POGZPogo transposable element with ZNF domain

SFARI Gene Score

High Confidence, Syndromic Criteria 1.1, Syndromic

Autism Reports / Total Reports

26 / 64

Rare Variants / Common Variants

204 / 0

EAGLE Score

35.4

Strong Learn More

Aliases

POGZ, RP11-806J18.2, KIAA0461, MGC71543, SUHW5, ZNF280E, ZNF635, ZNF635m

Associated Syndromes

White-Sutton syndrome, White-Sutton syndrome, DD, ID, White-Sutton syndrome, DD, White-Sutton syndrome, DD, epilepsy/seizures

Chromosome Band

1q21.3

Associated Disorders

DD/NDD, ASD, EPS, ID

Genetic Category

Rare Single Gene Mutation, Syndromic, Functional

Relevance to Autism

Recurrent mutations in the POGZ gene have been identified in multiple individuals with ASD as described below. De novo variants in the POGZ gene were initially identified in autistic probands in two separate reports. In the first, 1 of 175 de novo frameshift variants was found in the POGZ gene in Neale et al., 2012 (PMID 22495311). In the other, 1 of 343 likely gene-disrupting variants was found in the POGZ gene in Iossifov et al., 2012 (PMID 22542183). No likely gene-disruptive variants in POGZ were observed in controls (although many missense variants have been observed in EVS). A third de novo LoF variant in the POGZ gene was identified in an ASD proband from the Simons Simplex Collection in Iossifov et al., 2014 (PMID 25363768). 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 De Rubeis et al., 2014 identified POGZ as a gene meeting high statistical significance with a FDR 0.01, meaning that this gene had a 99% 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). Additional de novo LoF variants in POGZ were identified in White et al., 2016 in individuals with developmental delay/intellectual disability and, in two cases, ASD (PMID 26739615). Furthermore, a review of clinical information in individuals with POGZ variants in this report identified shared phentoypic features (developmental delay/intellectual disability, hypotonia, behavioral abnormalities, similar facial features) and proposed that POGZ LoF variants were responsible for a form of syndromic intellectual disability. Additional LoF variants in POGZ were identified in previously unreported cases with developmental delay/intellectual disability and/or ASD in Stessman et al., 2016 (PMID 26942287). The authors of this report estimated that protein-truncating POGZ variants were significantly enriched in individuals with ASD and/or intellectual disability in comparison to the general population (p=4.19E-13, odds ratio 35.8), and that the penetrance of POGZ LoF variant was 65.9% given the incidence of ID (5.12%) in the general population. 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 POGZ as a gene reaching exome-wide significance (P < 2.5E-06).

Molecular Function

The protein encoded by this gene appears to be a zinc finger protein containing a transposase domain at the C-terminus. This protein was found to interact with the transcription factor SP1 in a yeast two-hybrid system. Plays a role in mitotic cell cycle progression and is involved in kinetochore assembly and mitotic sister chromatid cohesion. Probably through its association with CBX5 plays a role in mitotic chromosome segregation by regulating aurora kinase B/AURKB activation and AURKB and CBX5 dissociation from chromosome arms.

SFARI Genomic Platforms

GPF browser SFARI genome browser

Reports (64)
Variants (204)
Gene Score
Protein Interactions (1)

Reports related to POGZ (64 Reports)

