Your search keyword '"Sadovnick, A. D."' showing total 20 results

1. To treat or not to treat the person with clinical multiple sclerosis--a dilemma.

Author

Sadovnick, A. D.

Subjects

*MULTIPLE sclerosis, *DISEASE management

Abstract

Disease-modifying therapies for MS are believed to reduce the exacerbation frequency and thus perhaps improve a patient's "quality of life". Increasingly, such therapies are being offered to young persons with relatively mild or very early disease. Concerns about whom to treat, based on knowledge about the role of genetics on "MS risk" and the possible teratogenic effects of disease-modifying treatments on a developing fetus, are discussed. [ABSTRACT FROM AUTHOR]

Published

2001

2. Evidence for genetic basis of multiple sclerosis.

Author

Sadovnick, A D, Ebers, G C, Dyment, D A, Risch, N J, and the Canadian Collaborative Study Group

Subjects

*GENETICS of multiple sclerosis

Abstract

Looks at research which attempted to find out the genetic contribution and environmental factors in the risk of multiple sclerosis (MS). Information about identical twins; Study of a Canadian-based sample of MS cases seen at 14 regional MS clinics; Information about studies of half-sibs; Evidence that a shared environment does not account for familial risk in MS; Findings about maternal effects.

Published

1996

3. Colony stimulation factor 1 receptor ( CSF1R) is not a common cause of multiple sclerosis.

Author

Sadovnick, A. D., Traboulsee, A. L., Lee, J. D., Ross, J. P., Bernales, C. Q., and Vilariño‐Güell, C.

Subjects

*MULTIPLE sclerosis, *COLONY-stimulating factors (Physiology)

Abstract

A letter to the editor regarding colony stimulation factor 1 receptor (CSF1R) which is a rare cause of multiple sclerosis in Canada.

Published

2013

4. Parent-of-origin effect in multiple sclerosis: observations in half-siblings.

Author

Ebers, G. C., Sadovnick, A. D., Dyment, D. A., Yee, I. M. L., Willer, C. J., and Risch, Neil

Subjects

*MULTIPLE sclerosis, *FAMILIAL diseases, *SIBLINGS, *DISEASE risk factors, *ETIOLOGY of diseases, *MEDICAL research, *RESEARCH methodology, *PARENT-child relationships, *HEALTH, *DISEASES

Abstract

Multiple sclerosis is a complex trait in which occurrence rates in offspring are 20--50-fold greater than in the general population. Parent-of-origin effects have been difficult to screen for, since most cases are sporadic. We have compared recurrence risks in half-siblings with respect to their parent in common. Of the 1567 index cases with half-siblings in multiple sclerosis clinics across Canada, we recorded 3436 half-siblings and 2706 full-siblings. Age-adjusted full-sibling risk was 3.11%. By contrast, half-sibling risk in the same families was significantly lower at 1.89% ( 2 test, p=0.006), but higher than expected if familial risk was simply polygenic. For maternal half-siblings, the risk was 2.35% (34 affected siblings of 1859), and 1.31% for paternal halfsiblings (15 of 1577), (p=0.048). The difference in risk suggests a maternal parent-of-origin effect in multiple sclerosis susceptibility. [ABSTRACT FROM AUTHOR]

Published

2004

5. A genetic basis for familial aggregation in multiple sclerosis.

Author

Ebers, G. C. and Sadovnick, A. D.

Subjects

*GENETICS of multiple sclerosis

Abstract

Indicates that familial aggregation of multiple sclerosis is genetically determined. Effect of shared environment; Increased family risk for monozygotic twins and first-degree relatives.

Published

1995

6. Population-based study of long-term outcomes after amniocentesis.

Author

Baird, P A, Yee, I M L, and Sadovnick, A D

Subjects

*AMNIOCENTESIS

Abstract

Determines whether children of women who had midtrimester amniocentesis are identified by a population-based database of congenital anomalies and disabilities at a different rate from children of women who did not undergo amniocentesis. Results showing that amniocentesis increases risk of hemolytic problems due to ABO immunization; Potential for isoimmunization during amniocentesis.

