Your search keyword '"Dahl, N."' showing total 33 results

1. Homozygosity for a missense variant in COMP gene associated with severe pseudoachondroplasia.

Author

Tariq, M., Khan, T. N., Lundin, L., Jameel, M., Lönnerholm, T., Baig, S. M., Dahl, N., and Klar, J.

Subjects

HOMOZYGOSITY, BONE diseases, EXTRACELLULAR matrix proteins, MULTIPLE epiphyseal dysplasia, SKELETAL dysplasia

Abstract

The phenotypic spectrum associated with heterozygous mutations in cartilage oligomeric matrix protein gene ( COMP) range from a mild form of multiple epiphyseal dysplasia ( MED) to pseudoachondroplasia ( PSACH). However, the phenotypic effect from biallelic COMP variants is unclear. We investigated a large consanguineous Pakistani family with a severe form of PSACH in 2 individuals. Another 14 family members presented with a mild PSACH phenotype similar to MED. Using exome sequencing and subsequent segregation analysis, we identified homozygosity for a COMP missense variant [c. 1423G>A; p.( D475N)] in the 2 severely affected individuals, whereas family members with the mild PSACH phenotype were heterozygous. Our observations show for the first time that a biallelic COMP variant may be associated with pronounced and widespread skeletal malformations suggesting an additive effect of the 2 mutated alleles. [ABSTRACT FROM AUTHOR]

Published

2018

2. Re-evaluation of the dysequilibrium syndrome.

Author

Melberg, A., Örlén, H., Raininko, R., Entesarian, M., Dahlqvist, J., Gustavson, K. H., and Dahl, N.

Subjects

DIZZINESS, BRAIN imaging, GENETIC mutation, MAGNETIC resonance imaging, BLOOD testing, CEREBELLAR ataxia, GLYCOSYLATION

Abstract

Melberg A, Örlén H, Raininko R, Entesarian M, Dahlqvist J, Gustavson KH, Dahl N. Re-evaluation of the dysequilibrium syndrome. Acta Neurol Scand: 2011: 123: 28-33. © 2010 The Authors Journal compilation © 2010 Blackwell Munksgaard. To re-evaluate middle-aged Swedish patients diagnosed with dysequilibrium syndrome (DES) in childhood and to compare their clinical and neuroimaging features to DES with VLDLR gene mutations (DES-VLDR). Six patients from five families underwent neurological examination and magnetic resonance imaging (MRI) of the brain. Blood samples from the patients were screened for serum carbohydrate-deficient transferrin (s-CDT; disialotransferrin). The very-low-density lipoprotein receptor ( VLDLR) gene was sequenced. Five patients had non-progressive cerebellar ataxia (NPCA), dysarthria and short stature. Mental retardation and strabismus, characteristic for DES-VLDLR, were inconsistent among our patients. None of our patients had VLDLR mutations or MRI findings characteristic of DES-VLDLR. MRI findings were variable from a normal cerebellum to marked cerebellar hypoplasia or atrophy and signal intensity changes. One patient was diagnosed with congenital disorder of glycosylation type 1a (CDG-1a). DES was originally coined on mainly clinical grounds before MRI and specific genetic tests were available, both of which should be used to arrive at an appropriate diagnosis. [ABSTRACT FROM AUTHOR]

Published

2011

3. Central nervous system involvement in severe congenital neutropenia: neurological and neuropsychological abnormalities associated with specific HAX1 mutations.

Author

Carlsson, G., van't Hooft, I., Melin, M., Entesarian, M., Laurencikas, E., Nennesmo, I., Trębińska, A., Grzybowska, E., Palmblad, J., Dahl, N., Nordenskjöld, M., Fadeel, B., and Henter, J.-I.

Subjects

GENETIC mutation, ORGANS (Anatomy), NERVOUS system, CENTRAL nervous system, CRYOBIOLOGY

Abstract

Objectives. Homozygous mutations in the HAX1 gene were recently identified in severe congenital neutropenia patients belonging to the original Kostmann family in northern Sweden. Our observations suggested that these patients also develop neurological and neuropsychological symptoms. Methods. Detailed clinical studies and mutation analyses were performed in the surviving patients belonging to the Kostmann kindred and in two patients not related to this family, along with studies of HAX1 splice variant expression in normal human tissues. Results. Five of six Kostmann family patients and one other patient from northern Sweden harboured homozygous HAX1 mutations (568C→T, Q190X) and one carried a heterozygous ELA2 gene mutation. One Swedish patient of Kurdish extraction carried alternative homozygous HAX1 mutations (131G→A, W44X). All the three patients with Q190X mutations who were alive and available for evaluation developed neurological disease with decreased cognitive function, and three of four patients who reached 10 years developed epilepsy. In contrast, the patients with the ELA2 and W44X HAX1 mutations, respectively, showed no obvious neurological abnormalities. Moreover, two alternative HAX1 splice variants were identified in normal human tissues, including the brain. Both transcripts contained exon 5, harbouring the Q190X mutation, whereas the 5′ end of exon 2 containing the W44X mutation was spliced out from the second transcript. Conclusions. We describe neurological and neuropsychological abnormalities for the first time in Kostmann disease patients. These central nervous system symptoms appear to be associated with specific HAX1 mutations. [ABSTRACT FROM AUTHOR]

Published

2008

4. Effects of oxybutynin transdermal system on health-related quality of life and safety in men with overactive bladder and prostate conditions.

