Your search keyword '"Síndrome de DiGeorge"' showing total 11 results

1. Investigação Citogenômica de Crianças com Doença Cardíaca Congênita: Experiência de um Centro no Brasil

Author

Leslie Domenici Kulikowski, Chong Kim, Nana Miura, Antonio Carlos Pastorino, Marcelo B. Jatene, Marília M. Montenegro, Evelin Aline Zanardo, Magda Carneiro-Sampaio, Mayra de Barros Dorna, and Marcília Sierro Grassi

Subjects

Diagnóstico Precoce, business.industry, Deleção Cromossômica, Newborn, Congenital Abnormalities, Congenital, Early Diagnosis, Recém-Nascido, Cardiopatias Congênitas, DiGeorge Syndrome, Anormalidades Congênitas, Medicine, Chromosome Deletion, Cardiology and Cardiovascular Medicine, business, Humanities, Heart Defects, Síndrome de DiGeorge

Abstract

Resumo Fundamento Algumas síndromes têm características específicas e facilmente reconhecíveis, enquanto outras podem ser mais complexas de se identificar e podem apresentar diferentes manifestações fenotípicas, por exemplo. Um diagnóstico etiológico é importante para entender a natureza da doença, para estabelecer o prognóstico e para começar o tratamento, permitindo a inclusão de pacientes na sociedade e reduzindo o custo financeiro dessas doenças. Objetivo A proposta inicial deste estudo foi a triagem citogenética para detectar a síndrome de deleção 22q11.2 (SD22q11.2) em recém-nascidos e crianças com doença cardíaca congênita utilizando a técnica da amplificação multiplex de sondas dependente de ligação (MLPA). Assim, por meio da pesquisa, outras mudanças genômicas foram identificadas nesses pacientes cardíacos. Nosso objetivo se estendeu a investigar essas outras mudanças citogenéticas. Métodos Investigamos 118 recém-nascidos com doenças cardíacas congênitas nascidos consecutivamente durante um ano, utilizando a técnica da MLPA. Resultados A técnica da MLPA permitiu a detecção da SD22q11.2 em 10/118 pacientes (8,5%). Outras alterações genômicas foram identificadas em 6/118 pacientes (5%): 1p36 del, 8p23 del (2 casos), 7q dup, 12 dup e 8q24 dup. Conclusão Este estudo ressalta a relevância da detecção de alterações genômicas que estão presentes em recém-nascidos e crianças com doenças cardíacas congênitas por meio de ferramentas citogenômicas. Abstract Background Some syndromes have specific and easily recognizable features, while others may be more complex to identify and may present different phenotypic manifestations, for example. An etiological diagnosis is important to understand the nature of the disease, to establish the prognosis and to start the treatment, allowing the inclusion of patients in society and reducing the financial cost of such diseases. Objective The initial proposal of this study was cytogenetic screening for the detection of the 22q11.2 deletion syndrome in consecutive newborns and infants with congenital heart disease using the multiplex ligation-dependent probe amplification (MLPA) technique. Therefore, throughout our research, other genomic alterations were identified in these cardiac patients. Thus, our objective was extended to investigate these other cytogenetic alterations. Methods We investigated 118 neonates with congenital heart diseases born consecutively during one year using the MLPA technique. Results The MLPA technique allowed the detection of 22q11.2DS in 10/118 patients (8.5%). Other genomic alterations were also identified in 6/118 patients (5%): 1p36 del, 8p23 del (2 cases), 7q dup, 12 dup and 8q24 dup. Conclusion This study highlights the relevance of detecting genomic alterations that are present in newborns and infants with congenital cardiac diseases using cytogenomic tools.

Published

2022

2. Case Report: Autoimmune Psychosis in Chromosome 22q11.2 Deletion Syndrome

Author

Nicolás Lundahl Ciano-Petersen, Omar Hamad-Cueto, Hania Drissi-Reyes, Álvaro Doña-Díaz, Guillermina García-Martín, [Ciano-Petersen,NL, García-Martín,G] Neuroimmunology and Neuroinflammation Group, Instituto de Investigación Biomédica de Málaga (IBIMA), Málaga, Spain. [Ciano-Petersen,NL, García-Martín,G] Servicio de Neurología, Hospital Regional Universitario de Málaga, Málaga, Spain. [Ciano-Petersen,NL] Andalucía Tech, Facultad de Medicina, Universidad de Málaga, Málaga, Spain. [Ciano-Petersen,NL, and García-Martín,G] Red Andaluza de Investigación Clínica y Traslacional en Neurología (Neuro-Reca), Málaga, Spain. [Hamad-Cueto,O] Servicio de Neurología, Hospital Clínico Universitario Virgen de la Victoria, Málaga, Spain. [Drissi-Reyes,H] Servicio de Urgencias, Hospital El Ángel, Málaga, Spain. [Doña-Díaz,Á] UGC Salud Mental, Hospital Universitario Virgen de la Victoria, Málaga, Spain.