Published

1994

7. Revisiting the T-cell receptor alpha/delta locus and possible associations with multiple sclerosis.

Author

Watson, C T, Para, A E, Lincoln, M R, Ramagopalan, S V, Orton, S M, Morrison, K M, Handunnetthi, L, Handel, A E, Chao, M J, Morahan, J, Sadovnick, A D, Breden, F, and Ebers, G C

Subjects

*GENETICS of multiple sclerosis, *T cell receptors, *LOCUS (Genetics), *MAJOR histocompatibility complex genetics, *GENETIC polymorphisms, *NUCLEOTIDE sequence, *GENETIC markers

Abstract

A role for T cells in the pathogenesis of multiple sclerosis (MS) is well supported, evidenced by myriad immunological studies, as well as the unequivocal genetic influence of the major histocompatibility complex (MHC). Despite many attempts, no convincing genetic associations have been made between T-cell receptor (TCR) gene loci and MS. However, these studies may not be definitive because of small sample sizes and under-representative marker coverage of the chromosomal regions being investigated. To explore potential roles between the TCR alpha locus and MS, we have genotyped a large family-based cohort, including 1360 affected individuals and 1659 of their unaffected first-degree relatives, at 40 single-nucleotide polymorphism (SNP) markers within the TCR alpha/delta locus. This represents the largest TCR alpha-MS study to date. From this screen, we identified three potential loci of interest in TCR alpha variable and constant gene regions using the transmission disequilibrium test. Although SNPs implicating each of these regions of interest will require genotyping in independent replication cohorts, these findings suggest a role for TCR gene polymorphisms in MS susceptibility. In the context of these findings we review the evidence. [ABSTRACT FROM AUTHOR]

Published

2011

8. Sex ratio of multiple sclerosis and clinical phenotype.

Author

Ramagopalan, S. V., Byrnes, J. K., Orton, S.-M., Dyment, D. A., Guimond, C., Yee, I. M., Ebers, G. C., and Sadovnick, A. D.

Subjects

*MULTIPLE sclerosis, *SEX ratio, *DEMYELINATION, *CLINICAL trials

Abstract

Background and purpose: In a longitudinal population-based dataset of patients with multiple sclerosis (MS), we have previously observed a substantial increase in the female to male sex ratio in Canada over the last 50 years. Here, we aimed to determine whether this change in sex ratio is related to the clinical course of MS. Methods: We calculated sex ratios by birth year in 11 868 patients with relapsing–remitting (RR) MS and 2825 patients with primary progressive (PP) MS identified as part of the Canadian Collaborative Project on the Genetic Susceptibility to MS. Results: Year of birth was a significant predictor for sex ratio in RR MS ( P < 0.0001, χ2 = 21.2; Spearman’s rank correlation r = 0.67), but not for PP MS ( P = 0.44, χ2 = 0.6; Spearman’s rank correlation r = 0.11). Conclusions: An increase in the number of female RR MS patients over time accounts for the increasing sex ratio of MS. This has implications for pathogenesis, for assessment of clinical trial results and for disease prevention. The factors underlying the selective increase in MS in females need to be uncovered. [ABSTRACT FROM AUTHOR]

Published

2010

9. Age of puberty and the risk of multiple sclerosis: a population based study.

Author

Ramagopalan, S. V., Valdar, W., Criscuoli, M., DeLuca, G. C., Dyment, D. A., Orton, S.-M., Yee, I. M., Ebers, G. C., and Sadovnick, A. D.

