Your search keyword '"Brunkow, ME"' showing total 34 results

1. Whole-genome sequencing suggests a chemokine gene cluster that modifies age at onset in familial Alzheimer's disease

Author

Lalli, MA, Bettcher, BM, Arcila, ML, Garcia, G, Guzman, C, Madrigal, L, Ramirez, L, Acosta-Uribe, J, Baena, A, Wojta, KJ, Coppola, G, Fitch, R, De Both, MD, Huentelman, MJ, Reiman, EM, Brunkow, ME, Glusman, G, Roach, JC, Kao, AW, Lopera, F, and Kosik, KS

Subjects

Psychiatry, Medical and Health Sciences, Biological Sciences, Psychology and Cognitive Sciences

Abstract

We have sequenced the complete genomes of 72 individuals affected with early-onset familial Alzheimer's disease caused by an autosomal dominant, highly penetrant mutation in the presenilin-1 (PSEN1) gene, and performed genome-wide association testing to identify variants that modify age at onset (AAO) of Alzheimer's disease. Our analysis identified a haplotype of single-nucleotide polymorphisms (SNPs) on chromosome 17 within a chemokine gene cluster associated with delayed onset of mild-cognitive impairment and dementia. Individuals carrying this haplotype had a mean AAO of mild-cognitive impairment at 51.0±5.2 years compared with 41.1±7.4 years for those without these SNPs. This haplotype thus appears to modify Alzheimer's AAO, conferring a large (∼10 years) protective effect. The associated locus harbors several chemokines including eotaxin-1 encoded by CCL11, and the haplotype includes a missense polymorphism in this gene. Validating this association, we found plasma eotaxin-1 levels were correlated with disease AAO in an independent cohort from the University of California San Francisco Memory and Aging Center. In this second cohort, the associated haplotype disrupted the typical age-associated increase of eotaxin-1 levels, suggesting a complex regulatory role for this haplotype in the general population. Altogether, these results suggest eotaxin-1 as a novel modifier of Alzheimer's disease AAO and open potential avenues for therapy.

Published

2015

2. Correction: Alternating Hemiplegia of Childhood: Retrospective Genetic Study and Genotype-Phenotype Correlations in 187 Subjects from the US AHCF Registry.

Author

Viollet, L, Glusman, G, Murphy, KJ, Newcomb, TM, Reyna, SP, Sweney, M, Nelson, B, Andermann, F, Andermann, E, Acsadi, G, Barbano, RL, Brown, C, Brunkow, ME, Chugani, HT, Cheyette, SR, Collins, A, DeBrosse, SD, Galas, D, Friedman, J, Hood, L, Huff, C, Jorde, LB, King, MD, LaSalle, B, Leventer, RJ, Lewelt, AJ, Massart, MB, Mérida, MR, Ptáček, LJ, Roach, JC, Rust, RS, Renault, F, Sanger, TD, Sotero de Menezes, MA, Tennyson, R, Uldall, P, Zhang, Y, Zupanc, M, Xin, W, Silver, K, Swoboda, KJ, Viollet, L, Glusman, G, Murphy, KJ, Newcomb, TM, Reyna, SP, Sweney, M, Nelson, B, Andermann, F, Andermann, E, Acsadi, G, Barbano, RL, Brown, C, Brunkow, ME, Chugani, HT, Cheyette, SR, Collins, A, DeBrosse, SD, Galas, D, Friedman, J, Hood, L, Huff, C, Jorde, LB, King, MD, LaSalle, B, Leventer, RJ, Lewelt, AJ, Massart, MB, Mérida, MR, Ptáček, LJ, Roach, JC, Rust, RS, Renault, F, Sanger, TD, Sotero de Menezes, MA, Tennyson, R, Uldall, P, Zhang, Y, Zupanc, M, Xin, W, Silver, K, and Swoboda, KJ

Published

2015

3. Alternating Hemiplegia of Childhood: Retrospective Genetic Study and Genotype-Phenotype Correlations in 187 Subjects from the US AHCF Registry

Author

Zhou, F, Viollet, L, Glusman, G, Murphy, KJ, Newcomb, TM, Reyna, SP, Sweney, M, Nelson, B, Andermann, F, Andermann, E, Acsadi, G, Barbano, RL, Brown, C, Brunkow, ME, Chugani, HT, Cheyette, SR, Collins, A, DeBrosse, SD, Galas, D, Friedman, J, Hood, L, Huff, C, Jorde, LB, King, MD, LaSalle, B, Leventer, RJ, Lewelt, AJ, Massart, MB, Merida, MR, Ptacek, LJ, Roach, JC, Rust, RS, Renault, F, Sanger, TD, de Menezes, MAS, Tennyson, R, Uldall, P, Zhang, Y, Zupanc, M, Xin, W, Silver, K, Swoboda, KJ, Zhou, F, Viollet, L, Glusman, G, Murphy, KJ, Newcomb, TM, Reyna, SP, Sweney, M, Nelson, B, Andermann, F, Andermann, E, Acsadi, G, Barbano, RL, Brown, C, Brunkow, ME, Chugani, HT, Cheyette, SR, Collins, A, DeBrosse, SD, Galas, D, Friedman, J, Hood, L, Huff, C, Jorde, LB, King, MD, LaSalle, B, Leventer, RJ, Lewelt, AJ, Massart, MB, Merida, MR, Ptacek, LJ, Roach, JC, Rust, RS, Renault, F, Sanger, TD, de Menezes, MAS, Tennyson, R, Uldall, P, Zhang, Y, Zupanc, M, Xin, W, Silver, K, and Swoboda, KJ

Abstract

Mutations in ATP1A3 cause Alternating Hemiplegia of Childhood (AHC) by disrupting function of the neuronal Na+/K+ ATPase. Published studies to date indicate 2 recurrent mutations, D801N and E815K, and a more severe phenotype in the E815K cohort. We performed mutation analysis and retrospective genotype-phenotype correlations in all eligible patients with AHC enrolled in the US AHC Foundation registry from 1997-2012. Clinical data were abstracted from standardized caregivers' questionnaires and medical records and confirmed by expert clinicians. We identified ATP1A3 mutations by Sanger and whole genome sequencing, and compared phenotypes within and between 4 groups of subjects, those with D801N, E815K, other ATP1A3 or no ATP1A3 mutations. We identified heterozygous ATP1A3 mutations in 154 of 187 (82%) AHC patients. Of 34 unique mutations, 31 (91%) are missense, and 16 (47%) had not been previously reported. Concordant with prior studies, more than 2/3 of all mutations are clusteredin exons 17 and 18. Of 143 simplex occurrences, 58 had D801N (40%), 38 had E815K(26%) and 11 had G947R (8%) mutations [corrected].Patients with an E815K mutation demonstrate an earlier age of onset, more severe motor impairment and a higher prevalence of status epilepticus. This study further expands the number and spectrum of ATP1A3 mutations associated with AHC and confirms a more deleterious effect of the E815K mutation on selected neurologic outcomes. However, the complexity of the disorder and the extensive phenotypic variability among subgroups merits caution and emphasizes the need for further studies.

