Your search keyword '"Kenneth Morgan"' showing total 102 results

1. Association between genome-wide association studies reported SNPs and pediatric-onset Crohn’s disease in Canadian children

Author

David R. Mack, Phlippe Lambrette, Guy Grimard, Jinsong Dong, Devendra Amre, Colette Deslandres, Alfreda Krupoves, David M. Israel, Kenneth Morgan, Zia Xhu, Irina Costea, Emile Levy, Ernest G. Seidman, and Houda Fegury

Subjects

Adult, Male, Canada, medicine.medical_specialty, Genotype, Single-nucleotide polymorphism, Genome-wide association study, Disease, Biology, Polymorphism, Single Nucleotide, Inflammatory bowel disease, Crohn Disease, Internal medicine, Genetics, medicine, Humans, SNP, Allele, Child, Alleles, Genetics (clinical), Pediatric gastroenterology, Genetic association, Genome, Research, medicine.disease, Genome-Wide Association Study

Abstract

A recent pediatric-focused genome-wide association study has implicated three novel susceptibility loci for Crohn' disease (CD).We aimed to investigate whether the three recently reported and other previously reported genes/loci were also associated with CD in Canadian children. A case-control design was implemented at three pediatric gastroenterology clinics in Canada. Children19 years of age with a confirmed diagnosis of CD were recruited along with controls. Single nucleotide polymorphisms (SNPs) in 19 reported genes/loci were genotyped. Associations between individual SNPs and CD were examined. A total of 563 cases and 553 controls were studied. The mean (+/-SD) age of the cases was 12.3 (+/-3.2) years. Most cases were male (56.0%), had ileo-colonic disease (L3 +/- L4, 48.8%) and inflammatory behavior (B1 +/- p, 87.9%) at diagnosis. Allelic association analysis (two-tailed) showed that 8 of the 19 targeted SNPs were significantly associated with overall susceptibility for CD. Associations with one additional SNP was borderline non-significant. Significantly associated SNPs included SNPs rs1250550 (p = 0.026) and rs8049439 (p = 0.04), recently reported to be specifically associated with pediatric-onset CD.Based on the results, we confirmed associations between two of the three novel pediatric-CD loci and other regions reported for associations with either pediatric and/or adult-onset CD.

Published

2010

2. Screening and instability ofFMR1alleles in a prospective sample of 24,449 mother–newborn pairs from the general population

Author

J. S. Côté, R. Rehel, M. L. Morel, Johanne Bussières, Kenneth Morgan, C. Dombrowski, Sébastien Lévesque, and François Rousseau

Subjects

Heterozygote, Offspring, Cost effectiveness, Population, Inheritance Patterns, Mothers, Biology, Genomic Instability, Fragile X Mental Retardation Protein, Neonatal Screening, Genetics, medicine, Humans, Genetic Testing, Prospective Studies, Allele, education, Alleles, Genetics (clinical), education.field_of_study, Genome, Human, Haplotype, Infant, Newborn, Exons, medicine.disease, FMR1, Confidence interval, Fragile X syndrome, Genetics, Population, Haplotypes, Female, Trinucleotide Repeat Expansion

Abstract

To study the instability of FMR1 triplet repeats in the general population, we screened a prospective sample of 24,449 anonymized mother-offspring pairs and analyzed transmissions of intermediate-size (45-54 triplets) and premutation-size (55-200 triplets) alleles. We screened all mothers for alleles > or = 45 triplets by Southern blot and studied transmission of 545 maternal alleles to their offspring using polymerase chain reaction. Out of 21,411 maternal samples with conclusive results, we identified 250 carriers of at least one intermediate-size allele and 39 carrying a premutation-size allele. Out of a subsample of 430 transmissions of normal-size alleles (< 45 triplets), we observed four (< 1%) unstable transmissions. There were 6/90 intermediate-size unstable alleles (7%) and 11/25 unstable premutation-size alleles (44%). Two mothers transmitted a typical full mutation. The incidence of fragile X syndrome was thus 1/12,225 newborns (upper limit of 95% confidence interval: 1/4638 newborns), but larger in males (1/6209) than females (none detected in over 12,000 newborn females). Intermediate-size alleles were more unstable than normal-size alleles (p = 0.0027), but more stable (about sixfold) than premutation-size alleles (p < 0.0001). Unstable premutation-size alleles harbored the major fragile X haplotype (T50-T42-T62), and this haplotype appeared to be a good predictor of instability in premutations (p = 0.02). Incidence and instability are important to determine the feasibility and cost effectiveness of putative FMR1 screening programs. Carriers of FMR1 alleles of 55+ triplets with no family history of the disease may have a significant risk of expansion to a full mutation in a single generation.

Published

2009

3. Associations between ABCB1/MDR1 gene polymorphisms and Crohnʼs disease: A gene-wide study in a pediatric population

Author

David R. Mack, Philippe Lambrette, Alfreda Krupoves, Emile Levy, Liliane Law, Ernest G. Seidman, David M. Israel, Irina Costea, Kenneth Morgan, Guy Grimard, Devendra Amre, and Colette Deslandres

Subjects

Male, ATP Binding Cassette Transporter, Subfamily B, Adolescent, Population, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Young Adult, Crohn Disease, Risk Factors, Polymorphism (computer science), Genotype, Humans, Immunology and Allergy, Genetic Predisposition to Disease, ATP Binding Cassette Transporter, Subfamily B, Member 1, Allele, Child, education, Genetic association, Genetics, education.field_of_study, Haplotype, Gastroenterology, Genomics, Odds ratio, Phenotype, Haplotypes, Immunology, Female

Abstract

Background: Functional studies support the involvement of the MDR1 gene in the pathways leading to Crohn's disease (CD). Two common single nucleotide polymorphisms (SNPs), C3435T and G2677T/A, thought to alter the function of the corresponding P-glycoprotein, have shown inconsistent associations with CD. We investigated whether DNA variants in the MDR1 gene were associated with susceptibility for CD and specific phenotypes in children. Methods: A case–control study was conducted at 3 gastroenterology clinics across Canada. Children with CD and population- or hospital-based controls were included. CD cases were classified using the Montreal Classification. Thirteen tag-SNPs and the C3435T variant in the MDR1 gene were genotyped. Single-SNP allelic, genotype as well as gene-wide haplotype associations with CD and its phenotypes at diagnosis were assessed. Results: A total of 270 CD cases and 336 controls were studied. Most cases were male (56.3%), had disease location L3±L4 (58.1%), and an inflammatory phenotype B1±p (88.5%). Allelic association analysis revealed that SNP rs17327442 was significantly associated with overall susceptibility to CD (odds ratio [OR] = 0.72, 95% confidence interval [CI] = 0.50–0.99, P = 0.04) but this association did not withstand corrections for multiple testing (q-value = 0.56). Genotype–phenotype analysis indicated that 2 SNPs (rs10248420, P = 0.007, q-value = 0.07; rs2032583, P = 0.01, q-value = 0.07) were significantly associated with colonic disease. Five SNPs, rs1128503 (P = 0.02), rs1202184 (P = 0.008), rs1202186 (P = 0.02), rs2091766 (P = 0.03), and rs2235046 (P = 0.03) were nominally associated with noninflammatory CD. Specific haplotypes comprising of the tag-SNPs were significantly associated with either colonic or noninflammatory CD. Conclusions: Our comprehensive gene-wide analysis suggests that the MDR1 gene may be associated with clinical phenotypes of CD in children. (Inflamm Bowel Dis 2008)

Published

2009

4. Investigation of associations between the pregnane-X receptor gene (NR1I2) and Crohnʼs disease in Canadian children using a gene-wide haplotype-based approach

Author

Devendra Amre, Ernest G. Seidman, Guy Grimard, Kenneth Morgan, Emile Levy, Colette Deslandres, Alfreda Krupoves, David R. Mack, Philippe Lambrette, David M. Israel, and Irina Costea

Subjects

Male, Parents, Canada, Receptors, Steroid, Adolescent, Genotype, Single-nucleotide polymorphism, Biology, Polymorphism, Single Nucleotide, Inflammatory bowel disease, Crohn Disease, medicine, Humans, Immunology and Allergy, SNP, Allele, Child, Genetics, Crohn's disease, Haplotype, Pregnane X Receptor, Gastroenterology, Case-control study, medicine.disease, Phenotype, Haplotypes, Case-Control Studies, Immunology, Colitis, Ulcerative, Female, SNP array

Abstract

Background: The pregnane-X-receptor (PXR) is involved in the metabolism and detoxification of numerous xenobiotics and is critical for maintaining intestinal integrity. The NR1I2 gene encoding PXR may confer susceptibility for Crohn’s disease (CD) but evidence for associations is conflicting. We investigated whether the NR1I2 gene was associated with susceptibility for pediatric CD. Methods: A case-control and family-based (case-parent) study was carried out at 3 inflammatory bowel disease (IBD) clinics across Canada. Confirmed cases of CD 20 years were diagnosed using standard criteria. For determination of gene associations parents of the cases and unrelated controls were evaluated. Clinical phenotypes were established based on the Montreal Classification scheme. Eight tag-SNPs (tag-single nucleotide polymorphisms) across the gene were genotyped for allelic or genotypic associations. Results: A total of 270 CD cases, 336 controls, and 395 parents were studied. The mean age (SD) of the cases was 12.1 (3.5) years of age. Most cases were male (56.3%), had disease location L3L4 (58.1%), and an inflammatory phenotype B1p (88.4%) at diagnosis. For 7 SNPs single SNP analysis using case– control or case–parent data did not reveal associations with development of CD and none of the SNPs were significantly associated with disease location or disease behavior at diagnosis. One SNP rs2461823 (P 0.05) was nominally associated with CD. No overall haplotype association (omnibus P-value 0.61) or associations with individual haplotypes was evident. Conclusions: Our gene-wide analysis in a pediatric cohort using both the case– control and case–parent designs suggests that the NR1I2 gene is not associated with CD in Canadian children. (Inflamm Bowel Dis 2008;14:1214 –1218)

Published

2008

5. Complex genetic control of susceptibility to Mycobacterium bovis (Bacille Calmette-Guérin) infection in wild-derived Mus spretus mice

Author

Philippe Gros, Erwin Schurr, Kenneth Morgan, K Turcotte, Paul R. Fortin, and J C Loredo-Osti

Subjects

Genetic Markers, Mycobacterium bovis, Models, Genetic, biology, Mus spretus, Stem Cells, Immunology, Genomics, Bacille Calmette Guerin, biology.organism_classification, Virology, Mice, Genetics, Animals, Tuberculosis, Genetic Predisposition to Disease, Cation Transport Proteins, Crosses, Genetic, Spleen, Genetics (clinical), Microsatellite Repeats

Abstract

Susceptibility to Mycobacterium bovis Bacille Calmette-Guérin (BCG) is genetically controlled by Nramp1 (Slc11a1). Inbred mouse strains harbor either the resistance (Nramp1(G169)) or the susceptibility (Nramp1(D169)) allele at Nramp1. Mus spretus (Nramp1(G169); SPRET/EiJ) is shown to display an intermediate level of BCG replication in the spleen (log(10) colony-forming units (CFU) approximately 5), compared to resistant A/J (log(10)CFU approximately 4.0) and susceptible C57BL/6J (log(10)CFU approximately 6.0) mice. The presence of genetic modifiers of Nramp1-dependent susceptibility to M. bovis (BCG) infection in Mus spretus was analyzed by whole-genome scanning in 175 mice of an informative (C57BL/6J x SPRET/EiJ) x C57BL/6J backcross. Nramp1 showed a major effect (D1Mcg4, P1e(-4)), but additional single marker effects were identified on chromosomes 4 (D4Mit150) and x (DXMit249) in male mice, and on chromosome 9 (D9Mit77) and 17 (D17Mit81) in female mice. A strong interaction between Nramp1 and the major histocompatibility locus was also noted in female mice. The mapped loci may act as modifiers of Nramp1 action, and constitute novel entry points for the parallel search of loci regulating susceptibility to mycobacterial infections in humans.

Published

2006

6. Identification of the gene responsible for methylmalonic aciduria and homocystinuria, cblC type

Author

Pierre Lepage, Johanna M. Rommens, Gail V Dunbar, Peter D. Pawelek, Emily Moras, Kenneth Morgan, Eric A. Shoubridge, Angela R Hosack, T. Mary Fujiwara, James W. Coulton, David S. Rosenblatt, Hana Antonicka, Daniel Leclerc, Carole Doré, Roy A. Gravel, Vince Forgetta, C. Melissa Dobson, Chantal F. Morel, Jamie C. Tirone, David Watkins, Jordan P. Lerner-Ellis, and Janet L Atkinson

Subjects

Protein Folding, Molecular Sequence Data, Homocystinuria, Locus (genetics), Biology, Cobalamin, Cell Line, chemistry.chemical_compound, Bacterial Proteins, Genetic linkage, Genetics, medicine, Humans, Amino Acid Sequence, Conserved Sequence, Chromosome Mapping, Membrane Proteins, Fibroblasts, Disease gene identification, medicine.disease, MMACHC, Vitamin B 12, Haplotypes, chemistry, Methylmalonic aciduria, Structural Homology, Protein, Mutation, CBLC, Carrier Proteins, Oxidoreductases, Metabolism, Inborn Errors, Methylmalonic Acid

Abstract

Methylmalonic aciduria and homocystinuria, cblC type (OMIM 277400), is the most common inborn error of vitamin B(12) (cobalamin) metabolism, with about 250 known cases. Affected individuals have developmental, hematological, neurological, metabolic, ophthalmologic and dermatologic clinical findings. Although considered a disease of infancy or childhood, some individuals develop symptoms in adulthood. The cblC locus was mapped to chromosome region 1p by linkage analysis. We refined the chromosomal interval using homozygosity mapping and haplotype analyses and identified the MMACHC gene. In 204 individuals, 42 different mutations were identified, many consistent with a loss of function of the protein product. One mutation, 271dupA, accounted for 40% of all disease alleles. Transduction of wild-type MMACHC into immortalized cblC fibroblast cell lines corrected the cellular phenotype. Molecular modeling predicts that the C-terminal region of the gene product folds similarly to TonB, a bacterial protein involved in energy transduction for cobalamin uptake.

