Human Gene Module / Chromosome 10 / PTEN

PTENphosphatase and tensin homolog (mutated in multiple advanced cancers 1)

SFARI Gene Score
1S
High Confidence, Syndromic Criteria 1.1, Syndromic
Autism Reports / Total Reports
48 / 108
Rare Variants / Common Variants
178 / 0
EAGLE Score
63.15
Strong Learn More
Aliases
PTEN, BZS,  MHAM,  TEP1,  MMAC1,  PTEN1,  MGC11227
Associated Syndromes
Cowden syndrome, Macrocephaly/autism syndrome, PTEN hamartoma tumor syndrome, Cowden syndrome 1, PTEN hamartoma tumor syndrome (PHTS), Cowden syndrome, ASD, Cowden syndrome 1, ASD, DD
Chromosome Band
10q23.31
Associated Disorders
DD/NDD, ADHD, ID, EPS, ASD
Genetic Category
Rare Single Gene Mutation, Syndromic, Functional
Relevance to Autism

Recurrent mutations in the PTEN gene have been identified in multiple individuals with ASD as described below. Deleterious variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR 0.05, meaning that this gene had a 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). A two-stage analysis of rare de novo and inherited coding variants in 42,607 ASD cases, including 35,130 new cases from the SPARK cohort, in Zhou et al., 2022 identified PTEN as a gene reaching exome-wide significance (P < 2.5E-06). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

Molecular Function

The protein encoded this gene is a phosphatidylinositol-3,4,5-trisphosphate 3-phosphatase. It contains a tensin like domain as well as a catalytic domain similar to that of the dual specificity protein tyrosine phosphatases.