Published

2015

4. Alternating hemiplegia of childhood: Retrospective genetic study and genotype-phenotype correlations in 187 subjects from the US AHCF registry

Author

Viollet, L, Glusman, G, Murphy, KJ, Newcomb, TM, Reyna, SP, Sweney, M, Nelson, B, Andermann, F, Andermann, E, Acsadi, G, Barbano, RL, Brown, C, Brunkow, ME, Chugani, HT, Cheyette, SR, Collins, A, DeBrosse, SD, Galas, D, Friedman, J, Hood, L, Huff, C, Jorde, LB, King, MD, LaSalle, B, Leventer, RJ, Lewelt, AJ, Massart, MB, Mérida, MR, Ptáček, LJ, Roach, JC, Rust, RS, Renault, F, Sanger, TD, De Menezes, MAS, Tennyson, R, Uldall, P, Zhang, Y, Zupanc, M, Xin, W, Silver, K, Swoboda, KJ, Viollet, L, Glusman, G, Murphy, KJ, Newcomb, TM, Reyna, SP, Sweney, M, Nelson, B, Andermann, F, Andermann, E, Acsadi, G, Barbano, RL, Brown, C, Brunkow, ME, Chugani, HT, Cheyette, SR, Collins, A, DeBrosse, SD, Galas, D, Friedman, J, Hood, L, Huff, C, Jorde, LB, King, MD, LaSalle, B, Leventer, RJ, Lewelt, AJ, Massart, MB, Mérida, MR, Ptáček, LJ, Roach, JC, Rust, RS, Renault, F, Sanger, TD, De Menezes, MAS, Tennyson, R, Uldall, P, Zhang, Y, Zupanc, M, Xin, W, Silver, K, and Swoboda, KJ

Abstract

Mutations in ATP1A3 cause Alternating Hemiplegia of Childhood (AHC) by disrupting function of the neuronal Na+/K+ ATPase. Published studies to date indicate 2 recurrent mutations, D801N and E815K, and a more severe phenotype in the E815K cohort. We performed mutation analysis and retrospective genotype-phenotype correlations in all eligible patients with AHC enrolled in the US AHC Foundation registry from 1997-2012. Clinical data were abstracted from standardized caregivers' questionnaires and medical records and confirmed by expert clinicians. We identified ATP1A3 mutations by Sanger and whole genome sequencing, and compared phenotypes within and between 4 groups of subjects, those with D801N, E815K, other ATP1A3 or no ATP1A3 mutations. We identified heterozygous ATP1A3 mutations in 154 of 187 (82%) AHC patients. Of 34 unique mutations, 31 (91%) are missense, and 16 (47%) had not been previously reported. Concordant with prior studies, more than 2/3 of all mutations are clustered in exons 17 and 18. Of 143 simplex occurrences, 58 had D801N (40%), 38 had E815K (26%) and 11 had G937R (8%) mutations. Patients with an E815K mutation demonstrate an earlier age of onset, more severe motor impairment and a higher prevalence of status epilepticus. This study further expands the number and spectrum of ATP1A3 mutations associated with AHC and confirms a more deleterious effect of the E815K mutation on selected neurologic outcomes. However, the complexity of the disorder and the extensive phenotypic variability among subgroups merits caution and emphasizes the need for further studies.

Published

2015

5. Rare variants in neuronal excitability genes influence risk for bipolar disorder

Author

Ament, SA, Szelinger, S, Glusman, G, Ashworth, J, Hou, L, Akula, N, Shekhtman, T, Badner, JA, Brunkow, ME, Mauldin, DE, Stittrich, AB, Rouleau, K, Detera-Wadleigh, SD, Nurnberger, JI, Edenberg, HJ, Gershon, ES, Schork, N, Price, ND, Gelinas, R, Hood, L, Craig, D, McMahon, FJ, Kelsoe, JR, Roach, JC, Ament, SA, Szelinger, S, Glusman, G, Ashworth, J, Hou, L, Akula, N, Shekhtman, T, Badner, JA, Brunkow, ME, Mauldin, DE, Stittrich, AB, Rouleau, K, Detera-Wadleigh, SD, Nurnberger, JI, Edenberg, HJ, Gershon, ES, Schork, N, Price, ND, Gelinas, R, Hood, L, Craig, D, McMahon, FJ, Kelsoe, JR, and Roach, JC

Abstract

We sequenced the genomes of 200 individuals from 41 families multiply affected with bipolar disorder (BD) to identify contributions of rare variants to genetic risk. We initially focused on 3,087 candidate genes with known synaptic functions or prior evidence from genome-wide association studies. BD pedigrees had an increased burden of rare variants in genes encoding neuronal ion channels, including subunits of GABAA receptors and voltage-gated calcium channels. Four uncommon coding and regulatory variants also showed significant association, including a missense variant in GABRA6. Targeted sequencing of 26 of these candidate genes in an additional 3,014 cases and 1,717 controls confirmed rare variant associations in ANK3, CACNA1B, CACNA1C, CACNA1D, CACNG2, CAMK2A, and NGF. Variants in promoters and 5' and 3' UTRs contributed more strongly than coding variants to risk for BD, both in pedigrees and in the case-control cohort. The genes and pathways identified in this study regulate diverse aspects of neuronal excitability. We conclude that rare variants in neuronal excitability genes contribute to risk for BD.

Published

2015

6. Polymorphisms in the sclerosteosis/van Buchem disease gene (SOST) region are associated with bone-mineral density in elderly whites

Author

Uitterlinden, André, Arp, Pascal, Paeper, BW, Charmley, P, Proll, S, Rivadeneira, Fernando, Fang, Y (Yue), van Meurs, Joyce, Britschgi, TB, Latham, JA, Chatzman, RC, Pols, Huib, Brunkow, ME, Uitterlinden, André, Arp, Pascal, Paeper, BW, Charmley, P, Proll, S, Rivadeneira, Fernando, Fang, Y (Yue), van Meurs, Joyce, Britschgi, TB, Latham, JA, Chatzman, RC, Pols, Huib, and Brunkow, ME

Published

2004

7. Multi-Omic characterization of the effects of Ocrelizumab in patients with relapsing-remitting multiple sclerosis.

Author

Kornilov SA, Price ND, Gelinas R, Acosta J, Brunkow ME, Gervasi-Follmar T, Winger RC, Aldershoff D, Lausted C, Troisch P, Smith B, Heath JR, Repovic P, Cohan S, and Magis AT

Subjects

Humans, Female, Adult, Male, Middle Aged, Biomarkers blood, Magnetic Resonance Imaging, B-Cell Activating Factor blood, Proteome drug effects, Proteome metabolism, Treatment Outcome, Multiomics, Antibodies, Monoclonal, Humanized therapeutic use, Antibodies, Monoclonal, Humanized pharmacology, Multiple Sclerosis, Relapsing-Remitting drug therapy, Multiple Sclerosis, Relapsing-Remitting blood, Multiple Sclerosis, Relapsing-Remitting diagnostic imaging, Immunologic Factors therapeutic use, Immunologic Factors pharmacology

Abstract

The study examined changes in the plasma proteome, metabolome, and lipidome of N = 14 patients with relapsing-remitting multiple sclerosis (RRMS) initiating treatment with ocrelizumab, assayed at baseline, 6 months, and 12 months. Analyses of >4000 circulating biomarkers identified depletion of B-cell associated proteins as the early effect observed following ocrelizumab (OCR) initiation, accompanied by the reduction in plasma abundance of cytokines and cytotoxic proteins, markers of neuronaxonal damage, and biologically active lipids including ceramides and lysophospholipids, at 6 months. B-cell depletion was accompanied by decreases in B-cell receptor and cytokine signaling but a pronounced increase in circulating plasma B-cell activating factor (BAFF). This was followed by an upregulation of a number of signaling and metabolic pathways at 12 months. Patients with higher baseline brain MRI lesion load demonstrated both higher levels of cytotoxic and structural proteins in plasma at baseline and more pronounced biomarker change trajectories over time. Digital cytometry identified a putative increase in myeloid cells and a pro-inflammatory subset of T-cells. Therapeutic effects of ocrelizumab extend beyond CD20-mediated B-cell lysis and implicate metabolic reprogramming, juxtaposing the early normalization of immune activation, cytokine signaling and metabolite and lipid turnover in periphery with changes in the dynamics of immune cell activation or composition. We identify BAFF increase following CD20 depletion as a tentative compensatory mechanism that contributes to the reconstitution of targeted B-cells, necessitating further research., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

8. Measurement of Organ-Specific and Acute-Phase Blood Protein Levels in Early Lyme Disease.

Author

Zhou Y, Qin S, Sun M, Tang L, Yan X, Kim TK, Caballero J, Glusman G, Brunkow ME, Soloski MJ, Rebman AW, Scavarda C, Cooper D, Omenn GS, Moritz RL, Wormser GP, Price ND, Aucott JN, and Hood L

Subjects

Adult, Aged, Biomarkers blood, Blotting, Western, Case-Control Studies, Erythema Chronicum Migrans blood, Erythema Chronicum Migrans etiology, Female, Humans, Immunity, Innate, Lyme Disease drug therapy, Lyme Disease etiology, Lyme Disease immunology, Male, Middle Aged, Multivariate Analysis, Organ Specificity, Acute-Phase Proteins analysis, Lyme Disease blood