#	Type	Title	Author, Year	Autism Report	Associated Disorders
1	Primary	Patterns and rates of exonic de novo mutations in autism spectrum disorders	Neale BM , et al. (2012)	Yes	-
2	Support	De novo gene disruptions in children on the autistic spectrum	Iossifov I , et al. (2012)	Yes	-
3	Support	Refinement and discovery of new hotspots of copy-number variation associated with autism spectrum disorder	Girirajan S , et al. (2013)	Yes	-
4	Recent Recommendation	Synaptic, transcriptional and chromatin genes disrupted in autism	De Rubeis S , et al. (2014)	Yes	-
5	Support	The contribution of de novo coding mutations to autism spectrum disorder	Iossifov I et al. (2014)	Yes	-
6	Support	Large-scale discovery of novel genetic causes of developmental disorders	Deciphering Developmental Disorders Study (2014)	No	Epilpesy/seizures
7	Support	A case of autism spectrum disorder arising from a de novo missense mutation in POGZ	Fukai R , et al. (2015)	Yes	-
8	Support	Excess of rare, inherited truncating mutations in autism	Krumm N , et al. (2015)	Yes	-
9	Recent Recommendation	Low load for disruptive mutations in autism genes and their biased transmission	Iossifov I , et al. (2015)	Yes	-
10	Support	Whole-exome sequencing and neurite outgrowth analysis in autism spectrum disorder	Hashimoto R , et al. (2015)	Yes	-
11	Recent Recommendation	POGZ truncating alleles cause syndromic intellectual disability	White J , et al. (2016)	No	ASD
12	Support	A novel de novo POGZ mutation in a patient with intellectual disability	Tan B , et al. (2016)	No	-
13	Recent Recommendation	De novo mutations in congenital heart disease with neurodevelopmental and other congenital anomalies	Homsy J , et al. (2016)	No	DD, learning disabilities
14	Recent Recommendation	Disruption of POGZ Is Associated with Intellectual Disability and Autism Spectrum Disorders	Stessman HA , et al. (2016)	No	ASD
15	Support	De novo POGZ mutations in sporadic autism disrupt the DNA-binding activity of POGZ	Matsumura K , et al. (2016)	No	-
16	Support	De novo POGZ mutations are associated with neurodevelopmental disorders and microcephaly	Ye Y , et al. (2016)	No	ASD
17	Support	Meta-analysis of 2,104 trios provides support for 10 new genes for intellectual disability	Lelieveld SH et al. (2016)	No	-
18	Support	Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics	Loviglio MN , et al. (2016)	No	Behavioral abnormalities (self-injurious, stereoty
19	Support	De novo genic mutations among a Chinese autism spectrum disorder cohort	Wang T , et al. (2016)	Yes	-
20	Support	Targeted sequencing identifies 91 neurodevelopmental-disorder risk genes with autism and developmental-disability biases	Stessman HA , et al. (2017)	Yes	-
21	Support	Whole genome sequencing resource identifies 18 new candidate genes for autism spectrum disorder	C Yuen RK et al. (2017)	Yes	-
22	Support	Integrative Analyses of De Novo Mutations Provide Deeper Biological Insights into Autism Spectrum Disorder	Takata A , et al. (2018)	Yes	-
23	Support	Genome sequencing identifies multiple deleterious variants in autism patients with more severe phenotypes	Guo H , et al. (2018)	Yes	-
24	Support	Genetic Diagnostic Evaluation of Trio-Based Whole Exome Sequencing Among Children With Diagnosed or Suspected Autism Spectrum Disorder	Du X , et al. (2018)	Yes	DD/ID
25	Support	Elucidation of the phenotypic spectrum and genetic landscape in primary and secondary microcephaly	Boonsawat P , et al. (2019)	No	DD
26	Support	POGZ-related epilepsy: Case report and review of the literature	Ferretti A , et al. (2019)	No	DD, ID, epilepsy/seizures, autistic features
27	Support	Rare inherited missense variants of POGZ associate with autism risk and disrupt neuronal development	Zhao W , et al. (2019)	Yes	-
28	Support	Increased diagnostic and new genes identification outcome using research reanalysis of singleton exome sequencing	Bruel AL , et al. (2019)	No	-
29	Support	POGZ de novo missense variants in neuropsychiatric disorders	Zhao W , et al. (2019)	Yes	-
30	Support	Exome sequencing of 457 autism families recruited online provides evidence for autism risk genes	Feliciano P et al. (2019)	Yes	-
31	Support	Phenotypic expansion of POGZ-related intellectual disability syndrome (White-Sutton syndrome)	Assia Batzir N , et al. (2019)	No	ASD or autistic features
32	Support	Large-Scale Exome Sequencing Study Implicates Both Developmental and Functional Changes in the Neurobiology of Autism	Satterstrom FK et al. (2020)	Yes	-
33	Recent recommendation	Pathogenic POGZ mutation causes impaired cortical development and reversible autism-like phenotypes	Matsumura K , et al. (2020)	Yes	-
34	Support	-	Hildebrand MS et al. (2020)	No	DD, ID
35	Support	A novel patient with White-Sutton syndrome refines the mutational and clinical repertoire of the POGZ-related phenotype and suggests further observations	Pascolini G et al. (2020)	No	ASD
36	Support	Large-scale targeted sequencing identifies risk genes for neurodevelopmental disorders	Wang T et al. (2020)	Yes	-
37	Support	-	Garde A et al. (2021)	No	DD, ID/learning disability, stereotypy
38	Support	-	Liu S et al. (2021)	No	ASD, ID, epilepsy/seizures
39	Support	-	Donnarumma B et al. (2021)	No	ASD, DD, ID
40	Support	-	Valentino F et al. (2021)	No	DD
41	Support	-	Pode-Shakked B et al. (2021)	Yes	-
42	Support	-	Mahjani B et al. (2021)	Yes	-
43	Recent Recommendation	-	Murch O et al. (2021)	No	ASD or autistic features, epilepsy/seizures
44	Support	-	Markenscoff-Papadimitriou E et al. (2021)	No	-
45	Support	-	Bruno LP et al. (2021)	No	-
46	Support	-	Nagy D et al. (2022)	No	ASD, ADHD, ID, epilepsy/seizures
47	Support	-	Deng L et al. (2022)	No	-
48	Support	-	Merriweather A et al. (2022)	No	Stereotypy
49	Support	-	Sun X et al. (2022)	No	-
50	Support	-	Conrow-Graham M et al. (2022)	No	-
51	Support	-	Giraldo-Ocampo S et al. (2022)	No	-
52	Support	-	Chen Y et al. (2021)	No	-
53	Support	-	Levchenko O et al. (2022)	No	-
54	Support	-	Zhou X et al. (2022)	Yes	-
55	Recent Recommendation	-	Weinschutz Mendes H et al. (2023)	Yes	-
56	Support	-	Spataro N et al. (2023)	No	ASD, learning disability
57	Support	-	Duan J et al. (2023)	No	-
58	Support	-	Wang J et al. (2023)	Yes	-
59	Support	-	Sun X et al. (2023)	No	-
60	Support	-	Sanchis-Juan A et al. (2023)	No	-
61	Support	-	Amerh S Alqahtani et al. (2023)	No	-
62	Support	-	Nanako Hamada et al. (2024)	No	-
63	Support	-	Shenglan Li et al. (2024)	No	Stereotypy
64	Support	-	Axel Schmidt et al. (2024)	No	ASD, ADHD

Rare Variants (204)