Published

2005

7. Impairment of Protective Immunity to Blood-Stage Malaria by Concurrent Nematode Infection

Author

J. Concepcion Loredo-Osti, Zhong Su, Kenneth Morgan, Mary M. Stevenson, and Mariela Segura

Subjects

Male, Erythrocytes, Immunology, Antibodies, Protozoan, Parasitemia, Microbiology, Plasmodium chabaudi, Mice, Immune system, Transforming Growth Factor beta, Immunity, parasitic diseases, medicine, Animals, Strongylida Infections, Mice, Inbred BALB C, Nematospiroides dubius, biology, Dendritic Cells, medicine.disease, biology.organism_classification, Virology, Malaria, Chronic infection, Infectious Diseases, Nematode infection, Cytokines, Female, Parasitology, Interleukin-4, Heligmosomoides polygyrus, Fungal and Parasitic Infections

Abstract

Helminthiases, which are highly prevalent in areas where malaria is endemic, have been shown to modulate or suppress the immune response to unrelated antigens or pathogens. In this study, we established a murine model of coinfection with a gastrointestinal nematode parasite,Heligmosomoides polygyrus, and the blood-stage malaria parasitePlasmodium chabaudiAS in order to investigate the modulation of antimalarial immunity by concurrent nematode infection. Chronic infection with the nematode for 2, 3, or 5 weeks beforeP. chabaudiAS infection severely impaired the ability of C57BL/6 mice to control malaria, as demonstrated by severe mortality and significantly increased malaria peak parasitemia levels. Coinfected mice produced significantly lower levels of gamma interferon (IFN-γ) duringP. chabaudiAS infection than mice infected with malaria alone. Concurrent nematode infection also suppressed production of type 1-associated, malaria-specific immunoglobulin G2a. Mice either infected with the nematode alone or coinfected with the nematode and malaria had high transforming growth factor β1 (TGF-β1) levels, and concurrent nematode and malaria infections resulted in high levels of interleukin-10 in vivo. Splenic CD11c+dendritic cells (DC) from mice infected with malaria alone and coinfected mice showed similarly increased expression of CD40, CD80, and CD86, but DC from coinfected mice were unable to induce CD4+T-cell proliferation and optimal IFN-γ production in response to the malaria antigen in vitro. Importantly, treatment of nematode-infected mice with an anthelmintic drug prior to malaria infection fully restored protective antimalarial immunity and reduced TGF-β1 levels. These results demonstrate that concurrent nematode infection strongly modulates multiple aspects of immunity to blood-stage malaria and consequently impairs the development of protective antimalarial immunity.

Published

2005

8. Epistasis between mouse Klra and major histocompatibility complex class I loci is associated with a new mechanism of natural killer cell–mediated innate resistance to cytomegalovirus infection

Author

Kenneth Morgan, Lewis L. Lanier, Silvia M. Vidal, Agnieszka Kielczewska, Melissa B. Lodoen, Sonia Girard Adam, Suzanne Lemieux, Marie-Pierre Desrosiers, J C. Loredo-Osti, Andrew P. Makrigiannis, and Trung H.M. Pham

Subjects

Muromegalovirus, Genetic Linkage, Molecular Sequence Data, Mice, Inbred Strains, Major histocompatibility complex, Article, Natural killer cell, Mice, Genetics, medicine, Animals, Receptors, Immunologic, Histocompatibility Antigen H-2D, Receptor, Gene, biology, Haplotype, H-2 Antigens, virus diseases, Epistasis, Genetic, Herpesviridae Infections, biology.organism_classification, Virology, Immunity, Innate, Killer Cells, Natural, Chromosome 17 (human), medicine.anatomical_structure, biology.protein, Antibody

Abstract

Experimental infection with mouse cytomegalovirus (MCMV) has been used to elucidate the intricate host-pathogen mechanisms that determine innate resistance to infection. Linkage analyses in F(2) progeny from MCMV-resistant MA/My (H2 (k)) and MCMV-susceptible BALB/c (H2 (d)) and BALB.K (H2 (k)) mouse strains indicated that only the combination of alleles encoded by a gene in the Klra (also called Ly49) cluster on chromosome 6, and one in the major histocompatibility complex (H2) on chromosome 17, is associated with virus resistance. We found that natural killer cell-activating receptor Ly49P specifically recognized MCMV-infected cells, dependent on the presence of the H2 (k) haplotype. This binding was blocked using antibodies to H-2D(k) but not antibodies to H-2K(k). These results are suggestive of a new natural killer cell mechanism implicated in MCMV resistance, which depends on the functional interaction of the Ly49P receptor and the major histocompatibility complex class I molecule H-2D(k) on MCMV-infected cells.

Published

2005

9. The most common mutation inFKRP causing limb girdle muscular dystrophy type 2I (LGMD2I) may have occurred only once and is present in Hutterites and other populations

Author

Mayana Zatz, Danielle Frappier, Klaus Wrogemann, Michaela Zaik, Nicole M. Roslin, Kate Bushby, Cheryl Hirst, Kenneth Morgan, Edward Nylen, Ryan E. Lamont, Cheryl R. Greenberg, T. Mary Fujiwara, Flavia de Paula, Patrick Frosk, Alysa A.P. Tennese, and Volker Straub

Subjects

Linkage disequilibrium, Genotype, DNA Mutational Analysis, Population, Locus (genetics), Chromosome 9, Biology, Genetics, medicine, Humans, Missense mutation, Pentosyltransferases, education, Genetics (clinical), education.field_of_study, Haplotype, Chromosome Mapping, Proteins, medicine.disease, Founder Effect, Phenotype, Muscular Dystrophies, Limb-Girdle, Mutation, North America, Chromosomes, Human, Pair 19, Founder effect, Limb-girdle muscular dystrophy

Abstract

Limb girdle muscular dystrophy (LGMD) is common in the Hutterite population of North America. We previously identified a mutation in the TRIM32 gene in chromosome region 9q32, causing LGMD2H in approximately two-thirds of the 60 Hutterite LGMD patients studied to date. A genomewide scan was undertaken in five families who did not show linkage to the LGMD2H locus on chromosome 9. A second LGMD locus, LGMD2I, was identified in chromosome region 19q13.3, and the causative mutation was identified as c.826C4A (L276I), a missense mutation in the FKRP gene. A comparison of the clinical characteristics of the two LGMD patient groups in this population reveals some differences. LGMD2I patients generally have an earlier age at diagnosis, a more severe course, and higher serum creatine kinase (CK) levels. In addition, some of these patients show calf hypertrophy, cardiac symptoms, and severe reactions to general anesthesia. None of these features are present among LGMD2H patients. A single common haplotype surrounding the FKRP gene was identified in the Hutterite LGMD2I patients. An identical core haplotype was also identified in 19 other non-Hutterite LGMD2I patients from Europe, Canada, and Brazil. The occurrence of this mutation on a common core haplotype suggests that L276I is a founder mutation that is dispersed among populations of European origin. Hum Mutat 25:38–44, 2005. r 2004 Wiley-Liss, Inc.

Published

2004

10. Localisation of a gene for mucopolysaccharidosis IIIC to the pericentromeric region of chromosome 8

Author

Jérôme Ausseil, Alexey V. Pshezhetsky, C Darmond-Zwaig, O. P. van Diggelen, Thomas J. Hudson, J C Loredo-Osti, Kenneth Morgan, Ben J. H. M. Poorthuis, Andrei Verner, T. M. Fujiwara, Irène Maire, Clinical Genetics, and Other departments

Subjects

Genetic Markers, Male, medicine.medical_specialty, Genotype, Genetic Linkage, Mucopolysaccharidosis, Centromere, Short Report, Locus (genetics), Biology, Mucopolysaccharidosis III, Gene mapping, Genetic linkage, Genetics, medicine, Humans, Genotyping, Genetics (clinical), Mucopolysaccharidosis Type IIIC, Homozygote, Chromosome Mapping, medicine.disease, Disease gene identification, Pedigree, Medical genetics, Female, Chromosomes, Human, Pair 8

Abstract

Mucopolysaccharidosis type IIIC (MPS IIIC, or Sanfilippo syndrome C) is a rare lysosomal storage disorder caused by a deficiency of acetyl-coenzyme A:alpha-glucosaminide-N-acetyltransferase. Patients develop progressive neuropsychiatric problems, mental retardation, hearing loss, and relatively minor visceral manifestations. The pattern of transmission is consistent with an autosomal recessive mode of inheritance. The aim of this study was to find a locus for MPS IIIC using a homozygosity mapping approach. A genomewide scan was performed on DNA from 27 affected individuals and 17 of their unaffected relatives. Additional patients were recruited, and DNA was obtained from a total of 44 affected individuals and 18 unaffected family members from 31 families from 10 countries. A working candidate interval was defined by looking for excess homozygosity in patients compared with their relatives. Additional markers were genotyped in regions of interest. Linkage analysis was performed to support the informal analysis. Inspection of the genomewide scan data showed apparent excess homozygosity in patients compared with their relatives for markers on chromosome 8. Additional genotyping identified 15 consecutive markers (from D8S1051 to D8S2332) in an 8.3 cM interval for which the genotypes of affected siblings were identical in state. A maximum multipoint lod score of 10.61 was found at marker D8S519. A locus for MPS IIIC maps to an 8.3 cM (16 Mbp) interval in the pericentromeric region of chromosome 8.

Published

2004

11. Identification of genetic loci controlling bacterial clearance in experimental Salmonella enteritidis infection: an unexpected role of Nramp1 (Slc11a1) in the persistence of infection in mice

Author

Kenneth Morgan, J C Loredo-Osti, Emil Skamene, J Caron, Line Laroche, and Danielle Malo

Subjects

Salmonella, Salmonella enteritidis, Quantitative Trait Loci, Immunology, Spleen, Quantitative trait locus, Biology, medicine.disease_cause, Asymptomatic, Sepsis, Mice, Genetics, medicine, Animals, Cation Transport Proteins, Crosses, Genetic, Genetics (clinical), SLC11A1, Salmonella Infections, Animal, Chromosome Mapping, medicine.disease, Null allele, Mice, Inbred C57BL, Disease Models, Animal, medicine.anatomical_structure, Chronic Disease, Salmonella Infections, biology.protein, Female, Lod Score, medicine.symptom, Microsatellite Repeats

Abstract

The Gram-negative bacteria, Salmonella, cause a broad spectrum of clinical diseases in both animals and humans ranging from asymptomatic carriage to life-threatening sepsis. We have developed a model to study the contribution of genetic factors to the susceptibility of 129sv and C57BL/6J inbred mice to Salmonella enteritidis during the late phase of infection. C57BL/6J mice were able to eliminate completely sublethal inoculums of S. enteritidis from their reticuloendothelial system, whereas 129sv mice could not even after 60 days post inoculation. A genome scan performed on 302 (C57BL/6J x 129sv) F2 progeny identified three dominant loci (designated Ses1 to Ses3) that are associated with disease susceptibility in 129sv mice. Two highly significant linkages were identified on chromosomes 1 (Ses1) and 7 (Ses2) with respective LOD scores of 9.9 (P = 1.4 x 10(-11)) at D1Mcg5 and 4.0 (P = 1.9 x 10(-5)) at D7Mit62. One highly suggestive QTL was located on chromosomes15 (Ses3) with a LOD score 3.4 (P = 1.2 x 10(-4)). The estimated effects of Ses1, Ses2 and Ses3 on the bacterial clearance were greater in females. Using a model of three loci, with interaction between Ses1 and Ses2 and sex as a covariate, the three QTLs explained 32% of the phenotypic variance. The candidacy of Nramp1 as the gene for Ses1 was evaluated using mice carrying a null allele at Nramp1 (129sv-Nramp1(tm1Mcg)). These mice have a significantly lower spleen bacterial load compared to the wild-type 129sv mice, strongly suggesting the involvement of Nramp1 in controlling S. enteritidis clearance during the late phase of infection.

