nails with prominent longitudinal grooves or syndactyly of fingers and toes were observed in individual patients. In two families the father of classical cases showed a milder pattern of abnormalities, consistent with the diagnosis. We present a 2- to 13-year follow-up on our patients. Hypotonia and laxity of joints are common and may necessitate supportive measures. Mild developmental delay was noted in three out of six classical cases studied in detail. Unlike almost all other X-linked disorders, clinical expression in CFND is generally much more severe in females than in males. In contrast to previous reports of this condition, one of our severely affected cases is a male.

Published

1992

215. Microdeletions in patients with gusher-associated, X-linked mixed deafness (DFN3).

Author

Bach I, Brunner HG, Beighton P, Ruvalcaba RH, Reardon W, Pembrey ME, van der Velde-Visser SD, Bruns GA, Cremers CW, and Cremers FP

Subjects

Chromosome Deletion, Chromosome Mapping, Genetic Linkage, Genetic Markers, Humans, Male, Deafness genetics, X Chromosome

Abstract

Employing various probes from the proximal part of the Xq21 region, which is known to harbor the DFN3 gene, we have investigated 13 unrelated male probands with X-linked deafness, to detect possible deletions. For two of these patients, microdeletions could be detected by using probe pHU16 (DXS26). One of these deletions also encompasses locus DXS169, indicating that it extends farther toward the centromere. The presence of normal hybridization patterns in the DNA of 25 unrelated control males suggests that these deletions are the primary cause of progressive mixed deafness in these patients. If so, their molecular characterization may pave the way for the identification and isolation of the corresponding gene.

Published

1992

216. Absent thumb, immune disorder, and congenital anemia presenting with hydrops fetalis.

Author

Semmekrot BA, Haraldsson A, Weemaes CM, Smeets DF, Geven WB, and Brunner HG

Subjects

Abnormalities, Multiple diagnosis, Diagnosis, Differential, Female, Humans, Infant, Newborn, Syndrome, Abnormalities, Multiple genetics, Anemia congenital, Hydrops Fetalis genetics, Immune System Diseases genetics, Thumb abnormalities

Abstract

A patient is described who presented with severe congenital anemia, hydrops fetalis, immune disorder, and absent thumbs. No toxic, infectious, or metabolic cause was found to explain these symptoms. Immunologic and cytogenetic studies excluded several syndromes that combine radial ray anomalies with hematological involvement. After careful study of the literature, it is concluded that the disorder described here represents a new syndrome that can be added to a growing list of hematological-radial syndromes.

Published

1992

217. Eye movement disorder: an early expression of the myotonic dystrophy gene?

Author

ter Bruggen JP, Tijssen CC, Brunner HG, van Oost BA, and Bastiaensen LA

Subjects

Adult, Electromyography, Female, Heterozygote, Humans, Male, Myotonic Dystrophy diagnosis, Myotonic Dystrophy epidemiology, Predictive Value of Tests, Eye Movements physiology, Gene Expression genetics, Genetic Carrier Screening methods, Myotonic Dystrophy genetics

Abstract

Eye movement recording (EMR) has been performed in 5 asymptomatic myotonic dystrophy (MyD) gene carriers, 7 mildly affected MyD patients, and 23 age- and sex-matched healthy controls. The purpose of the study was to evaluate whether eye movement abnormalities are an early expression of the MyD gene, and to determine the value of this procedure for detection of otherwise asymptomatic gene carriers. EMR did not reveal any abnormalities in the asymptomatic group, but in the mildly affected group showed significantly (P less than 0.01) decreased maximum velocities of the saccades, compared with controls. The results indicate that EMR may aid in the detection of mildly affected MyD patients. However, true presymptomatic diagnosis with EMR has not yet proven possible.

Published

1992

218. Myotonic dystrophy. Predictive value of normal results on clinical examination.

Author

Brunner HG, Smeets HJ, Nillesen W, van Oost BA, van den Biezenbos JB, Joosten EM, Pinckers AJ, Hamel BC, Theeuwes AG, and Wieringa B

Subjects

Biomarkers, DNA analysis, DNA Probes, Heterozygote, Humans, Myotonic Dystrophy genetics

Abstract

Myotonic dystrophy (DM) is well known for its highly variable clinical picture, including the age at which symptoms are first detected. In order to assess the proportion of asymptomatic gene carriers at different ages, we have used linked DNA markers to study individuals at 50% genetic risk of DM, in whom neurological examination, slit-lamp examination and electromyography (EMG) had failed to show diagnostic signs. A total of 139 asymptomatic offspring of DM patients were studied. Our analyses identified 11 out of these 139 as probable gene carriers. Our data show that penetrance of the DM gene increases with age. After correction for the possibility of genetic recombination between the DM gene and the DNA markers used, we calculated the residual chance of carrying the DM gene as 8.3% for clinically normal offspring aged between 20 and 39 yrs. We evaluated several factors that might influence this figure. Neither the sex of the propositus nor that of the affected parent modified the risk of carrying the DM gene. Presence of aspecific lens opacities also did not correlate with the risk of having inherited the DM gene. Since a significant proportion of DM gene carriers are not detected by neurological examination, including slit-lamp examination and EMG, these results confirm the need for DNA analysis in asymptomatic offspring of DM patients.