Allele Change	Residue Change	Variant Type	Inheritance Pattern	Parental Transmission	Family Type	PubMed ID	Author, Year
-	-	copy_number_loss	De novo	-	-	27148570	Ye Y , et al. (2016)
-	-	copy_number_loss	De novo	-	-	35052493	Nagy D et al. (2022)
c.3031C>T	p.Gln1011Ter	stop_gained	De novo	-	-	27148570	Ye Y , et al. (2016)
c.1447C>T	p.Gln483Ter	stop_gained	Unknown	-	-	33004838	Wang T et al. (2020)
c.1522C>T	p.Arg508Ter	stop_gained	Unknown	-	-	33004838	Wang T et al. (2020)
c.1608C>A	p.Tyr536Ter	stop_gained	Unknown	-	-	33004838	Wang T et al. (2020)
c.2053C>T	p.Arg685Ter	stop_gained	De novo	-	-	33004838	Wang T et al. (2020)
c.2080C>T	p.Arg694Ter	stop_gained	De novo	-	-	33004838	Wang T et al. (2020)
c.2190T>G	p.Tyr730Ter	stop_gained	De novo	-	-	35052493	Nagy D et al. (2022)
c.2545G>T	p.Gly849Ter	stop_gained	De novo	-	-	35052493	Nagy D et al. (2022)
c.538C>T	p.Gln180Ter	stop_gained	De novo	-	-	27824329	Wang T , et al. (2016)
c.2518+1del	-	splice_site_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.284-1G>T	-	splice_site_variant	De novo	-	-	26785492	Homsy J , et al. (2016)
c.2546-20T>A	-	intron_variant	De novo	-	-	38593811	Shenglan Li et al. (2024)
c.3022C>T	p.Arg1008Ter	stop_gained	De novo	-	-	33004838	Wang T et al. (2020)
c.3022C>T	p.Arg1008Ter	stop_gained	Unknown	-	-	33004838	Wang T et al. (2020)
c.3424C>T	p.Arg1142Ter	stop_gained	Unknown	-	-	33004838	Wang T et al. (2020)
c.3196A>T	p.Lys1066Ter	stop_gained	Unknown	-	-	35052493	Nagy D et al. (2022)
c.3259C>T	p.Arg1087Ter	stop_gained	De novo	-	-	35052493	Nagy D et al. (2022)
c.3022C>T	p.Arg1008Ter	stop_gained	De novo	-	-	35982159	Zhou X et al. (2022)
c.2092C>T	p.Arg698Ter	stop_gained	De novo	-	-	33277917	Garde A et al. (2021)
c.2310C>G	p.Tyr770Ter	stop_gained	De novo	-	-	33277917	Garde A et al. (2021)
c.2451C>A	p.Cys817Ter	stop_gained	De novo	-	-	33277917	Garde A et al. (2021)
c.833C>G	p.Ser278Ter	stop_gained	De novo	-	-	26739615	White J , et al. (2016)
c.2935C>T	p.Arg979Ter	stop_gained	De novo	-	-	26739615	White J , et al. (2016)
c.2989C>T	p.Arg997Ter	stop_gained	Unknown	-	-	34615535	Mahjani B et al. (2021)
c.2350C>T	p.Arg784Ter	stop_gained	De novo	-	-	36980980	Spataro N et al. (2023)
c.2546-20T>A	-	intron_variant	De novo	-	-	35396900	Merriweather A et al. (2022)
c.481C>T	p.Arg161Trp	missense_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.3259C>T	p.Arg1087Ter	stop_gained	De novo	-	-	36980980	Spataro N et al. (2023)
AC>A	-	frameshift_variant	Unknown	-	Unknown	25363760	De Rubeis S , et al. (2014)
c.1792C>G	p.Arg598Gly	missense_variant	De novo	-	-	33004838	Wang T et al. (2020)
c.1796C>T	p.Ser599Phe	missense_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.1958G>A	p.Arg653Gln	missense_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.2258G>A	p.Cys753Tyr	missense_variant	De novo	-	-	35052493	Nagy D et al. (2022)
c.538C>T	p.Gln180Ter	stop_gained	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.2405+1G>A	-	splice_site_variant	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.3116G>A	p.Arg1039His	missense_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.3694C>T	p.Arg1232Cys	missense_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.2369G>A	p.Ser746Asn	missense_variant	De novo	-	-	27824329	Wang T , et al. (2016)
c.1348G>A	p.Val450Ile	missense_variant	Unknown	-	-	31196716	Zhao W , et al. (2019)
c.1534C>A	p.His512Asn	missense_variant	De novo	-	-	31347273	Zhao W , et al. (2019)
c.1496G>T	p.Cys499Phe	missense_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.1727T>C	p.Leu576Pro	missense_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.2096C>T	p.Thr699Ile	missense_variant	De novo	-	-	34645992	Murch O et al. (2021)
-	p.Asn882LysfsTer14	frameshift_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.3631C>T	p.Arg1211Ter	stop_gained	De novo	-	-	32359026	Pascolini G et al. (2020)
c.1212C>A	p.Tyr404Ter	stop_gained	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.2708C>T	p.Ala903Val	stop_gained	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.2980G>T	p.Glu994Ter	stop_gained	De novo	-	-	28191889	Stessman HA , et al. (2017)
c.3118G>A	p.Glu1040Lys	missense_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.3914T>G	p.Leu1305Arg	missense_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.3040C>T	p.Gln1014Ter	stop_gained	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.3119C>T	p.Thr1040Ile	stop_gained	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.3847C>T	p.Gln1283Ter	stop_gained	De novo	-	-	26942287	Stessman HA , et al. (2016)
-	-	copy_number_gain	Familial	Maternal	Simplex	23375656	Girirajan S , et al. (2013)
c.460-2A>C	-	splice_site_variant	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.2310C>G	p.Tyr770Ter	stop_gained	De novo	-	Simplex	34645992	Murch O et al. (2021)