Published

2002

12. Shwachman-Diamond Syndrome with Exocrine Pancreatic Dysfunction and Bone Marrow Failure Maps to the Centromeric Region of Chromosome 7

Author

Graeme R.B. Boocock, Christine Bétard, Maja Popovic, Carl Brewer, Peter R. Durie, Sharan Goobie, T. Mary Fujiwara, Lynda Ellis, Jodi Morrison, Kenneth Morgan, Nicole M. Roslin, Hedy Ginzberg, Nadia Ehtesham, Thomas J. Hudson, and Johanna M. Rommens

Subjects

Male, Pancreatic disease, Genetic Linkage, Centromere, Genes, Recessive, Locus (genetics), Biology, Genetic Heterogeneity, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, Genetic linkage, Report, Genetics, medicine, Humans, Myeloid Cells, Genetics(clinical), 10. No inequality, Exocrine pancreatic insufficiency, Bone Marrow Diseases, Alleles, Genetics (clinical), 030304 developmental biology, Chromosome 7 (human), 0303 health sciences, Shwachman–Diamond syndrome, Models, Genetic, Genetic heterogeneity, Haplotype, Chromosome Mapping, Syndrome, medicine.disease, Musculoskeletal Abnormalities, Pedigree, Haplotypes, 030220 oncology & carcinogenesis, Mutation, Exocrine Pancreatic Insufficiency, Female, Lod Score, Chromosomes, Human, Pair 7, Software

Abstract

Shwachman-Diamond syndrome (SDS) is an autosomal recessive disorder characterized by exocrine pancreatic insufficiency and hematologic and skeletal abnormalities. A genomewide scan of families with SDS was terminated at approximately 50% completion, with the identification of chromosome 7 markers that showed linkage with the disease. Finer mapping revealed significant linkage across a broad interval that included the centromere. The maximum two-point LOD score was 8.7, with D7S473, at a recombination fraction of 0. The maximum multipoint LOD score was 10, in the interval between D7S499 and D7S482 (5.4 cM on the female map and 0 cM on the male map), a region delimited by recombinant events detected in affected children. Evidence from all 15 of the multiplex families analyzed provided support for the linkage, consistent with a single locus for SDS. However, the presence of several different mutations is suggested by the heterogeneity of disease-associated haplotypes in the candidate region.

Published

2001

13. Haplotype Analysis of BRCA2 8765delAG Mutation Carriers in French Canadian and Yemenite Jewish Hereditary Breast Cancer Families

Author

Steven A. Narod, Andrew Manning, Danielle Frappier, Anne-Marie Mes-Masson, Parviz Ghadirian, Kenneth Morgan, Julie A. Lambert, T. Mary Fujiwara, William D. Foulkes, Diane Provencher, Dvorah Abelovich, Patricia N. Tonin, André Robidoux, Tamar Peretz, and Teiling Wang

Subjects

Genetics, Judaism, Haplotype, Biology, medicine.disease, Identity by descent, Breast cancer, Mutation (genetic algorithm), medicine, French canadian, Microsatellite, Allele, Genetics (clinical)

Abstract

The BRCA2 8765delAG mutation was previously reported in hereditary breast cancer families of French Canadian and Yemenite Jewish descent. Haplotype analysis, using six microsatellite markers that span BRCA2 and two intragenic polymorphisms, was performed on 8765delAG mutation carriers to determine if there was evidence that the mutations were identical by descent. The alleles of the microsatellite markers most closely flanking BRCA2 (D13S1697 and D13S1701) were found to be identical in state in all the mutation carriers. However, the disease-associated allele of one of the intragenic markers differed between the Yemenite Jews and French Canadian families, indicating that the 8765delAG mutation has independent origins in these two geographically and ethnically distinct populations.

Published

2001

14. The Impact of Transmission-Ratio Distortion on Allele Sharing in Affected Sibling Pairs

Author

Celia M. T. Greenwood and Kenneth Morgan

Subjects

Male, Genetic Linkage, Segregation distortion, Matched-Pair Analysis, Biology, Nuclear Family, Bias, Genetic linkage, Distortion, Genetics, Humans, Genetics(clinical), Allele, Nuclear family, Genetics (clinical), Alleles, Genes, Dominant, Linkage (software), Sex Characteristics, Sample size, Genetic Diseases, Inborn, Chromosome Mapping, Meiotic drive, Diabetes Mellitus, Type 1, Sample size determination, Female, Allele sharing, Linkage analysis, Research Article

Abstract

There have been recent reports of transmission-ratio distortion (TRD) or segregation distortion in families not selected for genetic disease. If TRD exists but is ignored, linkage studies searching for disease genes in affected relatives may be misinterpreted. We show that the identical-by-descent sharing patterns for affected sib pairs are strongly affected by TRD and, further, that the estimated statistical significance of a sib-pair linkage study may be extremely biased. However, we also show that, if TRD is suspected during the planning stage of a study, the planned sample size of the study needs to be increased by only a small amount to maintain the desired power.

Published

2000

15. ARSACS, a spastic ataxia common in northeastern Québec, is caused by mutations in a new gene encoding an 11.5-kb ORF

Author

Eric S. Lander, Serge B. Melançon, Jean Mathieu, Kenneth Morgan, Andrea Richter, Jocelyne Mercier, James C. Engert, Martin Schalling, Jean-Pierre Bouchard, Thomas J. Hudson, Bing Ge, Pierre Bérubé, Pierre Lepage, and Carole Doré

Subjects

Molecular Sequence Data, Arabidopsis, Sequence alignment, Biology, Linkage Disequilibrium, Homology (biology), Mice, Open Reading Frames, Exon, Prevalence, Genetics, medicine, Animals, Humans, Amino Acid Sequence, Gene, Heat-Shock Proteins, Spinocerebellar Degenerations, Base Sequence, Chromosomes, Human, Pair 13, Sequence Homology, Amino Acid, Reverse Transcriptase Polymerase Chain Reaction, Haplotype, Quebec, Nucleic acid sequence, Chromosome Mapping, Autosomal recessive cerebellar ataxia, Exons, medicine.disease, Open reading frame, Mutation, Ataxia, Sequence Alignment

Abstract

Autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS or SACS) is an early onset neurodegenerative disease with high prevalence (carrier frequency 1/22) in the Charlevoix-Saguenay-Lac-Saint-Jean (CSLSJ) region of Quebec. We previously mapped the gene responsible for ARSACS to chromosome 13q11 and identified two ancestral haplotypes. Here we report the cloning of this gene, SACS, which encodes the protein sacsin. The ORF of SACS is 11,487 bp and is encoded by a single gigantic exon spanning 12,794 bp. This exon is the largest to be identified in any vertebrate organism. The ORF is conserved in human and mouse. The putative protein contains three large segments with sequence similarity to each other and to the predicted protein of an Arabidopsis thaliana ORF. The presence of heat-shock domains suggests a function for sacsin in chaperone-mediated protein folding. SACS is expressed in a variety of tissues, including the central nervous system. We identified two SACSmutations in ARSACS families that lead to protein truncation, consistent with haplotype analysis.

Published

2000

16. Autosomal Recessive Spastic Ataxia of Charlevoix–Saguenay (ARSACS): High-Resolution Physical and Transcript Map of the Candidate Region in Chromosome Region 13q11

Author

Andrea Richter, Kenneth Morgan, James C. Engert, Bing Ge, Christine Bétard, Serge B. Melançon, Jocelyne Mercier, Thomas J. Hudson, Pierre Bérubé, Bruce W. Birren, Keri Devon, Carolyn Owen, Carole Doré, and John D. Rioux

Subjects

Candidate gene, Transcription, Genetic, Genes, Recessive, Biology, Contig Mapping, Gene mapping, Genetic linkage, Chromosome regions, Genetics, Humans, Bacteriophage P1, Chromosomes, Artificial, Yeast, Gene Library, Sequence Tagged Sites, Spinocerebellar Degenerations, Chromosome 13, Polymorphism, Genetic, Chromosomes, Human, Pair 13, Contig, Haplotype, food and beverages, Chromosome, Chromosomes, Bacterial, Physical Chromosome Mapping, Genes

Abstract

Autosomal recessive spastic ataxia of Charlevoix–Saguenay (ARSACS or SACS) is a neurodegenerative disease frequent in northeastern Quebec. In a previous study, we localized the disease gene to chromosome region 13q11 by identifying excess sharing of a marker allele in patients followed by linkage analysis and haplotyping. To create a detailed physical map of this region, we screened CEPH mega-YACs with 41 chromosome 13 sequence-tagged-sites (STSs) known to map to 13q11–q12. The YAC contig, composed of 27 clones, extends on the genetic map from D13S175 to D13S221, an estimated distance of at least 19.3 cM. A high-resolution BAC and PAC map that includes the ARSACS critical region flanked by D13S1275 and D13S292 was constructed. These YAC and BAC/PAC maps allowed the accurate placement of 29 genes and ESTs previously mapped to the proximal region of chromosome 13q. We confirmed the position of two candidate genes within the critical region and mapped the other 27 genes and ESTs to nearby intervals. Six BAC/PAC clones form a contig between D13S232 and D13S787 for sequencing within the ARSACS critical region.

Published

1999

17. Exclusion of linkage of Shwachman-Diamond syndrome to chromosome regions 6q and 12q implicated by a de novo translocation

Author

Sharan Goobie, Mitsuo Masuno, Kiyoshi Imaizumi, T. Mary Fujiwara, Jodi Morrison, Kenneth Morgan, Lynda Ellis, Mary Corey, Peter R. Durie, Hedy Ginzberg, Yoshikazu Kuroki, and Johanna M. Rommens

Subjects

Genetic Markers, Male, congenital, hereditary, and neonatal diseases and abnormalities, Genetic Linkage, Chromosomal translocation, Chromosomal rearrangement, Biology, Bone and Bones, Translocation, Genetic, Gene mapping, Chromosome regions, medicine, Humans, Pancreas, Genetics (clinical), Genetics, Shwachman–Diamond syndrome, Chromosomes, Human, Pair 12, Haplotype, Genetic disorder, Syndrome, medicine.disease, Hematologic Diseases, Penetrance, Pedigree, Chromosomes, Human, Pair 6, Female, Lod Score

Abstract

Shwachman-Diamond syndrome is a rare genetic disorder of unknown pathogenesis involving exocrine pancreatic insufficiency and hematological and skeletal abnormalities. There is broad clinical variability; the extent of heterogeneity is unknown but comparisons within a large cohort of patients show no striking differences between patients of families with single or multiple affected offspring. Segregation analysis of a cohort of 69 families has suggested an autosomal recessive mode of inheritance. A single constitutional de novo chromosome rearrangement was reported in a Japanese patient involving a balanced translocation, t(6;12)(q16.2;q21.2), thereby suggesting possible loci for a genetic defect. Evenly spaced microsatellite markers spanning 26-32 cM intervals from D6S1056 to D6S304 and D12S375 to D12S346 were analyzed for linkage in members of 13 Shwachman-Diamond syndrome families with two or three affected children. Two-point lod scores were calculated for each marker under assumptions of recessive inheritance and complete penetrance. Negative lod scores indicated exclusion of both chromosome regions. Further, affected sibs were discordant for inheritance of chromosomes in most families based on constructed haplotypes. The cytogenetic abnormality is not associated with most cases of Shwachman-Diamond syndrome.

Published

1999

18. Location Score and Haplotype Analyses of the Locus for Autosomal Recessive Spastic Ataxia of Charlevoix-Saguenay, in Chromosome Region 13q11

Author

Andrea Richter, Jean-Pierre Bouchard, Josée Poirier, John D. Rioux, Gabor Gyapay, Jean Mathieu, Thomas J. Hudson, Kenneth Morgan, Jean Weissenbach, Dominique Julien, Serge B. Melançon, Bing Ge, and Jocelyne Mercier

Subjects

Ataxia, Databases, Factual, Genotype, Genetic Linkage, DNA Mutational Analysis, Locus (genetics), Biology, ARSACS (see Autosomal recessive spastic ataxia of Charlevoix-Saguenay), SGCG, Genetic linkage, Sarcoglycans, Autosomal recessive spastic ataxia of Charlevoix-Saguenay, Genetics, medicine, Humans, Point Mutation, Genetics(clinical), Allele, Alleles, Genetics (clinical), Spinocerebellar Degenerations, Chromosome 13, Membrane Glycoproteins, Polymorphism, Genetic, Chromosomes, Human, Pair 13, Haplotype, Quebec, Spastic ataxia, Exons, Syndrome, Founder effect, Cytoskeletal Proteins, Haplotypes, Lod Score, medicine.symptom, Microsatellite Repeats, Research Article

Abstract

Summary Autosomal recessive spastic ataxia of Charlevoix-Saguenay (ARSACS) is a clinically homogeneous form of early-onset familial spastic ataxia with prominent myelinated retinal nerve fibers. More than 300 patients have been identified, and most of their families originated in the Charlevoix-Saguenay region of northeastern Quebec, where the carrier prevalence has been estimated to be 1/22. Consistent with the hypothesis of a founder effect, we observed excess shared homozygosity at 13q11, among patients in a genomewide scan of 12 families. Analysis of 19 pedigrees demonstrated very tight linkage between the ARSACS locus and an intragenic polymorphism of the γ-sarcoglycan ( SGCG ) gene, but genomic DNA sequence analysis of all eight exons of SGCG revealed no disease-causing mutation. On the basis of haplotypes composed of seven marker loci that spanned 11.1 cM, the most likely position of the ARSACS locus was 0.42 cM distal to the SGCG polymorphism. Two groups of ARSACS-associated haplotypes were identified: a large group that carries a common SGCG allele and a small group that carries a rare SGCG allele. The haplotype groups do not appear to be closely related. Therefore, although chromosomes within each haplotype group may harbor a single ARSACS mutation identical by descent, the two mutations could have independent origins.

