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Dosage Compensation of Trisomy 21 and Its Implications for Hematopoietic Pathogenesis in Down SyndromeChiang, Jen-Chieh 06 November 2017 (has links)
Down Syndrome (DS), the most common aneuploidy seen in live-borns, is caused by trisomy for chromosome 21. DS imposes high risks for multiple health issues involving various systems of the body. The genetic complexity of trisomy 21 and natural variation between all individuals has impeded understanding of the specific cell pathologies and pathways involved. In addition, chromosomal disorders have been considered outside the hopeful progress in gene therapies for single-gene disorders. Here we test the feasibility of correcting imbalanced expression of genes across an extra chromosome by expression of a single gene, XIST, the key player in X chromosome inactivation. We targeted a large XIST transgene into one chromosome 21 in DS iPS cells, and demonstrated XIST RNA spreads and induces heterochromatin and gene silencing across that autosome in cis.
By making XIST inducible, this allows direct comparison of effects of trisomy 21 expression on cell function and phenotypes. Importantly, XIST-induction during in vitro hematopoiesis normalized excess production of differentiated blood cell types (megakaryocytes and erythrocytes), known to confer high risk for myeloproliferative disorder and leukemia. In contrast, trisomy silencing enhances production of iPS and neural stem cells, consistent with DS clinical features. Further analysis revealed that trisomy 21 initially impacts the endothelial hematopoietic transition (EHT) to generate excess CD43+ progenitors, and also increases their colony forming potential. Furthermore, results provide evidence for a key role for enhanced IGF signaling, involving over-expression of non-chromosome 21 genes controlled by trisomy 21. Finally, experiments to examine trisomy effects on angiogenesis showed no effect on production of endothelial cells, but it remains unclear whether trisomic cells may differ in ability to form vessels.
Collectively, this thesis demonstrates proof-of-principle for XIST-mediated “trisomy silencing”. Phenotypic improvement of hematopoietic and neural stem cells demonstrates the value for research into DS pathogenesis, but also provides a foundation of potential for future development of “chromosome therapy” for DS patients.
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Oral motor therapy with palatal plates in children with Down syndrome - A systematic reviewSvensson, Hanna, Eriksson, Ida January 2017 (has links)
Syfte: Syftet med denna studie var att utvärdera effekten av stimulerande gomplattor på den orala motoriken hos barn med Downs syndrom. Studien syftar också till att undersöka om behandlingen är kostnadseffektiv.Material och Metod: Studien är en systematisk litteraturstudie enligt PRISMAs kriterier och artiklarna kvalitetsgranskades med hjälp SBU: s handbok. De databaser som användes för litteratursökningen var PubMed, Cochrane Library, Scopus och CINAHL.Resultat: Screeningen av 107 unika artiklar resulterade i 14 relevanta publikationer. Kvaliteten på artiklarna var överlag låg och 9 artiklar bedömdes måttlig risk för bias och 5 artiklar bedömdes ha hög risk för bias. Alla 14 inkluderade artiklar visade en positiv effekt på minst en orofacial variabel men det finns ingen konsensus gällande utvärderingsmetoder för behandling med gomplattor, behandlingstider eller vilka orofaciala variabler som bör undersökas.Slutsats: I denna litteraturgenomgång identifierades ett antal studier, som undersökte effekten av behandling med stimulerande gomplattor. På grund av att artiklarna använde icke standardiserade metoder, hade olika behandlingstider och använde olika variabler för att mäta effekten, kan ingen slutsats dras från dessa studier. Fler RCT studier med större grupper av barn och standardiserade metoder för utvärdering behövs. / Aim: The aim of this study was to evaluate the effect of treatment with stimulating palatal plates on the oral motor function in children with Down syndrome. The study also aims to investigate if the treatment is cost-effective.Material and Method: The study is a systematic review made according to the PRISMA criteria. The articles were quality reviewed using Swedish Agency for Health Technology Assessment and Assessment of Social Services - SBU’s manual. The databases used for the literature search were PubMed, Cochrane Library, Scopus and CINAHL.Result: Screening of 107 unique papers resulted in 14 eligible publications. The quality of the articles was overall low. Nine articles were rated moderate risk of bias and 5 articles were rated high risk of bias. All 14 included articles showed a positive effect in one or more aspects on oral motor function but there is no consensus regarding evaluation methods for treatment with palatal plates, treatment times or which orofacial variables that should be investigated. No meta-analysis was made due to the lack of consensus.Conclusion: This literature review identified a number of studies, which investigated the effect of treatment with stimulating palatal plates. Due to the unstandardized methods, different treatment times, and different orofacial measuring variables, no consensus can be drawn from these studies. More RCT studies with larger groups of children and standardized methods for evaluation are required.