c.2711T>A	p.Leu904Ter	stop_gained	De novo	-	Simplex	34645992	Murch O et al. (2021)
c.1580A>G	p.Asp527Gly	missense_variant	Unknown	-	-	34615535	Mahjani B et al. (2021)
c.2433-1G>A	-	splice_site_variant	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.1522C>T	p.Arg508Ter	stop_gained	Familial	Maternal	-	35052493	Nagy D et al. (2022)
c.3001C>T	p.Arg1001Ter	stop_gained	De novo	-	Simplex	34645992	Murch O et al. (2021)
c.2716C>T	p.Pro906Ser	stop_gained	De novo	-	Simplex	34948243	Bruno LP et al. (2021)
c.1483C>T	p.Arg495Ter	stop_gained	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.1669G>T	p.Glu557Ter	stop_gained	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.2350C>T	p.Arg784Ter	stop_gained	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.2555G>A	p.Trp852Ter	stop_gained	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.2729C>A	p.Ser910Ter	stop_gained	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.2951C>T	p.Ala984Val	stop_gained	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.2989C>T	p.Arg997Ter	stop_gained	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.3139G>T	p.Glu1047Ter	stop_gained	Familial	Paternal	-	33004838	Wang T et al. (2020)
c.1457G>A	p.Arg486Gln	stop_gained	Unknown	-	Simplex	28263302	C Yuen RK et al. (2017)
c.3119C>T	p.Thr1040Ile	stop_gained	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.3424C>T	p.Arg1142Ter	stop_gained	Unknown	-	-	31782611	Assia Batzir N , et al. (2019)
c.493A>C	p.Asn165His	missense_variant	De novo	-	Simplex	37393044	Wang J et al. (2023)
c.2396G>A	p.Ser799Asn	missense_variant	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.1855C>G	p.Leu619Val	missense_variant	Unknown	-	-	39039281	Axel Schmidt et al. (2024)
c.1053C>A	p.Thr351=	stop_gained	De novo	-	Simplex	28191889	Stessman HA , et al. (2017)
c.2518+1dup	-	frameshift_variant	De novo	-	Simplex	26942287	Stessman HA , et al. (2016)
c.353del	p.Gly118AlafsTer9	frameshift_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.2763G>T	p.Glu921Asp	missense_variant	De novo	-	Simplex	30504930	Guo H , et al. (2018)
c.1664C>T	p.Pro555Leu	missense_variant	Unknown	-	Simplex	33004838	Wang T et al. (2020)
c.2248C>T	p.Arg750Trp	missense_variant	Unknown	-	Simplex	33004838	Wang T et al. (2020)
c.3022C>T	p.Arg1008Ter	stop_gained	De novo	-	Simplex	25363768	Iossifov I et al. (2014)
c.2711T>G	p.Leu904Ter	stop_gained	De novo	-	Simplex	31136090	Ferretti A , et al. (2019)
c.2487dup	p.Ser830LeufsTer25	frameshift_variant	De novo	-	-	27148570	Ye Y , et al. (2016)
c.2723dup	p.Pro909ThrfsTer26	frameshift_variant	De novo	-	-	27148570	Ye Y , et al. (2016)
c.3014del	p.Gln1005ArgfsTer5	frameshift_variant	De novo	-	-	27148570	Ye Y , et al. (2016)
c.2020del	p.Arg674ValfsTer9	frameshift_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.2366dup	p.Ser790GlufsTer9	frameshift_variant	De novo	-	-	33004838	Wang T et al. (2020)
c.2763del	p.Thr922LeufsTer6	frameshift_variant	De novo	-	-	35052493	Nagy D et al. (2022)
c.3184G>A	p.Glu1062Lys	missense_variant	De novo	-	Simplex	35873028	Chen Y et al. (2021)
c.941G>A	p.Ser314Asn	missense_variant	De novo	-	Simplex	25961944	Krumm N , et al. (2015)
c.1075C>T	p.Arg359Ter	stop_gained	Unknown	-	Unknown	25363760	De Rubeis S , et al. (2014)
c.1399C>T	p.Arg467Trp	missense_variant	Familial	Paternal	-	33004838	Wang T et al. (2020)
c.1610G>A	p.Arg537His	missense_variant	Familial	Maternal	-	33004838	Wang T et al. (2020)
c.2542C>T	p.Arg848Trp	missense_variant	Familial	Maternal	-	33004838	Wang T et al. (2020)
c.600dup	p.Gly201TrpfsTer105	frameshift_variant	De novo	-	-	35052493	Nagy D et al. (2022)
c.2171dup	p.Leu725SerfsTer19	frameshift_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.2403del	p.Lys801AsnfsTer10	frameshift_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.2501del	p.Leu834TrpfsTer20	frameshift_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.2076del	p.Val693TyrfsTer17	frameshift_variant	De novo	-	-	35052493	Nagy D et al. (2022)
c.2814A>G	p.Glu938%3D	synonymous_variant	De novo	-	Simplex	35982159	Zhou X et al. (2022)
c.566del	p.Pro189GlnfsTer21	frameshift_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.2400dup	p.Lys801GlnfsTer7	frameshift_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.3179_3180del	p.Tyr1060Ter	frameshift_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.3139G>T	p.Glu1047Ter	stop_gained	De novo	-	Simplex	26942287	Stessman HA , et al. (2016)
c.4054dup	p.Ser1352PhefsTer14	frameshift_variant	De novo	-	-	35982159	Zhou X et al. (2022)
c.1321G>A	p.Val441Ile	missense_variant	Familial	Paternal	-	27824329	Wang T , et al. (2016)