Published

1999

19. Validation of linkage by sampling based on environmental exposures

Author

Kenneth Morgan, Carl Brewer, and Celia M. T. Greenwood

Subjects

Linkage (software), medicine.diagnostic_test, Epidemiology, Genetic linkage, Covariate, Statistics, medicine, Sampling (statistics), Sample (statistics), Biology, Gene–environment interaction, Genetics (clinical), Genetic testing

Abstract

After detecting linkage in one sample, most researchers will attempt to validate this finding in another sample. Three strategies for validating a primary linkage were compared, with a focus on methods that might be appropriate in the presence of gene x environment interaction. First, a validation sample was collected and analyzed using the same ascertainment procedure and methods as the primary sample. Second, a sample of families with particular exposure patterns were ascertained subsequent to a significant test for heterogeneity due to the exposure in the primary sample. A third strategy ascertained by exposure status when exposure-defined subgroup tests were significant in the primary sample. The second strategy reduced the number of false positive linkage signals identified through exposure subgroup identification (i.e., the third strategy), but in this GAW11 data that contained no qualitative gene x environment interactions, it had poor sensitivity. Power to detect heterogeneity depends on the differences in risk between exposed and unexposed.

Published

1999

20. Founder BRCA1 and BRCA2 Mutations in French Canadian Breast and Ovarian Cancer Families

Author

Kenneth Morgan, P. Andrew Futreal, Steven A. Narod, Patricia N. Tonin, William D. Foulkes, David E. C. Cole, Anne-Marie Mes-Masson, Parviz Ghadirian, Diane Provencher, and Michelle Mahon

Subjects

Genetic Markers, Canada, endocrine system diseases, Genetic counseling, Genes, BRCA1, Breast Neoplasms, Biology, medicine.disease_cause, Polymerase Chain Reaction, Breast cancer, Ovarian cancer, medicine, Genetics, Humans, Point Mutation, Family, Genes, Tumor Suppressor, Genetics(clinical), skin and connective tissue diseases, Genetics (clinical), DNA Primers, Sequence Deletion, BRCA2 Protein, Ovarian Neoplasms, Mutation, BRCA1 Protein, Point mutation, Cancer, Neoplasms, Second Primary, Middle Aged, Founder effect, BRCA1, medicine.disease, BRCA2, Neoplasm Proteins, French Canadians, Female, France, Research Article, Transcription Factors

Abstract

SummaryWe have identified four mutations in each of the breast cancer–susceptibility genes, BRCA1 and BRCA2, in French Canadian breast cancer and breast/ovarian cancer families from Quebec. To identify founder effects, we examined independently ascertained French Canadian cancer families for the distribution of these eight mutations. Mutations were found in 41 of 97 families. Six of eight mutations were observed at least twice. The BRCA1 C4446T mutation was the most common mutation found, followed by the BRCA2 8765delAG mutation. Together, these mutations were found in 28 of 41 families identified to have a mutation. The odds of detection of any of the four BRCA1 mutations was 18.7× greater if one or more cases of ovarian cancer were also present in the family. The odds of detection of any of the four BRCA2 mutations was 5.3× greater if there were at least five cases of breast cancer in the family. Interestingly, the presence of a breast cancer case

Published

1998

21. A Gene for Autosomal Recessive Limb-Girdle Muscular Dystrophy in Manitoba Hutterites Maps to Chromosome Region 9q31-q33: Evidence for Another Limb-Girdle Muscular Dystrophy Locus

Author

Gail Coghlan, Edward Nylen, Klaus Wrogemann, Tracey Weiler, T M Fujiwara, Teresa Zelinski, M J Crumley, Cheryl R. Greenberg, and Kenneth Morgan

Subjects

Genetic Markers, Genotype, Genetic Linkage, Genes, Recessive, Locus (genetics), Chromosome 9q31-q33, Biology, Muscular Dystrophies, Gene mapping, Genetic linkage, Fukuyama congenital muscular dystrophy, Genetics, medicine, Humans, Genetics(clinical), Genetics (clinical), Linkage, Muscles, Haplotype, Chromosome Mapping, Manitoba, Hutterites, medicine.disease, Pedigree, Haplotypes, Genetic marker, Chromosomal region, Limb-girdle muscular dystrophy, DNA pooling, Lod Score, Chromosomes, Human, Pair 9, Research Article

Abstract

Characterized by proximal muscle weakness and wasting, limb-girdle muscular dystrophies (LGMDs) are a heterogeneous group of clinical disorders. Previous reports have documented either autosomal dominant or autosomal recessive modes of inheritance, with genetic linkage studies providing evidence for the existence of at least 12 distinct loci. Gene products have been identified for five genes responsible for autosomal recessive forms of the disorder. We performed a genome scan using pooled DNA from a large Hutterite kindred in which the affected members display a mild form of autosomal recessive LGMD. A total of 200 markers were used to screen pools of DNA from patients and their siblings. Linkage between the LGMD locus and D9S302 (maximum LOD score 5.99 at recombination fraction .03) was established. Since this marker resides within the chromosomal region known to harbor the gene causing Fukuyama congenital muscular dystrophy (FCMD), we expanded our investigations, to include additional markers in chromosome region 9q31-q34.1. Haplotype analysis revealed five recombinations that place the LGMD locus distal to the FCMD locus. The LGMD locus maps close to D9S934 (maximum multipoint LOD score 7.61) in a region that is estimated to be approximately 4.4 Mb (Genetic Location Database composite map). On the basis of an inferred ancestral recombination, the gene may lie in a 300-kb region between D9S302 and D9S934. Our results provide compelling evidence that yet another gene is involved in LGMD; we suggest that it be named "LGMD2H."

Published

1998

22. Parental Origin–Dependent, Male Offspring–Specific Transmission-Ratio Distortion at Loci on the Human X Chromosome

Author

Mark Leppert, Carmen Sapienza, Anna K. Naumova, David F. Barker, and Kenneth Morgan

Subjects

Genetics, 0303 health sciences, Chromosome X, Offspring, Embryo, Locus (genetics), Biology, 03 medical and health sciences, symbols.namesake, 0302 clinical medicine, Parental origin, Male offspring, Mendelian inheritance, symbols, Genetics(clinical), Epigenetics, Allele, Genomic imprinting, 030217 neurology & neurosurgery, Genetics (clinical), X chromosome, Transmission-ration distortion, 030304 developmental biology

Abstract

Summary We have analyzed the transmission of maternal alleles at loci spanning the length of the X chromosome in 47 normal, genetic disease–free families. We found a significant deviation from the expected Mendelian 1:1 ratio of grandpaternal:grandmaternal alleles at loci in Xp11.4-p21.1. The distortion in inheritance ratio was found only among male offspring and was manifested as a strong bias in favor of the inheritance of the alleles of the maternal grandfather. We found no evidence for significant heterogeneity among the families, which implies that the major determinant involved in the generation of the non-Mendelian ratio is epigenetic. Our analysis of recombinant chromosomes inherited by male offspring indicates that an 11.6-cM interval on the short arm of the X chromosome, bounded by DXS538 and DXS7, contains an imprinted gene that affects the survival of male embryos.

Published

1998

23. Limb girdle muscular dystrophy in Manitoba Hutterites does not map to any of the known LGMD loci

Author

T. Mary Fujiwara, Barbara Triggs-Raine, Edward Nylen, M. Joyce Crumley, Teresa Zelinski, William Halliday, Tracey Weiler, Kenneth Morgan, Cheryl R. Greenberg, Barbara E. Nickel, and Klaus Wrogemann

Subjects

musculoskeletal diseases, Genetics, Candidate gene, Locus (genetics), Limb girdle, Biology, medicine.disease, Phenotype, Gene mapping, Genetic linkage, medicine, Muscular dystrophy, Genetics (clinical), Limb-girdle muscular dystrophy

Abstract

Limb girdle muscular dystrophy (LGMD) is a heterogeneous group of disorders affecting primarily the shoulder and pelvic girdles. Autosomal dominant and recessive forms have been identified; 8 have been mapped and 1 more has been postulated on the basis of exclusion of linkage. An autosomal recessive muscular dystrophy was first described in 1976 in the Hutterite Brethren, a North American genetic and religious isolate [Shokeir and Kobrinsky, 1976; Clin Genet 9:197–202]. In this report, we discuss the results of linkage analysis in 4 related Manitoba Hutterite sibships with 21 patients affected with a mild autosomal recessive form of LGMD. Because of the difficulties in assigning a phenotype in some asymptomatic individuals, stringent criteria for the affected phenotype were employed. As a result, 7 asymptomatic relatives with only mildly elevated CK levels were assigned an unknown phenotype to prevent their possible misclassification. Two-point linkage analysis of the disease locus against markers linked to 7 of the known LGMD loci and 3 other candidate genes yielded lod scores of ≤−2 at θ=0.01 in all cases and in most cases at θ=0.05. This suggests that there is at least 1 additional locus for LGMD. Am. J. Med. Genet. 72:363–368, 1997. © 1997 Wiley-Liss, Inc.

Published

1997

24. SMNT and NAIP mutations in Canadian families with spinal muscular atrophy (SMA): Genotype/phenotype correlations with disease severity

Author

Camille Rochette, Kenneth Morgan, Alexandre Semionov, Louise R. Simard, and Michel Vanasse

Subjects

Male, Canada, Genotype, Nerve Tissue Proteins, Locus (genetics), Biology, Muscular Atrophy, Spinal, Exon, Genotype-phenotype distinction, medicine, Humans, Allele, Cyclic AMP Response Element-Binding Protein, Genetics (clinical), Genetics, Chimera, RNA-Binding Proteins, SMN Complex Proteins, Exons, Spinal muscular atrophy, SMA, medicine.disease, Introns, Neuronal Apoptosis-Inhibitory Protein, Pedigree, Phenotype, Haplotypes, Female, NAIP, Gene Deletion

Abstract

Childhood-onset spinal muscular atrophy (SMA) is an autosomal recessive neuropathy characterized by selective degeneration of alpha-motor neuron cells of the spinal cord. Age of onset and motor development varies greatly among patients, but the molecular basis of this variability remains unclear. The SMA locus contains two copies of a 500-kb element and deletions within the telomeric element have been shown to be the most common cause of SMA. To study the relationship between genotype and phenotype, 60 SMA families, all but two of which are of French Canadian origin, were screened for deletions in the telomeric survival motor neuron (SMN(T)) and the intact neuronal apoptosis inhibitory protein (NAIP) genes. Combining these results with those obtained for the multicopy microsatellite marker Ag1-CA (D5S1556) indicated that there are at least two types of SMA alleles. Most type I SMA patients are homozygous for large scale deletions involving the entire SMN(T) gene as well as exons 5 and 6 of the NAIP gene. The strong association between the 100-bp allele of Ag1-CA and large scale deletions in populations of diverse ethnic origin suggests that this allele marks an unstable or founder SMA chromosome. In contrast, most chronic SMA patients have at least one SMA allele with either an intragenic SMN(T) deletion or a SMN(C):SMN(T) chimeric gene which replaces the normal SMN(T) gene. The broad continuum of disease presentation in chronic SMA is most likely a consequence of the interaction between different SMA alleles.

Published

1997

25. Phenotypic variability in friedreich ataxia: Role of the associated GAA triplet repeat expansion

Author

Josée Poirier, Marie-Helene Seni, Stefano Di Donato, Laura Montermini, Serge B. Melançon, Gail Graham, Dominique Julien, Michel Vanasse, Kenneth Morgan, Bernard Lemieux, Jean-Pierre Bouchard, Bronya J.B. Keats, Andrea Richeter, Frederick Andermann, Jocelyne Mercier, Eva Andermann, Fiorentino Capozzoli, Massimo Pandolfo, Cristina M. Justice, Barbara Castellotti, and Jean Mathieu

Subjects

Genetics, Pathology, medicine.medical_specialty, Ataxia, biology, Triplet repeat, Haplotype, medicine.disease, Phenotype, Degenerative disease, Neurology, Polymorphism (computer science), Frataxin, biology.protein, medicine, Neurology (clinical), medicine.symptom, Repeated sequence

Abstract

We studied genotype-phenotype correlations in a group of 100 patients with typical Friedreich ataxia (FRDA), and in three groups of patients with atypical clinical presentations, including 44 Acadian FRDA, 8 late-onset FRDA (LOFA), and 6 FRDA with retained reflexes (FARR). All patients, except 3 with typical FRDA, carried two copies of the FRDA-associated GAA triplet repeat expansion. Overall, the phenotypic spectrum of FRDA appeared to be wider than defined by the currently used diagnostic criteria. Our study indicated the existence of several sources of variability in FRDA. Patients with larger GAA expansions tended to have earlier onset and were more likely to show additional manifestations of the disease. Mitotic instability of the expanded GAA repeats may partially account for the limited degree of correlation between expansion sizes as determined in lymphocytes and clinical parameters. Some clinical variants associated with specific FRDA haplotypes, such as Acadian FRDA and FARR, turned out to be unrelated to expansion sizes. No polymorphism in the frataxin coding sequence could be associated with these clinical variants.

Published

1997

26. Modeling the phenotype in parametric linkage analysis of bipolar disorder

Author

Gustavo Turecki, Kenneth Morgan, and Guy A. Rouleau

Subjects

Linkage (software), Genetics, Bipolar Disorder, Models, Statistical, Models, Genetic, Genetic Linkage, Epidemiology, Penetrance, Computational biology, Biology, medicine.disease, Phenotype, Exploratory data analysis, Risk Factors, Genetic linkage, medicine, Trait, Humans, Bipolar disorder, Lod Score, Genetics (clinical), Psychiatric genetics, Parametric statistics

Abstract

The definition of phenotype is a major problem in genetic studies of psychiatric disorders. Most linkage studies in bipolar disorder have defined the phenotype as a dichotomous trait and have usually employed different hierarchical classifications in order to overcome uncertainty resulting from phenotypic variability. In this study we explored the advantages of maximizing the evidence for linkage over different phenotypic definitions when conducting parametric linkage analysis of a complex trait. The GAW10 Problem 1 was used, focusing on chromosome 18 data sets. Three major phenotypic models were analyzed: quasi-quantitative, liability-based and affection-status models. Overall, no single phenotypic model performed consistently better than the others (i.e., lod scores greater than 1.0). Each model yielded higher lod scores than the others in particular instances, suggesting that it might be useful in exploratory data analysis, where the phenotype is variable, to maximize evidence for linkage over different phenotypic models.