Author

Staskin DR, Rosenberg MT, Dahl NV, Polishuk PV, Zinner NR, Staskin, D R, Rosenberg, M T, Dahl, N V, Polishuk, P V, and Zinner, N R

Abstract

Aims: Overactive bladder (OAB) is common in men and may exist concomitantly with benign prostatic hyperplasia (BPH) and obstruction. We present a subanalysis of results from men with OAB in a 6-month, open-label study of treatment with the oxybutynin transdermal system (OXY-TDS). Broad entry criteria were incorporated to yield a clinically representative population.Methods: All participants received OXY-TDS 3.9 mg/day. Effectiveness was assessed by changes in scores on validated questionnaires, which included the single-item Patient Perception of Bladder Condition (PPBC), the King's Health Questionnaire (KHQ) and the Beck Depression Inventory-II (BDI-II).Results: The proportion of men (n=369; mean age=69.6 years) who reported that their bladder condition caused moderate, severe or many severe problems (PPBC>or=4) improved from 77.3% at baseline to 38.1-53.6% in subsequent months. Mean KHQ scores decreased significantly (p12 (associated with a diagnosis of depression) decreased from 23.9% to 17.9% (p=0.0055). Men with a history of 'prostate problems' or use of 'BPH medication' (32.2%) had KHQ domain changes that were similar (p>or=0.1016) to those of other men. Most men (76.2%) reported no treatment-related adverse events; two men (0.5%) experienced symptoms of mild urinary retention, but neither required catheterisation.Conclusions: Oxybutynin transdermal system treatment of men with OAB was effective and well tolerated, regardless of history of prostate condition. [ABSTRACT FROM AUTHOR]

Published

2008

5. Depression in relation to age and gender in the general population: the Nord-Trøndelag Health Study (HUNT).

Author

Stordal, E., Bjartveit Krüger, M., Dahl, N. H., Krüger, Ø., Mykletun, A., and Dahl, A. A.

Subjects

MENTAL depression, SEX differences (Biology)

Abstract

Objective: Previous sample studies of depression have shown a higher prevalence of depression in women, and an inconsistent relation to age has been found for both genders. The aim of the present study was to investigate depression in relation to gender and age in the general adult population. Method: Of the total population of 92 100 individuals aged 20–89 years and living in Nord-Trøndelag county of Norway, 62 344 (67.7%) filled in valid ratings of depression on the Hospital Anxiety and Depression Scale (HADS). Results: Minimal gender difference was found in dimensional depression scores and in prevalence rates of depression. Both these measures were found to increase continuously with age in both genders. Conclusion: Our results of this population-based study differ from most sample studies reported, and these discrepancies are discussed with focus on study design, self-rating, and the concept of depression covered by HADS. [ABSTRACT FROM AUTHOR]

Published

2001

6. Herbs and supplements in dialysis patients: panacea or poison?

Author

Dahl, Naomi V. and Dahl, N V

Subjects

*ALTERNATIVE medicine, *KIDNEY disease treatments, *HERBAL medicine

Abstract

The safety of herbal remedies and supplement use is of particular concern in patients with renal disease, and reliable information is not always easy to find. Predialysis patients may be drawn to complementary and alternative medicine (CAM) because they believe it can help prevent the progression of their renal disease. The purpose of this series of articles on alternative medicine for nephrologists is to address concerns and issues specific to CAM use in dialysis patients and to provide a guide to reliable sources of information. This introductory article emphasizes safety issues with a focus primarily on herbal medicine. Lack of regulation means that patients may not actually be taking what they think they are. Independent laboratory analyses have shown a lack of stated label ingredients and many instances of supplements and traditional remedies being contaminated with pesticides, poisonous plants, heavy metals, or conventional drugs. While certain supplements are always unsafe (carcinogenic, hepatotoxic, glandular extracts), others are specifically contraindicated in renal disease. Supplement use may be especially hazardous in renal disease because of unpredictable pharmacokinetics, drug interactions, negative effects on kidney function, nephrotoxicity, hemodynamic alterations, unpredictable effects on blood pressure or blood glucose, or potentiation of electrolyte abnormalities. There are no data on potential dialyzability of either active compounds, or their potentially active or toxic metabolites. Many supplements contain metal ions and other minerals. Transplant recipients are also at risk from potential unpredictable effects on immune function. Recommendations and information resources are listed. [ABSTRACT FROM AUTHOR]

Published

2001

7. A microdeletion syndrome due to a 3-Mb deletion on 19q13.2 – Diamond–Blackfan anemia associated with macrocephaly, hypotonia, and psychomotor retardation.

