Your search keyword '"Bras J"' showing total 18 results

1. KCNN2 mutation in autosomal‐dominant tremulous myoclonus‐dystonia.

Author

Balint, B., Guerreiro, R., Carmona, S., Dehghani, N., Latorre, A., Cordivari, C., Bhatia, K. P., and Bras, J.

Subjects

MYOCLONUS, CALCIUM-dependent potassium channels, POTASSIUM channels

Abstract

Background and purpose: Despite recent advances in neurogenetics that have facilitated the identification of a number of dystonia genes, many familial dystonia syndromes remain without known cause. The aim of the study was to identify the cause of autosomal dominant tremulous myoclonus‐dystonia in a UK kindred with affected individuals in three generations. Methods: Known genetic causes of myoclonus‐dystonia were excluded. We combined clinical and electrophysiological phenotyping with whole‐exome sequencing and Sanger sequencing to identify candidate causal variants in a family with tremulous myoclonus‐dystonia. Results: The core phenotype consisted of childhood‐onset dystonia predominantly affecting hands and neck, with a fast tremor with superimposed myoclonus and, in some individuals, subtle cerebellar signs. We identified a novel missense variant in potassium calcium‐activated channel subfamily N member 2 (KCNN2) [NM_021614:c.1112G>A:p.(Gly371Glu)], which was the only variant that we were able to identify as segregating with the phenotype over three generations. This variant, which is absent from the most recent version of gnomAD, was predicted to be deleterious by SIFT and PolyPhen‐2 and had an overall CADD score of 29.7. Conclusions: KCNN2, a member of the KCNN family of potassium channel genes, is highly conserved across species and in humans is highly expressed in the brain, particularly the cerebellum. KCNN2 mutations have never been described as pathological in human disease, but are recognized abnormalities in two rodent models of fast, jerky tremor. Segregation, absence of the variant in the normal population and in‐silico prediction of a deleterious effect together with animal models compatible with the clinical phenotype are all in line with KCNN2 mutations being a plausible cause underlying myoclonus‐dystonia. [ABSTRACT FROM AUTHOR]

Published

2020

2. Whole‐exome sequencing of the BDR cohort: evidence to support the role of the PILRA gene in Alzheimer's disease.

Author

Patel, T., Brookes, K. J., Turton, J., Chaudhury, S., Guetta‐Baranes, T., Guerreiro, R., Bras, J., Hernandez, D., Singleton, A., Francis, P. T., Hardy, J., and Morgan, K.

Subjects

ALZHEIMER'S disease, NEUROLOGICAL disorders, GENOMES, EXOMES, PARKINSON'S disease, DEMENTIA

Abstract

Aim: Late‐onset Alzheimer's disease (LOAD) accounts for 95% of all Alzheimer's cases and is genetically complex in nature. Overlapping clinical and neuropathological features between AD, FTD and Parkinson's disease highlight the potential role of genetic pleiotropy across diseases. Recent genome‐wide association studies (GWASs) have uncovered 20 new loci for AD risk; however, these exhibit small effect sizes. Using NGS, here we perform association analyses using exome‐wide and candidate‐gene‐driven approaches. Methods: Whole‐exome sequencing was performed on 132 AD cases and 53 control samples. Exome‐wide single‐variant association and gene burden tests were performed for 76 640 nonsingleton variants. Samples were also screened for known causative mutations in familial genes in AD and other dementias. Single‐variant association and burden analysis was also carried out on variants in known AD and other neurological dementia genes. Results: Tentative single‐variant and burden associations were seen in several genes with kinase and protease activity. Exome‐wide burden analysis also revealed significant burden of variants in PILRA (P = 3.4 × 10−5), which has previously been linked to AD via GWAS, hit ZCWPW1. Screening for causative mutations in familial AD and other dementia genes revealed no pathogenic variants. Variants identified in ABCA7, SLC24A4, CD33 and LRRK2 were nominally associated with disease (P < 0.05) but did not withstand correction for multiple testing. APOE (P = 0.02) and CLU (P = 0.04) variants showed significant burden on AD. Conclusions: In addition, polygenic risk scores (PRS) were able to distinguish between cases and controls with 83.8% accuracy using 3268 variants, sex, age at death and APOE ε4 and ε2 status as predictors. [ABSTRACT FROM AUTHOR]

Published

2018

3. Is APOE ε4 required for Alzheimer's disease to develop in TREM2 p.R47H variant carriers?

Author

Guerreiro, R., Orme, T., Naj, A. C., Kuzma, A. B., Schellenberg, G. D., and Bras, J.