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Stéréotype explicite et implicite des personnes porteuses de trisomie 21. Relations entre typicalité du visage, jugement sur l'intelligence et niveau cognitif / Explicit and implicit stereotyping of trisomy 21. Relationships between typicality of faces, judgment of intelligence and cognitive level.Enéa Drapeau, Claire 20 December 2012 (has links)
La trisomie 21 (t21) est l'anomalie génétique la plus fréquente à l'origine d'une déficience intellectuelle. Bien que la recherche concernant le stéréotype social de la t21 soit limitée, les personnes porteuses de t21, et particulièrement les enfants, semblent être associées à des traits de personnalité tels que « affectueux » et « heureux », les caractéristiques positives l'emportant sur les négatives comme « retardé ». Cependant, ce stéréotype positif coexiste avec des attitudes ambivalentes notamment à propos de l'intégration scolaire de ces enfants. L'objectif principal de cette thèse est d'étudier ce stéréotype au niveau implicite ainsi que l'impact des caractéristiques faciales sur le stéréotype au niveau explicite et implicite. Nos résultats confirment d'une part, un stéréotype social positif explicite dans des échantillons d'étudiants, d'adultes non étudiant et de professionnels du handicap intellectuel. Les visages d'enfants présentant plus de traits faciaux associés à la t21 sont associés à un stéréotype moins positif que ceux en présentant moins. D'autre part, nous mettons en évidence un stéréotype négatif au niveau implicite, même chez les professionnels du handicap. Nous étudions l'influence des variables individuelles sexe, familiarité avec la t21 et théories implicites de l'intelligence sur le stéréotype explicite et implicite. Puis, nous montrons une relation négative entre la typicalité des visages et le jugement sur l'intelligence alors que nous n'observons pas de relation significative entre la typicalité des visages et le niveau cognitif. Nous discutons l'implication de ces résultats sur l'étude du stéréotype et sur les personnes stigmatisées. / Trisomy 21 (t21) or Down syndrome is the most frequent genetic disorder associated with intellectual disability. Although research on the social stereotype toward t21 is very limited, it seems that persons with t21 are typically viewed as “affectionate” and “happy”; with positive personality traits prevailing over the negative ones (e.g., “mentally retarded”). However, this positive stereotype coexists with ambivalent attitudes. The main objective of this study was to investigate the stereotype at the implicit level and the impact of t21 facial features on the stereotype of t21 at the both explicit and implicit levels. Our results confirm, on one hand, a positive social stereotype explicit in samples of young adult students, non-student adults and professional caregivers working with intellectually disabled persons. The positive bias typically found in explicit judgments of children with t21 is smaller for those whose facial features are highly characteristic of this disorder, compared to their counterparts with less distinctive features and to typically developing children. On the other hand, we also show that this bias can coexist with negative evaluations at the implicit level, even among professional caregivers but to a lesser extent. We study the influence of individual variables sex, familiarity with the t21 and implicit theories of intelligence on explicit and implicit stereotypes. Finally, we show a negative relationship between t21 typicality of faces and the judgment of the intelligence as we do not observe a significant relationship between typicality and the cognitive level. We discuss the implications of these results.