Author

Cario, H, Bode, H, Gustavsson, P, Dahl, N, and Kohne, E

Subjects

PURE red cell aplasia, PSYCHOMOTOR disorders, HUMAN abnormalities

Abstract

We report on a boy with congenital pure red blood cell aplasia [Diamond–Blackfan anemia (DBA)] and severe congenital hypotonia, macrocephaly, hypertelorism, a broad and tall forehead, medial epicanthus, and facial hypotonia with mouth-breathing and drooling, an affable and out-going personality, and a general psychomotor retardation. These features show similarity to the phenotype of the X-linked FG syndrome. DBA was diagnosed at the age of 4 months, and the boy underwent treatment with transfusion and with prednisolone. He had a normal 46, XY karyotype, but fluorescence in situ hybridization (FISH) analysis to metaphase chromosomes revealed a 3-Mb deletion on 19q13.2. This chromosomal region has previously been linked to the DBA phenotype and one 19q13 microdeletion has been identified in a patient with DBA. This deletion coincides with the deletion reported here. We suggest that the complex phenotype of our patient, including both DBA and the associated features, represent a microdeletion syndrome. [ABSTRACT FROM AUTHOR]

Published

1999

8. Exercise intensity and reduction in neurotic symptoms.

Author

Sexton, H., Mære, Å., and Dahl, N. H.

Published

1989

9. Genetic mapping of loci for X-linked retinitis pigmentosa.

Author

Dahl, N., Sundvall, M., Pettersson, U., Andréasson, S., Anvret, M., Kugelberg, U., Hagbyhn-Gericke, A., and Goonewardena, P.

Published

1991

10. Mutation analysis for prenatal diagnosis and heterozygote detection of Gaucher disease type III (Norrbottnian type).

Author

Dahl, Niklas, Wadelius, Claes, Annerén, Göran, Gustavson, Karl-Henrik, Dahl, N, Wadelius, C, Annerén, G, and Gustavson, K H

Published

1992

11. Molecular Xp deletion in a male: suggestion of a locus for hypogonadotropic hypogonadism distal to the glycerol kinase and adrenal hypoplasia loci.

Author

Goonewardena, P., Dahl, N., Ritzén, M., Ommen, G. J. B., and Pettersson, U.

Published

1989

12. A Case of Complete Trisomy 2p/Triploidy Mosaicism.

Author

DAHL, N., ELIASSON, I.-L., and GUSTAVSON, K.-H.

Published

1988

13. Anticipation of autosomal dominant progressive external ophthalmoplegia with hypogonadism.

Author

Melberg, Atle, Arnell, Henrik, Dahl, Niklas, Stålberg, Erik, Raininko, Raili, Oldfors, Anders, Bakall, Benjamin, Lundberg, Per Olov, Holme, Elisabeth, Melberg, A, Arnell, H, Dahl, N, Stålberg, E, Raininko, R, Oldfors, A, Bakall, B, Lundberg, P O, and Holme, E

Published

1996

14. THE PEOPLE OF GOD.

Author

Dahl, N. A.

Published

1957

15. Hemizygosity for chromosome 2q14.2-q22.1 spanning the GLI2 and PROC genes associated with growth hormone deficiency, polydactyly, deep vein thrombosis and urogenital abnormalities.

Author

Gustavsson, P., Schoumans, J., Staaf, J., Jönsson, G., Carlsson, F., Kristoffersson, U., Borg, Å, Nordenskjöld, M., and Dahl, N.

Subjects

LETTERS to the editor, GENETICS

Abstract

A letter to the editor is presented in response to the article "Hemizygosity for chromosome 2q14.2-q22.1 spanning the GLI2 and PROC genes associated with growth hormone deficiency, polydactyly, deep vein thrombosis and urogenital abnormalities," published in the April 2006 edition of Clinical Genetics.

Published

2006

16. LBOVI-A-1.

Author

Goldberg, R. P. and Dahl, N. V.

Subjects

BLADDER abnormalities, QUALITY of life, TRANSDERMAL medication, DRUG administration, PHARMACEUTICAL research, QUESTIONNAIRES

Abstract

Background/aims: Treatment history may impact perceived effectiveness of antimuscarinic therapy for overactive bladder (OAB). This analysis of the Multicenter Assessment of Transdermal Therapy in Overactive Bladder with Oxybutynin (MATRIX) compares quality of life (QOL) in treatment-experienced vs -naive patients.Methods: MATRIX, an open-label, multicenter prospective trial, evaluated adults with OAB treated with transdermal oxybutynin 3.9 mg/d (Oxytrol®, Watson Pharma, Corona, CA) for ≤6 mos. Study population included 3 predefined patient groups: treatment naive (n=973), recently discontinued (therapy stopped 0-29 days prior; n=785), lapsed (no therapy ≥30 days; n=566). King's Health Questionnaire® (KHQ) was used to evaluate QOL. P values based on ANCOVA.Results: MATRIX enrolled 2878 patients (mean age 62.5y±14.8y; 87% women). At baseline, 46% had OAB symptoms ≥4y; 57% had prior oral OAB treatment (32% of whom with multiple drugs), predominantly extended-release tolterodine or oxybutynin. Baseline differences in impairment were seen between groups (P<.0001) in 5 of 10 KHQ domains (trend for increasing severity: naive < recently discontinued < lapsed). At study end, all KHQ domains except general health perception showed significant improvement (P<.0001). Magnitude of response was similar between groups in 6 domains, with greater improvement among lapsed and naive patients in 4 domains.Conclusions: OAB patients benefit from transdermal oxybutynin, regardless of treatment history.Clinical Pharmacology & Therapeutics (2005) 79, P82–P82; doi: 10.1016/j.clpt.2005.12.293 [ABSTRACT FROM AUTHOR]

