Heterotrisomy, a significant contributing factor to ventricular septal defect associated with Down syndrome?

Baptista, Melisa J.; Fairbrother, Una; Howard, Catherine M.; Farrer, Matthew J.; Davies, Gail E.; Trikka, Dimitra; Maratou, Klio; Redington, Andrew N.; Greve, Gottfried; Njølstad, Pål R.; Kessling, Anna M.

doi:10.1007/s004390000395

Cited by 24 publications

(17 citation statements)

References 41 publications

(38 reference statements)

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“…Down's syndrome. Blood samples were taken from 30 nondiabetic schoolaged children with Down's syndrome (15 male and 15 female, 4 -21 years of age) during routine thyroid screening in the area covered by the Gloucestershire Health Authority, U.K. Aliquots of DNA samples from 83 children with Down's syndrome had been collected as part of a study of congenital heart disease in Down's syndrome (15). Samples were also available (109 DNA and 106 serum) for analysis from a population-based study of children with Down's syndrome in Manchester, the Hester Adrian Research Centre cohort (16).…”

Section: Methodsmentioning

confidence: 99%

Islet Autoimmunity in Children With Down’s Syndrome

et al. 2006

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There is an unexplained excess of type 1 diabetes and other organ-specific autoimmune diseases in children with Down's syndrome, but the immunogenetic characteristics of diabetes in Down's syndrome have not been investigated. We studied the frequency of islet autoantibodies in 106 children with Down's syndrome and no history of autoimmunity and analyzed HLA class II genotypes in 222 children with Down's syndrome, 40 children with Down's syndrome and type 1 diabetes, 120 age-and sex-matched children with type 1 diabetes, and 621 healthy control subjects. Co-occurrence of at least two islet autoantibody markers was observed in 6 of 106 nondiabetic children with Down's syndrome compared with 13 of 2,860 healthy agematched children (P < 0.001). There was an excess of diabetes-associated HLA class II genotypes in children with Down's syndrome and type 1 diabetes compared with ageand sex-matched healthy control subjects (P < 0.001). Down's syndrome children with type 1 diabetes were, however, less likely to carry the highest risk genotype DR4-DQ8/DR3-DQ2 than children with type 1 diabetes from the general population (P ‫؍‬ 0.01) but more likely to carry low-risk genotypes (P < 0.0001). The frequency of subclinical islet autoimmunity is increased in Down's syndrome, and susceptibility to type 1 diabetes in Down's syndrome is partially HLA mediated. Other factors, possibly including genes on chromosome 21, may increase the penetrance of type 1 diabetes in Down's syndrome. Diabetes 55: [3185][3186][3187][3188] 2006

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Section: Methodsmentioning

confidence: 99%

Islet Autoimmunity in Children With Down’s Syndrome

et al. 2006

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“…The COL-α1 (VI) and -α2 (VI) chains are encoded by genes located on Hsa21 and their overexpression has been associated with atrioventricular canal defects in Down syndrome [133,134]. The α3 (VI) chain is encoded by the COL6A3 located at chromosome 2, and individuals with Down syndrome who have single nucleotide polymorphisms in COL6A3 are at increased risk of muscle hypotonia and CHD [135].…”

Section: Congenital Heart Defects and Cardiovascular Disease In Down mentioning

confidence: 99%

What people with Down Syndrome can teach us about cardiopulmonary disease

Colvin

Yeager

2017

Eur Respir Rev

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Down syndrome is the most common chromosomal abnormality among live-born infants. Through full or partial trisomy of chromosome 21, Down syndrome is associated with cognitive impairment, congenital malformations ( particularly cardiovascular) and dysmorphic features. Immune disturbances in Down syndrome account for an enormous disease burden ranging from quality-of-life issues (autoimmune alopecia) to more serious health issues (autoimmune thyroiditis) and life-threatening issues (leukaemia, respiratory tract infections and pulmonary hypertension). Cardiovascular and pulmonary diseases account for ∼75% of the mortality seen in persons with Down syndrome. This review summarises the cardiovascular, respiratory and immune challenges faced by individuals with Down syndrome, and the genetic underpinnings of their pathobiology. We strongly advocate increased comparative studies of cardiopulmonary disease in persons with and without Down syndrome, as we believe these will lead to new strategies to prevent and treat diseases affecting millions of people worldwide.

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“…Distinguishing whether insulin deficiency in these young children is caused by accelerated autoimmunity or an alternative mechanism, such as a b-cell secretary deficit, could have consequences for treatment or provide insights into a more aggressive autoimmune process in children with DS. Aliquots of DNA samples from 83 children with DS had been collected as controls for a study of congenital heart disease in DS (13). DNA samples (n = 109) were also available for analysis from a population-based study of children with DS in Manchester, U.K. (14).…”

mentioning

confidence: 99%

Early-Onset, Coexisting Autoimmunity and Decreased HLA-Mediated Susceptibility Are the Characteristics of Diabetes in Down Syndrome

et al. 2013

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OBJECTIVEdDown syndrome (DS) is associated with an increased risk of diabetes, particularly in young children. HLA-mediated risk is however decreased in children with DS and diabetes (DSD). We hypothesized that early-onset diabetes in children with DS is etiologically different from autoimmune diabetes.RESEARCH DESIGN AND METHODSdClinical and immunogenetic markers of autoimmune diabetes were studied in 136 individuals with DSD and compared with 194 age-and sex-matched individuals with type 1 diabetes, 222 with DS, and 671 healthy controls. HLA class II was analyzed by sequence-specific primed PCR. Islet autoantibodies were measured by radioimmunoassay.RESULTSdAge at onset of diabetes was biphasic, with 22% of DS children diagnosed before 2 years of age, compared with only 4% in this age-group with type 1 diabetes in the general population (P , 0.0001). The frequency of the highest-risk type 1 diabetes-associated HLA genotype, DR3-DQ2/DR4-DQ8, was decreased in both early-and later-onset DSD compared with age-matched children with type 1 diabetes (P , 0.0001), although HLA DR3-DQ2 genotypes were increased (P = 0.004). Antibodies to GAD were observed in all five samples tested from children diagnosed at #2 years of age, and persistent islet autoantibodies were detected in 72% of DSD cases. Thyroid and celiac disease were diagnosed in 74 and 14%, respectively, of the DSD cohort.CONCLUSIONSdEarly-onset diabetes in children with DS is unlikely to be etiologically different from autoimmune diabetes occurring in older DS children. Overall, these studies demonstrate more extreme autoimmunity in DSD typified by early-onset diabetes with multiple autoimmunity, persistent islet autoantibodies, and decreased HLA-mediated susceptibility.

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Heterotrisomy, a significant contributing factor to ventricular septal defect associated with Down syndrome?

Cited by 24 publications

References 41 publications

Islet Autoimmunity in Children With Down’s Syndrome

Islet Autoimmunity in Children With Down’s Syndrome

What people with Down Syndrome can teach us about cardiopulmonary disease

Early-Onset, Coexisting Autoimmunity and Decreased HLA-Mediated Susceptibility Are the Characteristics of Diabetes in Down Syndrome

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