Subjects

autoimmune psychosis, Psychosis, Trastornos psicóticos, medicine.medical_treatment, chromosome 22q112 deletion syndrome, Immunology, Arthritis, Case Report, Chromosome 22q112 deletion syndrome, Persons::Persons::Age Groups::Adolescent [Medical Subject Headings], Organisms::Eukaryota::Animals::Chordata::Vertebrates::Mammals::Primates::Haplorhini::Catarrhini::Hominidae::Humans [Medical Subject Headings], Immune system, Enfermedades autoinmunes, Diseases::Immune System Diseases::Autoimmune Diseases [Medical Subject Headings], medicine, Diseases::Congenital, Hereditary, and Neonatal Diseases and Abnormalities::Genetic Diseases, Inborn::Chromosome Disorders::22q11 Deletion Syndrome::DiGeorge Syndrome [Medical Subject Headings], Psychiatry and Psychology::Mental Disorders::Schizophrenia and Disorders with Psychotic Features::Psychotic Disorders [Medical Subject Headings], Immunology and Allergy, psychosis, Autoimmune encephalitis, Publication Type::Study Characteristics::Case Reports [Medical Subject Headings], Síndrome de DiGeorge, Diseases::Nervous System Diseases::Central Nervous System Diseases::Brain Diseases::Encephalitis [Medical Subject Headings], cognitive impairment, business.industry, Chemicals and Drugs::Chemical Actions and Uses::Pharmacologic Actions::Physiological Effects of Drugs::Immunologic Factors [Medical Subject Headings], Encefalitis, Immunotherapy, RC581-607, medicine.disease, Autoimmune psychosis, Thrombocytopenic purpura, autoimmune encephalitis, Cognitive impairment, Check Tags::Female [Medical Subject Headings], Etiology, Disfunción cognitiva, Immunologic diseases. Allergy, business, Developmental regression

Abstract

Chromosome 22q11.2 deletion syndrome (22q11DS) is characterized by congenital cardiac abnormalities, hypoplastic thymus, palatal abnormalities, and hypocalcemia, although other clinical features are frequent such as autoimmune and psychiatric disorders. One-third of the patients have psychotic disorders, frequently followed by developmental regression and long-term cognitive disturbances. Despite humoral and cellular immunodeficiency are common in 22q11DS, it is associated with an increased prevalence of autoimmune disorders such as idiopathic thrombocytopenic purpura and juvenile idiopathic arthritis, likely due to immune dysregulations associated with thymic abnormalities, which plays a major role in self-tolerance. We report an unique case of a 14-year-old girl with 22q11DS that presented with subacute psychotic symptoms, intolerance to antipsychotics, CSF pleocytosis, and EEG abnormalities, that was successfully treated with empiric immunotherapy after fulfilling criteria for probable seronegative autoimmune encephalitis and probable autoimmune psychosis. The autoimmune etiology of these clinical features of 22q11DS has never been postulated despite the predisposition of this syndrome to present autoimmune disorders. We suggest the systematic evaluation with serum and CSF neuronal antibodies, MRI, and EEG of patients with 22q11DS that develop subacute psychotic symptoms or rapidly progressive cognitive decline. Early immunomodulatory therapies should be carefully considered if criteria of probable autoimmune psychosis or possible autoimmune encephalitis are fulfilled, as it may prevent long-term disabilities. Further studies are required to assess the autoimmune origin of psychosis and cognitive impairment associated with 22q11DS.

Published

2021

3. Live Vaccine in Children with DiGeorge/22q11.2 Deletion Syndrome

Author

Isabel Esteves, José Gonçalo Marques, Andreia Teixeira Martins, Ana Serra-Caetano, Mariana Miranda, Sara Carvalho, and Repositório da Universidade de Lisboa

Subjects

medicine.medical_specialty, Viral Vaccines/adverse effects, lcsh:Medicine, Criança, Child, Chromosome Deletion, Chromosome Disorders, Chromosomes, Human, Pair 22, DiGeorge Syndrome, Vaccines, Attenuated/adverse effects, Cromossomas Humanos Par 22, Vacinas Virais/efeitos adversos, Transtornos Cromossómicos, Medicine, Deletion syndrome, Chromosomes, human, Ppir 22, DiGeorge syndrome, Síndrome de DiGeorge, Chromosome disorders, Gynecology, Deleção Cromossómica, Vacinas Atenuadas/efeitos adversos, lcsh:R5-920, business.industry, lcsh:R, General Medicine, Chromosome deletion, Vaccines, attenuated/adverse effects, business, lcsh:Medicine (General)