SFARI Genomic Platforms
Reports related to PTEN (108 Reports)
# Type Title Author, Year Autism Report Associated Disorders
1 Primary PTEN mutation in a family with Cowden syndrome and autism Goffin A , et al. (2001) No ASD
2 Positive Association Subset of individuals with autism spectrum disorders and extreme macrocephaly associated with germline PTEN tumour suppressor gene mutations Butler MG , et al. (2005) Yes ASD, macrocephaly
3 Support - Valiente M , et al. (2005) No -
4 Recent Recommendation Electrical signals control wound healing through phosphatidylinositol-3-OH kinase-gamma and PTEN Zhao M , et al. (2006) No -
5 Recent Recommendation Free fatty acids inhibit insulin signaling-stimulated endothelial nitric oxide synthase activation through upregulating PTEN or inhibiting Akt kinase Wang XL , et al. (2006) No -
6 Support Mutation screening of the PTEN gene in patients with autism spectrum disorders and macrocephaly Buxbaum JD , et al. (2007) Yes -
7 Support Novel PTEN mutations in neurodevelopmental disorders and macrocephaly Orrico A , et al. (2008) Yes DD, ID
8 Support The prevalence of PTEN mutations in a clinical pediatric cohort with autism spectrum disorders, developmental delay, and macrocephaly Varga EA , et al. (2009) Yes -
9 Support Confirmation study of PTEN mutations among individuals with autism or developmental delays/mental retardation and macrocephaly McBride KL , et al. (2010) Yes -
10 Recent Recommendation PTEN is recruited to the postsynaptic terminal for NMDA receptor-dependent long-term depression Jurado S , et al. (2010) No -
11 Support A mutant form of PTEN linked to autism Redfern RE , et al. (2010) No -
12 Support Autistic spectrum disorder in a 9-year-old girl with macrocephaly Stein MT , et al. (2010) Yes -
13 Support Oligogenic heterozygosity in individuals with high-functioning autism spectrum disorders Schaaf CP , et al. (2011) Yes -
14 Support Sporadic autism exomes reveal a highly interconnected protein network of de novo mutations O'Roak BJ , et al. (2012) Yes -
15 Support Novel PTEN germline mutation in a family with mild phenotype: difficulties in genetic counseling Busa T , et al. (2012) No ID
16 Support Multiplex targeted sequencing identifies recurrently mutated genes in autism spectrum disorders O'Roak BJ , et al. (2012) Yes -
17 Support Biochemical screening and PTEN mutation analysis in individuals with autism spectrum disorders and macrocephaly Hobert JA , et al. (2013) Yes DD, epilepsy
18 Recent Recommendation A secreted PTEN phosphatase that enters cells to alter signaling and survival Hopkins BD , et al. (2013) No -
19 Positive Association De novo mutations in epileptic encephalopathies Epi4K Consortium , et al. (2013) No IS, LGS, DD, ID, ASD, ADHD
20 Recent Recommendation PTEN knockdown alters dendritic spine/protrusion morphology, not density Haws ME , et al. (2013) No -
21 Recent Recommendation Characteristic brain magnetic resonance imaging pattern in patients with macrocephaly and PTEN mutations Vanderver A , et al. (2014) No -
22 Recent Recommendation Loss of mTOR repressors Tsc1 or Pten has divergent effects on excitatory and inhibitory synaptic transmission in single hippocampal neuron cultures Weston MC , et al. (2014) No -
23 Support Autism-epilepsy phenotype with macrocephaly suggests PTEN, but not GLIALCAM, genetic screening Marchese M , et al. (2014) Yes ID, epilepsy
24 Recent Recommendation PTEN interacts with histone H1 and controls chromatin condensation Chen ZH , et al. (2014) No -
25 Recent Recommendation Molecular and phenotypic abnormalities in individuals with germline heterozygous PTEN mutations and autism Frazier TW , et al. (2014) No -
26 Recent Recommendation Synaptic, transcriptional and chromatin genes disrupted in autism De Rubeis S , et al. (2014) Yes -
27 Support Recurrent de novo mutations implicate novel genes underlying simplex autism risk O'Roak BJ , et al. (2014) Yes -
28 Recent Recommendation Functionally distinct groups of inherited PTEN mutations in autism and tumour syndromes Spinelli L , et al. (2014) No -
29 Recent Recommendation Conformational stability and catalytic activity of PTEN variants linked to cancers and autism spectrum disorders Johnston SB and Raines RT (2015) No -
30 Recent Recommendation Neural transcriptome of constitutional Pten dysfunction in mice and its relevance to human idiopathic autism spectrum disorder Tilot AK , et al. (2015) No -
31 Recent Recommendation The parvalbumin/somatostatin ratio is increased in Pten mutant mice and by human PTEN ASD alleles Vogt D , et al. (2015) No -
32 Support Excess of rare, inherited truncating mutations in autism Krumm N , et al. (2015) Yes -
33 Support Integrated analysis of whole-exome sequencing and transcriptome profiling in males with autism spectrum disorders Codina-Sol M , et al. (2015) Yes -
34 Support Molecular Diagnostic Yield of Chromosomal Microarray Analysis and Whole-Exome Sequencing in Children With Autism Spectrum Disorder Tammimies K , et al. (2015) No -
35 Recent Recommendation Low load for disruptive mutations in autism genes and their biased transmission Iossifov I , et al. (2015) Yes -
36 Support A recessive form of extreme macrocephaly and mild intellectual disability complements the spectrum of PTEN hamartoma tumour syndrome Schwerd T , et al. (2015) No -
37 Recent Recommendation Autistic-Like Traits and Cerebellar Dysfunction in Purkinje Cell PTEN Knock-Out Mice Cupolillo D , et al. (2015) No -
38 Support Cytoplasm-predominant Pten associates with increased region-specific brain tyrosine hydroxylase and dopamine D2 receptors in mouse model with autistic traits He X , et al. (2015) No -
39 Support Targeted DNA Sequencing from Autism Spectrum Disorder Brains Implicates Multiple Genetic Mechanisms D'Gama AM , et al. (2015) Yes -
40 Recent Recommendation A Retroviral CRISPR-Cas9 System for Cellular Autism-Associated Phenotype Discovery in Developing Neurons Williams MR , et al. (2016) No -
41 Support Altered proliferation and networks in neural cells derived from idiopathic autistic individuals Marchetto MC , et al. (2016) Yes -
42 Support A combination of genetic and biochemical analyses for the diagnosis of PI3K-AKT-mTOR pathway-associated megalencephaly Negishi Y , et al. (2017) No -
43 Support Prevalence of four Mendelian disorders associated with autism in 2392 affected families Saskin A , et al. (2017) Yes -
44 Support Whole genome sequencing resource identifies 18 new candidate genes for autism spectrum disorder C Yuen RK et al. (2017) Yes -
45 Support PTEN Loss Increases the Connectivity of Fast Synaptic Motifs and Functional Connectivity in a Developing Hippocampal Network Barrows CM , et al. (2017) No -
46 Support Improved diagnostic yield compared with targeted gene sequencing panels suggests a role for whole-genome sequencing as a first-tier genetic test Lionel AC , et al. (2017) No -
47 Support Contribution of rare inherited and de novo variants in 2,871 congenital heart disease probands Jin SC , et al. (2017) No Neurodevelopmental disorders (NDD)
48 Support Identification of mutations in the PI3K-AKT-mTOR signalling pathway in patients with macrocephaly and developmental delay and/or autism Yeung KS , et al. (2018) No ASD
49 Recent Recommendation Nuclear Excluded Autism-Associated Phosphatase and Tensin Homolog Mutations Dysregulate Neuronal Growth Fricano-Kugler CJ , et al. (2018) No -
50 Support Identification of a PTEN mutation with reduced protein stability, phosphatase activity, and nuclear localization in Hong Kong patients with autistic features, neurodevelopmental delays, and macrocephaly Wong CW , et al. (2018) No ASD or autistic features, DD, macrocephaly
51 Support A family with PTEN mutations with malignancy and an unusually high number of offspring with autism spectrum disorder: a case report Gruhl SL , et al. (2018) No ASD, macrocephaly
52 Support Clinical spectrum of PTEN mutation in pediatric patients. A bicenter experience Ciaccio C , et al. (2018) No DD, ASD
53 Support Genetic Diagnostic Evaluation of Trio-Based Whole Exome Sequencing Among Children With Diagnosed or Suspected Autism Spectrum Disorder Du X , et al. (2018) No Autistic features
54 Support Targeted resequencing of 358 candidate genes for autism spectrum disorder in a Chinese cohort reveals diagnostic potential and genotype-phenotype correlations Zhou WZ , et al. (2019) Yes -
55 Support Lessons Learned from Large-Scale, First-Tier Clinical Exome Sequencing in a Highly Consanguineous Population Monies D , et al. (2019) No ASD
56 Support A novel missense PTEN mutation identified in a patient with macrocephaly and developmental delay Ueno Y , et al. (2019) No Macrocephaly
57 Support Characterization of intellectual disability and autism comorbidity through gene panel sequencing Aspromonte MC , et al. (2019) Yes -
58 Support Autism-associated missense genetic variants impact locomotion and neurodevelopment in Caenorhabditis elegans Wong WR , et al. (2019) Yes -
59 Support Inherited and De Novo Genetic Risk for Autism Impacts Shared Networks Ruzzo EK , et al. (2019) Yes -
60 Support Phenotype-to-genotype approach reveals head-circumference-associated genes in an autism spectrum disorder cohort Wu H , et al. (2019) Yes Macrocephaly
