Biochemical screening and PTEN mutation analysis in individuals with autism spectrum disorders and macrocephaly

被引:0
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作者
Judith A Hobert
Rebecca Embacher
Jessica L Mester
Thomas W Frazier
Charis Eng
机构
[1] Genomic Medicine Institute,Department of Genetics and Genome Sciences
[2] Lerner Research Institute,undefined
[3] Cleveland Clinic,undefined
[4] Center for Autism,undefined
[5] Pediatrics Institute,undefined
[6] Cleveland Clinic,undefined
[7] Taussig Cancer Institute,undefined
[8] Cleveland Clinic,undefined
[9] Case Western Reserve University School of Medicine,undefined
[10] CASE Comprehensive Cancer Center,undefined
[11] Case Western Reserve University School of Medicine,undefined
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关键词
autism spectrum disorder; macrocephaly; Cowden syndrome;
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学科分类号
摘要
Unlike some other childhood neurodevelopmental disorders, no diagnostic biochemical marker has been identified in all individuals with an autism spectrum disorder (ASD). This deficit likely results from genetic heterogeneity among the population. Therefore, we evaluated a subset of individuals with ASDs, specifically, individuals with or without macrocephaly in the presence or absence of PTEN mutations. We sought to determine if amino or organic acid markers could be used to identify individuals with ASDs with or without macrocephaly in the presence or absence of PTEN mutations, and to establish the degree of macrocephaly in individuals with ASDs and PTEN mutation. Urine, blood and occipital–frontal circumference (OFC) measurements were collected from 69 individuals meeting DSM-IV-TR criteria. Urine and plasma samples were subjected to amino and organic acid analyses. PTEN was Sanger-sequenced from germline genomic DNA. Germline PTEN mutations were identified in 27% (6/22) of the macrocephalic ASD population. All six PTEN mutation-positive individuals were macrocephalic with average OFC+4.35 standard deviations (SDs) above the mean. No common biochemical abnormalities were identified in macrocephalic ASD individuals with or without PTEN mutations. In contrast, among the collective ASD population, elevation of urine aspartic acid (87%; 54/62), plasma taurine (69%; 46/67) and reduction of plasma cystine (72%; 46/64) were observed. PTEN sequencing should be carried out for all individuals with ASDs and macrocephaly with OFC ≥2SDs above the mean. A proportion of individuals with ASDs may have an underlying disorder in sulfur amino acid metabolism.
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页码:273 / 276
页数:3
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