期刊文献+
共找到4篇文章
< 1 >
每页显示 20 50 100
Online Social Skills Group Training for Adolescents and Young Adults with 22q11.2 Deletion Syndrome (22q11.2DS)
1
作者 Bronwyn Glaser Stephan Eliez +2 位作者 Hannah Cholemkery Christine M. Freitag Maude Schneider 《Journal of Behavioral and Brain Science》 2018年第3期126-145,共20页
Somatic, cognitive and psychiatric obstacles contribute to social impairment in 22q11.2DS and prevent adequate responses during interactions. We adapted the autism-specific SOSTA-FRA program for use during online grou... Somatic, cognitive and psychiatric obstacles contribute to social impairment in 22q11.2DS and prevent adequate responses during interactions. We adapted the autism-specific SOSTA-FRA program for use during online group sessions with geographically-isolated 22q11DS adolescents or adults. The 12 weekly sessions targeted communication, emotional awareness, and reciprocity. Twenty-two participants were evaluated on behaviour, social responsiveness, and cognition pre- and post-intervention. Parents completed a questionnaire to ascertain whether the intervention met their needs. Parents were satisfied with the format and curriculum contents and reported improved emotional awareness, well-being, and reciprocity post-intervention. Pre-post results suggest large effects on social awareness and small to medium effects on social motivation. Results indicate that online social skills training is feasible and effective for individuals with 22q11.2DS. 展开更多
关键词 GROUP SOCIAL 22q11.2 DELETION syndrome VCFS
下载PDF
免疫性血小板减少症起病的基因诊断22q11.2微缺失综合征:部分型DiGeorge综合征1例并文献复习 被引量:1
2
作者 马静瑶 张蕊 +5 位作者 吴颖 马洁 陈振萍 谷昊 傅玲玲 吴润晖 《血栓与止血学》 2018年第3期409-413,共5页
22q11.2微缺失综合征(22q11.2 deletion syn-drome,22q11.2DS)是由于22号染色体长臂近着丝粒端一处微片段22q11.21-q11.23(大小约3Mb)缺失所导致的先天性多器官发育异常的一组临床症候群,也是人类多种微缺失综合征中最常见... 22q11.2微缺失综合征(22q11.2 deletion syn-drome,22q11.2DS)是由于22号染色体长臂近着丝粒端一处微片段22q11.21-q11.23(大小约3Mb)缺失所导致的先天性多器官发育异常的一组临床症候群,也是人类多种微缺失综合征中最常见的一种。 展开更多
关键词 免疫性血小板减少症 22q11.2微缺失综合征(22q11.2 DS):部分型Di George综合征(DGS) 基因突变
下载PDF
Re-Challenge with Clozapine after Neuroleptic Malignant Syndrome and Seizure in a Patient with Di-George Syndrome: Case Report and Review of Literature
3
作者 Geetha Chandrashekar Ganesh Gopalakrishna +2 位作者 Austin Campbell Katherine Edwards Muaid Ithman 《Open Journal of Psychiatry》 2020年第1期9-14,共6页
Background: Individuals with 22q11.2DS, a genetic subtype of Schizophrenia, respond as well to clozapine as those with other forms of Schizophrenia. It has been reported that serious and rare adverse events like seizu... Background: Individuals with 22q11.2DS, a genetic subtype of Schizophrenia, respond as well to clozapine as those with other forms of Schizophrenia. It has been reported that serious and rare adverse events like seizures, and myocarditis have been associated with clozapine treatment in this population. To the best of our knowledge, the incidence of neuroleptic malignant syndrome (NMS) as an adverse effect of antipsychotic use in patients with this disorder has not yet been reported. Aim: In this article, we discuss a case of clozapine-induced NMS and subsequent re-challenge in a patient with 22q11.2DS-associated schizophrenia. The aim of this study is to accumulate scientific data about rare presentations, and serve as a major educational tool, and highlight the unique challenges faced when using clozapine in a patient with DiGeorge Syndrome. Methods: This is a descriptive case report of a patient encountered in the inpatient unit which includes retrospective review of the patient’s electronic medical record and a literature review of antipsychotic medications-induced NMS. Conclusion: This study demonstrates a successful re-challenge with clozapine after the patient developed NMS and seizures during the initial treatment and also highlights how, in addition to drug level monitoring, considering pharmacogenetic testing early in treatment might help minimize adverse drug reactions in individuals with known genetic disorders such as 22q11.2DS. 展开更多
关键词 CLOZAPINE DIGEORGE syndrome 22q11.2 Deletion syndrome Neuroleptic Malignant syndrome (NMS) SEIZURE Re-Challenge
下载PDF
Use of amniocytes for prenatal diagnosis of 22q11.2 microdeletion syndrome: a feasibility study 被引量:3
4
作者 LIU Tao LIU Qing +5 位作者 WANG Yi-xin YANG Dong XIN Yi FANG Zhen DING Shu-fang YANG Jie-fu 《Chinese Medical Journal》 SCIE CAS CSCD 2010年第4期438-442,共5页
Background A study of prenatal genetic diagnosis for 22q11.2 microdeletion, which has a wide phenotypic spectrum that involves almost all organs, is rarely reported in China. This study aimed to explore the prevalence... Background A study of prenatal genetic diagnosis for 22q11.2 microdeletion, which has a wide phenotypic spectrum that involves almost all organs, is rarely reported in China. This study aimed to explore the prevalence of 22q11.2 microdeletion in congenitally malformed fetuses via the fluorescent in situ hybridization (FISH) technique and to investigate the feasibility of use of amniocytes to diagnose 22q11 .2 microdeletion syndrome prenatally. Methods The study enrolled 23 cases of fetal cardiac malformation, as indicated by ultrasound in Beijing Anzhen Hospital and 14 cases of non-cardiac malformation, as determined by type-B ultrasound in Beijing Anzhen Hospital and other hospitals. Amniotic fluid was obtained by amniocentesis before odinopoeia, and the stillborn fetuses of the induced labor were preceded to autopsy. The amniotic fluid of 20 cesarean deliveries during the same period of time was used as a control. The TUPLE1 gene in the amniotic fluid of malformed and normal fetuses was assessed by the FISH method. Results The prevalence rates of the TUPLE1 gene deletion in the amniotic fluid cells from fetuses with cardiac deformations and fetuses without such malformations were 43.5% and 57.1%, respectively. The deletion of TUPLE1 was significantly associated with fetal malformation. Conclusion Chromosome 22q11.2 microdeletion is one of the major factors leading to fetal congenital malformations, and prenatal FISH screening for 22q11 .2 microdeletion syndrome is technically feasible using amniocytes. 展开更多
关键词 amniocyte chromosome 22q11.2 microdeletion fetal malformation
原文传递
上一页 1 下一页 到第
使用帮助 返回顶部