Subjects

ALZHEIMER'S disease, APOLIPOPROTEIN E4, ALLELES

Published

2019

4. Bilateral ceratohyoidectomy for the resolution of clinical signs associated with temporohyoid osteoarthropathy.

Author

Bras, J. J., Davis, E., and Beard, W. L.

Subjects

*JOINT diseases, *SYMPTOMS, *TEMPORAL bone, *PAIN management, *BONE fractures, *TONGUE, *LARYNX

Abstract

Temporohyoid osteoarthropathy (THO) is a progressive bilateral disease of unknown aetiology that most commonly affects adult horses. Irrespective of aetiology, THO frequently results in pain or fracture of the petrous temporal bone during normal movement of the tongue and larynx. In an effort to decrease pain and reduce the likelihood of petrous temporal bone fracture, partial stylohyoidectomy and ceratohyoidectomy have been developed. Serious complications have been reported following stylohyoidectomy and therefore the current recommendation is to perform unilateral ceratohyoidectomy. Benefits of ceratohyoidectomy include a lower risk of vascular and nerve damage and a reduced risk of clinical signs recurrence when compared with stylohyoidectomy. This report describes a case of THO in which clinical signs recurred approximately 2 years after unilateral ceratohyoidectomy was performed. Due to this complication, resection of the contralateral ceratohyoid bone was performed, which resulted in complete resolution of clinical signs. Although the clinical signs are frequently unilateral, the disease is most commonly a progressive bilateral condition and some horses may not have complete resolution of clinical signs when unilateral ceratohyoidectomy is performed. Therefore, if clinical signs persist after unilateral ceratohyoidectomy, a therapeutic consideration should include bilateral ceratohyoidectomy. This report suggests a favourable short-term prognosis for a horse treated with bilateral ceratohyoidectomy. [ABSTRACT FROM AUTHOR]

Published

2014

5. Consequences of shoaling of the Central American Seaway determined from modeling Nd isotopes.

Author

Sepulchre, P., Arsouze, T., Donnadieu, Y., Dutay, J.-C., Jaramillo, C., Le Bras, J., Martin, E., Montes, C., and Waite, A. J.

Published

2014

6. Exome sequencing in Parkinson's disease.

Author

Bras, J. M. and Singleton, A. B.

Subjects

*GENETIC research, *GENOMICS, *PARKINSON'S disease & genetics, *GENETIC mutation, *PATHOLOGY

Abstract

Exome sequencing is rapidly becoming a fundamental tool for genetics and functional genomics laboratories. This methodology has enabled the discovery of novel pathogenic mutations causing mendelian diseases that had, until now, remained elusive. In this review, we discuss not only how we envisage exome sequencing being applied to a complex disease, such as Parkinson's disease, but also what are the known caveats of this approach. [ABSTRACT FROM AUTHOR]

Published

2011

7. Dysautonomia in a six-year-old mule in the United States.

Author

WRIGHT, A., BEARD, L., BAWA, B., and BRAS, J.

Abstract

Equine dysautonomia, also known as equine grass sickness (EGS), is a well documented disease in several countries. To the authors' knowledge, EGS has not been reported previously in North America. This report describes EGS in a 6-year-old female mule in the USA. Failure initially to consider EGS resulted in a delayed diagnosis. EGS should be considered as a differential diagnosis and appropriate diagnostic tests performed in similar cases in North America. [ABSTRACT FROM AUTHOR]

Published

2010

8. Epidermal growth factor receptor targeting enhances adenoviral vector based suicide gene therapy of osteosarcoma.

Author

Witlox, M. A., van Beusechem, V. W., Grill, J., Haisma, H. J., Schaap, G., Bras, J., van Diest, P., de Gast, A., Curiel, D. T., Pinedo, H. M., Gerritsen, W. R., and Wuisman, P. I. J. M.