Abstract

Lyme disease results from infection of humans with the spirochete Borrelia burgdorferi . The first and most common clinical manifestation is the circular, inflamed skin lesion referred to as erythema migrans; later manifestations result from infections of other body sites. Laboratory diagnosis of Lyme disease can be challenging in patients with erythema migrans because of the time delay in the development of specific diagnostic antibodies against Borrelia . Reliable blood biomarkers for the early diagnosis of Lyme disease in patients with erythema migrans are needed. Here, we performed selected reaction monitoring, a targeted mass spectrometry-based approach, to measure selected proteins that (1) are known to be predominantly expressed in one organ (i.e., organ-specific blood proteins) and whose blood concentrations may change as a result of Lyme disease, or (2) are involved in acute immune responses. In a longitudinal cohort of 40 Lyme disease patients and 20 healthy controls, we identified 10 proteins with significantly altered serum levels in patients at the time of diagnosis, and we also developed a 10-protein panel identified through multivariate analysis. In an independent cohort of patients with erythema migrans, six of these proteins, APOA4, C9, CRP, CST6, PGLYRP2, and S100A9, were confirmed to show significantly altered serum levels in patients at time of presentation. Nine of the 10 proteins from the multivariate panel were also verified in the second cohort. These proteins, primarily innate immune response proteins or proteins specific to liver, skin, or white blood cells, may serve as candidate blood biomarkers requiring further validation to aid in the laboratory diagnosis of early Lyme disease.

Published

2020

9. Evolutionary history of Tibetans inferred from whole-genome sequencing.

Author

Hu H, Petousi N, Glusman G, Yu Y, Bohlender R, Tashi T, Downie JM, Roach JC, Cole AM, Lorenzo FR, Rogers AR, Brunkow ME, Cavalleri G, Hood L, Alpatty SM, Prchal JT, Jorde LB, Robbins PA, Simonson TS, and Huff CD

Subjects

Altitude, Cytochrome P-450 Enzyme System genetics, Female, Haplotypes, High-Throughput Nucleotide Sequencing, Humans, Hypoxia-Inducible Factor-Proline Dioxygenases genetics, Male, Molecular Sequence Annotation, Proteins genetics, Receptors, Calcitriol genetics, Tibet, Adaptation, Physiological genetics, Basic Helix-Loop-Helix Transcription Factors genetics, Genome, Human, Selection, Genetic genetics

Abstract

The indigenous people of the Tibetan Plateau have been the subject of much recent interest because of their unique genetic adaptations to high altitude. Recent studies have demonstrated that the Tibetan EPAS1 haplotype is involved in high altitude-adaptation and originated in an archaic Denisovan-related population. We sequenced the whole-genomes of 27 Tibetans and conducted analyses to infer a detailed history of demography and natural selection of this population. We detected evidence of population structure between the ancestral Han and Tibetan subpopulations as early as 44 to 58 thousand years ago, but with high rates of gene flow until approximately 9 thousand years ago. The CMS test ranked EPAS1 and EGLN1 as the top two positive selection candidates, and in addition identified PTGIS, VDR, and KCTD12 as new candidate genes. The advantageous Tibetan EPAS1 haplotype shared many variants with the Denisovan genome, with an ancient gene tree divergence between the Tibetan and Denisovan haplotypes of about 1 million years ago. With the exception of EPAS1, we observed no evidence of positive selection on Denisovan-like haplotypes.

Published

2017

10. Genomic architecture of inflammatory bowel disease in five families with multiple affected individuals.

Author

Stittrich AB, Ashworth J, Shi M, Robinson M, Mauldin D, Brunkow ME, Biswas S, Kim JM, Kwon KS, Jung JU, Galas D, Serikawa K, Duerr RH, Guthery SL, Peschon J, Hood L, Roach JC, and Glusman G

Abstract

Currently, the best clinical predictor for inflammatory bowel disease (IBD) is family history. Over 163 sequence variants have been associated with IBD in genome-wide association studies, but they have weak effects and explain only a fraction of the observed heritability. It is expected that additional variants contribute to the genomic architecture of IBD, possibly including rare variants with effect sizes larger than the identified common variants. Here we applied a family study design and sequenced 38 individuals from five families, under the hypothesis that families with multiple IBD-affected individuals harbor one or more risk variants that (i) are shared among affected family members, (ii) are rare and (iii) have substantial effect on disease development. Our analysis revealed not only novel candidate risk variants but also high polygenic risk scores for common known risk variants in four out of the five families. Functional analysis of our top novel variant in the remaining family, a rare missense mutation in the ubiquitin ligase TRIM11, suggests that it leads to increased nuclear factor of kappa light chain enhancer in B-cells (NF-κB) signaling. We conclude that an accumulation of common weak-effect variants accounts for the high incidence of IBD in most, but not all families we analyzed and that a family study design can identify novel rare variants conferring risk for IBD with potentially large effect size, such as the TRIM11 p.H414Y mutation.

Published

2016

11. Correction: Alternating Hemiplegia of Childhood: Retrospective Genetic Study and Genotype-Phenotype Correlations in 187 Subjects from the US AHCF Registry.

Author

Viollet L, Glusman G, Murphy KJ, Newcomb TM, Reyna SP, Sweney M, Nelson B, Andermann F, Andermann E, Acsadi G, Barbano RL, Brown C, Brunkow ME, Chugani HT, Cheyette SR, Collins A, DeBrosse SD, Galas D, Friedman J, Hood L, Huff C, Jorde LB, King MD, LaSalle B, Leventer RJ, Lewelt AJ, Massart MB, Mérida MR 2nd, Ptáček LJ, Roach JC, Rust RS, Renault F, Sanger TD, Sotero de Menezes MA, Tennyson R, Uldall P, Zhang Y, Zupanc M, Xin W, Silver K, and Swoboda KJ

Published

2015

12. Alternating Hemiplegia of Childhood: Retrospective Genetic Study and Genotype-Phenotype Correlations in 187 Subjects from the US AHCF Registry.

Author

Viollet L, Glusman G, Murphy KJ, Newcomb TM, Reyna SP, Sweney M, Nelson B, Andermann F, Andermann E, Acsadi G, Barbano RL, Brown C, Brunkow ME, Chugani HT, Cheyette SR, Collins A, DeBrosse SD, Galas D, Friedman J, Hood L, Huff C, Jorde LB, King MD, LaSalle B, Leventer RJ, Lewelt AJ, Massart MB, Mérida MR 2nd, Ptáček LJ, Roach JC, Rust RS, Renault F, Sanger TD, Sotero de Menezes MA, Tennyson R, Uldall P, Zhang Y, Zupanc M, Xin W, Silver K, and Swoboda KJ

Subjects

Child, Child, Preschool, Cohort Studies, DNA Mutational Analysis, Female, Genetic Association Studies, Hemiplegia physiopathology, Humans, Infant, Male, Registries, Hemiplegia genetics, Sodium-Potassium-Exchanging ATPase genetics

Abstract

Mutations in ATP1A3 cause Alternating Hemiplegia of Childhood (AHC) by disrupting function of the neuronal Na+/K+ ATPase. Published studies to date indicate 2 recurrent mutations, D801N and E815K, and a more severe phenotype in the E815K cohort. We performed mutation analysis and retrospective genotype-phenotype correlations in all eligible patients with AHC enrolled in the US AHC Foundation registry from 1997-2012. Clinical data were abstracted from standardized caregivers' questionnaires and medical records and confirmed by expert clinicians. We identified ATP1A3 mutations by Sanger and whole genome sequencing, and compared phenotypes within and between 4 groups of subjects, those with D801N, E815K, other ATP1A3 or no ATP1A3 mutations. We identified heterozygous ATP1A3 mutations in 154 of 187 (82%) AHC patients. Of 34 unique mutations, 31 (91%) are missense, and 16 (47%) had not been previously reported. Concordant with prior studies, more than 2/3 of all mutations are clusteredin exons 17 and 18. Of 143 simplex occurrences, 58 had D801N (40%), 38 had E815K(26%) and 11 had G947R (8%) mutations [corrected].Patients with an E815K mutation demonstrate an earlier age of onset, more severe motor impairment and a higher prevalence of status epilepticus. This study further expands the number and spectrum of ATP1A3 mutations associated with AHC and confirms a more deleterious effect of the E815K mutation on selected neurologic outcomes. However, the complexity of the disorder and the extensive phenotypic variability among subgroups merits caution and emphasizes the need for further studies.