Abstract

Copyright © Ordem dos Médicos 2019, Children with DiGeorge syndrome/chromosome 22q11.2 deletion syndrome might have a variable degree of immunodeficiency, which may limit the use of live vaccines. The aim of this study was to review the adverse effects of live vaccines and possible relation with immune status in patients with DiGeorge Syndrome/partial 22q11.2 deletion syndrome.Material e Métodos: Foi realizado um estudo retrospetivo por revisão dos processos clínicos das crianças com deleção do cromossoma 22q11.2 e fenótipo de síndrome de DiGeorge, seguidos num centro de referência de imunodeficiências primárias. Foi realizada colheita de dados, incluindo: características demográficas; história médica; historial de vacinação com vacinas vivas; contagem de linfócitos T-CD4+ e respostas proliferativas linfocitárias a antigénios e mitogénios; reações adversas; falências vacinais. Resultados: Foram incluídas 23 crianças com síndrome de DiGeorge/deleção 22q11.2, 65,2% do sexo masculino e idade média de diagnóstico de 11,3 meses. Destas, 18 crianças (78%) receberam a vacina bacillus Calmette-Guérin: todas com evidência de atividade tímica; três apresentaram linfopénia T-CD4+ moderada e respostas proliferativas linfocitárias anormais; uma com respostas proliferativas linfocitárias anormais para mitogénios, quatro para derivado de proteína purificada e uma para toxóide tetânico. A vacina tríplice contra o sarampo, parotidite e rubéola foi administrada a 15 crianças, três com imunossupressão moderada e respostas proliferativas linfocitárias anormais. A vacina viva atenuada contra poliomielite foi administrada a quatro crianças sem imunossupressão e a vacina contra o rotavírus a três crianças, uma com imunossupressão moderada. Não foram reportadas reações adversas. Discussão: Estes dados estão de acordo com as conclusões de outros estudos internacionais. Conclusão: Na nossa amostra, as vacinas vivas atenuadas foram bem toleradas, incluindo em crianças com linfopénia T-CD4+ moderada e com respostas proliferativas linfocitárias a antigénios/mitogénios anormais., Introduction: Children with DiGeorge syndrome/chromosome 22q11.2 deletion syndrome might have a variable degree of immunodeficiency, which may limit the use of live vaccines. The aim of this study was to review the adverse effects of live vaccines and possible relation with immune status in patients with DiGeorge Syndrome/partial 22q11.2 deletion syndrome. Material and Methods: Retrospective study with analysis of the clinical records of children with chromosome 22q11.2 deletion syndrome and DiGeorge syndrome phenotype, followed in a Primary Immunodeficiency center. Data were collected on: demographic characteristics; medical and vaccination history with live vaccines; T-CD4+ lymphocyte counts and lymphocyte proliferative responses to antigens and mitogens; adverse reactions; vaccine failure. Results: Twenty three children with DiGeorge syndrome/22q11.2 deletion syndrome were included, 65.2% male, with average age at diagnosis of 11.3 months. Eighteen children (78%) received bacillus Calmette-Guérin vaccine: all with evidence of thymic activity; three presented moderate T-CD4+ lymphopenia and abnormal lymphocyte proliferative responses; one had abnormal lymphocyte proliferative responses for mitogens, four for purified protein derivative and one for tetanus toxoid. Measles, mumps and rubella vaccine was administered to 15 children, three of them with moderate immunosuppression and abnormal lymphocyte proliferative responses. Live attenuated polio vaccine was administered to 4 children without immunosuppression and the rotavirus vaccine to three children, one with moderate immunosuppression. No significant adverse reactions were reported. Discussion: These data are in line with the findings of other international studies. Conclusion: In our sample, live vaccines were well-tolerated, even in children with moderate T-CD4+ lymphopenia and abnormal lymphocyte proliferative responses to antigens/mitogens.

Published

2019

4. Abordaje inmunológico del síndrome por deleción 22q11.2

Author

Rafael Lince, José Luis Franco, Federico Sierra, Claudia M. Trujillo-Vargas, Estefanía Vásquez-Echeverri, Carlos Garcés-Samudio, and Julio C. Orrego-Arango

Subjects

0301 basic medicine, Microbiology (medical), medicine.medical_specialty, Cardiopatía troncoconal, 03 medical and health sciences, Thymic hypoplasia, medicine, Immunodeficiency, Pharmacology (medical), Linfopenia congénita, Aplasia tímica, DiGeorge syndrome, Síndrome de DiGeorge, Congenital heart disease, Thymic Aplasia, Inmunodeficiencia, Gynecology, business.industry, Síndrome por deleción 22q11.2, medicine.disease, 030104 developmental biology, Infectious Diseases, Congenital lymphopenia, Thymic aplasia, 22q11.2 deletion syndrome, Hipoplasia tímica, business