Subjects

*MULTIPLE sclerosis, *PUBERTY, *MENARCHE, *DISEASE susceptibility, SEX differences (Biology)

Abstract

Background and purpose: Genetic and environmental factors have important roles in multiple sclerosis (MS) susceptibility. Given a potential role for sex hormones in MS, we have investigated whether or not the age of puberty influences the risk of developing MS in a population-based cohort. Methods: We identified 5493 MS index cases and 1759 spousal controls with age of puberty information from the Canadian Collaborative Project on Genetic Susceptibility to MS. Age of puberty was compared between index cases and controls, and any effect of age of puberty on the age of onset of MS was also investigated. Results: There were no significant differences between male index cases and controls with respect to age of puberty, P = 0.70. However, a significant difference was observed between female index cases and female controls, with average age of puberty being 12.4 and 12.6 years respectively, P = 0.00017, providing a relative risk decrease of 0.9 per year increase of age of puberty. There was no effect of the age of puberty on the age of MS onset in either sex. Conclusions: Earlier age at menarche increases the risk of MS in women. Whether this association is a surrogate for a disease causative factor or directly involved in MS disease aetiology needs to be uncovered. [ABSTRACT FROM AUTHOR]

Published

2009

10. A genome scan in a single pedigree with a high prevalence of multiple sclerosis.

Author

Dyment, D. A., Cader, M. Z., Herrera, B. M., Ramagopalan, S. V., Orton, S. M., Chao, M., Willer, C. J., Sadovnick, A. D., Risch, N., and Ebers, G. C.

Subjects

*GENOMES, *MULTIPLE sclerosis, *AUTOIMMUNE diseases, *MYELIN sheath diseases, *GENES, *GENETICS

Abstract

Background: Multiple sclerosis (MS) is a disease that is widely believed to be autoimmune in nature. Genetic-epidemiological studies implicate susceptibility genes in the pathogenesis of MS, although non-MHC susceptibility linkages have been difficult to confirm. Insight into pathways that are intrinsic to other complex diseases has come from the genetic analysis of large, autosomal-dominant kindreds. Here, we present a genetic study of a large and unique kindred in which MS appears to follow an autosomal-dominant pattern of inheritance, with consistent penetrance in four generations. Methods: Eighty-two individuals of this 370-member family were genotyped with 681 microsatellite markers spanning the genome, with an average spacing of 5.3 cM. Results: Parametric linkage analysis was performed and no significant LOD score (LOD >3.3) was observed. For a rare dominant disease model with reduced penetrance, 99.6% of the genome was excluded at a LOD score <-1 and 96% at a LOD score <-2. The HLA-DRB1 candidate gene was also genotyped by allele-specific methods. In each instance where at least one parent was positive for HLA-DRB1*15, one or more HLA-DRB1*15 alleles were transmitted to the affected offspring )1 1/1 1). HLA- DRB1*15 was transmitted equally from both the familial and the married-in parents and therefore this locus does not appear to be an autosomal-dominant acting gene in this family but an important modifier of risk. Conclusions: These results further stress the importance of the HLA-DRB1 *15-bearing haplotype in determining MS susceptibility. Furthermore, this study highlights the complexity of MS genetics, even in the presence of a single family, seemingly segregating MS as an autosomal-dominant trait. [ABSTRACT FROM AUTHOR]

Published

2008

11. An extremes of outcome strategy provides evidence that multiple sclerosis severity is determined by alleles at the HLA-DRB1 locus.

Author

Deluca, G. C., Ramagopalan, S. V., Herrera, B. M., Dyment, D. A., Lincoln, M. R., Montpetit, A., Pugliatti, M., Barnardo, M. C. N., Risch, N. J., Sadovnick, A. D., Chaott, M., Sotgiu, S., Hudson, T. J., and Ebers, G. C.