Published

1991

219. Linkage analysis in X-linked adrenoleukodystrophy and application in post- and prenatal diagnosis.

Author

van Oost BA, van Zandvoort PM, Tünte W, Brunner HG, Hoogeboom AJ, Maaswinkel-Mooy PD, Bakkeren J, Hamel B, and Ropers HH

Subjects

Adrenoleukodystrophy genetics, Female, Genetic Carrier Screening, Humans, Lod Score, Male, Pregnancy, Recombination, Genetic, Adrenoleukodystrophy diagnosis, Genetic Linkage, Polymorphism, Restriction Fragment Length, Prenatal Diagnosis, X Chromosome

Abstract

We have performed linkage analysis with the DNA markers DXS52 and the clotting factor VIII gene (F8C), in several large families with X-linked adrenoleukodystrophy (ALD). The tight linkage to DXS52 could be extended giving a maximal LOD score of 22.5 at 1 cM. F8C was also tightly linked to ALD with a maximal LOD score of 7.8 without recombination. Multipoint linkage analysis with the markers DXS304, DXS52, and F8C indicated that both the gene for ALD and for F8C are distal to DXS52. In four patients with ALD, no major structural rearrangement in the Xqter region was observed; in particular, there were no abnormalities in the vision blindness genes. DNA analysis appeared to be of use in determination of the carrier status of females at risk, for the determination of the origin of the mutation in a particular family, and for prenatal diagnosis.

Published

1991

220. Identification of variable simple sequence motifs in 19q13.2-qter: markers for the myotonic dystrophy locus.

Author

Smeets HJ, Hermens R, Brunner HG, Ropers HH, and Wieringa B

Subjects

Alleles, Base Sequence, Crossing Over, Genetic, Female, Genetic Linkage, Haplotypes, Humans, Male, Molecular Sequence Data, Mutation, Pedigree, Restriction Mapping, Chromosomes, Human, Pair 19, DNA Repair genetics, Genetic Markers, Myotonic Dystrophy genetics, Repetitive Sequences, Nucleic Acid genetics

Abstract

Variable simple sequence motifs (VSSMs), or microsatellites, were used for the genetic delimitation of the myotonic dystrophy (DM) region at 19q. Three simple sequence motifs were identified in and around the ERCC1 DNA-repair gene at 19q13.2-13.3 and one in the vicinity of the RRAS gene at 19q13.3-qter. A (TG)n repeat, situated within the ninth intron of the ERCC1 gene, was converted into a highly informative multiallelic marker using PCR-mediated DNA amplification and high-resolution gel analysis. The structurally similar sequence motif in the RRAS gene yielded a marker system with only two alleles. Use of these VSSMs for linkage analysis and haplotyping in a selected set of DM families revealed that the DM gene is distal but close to the ERCC1 locus and can be excluded from the CKM-ERCC1 interval at 19q13.2. The order for RRAS and other distally located markers was established as DM-D19S50-[RRAS,KLK]-D19S22-ter.

Published

1991

221. Molecular genetics of X-linked hearing impairment.

Author

Brunner HG, Smeets B, Smeets D, Nelen M, Cremers CW, and Ropers HH

Subjects

Chromosome Mapping, Congenital Abnormalities genetics, Female, Humans, Male, Pedigree, Polymorphism, Restriction Fragment Length, Syndrome, Deafness genetics, Hearing Loss genetics, X Chromosome

Published

1991

222. Acrocallosal syndrome.

Author

Hendriks HJ, Brunner HG, Haagen TA, and Hamel BC

Subjects

Animals, Brain diagnostic imaging, Foot Deformities diagnostic imaging, Humans, Infant, Newborn, Male, Mice, Radiography, Syndrome, Brain abnormalities, Foot Deformities genetics, Genes, Recessive

Abstract

Acrocallosal syndrome is an autosomal recessive disorder of brain malformation and complex polydactyly. We report on an additional patient with this disorder. It is suggested that increased birth weight and cerebellar hypoplasia occur in acrocallosal syndrome. The finding of an extra bone within the anterior fontanel in our patient suggests similarity to the Xt mouse mutant, which is homologous to Greig syndrome in man. This provides additional support for the hypothesis of allelism of the Greig and acrocallosal syndromes.

Published

1990

223. A multipoint linkage map around the locus for myotonic dystrophy on chromosome 19.

Author

Brunner HG, Smeets H, Lambermon HM, Coerwinkel-Driessen M, van Oost BA, Wieringa B, and Ropers HH

Subjects

Chromosome Mapping, Crossing Over, Genetic, DNA Mutational Analysis, Female, Genetic Markers, Humans, Male, Polymorphism, Restriction Fragment Length, Recombination, Genetic, Chromosomes, Human, Pair 19, Genetic Linkage, Muscular Dystrophies genetics

Abstract

Employing 16 polymorphic DNA markers as well as the chromosome 19 centromere heteromorphism, we have performed a genetic linkage study in 26 families with myotonic dystrophy. Fourteen of these markers had been assigned previously to one of five different intervals of the 19cen-19q13.2 segment by using somatic cell hybrids. For the long arm of chromosome 19, a genetic map that encompasses 9 polymorphic markers and the DM gene has been constructed. Our studies indicate that the DM and CKMM genes map distal to the ApoC2-ApoE gene cluster and to the anonymous polymorphic markers D19S15 and D19S16, but proximal to the D19S22 marker. The orientation of DM and CKMM remains to be determined.