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Investigação dos polimorfismos do gene PLAC4 na população brasileira / Investigation of PLAC4 gene polymorphisms in the Brazilian populationRomão, Renata Moscolini 07 March 2012 (has links)
Duzentas amostras de DNA obtidas de voluntários brasileiros não aparentados foram triadas para SNPs em uma região de 4079 pares de bases do gene PLAC4 através de reação em cadeia da polimerase (PCR) - utilizando o kit Taq Platinum DNA polymerase (Invitrogen, USA) ciclada em termociclador Eppendorf Mastercycle Gradient (Eppendorf, Germany); e posterior sequenciamento - utilizando o kit Big Dye Terminator Cycle Sequencing v3.1 (Applied Biosystems, USA) corrida em sequenciador ABI 3100 DNA Sequencer (Applied Biosystems, USA). Sete fragmentos foram amplificados utilizando pares de iniciadores desenhados com o auxílio do programa Primer 3 baseado em uma sequência do gene PLAC4 obtida do GenBank. Dez SNPs com taxa de heterozigozidade superior a 25% foram identificados, localizados em seis dos sete fragmentos estudados, que fazem a cobertura de 93% da população brasileira. Um painel combinando estes 10 SNPs apresenta potencial utilidade clínica em um teste pré-natal não invasivo da síndrome de Down fetal baseado na abordagem SNP/mRNA / Two hundred DNA samples obtained from unrelated Brazilian individuals were screened for SNPs in a region of 4079 bp of the exon of PLAC4 gene by polymerase chain reaction (PCR) - using Taq Platinum DNA polymerase kit (Invitrogen, USA) cycled on Eppendorf Mastercycle Gradient thermocycle (Eppendorf, Germany); and subsequent sequencing using Big Dye Terminator Cycle Sequencing v3.1 kit (Applied Biosystems, USA) on ABI 3100 DNA Sequencer (Applied Biosystems, USA). Seven fragments were amplified using primer pairs designed by primer 3 software based on PLAC4 sequence obtained from GenBank. Ten SNPs with heterozigosity rate above 25% were identified, located in six of the seven fragments studied, that covers up to 93% of Brazilian population. A panel combining this 10 SNPs show potential utility in clinical setting for a noninvasive prenatal diagnostic test for Down syndrome based in the SNP/mRNA approach
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Síndrome de Down e polimorfismos em genes envolvidos no metabolismo do folato.Marucci, Gustavo Henrique 12 December 2011 (has links)
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Previous issue date: 2011-12-12 / Down syndrome (DS) is a complex genetic disease resulting mainly from the presence of three copies of chromosome 21. It is the most frequent human chromosomal abnormality and, in most cases (about 95%) results from maternal chromosome nondisjunction, which occurs during meiosis I. Recent studies suggest that the etiology of maternal risk for DS in young mothers is associated with polymorphisms in genes of folate/homocysteine metabolism. The proper function of folate metabolism is essential for the synthesis of methyl groups necessary for DNA methylation. The deficiency of this metabolite has resulted in DNA hypomethylation, chromosomal breakage and aneuploidies. Objectives: Evaluate the influence of the C1420T polymorphism in serine hidroximetiltransferase (SHMT) gene on the maternal risk for DS, and investigate the association between this polymorphism and variation in the concentration of serum folate, plasma Hcy and methylmalonic acid (MMA); investigate the impact of 19 base pairs (pb) deletion polymorphism of the dihydrofolate reductase (DHFR) gene and the C1420T polymorphism of the SHMT gene on serum folate concentrations, plasma Hcy and MMA in individuals with DS. Material and methods: 105 mothers of individuals with free trisomy of chromosome 21 and 185 mothers of