c.2469del	p.Thr824ProfsTer30	frameshift_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.2809del	p.Asp937MetfsTer12	frameshift_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.3118G>A	p.Glu1040Lys	missense_variant	De novo	-	Simplex	25694107	Fukai R , et al. (2015)
c.1810G>T	p.Glu604Ter	stop_gained	De novo	-	Multiplex	26942287	Stessman HA , et al. (2016)
c.3312del	p.Phe1104LeufsTer18	frameshift_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.2882dup	p.Glu962GlyfsTer24	frameshift_variant	De novo	-	-	26739615	White J , et al. (2016)
c.2898dup	p.Lys967GlufsTer19	frameshift_variant	De novo	-	-	26739615	White J , et al. (2016)
c.2809del	p.Ala937ProfsTer4	frameshift_variant	De novo	-	-	31231135	Bruel AL , et al. (2019)
c.1504del	p.Arg502GlyfsTer2	frameshift_variant	Unknown	-	-	34615535	Mahjani B et al. (2021)
c.3118G>A	p.Glu1040Lys	missense_variant	De novo	-	Simplex	29346770	Takata A , et al. (2018)
c.1790A>G	p.Tyr597Cys	missense_variant	De novo	-	Simplex	25363768	Iossifov I et al. (2014)
c.3040C>T	p.Gln1014Ter	stop_gained	De novo	-	Simplex	34580403	Pode-Shakked B et al. (2021)
c.329T>G	p.Val110Gly	missense_variant	Unknown	-	Unknown	25363760	De Rubeis S , et al. (2014)
c.851G>A	p.Arg284Gln	missense_variant	Unknown	-	Unknown	25363760	De Rubeis S , et al. (2014)
c.2168_2169del	p.Pro723ArgfsTer11	frameshift_variant	Unknown	-	-	27148570	Ye Y , et al. (2016)
c.1153_1154del	p.Met385ValfsTer9	frameshift_variant	De novo	-	-	33004838	Wang T et al. (2020)
c.2323_2324del	p.Leu775ValfsTer4	frameshift_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.1153_1154del	p.Met385ValfsTer9	frameshift_variant	De novo	-	-	35052493	Nagy D et al. (2022)
c.2846_2847del	p.Ala949ValfsTer6	frameshift_variant	De novo	-	-	35052493	Nagy D et al. (2022)
c.3689del	p.Cys1230PhefsTer35	frameshift_variant	Unknown	-	-	34615535	Mahjani B et al. (2021)
c.2492del	p.His831ProfsTer14	splice_site_variant	De novo	-	-	31231135	Bruel AL , et al. (2019)
c.1295A>G	p.Arg432Gly	missense_variant	Unknown	-	Unknown	25363760	De Rubeis S , et al. (2014)
c.1610A>G	p.Asn537Ser	missense_variant	Unknown	-	Unknown	25363760	De Rubeis S , et al. (2014)
c.1580A>G	p.Asp527Gly	missense_variant	De novo	-	Simplex	30842647	Boonsawat P , et al. (2019)
c.2195_2196del	p.Pro732ArgfsTer11	frameshift_variant	Unknown	-	-	33004838	Wang T et al. (2020)
c.392dup	p.Met132HisfsTer9	frameshift_variant	De novo	-	Simplex	35982159	Zhou X et al. (2022)
c.1180_1181del	p.Met394ValfsTer9	frameshift_variant	De novo	-	-	33277917	Garde A et al. (2021)
c.2080C>T	p.Arg694Ter	stop_gained	Familial	Maternal	Multiplex	34645992	Murch O et al. (2021)
c.1099dup	p.Ile367AsnfsTer6	frameshift_variant	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.2381del	p.Leu794TrpfsTer8	frameshift_variant	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.2020del	p.Arg674ValfsTer9	frameshift_variant	De novo	-	-	27479843	Lelieveld SH et al. (2016)
c.2106del	p.Leu703CysfsTer7	frameshift_variant	De novo	-	-	28191889	Stessman HA , et al. (2017)
c.3574_3575del	p.Asp1192Ter	frameshift_variant	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.3014G>A	p.Arg1005His	missense_variant	Unknown	-	Unknown	25363760	De Rubeis S , et al. (2014)
c.3125A>G	p.Gln1042Arg	missense_variant	De novo	-	Simplex	26582266	Hashimoto R , et al. (2015)
c.2497C>A	p.His833Asn	missense_variant	De novo	-	Simplex	32345733	Hildebrand MS et al. (2020)
c.3259C>T	p.Arg1087Ter	stop_gained	Unknown	-	Unknown	37799141	Amerh S Alqahtani et al. (2023)
c.1613_1623del	p.Cys538Ter	frameshift_variant	De novo	-	Simplex	34645992	Murch O et al. (2021)
c.1524-3C>G	-	splice_region_variant	Familial	Paternal	Multiplex	33277917	Garde A et al. (2021)
c.1965del	p.Glu655AspfsTer19	frameshift_variant	De novo	-	-	26942287	Stessman HA , et al. (2016)
c.2455dup	p.Asp819GlyfsTer36	frameshift_variant	De novo	-	-	34215294	Donnarumma B et al. (2021)
c.1823A>G	p.His608Arg	missense_variant	Unknown	-	Simplex	37541188	Sanchis-Juan A et al. (2023)
c.2068_2069insACTA	p.Thr690AsnfsTer8	frameshift_variant	De novo	-	-	27148570	Ye Y , et al. (2016)
c.4042G>C	p.Glu1348Gln	missense_variant	Familial	Maternal	Simplex	34133408	Liu S et al. (2021)
c.1981G>A	p.Asp661Asn	missense_variant	Familial	Paternal	Simplex	33004838	Wang T et al. (2020)
c.2746del	p.Thr916ProfsTer12	frameshift_variant	De novo	-	Simplex	37016333	Duan J et al. (2023)
c.978del	p.Pro327GlnfsTer23	frameshift_variant	De novo	-	Simplex	34645992	Murch O et al. (2021)
c.1153_1154del	p.Met385ValfsTer9	frameshift_variant	De novo	-	-	36980980	Spataro N et al. (2023)
c.3258G>A	p.Arg1086=	synonymous_variant	De novo	-	Simplex	31981491	Satterstrom FK et al. (2020)
c.3792_3800del	p.Leu1264_Cys1267delinsPhe	inframe_indel	De novo	-	-	35982159	Zhou X et al. (2022)