61 Support Large-Scale Exome Sequencing Study Implicates Both Developmental and Functional Changes in the Neurobiology of Autism Satterstrom FK et al. (2020) Yes -
62 Support Next-Generation Sequencing in Korean Children With Autism Spectrum Disorder and Comorbid Epilepsy Lee J et al. (2020) Yes -
63 Support Polymicrogyria is Associated With Pathogenic Variants in PTEN Shao DD et al. (2020) No -
64 Support - Abe-Hatano C et al. (2021) No -
65 Support - Kaymakcalan H et al. (2021) Yes ADHD, ID
66 Support - Chai AP et al. (2021) Yes -
67 Support - Dhaliwal N et al. (2021) No -
68 Support - Cummings K et al. (2022) No ASD
69 Support - Getz SA et al. (2022) No -
70 Support - Clipperton-Allen AE et al. (2022) No -
71 Support - Woodbury-Smith M et al. (2022) Yes -
72 Support - Yehia L et al. (2022) No ASD, DD
73 Support - Verberne EA et al. (2022) No -
74 Support - Ledderose JMT et al. (2022) No -
75 Support - Hu C et al. (2022) Yes -
76 Support - Levchenko O et al. (2022) No -
77 Support - Zhou X et al. (2022) Yes -
78 Support - Hendricks LAJ et al. (2022) No DD
79 Support - Ermakova G et al. (2022) Yes -
80 Support - Zhou X et al. (2022) Yes -
81 Support - Busch RM et al. (2023) No -
82 Support - Kagan M et al. (2023) Yes -
83 Support - Yuan B et al. (2023) Yes -
84 Recent Recommendation - Pintacuda G et al. (2023) Yes -
85 Support - Spataro N et al. (2023) No Autistic features
86 Support - Hu C et al. (2023) Yes -
87 Support - Zhang Y et al. (2023) Yes DD, ID
88 Recent Recommendation - Fu S et al. (2023) Yes -
89 Support - Pigoni M et al. (2023) Yes -
90 Support - Wang J et al. (2023) Yes -
91 Support - Balasar et al. (2023) No -
92 Support - Sanchis-Juan A et al. (2023) No -
93 Support - Masahiro Hitomi et al. (2023) No ASD
94 Recent Recommendation - Shin Chung Kang et al. () Yes -
95 Support - Erica Rosina et al. (2024) No -
96 Support - Lena H Nguyen et al. (2024) No -
97 Support - Tamam Khalaf et al. (2024) No -
98 Support - Andrew Dhawan et al. (2024) No ASD, epilepsy/seizures
99 Support - Gemma Molinaro et al. (2024) Yes Epilepsy/seizures
100 Support - Kakha Bregvadze et al. (2024) Yes -
101 Support - Navroop K Dhaliwal et al. (2024) No -
102 Support - Ruohao Wu et al. (2024) Yes -
103 Support - Axel Schmidt et al. (2024) No -
104 Support - Katilynne Croom et al. (2024) Yes -
105 Support - Karen Lob et al. () Yes DD
106 Highly Cited PTEN, a putative protein tyrosine phosphatase gene mutated in human brain, breast, and prostate cancer Li J , et al. (1997) No -
107 Highly Cited The tumor suppressor, PTEN/MMAC1, dephosphorylates the lipid second messenger, phosphatidylinositol 3,4,5-trisphosphate Maehama T and Dixon JE (1998) No -
108 Highly Cited Negative regulation of PKB/Akt-dependent cell survival by the tumor suppressor PTEN Stambolic V , et al. (1998) No -
Rare Variants   (178)
Status Allele Change Residue Change Variant Type Inheritance Pattern Parental Transmission Family Type PubMed ID Author, Year
- - copy_number_loss Unknown - - 39136901 Karen Lob et al. ()
C>G - intron_variant De novo - - 19265751 Varga EA , et al. (2009)
- - copy_number_loss Unknown - Unknown 32959437 Shao DD et al. (2020)
G>A - splice_site_variant Unknown - - 19265751 Varga EA , et al. (2009)
c.-903G>A - 5_prime_UTR_variant - - - 17427195 Buxbaum JD , et al. (2007)
- - copy_number_loss Unknown - Simplex 21624971 Schaaf CP , et al. (2011)
c.-1088C>T - 5_prime_UTR_variant - - - 17427195 Buxbaum JD , et al. (2007)
c.697C>T p.Arg233Ter stop_gained Unknown - - 35741772 Hu C et al. (2022)
c.249C>A p.Cys83Ter stop_gained Unknown - - 32477112 Lee J et al. (2020)
c.-132C>T - stop_gained Unknown - Unknown 32959437 Shao DD et al. (2020)
c.259C>T p.Gln87Ter stop_gained De novo - - 35982159 Zhou X et al. (2022)
c.165-2A>G - splice_site_variant De novo - - 35982159 Zhou X et al. (2022)
c.253+1G>A - splice_site_variant De novo - - 35982159 Zhou X et al. (2022)
c.87T>G p.Tyr29Ter stop_gained De novo - - 28991257 Jin SC , et al. (2017)
c.388C>T p.Gln130Ter stop_gained De novo - - 35982159 Zhou X et al. (2022)
c.388C>T p.Arg130Ter stop_gained De novo - - 36881370 Yuan B et al. (2023)
T>C - intron_variant Familial Maternal - 17427195 Buxbaum JD , et al. (2007)
c.23T>A p.Ile8Asn missense_variant De novo - - 35982159 Zhou X et al. (2022)
c.-478del - frameshift_variant Unknown - - 24580998 Marchese M , et al. (2014)
c.1003C>T p.Arg335Ter stop_gained De novo - - 29608813 Wong CW , et al. (2018)
c.634+2T>G - splice_site_variant De novo - - 30528446 Ciaccio C , et al. (2018)
- - 2KB_upstream_variant Familial Maternal - 30528446 Ciaccio C , et al. (2018)
c.734A>C p.Gln245Pro missense_variant Unknown - - 39136901 Karen Lob et al. ()
c.149T>C p.Ile50Thr missense_variant De novo - - 35982159 Zhou X et al. (2022)
c.1003C>T p.Arg335Ter stop_gained De novo - - 20814261 Stein MT , et al. (2010)
c.697C>T p.Arg233Ter stop_gained De novo - - 30528446 Ciaccio C , et al. (2018)
c.697C>T p.Arg233Ter stop_gained Unknown - - 30528446 Ciaccio C , et al. (2018)
c.-479_-477del - inframe_deletion Unknown - - 30528446 Ciaccio C , et al. (2018)
c.-835C>T - 5_prime_UTR_variant Unknown - - 38438125 Tamam Khalaf et al. (2024)
c.*10del - 3_prime_UTR_variant Unknown - - 34268892 Kaymakcalan H et al. (2021)
c.403A>C p.Ile135Leu missense_variant De novo - - 35982159 Zhou X et al. (2022)
c.424C>T p.Arg142Trp missense_variant De novo - - 35982159 Zhou X et al. (2022)
c.479C>T p.Pro160Leu missense_variant De novo - - 35982159 Zhou X et al. (2022)
c.514A>G p.Arg172Gly missense_variant De novo - - 35982159 Zhou X et al. (2022)
c.626G>T p.Gly209Val missense_variant De novo - - 35982159 Zhou X et al. (2022)
c.820T>G p.Trp274Gly missense_variant De novo - - 35982159 Zhou X et al. (2022)
c.1003C>T p.Arg335Ter stop_gained De novo - - 30528446 Ciaccio C , et al. (2018)
c.493-2A>G - splice_site_variant De novo - Simplex 35982159 Zhou X et al. (2022)
c.27dup p.Ser10Ter frameshift_variant De novo - - 37035742 Zhang Y et al. (2023)
c.77C>T p.Thr26Ile missense_variant De novo - - 36980980 Spataro N et al. (2023)
c.1003C>T p.Arg335Ter stop_gained Unknown - - 35253369 Verberne EA et al. (2022)
c.164+1G>A - splice_site_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.209+5G>A - splice_site_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.303T>C p.Ile101Thr missense_variant De novo - - 29608813 Wong CW , et al. (2018)
c.204A>G p.Tyr68Cys missense_variant De novo - - 29296277 Yeung KS , et al. (2018)
c.102C>T p.Ala34Val missense_variant Unknown - - 31130284 Monies D , et al. (2019)
c.44G>T p.Arg15Ile missense_variant De novo - - 28771251 Lionel AC , et al. (2017)
c.75G>T p.Leu25Phe missense_variant Unknown - - 30528446 Ciaccio C , et al. (2018)
c.7_9del p.Ala3del inframe_deletion De novo - - 30528446 Ciaccio C , et al. (2018)
c.1008C>G p.Tyr336Ter stop_gained Familial Maternal - 37007974 Hu C et al. (2023)
c.388C>T p.Gln130Ter stop_gained Unknown - Unknown 32959437 Shao DD et al. (2020)
c.686C>A p.Ser229Ter stop_gained Unknown - Unknown 32959437 Shao DD et al. (2020)
c.1027-1G>A - splice_site_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.353A>C p.His118Pro missense_variant De novo - - 18759867 Orrico A , et al. (2008)
c.527A>G p.Tyr176Cys missense_variant De novo - - 18759867 Orrico A , et al. (2008)
c.827A>G p.Asn276Ser missense_variant De novo - - 18759867 Orrico A , et al. (2008)
c.605C>T p.Thr202Ile missense_variant De novo - - 19265751 Varga EA , et al. (2009)
c.315G>T p.Cys105Phe missense_variant De novo - - 29296277 Yeung KS , et al. (2018)
c.510G>C p.Ser170Thr missense_variant De novo - - 29296277 Yeung KS , et al. (2018)
c.-115dup - frameshift_variant De novo - Simplex 23160955 O'Roak BJ , et al. (2012)
c.1027-2A>G - splice_site_variant De novo - Multiplex 35982159 Zhou X et al. (2022)
c.302T>C p.Ile101Thr missense_variant De novo - - 30528446 Ciaccio C , et al. (2018)
c.389G>C p.Arg130Pro missense_variant De novo - - 30528446 Ciaccio C , et al. (2018)
c.801G>T p.Lys267Asn missense_variant De novo - - 30528446 Ciaccio C , et al. (2018)
c.388C>T p.Arg130Ter stop_gained De novo - - 38585419 Kakha Bregvadze et al. (2024)
c.97A>G p.Asn33Asp missense_variant De novo - Simplex 35982159 Zhou X et al. (2022)
c.80-1G>A - splice_site_variant Familial Maternal - 28250423 Saskin A , et al. (2017)
c.445C>T p.Gln149Ter stop_gained De novo - Simplex 28263302 C Yuen RK et al. (2017)
c.195C>A p.Cys65Ter stop_gained Unknown - Unknown 26637798 D'Gama AM , et al. (2015)
c.209+5G>A - splice_site_variant Unknown - Unknown 23695273 Hobert JA , et al. (2013)
c.976G>A p.Asp326Asn missense_variant De novo - - 17427195 Buxbaum JD , et al. (2007)
c.278A>G p.His93Arg missense_variant Unknown - - 38438125 Tamam Khalaf et al. (2024)
c.714C>A p.Tyr238Ter stop_gained Unknown - - 35205252 Woodbury-Smith M et al. (2022)
c.737C>T p.Pro246Leu missense_variant De novo - Simplex 30555518 Du X , et al. (2018)
c.810T>A p.Met270Lys missense_variant De novo - Simplex 31674007 Wu H , et al. (2019)
c.220A>G p.Arg74Gly missense_variant De novo - Simplex 35982159 Zhou X et al. (2022)
A>G - splice_site_variant Familial Paternal Simplex 19265751 Varga EA , et al. (2009)
c.494G>T p.Gly165Val missense_variant De novo - - 26325558 Tammimies K , et al. (2015)