individuals without the syndrome (no history of miscarriage), and 85 individuals with free trisomy of 21 chromosome were included in this study. The polymorphism of DHFR gene was evaluated by Polymerase Chain Reaction (PCR) by fragment size difference, and the polymorphism of SHMT gene was analyzed by real-time PCR allelic discrimination. Results: The SHMT CC and CT genotypes were associated with decreased maternal risk for DS (CC: P= 0.0002; 95% CI: 0.20 0.60; OR: 0.35. CT: P < 0.0001; 95% IC: 0.11 - 0.39; OR: 0.21). The different genotypes did not influence the concentrations of metabolites studied. In individuals with DS, the combined genotypes DHFR II/ SHMT TT and DHFR DD/ SHMT TT were associated, respectively, with increased concentrations of Hcy (P<0.001) and folate (P<0.001). Moreover, individuals with DHFR II/ SHMT CT genotypes presented a reduction of folate concentration (P= 0.01). Conclusion: The CC and CT genotypes of SHMT C1020T polymorphism has a protector effect for maternal risk for DS. This polymorphism does not seem to influence the folate, Hcy and MMA concentrations. The del 19pb DHFR and SHMT C1420T polymorphisms present a synergic effect in modulating folate and Hcy concentrations in individuals with DS. / A síndrome de Down (SD) é uma doença genética complexa resultante, principalmente, da presença de três cópias do cromossomo 21. É a cromossomopatia humana mais frequente e, na maioria dos casos (cerca de 95%), decorrente da não disjunção cromossômica materna, ocorridas durante a meiose I. Recentes estudos sugerem que a etiologia do risco materno para a SD em mães jovens está relacionada com polimorfismos em genes do metabolismo do folato/homocisteína (Hcy). O funcionamento adequado do metabolismo do folato é essencial para a síntese de grupos metil necessários para a metilação do DNA. A deficiência deste metabólito tem como resultado, a hipometilação do DNA, quebras cromossômicas e aneuploidias. Objetivos: Avaliar a influência do polimorfismo C1420T do gene serina hidroximetiltransferase (SHMT) no risco materno para a SD e nas concentrações de folato sérico, Hcy e ácido metilmalônico (MMA) plasmáticos ; investigar o impacto dos polimorfismos de deleção de 19 pares de base (pb) do gene dihidrofolato redutase (DHFR) e de transição C1420T do gene SHMT nas concentrações de folato sérico, Hcy e MMA plasmáticos em indivíduos com SD. Casuística e métodos: Foram incluídas no estudo 105 mães de indivíduos com trissomia livre do cromossomo 21 e 185 mães de indivíduos sem a síndrome (sem história prévia de aborto espontâneo), e 85 indivíduos com trissomia livre do cromossomo 21. O polimorfismo do gene DHFR foi avaliado por meio da Reação em Cadeia da Polimerase (PCR) por diferença de tamanho de fragmentos, e o polimorfismo SHMT C1420T foi analisado por PCR em tempo real. Resultados: Os genótipos CC e CT do polimorfismo SHMT C1420T foram associados à redução do risco materno para SD (CC: P = 0,0002; 95% IC: 0,20 0,60; OR: 0,35. CT: P < 0,0001; 95% IC: 0,11 0,39; OR: 0,21). Os diferentes genótipos não influenciaram as concentrações dos metabólitos estudados. No grupo de indivíduos com SD, os genótipos combinados DHFR II/SHMT TT e DHFR DD/SHMT TT foram associados, respectivamente, com concentrações aumentadas de Hcy (P < 0,001) e de folato (P < 0,001). Além disso, indivíduos com os genótipos DHFR II/SHMT CT apresentaram concentração reduzida de folato (P = 0,01). Conclusão: Os genótipos CC e CT do polimorfismo SHMT C1420T conferem um efeito materno protetor para SD. Este polimorfismo parece não influenciar as concentrações de folato, Hcy e MMA. Os polimorfismos del 19pb DHFR e C1420T SHMT apresentam um efeito sinérgico na modulação das concentrações de folato e Hcy de indivíduos com SD.