Subjects

*MULTIPLE sclerosis, *DEMYELINATION, *MYELIN sheath diseases, *VIRUS diseases, *CENTRAL nervous system, *ORGANS (Anatomy)

Abstract

Multiple sclerosis (MS) is a common inflammatory disease of the central nervous system unsurpassed for variability in disease out- come. A cohort of sporadic MS cases (n = 163). taken from opposite extremes of the distribution of long-term outcome, was used to determine the role of the HLA-DRB1 locus on MS disease severity. Genotyping sets of benign and malignant MS patients showed that HLA-DRB1*01 was significantly underrepresented in malignant compared with benign cases. This allele appears to attenuate the progressive disability that characterizes MS in the long term. The observation was doubly replicated in (i) Sardinian benign and malignant patients and (ii) a cohort of affected sibling pairs discordant for HLA-DRB1*01. Among the latter, mean disability progression indices were significantly lower in those carrying the HLA-DRB1*01 allele compared with their disease-concordant siblings who did not. The findings were additionally supported by similar transmission distortion of HLA-DRB1*04 subtypes closely related to HLA-DRB1*01. The protective effect of HLA-DRB1*01 in sibling pairs may result from a specific epistatic interaction with the susceptibility allele HLA-DRB1* 1501. A high-density (>700) SNP examination of the MHC region in the benign and malignant patients could not identify variants differing significantly between the two groups, suggesting that HLA-DRB1 may itself be the disease-modifying locus. We conclude that HLA-DRB1*01, previously implicated in disease resistance, acts as an independent modifier of disease progression. These results closely link susceptibility to long-term outcome in MS. suggesting that shared quantitative MHC-based mechanisms are common to both, emphasizing the central role of this region in pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2007

12. The role of hereditary spastic paraplegia related genes in multiple sclerosis.

Author

DeLuca, G., Ramagopalan, S. V., Cader, M. Z., Dyment, D. A., Herrera, B. M., Orton, S., Degenhardt, A., Pugliatti, M., Sadovnick, A. D., Sotgiu, S., and Ebers, G. C.

Subjects

*MULTIPLE sclerosis, *MYELIN sheath diseases, *DEMYELINATION, *PARAPLEGIA, *LEG diseases, *CENTRAL nervous system diseases, *GENETICS

Abstract

Multiple sclerosis (MS) is a common inflammatory disease of the central nervous system unsurpassed for its variability in disease outcome. It has been observed that axonal loss in MS is significant and that irreversible clinical disability relates to such axonal loss. The clinical similarities between Hereditary Spastic Paraplegia (HSP) and progressive MS, along with their analogous profiles of axonal loss in the long tracts, make the genes known to cause HSP biologically relevant candidates for the study of clinical outcome in MS. A cohort of sporadic MS cases and a set of unaffected controls were used to determine the role of HSP genes on MS susceptibility and disease severity. The MS cases were taken from opposite extremes of the putative distribution of long-term outcome using the most stringent clinical criteria to date. Genotyping the two sets of MS patients and controls could not provide any evidence to suggest that genes involved in the pathogenesis of HSP ( Paraplegin, NIPA1, KIF5A, HSPD1, Atlastin, Spartin, Spastin, PLP1, L1CAM, Maspardin and BSCL2) play a role in susceptibility to, or modifying the course of, MS, although small effects of these genes cannot be ruled out. [ABSTRACT FROM AUTHOR]

Published

2007

13. Multiple sclerosis susceptibility and the X chromosome.

Author

Herrera, B. M., Cader, M. Z., Dyment, D. A., Bell, J. T., DeLuca, G. C., Willer, C. J., Lincoln, M. R., Ramagopalan, S. V., Chao, M., Orton, S.-M., Sadovnick, A. D., and Ebers, G. C.

Subjects

*MULTIPLE sclerosis, *X chromosome, *GENETICS of disease susceptibility, *SEX factors in disease, *SEX chromosomes, *ETIOLOGY of diseases, *MEDICAL genetics