c.370T>A p.Cys124Ser missense_variant De novo - - 39039281 Axel Schmidt et al. (2024)
c.253+1dup - frameshift_variant De novo - Simplex 33624935 Abe-Hatano C et al. (2021)
c.235G>A p.Ala79Thr missense_variant Unknown - - 34268892 Kaymakcalan H et al. (2021)
c.302T>C p.Ile101Thr missense_variant De novo - Simplex 35982159 Zhou X et al. (2022)
c.320A>T p.Lys107Met missense_variant De novo - Simplex 35982159 Zhou X et al. (2022)
c.723T>G p.Phe241Leu missense_variant De novo - Simplex 35982159 Zhou X et al. (2022)
c.466G>A p.Gly156Arg missense_variant De novo - Simplex 37393044 Wang J et al. (2023)
c.518G>T p.Arg173Leu missense_variant De novo - Simplex 37393044 Wang J et al. (2023)
c.534T>G p.Tyr178Ter stop_gained Familial Maternal - 11496368 Goffin A , et al. (2001)
c.1003C>T p.Arg335Ter stop_gained Unknown - Unknown 23695273 Hobert JA , et al. (2013)
c.388C>T p.Gln130Ter stop_gained Unknown - Unknown 35887114 Levchenko O et al. (2022)
- - 5_prime_UTR_variant Familial Maternal Multiplex 17427195 Buxbaum JD , et al. (2007)
c.493-1G>A - splice_site_variant De novo - Simplex 25363760 De Rubeis S , et al. (2014)
c.403A>C p.Ile135Leu missense_variant Unknown - - 27378147 Marchetto MC , et al. (2016)
c.239-21G>C - inframe_insertion De novo - Simplex 25969726 Codina-Sol M , et al. (2015)
c.19G>T p.Glu7Ter stop_gained De novo - Simplex 31981491 Satterstrom FK et al. (2020)
c.960T>C p.Leu320Ser missense_variant De novo - Simplex 31149344 Ueno Y , et al. (2019)
c.323T>C p.Leu108Pro missense_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.380G>C p.Gly127Ala missense_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.389G>A p.Arg130Gln missense_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.406T>C p.Cys136Arg missense_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.464A>C p.Tyr155Ser missense_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.521A>G p.Tyr174Cys missense_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.737C>T p.Pro246Leu missense_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.274G>A p.Asp92Asn missense_variant De novo - Simplex 25961944 Krumm N , et al. (2015)
c.38A>G p.Lys13Glu missense_variant Unknown - Unknown 31130284 Monies D , et al. (2019)
c.697C>T p.Arg233Ter stop_gained Familial Paternal - 30528446 Ciaccio C , et al. (2018)
c.-1026C>A - 5_prime_UTR_variant Familial Maternal - 17427195 Buxbaum JD , et al. (2007)
c.389G>A p.Arg130Gln missense_variant Unknown - Simplex 37524782 Balasar et al. (2023)
c.131G>A p.Gly44Asp missense_variant Unknown - Unknown 19265751 Varga EA , et al. (2009)
c.182C>T p.His61Tyr missense_variant Unknown - Unknown 31130284 Monies D , et al. (2019)
c.697C>T p.Arg233Ter stop_gained De novo - Simplex 34268892 Kaymakcalan H et al. (2021)
c.54_56del p.Gly19del inframe_deletion De novo - Multiplex 35982159 Zhou X et al. (2022)
c.723T>G p.Phe241Leu missense_variant De novo - Simplex 28263302 C Yuen RK et al. (2017)
c.737C>T p.Pro246Leu missense_variant De novo - Simplex 28263302 C Yuen RK et al. (2017)
c.464A>G p.Tyr155Cys missense_variant De novo - Simplex 38764027 Ruohao Wu et al. (2024)
c.278A>G p.His93Arg missense_variant De novo - Simplex 15805158 Butler MG , et al. (2005)
c.232A>G p.Thr78Ala missense_variant De novo - Simplex 21624971 Schaaf CP , et al. (2011)
c.208C>G p.Pro70Ala missense_variant Unknown - Unknown 23695273 Hobert JA , et al. (2013)
c.1027del p.Val343Ter frameshift_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.329dup p.Gln110ProfsTer5 frameshift_variant Familial - - 29608813 Wong CW , et al. (2018)
c.149T>C p.Ile50Thr missense_variant Familial Maternal - 28250423 Saskin A , et al. (2017)
c.520dup p.Tyr174LeufsTer6 frameshift_variant De novo - - 19265751 Varga EA , et al. (2009)
c.722T>C p.Phe241Ser missense_variant De novo - Simplex 15805158 Butler MG , et al. (2005)
c.755A>G p.Asp252Gly missense_variant De novo - Simplex 15805158 Butler MG , et al. (2005)
c.618C>G p.Phe206Leu missense_variant Unknown - Simplex 21624971 Schaaf CP , et al. (2011)
c.500C>A p.Thr167Asn missense_variant De novo - Simplex 22495309 O'Roak BJ , et al. (2012)
c.392C>T p.Ala131Val missense_variant De novo - Simplex 23160955 O'Roak BJ , et al. (2012)
c.320A>T p.Lys107Met missense_variant De novo - Simplex 25418537 O'Roak BJ , et al. (2014)
c.741T>C p.Leu247Ser missense_variant De novo - Simplex 28086757 Negishi Y , et al. (2017)
c.737C>T p.Pro246Leu missense_variant De novo - - 23934111 Epi4K Consortium , et al. (2013)
c.397G>A p.Ala133Thr missense_variant Familial Maternal - 28250423 Saskin A , et al. (2017)
c.549del p.Lys183ArgfsTer16 frameshift_variant De novo - - 29296277 Yeung KS , et al. (2018)
c.302T>C p.Ile101Thr missense_variant De novo - Multiplex 31398340 Ruzzo EK , et al. (2019)
c.3G>T p.Leu1? initiator_codon_variant Unknown - Unknown 23695273 Hobert JA , et al. (2013)
c.369C>G p.Tyr123Ter missense_variant Unknown - Unknown 20533527 McBride KL , et al. (2010)
c.737C>T p.Pro246Leu missense_variant Unknown - Unknown 35887114 Levchenko O et al. (2022)
c.502_503del p.Ser168ProfsTer15 frameshift_variant De novo - - 35982159 Zhou X et al. (2022)
c.510T>A p.Ser170Arg missense_variant Familial Maternal - 30528446 Ciaccio C , et al. (2018)
c.400A>T p.Met134Leu missense_variant Unknown - Unknown 25363760 De Rubeis S , et al. (2014)
c.-1034_-1030dupGCCCT - 2KB_upstream_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.388C>T p.Arg130Ter stop_gained Familial Paternal Simplex 19265751 Varga EA , et al. (2009)
c.416T>A p.Leu139Ter stop_gained Familial Paternal Simplex 19265751 Varga EA , et al. (2009)
c.611C>T p.Pro204Leu missense_variant De novo - Simplex 34268892 Kaymakcalan H et al. (2021)
c.1013del p.Ser338LeufsTer6 frameshift_variant De novo - Simplex 31674007 Wu H , et al. (2019)
c.27del p.Ser10AlafsTer14 frameshift_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.640C>T p.Gln214Ter stop_gained Familial Maternal Simplex 23160955 O'Roak BJ , et al. (2012)
c.302T>C p.Ile101Thr missense_variant De novo - Simplex 31981491 Satterstrom FK et al. (2020)
c.449A>G p.Glu150Gly missense_variant De novo - Simplex 31981491 Satterstrom FK et al. (2020)
c.821G>T p.Trp274Leu missense_variant Unknown - Simplex 37541188 Sanchis-Juan A et al. (2023)
c.389G>A p.Arg130Gln missense_variant Unknown Not maternal - 30528446 Ciaccio C , et al. (2018)
c.235G>A p.Ala79Thr missense_variant Familial Maternal - 31209962 Aspromonte MC , et al. (2019)
c.752G>A p.Gly251Asp missense_variant Familial Maternal Simplex 36699461 Kagan M et al. (2023)
c.611del p.Pro204GlnfsTer17 frameshift_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.955insA p.Thr319AsnfsTer6 frameshift_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.1176del p.Phe392LeufsTer24 frameshift_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.640C>T p.Gln214Ter stop_gained Unknown Not maternal Simplex 28086757 Negishi Y , et al. (2017)
c.402G>C p.Glu134Asp missense_variant Familial Maternal Multiplex 23124040 Busa T , et al. (2012)
c.697C>T p.Arg233Ter stop_gained Unknown Not paternal Multiplex 19265751 Varga EA , et al. (2009)
NM_000314.5:c.1006C>G p.Tyr336Ter stop_gained De novo - Simplex 28086757 Negishi Y , et al. (2017)
c.405dup p.Cys136MetfsTer44 frameshift_variant Familial Paternal - 30763456 Zhou WZ , et al. (2019)
c.462dup p.Tyr155LeufsTer25 frameshift_variant Familial Maternal - 30763456 Zhou WZ , et al. (2019)
NM_001304717.3:c.1011+2T>G - splice_site_variant Unknown - Simplex 31130284 Monies D , et al. (2019)
c.225_226del p.His75LeufsTer2 frameshift_variant De novo - Simplex 31130284 Monies D , et al. (2019)
c.518G>A p.Arg173His missense_variant Familial Paternal Simplex 20533527 McBride KL , et al. (2010)
c.66C>G p.Asp22Glu missense_variant Familial Paternal Multiplex 17427195 Buxbaum JD , et al. (2007)
c.100del p.Ala34LeufsTer20 frameshift_variant Unknown - Unknown 25363760 De Rubeis S , et al. (2014)
c.512_513insACA p.Leu171_Pro172insHis inframe_insertion De novo - - 30528446 Ciaccio C , et al. (2018)
c.176C>G p.Pro59Arg stop_gained Familial Paternal Multi-generational 30482242 Gruhl SL , et al. (2018)
c.548del p.Lys183ArgfsTer16 frameshift_variant De novo - Simplex 31981491 Satterstrom FK et al. (2020)
c.420_421insA p.Ala141SerfsTer43 frameshift_variant Unknown - Unknown 23695273 Hobert JA , et al. (2013)
c.545T>C p.Val182Ala missense_variant Familial Both parents Multiplex 26443266 Schwerd T , et al. (2015)
c.361_362dup p.Ser121ArgfsTer55 frameshift_variant De novo - Simplex 38041506 Erica Rosina et al. (2024)
c.525_526dup p.Tyr176CysfsTer8 frameshift_variant De novo - Simplex 34268892 Kaymakcalan H et al. (2021)
c.1110_1111insATAGT p.Asp371IlefsTer47 frameshift_variant Unknown - Unknown 32959437 Shao DD et al. (2020)
c.518G>A p.Arg173His missense_variant Familial Maternal Multi-generational 19265751 Varga EA , et al. (2009)
c.493G>T p.Lys164Asn missense_variant Familial Maternal Multi-generational 29296277 Yeung KS , et al. (2018)
c.470A>G p.Gln157Arg missense_variant De novo - Multiplex (identical twins) 19265751 Varga EA , et al. (2009)
c.401T>C p.Met134Thr missense_variant Familial Maternal Multi-generational 20533527 McBride KL , et al. (2010)
c.821G>T p.Trp274Leu missense_variant Familial Maternal Multi-generational 20533527 McBride KL , et al. (2010)
Common Variants  