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Investigação dos polimorfismos do gene PLAC4 na população brasileira / Investigation of PLAC4 gene polymorphisms in the Brazilian populationRenata Moscolini Romão 07 March 2012 (has links)
Duzentas amostras de DNA obtidas de voluntários brasileiros não aparentados foram triadas para SNPs em uma região de 4079 pares de bases do gene PLAC4 através de reação em cadeia da polimerase (PCR) - utilizando o kit Taq Platinum DNA polymerase (Invitrogen, USA) ciclada em termociclador Eppendorf Mastercycle Gradient (Eppendorf, Germany); e posterior sequenciamento - utilizando o kit Big Dye Terminator Cycle Sequencing v3.1 (Applied Biosystems, USA) corrida em sequenciador ABI 3100 DNA Sequencer (Applied Biosystems, USA). Sete fragmentos foram amplificados utilizando pares de iniciadores desenhados com o auxílio do programa Primer 3 baseado em uma sequência do gene PLAC4 obtida do GenBank. Dez SNPs com taxa de heterozigozidade superior a 25% foram identificados, localizados em seis dos sete fragmentos estudados, que fazem a cobertura de 93% da população brasileira. Um painel combinando estes 10 SNPs apresenta potencial utilidade clínica em um teste pré-natal não invasivo da síndrome de Down fetal baseado na abordagem SNP/mRNA / Two hundred DNA samples obtained from unrelated Brazilian individuals were screened for SNPs in a region of 4079 bp of the exon of PLAC4 gene by polymerase chain reaction (PCR) - using Taq Platinum DNA polymerase kit (Invitrogen, USA) cycled on Eppendorf Mastercycle Gradient thermocycle (Eppendorf, Germany); and subsequent sequencing using Big Dye Terminator Cycle Sequencing v3.1 kit (Applied Biosystems, USA) on ABI 3100 DNA Sequencer (Applied Biosystems, USA). Seven fragments were amplified using primer pairs designed by primer 3 software based on PLAC4 sequence obtained from GenBank. Ten SNPs with heterozigosity rate above 25% were identified, located in six of the seven fragments studied, that covers up to 93% of Brazilian population. A panel combining this 10 SNPs show potential utility in clinical setting for a noninvasive prenatal diagnostic test for Down syndrome based in the SNP/mRNA approach
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Aspects pratiques et enjeux éthiques du dépistage prénatal non invasif de la trisomie 21 : mise au point et enquête auprès de professionnels de santé et de patientes / Practical aspects and ethical issues related to non invasive prenatal testing for trisomy 21 : update and investigation of healthcare professionals and patientsMiry, Claire 22 September 2016 (has links)
La place du Dépistage Prénatal Non Invasif (DPNI) n’est pas encore clairement définie dans le dépistage prénatal de la trisomie 21 en France. Nos objectifs étaient d’évaluer la compréhension, les connaissances, et l’attitude de professionnels de santé et de patientes concernant le DPNI.Une étude prospective multicentrique par questionnaire auprès de patientes enceintes et de professionnels de santé a été menée dans différents hôpitaux français entre février 2014 et juillet 2015.Sur les 260 questionnaires recueillis chez les professionnels, le score moyen de connaissances était 5,38±2,83(sur 10)et 92,7%(n=241) avaient une attitude favorable face au DPNI. En analyse multivariée, les facteurs associés à un bon niveau de connaissances étaient la profession de gynécologue ou de conseiller en génétique, l’âge<30 ans, le fait de travailler à l’hôpital ou en cabinet et le fait de suivre>50 grossesses par an.Sur les 380 questionnaires de patientes, le score moyen de connaissances était faible 2,20±1,88(sur 10) et 89,9%(n=328) avaient une attitude favorable face au DPNI. En analyse multivariée, les facteurs associés à un bon niveau de connaissances chez les patientes étaient l’âge maternel et le fait de consulter en secteur privé.Le niveau de connaissances des professionnels et des patientes sur le DPNI est faible. La plupart des patientes ne peuvent pas formuler de consentement éclairé. Toutefois, la plupart des professionnels et des patientes sont très en faveur de ce test. La généralisation du DPNI dans le dépistage de la trisomie 21 implique un important programme de formation des professionnels afin qu'ils délivrent une information prénatale de qualité et non directive. / The place of Non Invasive Prenatal Testing(NIPT) is not clearly established for prenatal screening for Down syndrome in France. Our objectives were to assess the understanding, knowledge of, and attitudes towards NIPT in French patients and healthcare providers.A prospective multicenter study was performed in several French hospital centers between February 2014 and July 2015. A survey was administered to pregnant patients and to healthcare professionals.A total of 260 questionnaires were completed by healthcare providers. The average knowledge score was 5,38±2,83(out of a possible 10). In multivariate analysis, the characteristics associated with satisfactory knowledge were: profession as obstetrician or genetic counsellor, age<30 years, working in hospital or in doctor’s office, more than 50 pregnancies followed per year. Among professionals, 92,7%n=241) had a favorable attitude towards NIPT.We collected 380 questionnaires from pregnant women. The average knowledge score was very low: 2,20±1,88(out of 10). In multivariate analysis, the two significant characteristics associated with satisfactory knowledge was maternal age and having prenatal care in private practice. Among patients, 89,9%(n=328) had a favorable attitude towards NIPT.The level of knowledge of NIPT of healthcare professionals and patients is low. Many patients can not provide informed consent. However most professionals and patients are in favor of the use of this test. The input of NIPT in prenatal screening for trisomy 21 requires a considerable teaching program for healthcare providers so they can give balanced pretest information and non-directive counselling.
