Fine mapping of Xq11.1‐q21.33 and mutation screening of RPS6KA6, ZNF711, ACSL4, DLG3, and IL1RAPL2 for autism spectrum disorders (ASD)

自闭症 遗传学 遗传连锁 生物 候选基因 拷贝数变化 X染色体 基因 基因组 心理学 发展心理学
作者
Katri Kantojärvi,Ilona Kotala,Karola Rehnström,Tero Ylisaukko‐oja,Raija Vanhala,Taina Nieminen von Wendt,Lennart von Wendt,Irma Järvelä
出处
期刊:Autism Research [Wiley]
卷期号:4 (3): 228-233 被引量:21
标识
DOI:10.1002/aur.187
摘要

Abstract About 80% of cases with autism express intellectual disability. Both in autism and in mental retardation without autism the majority of the cases are males, suggesting a X‐chromosomal effect. In fact, some molecular evidence has been obtained for a common genetic background for autism spectrum disorders (ASD) and X‐linked mental retardation (XLMR). In several genome‐wide scans (GWS), evidence for linkage at X‐chromosome has been reported including the GWS of Finnish ASD families with the highest multipoint lod score (MLS) of 2.75 obtained close to DXS7132 at Xq11.1. To further dissect the relationship between autism and genes implicated in XLMR, we have fine‐mapped Xq11.1‐q21.33 and analyzed five candidate genes in the region. We refined the region using 26 microsatellite markers and linkage analysis in 99 Finnish families with ASD. The most significant evidence for linkage was observed at DXS1225 on Xq21.1 with a nonparametric multipoint NPL all value of 3.43 ( P = 0.0004). We sequenced the coding regions and splice sites of RPS6KA6 and ZNF711 residing at the peak region in 42 male patients from families contributing to the linkage. We also analyzed ACSL4 and DLG3 , which have previously been known to cause XLMR and IL1RAPL2 , a homologous gene for IL1RAPL1 that is mutated in autism and XLMR. A total of six novel and 11 known single nucleotide polymorphisms were identified. Further studies are warranted to analyze the candidate genes at Xq11.1‐q21.33. Autism Res 2011,4:228–233 . © 2011 International Society for Autism Research, Wiley Periodicals, Inc.
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