c.3329del	p.Leu1110CysfsTer3	frameshift_variant	De novo	-	Simplex	34645992	Murch O et al. (2021)
c.3456_3457del	p.Glu1154ThrfsTer4	frameshift_variant	Unknown	-	-	34615535	Mahjani B et al. (2021)
c.2827del	p.Thr943ProfsTer6	frameshift_variant	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.1993del	p.Arg665ValfsTer9	frameshift_variant	Familial	Paternal	-	34645992	Murch O et al. (2021)
c.2316_2318del	p.Cys773del	inframe_deletion	De novo	-	Simplex	26942287	Stessman HA , et al. (2016)
c.2967dup	p.Pro990SerfsTer28	frameshift_variant	Unknown	-	-	31782611	Assia Batzir N , et al. (2019)
c.1124_1125del	p.Phe375SerfsTer4	frameshift_variant	De novo	-	Simplex	30555518	Du X , et al. (2018)
c.3432_3433del	p.Glu1145ThrfsTer4	frameshift_variant	De novo	-	-	31452935	Feliciano P et al. (2019)
c.2819_2826del	p.Leu940ArgfsTer2	frameshift_variant	De novo	-	-	39039281	Axel Schmidt et al. (2024)
c.3159del	p.Phe1056LeufsTer17	frameshift_variant	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.2906_2907dup	p.Arg970PhefsTer3	frameshift_variant	De novo	-	Simplex	34645992	Murch O et al. (2021)
c.600dup	p.Gly201TrpfsTer114	frameshift_variant	De novo	-	Simplex	35887114	Levchenko O et al. (2022)
c.398C>G	p.Thr133Ser	missense_variant	Familial	Paternal	Simplex	25363760	De Rubeis S , et al. (2014)
c.407A>G	p.Asn136Ser	missense_variant	Familial	Maternal	Simplex	25363760	De Rubeis S , et al. (2014)
c.1479del	p.Arg493SerfsTer2	frameshift_variant	Unknown	-	Unknown	25363760	De Rubeis S , et al. (2014)
c.1222_1223insC	p.Val408AlafsTer11	frameshift_variant	De novo	-	Simplex	26763879	Tan B , et al. (2016)
c.2493_2494del	p.His831GlnfsTer23	frameshift_variant	De novo	-	Simplex	34645992	Murch O et al. (2021)
c.1577del	p.Cys526PhefsTer45	frameshift_variant	Unknown	-	Unknown	25363760	De Rubeis S , et al. (2014)
c.1965del	p.Glu655AspfsTer19	frameshift_variant	De novo	-	Simplex	26942287	Stessman HA , et al. (2016)
c.2410del	p.Ile804SerfsTer41	frameshift_variant	De novo	-	Simplex	26942287	Stessman HA , et al. (2016)
c.2692del	p.Ala898HisfsTer21	frameshift_variant	De novo	-	Simplex	26942287	Stessman HA , et al. (2016)
c.2955del	p.Glu985AspfsTer25	frameshift_variant	De novo	-	Simplex	26942287	Stessman HA , et al. (2016)
c.2664del	p.Glu889LysfsTer4	splice_site_variant	De novo	-	Simplex	26942287	Stessman HA , et al. (2016)
c.1125_1126del	p.Phe375LeufsTer4	frameshift_variant	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.3085C>T	p.His1029Tyr	missense_variant	Familial	Paternal	Simplex	25363760	De Rubeis S , et al. (2014)
c.3140G>A	p.Arg1047Gln	missense_variant	Familial	Paternal	Simplex	25363760	De Rubeis S , et al. (2014)
c.406C>T	p.Pro189Ser	missense_variant	Familial	Maternal	Multiplex	25363760	De Rubeis S , et al. (2014)
c.3043_3044del	p.Ser1015LeufsTer2	frameshift_variant	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.3324_3325del	p.Leu1108PhefsTer9	frameshift_variant	De novo	-	-	31782611	Assia Batzir N , et al. (2019)
c.3689del	p.Cys1230PhefsTer35	frameshift_variant	De novo	-	Simplex	31981491	Satterstrom FK et al. (2020)
c.3710_3711del	p.Ser1237Ter	frameshift_variant	Familial	Maternal	-	31782611	Assia Batzir N , et al. (2019)
c.3308del	p.Leu1103ProfsTer19	frameshift_variant	Unknown	-	Simplex	35821784	Giraldo-Ocampo S et al. (2022)
c.2439_2442del	p.Phe813LeufsTer31	frameshift_variant	Unknown	Not maternal	-	26739615	White J , et al. (2016)
c.2432_2433insGTAC	p.Cys811TrpfsTer45	frameshift_variant	De novo	-	Simplex	22495311	Neale BM , et al. (2012)
c.3573_3574insTGATGACG	p.Asp1192Ter	frameshift_variant	De novo	-	Simplex	22542183	Iossifov I , et al. (2012)
c.2321_2324del	p.Ser774CysfsTer16	frameshift_variant	De novo	-	Simplex	31981491	Satterstrom FK et al. (2020)
c.3456_3457del	p.Glu1154ThrfsTer4	frameshift_variant	De novo	-	Simplex	31981491	Satterstrom FK et al. (2020)
c.2711T>A	p.Leu904Ter	stop_gained	De novo	-	Simplex	25533962	Deciphering Developmental Disorders Study (2014)
c.2296_2299del	p.Leu766ValfsTer15	frameshift_variant	Unknown	Not maternal	-	27799067	Loviglio MN , et al. (2016)
c.2619del	p.Asn873LysfsTer6	frameshift_variant	Unknown	-	Multi-generational	26942287	Stessman HA , et al. (2016)
c.1180_1181del	p.Met394ValfsTer9	frameshift_variant	Familial	Maternal	Multiplex	34356170	Valentino F et al. (2021)
c.2369G>A;c.2396G>A	p.Ser746Asn;p.Ser799Asn	missense_variant	Familial	Paternal	Simplex	27824329	Wang T , et al. (2016)
c.3327del	p.Leu1110CysfsTer3	frameshift_variant	De novo	-	Simplex	25533962	Deciphering Developmental Disorders Study (2014)
c.C1638C>G;c.1737C>G;c.1764C>G;c.1896C>G;c.1923C>G	p.His546Gln;p.His579Gln;.p.His588Gln;p.His632Gln;p.His641Gln	missense_variant	De novo	-	Simplex	28263302	C Yuen RK et al. (2017)