Published

2006

17. Crustal stress in the northern North Sea as inferred from borehole breakouts and earthquake focal mechanisms

Author

Dahl, N., Atakan, K., Aadnoy, B. S., Bratli, R. K., Bungum, J., Torudbakken, B., and Lindholm, C. D.

Subjects

EARTHQUAKES, GEOLOGY

Published

1995

18. Frequency of four cystic fibrosis mutations in a Swedish population.

Author

Dahl, N, Grandell, U, Martinsson, T, Allen, M, Johansson, L, Stolpe, L, Gyllensten, U, Hjelte, L, Kollberg, H, Strandvik, B, Wahlstrom, J, and Anvret, M

Published

1993

19. Recurrent GATA1 mutations in Diamond-Blackfan anaemia.

Author

Klar J, Khalfallah A, Arzoo PS, Gazda HT, and Dahl N

Subjects

Adult, Humans, Male, Pedigree, Recurrence, Young Adult, Anemia, Diamond-Blackfan genetics, GATA1 Transcription Factor genetics, Mutation genetics

Published

2014

20. WNT10A mutations account for ¼ of population-based isolated oligodontia and show phenotypic correlations.

Author

Arzoo PS, Klar J, Bergendal B, Norderyd J, and Dahl N

Subjects

Alleles, Anodontia epidemiology, Female, Genetic Association Studies, Genotype, Humans, Male, Population Surveillance, Sweden epidemiology, Anodontia diagnosis, Anodontia genetics, Mutation, Phenotype, Wnt Proteins genetics

Abstract

A large proportion (>50%) of patients with isolated oligodontia were recently reported with WNT10A mutations. We have analyzed a population-based cohort of 102 individuals diagnosed with non-syndromic oligodontia and a mean of 8.2 missing teeth. The cohort included 94 families and screening of WNT10A identified that 26 probands (27.7%) had at least one WNT10A variant. When we included the MSX1, PAX9, AXIN2, EDA, EDAR, and EDARADD genes, 38.3% of probands were positive for a mutation. Biallelic WNT10A mutations were strongly associated with a larger number of missing teeth (11.09) when compared to both monoallelic WNT10 mutations (6.82) and the group without mutations in WNT10A, MSX1, PAX9, AXIN2, EDA, EDAR, or EDARADD (7.77). Genotype-phenotype analysis of individuals with WNT10A mutations showed that premolars were the most common missing teeth. Furthermore, biallelic WNT10A mutations were associated with absence of maxillary and mandibular molars as well as mandibular central incisors. Maxillary central incisors were always present. Thus, our study indicates that WNT10A mutations are associated with both the type and numbers of missing teeth. Furthermore, we show that this population-based cohort of isolated oligodontia had a considerably lower frequency of mutated WNT10A alleles and a lower mean number of missing teeth when compared to patients recruited from dental specialist centers., (© 2013 Wiley Periodicals, Inc.)

Published

2014

21. Inherited mosaicism for the supernumerary marker chromosome in cat eye syndrome: inter- and intra-individual variation and correlation to the phenotype.

Author

Kvarnung M, Lindstrand A, Malmgren H, Thåström A, Jacobson L, Dahl N, Lundin J, and Blennow E

Subjects

Aneuploidy, Child, Chromosomes, Human, Pair 22 genetics, Eye Abnormalities, Family, Humans, In Situ Hybridization, Fluorescence, Male, Phenotype, Spermatozoa, Chromosome Disorders genetics, Genetic Markers, Mosaicism

Abstract

We have studied a family with repeated transmission of mosaicism for a supernumerary marker chromosome (SMC), giving rise to varying symptoms of the cat eye syndrome (CES) in the offspring. The frequency of the SMC was investigated using FISH with probes from the CES critical region on lymphocytes as well as buccal cells. The same probes were used to study the frequency of the SMC in spermatozoa from the father. The SMC was characterized in detail using array-CGH and was found to correspond to a symmetrical cat eye SMC type I, with two extra copies of the most proximal part of 22q11, not extending into the classical 22q11.2 deletion region. Mosaicism for the SMC was detected in 4 out of 7 family members, the father and all his three children. The degree of mosaicism varied greatly between individuals as well as between tissues, with twice as many cells with the SMC in epithelial cells compared to blood. The highest frequency (almost 50%) was found in spermatozoa from the father. There was a direct correlation between the degree of mosaicism and the symptoms, varying from no obvious symptoms to classical CES. The study confirms the occurrence of direct transmission of SMC-mosaicism in CES. The results indicate that examination of parental epithelial cells should be preferred compared to blood cells in order to exclude a recurrence risk in parents of a child with CES. Interphase FISH analysis of spermatozoa is the most sensitive method to exclude paternal germ line mosaicsm., (Copyright © 2012 Wiley Periodicals, Inc.)