Published

1997

27. Friedreich ataxia in Acadian families from eastern Canada: Clinical diversity with conserved haplotypes

Author

Kenneth Morgan, J.P. Bouchard, D Julien, J Poirier, M. Roy, Andrea Richter, Jocelyne Mercier, F Gosselin, and Serge B. Melançon

Subjects

Genetics, Ataxia, Gene mapping, Hereditary Diseases, Haplotype, medicine, Gene mutation, Biology, medicine.symptom, Genetic recombination, Gene, Phenotype, Genetics (clinical)

Abstract

The gene for Friedreich ataxia (FRDA), an autosomal-recessive neurodegenerative disease, remains elusive. The current candidate region of about 150 kb lies between loci FR2 and F8101 near the D9S15/D9S5 linkage group at 9q13-21.1. Linkage homogeneity between classical FRDA and a milder, slowly progressive Acadian variant (FRDA-Acad) has been demonstrated. An extended D9S15-D9S5 haplotype (C6) predominates in FRDA-Acad chromosomes from Louisiana. We studied 10 Acadian families from New Brunswick, Canada. In eight families, affected individuals conformed to the clinical description of FRDA-Acad; in one, 2 sibs presented with spastic ataxia (SPA-Acad). In the last family, 2 sibs had FRDA-Acad, and one had SPA-Acad. We found that SPA-Acad is linked to the FRDA gene region. The C6 haplotype and a second major haplotype (B7) were identified. The same ataxia-linked haplotypes segregated with both FRDA-Acad and SPA-Acad in two unrelated families. The parental origins of these haplotypes were different. Our observation of different phenotypes associated with the same combination of haplotypes may point to the influence of the parent of origin on gene expression, indicate the effect of modifier genes, or reflect the presence of different mutations on the same haplotypes. Our findings underline the need to investigate families with autosomal-recessive ataxias for linkage to the FRDA region, despite lack of key diagnostic manifestations such as cardiomyopathy or absent deep-tendon reflexes.

Published

1996

28. The Human Mammary-Derived Growth Inhibitor (MDGI) Gene: Genomic Structure and Mutation Analysis in Human Breast Tumors

Author

Kenneth Morgan, P. Andrew Futreal, Catherine M. Phelan, M.H. Ruttledge, Stephen Baird, Huynh Hung, Michael Pollak, Catharina Larsson, Patricia N. Tonin, Steven A. Narod, and Robert G. Korneluk

Subjects

Genetic Markers, Heterozygote, Tumor suppressor gene, Molecular Sequence Data, Breast Neoplasms, DNA, Satellite, Gene mutation, Biology, Fatty Acid-Binding Proteins, medicine.disease_cause, Loss of heterozygosity, Exon, Gene mapping, Genetics, medicine, Humans, Genes, Tumor Suppressor, Cloning, Molecular, Regulation of gene expression, Polymorphism, Genetic, Base Sequence, Exons, Middle Aged, Candidate Tumor Suppressor Gene, Molecular biology, Introns, Chromosomes, Human, Pair 1, Mutation, Cancer research, Female, Carrier Proteins, Carcinogenesis, Fatty Acid Binding Protein 3

Abstract

The mammary-derived growth inhibitor (MDGI) gene is a candidate tumor suppressor gene for human breast cancer. It has been shown to reduce the tumorigenicity of breast cancer cell lines in nude mice, and loss of expression of this gene has been shown in primary breast tumors. Furthermore, the human MDGI gene has been mapped to human chromosome 1p32-p35, a common region of deletion in sporadic breast tumors. We have determined the genomic structure of the human MDGI gene from a cosmid clone mapping to chromosome 1p32-p35 and have more finely mapped the MDGI gene relative to chromosome 1p microsatellite markers. The gene covers approximately 8 kb of genomic DNA and is divided into four exons. In an attempt to identify possible inactivating mutations in the MDGI gene in human breast cancer, we have sequenced all four exons and their surrounding splice junctions in 30 sporadic breast tumors. Ten of these tumors showed loss of heterozygosity (LOH) in the 1p32-p35 regions, with 5 tumors showing LOH in the subregion containing the MDGI gene. No mutations were found in this analysis. A polymorphism was identified in exon 2 in the constitutional DNA of 1/30 cases in this study, which resulted in themore » conversion of a lysine to an arginine residue at codon 53. This variant was present in the constitutional DNA of a further 3/26 women with sporadic breast cancer and 2/90 control individual (P=0.20). Despite experimental evidence that MDGI has tumor suppressor activity, our data suggest that mutations in the coding region are uncommon in human breast tumorigenesis. 29 refs., 3 figs., 2 tabs.« less

Published

1996

29. Large-scale cloning of human chromosome 2-specific yeast artificial chromosomes (YACs) using an interspersed repetitive sequences (IRS)-PCR approach

Author

T. Mary Fujiwara, David E. Housman, Jian-Xue Wang, Erwin Schurr, Kenneth Morgan, Vincent P. Stanton, Jing Liu, M. Joyce Crumley, Rebeca Rezonzew, and Philippe Gros

Subjects

Yeast artificial chromosome, congenital, hereditary, and neonatal diseases and abnormalities, Molecular Sequence Data, Alu element, chemical and pharmacologic phenomena, DNA, Satellite, Hybrid Cells, Biology, Polymerase Chain Reaction, Cricetinae, hemic and lymphatic diseases, Chromosome 19, Chromosome regions, Genetics, Animals, Humans, Cloning, Molecular, Chromosomes, Artificial, Yeast, Repetitive Sequences, Nucleic Acid, Base Sequence, Contig, Genome, Human, Chromosome, Interspersed Repetitive Sequences, Chromosomes, Human, Pair 2, Chromosome 22

Abstract

We report here an efficient approach to the establishment of extended YAC contigs on human chromosome 2 by using an interspersed repetitive sequences (IRS)-PCR-based screening strategy for YAC DNA pools. Genomic DNA was extracted from 1152 YAC pools comprised of 55,296 YACs mostly derived from the CEPH Mark I library. Alu -element-mediated PCR was performed for each pool, and amplification products were spotted on hybridization membranes (IRS filters). IRS probes for the screening of the IRS filters were obtained by Alu -element-mediated PCR. Of 708 distinct probes obtained from chromosome 2-specific somatic cell hybrids, 85% were successfully used for library screening. Similarly, 80% of 80 YAC walking probes were successfully used for library screening. Each probe detected an average of 6.6 YACs, which is in good agreement with the 7- to 7.5-fold genome coverage provided by the library. In a preliminary analysis, we have identified 188 YAC groups that are the basis for building contigs for chromosome 2. The coverage of the telomeric half of chromosome 2q was considered to be good since 31 of 34 microsatellites and 22 of 23 expressed sequence tags that were chosen from chromosome region 2q13–q37 were contained in a chromosome 2 YAC sublibrary generated by our experiments. We have identified a minimum of 1610 distinct chromosome 2-specific YACs, which will be a valuable asset for the physical mapping of the second largest human chromosome.

Published

1995

30. Allelic association and deletions in autosomal recessive proximal spinal muscular atrophy: association of marker genotype with disease severity and candidate cDNAs

Author

Klaus Zerres, Kenneth Morgan, A. Dadze, Arthur H.M. Burghes, Sabine Rudnik-Schöneborn, Christine J. DiDonato, Brunhilde Wirth, E. Hahnen, and Louise R. Simard

Subjects

Genetic Markers, Male, Heterozygote, Candidate gene, DNA, Complementary, Genotype, Genes, Recessive, Biology, Compound heterozygosity, Muscular Dystrophies, Spinal Cord Diseases, Genetics, medicine, Humans, Allele, Molecular Biology, Alleles, Genetics (clinical), Models, Genetic, General Medicine, Spinal muscular atrophy, medicine.disease, SMA, Pedigree, Genotype frequency, Phenotype, Haplotypes, Chromosomes, Human, Pair 5, Female, NAIP, Gene Deletion

Abstract

The candidate region for spinal muscular atrophy (SMA) has been defined as a 750 kb interval on 5q13. In this study, we performed allelic association studies in 154 German SMA families with the multicopy markers Ag1-CA (D5S1556) ; C212 (D5F149S1/S2) and correlated genotype data with deletion of candidate genes. Both multicopy markers recognize 0-3 alleles pro chromosome. Deletions were detected for all copies of the markers Agl-CA (C272) and C212 in 13 of 88 (15%) type I SMA patients and three of 48 (6%) type II patients. In all informative cases, the deletion was inherited from one parent. In two further cases (one type I and one type III SMA), de novo deletions of only one copy of Agl-CA and C212 were found. In both cases the patients were homozygously deleted for the survival motor neuron (SMN) gene (exons 7 and 8) but only the type I SMA patient was deleted for the neuronal apoptosis inhibitory protein (NAIP) gene (exons 5 and 6). A third case (type II SMA) showed de novo deletion of SMN, but not of Agl-CA, C212 and NAIP. Specific alleles of Agl-CA and C212 showed significant association with SMA, particularly in type I SMA. When the number of marker copies defines genotypes, 1,1 (one allele on each chromosome) is found to be increased in type I SMA (50%) and 1,2 (one allele on one chromosome and two alleles on the other one) in type II SMA (60%). The 2,2 genotype (two alleles on each chromosome) was found in 4% of type I and II patients. By comparison, pooled normal genotype frequencies were 20, 44 and 36%, respectively. These results suggest a strong correlation between genotype and severity of disease. Based on these data we propose a model which indicates that type I SMA patients are composed of two severe alleles, type II of a mild and a severe, and type III of two mild alleles. Correlation of Agl-CA genotype with deletion of the XS2G3/NAIP genes indicates that most patients with a deletion have a 1,1 genotype. Owing to the physical proximity of these markers, we propose that a large deletion occurs on type I SMA chromosomes that removes DNA between C212 and XS2G3/NAIP and that type II SMA results from compound heterozygosity for mild (small deletion) and severe mutations.

Published

1995

31. The oculopharyngeal muscular dystrophy locus maps to the region of the cardiac α and β myosin heavy chain genes on chromosome 14q11.2−q13

Author

Michel Fardeau, Ya-Gang Xie, Kenneth Morgan, Marc Sanson, Jean-Pierre Bouchard, Guy A. Rouleau, Amos D. Korczyn, Jean Weissenbach, Sergiu C. Blumen, Fernando M.S. Tomé, and Bernard Brais

Subjects

Genetic Markers, Male, Genetic Linkage, Molecular Sequence Data, Population, Locus (genetics), Myosins, Biology, Muscular Dystrophies, White People, Oculopharyngeal muscular dystrophy, Gene mapping, Myosin, Genetics, medicine, Blepharoptosis, Humans, Muscular dystrophy, Muscle, Skeletal, education, Molecular Biology, Genetics (clinical), Chromosomes, Human, Pair 14, Inclusion Bodies, Recombination, Genetic, education.field_of_study, Base Sequence, Chromosome Mapping, General Medicine, medicine.disease, Pedigree, Haplotypes, Genetic marker, Female, MYH7, Deglutition Disorders

Abstract

Oculopharyngeal muscular dystrophy (OPMD) is a late-onset autosomal dominant muscular dystrophy which presents typically after the age of 50 with progressive eyelid drooping and an increasing difficulty in swallowing. Though OPMD has a world-wide incidence, it is more common in the French Canadian population. We have identified a homogeneous group of families and studied 166 polymorphic markers as part of a genome search before establishing linkage to chromosome 14. We determined that the OPMD locus maps to a less than 5 cM region of chromosome 14q11.2-q13. The maximum two-point lod score in three French Canadian families of 14.73 (theta = 0.03) was obtained for an intronic cardiac beta myosin heavy chain gene (MYH7) marker. The regional localization for the OPMD locus raises the intriguing possibility that either the cardiac alpha or beta myosin heavy chain genes may play a role in this disease.

