Does epilepsy in multiplex autism pedigrees define a different subgroup in terms of clinical characteristics and genetic risk?

Claire Amiet; Isabelle Gourfinkel-An; Claudine Laurent; Nicolas Bodeau; Bérengère Génin; Eric Leguern; Sylvie Tordjman; David Cohen

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Does epilepsy in multiplex autism pedigrees define a different subgroup in terms of clinical characteristics and genetic risk?

机译：多重自闭症谱系中的癫痫是否在临床特征和遗传风险方面定义了不同的亚组？

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Background Autism spectrum disorders (ASD) and epilepsy frequently occur together. Prevalence rates are variable, and have been attributed to age, gender, comorbidity, subtype of pervasive developmental disorder (PDD) and risk factors. Recent studies have suggested disparate clinical and genetic settings depending on simplex or multiplex autism. The aim of this study was to assess: 1) the prevalence of epilepsy in multiplex autism and its association with genetic and non-genetic risk factors of major effect, intellectual disability and gender; and 2) whether autism and epilepsy cosegregate within multiplex autism families. Methods We extracted from the Autism Genetic Resource Exchange (AGRE) database (n?=?3,818 children from 1,264 families) all families with relevant medical data (n?=?664 children from 290 families). The sample included 478 children with ASD and 186 siblings without ASD. We analyzed the following variables: seizures, genetic and non-genetic risk factors, gender, and cognitive functioning as assessed by Raven’s Colored Progressive Matrices (RCPM) and Vineland Adaptive Behavior Scales (VABS). Results The prevalence of epilepsy was 12.8% in cases with ASD and 2.2% in siblings without ASD (P <10-5). With each RCPM or VABS measure, the risk of epilepsy in multiplex autism was significantly associated with intellectual disability, but not with gender. Identified risk factors (genetic or non-genetic) of autism tended to be significantly associated with epilepsy (P?=?0.052). When children with prematurity, pre- or perinatal insult, or cerebral palsy were excluded, a genetic risk factor was reported for 6/59 (10.2%) of children with epilepsy and 12/395 (3.0%) of children without epilepsy (P?=?0.002). Finally, using a permutation test, there was significant evidence that the epilepsy phenotype co-segregated within families (P <10-4). Conclusions Epilepsy in multiplex autism may define a different subgroup in terms of clinical characteristics and genetic risk.

机译：背景自闭症谱系障碍（ASD）和癫痫病经常并发。患病率是可变的，并已归因于年龄，性别，合并症，普遍性发育障碍（PDD）的亚型和危险因素。最近的研究表明，取决于单纯性或多重自闭症的临床和遗传背景不同。这项研究的目的是评估：1）癫痫在多发性自闭症中的流行及其与主要影响，智力残疾和性别的遗传和非遗传危险因素的关联; 2）自闭症和癫痫是否在多重自闭症家族中共分离。方法我们从自闭症遗传资源交换（AGRE）数据库（n = 3,818名来自1,264个家庭的儿童）中提取所有具有相关医学数据的家庭（n == 664名来自290个家庭的儿童）。样本包括478名患有ASD的儿童和186名没有ASD的兄弟姐妹。我们分析了以下变量：癫痫发作，遗传和非遗传危险因素，性别和认知功能，方法是通过Raven的有色进步矩阵（RCPM）和葡萄园适应行为量表（VABS）进行评估。结果ASD患儿的癫痫患病率为12.8％，而无ASD的同胞患病的癫痫患病率为2.2％（P <10-5）。通过每项RCPM或VABS量度，多元自闭症中癫痫的风险与智力残疾显着相关，但与性别无关。确定的自闭症危险因素（遗传性或非遗传性）往往与癫痫病有显着相关性（P = 0.052）。当排除早产儿，产前或围产期侮辱或脑瘫患儿时，有遗传危险因素的报告为癫痫患儿占6/59（10.2％），无癫痫患儿占12/395（3.0％）（P？ =？0.002）。最后，使用排列检验，有大量证据表明癫痫表型在家庭内部共隔离（P <10-4）。结论多元性自闭症的癫痫病在临床特征和遗传风险方面可能定义了不同的亚组。

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《Molecular Autism》 |2013年第1期|共页
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Claire Amiet; Isabelle Gourfinkel-An; Claudine Laurent; Nicolas Bodeau; Bérengère Génin; Eric Leguern; Sylvie Tordjman; David Cohen;
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5. Identifying biological pathways implicated in defined subgroups of phenotypic expression for autism spectrum disorders & evaluating small molecule effects on expression of ASMT [D] . Veatch, Olivia Jean 2013

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6. Does epilepsy in multiplex autism pedigrees define a different subgroup in terms of clinical characteristics and genetic risk? [O] . Claire Amiet, Isabelle Gourfinkel-An, Claudine Laurent, 2013

机译：多重自闭症谱系中的癫痫是否在临床特征和遗传风险方面定义了不同的亚组？
7. Does epilepsy in multiplex autism pedigrees define a different subgroup in terms of clinical characteristics and genetic risk? [O] . Amiet, Claire, Gourfinkel-An, Isabelle, Laurent, Claudine, 2013

机译：多重自闭症谱系中的癫痫是否在临床特征和遗传风险方面定义了不同的亚组？

Does epilepsy in multiplex autism pedigrees define a different subgroup in terms of clinical characteristics and genetic risk?

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