Abstract

ResumenEl síndrome por deleción 22q11.2 (SD22q11) es el síndrome por deleción cromosómica más frecuente en humanos y se caracteriza por la tríada clínica que incluye cardiopatía congénita, hipocalcemia e inmunodeficiencia primaria. El 85-90% de los pacientes tienen microdeleciones en el cromosoma 22q11.2. Tomando como punto cardinal la cardiopatía congénita, se diseñó una estrategia para tamización y diagnóstico de SD22q11 con énfasis en la evaluación inmune. Es imprescindible realizar una historia clínica detallada y, posteriormente, un análisis cuantitativo y funcional de las subpoblaciones de linfocitos en sangre periférica para clasificarlo en SD22q11 completo (

Published

2016

5. Early onset intellectual disability in chromosome 22q11.2 deletion syndrome

Author

Marco Cascella and Maria Rosaria Muzio

Subjects

Male, Pediatrics, medicine.medical_specialty, Velocardiofacial syndrome, Adolescent, Síndrome velocardiofacial, Tetralogía de Fallot, Microdeletion syndrome, Intellectual disability disorders, Deterioro cognitivo, Trastornos de discapacidad intelectual, Cognition, 22q11 Deletion Syndrome, Intellectual Disability, DiGeorge syndrome, Intellectual disability, medicine, Humans, Pediatrics, Perinatology, and Child Health, Age of Onset, Cognitive decline, Síndrome de DiGeorge, 22q11 deletion syndrome, business.industry, Genetic disorder, Síndrome de microdeleción, medicine.disease, Cognitive impairment, Schizophrenia, Pediatrics, Perinatology and Child Health, Tetralogy of Fallot, business, Síndrome de deleción 22q11, Chromosome 22

Abstract

Chromosome 22q11.2 deletion syndrome, or DiGeorge syndrome, or velocardiofacial syndrome, is one of the most common multiple anomaly syndromes in humans. This syndrome is commonly caused by a microdelection from chromosome 22 at band q11.2. Although this genetic disorder may reflect several clinical abnormalities and different degrees of organ commitment, the clinical features that have driven the greatest amount of attention are behavioral and developmental features, because individuals with 22q11.2 deletion syndrome have a 30-fold risk of developing schizophrenia. There are differing opinions about the cognitive development, and commonly a cognitive decline rather than an early onset intellectual disability has been observed. We report a case of 22q11.2 deletion syndrome with both early assessment of mild intellectual disabilities and tetralogy of Fallot as the only physic manifestation.

Published

2015

6. Síndrome de deleção 22q11.2 e cardiopatias congênitas

Author

Rafael Fabiano Machado Rosa, Paulo Ricardo Gazzola Zen, Carla Graziadio, and Giorgio Adriano Paskulin

Subjects

business.industry, human chromosome, pair 22, heart defects, congenital, hibridização in situ fluorescente, cardiopatias congênitas, Pediatrics, Perinatology and Child Health, síndrome de DiGeorge, Medicine, in situ hybridization, fluorescence, cromossomos humanos, par 22, business, DiGeorge syndrome, Humanities

Abstract

OBJETIVO: Revisar as características clínicas, etiológicas e diagnósticas da síndrome de deleção 22q11 e sua associação com as cardiopatias congênitas. FONTES DOS DADOS: Foram pesquisados artigos científicos presentes nos portais Medline, Lilacs e SciELO, utilizando-se descritores específicos como "22q11", "DiGeorge syndrome", "velocardiofacial syndrome", "congenital heart defects" e "cardio-vascular malformations". O período adotado para a revisão foi de 1980 a 2009. SÍNTESE DOS DADOS: As malformações cardíacas são os defeitos congênitos observados mais frequentemente ao nascimento e representam um problema importante de Saúde Pública. Dentre suas principais causas conhecidas destaca-se a síndrome de deleção 22q11, também chamada de síndrome de DiGeorge, síndrome velocardiofacial e CATCH22. Trata-se de uma doença autossômica domi-nante caracterizada por um fenótipo altamente variável, o que dificulta em muito seu reconhecimento clínico. Além disso, a maior parte dos pacientes apresenta uma microdeleção identificada principalmente por técnicas de citogenética molecular, como a hibridização in situ fluorescente, pouco disponíveis em nosso meio. De forma similar a outras síndromes, a síndrome de deleção 22q11 associa-se a certos defeitos cardíacos específicos, no caso os do tipo conotruncal. Apesar disso, não há ainda na literatura um consenso sobre quais os pacientes com car-diopatia congênita que deveriam ser investigados para a síndrome de deleção 22q11. CONCLUSÕES: Cardiologistas e cirurgiões cardíacos, espe-cialmente pediátricos, devem estar cientes das peculiaridades e dos cuidados dispensados à síndrome de deleção 22q11. Os indivíduos com a síndrome apresentam comumente alterações envolvendo vários sistemas, o que pode levar a dificuldades e a complicações durante seu manejo clínico e cirúrgico. OBJECTIVE: To review clinical, etiological and diagnostic characteristics of the 22q11 deletion syndrome and its as-sociation with congenital heart defects. DATA SOURCES: Medline, Lilacs and SciELO databases were searched from 1980 to 2009 using specific descrip-tors as "22q11", "DiGeorge syndrome", "velocardiofacial syndrome", "congenital heart defects" and "cardiovascular malformations". DATA SYNTHESIS: Heart malformations are the most fre-quent congenital defects at birth and represent an important Public Health problem. The 22q11 deletion syndrome, also called DiGeorge syndrome, velocardiofacial syndrome and CATCH22, stands out as one of the main known causes of congenital heart defects. This is an autosomal dominant genetic disease characterized by a highly variable phenotype, which renders its difficult clinical identification. In addition, the majority of the patients present a microdeletion identified mainly by molecular cytogenetic techniques as fluorescent in situ hybridization, which are rarely available in Brazil. Similarly to other syndromes, 22q11 deletion syndrome is associated to some specific heart defects, espe-cially conotruncal. It is still not clear which patients with congenital heart defect should be screened for 22q11 dele-tion syndrome. CONCLUSIONS: Cardiologists and cardiac surgeons, particu-larly the pediatric ones, must be aware about the features and health care related to 22q11 deletion syndrome. Subjects with the syndrome very often present abnormalities of mul-tiple systems, that could result in difficulties and complica-tions during their clinical and surgical course.