Published

2012

22. Isolated oligodontia associated with mutations in EDARADD, AXIN2, MSX1, and PAX9 genes.

Author

Bergendal B, Klar J, Stecksén-Blicks C, Norderyd J, and Dahl N

Subjects

Axin Protein, Female, Genetic Association Studies, Genetic Predisposition to Disease genetics, Humans, Male, Anodontia genetics, Cytoskeletal Proteins genetics, Edar-Associated Death Domain Protein genetics, MSX1 Transcription Factor genetics, Mutation genetics, PAX9 Transcription Factor genetics

Abstract

Oligodontia is defined as the congenital lack of six or more permanent teeth, excluding third molars. Oligodontia as well as hypodontia (lack of one or more permanent teeth) are highly heritable conditions associated with mutations in the AXIN2, MSX1, PAX9, EDA, and EDAR genes. Here we define the prevalence of mutations in the AXIN2, MSX1, PAX9, EDA, and EDAR genes, and the novel candidate gene EDARADD in a cohort of 93 Swedish probands with non-syndromic, isolated oligodontia. Mutation screening was performed using denaturing gradient gel electrophoresis and DNA sequence analysis. Analyses of the coding sequences of the six genes showed sequence alterations predicted to be damaging or potentially damaging in ten of 93 probands (10.8%). Mutations were identified in the EDARADD (n = 1), AXIN2 (n = 3), MSX1 (n = 2), and PAX9 (n = 4) genes, respectively. None of the 10 probands with mutations had other self-reported symptoms from ectodermal tissues. The oral parameters were similar when comparing individuals with and without mutations but a family history of oligodontia was three times more frequent for probands with mutations. EDARADD mutations have previously been reported in a few families segregating hypohidrotic ectodermal dysplasia and this is, to our knowledge, the first report of an EDARADD mutation associated with isolated oligodontia., (Copyright © 2011 Wiley-Liss, Inc.)

Published

2011

23. Somatic mosaicism for chromosome X and Y aneuploidies in monozygotic twins heterozygous for sickle cell disease mutation.

Author

Razzaghian HR, Shahi MH, Forsberg LA, de Ståhl TD, Absher D, Dahl N, Westerman MP, and Dumanski JP

Subjects

Chromosomes, Human, Pair 18 genetics, Female, Genetic Variation, Genotype, Heterozygote, Humans, Male, Middle Aged, Anemia, Sickle Cell genetics, Aneuploidy, Chromosomes, Human, X genetics, Chromosomes, Human, Y genetics, Turner Syndrome genetics, Twins, Monozygotic genetics

Abstract

Somatic genetic variation in health and disease is poorly explored. Monozygotic (MZ) twins are a suitable model for studies of somatic mosaicism since genetic differences in twins derived from the same zygote represent an irrefutable example of somatic variation. We report the analysis of a pair of generally healthy female MZ twins, discordant for somatic mosaicism for aneuploidy of chromosomes X and Y. Both twins are heterozygous carriers of sickle cell disease mutation. Genotyping of blood DNA from both twins using Illumina Human 610 SNP array revealed a copy number imbalance for chromosome X in a proportion of cells in one twin. Fluorescent in situ hybridization (FISH) analysis confirmed monosomy X (45,X) in 7% of proband nucleated blood cells. Unexpectedly, FISH analysis of cells from the other twin revealed 45,X and 46,XY lineages, both present in 1% of cells. The mechanism behind formation of these aneuploidies suggests several aberrant chromosome segregation events in meiosis and mitoses following conception. Our report contributes to the delineation of the frequency of somatic structural genomic variation in normal MZ twins. These results also illustrate the plasticity of the human genome for tolerating large copy number changes in healthy subjects and show the sensitivity of the Illumina platform for detection of aberrations that are present in a minority of the studied cells., (Copyright © 2010 Wiley-Liss, Inc.)

Published

2010

24. Screening for copy number alterations in loci associated with autism spectrum disorders by two-color multiplex ligation-dependent probe amplification.

Author

Bremer A, Giacobini M, Nordenskjöld M, Brøndum-Nielsen K, Mansouri M, Dahl N, Anderlid B, and Schoumans J

Subjects

Child, Chromosomes, Human, Pair 15, DNA Probes, Humans, Spectral Karyotyping, Child Development Disorders, Pervasive genetics, Gene Dosage, Polymerase Chain Reaction methods

Abstract

The autism spectrum disorder (ASD) is a heterogenous condition characterized by impaired socialization and communication in association with stereotypic behaviors. ASD is highly heritable and heterogeneous with a complex genetic etiology. Recurrent submicroscopic deletions or duplications have been identified in a subgroup of individuals with ASD using array technology. Adequate genetic testing for these genomic imbalances have not yet been widely implemented in the diagnostic setting due to lack of feasible and cost-effective methods as well as difficulties to interpret the clinical significance of these small copy number variants (CNVs). We developed a multiplex ligation-dependent probe amplification (MLPA) assay to investigate its usefulness for detection of copy number alterations (CNAs) in autistic patients. This test proved to be easy to perform, fast, cost-effective, and suitable for reliable detection of multiple loci in a single reaction. We screened 148 autistic patients for 15 different loci covering 26 genes and found a 15q11-13 interstitial duplication that had escaped detection by conventional karyotyping in 1.3% of the patients. Synthetic probe MLPA allows for a flexible analysis of a continuously increasing number of CNAs associated with autism. Our result show that MLPA assay is an easy and cost-effective method for the identification of selected CNAs in diagnostic laboratories., ((c) 2009 Wiley-Liss, Inc.)