No common variants reported.

SFARI Gene score
1S

High Confidence, Syndromic

Score Delta: Score remained at 1S

1

High Confidence

See all Category 1 Genes

We considered a rigorous statistical comparison between cases and controls, yielding genome-wide statistical significance, with independent replication, to be the strongest possible evidence for a gene. These criteria were relaxed slightly for category 2.

The syndromic category includes mutations that are associated with a substantial degree of increased risk and consistently linked to additional characteristics not required for an ASD diagnosis. If there is independent evidence implicating a gene in idiopathic ASD, it will be listed as "#S" (e.g., 2S, 3S, etc.). If there is no such independent evidence, the gene will be listed simply as "S."

1/1/2021
1
icon
1

Score remained at 1

Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR 0.05, meaning that this gene had a 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

10/1/2020
1
icon
1

Score remained at 1

Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR 0.05, meaning that this gene had a 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

4/1/2020
1
icon
1

Score remained at 1

Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR 0.05, meaning that this gene had a 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

1/1/2020
1
icon
1

Score remained at 1

Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR 0.05, meaning that this gene had a 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

10/1/2019
1S
icon
1

Score remained at 1

New Scoring Scheme
Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR 0.05, meaning that this gene had a 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

7/1/2019
1S
icon
1S

Score remained at 1S

Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR 0.05, meaning that this gene had a 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

1/1/2019
1S
icon
1S

Score remained at 1S

Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR 0.05, meaning that this gene had a 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

10/1/2018
1S
icon
1S

Score remained at 1S

Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR 0.05, meaning that this gene had a 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

10/1/2017
1S
icon
1S

Score remained at 1S

Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR ? 0.05, meaning that this gene had a ? 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

7/1/2017
1S
icon
1S

Score remained at 1S

Description

Variants in PTEN have been identified in individuals presenting with ASD and macrocephaly in multiple studies (PMIDs 15805158, 18759867, 19265751, 20533527). Two de novo deleterious events in the PTEN gene were identified in exome sequencing studies in simplex ASD cases in 2012: a missense variant (p.Thr167Asn) that was classified as "severe" in O'Roak et al. Nature 2012 (PMID 22495309); and a frameshift variant (p.Cys136MetfsX44) in O'Roak et al. Science 2012 (PMID 23160955). A detailed examination of ASD cases with heterozygous PTEN mutations in Frazier et al., 2015 found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). An additional de novo loss-of-function variant in the PTEN gene was subsequently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium in De Rubeis et al., 2014 (PMID 25363760). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) in this report furthermore identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR ? 0.05, meaning that this gene had a ? 95% chance of being a true autism gene. This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017). PTEN has also been designated as a syndromic ASD gene, as mutations in the PTEN gene are causative for Cowden syndrome, a disorder in which a subpopulation of individuals with the syndrome develop autism (PMID 11496368).

4/1/2017
1S
icon
1S

Score remained at 1S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LoF events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified." A de novo LoF variant in the PTEN gene was recently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium (PMID 25363760). A detailed examination of ASD cases with heterozygous PTEN mutations found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) identified PTEN as a gene meeting high statistical significance with a 0.01< FDR ?0.05, meaning that this gene had a ?95% chance of being a true autism gene (PMID 25363760). This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017).

Reports Added
[Mutation screening of the PTEN gene in patients with autism spectrum disorders and macrocephaly.2007] [Autistic spectrum disorder in a 9-year-old girl with macrocephaly.2010] [Oligogenic heterozygosity in individuals with high-functioning autism spectrum disorders.2011] [Sporadic autism exomes reveal a highly interconnected protein network of de novo mutations.2012] [Multiplex targeted sequencing identifies recurrently mutated genes in autism spectrum disorders.2012] [Biochemical screening and PTEN mutation analysis in individuals with autism spectrum disorders and macrocephaly.2013] [Autism-epilepsy phenotype with macrocephaly suggests PTEN, but not GLIALCAM, genetic screening.2014] [Synaptic, transcriptional and chromatin genes disrupted in autism.2014] [Novel PTEN mutations in neurodevelopmental disorders and macrocephaly.2008] [The prevalence of PTEN mutations in a clinical pediatric cohort with autism spectrum disorders, developmental delay, and macrocephaly.2009] [Confirmation study of PTEN mutations among individuals with autism or developmental delays/mental retardation and macrocephaly.2010] [PTEN mutation in a family with Cowden syndrome and autism.2001] [De novo mutations in epileptic encephalopathies.2013] [Subset of individuals with autism spectrum disorders and extreme macrocephaly associated with germline PTEN tumour suppressor gene mutations.2005] [Novel PTEN germline mutation in a family with mild phenotype: difficulties in genetic counseling.2012] [PTEN, a putative protein tyrosine phosphatase gene mutated in human brain, breast, and prostate cancer.1997] [The tumor suppressor, PTEN/MMAC1, dephosphorylates the lipid second messenger, phosphatidylinositol 3,4,5-trisphosphate.1998] [Negative regulation of PKB/Akt-dependent cell survival by the tumor suppressor PTEN.1998] [Electrical signals control wound healing through phosphatidylinositol-3-OH kinase-gamma and PTEN.2006] [Free fatty acids inhibit insulin signaling-stimulated endothelial nitric oxide synthase activation through upregulating PTEN or inhibiting Akt kinase.2006] [PTEN is recruited to the postsynaptic terminal for NMDA receptor-dependent long-term depression.2010] [A secreted PTEN phosphatase that enters cells to alter signaling and survival.2013] [PTEN knockdown alters dendritic spine/protrusion morphology, not density.2013] [Characteristic brain magnetic resonance imaging pattern in patients with macrocephaly and PTEN mutations.2014] [Loss of mTOR repressors Tsc1 or Pten has divergent effects on excitatory and inhibitory synaptic transmission in single hippocampal neuron cultures.2014] [Functionally distinct groups of inherited PTEN mutations in autism and tumour syndromes.2014] [PTEN interacts with histone H1 and controls chromatin condensation.2014] [Molecular and phenotypic abnormalities in individuals with germline heterozygous PTEN mutations and autism.2014] [Conformational stability and catalytic activity of PTEN variants linked to cancers and autism spectrum disorders.2015] [A mutant form of PTEN linked to autism.2010] [Neural transcriptome of constitutional Pten dysfunction in mice and its relevance to human idiopathic autism spectrum disorder.2015] [Integrated analysis of whole-exome sequencing and transcriptome profiling in males with autism spectrum disorders.2015] [The parvalbumin/somatostatin ratio is increased in Pten mutant mice and by human PTEN ASD alleles.2015] [Excess of rare, inherited truncating mutations in autism.2015] [Molecular Diagnostic Yield of Chromosomal Microarray Analysis and Whole-Exome Sequencing in Children With Autism Spectrum Disorder.2015] [A recessive form of extreme macrocephaly and mild intellectual disability complements the spectrum of PTEN hamartoma tumour syndrome.2015] [Autistic-Like Traits and Cerebellar Dysfunction in Purkinje Cell PTEN Knock-Out Mice.2015] [Targeted DNA Sequencing from Autism Spectrum Disorder Brains Implicates Multiple Genetic Mechanisms.2015] [Low load for disruptive mutations in autism genes and their biased transmission.2015] [A Retroviral CRISPR-Cas9 System for Cellular Autism-Associated Phenotype Discovery in Developing Neurons.2016] [A combination of genetic and biochemical analyses for the diagnosis of PI3K-AKT-mTOR pathway-associated megalencephaly.2017] [Whole genome sequencing resource identifies 18 new candidate genes for autism spectrum disorder2017] [Prevalence of four Mendelian disorders associated with autism in 2392 affected families.2017]
1/1/2017
1S
icon
1S

Score remained at 1S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LoF events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified." A de novo LoF variant in the PTEN gene was recently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium (PMID 25363760). A detailed examination of ASD cases with heterozygous PTEN mutations found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) identified PTEN as a gene meeting high statistical significance with a 0.01 < FDR ?0.05, meaning that this gene had a ?95% chance of being a true autism gene (PMID 25363760). This gene was identified in Iossifov et al. 2015 as a strong candidate to be an ASD risk gene based on a combination of de novo mutational evidence and the absence or very low frequency of mutations in controls (PMID 26401017).