Common Variants

No common variants reported.

Current Score
Scoring History
3rd Party Scoring

SFARI Gene score

High Confidence, Syndromic

Score Delta: Score remained at 1S

criteria met

See SFARI Gene'scoring criteria

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.

Syndromic

See all Category S Genes

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

Score remained at 1

Description

De novo variants in the POGZ gene were initially identified in autistic probands in two separate reports. In the first, 1 of 175 de novo frameshift variants was found in the POGZ gene in Neale et al., 2012 (PMID 22495311). In the other, 1 of 343 likely gene-disrupting variants was found in the POGZ gene in Iossifov et al., 2012 (PMID 22542183). No likely gene-disruptive variants in POGZ were observed in controls (although many missense variants have been observed in EVS). A third de novo LoF variant in the POGZ gene was identified in an ASD proband from the Simons Simplex Collection in Iossifov et al., 2014 (PMID 25363768). 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 De Rubeis et al., 2014 identified POGZ as a gene meeting high statistical significance with a FDR 0.01, meaning that this gene had a 99% 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). Additional de novo LoF variants in POGZ were identified in PMID 26739615 in individuals with developmental delay/intellectual disability and, in two cases, ASD. A review of clinical information in individuals with POGZ variants in PMID 26739615 identified shared phentoypic features (developmental delay/intellectual disability, hypotonia, behavioral abnormalities, similar facial features) and proposed that POGZ LoF variants were responsible for a form of syndromic intellectual disability. Additional LoF variants in POGZ were identified in previously unreported cases with developmental delay/intellectual disability and/or ASD in PMID 26942287. The authors of this report estimated that protein-truncating POGZ variants were significantly enriched in ASD and/or ID individuals in comparison to the general population (p=4.19E-13, odds ratio 35.8), and that the penetrance of POGZ LoF variant was 65.9% given the incidence of ID (5.12%) in the general population. Functional analysis of two previously reported inherited missense variants in the POGZ gene that were identified in ASD probands from the Autism Clinical and Genetic Resources in China (ACGC) cohort demonstrated that these variants resulted in aberrant subcellular localization in transfected HEK293 cells, as well as a failure to rescue deficits in neurite and dendritic spine development in cultured mouse cortical neurons with Pogz knockdown (Zhao et al., 2019). The authors also observed a significant burden of rare POGZ missense variants in ASD cases compared to controls (P = 4.6E-05, odds ratio 3.96).

Reports Added

[Neuropsychological study in 19 French patients with White-Sutton syndrome and POGZ mutations2021]

10/1/2020

Score remained at 1

Description

Reports Added

[Large-scale targeted sequencing identifies risk genes for neurodevelopmental disorders2020]

4/1/2020

Score remained at 1

Description

Reports Added

[A novel patient with White-Sutton syndrome refines the mutational and clinical repertoire of the POGZ-related phenotype and suggests further observations2020]

1/1/2020

Score remained at 1

Description

Reports Added

[Phenotypic expansion of POGZ-related intellectual disability syndrome (White-Sutton syndrome).2019] [Large-Scale Exome Sequencing Study Implicates Both Developmental and Functional Changes in the Neurobiology of Autism2020] [Pathogenic POGZ mutation causes impaired cortical development and reversible autism-like phenotypes.2020]

10/1/2019

Score remained at 1

New Scoring Scheme

Description

Reports Added

[Exome sequencing of 457 autism families recruited online provides evidence for autism risk genes2019] [New Scoring Scheme]