Published

1989

224. Use of variable simple sequence motifs as genetic markers: application to study of myotonic dystrophy.

Author

Smeets HJ, Brunner HG, Ropers HH, and Wieringa B

Subjects

Apolipoprotein C-II, Apolipoproteins C genetics, Chromosomes, Human, Pair 19, Female, Humans, Male, Molecular Sequence Data, Multigene Family, Oligonucleotide Probes, Pedigree, Polymerase Chain Reaction, Polymorphism, Restriction Fragment Length, Genetic Markers, Myotonic Dystrophy genetics, Repetitive Sequences, Nucleic Acid

Abstract

Among the many classes of repetitive elements present in the human genome, the ubiquitous "simple sequence motifs" (SSMs) composed of [A]n, [TG]n, [AG]n or codon-tandem repeats form a major source of genetic variation. Here we report a detailed molecular-genetic study of a "variable simple sequence motif" (VSSM) in the apolipoprotein C2 (apoC2) gene, which maps to the 19q13.2 region in the vicinity of the myotonic dystrophy (DM) locus. By combining in vitro DNA-amplification using the polymerase chain reaction and high-resolution gel electrophoresis, we could demonstrate a high degree of allelic variation with at least ten alleles, which differ in the number of repeated [TG] or [AG] dinucleotide units. Similar results were found for the somatostatin I gene locus. To evaluate the usefulness of SSM-length polymorphisms as genetic markers, the apoC2-VSSM was employed for linkage analysis in DM families. Our results establish that the orientation of the apolipoprotein gene cluster on 19q is cenapoE-apoC2-ter and indicate that the many thousands of structurally similar VSSMs in the human genome represent a rich source of highly informative genetic and diagnostic markers.

Published

1989

225. [Alport's syndrome].

Author

Schröder CH, Monnens LA, Veerkamp JH, and Brunner HG

Subjects

Adult, Basement Membrane ultrastructure, Biopsy, Child, Female, Humans, Kidney ultrastructure, Kidney Failure, Chronic etiology, Male, Nephritis, Hereditary complications, Nephritis, Hereditary pathology, Sex Factors, Basement Membrane metabolism, Collagen metabolism, Nephritis, Hereditary metabolism

Published

1988

226. The gene for X-linked progressive mixed deafness with perilymphatic gusher during stapes surgery (DFN3) is linked to PGK.

Author

Brunner HG, van Bennekom A, Lambermon EM, Oei TL, Cremers WR, Wieringa B, and Ropers HH

Subjects

DNA Probes, Deafness surgery, Female, Genetic Markers, Humans, Male, Pedigree, Perilymph, Polymorphism, Restriction Fragment Length, Recombination, Genetic, Stapes Surgery, Deafness genetics, Genetic Linkage, Phosphoglycerate Kinase genetics, X Chromosome

Abstract

A linkage analysis has been performed in a large Dutch kindred with progressive mixed deafness with perilymphatic gusher during stapes surgery (DFN3) using a panel of X-chromosomal RFLPs. Tight linkage (zmax = 3.07 at 0 = theta = 0.00) was demonstrated with the locus for phosphoglycerate kinase (PGK), which is located at Xq13. Tight linkage was excluded for DXS9 (probe RC8) and DXS41 (probe 99.6) on Xp and for blood clotting factor 9 (FIX) on distal Xq. Deafness is one of the predominant clinical features in males with deletions of the Xq21 band. Our results suggest that this association may be due to involvement of the DFN3 gene.

Published

1988

227. Myotonic dystrophy is closely linked to the gene for muscle-type creatine kinase (CKMM).

Author

Brunner HG, Korneluk RG, Coerwinkel-Driessen M, MacKenzie A, Smeets H, Lambermon HM, van Oost BA, Wieringa B, and Ropers HH

Subjects

Apolipoprotein C-II, Apolipoproteins C genetics, Gene Frequency, Genetic Markers, Humans, Isoenzymes, Recombination, Genetic, Chromosomes, Human, Pair 19, Creatine Kinase genetics, Genetic Linkage, Myotonic Dystrophy genetics

Abstract

We have studied genetic linkage between the gene for creatine kinase muscle type (CKMM) and the gene for myotonic dystrophy (DM). In a panel of 65 myotonic dystrophy families from Canada and the Netherlands, a maximum lod score (Zmax) of 22.8 at a recombination frequency (theta) of 0.03 was obtained. Tight linkage was also demonstrated for CKMM and the gene for apolipoprotein C2 (ApoC2). This establishes CKMM as a useful marker for myotonic dystrophy.

Published

1989