4/1/2016
1S
icon
1S

Score remained at 1S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LoF events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified." A de novo LoF variant in the PTEN gene was recently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium (PMID 25363760). A detailed examination of ASD cases with heterozygous PTEN mutations found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) identified PTEN as a gene meeting high statistical significance with a 0.01

Reports Added
[Mutation screening of the PTEN gene in patients with autism spectrum disorders and macrocephaly.2007] [Autistic spectrum disorder in a 9-year-old girl with macrocephaly.2010] [Oligogenic heterozygosity in individuals with high-functioning autism spectrum disorders.2011] [Sporadic autism exomes reveal a highly interconnected protein network of de novo mutations.2012] [Multiplex targeted sequencing identifies recurrently mutated genes in autism spectrum disorders.2012] [Biochemical screening and PTEN mutation analysis in individuals with autism spectrum disorders and macrocephaly.2013] [Autism-epilepsy phenotype with macrocephaly suggests PTEN, but not GLIALCAM, genetic screening.2014] [Synaptic, transcriptional and chromatin genes disrupted in autism.2014] [Novel PTEN mutations in neurodevelopmental disorders and macrocephaly.2008] [The prevalence of PTEN mutations in a clinical pediatric cohort with autism spectrum disorders, developmental delay, and macrocephaly.2009] [Confirmation study of PTEN mutations among individuals with autism or developmental delays/mental retardation and macrocephaly.2010] [PTEN mutation in a family with Cowden syndrome and autism.2001] [De novo mutations in epileptic encephalopathies.2013] [Subset of individuals with autism spectrum disorders and extreme macrocephaly associated with germline PTEN tumour suppressor gene mutations.2005] [Novel PTEN germline mutation in a family with mild phenotype: difficulties in genetic counseling.2012] [PTEN, a putative protein tyrosine phosphatase gene mutated in human brain, breast, and prostate cancer.1997] [The tumor suppressor, PTEN/MMAC1, dephosphorylates the lipid second messenger, phosphatidylinositol 3,4,5-trisphosphate.1998] [Negative regulation of PKB/Akt-dependent cell survival by the tumor suppressor PTEN.1998] [Electrical signals control wound healing through phosphatidylinositol-3-OH kinase-gamma and PTEN.2006] [Free fatty acids inhibit insulin signaling-stimulated endothelial nitric oxide synthase activation through upregulating PTEN or inhibiting Akt kinase.2006] [PTEN is recruited to the postsynaptic terminal for NMDA receptor-dependent long-term depression.2010] [A secreted PTEN phosphatase that enters cells to alter signaling and survival.2013] [PTEN knockdown alters dendritic spine/protrusion morphology, not density.2013] [Characteristic brain magnetic resonance imaging pattern in patients with macrocephaly and PTEN mutations.2014] [Loss of mTOR repressors Tsc1 or Pten has divergent effects on excitatory and inhibitory synaptic transmission in single hippocampal neuron cultures.2014] [Functionally distinct groups of inherited PTEN mutations in autism and tumour syndromes.2014] [PTEN interacts with histone H1 and controls chromatin condensation.2014] [Molecular and phenotypic abnormalities in individuals with germline heterozygous PTEN mutations and autism.2014] [Conformational stability and catalytic activity of PTEN variants linked to cancers and autism spectrum disorders.2015] [A mutant form of PTEN linked to autism.2010] [Neural transcriptome of constitutional Pten dysfunction in mice and its relevance to human idiopathic autism spectrum disorder.2015] [Integrated analysis of whole-exome sequencing and transcriptome profiling in males with autism spectrum disorders.2015] [The parvalbumin/somatostatin ratio is increased in Pten mutant mice and by human PTEN ASD alleles.2015] [Excess of rare, inherited truncating mutations in autism.2015] [Molecular Diagnostic Yield of Chromosomal Microarray Analysis and Whole-Exome Sequencing in Children With Autism Spectrum Disorder.2015] [A recessive form of extreme macrocephaly and mild intellectual disability complements the spectrum of PTEN hamartoma tumour syndrome.2015] [Autistic-Like Traits and Cerebellar Dysfunction in Purkinje Cell PTEN Knock-Out Mice.2015] [Targeted DNA Sequencing from Autism Spectrum Disorder Brains Implicates Multiple Genetic Mechanisms.2015] [Low load for disruptive mutations in autism genes and their biased transmission.2015] [A Retroviral CRISPR-Cas9 System for Cellular Autism-Associated Phenotype Discovery in Developing Neurons.2016]
1/1/2016
1S
icon
1S

Score remained at 1S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LoF events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified." A de novo LoF variant in the PTEN gene was recently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium (PMID 25363760). A detailed examination of ASD cases with heterozygous PTEN mutations found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) identified PTEN as a gene meeting high statistical significance with a 0.01

Reports Added
[Mutation screening of the PTEN gene in patients with autism spectrum disorders and macrocephaly.2007] [Autistic spectrum disorder in a 9-year-old girl with macrocephaly.2010] [Oligogenic heterozygosity in individuals with high-functioning autism spectrum disorders.2011] [Sporadic autism exomes reveal a highly interconnected protein network of de novo mutations.2012] [Multiplex targeted sequencing identifies recurrently mutated genes in autism spectrum disorders.2012] [Biochemical screening and PTEN mutation analysis in individuals with autism spectrum disorders and macrocephaly.2013] [Autism-epilepsy phenotype with macrocephaly suggests PTEN, but not GLIALCAM, genetic screening.2014] [Synaptic, transcriptional and chromatin genes disrupted in autism.2014] [Novel PTEN mutations in neurodevelopmental disorders and macrocephaly.2008] [The prevalence of PTEN mutations in a clinical pediatric cohort with autism spectrum disorders, developmental delay, and macrocephaly.2009] [Confirmation study of PTEN mutations among individuals with autism or developmental delays/mental retardation and macrocephaly.2010] [PTEN mutation in a family with Cowden syndrome and autism.2001] [De novo mutations in epileptic encephalopathies.2013] [Subset of individuals with autism spectrum disorders and extreme macrocephaly associated with germline PTEN tumour suppressor gene mutations.2005] [Novel PTEN germline mutation in a family with mild phenotype: difficulties in genetic counseling.2012] [PTEN, a putative protein tyrosine phosphatase gene mutated in human brain, breast, and prostate cancer.1997] [The tumor suppressor, PTEN/MMAC1, dephosphorylates the lipid second messenger, phosphatidylinositol 3,4,5-trisphosphate.1998] [Negative regulation of PKB/Akt-dependent cell survival by the tumor suppressor PTEN.1998] [Electrical signals control wound healing through phosphatidylinositol-3-OH kinase-gamma and PTEN.2006] [Free fatty acids inhibit insulin signaling-stimulated endothelial nitric oxide synthase activation through upregulating PTEN or inhibiting Akt kinase.2006] [PTEN is recruited to the postsynaptic terminal for NMDA receptor-dependent long-term depression.2010] [A secreted PTEN phosphatase that enters cells to alter signaling and survival.2013] [PTEN knockdown alters dendritic spine/protrusion morphology, not density.2013] [Characteristic brain magnetic resonance imaging pattern in patients with macrocephaly and PTEN mutations.2014] [Loss of mTOR repressors Tsc1 or Pten has divergent effects on excitatory and inhibitory synaptic transmission in single hippocampal neuron cultures.2014] [Functionally distinct groups of inherited PTEN mutations in autism and tumour syndromes.2014] [PTEN interacts with histone H1 and controls chromatin condensation.2014] [Molecular and phenotypic abnormalities in individuals with germline heterozygous PTEN mutations and autism.2014] [Conformational stability and catalytic activity of PTEN variants linked to cancers and autism spectrum disorders.2015] [A mutant form of PTEN linked to autism.2010] [Neural transcriptome of constitutional Pten dysfunction in mice and its relevance to human idiopathic autism spectrum disorder.2015] [Integrated analysis of whole-exome sequencing and transcriptome profiling in males with autism spectrum disorders.2015] [The parvalbumin/somatostatin ratio is increased in Pten mutant mice and by human PTEN ASD alleles.2015] [Excess of rare, inherited truncating mutations in autism.2015] [Molecular Diagnostic Yield of Chromosomal Microarray Analysis and Whole-Exome Sequencing in Children With Autism Spectrum Disorder.2015] [A recessive form of extreme macrocephaly and mild intellectual disability complements the spectrum of PTEN hamartoma tumour syndrome.2015] [Autistic-Like Traits and Cerebellar Dysfunction in Purkinje Cell PTEN Knock-Out Mice.2015] [Targeted DNA Sequencing from Autism Spectrum Disorder Brains Implicates Multiple Genetic Mechanisms.2015] [Low load for disruptive mutations in autism genes and their biased transmission.2015]
7/1/2015
1S
icon
1S