Published

2002

9. In vitro antimalarial activity, chloroquine potentiating effect and cytotoxicity of alkaloids of Hernandia voyronii Jum. (Hernandiaceae).

Author

Ratsimamanga-Urverg, S., Rasoanaivo, P., Milijaona, R., Rakotoarimanga, J., Rafatro, H., Robijaona, B., Rakoto-Ratsimamanga, A., Verdier, F., and le Bras, J.

Published

1994

10. In vitro activity of the enantiomers of mefloquine, halofantrine and enpiroline against Plasmodium falciparum.

Author

Basco, LK, Gillotin, C, Gimenez, F, Farinotti, R, and Bras, J

Abstract

The in vitro activity of the enantiomers of mefloquine, halofantrine and enpiroline was compared against chloroquine-resistant and - susceptible strains of Plasmodium falciparum using a semi-micro drug susceptibility test. For each strain, the corresponding enantiomers exhibited similar activities. The enantiomers of halofantrine were the most active against both susceptible and resistant strains, followed by the enantiomers of mefloquine and enpiroline. [ABSTRACT FROM AUTHOR]

Published

1992

11. Young-onset parkinsonism due to homozygous duplication of α-synuclein in a consanguineous family.

Author

Kojovic M, Sheerin UM, Rubio-Agusti I, Saha A, Bras J, Gibbons V, Palmer R, Houlden H, Hardy J, Wood NW, Bhatia KP, Kojovic, Maja, Sheerin, Una-Marie, Rubio-Agusti, Ignacio, Saha, Anirban, Bras, Jose, Gibbons, Vaneesha, Palmer, Rodger, Houlden, Henry, and Hardy, John

Published

2012

12. ChemInform Abstract: A Convenient Synthesis of γ,δ-Unsaturated N-Formylenamines by Wittig Alkenylation of γ,δ-Unsaturated Diformamides.

Author

VAN VLIET, M. C. A., MEUZELAAR, G. J., BRAS, J., MAAT, L., and SHELDON, R. A.

Published

1997

13. Genetic analysis reveals novel variants for vascular cognitive impairment.

Author

Mönkäre S, Kuuluvainen L, Schleutker J, Bras J, Roine S, Pöyhönen M, Guerreiro R, and Myllykangas L

Subjects

3' Untranslated Regions, Genetic Testing, High-Temperature Requirement A Serine Peptidase 1 genetics, Humans, Cerebral Small Vessel Diseases complications, Cognitive Dysfunction complications, Cognitive Dysfunction genetics, Dementia, Vascular diagnosis, Dementia, Vascular genetics, Stroke complications

Abstract

Objectives: The genetic background of vascular cognitive impairment (VCI) is poorly understood compared to other dementia disorders. The aim of the study was to investigate the genetic background of VCI in a well-characterized Finnish cohort., Materials & Methods: Whole-exome sequencing (WES) was applied in 45 Finnish VCI patients. Copy-number variant (CNV) analysis using a SNP array was performed in 80 VCI patients. This study also examined the prevalence of variants at the miR-29 binding site of COL4A1 in 73 Finnish VCI patients., Results: In 40% (18/45) of the cases, WES detected possibly causative variants in genes associated with cerebral small vessel disease (CSVD) or other neurological or stroke-related disorders. These variants included HTRA1:c.847G>A p.(Gly283Arg), TREX1:c.1079A>G, p.(Tyr360Cys), COLGALT1:c.1411C>T, p.(Arg471Trp), PRNP: c.713C>T, p.(Pro238Leu), and MTHFR:c.1061G>C, p.(Gly354Ala). Additionally, screening of variants in the 3'UTR of COL4A1 gene in a sub-cohort of 73 VCI patients identified a novel variant c.*36T>A. CNV analysis showed that pathogenic CNVs are uncommon in VCI., Conclusions: These data support pathogenic roles of variants in HTRA1, TREX1 and in the 3'UTR of COL4A1 in CSVD and VCI, and suggest that vascular pathogenic mechanisms are linked to neurodegeneration, expanding the understanding of the genetic background of VCI., (© 2022 The Authors. Acta Neurologica Scandinavica published by John Wiley & Sons Ltd.)