Published

2011

7. Síndrome de deleção 22q11.2: compreendendo o CATCH22

Author

Giorgio Adriano Paskulin, Tatiana Roman, Rafael Fabiano Machado Rosa, Carla Graziadio, and Paulo Ricardo Gazzola Zen

Subjects

medicine.medical_specialty, Pediatrics, genetic counseling, business.industry, Data synthesis, MEDLINE, síndrome velocardiofacial, hibridização in situ, Recurrence risk, human chromosomes, cromossomos humanos, velocardiofacial syndrome, Pediatrics, Perinatology and Child Health, Epidemiology, medicine, Etiology, síndrome de DiGeorge, conselhamento genético, Deletion syndrome, in situ hybridization, business, DiGeorge syndrome

Abstract

OBJETIVO:Realizar uma revisão dos aspectos históricos, epidemiológicos, clínicos, etiológicos e laboratoriais da síndrome de deleção 22q11.2, salientando-se a importância e as dificuldades do seu diagnóstico. FONTES DE DADOS: Pesquisa nas bases de dados Medline, Lilacs e SciELO, além da Internet e capítulos de livros em inglês, acerca de publicações feitas entre 1980 e 2008. Para isso, utilizaram-se os descritores "22q11", "DiGeorge", "Velocardiofacial" e "CATCH22". SÍNTESE DOS DADOS: A síndrome de deleção 22q11.2, também conhecida como síndrome de DiGeorge ou velocardiofacial, foi identificada no começo da década de 1990. A microdeleção 22q11.2 é considerada uma das síndromes de microdeleção genética mais frequentes em seres humanos. Caracteriza-se por um espectro fenotípico bastante amplo, com mais de 180 achados clínicos já descritos do ponto de vista físico e comportamental. Contudo, nenhum achado é patognomônico ou mesmo obrigatório. A maioria dos pacientes apresenta uma deleção pequena, detectada somente por técnicas de genética molecular, como a hibridização in situ fluorescente. Apresenta padrão de herança autossômico dominante, ou seja, indivíduos acometidos apresentam um risco de 50% de transmiti-la a seus filhos. CONCLUSÕES: Pacientes com a síndrome de deleção 22q11.2 frequentemente necessitam, ao longo de suas vidas, de um grande número de intervenções médicas e hospitalizações. O diagnóstico precoce é fundamental para a adequada avaliação e manejo clínico dos indivíduos e seus familiares. OBJECTIVE:To review historical, epidemiological, clinical, etiological and laboratorial aspects of the 22q11.2 deletion syndrome, highlighting the importance of the diagnosis and its difficulties. DATA SOURCES: MedLine, Lilacs e SciELO databases, as well as internet and book chapters written in English, were searched for the period of 1980-2008, with the following descriptors "22q11", "DiGeorge", "Velocardiofacial" and "CATCH22". DATA SYNTHESIS: 22q11.2 deletion syndrome, also known as DiGeorge or velocardiofacial syndrome, was identified in the beginning of the 1990 decade. The 22q11.2 microdeletion is one of the most common human genetic microdeletion syndromes. It is characterized by a very broad phenotypic spectrum. More than 180 physical and behavioral clinical findings have already been described. However, none of them is characteristic or essential to diagnosis. The majority of the patients present a small deletion only detected by molecular genetic techniques as the fluorescent in situ hybridization. The deletion segregates in the families with an autosomal dominant pattern of inheritance, so the recurrence risk in the families is 50%. CONCLUSIONS: Individuals with 22q11.2 deletion syndrome have a great possibility to undergo medical interventions and hospitalizations throughout their lives. Early diagnosis is essential for the evaluation and clinical management of the patients and their families.