Abstract

Multiple sclerosis (MS) is a chronic autoimmune complex trait with strong evidence for a genetic component. A female gender bias is clear but unexplained and a maternal parent-of-origin effect has been described. X-linked transmission of susceptibility has been previously proposed, based on pedigree, association and linkage studies. We genotyped 726 relative pairs including 552 affected sib-pairs for 22 X-chromosome microsatellite markers and a novel dataset of 195 aunt-uncle/niece-nephew (AUNN) affected pairs for 18 markers. Parent-of-origin effects were explored by dividing AUNN families into likely maternal and paternal trait transmission. For the sib-pair dataset we were able to establish exclusion at a λs=1.9 for all markers using an exclusion threshold of LOD⩽-2. Similarly for the AUNN dataset, we established exclusion at λAV=1.9. For the combined dataset we estimate exclusion of λ=1.6. We did not identify significant linkage in either the sib-pairs or the AUNN dataset nor when datasets were stratified for the presence/absence of the HLA-DRB1*15 allele or for paternal or maternal transmission. This comprehensive scrutiny of the X-chromosome suggests that it is unlikely to harbour an independent susceptibility locus or one which interacts with the HLA. Complex interactions including epigenetic ones, and masking by balanced polymorphisms are mechanisms not excluded by the approach taken. [ABSTRACT FROM AUTHOR]

Published

2007

14. Follow-up investigation of 12 proposed linkage regions in multiple sclerosis.

Author

Herrera, B M, Cader, M Z, Dyment, D A, Bell, J T, Ramagopalan, S V, Lincoln, M R, Orton, S, Chao, M J, Sadovnick, A D, and Ebers, G C

Subjects

*MULTIPLE sclerosis, *AUTOIMMUNE diseases, *LYMPHOCYTES, *MICROSATELLITE repeats, *MAJOR histocompatibility complex

Abstract

Multiple sclerosis (MS) is an autoimmune disease with overwhelming evidence for genetic determination, and for which a maternal parent-of-origin effect has been reported. As with many complex diseases, multiple suggestive linkage signals have been observed. However, the only unambiguous association and linkage identified to date is with alleles of the human lymphocyte antigen (HLA) class II region. We have now carried out high-density microsatellite genotyping for 12 of the most promising regions (1p, 1q, 2q, 4q, 5p, 9q, 10p, 11p, 12q, 17q, 18p, 19p) from a whole-genome scan in 552 affected sibling pairs. This has been carried out in 194 families containing avuncular pairs. These permit examination of parent-of-origin effects in non-colineal pairs when divided into likely maternal and paternal trait transmission. The results do not confirm any non-major histocompatibility complex linkage in the overall subset nor in the maternal, paternal or HLA-DRB1*1501 subsets. We were able to establish exclusion for a locus with λAV1.3 for all the previously suggested regions. These results again raise the possibility that the paradigm of multiple genes of small individual effect used to justify genome searches in MS is incorrect.Genes and Immunity (2006) 7, 366–371. doi:10.1038/sj.gene.6364308; published online 1 June 2006 [ABSTRACT FROM AUTHOR]

Published

2006

15. TCR ß polymorphisms and multiple sclerosis.

Author

Dyment, D. A., Steckley, J. L., Morrison, K., Willer, C. J., Cader, M. Z., DeLuca, G. C., Sadovnick, A. D., Risch, N., and Ebers, G. C.

Subjects

*FAMILIES, *MULTIPLE sclerosis, *GENES, *IMMUNITY

Abstract

A total of 267 families with two or more siblings with multiple sclerosis (MS) were genotyped with 14 restriction fragment length polymorphisms at the TCR ß locus. A nonparametric linkage analysis of the data showed no evidence for linkage to this locus (mlod=0.11). No significant allelic or haplotype transmissions were observed in the total sample of 565 patients. After stratification for the presence of HLA DRB1*15, an association was observed between the BV25S1*1-BV26S1*1-BV2S1*1 haplotype and MS (P=0.00089). This was not significant upon correction for multiple comparisons. It was also not significant when the haplotype frequency in affected individuals was compared to a normal control sample (P=0.77). Furthermore, the associated haplotype was followed-up in an independent sample of 97 nuclear families with a single DRB1*15-positive child with MS. The BV25S1*1-BV26S1*1-BV2S1*1 haplotype did not show significant evidence for transmission distortion but the same trend was seen (P=0.21). There were no significant associations observed in the DRB1*15-negative patients and no detectable difference was seen in the DRB1*15-positive BV25S1*1-BV26S1*1-BV2S1*1 association when comparing different subgroups based on clinical course of MS. These results show no evidence for linkage and fail to establish an association between MS susceptibility and the TCR ß locus.Genes and Immunity (2004) 5, 337-342. doi:10.1038/sj.gene.6364091 Published online 3 June 2004 [ABSTRACT FROM AUTHOR]