Published

2015

13. Rare variants in neuronal excitability genes influence risk for bipolar disorder.

Author

Ament SA, Szelinger S, Glusman G, Ashworth J, Hou L, Akula N, Shekhtman T, Badner JA, Brunkow ME, Mauldin DE, Stittrich AB, Rouleau K, Detera-Wadleigh SD, Nurnberger JI Jr, Edenberg HJ, Gershon ES, Schork N, Price ND, Gelinas R, Hood L, Craig D, McMahon FJ, Kelsoe JR, and Roach JC

Subjects

Case-Control Studies, Female, Genetic Association Studies, Humans, Male, Pedigree, Polymorphism, Single Nucleotide genetics, Risk Factors, Signal Transduction genetics, White People genetics, Bipolar Disorder genetics, Bipolar Disorder physiopathology, Genetic Predisposition to Disease, Genetic Variation, Neurons physiology

Abstract

We sequenced the genomes of 200 individuals from 41 families multiply affected with bipolar disorder (BD) to identify contributions of rare variants to genetic risk. We initially focused on 3,087 candidate genes with known synaptic functions or prior evidence from genome-wide association studies. BD pedigrees had an increased burden of rare variants in genes encoding neuronal ion channels, including subunits of GABAA receptors and voltage-gated calcium channels. Four uncommon coding and regulatory variants also showed significant association, including a missense variant in GABRA6. Targeted sequencing of 26 of these candidate genes in an additional 3,014 cases and 1,717 controls confirmed rare variant associations in ANK3, CACNA1B, CACNA1C, CACNA1D, CACNG2, CAMK2A, and NGF. Variants in promoters and 5' and 3' UTRs contributed more strongly than coding variants to risk for BD, both in pedigrees and in the case-control cohort. The genes and pathways identified in this study regulate diverse aspects of neuronal excitability. We conclude that rare variants in neuronal excitability genes contribute to risk for BD.

Published

2015

14. Identification of copy number variants in whole-genome data using Reference Coverage Profiles.

Author

Glusman G, Severson A, Dhankani V, Robinson M, Farrah T, Mauldin DE, Stittrich AB, Ament SA, Roach JC, Brunkow ME, Bodian DL, Vockley JG, Shmulevich I, Niederhuber JE, and Hood L

Abstract

The identification of DNA copy numbers from short-read sequencing data remains a challenge for both technical and algorithmic reasons. The raw data for these analyses are measured in tens to hundreds of gigabytes per genome; transmitting, storing, and analyzing such large files is cumbersome, particularly for methods that analyze several samples simultaneously. We developed a very efficient representation of depth of coverage (150-1000× compression) that enables such analyses. Current methods for analyzing variants in whole-genome sequencing (WGS) data frequently miss copy number variants (CNVs), particularly hemizygous deletions in the 1-100 kb range. To fill this gap, we developed a method to identify CNVs in individual genomes, based on comparison to joint profiles pre-computed from a large set of genomes. We analyzed depth of coverage in over 6000 high quality (>40×) genomes. The depth of coverage has strong sequence-specific fluctuations only partially explained by global parameters like %GC. To account for these fluctuations, we constructed multi-genome profiles representing the observed or inferred diploid depth of coverage at each position along the genome. These Reference Coverage Profiles (RCPs) take into account the diverse technologies and pipeline versions used. Normalization of the scaled coverage to the RCP followed by hidden Markov model (HMM) segmentation enables efficient detection of CNVs and large deletions in individual genomes. Use of pre-computed multi-genome coverage profiles improves our ability to analyze each individual genome. We make available RCPs and tools for performing these analyses on personal genomes. We expect the increased sensitivity and specificity for individual genome analysis to be critical for achieving clinical-grade genome interpretation.

Published

2015

15. Origin of the PSEN1 E280A mutation causing early-onset Alzheimer's disease.

Author

Lalli MA, Cox HC, Arcila ML, Cadavid L, Moreno S, Garcia G, Madrigal L, Reiman EM, Arcos-Burgos M, Bedoya G, Brunkow ME, Glusman G, Roach JC, Hood L, Kosik KS, and Lopera F

Subjects

Age of Onset, Colombia, Founder Effect, Haplotypes, Humans, Inheritance Patterns, White People genetics, Alzheimer Disease genetics, Genetic Predisposition to Disease, Mutation, Presenilin-1 genetics

Abstract

Background: A mutation in presenilin 1 (E280A) causes early-onset Alzheimer's disease. Understanding the origin of this mutation will inform medical genetics., Methods: We sequenced the genomes of 102 individuals from Antioquia, Colombia. We applied identity-by-descent analysis to identify regions of common ancestry. We estimated the age of the E280A mutation and the local ancestry of the haplotype harboring this mutation., Results: All affected individuals share a minimal haplotype of 1.8 Mb containing E280A. We estimate a time to most recent common ancestor of E280A of 10 (95% credible interval, 7.2-12.6) generations. We date the de novo mutation event to 15 (95% credible interval, 11-25) generations ago. We infer a western European geographic origin of the shared haplotype., Conclusions: The age and geographic origin of E280A are consistent with a single founder dating from the time of the Spanish Conquistadors who began colonizing Colombia during the early 16th century., (Copyright © 2014 The Alzheimer's Association. Published by Elsevier Inc. All rights reserved.)

Published

2014

16. Sclerostin: how human mutations have helped reveal a new target for the treatment of osteoporosis.

Author

Robinson MK, Caminis J, and Brunkow ME

Subjects

Adaptor Proteins, Signal Transducing, Animals, Antibodies pharmacology, Bone Density Conservation Agents pharmacology, Bone Morphogenetic Proteins antagonists & inhibitors, Bone Morphogenetic Proteins immunology, Genetic Markers immunology, Genetic Predisposition to Disease, Humans, Hyperostosis genetics, Hyperostosis metabolism, Osteoporosis genetics, Osteoporosis metabolism, Phenotype, Syndactyly genetics, Syndactyly metabolism, Treatment Outcome, Antibodies therapeutic use, Bone Density Conservation Agents therapeutic use, Bone Morphogenetic Proteins genetics, Drug Discovery, Genetic Markers genetics, Hyperostosis drug therapy, Molecular Targeted Therapy, Mutation, Osteoporosis drug therapy, Syndactyly drug therapy

Abstract

In the 1990s there was a tremendous mood of optimism among pharmaceutical scientists that identification of disease-associated variations in the human genome would result in a surge of new drug targets (the 'gene-to-drug' mantra). To date the expected deluge of new drugs has not arrived. However, a small number of drugs arising directly from the study of rare human disorders showing Mendelian inheritance are now entering late stage clinical trials. Here we describe the advantages of this approach and discuss the background and early clinical trial findings with antibodies directed at a target identified in this way., (Copyright © 2013 Elsevier Ltd. All rights reserved.)