Published

2009

8. Congenital Heart Disease as a Warning Sign for the Diagnosis of the 22q11.2 Deletion

Author

Leslie Domenici Kulikowski, Magda Carneiro-Sampaio, Roberta Lelis Dutra, Chong Ae Kim, Stephanie Pucci Pegler, Marcília Sierro Grassi, Cristina Miuki Abe Jacob, Antonio Carlos Pastorino, Nana Miura, and Marcelo B. Jatene

Subjects

Pediatrics, medicine.medical_specialty, lcsh:Diseases of the circulatory (Cardiovascular) system, Heart disease, Parathyroid hormone, Short stature, Chromosomes, Hypogammaglobulinemia, Congenital, medicine, Multiplex ligation-dependent probe amplification, Craniofacial, Hipocalcemia, Tetralogy of Fallot, Síndrome de DiGeorge, Heart Defects, biology, Hypocalcemia, business.industry, Cromossomos Humanos, Deleção Cromossômica, Original Articles, medicine.disease, DiGeorge Syndrme, Crromosome Delection, Immunoglobulin M, lcsh:RC666-701, biology.protein, medicine.symptom, Cardiology and Cardiovascular Medicine, business, Cardiopatias Congenitas, Human

Abstract

Background: To alert for the diagnosis of the 22q11.2 deletion syndrome (22q11.2DS) in patients with congenital heart disease (CHD). Objective: To describe the main CHDs, as well as phenotypic, metabolic and immunological findings in a series of 60 patients diagnosed with 22q11.2DS. Methods: The study included 60 patients with 22q11.2DS evaluated between 2007 and 2013 (M:F=1.3, age range 14 days to 20 years and 3 months) at a pediatric reference center for primary immunodeficiencies. The diagnosis was established by detection of the 22q11.2 microdeletion using FISH (n = 18) and/or MLPA (n = 42), in association with clinical and laboratory information. Associated CHDs, progression of phenotypic facial features, hypocalcemia and immunological changes were analyzed. Results: CHDs were detected in 77% of the patients and the most frequent type was tetralogy of Fallot (38.3%). Surgical correction of CHD was performed in 34 patients. Craniofacial dysmorphisms were detected in 41 patients: elongated face (60%) and/or elongated nose (53.3%), narrow palpebral fissure (50%), dysplastic, overfolded ears (48.3%), thin lips (41.6%), elongated fingers (38.3%) and short stature (36.6%). Hypocalcemia was detected in 64.2% and decreased parathyroid hormone (PTH) level in 25.9%. Decrease in total lymphocytes, CD4 and CD8 counts were present in 40%, 53.3% and 33.3%, respectively. Hypogammaglobulinemia was detected in one patient and decreased concentrations of immunoglobulin M (IgM) in two other patients. Conclusion: Suspicion for 22q11.2DS should be raised in all patients with CHD associated with hypocalcemia and/or facial dysmorphisms, considering that many of these changes may evolve with age. The 22q11.2 microdeletion should be confirmed by molecular testing in all patients. Fundamento: Alertar para o diagnóstico da síndrome da deleção 22q11.2 (SD 22q11.2) em pacientes com cardiopatias congênitas. Objetivo: Descrever as principais cardiopatias, alterações fenotípicas, metabólicas e imunológicas em uma série de 60 pacientes com a SD22q11.2. Métodos: Foram incluídos 60 pacientes com SD22q11.2 avaliados entre 2007 e 2013 (M:F = 1,3; idades entre 14 dias a 20 anos e 3 meses) em um centro pediátrico de referência para imunodeficiências primárias. O diagnóstico foi feito pela detecção da microdeleção 22q11.2 através de FISH (n = 18) e/ou MLPA (n = 42), associados a dados clínicos e laboratoriais. Foram analisadas as cardiopatias, aspectos fenotípicos evolutivos da fácies, a hipocalcemia e alterações imunológicas associadas. Resultados: Cardiopatias congênitas ocorreram em 77% dos casos, sendo que a tetralogia de Fallot ocorreu em 38,3%. Correção cirúrgica da cardiopatia foi realizada em 34 pacientes. Os dismorfismos craniofaciais foram detectados em 41 pacientes: face (60%) e/ou nariz alongados (53,3%), fenda palpebral estreita (50%), orelhas displásicas com hiperdobramento (48,3%), lábios finos (41,6%), dedos alongados (38,3%) e baixa estatura (36,6%). Hipocalcemia foi observada em 64,2% com redução do nível de paratormônio (PTH) em 25,9%. Observou-se número reduzido de linfócitos totais, CD4 e CD8 em 40%, 53,3%, e 33,3%, respectivamente. Detectou-se hipogamaglobulinemia em um paciente e redução das concentrações de imunoglobulina M (IgM) em outros dois pacientes. Conclusão: Deve-se suspeitar da SD22q11.2 em todos os portadores de cardiopatia congênita com hipocalcemia e/ou dismorfismos faciais, ressaltando-se que muitas dessas alterações podem ser evolutivas. A microdeleção 22q11.2 deve ser confirmada por testes moleculares em todos os pacientes.