Published

2004

16. Twin concordance and sibling recurrence rates in multiple sclerosis.

Author

Willer, C. J., Dyment, D. A., Risch, N. J., Sadovnick, A. D., and Ebers, G. C.

Subjects

*MULTIPLE sclerosis, *HUMAN genetics, *TWINS

Abstract

Size and ascertainment constraints often limit twin studies to concordance comparisons between identical and fraternal twins. Here we report the final results of a longitudinal, population-based study of twins with multiple sclerosis (MS) in Canada. Bias was demonstrably minimized, and an estimated 75% of all Canadian MS twin pairs were ascertained, giving a sample sufficiently large (n = 370) to permit additional informative comparisons. Twinning was not found to affect prevalence, and twins with MS did not differ from nontwins for DR15 allele frequency nor for MS risk to their siblings. Probandwise concordance rates of 25.3% (SE ñ 4.4) for monozygotic (MZ), 5.4% (±2.8) for dizygotic (DZ), and 2.9% (±0.6) for their nontwin siblings were found. MZ twin concordance was in excess of DZ twin concordance. The excess concordance in MZ was derived primarily from like-sexed female pairs with a probandwise concordance rate of 34 of 100 (34 ñ 5.7%) compared with 3 of 79 (3.8 ± 2.8%) for female DZ pairs. We did not demonstrate an MZ/DZ difference in males, although the sample size was small. We observed a 2-fold increase in risk to DZ twins over nontwin siblings of twins, but the difference was not significant. [ABSTRACT FROM AUTHOR]

Published

2003

17. Evidence that a single nucleotide polymorphism in the promoter of the G protein receptor kinase 3 gene is associated with bipolar disorder.

Author

Barrett, T B, Hauger, R L, Kennedy, J L, Sadovnick, A D, Remick, R A, Keck, P E, McElroy, S L, Alexander, M, Shaw, S H, and Kelsoe, J R

Subjects

*GENETIC polymorphisms, *LINKAGE (Genetics), *BIPOLAR disorder, *G proteins

Abstract

In a genome-wide linkage survey, we have previously shown evidence suggesting that the chromosome 22q12 region contains a susceptibility locus for bipolar disorder (BPD). Two independent family sets yielded lod scores suggestive of linkage at markers in this region near the gene G protein receptor kinase 3 (GRK3). GRK3 is an excellent candidate risk gene for BPD since GRK3 is expressed widely in the brain, and since GRKs play key roles in the homologous desensitization of G protein-coupled receptor signaling. We have also previously shown GRK3 expression to be induced by amphetamine in an animal model of mania using microarray-based expression profiling. To identify possible functional mutations in GRK3, we sequenced the putative promoter region, all 21 exons, and intronic sequence flanking each exon, in 14-22 individuals with BPD. We found six sequence variants in the 5'-UTR/promoter region, but no coding or obvious splice variants. Transmission disequilibrium analyses of one set of 153 families indicated that two of the 5'-UTR/promoter variants are associated with BPD in families of northern European Caucasian ancestry. A supportive trend towards association to one of these two variants (P-5) was then subsequently obtained in an independent sample of 237 families. In the combined sample, the P-5 variant had an estimated allele frequency of 3% in bipolar subjects, and displayed a transmission to non-transmission ratio of 26 : 7.7 (χ[SUP2] = 9.6, one-sided P value = 0.0019). Altogether, these data support the hypothesis that a dysregulation in GRK3 expression alters signaling desensitization, and thereby predisposes to the development of BPD. [ABSTRACT FROM AUTHOR]