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SKELETAL DEFICITS IN MALE AND FEMALE MOUSE MODELS OF DOWN SYNDROMEJared Thomas (8766693) 14 May 2020 (has links)
<p>Down syndrome (DS) is a genetic disorder that results from triplication of human chromosome 21 (Hsa21) and occurs in around 1 in 1000 live births. All individuals with DS present with skeletal abnormalities typified by craniofacial features, short stature and low bone mineral density (BMD). Differences between males and females with DS suggest a sexual dimorphism in how trisomy affects skeletal deficits associated with trisomy 21 (Ts21). Previous investigations of skeletal abnormalities in DS have varied methodology, sample sizes and ages making the underlying causes of deficits uncertain. Mouse models of DS were used to characterize skeletal abnormalities, but the genetic and developmental origin remain unidentified. Over-expression <i>Dyrk1a</i>, found on Hsa21 and mouse chromosome 16 (Mmu16) has been linked to cognitive deficits and skeletal deficiencies. Dp1Tyb mice contain three copies of all of the genes on Mmu16 that are homologous to Hsa21, males and females are fertile, and therefore are an excellent model to test the hypothesis that gene dosage influences the sexual dimorphism of bone abnormalities in DS. Dp1Tyb at 6 weeks 16 weeks showed distinctive abnormalities in BMD, trabecular architecture, and reduced bone strength over time that occur generally through an interaction between sex and genotype. Increased gene dosage and sexual dimorphism in Dp1Tyb mice revealed distinct phenotypes in bone formation and resorption. To assess how <i>Dyrk1a</i> influences the activity and function of osteoblasts Ts65Dn female trisomic mice, female mice with a floxed <i>Dyrk1a</i> gene (Ts65Dn, <i>Dyrk1a</i><sup>fl/+</sup>) were be bred to <i>Osx1</i>-GFP::Cre+ mice to generate Ts65Dn animals with a reduced copy of <i>Dyrk1a </i>in mature osteoblast cells. Female Ts65Dn,<i>Dyrk1a<sup>+/+/+</sup></i><sup> </sup>and Ts65Dn,<i>Dyrk1a<sup>+/+/-</sup></i>displayed significant defects in both trabecular architecture and cortical geometry. Ultimate force was reduced in trisomic animals, suggesting whole bone and tissue level properties are not adversely affected by trisomy. Reduction of <i>Dyrk1a</i> functional copy number in female mice did not improve skeletal deficits in an otherwise trisomic animal. <i>Dyrk1a </i>may not alter osteoblast cellular activity in an autonomous manner in trisomic female mice. These data establish sex, gene dosage, skeletal site and age as important factors in skeletal development of the skeleton in DS mice, potentially paving the way for identification of the causal dosage-sensitive genes in both male and female animals. </p>
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Prévalence de l’aplasie et de l’hypoplasie des glandes salivaires majeures chez les enfants atteints du syndrome de Down (trisomie 21)Nguyen, Julie Mi 07 1900 (has links)
No description available.