Published

2013

17. Disruption of Fnip1 reveals a metabolic checkpoint controlling B lymphocyte development.

Author

Park H, Staehling K, Tsang M, Appleby MW, Brunkow ME, Margineantu D, Hockenbery DM, Habib T, Liggitt HD, Carlson G, and Iritani BM

Subjects

AMP-Activated Protein Kinase Kinases, Animals, Apoptosis genetics, Cell Division genetics, Hematopoiesis genetics, Immunoglobulin Heavy Chains genetics, Immunoglobulin Heavy Chains metabolism, Mice, Mice, Transgenic, Precursor Cells, B-Lymphoid metabolism, Protein Kinases genetics, Protein Kinases metabolism, Proto-Oncogene Proteins c-myc genetics, Proto-Oncogene Proteins c-myc metabolism, Signal Transduction genetics, TOR Serine-Threonine Kinases genetics, TOR Serine-Threonine Kinases metabolism, B-Lymphocytes cytology, B-Lymphocytes metabolism, Carrier Proteins genetics, Carrier Proteins metabolism, Cell Differentiation genetics, Estrone genetics, Estrone metabolism

Abstract

The coordination of nutrient and energy availability with cell growth and division is essential for proper immune cell development and function. By using a chemical mutagenesis strategy in mice, we identified a pedigree that has a complete block in B cell development at the pre-B cell stage resulting from a deletion in the Fnip1 gene. Enforced expression of an immunoglobulin transgene failed to rescue B cell development. Whereas essential pre-B cell signaling molecules were activated normally in Fnip1-null pre-B cells, the metabolic regulators AMPK and mTOR were dysregulated, resulting in excessive cell growth and enhanced sensitivity to apoptosis in response to metabolic stress (pre-B cell receptor crosslinking, oncogene activation). These results indicate that Folliculin-interacting protein 1 (Fnip1) is vital for B cell development and metabolic homeostasis and reveal a metabolic checkpoint that may ensure that pre-B cells have sufficient metabolic capacity to support division, while limiting lymphomagenesis caused by deregulated growth., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

18. A point mutation in the murine Hem1 gene reveals an essential role for Hematopoietic protein 1 in lymphopoiesis and innate immunity.

Author

Park H, Staehling-Hampton K, Appleby MW, Brunkow ME, Habib T, Zhang Y, Ramsdell F, Liggitt HD, Freie B, Tsang M, Carlson G, Friend S, Frevert C, and Iritani BM

Subjects

Actins metabolism, Anemia immunology, Animals, B-Lymphocytes cytology, B-Lymphocytes physiology, Cell Movement physiology, DNA Mutational Analysis, Hematopoietic Stem Cells physiology, Hematopoietic System cytology, Hematopoietic System physiology, Interferon-gamma immunology, Interleukin-17 metabolism, Interleukin-2 immunology, Lymphocyte Activation, Lymphopenia immunology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Neutrophils cytology, Neutrophils immunology, Neutrophils physiology, Phagocytosis physiology, T-Lymphocytes cytology, T-Lymphocytes physiology, Transplantation Chimera, Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing immunology, Immunity, Innate physiology, Lymphopoiesis physiology, Membrane Proteins genetics, Membrane Proteins immunology, Point Mutation

Abstract

Hem1 (Hematopoietic protein 1) is a hematopoietic cell-specific member of the Hem family of cytoplasmic adaptor proteins. Orthologues of Hem1 in Dictyostelium discoideum, Drosophila melanogaster, and Caenorhabditis elegans are essential for cytoskeletal reorganization, embryonic cell migration, and morphogenesis. However, the in vivo functions of mammalian Hem1 are not known. Using a chemical mutagenesis strategy in mice to identify novel genes involved in immune cell functions, we positionally cloned a nonsense mutation in the Hem1 gene. Hem1 deficiency results in defective F-actin polymerization and actin capping in lymphocytes and neutrophils caused by loss of the Rac-controlled actin-regulatory WAVE protein complex. T cell development is disrupted in Hem1-deficient mice at the CD4(-)CD8(-) (double negative) to CD4(+)CD8(+) (double positive) cell stages, whereas T cell activation and adhesion are impaired. Hem1-deficient neutrophils fail to migrate in response to chemotactic agents and are deficient in their ability to phagocytose bacteria. Remarkably, some Rac-dependent functions, such as Th1 differentiation and nuclear factor kappaB (NF-kappaB)-dependent transcription of proinflammatory cytokines proceed normally in Hem1-deficient mice, whereas the production of Th17 cells are enhanced. These results demonstrate that Hem1 is essential for hematopoietic cell development, function, and homeostasis by controlling a distinct pathway leading to cytoskeletal reorganization, whereas NF-kappaB-dependent transcription proceeds independently of Hem1 and F-actin polymerization.

Published

2008

19. Polymorphisms in the sclerosteosis/van Buchem disease gene (SOST) region are associated with bone-mineral density in elderly whites.

Author

Uitterlinden AG, Arp PP, Paeper BW, Charmley P, Proll S, Rivadeneira F, Fang Y, van Meurs JB, Britschgi TB, Latham JA, Schatzman RC, Pols HA, and Brunkow ME

Subjects

Adaptor Proteins, Signal Transducing, Aged, Analysis of Variance, Bone Morphogenetic Proteins metabolism, Cohort Studies, DNA Primers, Female, Gene Frequency, Genotype, Haplotypes genetics, Humans, Linkage Disequilibrium, Male, Middle Aged, Netherlands, Odds Ratio, Promoter Regions, Genetic genetics, Regression Analysis, Sequence Analysis, DNA, Spinal Injuries genetics, Spinal Injuries pathology, White People, Bone Density genetics, Bone Morphogenetic Proteins genetics, Genetic Markers genetics, Osteoporosis genetics, Polymorphism, Genetic

Abstract

Osteoporosis has a strong genetic component, but the genes involved are poorly defined. We studied whether the sclerosteosis/van Buchem disease gene (SOST) is an osteoporosis-risk gene by examining its association with bone-mineral density (BMD). Mutations in SOST result in sclerosteosis, and alterations in the SOST gene expression may be causal in the closely related van Buchem disease. We used a set of eight polymorphisms from the SOST gene region to genotype 1,939 elderly men and women from a large population-based prospective-cohort study of Dutch whites. A 3-bp insertion (f=0.38) in the presumed SOST promoter region (SRP3) was associated with decreased BMD in women at the femoral neck (FN) (P=.05) and lumbar spine (LS) (P=.01), with evidence of an allele-dose effect in the oldest age group (P=.006). Similarly, a G variant (f=0.40) in the van Buchem deletion region (SRP9) was associated with increased BMD in men at the FN (P=.007) and LS (P=.02). In both cases, differences between extreme genotypes reached 0.2 SD. We observed no genotype effects on fracture risk, for the 234 osteoporotic fractures validated during 8.2 years of follow-up and for the 146 vertebral prevalent fractures analyzed. We did not find association between any of several frequent haplotypes across the SOST gene region and BMD. We did find evidence of additive effects of SRP3 with the COLIA1 Sp1 polymorphism but not with haplotypes of 3' polymorphisms in the vitamin-D receptor gene. The SOST-COLIA1 additive effect increased with age and reached 0.5 SD difference in BMD at LS in the oldest age group (P=.02). The molecular mechanism whereby these moderate SOST genotype effects are mediated remains to be elucidated, but it is likely to involve differences in regulation of SOST gene expression.

Published

2004

20. A novel mutation in CD83 results in the development of a unique population of CD4+ T cells.

Author

García-Martínez LF, Appleby MW, Staehling-Hampton K, Andrews DM, Chen Y, McEuen M, Tang P, Rhinehart RL, Proll S, Paeper B, Brunkow ME, Grandea AG 3rd, Howard ED, Walker DE, Charmley P, Jonas M, Shaw S, Latham JA, and Ramsdell F

Subjects

Amino Acid Sequence, Animals, Antigens, CD, Base Sequence, CD4-Positive T-Lymphocytes metabolism, Cytokines metabolism, Dendritic Cells immunology, Female, Immunoglobulins immunology, Male, Membrane Glycoproteins immunology, Mice, Molecular Sequence Data, Mutation, Pedigree, CD83 Antigen, CD4-Positive T-Lymphocytes immunology, Immunoglobulins genetics, Membrane Glycoproteins genetics

Abstract

Using a mouse mutagenesis screen, we have identified CD83 as being critical for the development of CD4(+) T cells and for their function postactivation. CD11c(+) dendritic cells develop and function normally in mice with a mutated CD83 gene but CD4(+) T cell development is substantially reduced. Additionally, we now show that those CD4(+) cells that develop in a CD83 mutant animal fail to respond normally following allogeneic stimulation. This is at least in part due to an altered cytokine expression pattern characterized by an increased production of IL-4 and IL-10 and diminished IL-2 production. Thus, in addition to its role in selection of CD4(+) T cells, absence of CD83 results in the generation of cells with an altered activation and cytokine profile.