Published

2010

25. SPG11 mutations cause Kjellin syndrome, a hereditary spastic paraplegia with thin corpus callosum and central retinal degeneration.

Author

Orlén H, Melberg A, Raininko R, Kumlien E, Entesarian M, Söderberg P, Påhlman M, Darin N, Kyllerman M, Holmberg E, Engler H, Eriksson U, and Dahl N

Subjects

Adolescent, Adult, DNA Mutational Analysis, Female, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Ophthalmology, Pedigree, Positron-Emission Tomography, Retinal Degeneration genetics, Syndrome, Abnormalities, Multiple genetics, Corpus Callosum pathology, Mutation genetics, Proteins genetics, Retinal Degeneration complications, Spastic Paraplegia, Hereditary complications, Spastic Paraplegia, Hereditary genetics

Abstract

Autosomal recessive hereditary spastic paraplegia (ARHSP) with thin corpus callosum (TCC) is genetically heterogenous and approximately 35% of patients carry mutations in either of the SPG11 or SPG15 genes. Disease onset is during the first three decades of life with spastic paraplegia and mental impairment. Peripheral neuropathy and amyotrophy may occur. Kjellin syndrome is characterized by central retinal degeneration in addition to ARHSP-TCC and the disease is associated with mutations in the SPG15 gene. We identified five patients in four unrelated kindreds with spastic paraplegia and mental impairment. Magnetic resonance imaging revealed TCC, atrophy elsewhere in the brain and increased T2 signal intensity in the periventricular white matter. Probands from the four kindreds were screened for mutations in the SPG11 gene. All patients were found homozygous or compound heterozygous for truncating SPG11 mutations of which four are reported for the first time. Ophthalmological investigations revealed that the four index cases have central retinal degeneration consistent with Kjellin syndrome. PET examinations with N-[11C-methyl]-L-deuterodeprenyl (DED) and fluor-18 2-fluorodeoxyglucose (FDG) were performed in two patients with Kjellin syndrome. We observed a reduced glucose uptake in the thalami, anterior cingulum, and sensorimotor cortex indicating neuronal loss, and an increased DED binding in the thalami and pons which suggests astrogliosis. From our results we extend the SPG11 associated phenotype to comprise also Kjellin syndrome, previously found to be associated with mutations in the SPG15 gene. We anticipate that degeneration of the central retina is a common and previously unrecognized feature in SPG11 related disease., ((c) 2009 Wiley-Liss, Inc.)

Published

2009

26. Calculating contingencies in natural environments: issues in the application of sequential analysis.

Author

McComas JJ, Moore T, Dahl N, Hartman E, Hoch J, and Symons F

Subjects

Child, Preschool, Female, Humans, Male, Social Environment, Child Behavior, Social Behavior, Statistics as Topic methods

Abstract

Analysis and interpretation of behavior-environment relations are increasingly being conducted with data that have been derived descriptively. This paper provides an overview of the logic that underlies a sequential analytic approach to the analysis of descriptive data. Several methods for quantifying sequential relations are reviewed along with their strengths and weaknesses. Data from descriptive analyses are used to illustrate key points. Issues germane to contingency analysis in natural environments are discussed briefly. It is concluded that the conceptual distinctions among contiguity, contingency, and dependency are critical if the logic of sequential analysis is to be extended successfully to a behavior-analytic account of reinforcement in natural environments.

Published

2009

27. A chromosome 10 variant with a 12 Mb inversion [inv(10)(q11.22q21.1)] identical by descent and frequent in the Swedish population.

Author

Entesarian M, Carlsson B, Mansouri MR, Stattin EL, Holmberg E, Golovleva I, Stefansson H, Klar J, and Dahl N

Subjects

Amniocentesis, Chi-Square Distribution, Chromosome Breakage, Chromosomes, Artificial, Bacterial, Cloning, Molecular, Cytogenetic Analysis, Genetic Markers, Geography, Haplotypes, Heterozygote, Humans, In Situ Hybridization, Fluorescence, Microsatellite Repeats, Polymerase Chain Reaction, Population Groups, Sequence Analysis, DNA, Sweden, Chromosome Inversion, Chromosomes, Human, Pair 10, Gene Frequency, Genetic Variation