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Óbito fetal em gestações únicas com diagnóstico de trissomias dos cromossomos 21,18 13 e monossomia do X / Intrauterine death in pregnancies with trisomy 21, 18, 13 and X monosomyGoulart, Vanessa Vigna 10 September 2014 (has links)
Objetivos: Descrever a frequência, e investigar fatores preditivos, de óbito fetal espontâneo (OF), em gestações com anomalias cromossômicas. Métodos: Trata-se de estudo retrospectivo, abrangendo o período de novembro de 2004 a maio de 2012, realizado na Clínica Obstétrica do Hospital das Clínicas da Faculdade de Medicina da Universidade de São Paulo. Foram incluídas gestações únicas com diagnóstico pré-natal de trissomia dos cromossomos 21 (T21), 18, 13 (T13/18) e monossomia do X (45X), realizado até a 26ª semana de gestação. Resultados: Foram incluídas 92 gestantes com idade materna média de 32,7 ± 8,7 anos. O diagnóstico das anomalias cromossômicas (T21 n=36, T13/T18 n=25, 45X n=31) foi realizado em idade gestacional média de 18,3 ± 3,7 semanas, por meio de biópsia de vilo corial (n=22, 24%), amniocentese (n=66, 72%) e cordocentese (n=4, 4%). Malformação major estava presente em 45 (49%); e hidropisia foi identificada em 32 (35%) fetos, sendo mais frequente no grupo 45X (n=24/31 (77%) versus T21: n=6/36 (17%) e T13/18: n=2/25 (8%), p < 0,001). Exame ecocardiográfico fetal especializado foi realizado em 60% (55/92) das gestações. Dessas, 60% (33/55) apresentaram alterações na morfologia e/ou função cardíaca, sendo o achado mais frequente a comunicação interventricular (39%). Fetos com T13/18 apresentaram incidência maior de anomalias cardíacas (60% versus 25% (T21) e 29% (45X), p= 0,01). Óbito fetal ocorreu em 55 (60%) gestações e foi mais frequente no grupo 45X (n=26/31 (84%) versus T21: n=13/36 (36%) e T13/18: n=16/25 (64%), p < 0,01). A análise multivariada stepwise demonstrou associação entre hidropisia e OF em fetos com trissomia 21 (LR= 4,29; IC95%= 1,9-8,0, p< 0,0001). Em fetos com monossomia X, a presença de alterações ecocardiográficas esteve associada com menor risco de OF (LR= 0,56; IC95% = 0,27-0,85, p= 0,005). Não foram identificados fatores preditores no grupo T13/18. Conclusão: A letalidade intrauterina de fetos com anomalias cromossômicas é elevada. A presença de hidropisia aumenta o risco de óbito fetal, em gestações com trissomia 21. Enquanto, em gestações com monossomia X, a ocorrência de alterações ecocardiográficas reduz esse risco / Objectives: To describe the frequency, and associated factors, of intrauterine fetal death (IUD), in pregnancies with chromosomal abnormality. Methods: This was a retrospective (November 2004 to May 2012) performed at de department of obstetrics, Hospital das Clínicas, São Paulo University Medical School. Inclusion criteria were: singleton pregnancies with prenatal diagnosis of trisomy 21 (T21), 18, 13 (T13/18) and X monosomy (45X), performed up to 26 weeks gestation. Results: 92 women were included in the study with a mean maternal age of 32.7 ± 8.7 years. Fetal chromosomal abnormalities (T21 n=36, T13/T18 n=25, 45X n=31) were diagnosed at a mean gestational age of 18.3 ± 3.7 weeks, by chorionic villus sampling (n=22, 24%), amniocentesis (n=66, 72%) and cordocentesis (n=4, 4%). Major fetal structural abnormality was present in 45 (49%) cases; hydrops was diagnosed in 32 (35%) fetuses, and was more common in 45X group (n=24/31 (77%) versus T21: n=6/36 (17%) and T13/18: n=2/25 (8%), p < 0.001). Specialist fetal echocardiography was performed in 55 (60%) pregnancies and showed structural and/or functional abnormalities in 33 (60%) fetuses; ventricular septal defect was the most common finding (39%). T13/18 fetuses showed a higher incidence of cardiac abnormalities (60% versus 25% (T21) and 29% (45X), p= 0.01). IUD occurred in 55 (60%) pregnancies and was more common in 45X group (n=26/31 (84%) versus T21: n=13/36 (36%) and T13/18: n=16/25 (64%), p < 0.01). Stepwise logistic regression analysis demonstrated an association between hydrops and IUD in T21 pregnancies (LR= 4.29; 95%CI= 1.9-8.0, p < 0.0001). In 45X pregnancies, cardiac abnormalities were associated with a lower risk of IUD (LR= 0.56; 95%CI = 0.27-0.85, p= 0.005). No predictors of IUD were identified in T13/18 group. Conclusion: Intrauterine death rate is high in pregnancies with a fetal chromosomal abnormality. Presence of hydrops increases the risk of this complication in trisomy 21 fetuses. Whereas the presence of a cardiac abnormality is protective in X monosomy pregnancies
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