Score remained at 1S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LoF events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified." A de novo LoF variant in the PTEN gene was recently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium (PMID 25363760). A detailed examination of ASD cases with heterozygous PTEN mutations found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) identified PTEN as a gene meeting high statistical significance with a 0.01

Reports Added
[Mutation screening of the PTEN gene in patients with autism spectrum disorders and macrocephaly.2007] [Autistic spectrum disorder in a 9-year-old girl with macrocephaly.2010] [Oligogenic heterozygosity in individuals with high-functioning autism spectrum disorders.2011] [Sporadic autism exomes reveal a highly interconnected protein network of de novo mutations.2012] [Multiplex targeted sequencing identifies recurrently mutated genes in autism spectrum disorders.2012] [Biochemical screening and PTEN mutation analysis in individuals with autism spectrum disorders and macrocephaly.2013] [Autism-epilepsy phenotype with macrocephaly suggests PTEN, but not GLIALCAM, genetic screening.2014] [Synaptic, transcriptional and chromatin genes disrupted in autism.2014] [Novel PTEN mutations in neurodevelopmental disorders and macrocephaly.2008] [The prevalence of PTEN mutations in a clinical pediatric cohort with autism spectrum disorders, developmental delay, and macrocephaly.2009] [Confirmation study of PTEN mutations among individuals with autism or developmental delays/mental retardation and macrocephaly.2010] [PTEN mutation in a family with Cowden syndrome and autism.2001] [De novo mutations in epileptic encephalopathies.2013] [Subset of individuals with autism spectrum disorders and extreme macrocephaly associated with germline PTEN tumour suppressor gene mutations.2005] [Novel PTEN germline mutation in a family with mild phenotype: difficulties in genetic counseling.2012] [PTEN, a putative protein tyrosine phosphatase gene mutated in human brain, breast, and prostate cancer.1997] [The tumor suppressor, PTEN/MMAC1, dephosphorylates the lipid second messenger, phosphatidylinositol 3,4,5-trisphosphate.1998] [Negative regulation of PKB/Akt-dependent cell survival by the tumor suppressor PTEN.1998] [Electrical signals control wound healing through phosphatidylinositol-3-OH kinase-gamma and PTEN.2006] [Free fatty acids inhibit insulin signaling-stimulated endothelial nitric oxide synthase activation through upregulating PTEN or inhibiting Akt kinase.2006] [PTEN is recruited to the postsynaptic terminal for NMDA receptor-dependent long-term depression.2010] [A secreted PTEN phosphatase that enters cells to alter signaling and survival.2013] [PTEN knockdown alters dendritic spine/protrusion morphology, not density.2013] [Characteristic brain magnetic resonance imaging pattern in patients with macrocephaly and PTEN mutations.2014] [Loss of mTOR repressors Tsc1 or Pten has divergent effects on excitatory and inhibitory synaptic transmission in single hippocampal neuron cultures.2014] [Functionally distinct groups of inherited PTEN mutations in autism and tumour syndromes.2014] [PTEN interacts with histone H1 and controls chromatin condensation.2014] [Molecular and phenotypic abnormalities in individuals with germline heterozygous PTEN mutations and autism.2014] [Conformational stability and catalytic activity of PTEN variants linked to cancers and autism spectrum disorders.2015] [A mutant form of PTEN linked to autism.2010] [Neural transcriptome of constitutional Pten dysfunction in mice and its relevance to human idiopathic autism spectrum disorder.2015] [Integrated analysis of whole-exome sequencing and transcriptome profiling in males with autism spectrum disorders.2015] [The parvalbumin/somatostatin ratio is increased in Pten mutant mice and by human PTEN ASD alleles.2015] [Excess of rare, inherited truncating mutations in autism.2015] [Molecular Diagnostic Yield of Chromosomal Microarray Analysis and Whole-Exome Sequencing in Children With Autism Spectrum Disorder.2015]
4/1/2015
1S
icon
1S

Score remained at 1S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LoF events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified." A de novo LoF variant in the PTEN gene was recently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium (PMID 25363760). A detailed examination of ASD cases with heterozygous PTEN mutations found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) identified PTEN as a gene meeting high statistical significance with a 0.01

1/1/2015
1S
icon
1S

Score remained at 1S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LGD events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified." A de novo LoF variant in the PTEN gene was recently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium (PMID 25363760). A detailed examination of ASD cases with heterozygous PTEN mutations found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) identified PTEN as a gene meeting high statistical significance with a 0.01

10/1/2014
2S
icon
1S

Decreased from 2S to 1S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LGD events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified." A de novo LoF variant in the PTEN gene was recently identified in an ASD proband from 2,270 trios screened by the Autism Sequencing Consortium (PMID 25363760). A detailed examination of ASD cases with heterozygous PTEN mutations found that these cases had a high proportion of missense variants, showed reduced PTEN protein levels, and exhibited prominent white-matter and cognitive abnormalities compared to other groups (PMID 25288137). Analysis of rare coding variation in 3,871 ASD cases and 9,937 ancestry-matched or paternal controls from the Autism Sequencing Consortium (ASC) identified PTEN as a gene meeting high statistical significance with a 0.01

7/1/2014
No data
icon
2S

Increased from No data to 2S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LGD events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified."

Reports Added
[PTEN, a putative protein tyrosine phosphatase gene mutated in human brain, breast, and prostate cancer.1997] [The tumor suppressor, PTEN/MMAC1, dephosphorylates the lipid second messenger, phosphatidylinositol 3,4,5-trisphosphate.1998] [Negative regulation of PKB/Akt-dependent cell survival by the tumor suppressor PTEN.1998] [PTEN mutation in a family with Cowden syndrome and autism.2001] [Subset of individuals with autism spectrum disorders and extreme macrocephaly associated with germline PTEN tumour suppressor gene mutations.2005] [Electrical signals control wound healing through phosphatidylinositol-3-OH kinase-gamma and PTEN.2006] [Free fatty acids inhibit insulin signaling-stimulated endothelial nitric oxide synthase activation through upregulating PTEN or inhibiting Akt kinase.2006] [Mutation screening of the PTEN gene in patients with autism spectrum disorders and macrocephaly.2007] [PTEN is recruited to the postsynaptic terminal for NMDA receptor-dependent long-term depression.2010] [Autistic spectrum disorder in a 9-year-old girl with macrocephaly.2010] [Oligogenic heterozygosity in individuals with high-functioning autism spectrum disorders.2011] [Sporadic autism exomes reveal a highly interconnected protein network of de novo mutations.2012] [Novel PTEN germline mutation in a family with mild phenotype: difficulties in genetic counseling.2012] [Multiplex targeted sequencing identifies recurrently mutated genes in autism spectrum disorders.2012] [Biochemical screening and PTEN mutation analysis in individuals with autism spectrum disorders and macrocephaly.2013] [A secreted PTEN phosphatase that enters cells to alter signaling and survival.2013] [De novo mutations in epileptic encephalopathies.2013] [PTEN knockdown alters dendritic spine/protrusion morphology, not density.2013] [Characteristic brain magnetic resonance imaging pattern in patients with macrocephaly and PTEN mutations.2014] [Loss of mTOR repressors Tsc1 or Pten has divergent effects on excitatory and inhibitory synaptic transmission in single hippocampal neuron cultures.2014] [Autism-epilepsy phenotype with macrocephaly suggests PTEN, but not GLIALCAM, genetic screening.2014] [PTEN interacts with histone H1 and controls chromatin condensation.2014]
4/1/2014
No data
icon
2S

Increased from No data to 2S

Description

Syndromic because of causative mutations in Cowden syndrome. Two de novo LGD events in PTEN from recent exome sequencing studies in simplex ASD cases: from O'Roak et al. Nature 2012 (PMID 22495309) a de novo missense variant (p.Thr167Asn) that was ranked severe"; and from O'Roak et al. Science 2012 (PMID 23160955) a de novo frameshift insertion (p.Cys136MetfsX44) was also identified."