Published

2003

18. Linkage of a bipolar disorder susceptibility locus to human chromosome 13q32 in a new pedigree series.

Author

Shaw, S H, Mroczkowski-Parker, Z, Shekhtman, T, Alexander, M, Remick, R A, Sadovnick, A D, McElroy, S L, Keck, P E, and Kelsoe, J R

Subjects

*LINKAGE (Genetics), *BIPOLAR disorder, *GENEALOGY, *GENETIC markers

Abstract

Bipolar (BP) disorder or manic depressive illness is a major psychiatric disorder for which numerous family, twin and adoption studies support a substantial genetic contribution. Recently, we reported the results of a genome-wide search for BP disorder susceptibility loci in 20 pedigrees. Suggestive evidence for linkage was found in this study at three markers on 13q, representing possibly two peaks separated by 18 cM. We have now collected a second set of 32 pedigrees segregating BP disorder and have tested for evidence of linkage to markers on human chromosome 13q. In this sample, we have replicated the linkage result in 13q32 at D13S154 (lod = 2.29), the more proximal of the two original peaks. When all 52 pedigrees were combined, the multipoint maximum lod score peaked approximately 7 cM proximal to D13S154 (lod = 3.40), with a second peak occurring between D13S225 and D13S796 (lod = 2.58). There have been several other reports of significant linkage to both BP disorder and schizophrenia in this region of chromosome 13. These pedigrees provide additional evidence for at least one locus for BP disorder in 13q32, and are consistent with other reports of a possible genetic overlap between these disorders. [ABSTRACT FROM AUTHOR]

Published

2003

19. Maternal age and birth defects: a population study.

Author

Baird PA, Sadovnick AD, Yee IML, Baird, P A, Sadovnick, A D, and Yee, I M

Abstract

Since more and more women in developed countries are delaying childbearing to an older age, it is important to find out whether birth defects, other than those resulting from chromosomal anomalies, are related to maternal age. We have studied all 26,859 children with birth defects of unknown aetiology identified among 576,815 consecutive livebirths in British Columbia. All these cases' records were linked with provincial birth records to allow determination of maternal age at birth. We excluded children with chromosomal anomalies and those with other birth defects of known aetiology. Only 3 of the 43 birth defect categories studied showed significant maternal-age-specific trends: there were decreasing linear trends with maternal age for patent ductus arteriosus (chi 2 = 36.65, 1 df, p less than 0.01) and hypertrophic pyloric stenosis (chi 2 = 4.90, 1 df, p less than 0.05) and a bell-shaped curve (risk increasing to maternal age 30 then falling) for congenital dislocatable hip/hip click. The findings from this population-based analysis of no association between the incidence of birth defects of unknown aetiology and advancing maternal age should be reassuring to healthy women who opt to delay childbearing. [ABSTRACT FROM AUTHOR]

Published

1991

20. Multiple sclerosis in stepsiblings: recurrence risk and ascertainment.

Author

Dyment, D. A., Yee, I. M. L., Ebers, G. C., and Sadovnick, A. D.

Subjects

*MULTIPLE sclerosis, *DIAGNOSIS, *GENETIC research, *EPIDEMIOLOGY, *FAMILIES

Abstract

Reports implicating specific transmissible agents in multiple sclerosis (MS) susceptibility continue to appear. We therefore re-evaluated MS risk in 687 stepsiblings of 19 746 MS index cases. We found the risk of MS to be indistinguishable from that of the general population after diagnostic verification. These results are coherent with studies of adopted children, half siblings and conjugals, showing no risk attributable to the familial microenvironment. This family based genetic epidemiological approach found no trace of transmissibility other than genetic from one affected individual to another in the high prevalence area of Canada. This adds to existing data showing that the action of environment in influencing MS risk is operative at a population level. [ABSTRACT FROM AUTHOR]

Published

2006