Published

1995

32. Susceptibility to Progressive Cryptococcus neoformans Pulmonary Infection Is Regulated by Loci on Mouse Chromosomes 1 and 9

Author

Kenneth Morgan, Scott F. Carroll, Adam Flaczyk, T. Mary Fujiwara, Robert J. Homer, Salman T. Qureshi, J C. Loredo-Osti, and Erin I. Lafferty

Subjects

Immunology, Quantitative Trait Loci, Microbiology, Pathogenesis, Mice, Immune system, Th2 Cells, medicine, Eosinophilia, Animals, Genetic Predisposition to Disease, Allele, Lung, Cryptococcal Pneumonia, Cryptococcus neoformans, Host Response and Inflammation, Mice, Inbred C3H, biology, Lung Diseases, Fungal, Cryptococcosis, Th1 Cells, biology.organism_classification, medicine.disease, Chromosomes, Mammalian, Neutrophilia, Infectious Diseases, Mice, Inbred CBA, Cytokines, Parasitology, medicine.symptom

Abstract

Genetic factors that regulate the pathogenesis of pneumonia caused by the fungus Cryptococcus neoformans are poorly understood. Through a phenotypic strain survey we observed that inbred C3H/HeN mice develop a significantly greater lung fungal burden than mice of the resistant CBA/J strain 4 weeks following intratracheal infection with C. neoformans ATCC 24067. The aim of the present study was to characterize the inflammatory response of C3H/HeN mice following C. neoformans pulmonary infection and to identify genetic loci that regulate host defense. Following cryptococcal infection, C3H/HeN mice demonstrated a Th2 immune response with heightened airway and tissue eosinophilia, goblet cell metaplasia, and significantly higher lung interleukin-5 (IL-5) and IL-13 protein expression relative to CBA/J mice. Conversely, CBA/J mice exhibited greater airway and tissue neutrophilia that was associated with significantly higher pulmonary expression of gamma interferon, CXCL10, and IL-17 proteins than C3H/HeN mice. Using the fungal burden at 4 weeks postinfection as a phenotype, genome-wide quantitative trait locus (QTL) analysis among 435 segregating (C3H/HeN × CBA/J)F2 (C3HCBAF2) hybrids identified two significant QTLs on chromosomes 1 ( Cnes4 ) and 9 ( Cnes5 ) that control susceptibility to cryptococcal pneumonia in an additive manner. Susceptible C3H/HeN mice carry a resistance allele at Cnes4 and a susceptibility allele at Cnes5 . These studies reveal additional genetic complexity of the host response to C. neoformans that is associated with divergent patterns of pulmonary inflammation.

Published

2012

33. Common origins of BRCA1 mutations in Canadian breast and ovarian cancer families

Author

Donna M Shattuck-Eidens, Carole Bélanger, David E. Goldgar, J.-F. Leblanc, Patricia N. Tonin, Johanna M. Rommens, Steven A. Narod, Qingyun Liu, Francine Durocher, Sebastien Gingras, Mark H. Skolnick, Chantal Samson, F. Dion, Fernand Labrie, Kenneth Morgan, and Jacques Simard

Subjects

Male, Canada, Molecular Sequence Data, Breast Neoplasms, Biology, medicine.disease_cause, Frameshift mutation, Breast cancer, Genetics, medicine, Humans, Amino Acid Sequence, Insertion, Allele, Frameshift Mutation, DNA Primers, Ovarian Neoplasms, Mutation, Base Sequence, BRCA1 Protein, Haplotype, Chromosome, medicine.disease, Neoplasm Proteins, Pedigree, Haplotypes, Female, Ovarian cancer, Transcription Factors

Abstract

Women who carry mutations in the BRCA1 gene on chromosome 17q have an 85% lifetime risk of breast cancer, and a 60% risk of ovarian cancer. We have identified BRCA1 mutations in 12 of 30 (40%) Canadian families with breast and/or ovarian cancer, including six of the eight families (75%) that contained two cases of early-onset breast cancer and two cases of ovarian cancer. Six frameshift mutations account for all 12 mutant alleles, including nucleotide insertions (two mutations) and deletions (four mutations). Four independent families carried the same 1 basepair (bp) insertion mutation in codon 1755 and four other families shared a 2 bp deletion mutation in codons 22-23. These families were not known to be related, but haplotype analysis suggests that the carriers of each of these mutations have common ancestors.

Published

1994

34. DNA haplotype analysis of Huntington disease reveals clues to the origins and mechanisms of CAG expansion and reasons for geographic variations of prevalence

Author

E. Almqvist, J Theilmann, N. Spence, Maria Anvret, K. Nichol, H Telenius, Ichiro Kanazawa, J. Goto, Leena Peltonen, Michael R. Hayden, Biaoyang Lin, Ferdinando Squitieri, Kenneth Morgan, Susan E. Andrew, J. Zelsler, J. Vesa, Jacquie Greenberg, G Napolitano, Y P Goldberg, and B. Kremer

Subjects

Canada, congenital, hereditary, and neonatal diseases and abnormalities, Linkage disequilibrium, Prevalence, Disease, Biology, Linkage Disequilibrium, chemistry.chemical_compound, Genetics, Humans, Allele, Molecular Biology, Gene, Genetics (clinical), Repetitive Sequences, Nucleic Acid, Polymorphism, Genetic, Asia, Eastern, Haplotype, DNA, General Medicine, Europe, Huntington Disease, Haplotypes, chemistry, Case-Control Studies, Africa, Mutation (genetic algorithm)

Abstract

This study of allelic association using three intra- and two extragenic markers within 150 kb of the Huntington disease (HD) mutation has provided evidence for linkage disequilibrium for four of five markers. Haplotype analysis of 67 HD families using markers in strong linkage disequilibrium with HD identified two haplotypes underlying 77.6% of HD chromosomes. Normal chromosomes with these two haplotypes had a mean number of CAG repeats significantly larger than and an altered distribution of CAG repeats compared with other normal chromosomes. Furthermore, haplotype analysis of five new mutation families reveals that HD has arisen on these same two chromosomal haplotypes. These findings suggest that HD arises more frequently on chromosomes with specific DNA haplotypes and higher CAG repeat lengths. We then studied CAG and CCG repeat lengths in the HD gene on 896 control chromosomes from different ancestries to determine whether the markedly reduced frequency of HD in Finland, Japan, China and African Blacks is associated with an altered frequency of DNA haplotypes and subsequently lower CAG lengths on control chromosomes compared to populations of Western European descent. The results show a highly significant inverse relationship between CAG and CCG repeat lengths. In populations with lowered prevalence rates of HD, CAG repeat lengths are smaller and the distribution of CCG alleles is markedly different from Western European populations. These findings suggest that, in addition to European emigration, new mutations make a contribution to geographical variation of prevalence rates and is consistent with a multistep model of HD developing from normal chromosomes with higher CAG repeat lengths.

Published

1994

35. Linkage disequilibrium analysis of childhood-onset spinal muscular atrophy (SMA) in the French — Canadian population

Author

Lemieux B, Jean Mathieu, Kenneth Morgan, S B Melancon, M Vanasse, G. Prescott, C. | Rochette, and Louise R. Simard

Subjects

Male, Canada, Linkage disequilibrium, Genetic Linkage, Duchenne muscular dystrophy, Population, Spinal Muscular Atrophies of Childhood, Biology, Linkage Disequilibrium, Gene mapping, Genetic linkage, Genetics, medicine, Humans, Age of Onset, Allele, Child, education, Molecular Biology, Genetics (clinical), Recombination, Genetic, education.field_of_study, General Medicine, Spinal muscular atrophy, medicine.disease, SMA, Haplotypes, Female, France

Abstract

Spinal muscular atrophy (SMA) is, after Duchenne muscular dystrophy, the most common neuromuscular disorder in childhood. The gene responsible for childhood SMA has been mapped to the q11.2-q13.3 region of chromosome 5. We have extended our linkage studies of SMA in the French-Canadian population to include microsatellite markers at the D5S125, D5S351, D5S435, JK53CA1/2 and MAP1B loci. These markers span about 4 cM of the SMA candidate region. We observed significant evidence for linkage between SMA and all the markers tested. The analysis of recombinant chromosomes provide evidence for the following genetic order: D5S125-D5S435-MAP1B-3'-JK53CA1/2 and places D5S351 proximal to JK53CA1/2. Furthermore, we confirm the current localization of the SMA gene distal to D5S435. Finally, we provide demonstration of significant linkage disequilibrium between childhood-onset SMA and four of the five marker loci, D5S125, D5S435, D5S351 and JK53CA1/2. Analysis of SMA-region haplotypes suggests that there may be a predominant SMA allele that is present on about 17% of SMA chromosomes in this sample of the French-Canadian population. We conclude that the observed linkage disequilibrium is likely due to genetic drift among regions of Quebec, consistent with this population's early history.

Published

1994

36. Genes involved in the metabolism of poly-unsaturated fatty-acids (PUFA) and risk for Crohn's disease in children & young adults

Author

David R. Mack, Philippe Lambrette, Kenneth Morgan, Colette Deslandres, Devendra Amre, Guy Grimard, Alfreda Krupoves, David M. Israel, Ernest G. Seidman, Emile Levy, and Irina Costea

Subjects

Male, Epidemiology, CYP4F2, lcsh:Medicine, Genome-wide association study, Inflammatory bowel disease, Biochemistry, Pediatrics, 0302 clinical medicine, Crohn Disease, Genotype, Child, Pediatric Epidemiology, lcsh:Science, Genetics, 0303 health sciences, Multidisciplinary, Child Health, Lipids, 3. Good health, Child, Preschool, Genetic Epidemiology, Fatty Acids, Unsaturated, Medicine, 030211 gastroenterology & hepatology, Female, Pediatric Gastroenterology, Public Health, Research Article, Adult, medicine.medical_specialty, Canada, Adolescent, Clinical Research Design, Single-nucleotide polymorphism, Gastroenterology and Hepatology, Biology, Leukotriene B4, Polymorphism, Single Nucleotide, 03 medical and health sciences, Internal medicine, medicine, SNP, Humans, Allele, Genetic Association Studies, 030304 developmental biology, Inflammation, Haplotype, Inflammatory Bowel Disease, lcsh:R, Genetic Variation, Human Genetics, medicine.disease, Lipid Metabolism, Endocrinology, Metabolism, Haplotypes, Case-Control Studies, lcsh:Q

Abstract

Background and Objectives Epidemiological evidence for the role of polyunsaturated fatty-acids (PUFA) in Crohn's disease (CD) is unclear, although the key metabolite leucotriene B4 (LTB4) is closely linked to the inflammatory process. We hypothesized that inherited variation in key PUFA metabolic enzymes may modify susceptibility for CD. Methods and Principal Results A case-control design was implemented at three pediatric gastroenterology clinics in Canada. Children ≤20 yrs diagnosed with CD and controls were recruited. 19 single nucleotide polymorphisms (SNPs) across the ALOX5 (4) CYP4F3 (5) and CYP4F2 (10) genes, were genotyped. Associations between SNPs/haplotypes and CD were examined. A total of 431 cases and 507 controls were studied. The mean (±SD) age of the cases was 12.4 (±3.3) years. Most cases were male (56.4%), had ileo-colonic disease (L3±L4, 52.7%) and inflammatory behavior (B1±p, 87%) at diagnosis. One genotyped CYP4F3 SNP (rs2683037) not in Hardy-Weinberg Equilibrium was excluded. No associations with the remaining 4 CYP4F3 SNPs with CD were evident. However haplotype analysis revealed associations with a two-marker haplotype (TG) (rs3794987 & rs1290617) (p = 0.02; permuted p = 0.08). CYP4F2 SNPs, rs3093158 (OR (recessive) = 0.56, 95% CI = 0.35–0.89; p = 0.01), rs2074902 (OR (trend) = 1.26, 95% CI = 1.00–1.60; p = 0.05), and rs2108622 (OR (recessive) = 1.6, 95% CI = 1.00–2.57; p = 0.05) were significantly associated whereas rs1272 (OR (recessive) = 0.58, 95% CI = 0.30–1.13; p = 0.10) showed suggestions for associations with CD. A haplotype comprising these 4 SNPs was significantly associated (p = 0.007, permuted p = 0.02) with CD. Associations with SNP rs3780901 in the ALOX5 gene were borderline non-significant (OR (dominant) = 1.29, 95% CI = 0.99–1.67; p = 0.056). A haplotype comprising the 4 ALOX5 SNPs (TCAA, p = 0.036) was associated with CD, but did not withstand corrections for multiple comparisons (permuted p = 0.14). Conclusions Inherited variation in enzymes involved in the synthesis/metabolism of LTB4 may be associated with CD. These findings implicate PUFA metabolism as a important pathway in the CD pathogenesis.

Published

2010

37. Cystic fibrosis mutations in French Canadians: Three CFTR mutations are relatively frequent in a Quebec population with an elevated incidence of cystic fibrosis

Author

T. Mary Fujiwara, G Aubin, Marc De Braekeleer, Linda Lamoureux, Maria Gerdes, J Daigneault, F Simard, Leonor Ferreira-Rajabi, Rima Rozen, and Kenneth Morgan

Subjects

medicine.medical_specialty, Cystic Fibrosis, Genotype, DNA Mutational Analysis, Population, medicine.disease_cause, Gastroenterology, Cystic fibrosis, Internal medicine, medicine, Humans, ΔF508, education, Genetics (clinical), Mutation, education.field_of_study, biology, business.industry, Incidence (epidemiology), Respiratory disease, Quebec, medicine.disease, Cystic fibrosis transmembrane conductance regulator, biology.protein, business, Founder effect

Abstract

The French-Canadian population in the Saguenay-Lac St. Jean region of northeastern Quebec has an elevated frequency of cystic fibrosis (CF). The average incidence of cystic fibrosis was 1 in 891 births and the prevalence of CF carriers was estimated to be 1 in 15. We tested for 10 mutations in the cystic fibrosis transmembrane conductance regulator (CFTR) gene in 133 French-Canadian CF families from Quebec. Ninety-one families were from the Saguenay-Lac St. Jean region and 42 families were referred from other regions of Quebec. We detected the CFTR mutation in 93 and 92% of the CF chromosomes in the Saguenay-Lac St. Jean and the major-urban Quebec families, respectively. The two groups of French-Canadian families were significantly different for the proportions of CFTR mutations. The three most common mutations in the Saguenay-Lac St. Jean families were delta F508 (58%), 621 + 1G----T (23%), and A455E (8%); and in the major-urban Quebec families were delta F508 (71%), 711 + 1G----T (9%), and 621 + 1G----T (5%). These results provide evidence for the role of founder effect in the elevated incidence of cystic fibrosis in the Saguenay-Lac St. Jean population.