Krishnan Probability Score

Score 0.49831091848158

Ranking 2260/25841 scored genes


[Show Scoring Methodology]
Krishnan and colleagues generated probability scores genome-wide by using a machine learning approach on a human brain-specific gene network. The method was first presented in Nat Neurosci 19, 1454-1462 (2016), and scores for more than 25,000 RefSeq genes can be accessed in column G of supplementary table 3 (see: http://www.nature.com/neuro/journal/v19/n11/extref/nn.4353-S5.xlsx). A searchable browser, with the ability to view networks of associated ASD risk genes, can be found at asd.princeton.edu.
ExAC Score

Score 0.97550686584803

Ranking 2246/18225 scored genes


[Show Scoring Methodology]
The Exome Aggregation Consortium (ExAC) is a summary database of 60,706 exomes that has been widely used to estimate 'constraint' on mutation for individual genes. It was introduced by Lek et al. Nature 536, 285-291 (2016), and the ExAC browser can be found at exac.broadinstitute.org. The pLI score was developed as measure of intolerance to loss-of- function mutation. A pLI > 0.9 is generally viewed as highly constrained, and thus any loss-of- function mutations in autism in such a gene would be more likely to confer risk. For a full list of pLI scores see: ftp://ftp.broadinstitute.org/pub/ExAC_release/release0.3.1/functional_gene_constraint/fordist_cle aned_exac_nonTCGA_z_pli_rec_null_data.txt
Iossifov Probability Score

Score 0.973

Ranking 52/239 scored genes


[Show Scoring Methodology]
Supplementary dataset S2 in the paper by Iossifov et al. (PNAS 112, E5600-E5607 (2015)) lists 239 genes with a probability of at least 0.8 of being associated with autism risk (column I). This probability metric combines the evidence from de novo likely-gene- disrupting and missense mutations and assesses it against the background mutation rate in unaffected individuals from the University of Washington’s Exome Variant Sequence database (evs.gs.washington.edu/EVS/). The list of probability scores can be found here: www.pnas.org/lookup/suppl/doi:10.1073/pnas.1516376112/- /DCSupplemental/pnas.1516376112.sd02.xlsx
Sanders TADA Score

Score 0.00071064664987682

Ranking 18/18665 scored genes


[Show Scoring Methodology]
The TADA score ('Transmission and De novo Association') was introduced by He et al. PLoS Genet 9(8):e1003671 (2013), and is a statistic that integrates evidence from both de novo and transmitted mutations. It forms the basis for the claim of 65 individual genes being strongly associated with autism risk at a false discovery rate of 0.1 (Sanders et al. Neuron 87, 1215-1233 (2015)). The calculated TADA score for 18,665 RefSeq genes can be found in column P of Supplementary Table 6 in the Sanders et al. paper (the column headed 'tadaFdrAscSscExomeSscAgpSmallDel'), which represents a combined analysis of exome data and small de novo deletions (see www.cell.com/cms/attachment/2038545319/2052606711/mmc7.xlsx).
Larsen Cumulative Evidence Score

Score 82

Ranking 13/461 scored genes


[Show Scoring Methodology]
Larsen and colleagues generated gene scores based on the sum of evidence for all available ASD-associated variants in a gene, with assessments based on mode of inheritance, effect size, and variant frequency in the general population. The approach was first presented in Mol Autism 7:44 (2016), and scores for 461 genes can be found in column I in supplementary table 4 from that paper.
Zhang D Score

Score 0.24988226958981

Ranking 3481/20870 scored genes


[Show Scoring Methodology]
The DAMAGES score (disease-associated mutation analysis using gene expression signatures), or D score, was developed to combine evidence from de novo loss-of- function mutation with evidence from cell-type- specific gene expression in the mouse brain (specifically translational profiles of 24 specific mouse CNS cell types isolated from 6 different brain regions). Genes with positive D scores are more likely to be associated with autism risk, with higher-confidence genes having higher D scores. This statistic was first presented by Zhang & Shen (Hum Mutat 38, 204- 215 (2017), and D scores for more than 20,000 RefSeq genes can be found in column M in supplementary table 2 from that paper.
Interaction Table
Interactor Symbol Interactor Name Interactor Organism Interactor Type Entrez ID Uniprot ID
Beclin-1 Beclin-1 Human Direct Regulation 8678 Q14457
BMP9 Growth/differentiation factor 2 Mouse Protein Binding 12165 Q9WV56
C19orf29OS chromosome 19 open reading frame 29 opposite strand Human Protein Binding 404665 Q8N1I8
CHGB chromogranin B (secretogranin 1) Human Protein Binding 1114 P05060
cyclin D1 G1/S-specific cyclin-D1 Human Protein Binding 595 P24385
DJ1 Protein deglycase DJ-1 Human Protein Modification 11315 Q99497
FRK fyn-related kinase Human Protein Modification 2444 P42685
GFRA2 GDNF family receptor alpha 2 Human Protein Binding 2675 E9PD47
GPR113 G protein-coupled receptor 113 Human Protein Binding 165082 Q8IZF5
HBA1 hemoglobin, alpha 1 Human Protein Binding 3039 P69905
Histone H1.2 Histone H1.2 Human Protein Binding 3006 P16403
HP1 alpha Chromobox protein homolog 5 Human Protein Binding 23468 P45973
LEPREL4 leprecan-like 4 Human Protein Binding 10609 Q92791
lncRNA-BGL3 beta globin locus transcript 3 (non-protein coding) Human RNA Binding 103344929 N/A
miR-106b microRNA 106b Human RNA Binding 406900 N/A
miR-130b microRNA 130b Human RNA Binding 406920 N/A
miR-21 microRNA 21 Human RNA Binding 406991 N/A
miR-221 microRNA 221 Human RNA Binding 407006
miR-29a microRNA mir-29a Rat RNA Binding 100314230 N/A
miR-518c microRNA 518c Human RNA Binding 574477 N/A
miR-638 microRNA 638 Human RNA Binding 693223 N/A
miR-7 leukocyte immunoglobulin-like receptor, subfamily B (with TM and ITIM domains), member 1 Human RNA Binding 10859 Q8NHL6
miR-802 microRNA 802 Human RNA Binding 768219 N/A
miR-92a microRNA 29a Human Direct Regulation 407021 N/A
miR-BART7 ebv-mir-BART7 (MI0003729) HHV-4 RNA Binding N/A N/A
miR1297 microRNA 1297 Human RNA Binding 100302187 N/A
miR20b microRNA 20b Human RNA Binding 574032 N/A
miR214 microRNA 214 Human RNA Binding 406996 N/A
MIR221 microRNA 221 Human RNA Binding 407006 N/A
miR26a microRNA 26a-1 Human RNA Binding 407015 N/A
MIR29C microRNA 29c Human RNA Binding 407026 N/A
p21 cyclin-dependent kinase inhibitor 1A (p21, Cip1) Human Protein Binding 1026 P38936
PTPN6 protein tyrosine phosphatase, non-receptor type 6 Human Protein Modification 5777 P29350
PTPRZ1 N/A Pig Protein Modification 100511294 N/A
QRFPR pyroglutamylated RFamide peptide receptor Human Protein Binding 84109 Q96P65
SLUG Zinc finger protein SNAI2 Human DNA Binding 6591 O43623
TCEB3C transcription elongation factor B polypeptide 3C (elongin A3) Human Protein Binding 162699 Q8NG57
TNKS1 Tankyrase-1 Human Protein Modification 8658 O95271
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