Published

2014

9. Síndrome de Di George

Author

Vicente Martín Gutiérrez, Pilar Casaseca García, Lucía Sierra Santos, and Alfonso García Moreno

Subjects

Pediatrics, medicine.medical_specialty, Síndrome Velocardiofacial, Heart disease, medicine.diagnostic_test, business.industry, General Medicine, Hyperplasia, medicine.disease, Hypoparathyroidism, Inmunidad, DiGeorge syndrome, Immunology, Intellectual disability, medicine, Timo, 22q11 deletion, business, Chromosome 22, Genetic testing, Síndrome de DiGeorge

Abstract

El síndrome de Di George o velocardiofacial ocurre en 1:4000 nacidos vivos y es una rara alteración que en el 90 % de los casos corresponde a una deleción del cromosoma 22 en la porción 22q11. Dicho síndrome puede incluir defectos faciales, cardiopatías congénitas, hipoplasia tímica, hipoparatiroidismo, alteraciones renales, inmunológicas y psiquiátricas. Muchos de estos pacientes pueden llegar a la edad adulta y precisan de atención y seguimiento médico toda su vida.

Published

2014

10. Malformations detected by abdominal ultrasound in children with congenital heart disease

Author

Rosana Cardoso Manique Rosa, Paulo Ricardo Gazzola Zen, Giorgio Adriano Paskulin, Eliete Golendziner, Ceres Andréia Vieira de Oliveira, Marileila Varella-Garcia, Rafael Fabiano Machado Rosa, and José Antônio Monteiro Flores

Subjects

Gynecology, Heart Defects, Congenital, Chromosome Aberrations, medicine.medical_specialty, lcsh:Diseases of the circulatory (Cardiovascular) system, business.industry, Abdominal ultrasound, Ultrassonografia, Recem nascido, Criança, Anormalidades Urogenitais, Cardiopatias Congênitas, lcsh:RC666-701, Urogenital Abnormalities, medicine, DiGeorge Syndrome, Age distribution, Ultrasonography, Cardiology and Cardiovascular Medicine, business, Kidney abnormalities, Child, Síndrome de DiGeorge, Aberrações Cromossômicas

Abstract

FUNDAMENTO: Malformações extracardíacas podem estar presentes em pacientes com cardiopatia congênita (CC), trazendo maior risco de comorbidade e mortalidade. OBJETIVO: Verificar a frequência e os tipos de anormalidades abdominais detectadas em crianças com e sem CC através do ultrassom abdominal (USA), comparar os pacientes quanto a seus achados dismórficos/citogenéticos e realizar uma estimativa do custo-benefício da triagem pelo USA. MÉTODOS: Foi realizado um estudo transversal com controle. Os casos consistiram de pacientes com CC admitidos pela primeira vez em uma unidade de terapia intensiva pediátrica; os controles consistiram de crianças sem CC submetidas ao USA no hospital logo após cada caso. Todos os pacientes com CC foram submetidos ao USA, ao cariótipo de alta resolução e à hibridização in situ fluorescente (FISH) para microdeleção 22q11.2. RESULTADOS: USA identificou anormalidades clinicamente significativas em 12,2% dos casos e em 5,2% dos controles (p = 0,009), com um poder de significância de 76,6%. A maioria das malformações com significado clínico foi de anomalias renais (10,4% nos casos e 4,9% nos controles, p = 0,034). No Brasil, o custo de um exame de USA pelo Sistema Único de Saúde é de 21 dólares. Uma vez que anormalidades clinicamente significativas foram observadas em um a cada 8,2 pacientes com CC, o custo para identificar uma criança afetada foi de 176 dólares. CONCLUSÃO: Pacientes com CC apresentam uma frequência significativa de anomalias detectadas pelo USA, um método diagnóstico barato e não invasivo, com boa sensibilidade. O custo da triagem para esses defeitos é consideravelmente menor que o custo para tratar as complicações do diagnóstico tardio de malformações abdominais, como a doença renal. BACKGROUND: Extracardiac malformations may be present in patients with congenital heart disease (CHD), bringing greater risk of comorbidity and mortality. OBJECTIVE: Verify frequency and types of abdominal abnormalities detected in children with and without CHD through abdominal ultrasound (AUS), compare the patients in relation to their dysmorphic/cytogenetic findings and perform an estimative of the cost-effectiveness of the screening through AUS. METHODS: We conducted a cross-sectional study with a control cohort. The cases consisted of patients with CHD admitted for the first time in a pediatric intensive care unit; the controls consisted of children without CHD who underwent AUS at the hospital shortly thereafter a case. All patients with CHD underwent AUS, high-resolution karyotype and fluorescence in situ hybridization (FISH) for microdeletion 22q11.2. RESULTS: AUS identified clinically significant abnormalities in 12.2% of the cases and 5.2% of controls (p= 0.009), with a power of significance of 76.6%. Most malformations with clinical significance were renal anomalies (10.4% in cases and 4.9% in controls; p= 0.034). In Brazil, the cost of an AUS examination for the Unified Health System is US$ 21. Since clinically significant abnormalities were observed in one in every 8.2 CHD patients, the cost to identify an affected child was calculated as approximately US$ 176. CONCLUSION: Patients with CHD present a significant frequency of abdominal abnormalities detected by AUS, an inexpensive and noninvasive diagnostic method with good sensitivity. The cost of screening for these defects is considerably lower than the cost to treat the complications of late diagnoses of abdominal malformations such as renal disease.