Published

1992

38. Genetics of Leprosy

Author

Erwin Schurr, Emil Skamene, Kenneth Morgan, and Philippe Gros

Subjects

Genetic Linkage, Genes, MHC Class II, Tuberculoid leprosy, Hypopigmented skin, Disease, Biology, Hypopigmented skin lesions, Mice, HLA Antigens, Leprosy, Virology, medicine, Animals, Humans, Chronic infectious disease, Mycobacterium leprae, Mycobacterium Infections, Models, Genetic, Third world, medicine.disease, biology.organism_classification, Infectious Diseases, Chromosomes, Human, Pair 2, Immunology, Parasitology, Disease Susceptibility

Abstract

Leprosy is a chronic infectious disease of man which is caused by Mycobacterium leprae. It is mainly a disease of the skin and the peripheral nerves although, in some cases, M. leprae can be found in large numbers in other tissues. Presently, it is estimated that about 15 million people are affected by the disease, mainly in developing countries of the Third World. Clinically, a number of different forms of leprosy can be distinguished. Indeterminate leprosy is probably the earliest sign of infection. Only few, slightly hypopigmented skin plaques are seen and bacilli are detected only rarely in these lesions. Many of those affected by indeterminate leprosy resolve the infection without treatment and, like subclinically infected contacts, are considered as innately resistant to leprosy, thus defining the limits of resistance and susceptibility to clinically evident infection. Tuberculoid leprosy is characterized by the presence of few, hypopigmented skin lesions involving differing degrees of anesthesia.

Published

1991

39. Genetic control of innate resistance to mycobacterial infections

Author

Philippe Gros, Emil Skamene, Erwin Schurr, Danuta Radzioch, Ellen Buschman, Kenneth Morgan, and Danielle Malo

Subjects

Genetic Markers, Salmonella, Tuberculosis, Immunology, Biology, medicine.disease_cause, Microbiology, Mice, Leprosy, medicine, Animals, Humans, Interferon gamma, Gene, Genes, Dominant, Regulation of gene expression, Mycobacterium Infections, Macrophages, Chromosome Mapping, Macrophage Activation, biology.organism_classification, medicine.disease, Leishmania, Immunity, Innate, Phenotype, Gene Expression Regulation, Genetic marker, Parasitology, Mycobacterium, medicine.drug

Abstract

The Mendelian segregation of resistance to infection in different strains of mice infected with mycobacteria, Salmonella and Leishmania spp, all of which live in macrophages, is currently under close scrutiny. Here, Erwin Schurr and colleagues review the nature and function of the Bcg gene in controlling innate resistance to mycobacterial infection in mice and speculate on the occurrence of a possible human equivalent.

Published

1991

40. Sex differences in the genetic architecture of susceptibility to Cryptococcus neoformans pulmonary infection

Author

J C Loredo Osti, Loïc Guillot, Salman T. Qureshi, Kenneth Morgan, and Scott F. Carroll

Subjects

Male, Immunology, Locus (genetics), Quantitative trait locus, Mice, Quantitative Trait, Heritable, Genetics, medicine, Animals, Genetic Predisposition to Disease, Lung, Genetics (clinical), Cryptococcal Pneumonia, Cryptococcus neoformans, Sex Characteristics, biology, Cryptococcosis, Pneumonia, biology.organism_classification, Fungal pneumonia, medicine.disease, Genetic architecture, Immunity, Innate, Chromosome 17 (human), Mice, Inbred C57BL, Mice, Inbred CBA, Female

Abstract

Cryptococcus neoformans is a major cause of fungal pneumonia, meningitis and disseminated disease in the immune compromised host. Here we have used a clinically relevant model to investigate the genetic determinants of susceptibility to progressive cryptococcal pneumonia in C57BL/6J and CBA/J inbred mice. At 5 weeks after infection, the lung fungal burden was over 1000-fold higher in C57BL/6J compared to CBA/J mice. A genome-wide scan performed on 210 male and 203 female (CBA/J x C57BL/6J) F2 progeny using lung colony-forming units as a quantitative trait revealed a sex difference in genetic architecture with three loci (designated Cnes1-Cnes3) associated with susceptibility to cryptococcal pneumonia. Single locus analysis identified significant loci on chromosomes 3 (Cnes1) and 17 (Cnes2) with logarithm of the odds (LOD) scores of 4.09 (P=0.0110) and 7.30 (P

Published

2008

41. Identification of a chromosome 8p locus for early-onset coronary heart disease in a French Canadian population

Author

Daniel Gaudet, Christine Bétard, Carole Doré, Yannick Renaud, Mathieu Lemire, Nicole M. Roslin, Gérald Tremblay, Julie St-Pierre, T. Mary Fujiwara, Jill Platko, Janet Faith, Diane Brisson, Carl G. Brewer, Thomas J. Hudson, Andrei Verner, Corinne Darmond-Zwaig, Swneke D. Bailey, Kenneth Morgan, James C. Engert, John D. Rioux, and Alexandre Montpetit

Subjects

Adult, Genetic Markers, Male, Candidate gene, Population, Locus (genetics), Coronary Disease, Biology, Cohort Studies, Gene mapping, Genetic linkage, Genetics, Humans, Age of Onset, education, Genetics (clinical), Genetic association, Aged, Aged, 80 and over, education.field_of_study, Polymorphism, Genetic, Genome, Human, Quebec, Family aggregation, Chromosome Mapping, DNA, Middle Aged, Founder Effect, Female, France, Founder effect, Chromosomes, Human, Pair 8, Microsatellite Repeats

Abstract

Susceptibility to coronary heart disease (CHD) has long been known to exhibit familial aggregation, with heritability estimated to be greater than 50%. The French Canadian population of the Saguenay-Lac Saint-Jean region of Quebec, Canada is descended from a founder population that settled this region 300–400 years ago and this may provide increased power to detect genes contributing to complex traits such as CHD. Probands with early-onset CHD, defined by angiographically determined coronary stenosis, and their relatives were recruited from this population (average sibship size of 6.4). Linkage analysis was performed following a genome-wide microsatellite marker scan on 42 families with 284 individuals. Nonparametric linkage (NPL) analysis provided suggestive evidence for a CHD susceptibility locus on chromosome 8 with an NPL score of 3.14 (P=0.001) at D8S1106. Linkage to this locus was verified by fine mapping in an enlarged sample of 50 families with 320 individuals. This analysis provided evidence of linkage at D8S552 (NPL score=3.53, P=0.0003), a marker that maps to the same location as D8S1106. Candidate genes in this region, including macrophage scavenger receptor 1, farnesyl-diphosphate farnesyltransferase 1, fibrinogen-like 1, and GATA-binding protein 4, were resequenced in all coding exons in both affected and unaffected individuals. Association studies with variants in these and five other genes did not identify a disease-associated mutation. In conclusion, a genome-wide scan and additional fine mapping provide evidence for a locus on chromosome 8 that contributes to CHD in a French Canadian population.

Published

2007

42. Transmission ratio distortion in the myotonic dystrophy locus in human preimplantation embryos

Author

Anna K. Naumova, Seang Lin Tan, Kenneth Morgan, Nicola Dean, Asangla Ao, T. Mary Fujiwara, and J. Concepcion Loredo-Osti

Subjects

musculoskeletal diseases, Male, congenital, hereditary, and neonatal diseases and abnormalities, Heterozygote, Genotype, Offspring, Mothers, Locus (genetics), Fertilization in Vitro, Biology, Protein Serine-Threonine Kinases, Myotonic dystrophy, Myotonin-Protein Kinase, Fathers, Gene Frequency, Chromosome regions, Genetics, medicine, Humans, Myotonic Dystrophy, Allele, Gene, Genetics (clinical), Alleles, Repetitive Sequences, Nucleic Acid, Chromosome Mapping, Embryo, Myotonia, medicine.disease, Embryo, Mammalian, Spermatozoa, Blastocyst, Fertilization, Mutation, Female, Trinucleotide Repeat Expansion, Chromosomes, Human, Pair 19

Abstract

One form of myotonic dystrophy, dystrophia myotonica 1 (DM1), is caused by the expansion of a (CTG)(n) repeat within the dystrophia myotonica-protein kinase (DMPK) gene located in chromosome region 19q13.3. Unaffected individuals carry alleles with repeat size (CTG)(5-37), premutation carriers (CTG)(38-49) and DM1 affected individuals (CTG)(50-6,000). Preferential transmission both of expanded repeats from DM1-affected parents and larger DMPK alleles in the normal-size range have been reported in live-born offspring. To determine the moment in development when transmission ratio distortion (TRD) for larger normal-size DMPK alleles is generated, the transmission from heterozygous parents with one repeat within the (CTG)(5-18) range (Group I repeat) and the other within the (CTG)(19-37) range (Group II repeat) to human preimplantation embryos was analysed. A statistically significant TRD of 59% (95% confidence interval of 54-64) in favour of Group II repeats from both mothers and fathers was observed in preimplantation embryos, which remained significant when female embryos were considered separately. In contrast, no significant TRD was detected for repeats from informative Group I/Group I parents. Our analysis showed that Group II repeats specifically were preferentially transmitted in human preimplantation embryos. We suggest that TRD, in Group II repeats at the DMPK locus, is likely to result from events occurring at or around the time of fertilisation.

Published

2006

43. Mutations in TMEM76* cause mucopolysaccharidosis IIIC (Sanfilippo C syndrome)

Author

Jacek Majewski, Robert Ivanek, Jérôme Ausseil, Viktor Stránecký, Volkan Seyrantepe, Kenneth Morgan, David Roquis, Jiddeke M. van de Kamp, Nicole M. Roslin, Andrei Verner, Otto P. van Diggelen, Stanislav Kmoch, Ben J. H. M. Poorthuis, Irène Maire, T. Mary Fujiwara, Clare E. Beesley, Hana Hartmannová, Ron A. Wevers, Martin Hřebíček, Stéphanie Durand, Thomas J. Hudson, Jana Uřinovská, Alexey V. Pshezhetsky, Helena Poupětová, Alena Čížková, Jiří Zeman, Lenka Nosková, Pierre Lepage, Lenka Mrázová, Jakub Sikora, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, and Medical Biochemistry

Subjects

Male, DNA, Complementary, Energy and redox metabolism [NCMLS 4], Recombinant Fusion Proteins, Mucopolysaccharidosis, DNA Mutational Analysis, Molecular Sequence Data, Nonsense mutation, Gene Expression, Neuroinformatics [DCN 3], Biology, Transfection, medicine.disease_cause, Polymerase Chain Reaction, Article, Cell Line, Frameshift mutation, Mice, Mucopolysaccharidosis III, Acetyltransferases, Perception and Action [DCN 1], medicine, Genetics, Animals, Humans, Genetics(clinical), Amino Acid Sequence, Cloning, Molecular, Genetics (clinical), Mutation, Base Sequence, Sequence Homology, Amino Acid, Mucopolysaccharidosis Type IIIC, Chromosome Mapping, Exons, Glycostation disorders [IGMD 4], medicine.disease, Molecular biology, Neuromuscular development and genetic disorders [UMCN 3.1], Transmembrane protein, Pedigree, Transmembrane domain, Genetic defects of metabolism [UMCN 5.1], Female, Chromosomes, Human, Pair 8

Abstract

Contains fulltext : 50018.pdf (Publisher’s version ) (Closed access) Mucopolysaccharidosis IIIC (MPS IIIC, or Sanfilippo C syndrome) is a lysosomal storage disorder caused by the inherited deficiency of the lysosomal membrane enzyme acetyl-coenzyme A: alpha -glucosaminide N-acetyltransferase (N-acetyltransferase), which leads to impaired degradation of heparan sulfate. We report the narrowing of the candidate region to a 2.6-cM interval between D8S1051 and D8S1831 and the identification of the transmembrane protein 76 gene (TMEM76), which encodes a 73-kDa protein with predicted multiple transmembrane domains and glycosylation sites, as the gene that causes MPS IIIC when it is mutated. Four nonsense mutations, 3 frameshift mutations due to deletions or a duplication, 6 splice-site mutations, and 14 missense mutations were identified among 30 probands with MPS IIIC. Functional expression of human TMEM76 and the mouse ortholog demonstrates that it is the gene that encodes the lysosomal N-acetyltransferase and suggests that this enzyme belongs to a new structural class of proteins that transport the activated acetyl residues across the cell membrane.