Published

2022

14. Cytologic features and diagnostic value of PeriView FLEX transbronchial needle aspiration targeting pulmonary nodules.

Author

Naso J, Bras J, Villamil C, Ionescu DN, Wang G, Shaipanich T, Beaudoin EL, Myers R, Lam S, and Zhou C

Subjects

Adult, Aged, Aged, 80 and over, Female, Follow-Up Studies, Humans, Lung Neoplasms diagnostic imaging, Male, Middle Aged, Multiple Pulmonary Nodules diagnostic imaging, Prognosis, Retrospective Studies, Solitary Pulmonary Nodule diagnostic imaging, Endoscopic Ultrasound-Guided Fine Needle Aspiration methods, Lung Neoplasms diagnosis, Multiple Pulmonary Nodules diagnosis, Solitary Pulmonary Nodule diagnosis

Abstract

Background: Transbronchial needle aspiration (TBNA) of peripheral lung nodules can be difficult with conventional devices due to their limited flexibility. A promising new technology for accessing these lesions is the PeriView FLEX TBNA device, which has a flexible spiral-grooved needle. The present study reports the unique cytologic features, diagnostic value, and potential pitfalls of PeriView FLEX TBNA specimens., Methods: This study retrospectively evaluates 113 consecutive cases of lung nodules sampled using the PeriView FLEX device with radial endobronchial ultrasound guidance., Results: PeriView FLEX specimens were satisfactory for evaluation in 111 of 113 cases (98%). A diagnosis of malignancy was made on 64 specimens (57%), with 100% specificity and 70% sensitivity for malignancy. In 4 cases, the PeriView FLEX sample was the only specimen from bronchoscopy that was diagnostic of malignancy. Of the 64 PeriView FLEX specimens with malignant cells, 58 (91%) were adequate for immunohistochemistry and 44 (69%) were adequate for molecular genetic testing. Potential pitfalls were largely ameliorated through education regarding the unique features of PeriView FLEX samples, such as the expected abundance of anthracotic pigment and the paucity of lymphocytes., Conclusions: TBNA using the PeriView FLEX device to sample pulmonary nodules contributed to the diagnostic value of bronchoscopy and tended to provide sufficient tissue for ancillary studies. Many of the possible pitfalls may be avoided through consideration of the unique cytologic features associated with this novel sampling method., (© 2020 American Cancer Society.)

Published

2020

15. Primary familial brain calcification linked to deletion of 5' noncoding region of SLC20A2.

Author

Pasanen P, Mäkinen J, Myllykangas L, Guerreiro R, Bras J, Valori M, Viitanen M, Baumann M, Tienari PJ, Pöyhönen M, and Baumann P

Subjects

5' Flanking Region, Brain Diseases diagnosis, Calcinosis diagnosis, DNA Copy Number Variations, Exome, Female, Heterozygote, Humans, Male, Pedigree, Point Mutation, Xenotropic and Polytropic Retrovirus Receptor, Brain Diseases genetics, Calcinosis genetics, Gene Deletion, Sodium-Phosphate Cotransporter Proteins, Type III genetics

Abstract

Objectives: Primary familial brain calcification (PFBC) is a rare neurological disease often inherited as a dominant trait. Mutations in four genes (SLC20A2, PDGFB, PDGFRB, and XPR1) have been reported in patients with PFBC. Of these, point mutations or small deletions in SLC20A2 are most common. Thus far, only one large deletion covering entire SLC20A2 and several smaller, exonic deletions of SLC20A2 have been reported. The aim of this study was to identify the causative gene defect in a Finnish PFBC family with three affected patients., Materials and Methods: A Finnish family with three PFBC patients and five unaffected subjects was studied. Sanger sequencing was used to exclude mutations in the coding and splice site regions of SLC20A2, PDGFRB, and PDGFB. Whole-exome (WES) and whole-genome sequencing (WGS) were performed to identify the causative mutation. A SNP array was used in segregation analysis., Results: Copy number analysis of the WGS data revealed a heterozygous deletion of ~578 kb on chromosome 8. The deletion removes the 5' UTR region, the noncoding exon 1 and the putative promoter region of SLC20A2 as well as the coding regions of six other genes., Conclusions: Our results support haploinsufficiency of SLC20A2 as a pathogenetic mechanism in PFBC. Analysis of copy number variations (CNVs) is emerging as a crucial step in the molecular genetic diagnostics of PFBC, and it should not be limited to coding regions, as causative variants may reside in the noncoding parts of known disease-associated genes., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2017