Published

2012

11. Síndrome de deleção 22q11 e cardiopatias congênitas complexas

Author

Dayane Bohn Koshiyama, Patrícia Trevisan, Carlo Benatti Pilla, Marileila Varella-Garcia, Rafael Fabiano Machado Rosa, Paulo Ricardo Gazzola Zen, and Giorgio Adriano Paskulin

Subjects

Gynecology, medicine.medical_specialty, business.industry, congenital, cromossomos humanos par 22, General Medicine, heart defects, congenital, hibridização in situ fluorescente, cardiopatias congênitas, heart defects, medicine, in situ hybridization, fluorescence, chromosomes, human, pair 22, business, DiGeorge syndrome, Síndrome de DiGeorge, cardiopatias congêni tas

Abstract

OBJETIVO: Verificar a frequência da síndrome de deleção 22q11 (SD22q11) entre pacientes portadores de cardiopatia congênita do tipo complexa. MÉTODOS: A amostra foi constituída por uma coorte prospectiva e consecutiva de pacientes com cardiopatia complexa em sua primeira hospitalização em uma unidade de tratamento intensivo cardiológica de um hospital pediátrico. Para cada paciente foi preenchida uma ficha de avaliação, com coleta de dados clínicos, e realizado o cariótipo de alta resolução e técnica de hibridização in situ fluorescente (FISH) com pesquisa de microdeleção 22q11. Os defeitos cardíacos foram classificados por um cardiologista participante do estudo. RESULTADOS: A amostra foi composta de 66 pacientes. Quanto à análise cariotípica, alterações foram observadas em cinco pacientes (7,6%); contudo, nenhum deles apresentava deleção 22q11. A avaliação pela técnica de FISH pôde ser realizada com sucesso em 65 pacientes, sendo que a microdeleção 22q11 foi identificada em dois (3,1%). Dos 66 pacientes com defeitos complexos, 52 eram portadores de malformações do tipo conotruncal, sendo que em 51 a pesquisa para microdeleção 22q11 foi realizada. Os dois pacientes portadores da microdeleção 22q11 fizeram parte deste grupo, representando uma frequência de 3,9%. Eles apresentavam tetralogia de Fallot. CONCLUSÃO: A SD22q11 é uma anormalidade frequente entre pacientes com cardiopatias congênitas complexas e conotruncais. Variações da frequência da SD22q11 entre os estudos parecem estar associadas, principalmente, com a forma adotada para a seleção da amostra e às características da população em análise. OBJECTIVE: Investigate the frequency of 22q11 deletion syndrome among patients with complex congenital heart disease. METHODS: A prospective and consecutive cohort of patients with complex heart defects was evaluated in their first hospitalization at a cardiac intensive care unit of a pediatric hospital. For each patient a protocol of demographic and clinical evaluation was filled. High resolution karyotype and 22q11 microdeletion by fluorescence in situ hybridization was investigated. The heart defects were classified by a cardiologist of the study. RESULTS: The cohort comprised 66 patients. Karyotypic anomalies were observed in 5 patients (7.6%), however none of those was the 22q11 deletion. Evaluation by means of FISH was successful in 65 patients and 22q11 microdeletion was identified in 2 (3.1%). Of the 66 patients with complex defects, 52 were carriers of conotruncal malformations and in 51 the 22q11 microdeletion analysis by FISH was successful. Both 22q11 microdeletion carriers belonged to this group, representing a frequency of 3.9%. They presented tetralogy of Fallot. CONCLUSION: 22q11DS is a frequent abnormality among patients with complex and conotruncal heart defects. Variations of the 22q11DS frequency among studies seem to be mainly associated to criteria for patient selection and specific characteristics of the population in analysis.