Published

2004

21. Osteocyte control of bone formation via sclerostin, a novel BMP antagonist.

Author

Winkler DG, Sutherland MK, Geoghegan JC, Yu C, Hayes T, Skonier JE, Shpektor D, Jonas M, Kovacevich BR, Staehling-Hampton K, Appleby M, Brunkow ME, and Latham JA

Subjects

Adaptor Proteins, Signal Transducing, Alkaline Phosphatase metabolism, Animals, Base Sequence, Bone Density, Bone Diseases, Metabolic genetics, Bone Morphogenetic Protein 6, Bone Morphogenetic Proteins genetics, Bone Morphogenetic Proteins metabolism, Bone Morphogenetic Proteins pharmacology, Cell Line, Cloning, Molecular, DNA Primers, Genetic Markers genetics, Glycoproteins, Humans, Intercellular Signaling Peptides and Proteins, Kinetics, Mesoderm drug effects, Mesoderm physiology, Mice, Mice, Inbred C3H, Mice, Transgenic, Recombinant Proteins metabolism, Recombinant Proteins pharmacology, Reverse Transcriptase Polymerase Chain Reaction, Bone Development physiology, Bone Morphogenetic Proteins antagonists & inhibitors, Bone Morphogenetic Proteins physiology, Genetic Markers physiology, Osteocytes physiology

Abstract

There is an unmet medical need for anabolic treatments to restore lost bone. Human genetic bone disorders provide insight into bone regulatory processes. Sclerosteosis is a disease typified by high bone mass due to the loss of SOST expression. Sclerostin, the SOST gene protein product, competed with the type I and type II bone morphogenetic protein (BMP) receptors for binding to BMPs, decreased BMP signaling and suppressed mineralization of osteoblastic cells. SOST expression was detected in cultured osteoblasts and in mineralizing areas of the skeleton, but not in osteoclasts. Strong expression in osteocytes suggested that sclerostin expressed by these central regulatory cells mediates bone homeostasis. Transgenic mice overexpressing SOST exhibited low bone mass and decreased bone strength as the result of a significant reduction in osteoblast activity and subsequently, bone formation. Modulation of this osteocyte-derived negative signal is therapeutically relevant for disorders associated with bone loss.

Published

2003

22. A 52-kb deletion in the SOST-MEOX1 intergenic region on 17q12-q21 is associated with van Buchem disease in the Dutch population.

Author

Staehling-Hampton K, Proll S, Paeper BW, Zhao L, Charmley P, Brown A, Gardner JC, Galas D, Schatzman RC, Beighton P, Papapoulos S, Hamersma H, and Brunkow ME

Subjects

Adaptor Proteins, Signal Transducing, Africa, Base Sequence, DNA, Intergenic genetics, Female, Genetic Predisposition to Disease genetics, Haplotypes, Humans, Male, Microsatellite Repeats, Netherlands, Osteochondrodysplasias pathology, Osteosclerosis genetics, Polymorphism, Single Nucleotide, Proteins genetics, Bone Morphogenetic Proteins, Chromosome Deletion, Chromosomes, Human, Pair 17 genetics, Genetic Markers, Osteochondrodysplasias genetics

Abstract

Van Buchem disease is an autosomal recessive sclerosing bone dysplasia characterized by skeletal hyperostosis, overgrowth of the mandible, and a liability to entrapment of the seventh and eighth cranial nerves. The genetic determinant maps to chromosome 17q12-q21. We refined the critical interval to the < 1-Mb region between D17S2250 and D17S2253 in 15 affected individuals, all of whom shared a common disease haplotype. Furthermore, we report here the identification of a 52-kb deletion located within the interval and encompassing D17S1789 that is 100% concordant with the disorder. Although the deletion itself does not appear to disrupt the coding region of any known or novel gene(s), the closest flanking genes are MEOX1 on the proximal side, and SOST on the distal side of the deletion. MEOX1 is known to be important for the development of the axial skeleton, whereas the SOST gene is the determinant of sclerosteosis, a disorder that shares many features with van Buchem disease, thus raising the possibility that van Buchem disease results from dysregulation of the expression of one or both of these genes., (Copyright 2002 Wiley-Liss, Inc.)

Published

2002

23. The amount of scurfin protein determines peripheral T cell number and responsiveness.

Author

Khattri R, Kasprowicz D, Cox T, Mortrud M, Appleby MW, Brunkow ME, Ziegler SF, and Ramsdell F

Subjects

Animals, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes metabolism, CD4-Positive T-Lymphocytes pathology, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes metabolism, CD8-Positive T-Lymphocytes pathology, Cells, Cultured, DNA-Binding Proteins physiology, Forkhead Transcription Factors, Gene Expression Regulation immunology, Histocytochemistry, Immunophenotyping, Lymphocyte Activation immunology, Lymphocyte Count, Lymphocyte Culture Test, Mixed, Lymphopenia genetics, Lymphopenia immunology, Lymphopenia pathology, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Mutant Strains, Mice, Transgenic, T-Lymphocyte Subsets metabolism, Thymus Gland immunology, Thymus Gland metabolism, Thymus Gland pathology, Transgenes immunology, DNA-Binding Proteins biosynthesis, DNA-Binding Proteins genetics, Lymphocyte Activation genetics, T-Lymphocyte Subsets immunology, T-Lymphocyte Subsets pathology

Abstract

In the absence of the recently identified putative transcription factor scurfin, mice develop a lymphoproliferative disorder resulting in death by 3 wk of age from a pathology that resembles TGF-beta or CTLA-4 knockout mice. In this report, we characterize mice that overexpress the scurfin protein and demonstrate that these animals have a dramatically depressed immune system. Mice transgenic for the Foxp3 gene (which encodes the scurfin protein) have fewer T cells than their littermate controls, and those T cells that remain have poor proliferative and cytolytic responses and make little IL-2 after stimulation through the TCR. Although thymic development appears normal in these mice, peripheral lymphoid organs, particularly lymph nodes, are relatively acellular. In a separate transgenic line, forced expression of the gene specifically in the thymus can alter thymic development; however, this does not appear to affect peripheral T cells and is unable to prevent disease in mice lacking a functional Foxp3 gene, indicating that the scurfin protein acts on peripheral T cells. The data indicate a critical role for the Foxp3 gene product in the function of the immune system, with both the number and functionality of peripheral T cells under the aegis of the scurfin protein.

Published

2001

24. A rare polyadenylation signal mutation of the FOXP3 gene (AAUAAA-->AAUGAA) leads to the IPEX syndrome.

Author

Bennett CL, Brunkow ME, Ramsdell F, O'Briant KC, Zhu Q, Fuleihan RL, Shigeoka AO, Ochs HD, and Chance PF

Subjects

Cells, Cultured, DNA Mutational Analysis, DNA-Binding Proteins biosynthesis, Female, Forkhead Transcription Factors, Genetic Linkage, Humans, Male, Pedigree, RNA, Messenger analysis, Reverse Transcriptase Polymerase Chain Reaction, T-Lymphocytes metabolism, X Chromosome, DNA-Binding Proteins genetics, Mutation, Poly A metabolism, Polyendocrinopathies, Autoimmune genetics

Abstract

The mouse scurfy gene, Foxp3, and its human orthologue, FOXP3, which maps to Xp11.23-Xq13.3, were recently identified by positional cloning. Point mutations and microdeletions of the FOXP3 gene were found in the affected members of eight of nine families with IPEX (immune dysfunction, polyendocrinopathy, enteropathy, X-linked; OMIM 304930). We evaluated a pedigree with clinically typical IPEX in which mutations of the coding exons of FOXP3 were not detected. Our reevaluation of this pedigree identified an A-->G transition within the first polyadenylation signal (AAUAAA-->AAUGAA) after the stop codon. The next polyadenylation signal is not encountered for a further 5.1 kb. This transition was not detected in over 212 normal individuals (approximately 318 X chromosomes), excluding the possibility of a rare polymorphism. We suggest that this mutation is causal of IPEX in this family by a mechanism of nonspecific degradation of the FOXP3 gene message.