Published

2006

44. Mapping of interactions and mouse congenic strains identified novel epistatic QTLs controlling the persistence of Salmonella Enteritidis in mice

Author

Danielle Malo, J C Loredo-Osti, J Caron, and Kenneth Morgan

Subjects

Male, Salmonella, Salmonella enteritidis, Immunology, Quantitative Trait Loci, Congenic, Salmonella infection, Biology, Quantitative trait locus, medicine.disease_cause, Mice, Sex Factors, Genetic linkage, Genetics, medicine, Animals, Genetics (clinical), Mice, Inbred BALB C, Chromosome Mapping, Epistasis, Genetic, medicine.disease, Genetic architecture, Salmonella Infections, Epistasis, Female

Abstract

The host response to infection in humans is multifactorial and involves the complex interaction between two genomes (the host and the pathogen) and the environment. Using an experimental mouse model of chronic infection, we have previously identified the individual effect of three significant and one suggestive quantitative trait loci (QTLs) (Ses1, Ses2, Ses3 and Ses1.1) on Salmonella Enteritidis persistence in target organs of 129S6/SvEvTac mice. Congenic strain construction was performed by transferring each of these QTLs from C57BL/6J onto the 129S6/SvEvTac background, and phenotypic analysis confirmed that Ses1 and Ses1.1 contribute to bacterial clearance. Additional QTLs regulating Salmonella carriage in 129S6/SvEvTac mice were identified using a two-locus epistasis QTL linkage mapping approach conducted separately in females and males. The epistatic model for females included the individual effect of Ses3 and two significant interactions (Ses1–D7Mit267 and Ses1–DXMit48) accounting for 47% of the total phenotypic variance. The model for males included the individual effect of Ses1.1, three interactions (Ses1–D9Mit218, D2Mit197–D4Mit2 and D3Mit256–D13Mit36) and explained 47% of the phenotypic variance. Our results suggest that the oligogenic nature of Salmonella persistence and epistasis are important constituents of the genetic architecture of the host response to chronic Salmonella infection.

Published

2005

45. A locus for Bowen-Conradi syndrome maps to chromosome region 12p13.3

Author

Kenneth Morgan, Ryan E. Lamont, T. Mary Fujiwara, Edward Nylen, J C. Loredo-Osti, Klaus Wrogemann, Edward G. Lemire, R. Brian Lowry, A. Micheil Innes, Gail Coghlan, Jill Mauthe, Danielle Frappier, Cheryl R. Greenberg, Barbara Triggs-Raine, Nicole M. Roslin, and Teresa Zelinski

Subjects

Male, Population, Micrognathism, Locus (genetics), Biology, Nose, Identity by descent, Consanguinity, Gene mapping, Genetic linkage, Chromosome regions, Genetics, Ethnicity, Humans, Abnormalities, Multiple, education, Genetics (clinical), Chromosome 12, education.field_of_study, Chromosomes, Human, Pair 12, Fetal Growth Retardation, Haplotype, Chromosome Mapping, Syndrome, Pedigree, Microcephaly, Female, Lod Score, Microsatellite Repeats

Abstract

Bowen-Conradi syndrome (BCS) is a lethal autosomal recessive disorder with an estimated incidence of 1 in 355 live births in the Hutterite population. A few cases have been reported in other populations. Here, we report the results of a genome-wide scan and fine mapping of the BCS locus in Hutterite families. By linkage and haplotype analysis the BCS locus was mapped to a 3.5 cM segment (1.9 Mbp) in chromosome region 12p13.3 bounded by F8VWF and D12S397. When genealogical relationships among the families were taken into account in the linkage analysis, the evidence for linkage was stronger and the number of potentially linked regions was reduced to one. Under the assumption that all the Hutterite patients were identical by descent for a disease-causing mutation, haplotype analysis was used to infer likely historical recombinants and thereby narrow the candidate region to a chromosomal segment shared in common by all the affected children. This study also demonstrates that BCS and cerebro-oculo-facial-skeletal syndrome (COFS) are genetically distinct.

Published

2004

46. A frequent regulatory variant of the estrogen-related receptor alpha gene associated with BMD in French-Canadian premenopausal women

Author

Kenneth Morgan, Latifa Elfassihi, Vincent Giguère, Nathalie Laflamme, Sylvie Giroux, Sylvie Dodin, J. Concepción Loredo-Osti, Claudine Blanchet, and François Rousseau

Subjects

musculoskeletal diseases, Adult, medicine.medical_specialty, Canada, Heel, DNA, Complementary, Genotype, Endocrinology, Diabetes and Metabolism, Osteoporosis, Receptors, Cytoplasmic and Nuclear, Biology, Bone and Bones, Bone remodeling, Estrogen-related receptor, Lumbar, Absorptiometry, Photon, Bone Density, Internal medicine, medicine, Humans, Orthopedics and Sports Medicine, Genetic association, Femoral neck, Gene Library, Ultrasonography, Lumbar Vertebrae, Polymorphism, Genetic, Femur Neck, Genetic Variation, Middle Aged, medicine.disease, Endocrinology, medicine.anatomical_structure, Premenopause, Receptors, Estrogen, Multivariate Analysis, Female

Abstract

Genes are important BMD determinants. We studied the association of an ESRRA gene func- tional variant with BMD in 1335 premenopausal women. The ESRRA genotype was an independent predictor of L 2 -L 4 BMD, with an effect similar to smoking and equivalent to a 10-kg difference in weight. Introduction: Several genetic polymorphisms have been associated with osteoporosis or osteoporosis frac- tures, but no functional effect has been shown for most of these gene variants. Because functional studies have implicated estrogen-related receptor (ESRRA) in bone metabolism, we evaluated whether a recently described regulatory variant of the ESRRA gene is associated with lumbar and hip BMD as measured by DXA and with heel bone parameters as measured by quantitative ultrasound (QUS). Materials and Methods: Heel bone parameters were measured by right calcaneal QUS in 1335 healthy French-Canadian premenopausal women, and one-half of these women also had their BMD evaluated at two sites: femoral neck and lumbar spine (L2-L4) by DXA. All bone measures were tested separately for asso- ciation with the ESRRA genotype by analysis of covariance. The significance of the ESRRA contribution to the model was also assessed by two different permutation tests. Results: A statistically significant association between ESRRA genotype and lumbar spine BMD was ob- served: women carrying the long ESRRA genotype had a 3.9% (0.045 g/cm 2 ) higher lumbar spine BMD than those carrying the short ESRRA genotype (p 0.004), independently of other risk factors measured. This effect of ESRRA genotype is similar to the effect of smoking and equivalent to a 10-kg difference in weight. This association was confirmed by permutation tests (p 0.004). The same trend was observed for femoral neck BMD (2.6%, p 0.07). However, no association was observed between ESRRA and QUS heel bone measures. Conclusion: These results support the genetic influence of this ESRRA regulatory variant on BMD. J Bone Miner Res 2005;20:938-944. Published online on February 7, 2005; doi: 10.1359/JBMR.050203

Published

2004

47. A survey of genetic and epigenetic variation affecting human gene expression

Author

Scott Gurd, Robert Sladek, Amelie Villeneuve, Anna K. Naumova, Jade Kingsley, Tomi Pastinen, Alya’a Sammak, Marie-Claude Vohl, Daniel Sinnett, Andrei Verner, Kenneth Morgan, Pierre Lepage, Karine Lavergne, Helena Brändström, Eef Harmsen, Allon Beck, Thomas J. Hudson, Bing Ge, Damian Labuda, and Tiffany Gaudin

Subjects

Male, Transcription, Genetic, Physiology, Biology, Allelic Imbalance, Polymorphism, Single Nucleotide, Cell Line, Dosage Compensation, Genetic, Genetic variation, Genetics, Humans, Epigenetics, Allele, Regulation of gene expression, Gene Expression Profiling, Genetic Variation, Sequence Analysis, DNA, Pedigree, Gene expression profiling, Gene Expression Regulation, Haplotypes, Allelic heterogeneity, Human genome, Female

Abstract

The identification of human sequence polymorphisms that regulate gene expression is key to understanding human genetic diseases. We report a survey of human genes that demonstrate allelic differences in gene expression, reflecting the presence of putative allele-specific cis-acting factors of either genetic or epigenetic nature. The expression of allelic transcripts in heterozygous samples is assessed directly by relative quantitation of intragenic marker alleles in messenger or heteronuclear RNA derived from cells or tissues. This survey used 193 single-nucleotide polymorphisms (SNPs) from 129 genes expressed in lymphoblastoid cell lines, to identify 23 genes (18%) with common allele-specific transcripts whose expression deviated from the expected equimolar ratio. A subset of these deviations, or “allelic imbalances,” can be observed in multiple samples derived from reference CEPH (“Centre d’Etude du Polymorphisme Humain”) pedigrees and demonstrate a spectrum of patterns of transmission, including cosegregation of allelic skewing across generations compatible with Mendelian inheritance as well as random monoallelic expression for three genes ( IL1A, HTR2A, and FGB). Additional studies for BTN3A2 provide evidence of SNPs and haplotypes in complete linkage disequilibrium with high- and low-expressing transcripts. The pipeline described herein offers tools for efficient identification and characterization of allelic expression allowing identification of regulatory sequence variants as well as epigenetic variation affecting human gene expression.

Published

2003

48. Allelic variation in TLR4 is linked to susceptibility to Salmonella enterica serovar Typhimurium infection in chickens

Author

Nat Bumstead, Adrian Smith, Paul A. Barrow, Gary Leveque, J C. Loredo-Osti, Danielle Malo, Vincenzo Forgetta, Kenneth Morgan, and Shaun Morroll

Subjects

Salmonella typhimurium, Salmonella, animal structures, Immunology, Molecular Sequence Data, Receptors, Cell Surface, medicine.disease_cause, Microbiology, medicine, Animals, Drosophila Proteins, Bursa of Fabricius, Genetic Predisposition to Disease, Northern blot, Amino Acid Sequence, RNA, Messenger, Gene, Alleles, Poultry Diseases, Genetics, Salmonella Infections, Animal, Host Response and Inflammation, Membrane Glycoproteins, biology, Toll-Like Receptors, Chromosome Mapping, Genetic Variation, biology.organism_classification, Molecular biology, Transmembrane protein, Toll-Like Receptor 4, Transmembrane domain, Infectious Diseases, Salmonella enterica, Microchromosome, Parasitology, Chickens

Abstract

Toll-like receptor 4 (TLR4) is part of a group of evolutionarily conserved pattern recognition receptors involved in the activation of the immune system in response to various pathogens and in the innate defense against infection. We describe here the cloning and characterization of the avian orthologue of mammalian TLR4 . Chicken TLR4 encodes a 843-amino-acid protein that contains a leucine-rich repeat extracellular domain, a short transmembrane domain typical of type I transmembrane proteins, and a Toll-interleukin-1R signaling domain characteristic of all TLR proteins. The chicken TLR4 protein shows 46% identity (64% similarity) to human TLR4 and 41% similarity to other TLR family members. Northern blot analysis reveals that TLR4 is expressed at approximately the same level in all tissues tested, including brain, thymus, kidney, intestine, muscle, liver, lung, bursa of Fabricius, heart, and spleen. The probe detected only one transcript of ca. 4.4 kb in length for all tissues except muscle where the size of TLR4 mRNA was ca. 9.6 kb. We have mapped TLR4 to microchromosome E41W17 in a region harboring the gene for tenascin C and known to be well conserved between the chicken and mammalian genomes. This region of the chicken genome was shown previously to harbor a Salmonella susceptibility locus. By using linkage analysis, TLR4 was shown to be linked to resistance to infection with Salmonella enterica serovar Typhimurium in chickens (likelihood ratio test of 10.2, P = 0.00138), suggesting a role of TLR4 in the host response of chickens to Salmonella infection.

Published

2003

49. Evidence for origin, by recurrent mutation, of the phenylalanine hydroxylase R408W mutation on two haplotypes in European and Quebec populations

Author

L. A. Tyfield, Bernd Dworniczak, Susan Byck, Kenneth Morgan, and Charles R. Scriver

Subjects

Untranslated region, Phenylalanine hydroxylase, Molecular Sequence Data, Minisatellite Repeats, Biology, Phenylketonurias, Genetics, Humans, Molecular Biology, Gene, Alleles, Genetics (clinical), Recombination, Genetic, Base Sequence, Haplotype, Quebec, Phenylalanine Hydroxylase, Chromosome, DNA, General Medicine, Europe, Genetics, Population, Haplotypes, Oligodeoxyribonucleotides, CpG site, Genetic marker, Mutation, Mutation (genetic algorithm), biology.protein

Abstract

The R408W mutation in the phenylalanine hydroxylase gene (PAH) of phenylketonuria patients occurs on haplotypes 2.3 and 1.8 in Europeans. The mutation involves a CpG dinucleotide; nonetheless, a single recombination event might also explain the two haplotype associations. By analysis of an STR in the PAH gene 5' to the 408 codon and of the VNTR system in the 3' UTR, we identified unique features of the haplotype 1.8 chromosome harbouring the R408W mutation which are not accounted for by recombination. We conclude that recurrent mutation is the origin of R408W on different PAH haplotypes in Europeans.

Published

1994

50. X chromosome effect on maternal recombination and meiotic drive in the mouse

Author

Carmen Sapienza, Fernando Pardo-Manuel de Villena, Joe E. Vaughan, J. Concepcion Loredo-Osti, Kenneth Morgan, Jan Michel Malette, Tammi L. Briscoe, and Elena de la Casa-Esperón

Subjects

Genetics, Recombination, Genetic, X Chromosome, Models, Genetic, Locus (genetics), Biology, Genetic recombination, Mice, Inbred C57BL, Meiosis, Mice, Meiotic drive, Dosage Compensation, Genetic, Animals, Female, Allele, Homologous recombination, Skewed X-inactivation, X chromosome, Research Article

Abstract

We observed that maternal meiotic drive favoring the inheritance of DDK alleles at the Om locus on mouse chromosome 11 was correlated with the X chromosome inactivation phenotype of (C57BL/ 6-Pgk1a × DDK)F1 mothers. The basis for this unexpected observation appears to lie in the well-documented effect of recombination on meiotic drive that results from nonrandom segregation of chromosomes. Our analysis of genome-wide levels of meiotic recombination in females that vary in their X-inactivation phenotype indicates that an allelic difference at an X-linked locus is responsible for modulating levels of recombination in oocytes.

Published

2002