16. PTEN hamartoma tumor syndrome and Gorham-Stout phenomenon.

Author

Hopman SM, Van Rijn RR, Eng C, Bras J, Alders M, van der Horst CM, Hennekam RC, and Merks JH

Subjects

Family, Fatal Outcome, Germ-Line Mutation, Hamartoma Syndrome, Multiple genetics, Heterozygote, Humans, Infant, Male, Osteolysis, Essential genetics, PTEN Phosphohydrolase genetics, Hamartoma Syndrome, Multiple diagnosis, Osteolysis, Essential diagnosis

Abstract

PTEN: hamartoma tumor syndrome (PHTS) is a group of syndromes caused by mutations in PTEN. Gorham-Stout phenomenon (GSP) is a rare condition characterized by proliferation of vascular structures in bones, resulting in progressive osteolysis. Here we present a 1-year-old boy with PHTS and GSP. The lesion that later proved to be GSP was evident from the age of 4 months, and became symptomatic at the age of 1 year. Eventually, he developed a fatal chylothorax. Mutation analysis revealed a germline heterozygous mutation c.517 C>T (p.Arg173Cys) in exon 6 of PTEN. Analysis of the lymphatic malformation (LM) tissue revealed no loss of heterozygosity (LOH) nor a second, somatic PTEN mutation of the remaining wild type allele. The germline p.Arg173Cys mutation was also present in the mother and the propositus' younger sister and brother. Further molecular work-up showed a heterozygous variant c.2180C>T (p.Ala727Val) FLT4 in the LM tissue, which was also present in the germline of mother and two siblings. GSP has not been reported before in a patient with a PTEN mutation. Up to this date, this mutation is the only genetic defect possibly involved in the etiology of GSP which is plausible given the known function of PTEN in angiogenic signaling., (Copyright © 2012 Wiley Periodicals, Inc.)

Published

2012

17. Mediators of structural remodeling in peripheral spondylarthritis.

Author

Vandooren B, Yeremenko N, Noordenbos T, Bras J, Tak PP, and Baeten D

Subjects

Animals, Arthritis, Rheumatoid metabolism, Arthritis, Rheumatoid physiopathology, Biomarkers metabolism, Cartilage, Articular metabolism, Cell Differentiation, Cytokines metabolism, Disease Models, Animal, Humans, Joints metabolism, Mesenchymal Stem Cells cytology, Mesenchymal Stem Cells physiology, Spondylarthritis physiopathology, Synovial Membrane metabolism, Synovial Membrane pathology, Bone Remodeling physiology, Spondylarthritis metabolism

Published

2009

18. In vitro activity of chloroquine and quinine in combination with desferrioxamine against Plasmodium falciparum.

Author

Basco LK and Le Bras J

Subjects

Animals, Anti-Bacterial Agents, Drug Resistance, Microbial genetics, Drug Therapy, Combination, Humans, Plasmodium falciparum genetics, Chloroquine pharmacology, Deferoxamine pharmacology, Plasmodium falciparum drug effects, Quinine pharmacology

Abstract

The activity of chloroquine and quinine, alone and in combination with desferrioxamine (7 mumol/liter), was evaluated in vitro against susceptible and resistant clones of Plasmodium falciparum by a semimicroassay system. The addition of desferrioxamine had no effect on the activity of chloroquine against both clones. Desferrioxamine had no effect on the activity of quinine against the susceptible clone but had slightly enhanced quinine action against the resistant clone. Further development of desferrioxamine as an antimalarial drug may be of limited interest.

Published

1993