Published

2001

25. Bone dysplasia sclerosteosis results from loss of the SOST gene product, a novel cystine knot-containing protein.

Author

Brunkow ME, Gardner JC, Van Ness J, Paeper BW, Kovacevich BR, Proll S, Skonier JE, Zhao L, Sabo PJ, Fu Y, Alisch RS, Gillett L, Colbert T, Tacconi P, Galas D, Hamersma H, Beighton P, and Mulligan J

Subjects

Adaptor Proteins, Signal Transducing, Alternative Splicing, Amino Acid Sequence, Animals, Base Sequence, Black People, Bone Diseases pathology, Chromosome Mapping, Consanguinity, Conserved Sequence, Cystine, Female, Genetic Markers, Homozygote, Humans, Male, Molecular Sequence Data, Netherlands ethnology, Pedigree, Proteins chemistry, Recombination, Genetic, Sclerosis, Senegal ethnology, South Africa, White People, Bone Diseases genetics, Bone Morphogenetic Proteins, Chromosomes, Human, Pair 17, Mutation, Missense, Proteins genetics

Abstract

Sclerosteosis is an autosomal recessive sclerosing bone dysplasia characterized by progressive skeletal overgrowth. The majority of affected individuals have been reported in the Afrikaner population of South Africa, where a high incidence of the disorder occurs as a result of a founder effect. Homozygosity mapping in Afrikaner families along with analysis of historical recombinants localized sclerosteosis to an interval of approximately 2 cM between the loci D17S1787 and D17S930 on chromosome 17q12-q21. Here we report two independent mutations in a novel gene, termed "SOST." Affected Afrikaners carry a nonsense mutation near the amino terminus of the encoded protein, whereas an unrelated affected person of Senegalese origin carries a splicing mutation within the single intron of the gene. The SOST gene encodes a protein that shares similarity with a class of cystine knot-containing factors including dan, cerberus, gremlin, prdc, and caronte. The specific and progressive effect on bone formation observed in individuals affected with sclerosteosis, along with the data presented in this study, together suggest that the SOST gene encodes an important new regulator of bone homeostasis.

Published

2001

26. X-linked neonatal diabetes mellitus, enteropathy and endocrinopathy syndrome is the human equivalent of mouse scurfy.

Author

Wildin RS, Ramsdell F, Peake J, Faravelli F, Casanova JL, Buist N, Levy-Lahad E, Mazzella M, Goulet O, Perroni L, Bricarelli FD, Byrne G, McEuen M, Proll S, Appleby M, and Brunkow ME

Subjects

Amino Acid Sequence, Animals, DNA Mutational Analysis, DNA-Binding Proteins chemistry, DNA-Binding Proteins metabolism, Disease Models, Animal, Forkhead Transcription Factors, Genetic Linkage genetics, Humans, Infant, Newborn, Mice, Mice, Mutant Strains, Molecular Sequence Data, Mutation genetics, Sequence Alignment, Syndrome, Animal Diseases genetics, DNA-Binding Proteins genetics, Diabetes Mellitus congenital, Diabetes Mellitus genetics, Polyendocrinopathies, Autoimmune genetics, Protein-Losing Enteropathies genetics, X Chromosome genetics

Abstract

To determine whether human X-linked neonatal diabetes mellitus, enteropathy and endocrinopathy syndrome (IPEX; MIM 304930) is the genetic equivalent of the scurfy (sf) mouse, we sequenced the human ortholog (FOXP3) of the gene mutated in scurfy mice (Foxp3), in IPEX patients. We found four non-polymorphic mutations. Each mutation affects the forkhead/winged-helix domain of the scurfin protein, indicating that the mutations may disrupt critical DNA interactions.

Published

2001

27. Disruption of a new forkhead/winged-helix protein, scurfin, results in the fatal lymphoproliferative disorder of the scurfy mouse.

Author

Brunkow ME, Jeffery EW, Hjerrild KA, Paeper B, Clark LB, Yasayko SA, Wilkinson JE, Galas D, Ziegler SF, and Ramsdell F

Subjects

Amino Acid Motifs, Amino Acid Sequence, Animals, Cloning, Molecular, Conserved Sequence, DNA Mutational Analysis, DNA-Binding Proteins genetics, Female, Forkhead Transcription Factors, Gene Expression Profiling, Genes, Recessive genetics, Genetic Complementation Test, Humans, Lymph Nodes immunology, Lymph Nodes pathology, Lymphocyte Count, Lymphoproliferative Disorders immunology, Lymphoproliferative Disorders pathology, Male, Mice, Mice, Mutant Strains, Mice, Transgenic, Molecular Sequence Data, Phenotype, Physical Chromosome Mapping, Protein Structure, Tertiary, RNA, Messenger analysis, RNA, Messenger genetics, Sequence Alignment, DNA-Binding Proteins chemistry, DNA-Binding Proteins metabolism, Genes, Essential genetics, Lymphoproliferative Disorders genetics, Mutation genetics

Abstract

Scurfy (sf) is an X-linked recessive mouse mutant resulting in lethality in hemizygous males 16-25 days after birth, and is characterized by overproliferation of CD4+CD8- T lymphocytes, extensive multiorgan infiltration and elevation of numerous cytokines. Similar to animals that lack expression of either Ctla-4 or Tgf-beta, the pathology observed in sf mice seems to result from an inability to properly regulate CD4+CD8- T-cell activity. Here we identify the gene defective in sf mice by combining high-resolution genetic and physical mapping with large-scale sequence analysis. The protein encoded by this gene (designated Foxp3) is a new member of the forkhead/winged-helix family of transcriptional regulators and is highly conserved in humans. In sf mice, a frameshift mutation results in a product lacking the forkhead domain. Genetic complementation demonstrates that the protein product of Foxp3, scurfin, is essential for normal immune homeostasis.

Published

2001

28. The immune dysregulation, polyendocrinopathy, enteropathy, X-linked syndrome (IPEX) is caused by mutations of FOXP3.

Author

Bennett CL, Christie J, Ramsdell F, Brunkow ME, Ferguson PJ, Whitesell L, Kelly TE, Saulsbury FT, Chance PF, and Ochs HD

Subjects

Amino Acid Sequence, Animals, DNA-Binding Proteins chemistry, DNA-Binding Proteins metabolism, Female, Forkhead Transcription Factors, Humans, Male, Mice, Molecular Sequence Data, Pedigree, Phenotype, Sequence Alignment, Syndrome, DNA-Binding Proteins genetics, Genetic Linkage genetics, Mutation genetics, Polyendocrinopathies, Autoimmune genetics, Protein-Losing Enteropathies genetics, X Chromosome genetics

Abstract

IPEX is a fatal disorder characterized by immune dysregulation, polyendocrinopathy, enteropathy and X-linked inheritance (MIM 304930). We present genetic evidence that different mutations of the human gene FOXP3, the ortholog of the gene mutated in scurfy mice (Foxp3), causes IPEX syndrome. Recent linkage analysis studies mapped the gene mutated in IPEX to an interval of 17-20-cM at Xp11. 23-Xq13.3.

Published

2001

29. Cellular and molecular characterization of the scurfy mouse mutant.

Author

Clark LB, Appleby MW, Brunkow ME, Wilkinson JE, Ziegler SF, and Ramsdell F

Subjects

Abatacept, Animals, Antigens, CD, Antigens, Differentiation analysis, B7-1 Antigen analysis, Benzoquinones, CTLA-4 Antigen, Cyclosporine pharmacology, Female, Genistein pharmacology, Granulocyte-Macrophage Colony-Stimulating Factor biosynthesis, Lactams, Macrocyclic, Leukocyte Common Antigens analysis, Lymphocyte Activation, Lymphoproliferative Disorders immunology, Male, Mice, Mice, Inbred C3H, Mice, Mutant Strains, Nuclear Proteins analysis, Quinones pharmacology, Receptors, Antigen, T-Cell physiology, Rifabutin analogs & derivatives, Transcription Factors analysis, Immunoconjugates, Lymphoproliferative Disorders genetics, T-Lymphocytes immunology

Abstract

Mice hemizygous (Xsf/Y) for the X-linked mutation scurfy (sf) develop a severe and rapidly fatal lymphoproliferative disease mediated by CD4+CD8- T lymphocytes. We have undertaken phenotypic and functional studies to more accurately identify the immunologic pathway(s) affected by this important mutation. Flow cytometric analyses of lymphoid cell populations reveal that scurfy syndrome is characterized by changes in several phenotypic parameters, including an increase in Mac-1+ cells and a decrease in B220+ cells, changes that may result from the production of extremely high levels of the cytokine granulocyte-macrophage CSF by scurfy T cells. Scurfy T cells also exhibit strong up-regulation of cell surface Ags indicative of in vivo activation, including CD69, CD25, CD80, and CD86. Both scurfy and normal T cells are responsive to two distinct signals provided by the TCR and by ligation of CD28; scurfy cells, however, are hyperresponsive to TCR ligation and exhibit a decreased requirement for costimulation through CD28 relative to normal controls. This hypersensitivity may result, in part, from increased costimulation through B7-1 and B7-2, whose expression is up-regulated on scurfy T cells. Although the specific defect leading to this hyperactivation has not been identified, we also demonstrate that scurfy T cells are less sensitive than normal controls to inhibitors of tyrosine kinases such as genistein and herbimycin A, and the immunosuppressant cyclosporin A. One interpretation of our data would suggest that the scurfy mutation results in a defect, which interferes with the normal down-regulation of T cell activation.