Abstract

We identified a paracentric inversion of chromosome 10 [inv(10)(q11.22q21.1)] in 0.20% of Swedish individuals (15/7,439) referred for cytogenetic analysis. A retrospective analysis of 8,896 karyotypes from amniocenteses in Sweden revealed a carrier frequency of 0.079% (7/8,896) for the inversion. Cloning and detailed analysis of the inversion breakpoint regions show enrichment for interspersed repeat elements and AT-stretches. The centromeric breakpoint coincides with that of a predicted inversion from HapMap data, which suggests that this region is involved in several chromosome 10 variants. No known gene or predicted transcript are disrupted by the inversion which spans approximately 12 Mb. Carriers from four non-related Swedish families have identical inversion breakpoints and haplotype analysis confirmed that the rearrangement is identical by descent. Diagnosis was retrieved in 6 out of the 15 carriers referred for cytogenetic analysis. No consistent phenotype was found to be associated with the inversion. Our study demonstrates that the inv(10)(q11.22q21.1) is a rare and inherited chromosome variant with a broad geographical distribution in Sweden., (2009 Wiley-Liss, Inc.)

Published

2009

28. Diagnosing and treating Diamond Blackfan anaemia: results of an international clinical consensus conference.

Author

Vlachos A, Ball S, Dahl N, Alter BP, Sheth S, Ramenghi U, Meerpohl J, Karlsson S, Liu JM, Leblanc T, Paley C, Kang EM, Leder EJ, Atsidaftos E, Shimamura A, Bessler M, Glader B, and Lipton JM

Subjects

Adult, Anemia, Diamond-Blackfan complications, Anemia, Diamond-Blackfan genetics, Child, Congenital Abnormalities etiology, Diagnosis, Differential, Erythrocyte Transfusion, Female, Genetic Predisposition to Disease, Glucocorticoids therapeutic use, Hematopoietic Stem Cell Transplantation, Humans, Neoplasms etiology, Pregnancy, Pregnancy Complications, Hematologic therapy, Treatment Outcome, Anemia, Diamond-Blackfan diagnosis, Anemia, Diamond-Blackfan therapy

Abstract

Diamond Blackfan anaemia (DBA) is a rare, genetically and clinically heterogeneous, inherited red cell aplasia. Classical DBA affects about seven per million live births and presents during the first year of life. However, as mutated genes have been discovered in DBA, non-classical cases with less distinct phenotypes are being described in adults as well as children. In caring for these patients it is often difficult to have a clear understanding of the treatment options and their outcomes because of the lack of complete information on the natural history of the disease. The purpose of this document is to review the criteria for diagnosis, evaluate the available treatment options, including corticosteroid and transfusion therapies and stem cell transplantation, and propose a plan for optimizing patient care. Congenital anomalies, mode of inheritance, cancer predisposition, and pregnancy in DBA are also reviewed. Evidence-based conclusions will be made when possible; however, as in many rare diseases, the data are often anecdotal and the recommendations are based upon the best judgment of experienced clinicians. The recommendations regarding the diagnosis and management described in this report are the result of deliberations and discussions at an international consensus conference.

Published

2008

29. Kostmann syndrome or infantile genetic agranulocytosis, part two: Understanding the underlying genetic defects in severe congenital neutropenia.

Author

Carlsson G, Melin M, Dahl N, Ramme KG, Nordenskjöld M, Palmblad J, Henter JI, and Fadeel B

Subjects

Adaptor Proteins, Signal Transducing, Apoptosis genetics, DNA-Binding Proteins genetics, Genes, Recessive, Granulocyte Colony-Stimulating Factor, Humans, Infant, Leukemia genetics, Leukocyte Elastase genetics, Mutation, Myeloid Progenitor Cells physiology, Neoplasms, Second Primary etiology, Neutropenia congenital, Pedigree, Proteins genetics, Receptors, Granulocyte Colony-Stimulating Factor genetics, Syndrome, Transcription Factors genetics, Neutropenia genetics

Abstract

Unlabelled: Congenital neutropenia in man was first reported 50 years ago by the Swedish paediatrician Rolf Kostmann. He coined the term 'infantile genetic agranulocytosis' for this condition, which is now known as Kostmann syndrome. Recent studies have revealed mutations in ELA-2, encoding the neutrophil granule protease, neutrophil elastase, in autosomal dominant neutropenia, and mutations in HAX-1, encoding an anti-apoptotic protein, in autosomal recessive neutropenia., Conclusion: Future studies should aim to clarify the mechanisms underlying the evolution of secondary malignancies in these patients.