Published

1999

30. Embryonic and adult expression patterns of the Tec tyrosine kinase gene suggest a role in megakaryocytopoiesis, blood vessel development, and melanogenesis.

Author

Klüppel M, Donoviel DB, Brunkow ME, Motro B, and Bernstein A

Subjects

Animals, Blood Vessels embryology, Blood Vessels growth & development, Blotting, Northern, Embryonic and Fetal Development physiology, Gene Expression, In Situ Hybridization, Megakaryocytes cytology, Melanocytes cytology, Melanocytes physiology, Mice, Protein-Tyrosine Kinases physiology, RNA, Messenger analysis, Somites physiology, Embryonic and Fetal Development genetics, Hematopoiesis genetics, Megakaryocytes physiology, Neovascularization, Physiologic genetics, Protein-Tyrosine Kinases genetics

Abstract

The Tec cytoplasmic tyrosine kinase is a member of a family of src-like proteins that are thought to play important roles in hematopoiesis. Here we describe the temporal and spatial expression of the Tec gene during embryogenesis and in the adult. Our data demonstrate that embryonic Tec expression is restricted to distinct hematopoietic cells as well as structures and cell types that share a common feature of containing fluid in an enclosed cavity, e.g., endothelial cells. In addition, Tec is expressed in melanocytes late in gestation. The observed developmental expression pattern of Tec suggests a role for this gene in several aspects of hematopoiesis and/or blood vessel development as well as in late stages of melanogenesis.

Published

1997

31. A 1.8-Mb YAC contig spanning three members of the receptor tyrosine kinase gene family (Pdgfra, Kit, and Flk1) on mouse chromosome 5.

Author

Brunkow ME, Nagle DL, Bernstein A, and Bucan M

Subjects

Animals, Base Sequence, Gene Expression, Genes, Mice, Inbred C57BL, Molecular Sequence Data, Muridae genetics, Proto-Oncogene Proteins c-kit, Receptor, Platelet-Derived Growth Factor alpha, Receptors, Vascular Endothelial Growth Factor, Sequence Deletion, Chromosome Mapping, Chromosomes, Artificial, Yeast, Mice genetics, Proto-Oncogene Proteins genetics, Receptor Protein-Tyrosine Kinases genetics, Receptors, Colony-Stimulating Factor genetics, Receptors, Growth Factor genetics, Receptors, Platelet-Derived Growth Factor genetics

Abstract

We constructed a yeast artificial chromosome (YAC) contig spanning the genes encoding Kit (Kit), the platelet-derived growth factor alpha receptor (Pdgfra), and fetal liver kinase 1 (Flk1), three members of a receptor tyrosine kinase gene family located in the central portion of mouse chromosome 5. The orientation of YAC clones and the extent of their overlap was determined by "probe content mapping," that is, hybridization analysis of YAC clones using the available gene probes and YAC end sequences. For four YAC clones, which constitute a minimal set spanning 1.8 Mb, a detailed restriction map was constructed. This map, in conjunction with the previously published long-range restriction map, indicates the order, the physical distances, and the relative transcriptional orientations of the Pdgfra, Kit, and Flk1 genes. The YAC clones and corresponding YAC end probes presented here provide an important resource for the molecular analysis of a cluster of developmental mutations, namely dominant white spotting (W), patch (Ph), recessive spotting (rs), and rump-white (Rw), associated with this chromosomal region.

Published

1995

32. Epigenetic mechanisms underlying the imprinting of the mouse H19 gene.

Author

Bartolomei MS, Webber AL, Brunkow ME, and Tilghman SM

Subjects

Alleles, Animals, Chromatin, DNA metabolism, Embryo, Mammalian cytology, Enhancer Elements, Genetic, Female, Male, Methylation, Mice, Mice, Inbred C57BL, Mice, Inbred DBA, Polymorphism, Restriction Fragment Length, Promoter Regions, Genetic, Spermatozoa metabolism, Stem Cells metabolism, Genes, RNA genetics

Abstract

The expression of the H19 gene is governed by parental imprinting in mammals. H19, an unusual gene encoding an RNA with no known function, is exclusively expressed from the maternal chromosome. In mouse, it lies 90 kb downstream from the Igf2 gene, which encodes a fetal-specific growth factor, insulin-like growth factor II, and is expressed primarily from the paternally inherited chromosome. In this report we have utilized interspecific hybrid mice to identify male-specific DNA methylation of a 7- to 9-kb domain surrounding the H19 gene and its promoter. This allele-specific methylation could function as a mark to suppress transcription of the H19 paternal allele. Consistent with this proposal, the H19 promoter displayed an open chromatin conformation only on the relatively unmethylated active maternal allele. In contrast, a cell type-specific enhancer that lies outside the methylation domain is hypersensitive to restriction enzyme digestion in nuclei on both maternal and paternal chromosomes. That the allele-specific methylation domain, coupled to the two H19 enhancers, contains all the information necessary for its imprinting was tested by examining two transgenic lines containing an internally deleted H19 transgene. Both displayed paternal-specific methylation of the transgene and maternal-specific expression. Although neither line has been tested in an inbred genetic background, and therefore the action of complex modifiers cannot be formally excluded, the result suggests that the sequences necessary for the imprinting of H19 have been identified.

Published

1993

33. Parental imprinting of the H19 and Igf2 genes in the mouse.

Author

Tilghman SM, Bartolomei MS, Webber AL, Brunkow ME, Saam J, Leighton PA, Pfeifer K, and Zemel S

Subjects

Alleles, Animals, DNA genetics, DNA metabolism, Female, Genes, Regulator, Male, Methylation, Mice, Inbred C57BL, Mice, Inbred DBA, Mice, Transgenic, Models, Genetic, Insulin-Like Growth Factor II genetics, Mice genetics

Published

1993

34. Ectopic expression of the H19 gene in mice causes prenatal lethality.

Author

Brunkow ME and Tilghman SM

Subjects

Animals, Chromosome Deletion, Deoxyribonuclease I metabolism, Gene Expression, Genes, Dominant, Mice, Mice, Inbred C57BL, Mice, Transgenic, Microinjections, Organ Specificity genetics, RNA, Messenger biosynthesis, RNA, Messenger genetics, Restriction Mapping, Transcription, Genetic, Fetal Death genetics, Genes, Lethal

Abstract

The mouse H19 gene is expressed in a broad array of tissues of both endoderm and mesoderm origin in the developing mouse embryo. Its expression is repressed in all tissues except skeletal muscle shortly after birth. This gene is unusual in that it may not encode a protein, despite its conservation in mammals. The RNA product is found as a spliced and polyadenylated RNA in a cytoplasmic particle. To probe whether this unusual gene is functional, excess copies were introduced into mouse zygotes. Transgenic progeny were obtained at a very low frequency, but in no instance was the transgene expressed. That the gene itself was deleterious to embryos was established by introducing into zygotes a mutant of the structural gene in which its most conserved segment was deleted. Transgenic founders were obtained at a higher frequency, and these expressed the altered transgene at high rates in a subset of the tissues that express the endogenous H19 gene. The lethal effects are manifested late in gestation, between day 14 and birth.

Published

1991