Published

2007

30. Adult-onset autosomal dominant leukodystrophy with autonomic symptoms restricted to 1.5 Mbp on chromosome 5q23.

Author

Marklund L, Melin M, Melberg A, Giedraitis V, and Dahl N

Subjects

Adult, Base Pairing, Base Sequence, DNA Primers, Female, Genetic Linkage, Haplotypes, Humans, Male, Pedigree, Chromosomes, Human, Pair 5, Sphingolipidoses genetics

Abstract

Autosomal dominant leukodystrophy (ADLD) with autonomic symptoms is a slowly progressive leukodystrophy with an onset in the 4th to 6th decade of life. Early symptoms are derived from the autonomic nervous system with bladder dysfunction in the majority of patients. The disease progresses slowly with loss of fine motor skills, ataxia, and affected individuals may survive for two decades after onset of symptoms. The molecular basis behind ADLD remains unknown but the causative locus was previously mapped to a 4 cM region on chromosome 5. We have recently identified a large family of Swedish origin with this type of ADLD. Linkage analysis on samples from family members confirmed linkage to 5q23 and supports genetic homogeneity for the disease. We fine mapped and localized the ADLD gene to a 0.96 cM region between D5S1495 and CTT/CCT15. A maximum parametric multipoint location score of 9.45 was obtained for a position at the marker CTT55. From our results we conclude that the ADLD gene locus is restricted to a 1.47 Mbp interval containing 13 known or putative genes.

Published

2006

31. A Meniere's disease gene linked to chromosome 12p12.3.

Author

Klar J, Frykholm C, Friberg U, and Dahl N

Subjects

Family Health, Female, Genetic Linkage, Genetic Predisposition to Disease genetics, Genotype, Haplotypes, Humans, Lod Score, Male, Microsatellite Repeats genetics, Pedigree, Phosphatidylinositol 3-Kinases genetics, Protein Subunits genetics, Chromosome Mapping methods, Chromosomes, Human, Pair 12 genetics, Meniere Disease genetics

Abstract

Meniere's disease (MD) is characterized by spontaneous attacks of vertigo, fluctuating sensorineural hearing loss, tinnitus, and aural fullness. The majority of patients with MD appear sporadic but 5%-13% of the cases have a family history for the disease. The cause of both the sporadic and inherited forms of MD remains unclear despite a number of candidate genes defined from their association with hearing loss. We have performed a genome wide linkage scan on a large Swedish family segregating MD in five generations. Five candidate regions with a lod score of >1 were identified. Two additional families with autosomal dominant MD were analyzed for linkage to these regions and a cumulative Z(max) of 3.46 was obtained for a single region on chromosome 12p. In two of the three families, a shared haplotype was found to extend over 1.7 Mb which suggests a common ancestral origin. Within this region, a single recombination event restricts the candidate region to 463 kb., ((c) 2006 Wiley-Liss, Inc.)

Published

2006

32. Familial transient erythroblastopenia of childhood is associated with the chromosome 19q13.2 region but not caused by mutations in coding sequences of the ribosomal protein S19 (RPS19) gene.

Author

Gustavsson P, Klar J, Matsson H, Forestier E, Henter JI, Rao S, Seip M, Skeppner G, and Dahl N

Subjects

Adult, Child, Genetic Linkage genetics, Genotype, Humans, Mutation genetics, Pedigree, Sequence Analysis, Chromosomes, Human, Pair 19 genetics, Erythroblasts, Hematologic Diseases genetics, Ribosomal Proteins genetics

Abstract

Transient erythroblastopenia of childhood (TEC) is a rare condition, which at onset may be difficult to distinguish from Diamond-Blackfan anaemia (DBA). We have previously shown that mutations in the ribosomal protein S19 gene (RPS19) cause DBA. In order to clarify whether TEC and DBA are allelic, we investigated the segregation of markers spanning the RPS19 gene region on chromosome 19q13.2 and performed sequence analysis of all exons in the RPS19 gene in seven TEC sibling pairs. Linkage analysis supported allelism for TEC and DBA at the RPS19 gene locus and implies molecular mechanisms other than structural mutations in the RPS19 gene.

Published

2002

33. Diamond-Blackfan anaemia in the Italian population.

Author

Ramenghi U, Garelli E, Valtolina S, Campagnoli MF, Timeus F, Crescenzio N, Mair M, Varotto S, D'Avanzo M, Nobili B, Massolo F, Mori PG, Locatelli F, Gustavsson P, Dahl N, and Dianzani I

Subjects

Child, Child, Preschool, Chromosome Aberrations, Chromosome Segregation, Fanconi Anemia epidemiology, Female, Humans, Incidence, Infant, Infant, Newborn, Italy epidemiology, Male, Pedigree, Fanconi Anemia genetics

Abstract

Diamond-Blackfan anaemia (DBA) is a congenital disease characterized by defective erythroid progenitor maturation: 30% of patients have congenital malformations. The link between these malformations and defective erythropoiesis is unclear: a defect in a molecule acting both on embryo development and haemopoiesis has been proposed. Inheritance is autosomal dominant in most familial cases, but recessive families have also been reported. Many cases are sporadic. A DBA locus has been mapped on chromosome 19q13.2 (Gustavsson et al, 1997), but several families unlinked to this locus have also been reported (Gustavsson et al, 1998). This paper presents clinical, epidemiological and molecular data for DBA in the Italian population. Segregation analysis of 19q markers in patients with DBA showed exclusion of this locus in 5/12 families with inherited DBA. There was evidently locus heterogeneity for DBA in this population. A new microdeletion was identified in one patient. Other families, in which DBA segregates concordantly with the 19q critical region, suggest incomplete penetrance and expressivity of the DBA gene.

Published

1999