7/1/2019

Score remained at 1S

Description

Reports Added

4/1/2019

Score remained at 1S

Description

Reports Added

[Elucidation of the phenotypic spectrum and genetic landscape in primary and secondary microcephaly.2019]

1/1/2019

Score remained at 1S

Description

Reports Added

[Genetic Diagnostic Evaluation of Trio-Based Whole Exome Sequencing Among Children With Diagnosed or Suspected Autism Spectrum Disorder.2018]

10/1/2018

Score remained at 1S

Description

Reports Added

[Genome sequencing identifies multiple deleterious variants in autism patients with more severe phenotypes.2018]

4/1/2017

Score remained at 1S

Description

De novo variants in the POGZ gene have been identified in autistic probands in two separate reports. In the first, 1 of 175 de novo frameshift variants was found in the POGZ gene (PMID 22495311). In the other, 1 of 343 likely gene-disrupting variants was found in the POGZ gene (PMID 22542183). no controls (many missense have been observed in EVS). A third de novo LoF variant in the POGZ gene was recently identified in an ASD proband from the Simons Simplex Collection (PMID 25363768). 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 POGZ as a gene meeting high statistical significance with a FDR ?0.01, meaning that this gene had a ?99% 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). Additional de novo LoF variants in POGZ were identified in PMID 26739615 in individuals with developmental delay/intellectual disability and, in two cases, ASD. A review of clinical information in individuals with POGZ variants in PMID 26739615 identified shared phentoypic features (developmental delay/intellectual disability, hypotonia, behavioral abnormalities, similar facial features) and proposed that POGZ LoF variants were responsible for a form of syndromic ID. Additional LoF variants in POGZ were identified in previously unreported cases with developmental delay/intellectual disability and/or ASD in PMID 26942287. The authors of this report estimated that protein-truncating POGZ variants were significantly enriched in ASD and/or ID individuals in comparison to the general population (p=4.19E-13, odds ratio 35.8), and that the penetrance of POGZ LoF variant was 65.9% given the incidence of ID (5.12%) in the general population.

Reports Added

[Patterns and rates of exonic de novo mutations in autism spectrum disorders.2012] [De novo gene disruptions in children on the autistic spectrum.2012] [Refinement and discovery of new hotspots of copy-number variation associated with autism spectrum disorder.2013] [Synaptic, transcriptional and chromatin genes disrupted in autism.2014] [The contribution of de novo coding mutations to autism spectrum disorder2014] [A case of autism spectrum disorder arising from a de novo missense mutation in POGZ.2015] [Large-scale discovery of novel genetic causes of developmental disorders.2014] [Excess of rare, inherited truncating mutations in autism.2015] [Whole-exome sequencing and neurite outgrowth analysis in autism spectrum disorder.2015] [Low load for disruptive mutations in autism genes and their biased transmission.2015] [POGZ truncating alleles cause syndromic intellectual disability.2016] [A novel de novo POGZ mutation in a patient with intellectual disability.2016] [De novo mutations in congenital heart disease with neurodevelopmental and other congenital anomalies.2016] [Disruption of POGZ Is Associated with Intellectual Disability and Autism Spectrum Disorders.2016] [De novo POGZ mutations in sporadic autism disrupt the DNA-binding activity of POGZ.2016] [De novo POGZ mutations are associated with neurodevelopmental disorders and microcephaly.2016] [Meta-analysis of 2,104 trios provides support for 10 new genes for intellectual disability2016] [Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics.2016] [De novo genic mutations among a Chinese autism spectrum disorder cohort.2016] [Targeted sequencing identifies 91 neurodevelopmental-disorder risk genes with autism and developmental-disability biases.2017] [Whole genome sequencing resource identifies 18 new candidate genes for autism spectrum disorder2017]

1/1/2017

Score remained at 1S

Description

Reports Added

[Targeted sequencing identifies 91 neurodevelopmental-disorder risk genes with autism and developmental-disability biases.2017]

10/1/2016

Score remained at 1S

Description

Reports Added

[Identification of a RAI1-associated disease network through integration of exome sequencing, transcriptomics, and 3D genomics.2016] [De novo genic mutations among a Chinese autism spectrum disorder cohort.2016]

7/1/2016

Score remained at 1S

Description

Reports Added

[Meta-analysis of 2,104 trios provides support for 10 new genes for intellectual disability2016]

4/1/2016

Score remained at 1S

Description

Reports Added

1/1/2016

Score remained at 1S

Description

Reports Added

4/1/2015

Score remained at 1

Description

Reports Added

[Excess of rare, inherited truncating mutations in autism.2015]

1/1/2015

Score remained at 1

Description

Reports Added

[A case of autism spectrum disorder arising from a de novo missense mutation in POGZ.2015] [Large-scale discovery of novel genetic causes of developmental disorders.2014]

10/1/2014

Decreased from 3 to 1

Description

Reports Added

[Synaptic, transcriptional and chromatin genes disrupted in autism.2014] [The contribution of de novo coding mutations to autism spectrum disorder2014]

7/1/2014

No data

Increased from No data to 3

Description

4/1/2014

No data

Increased from No data to 3

Description

Krishnan Probability Score

Score 0.51637770010842

Ranking 1745/25841 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.

Original Source

ExAC Score

Score 0.99999912812546

Ranking 292/18225 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

Original Source

Iossifov Probability Score

Score 0.958

Ranking 73/239 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 Washingtonâs 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

Original Source

Sanders TADA Score

Score 4.6761079775445E-5

Ranking 11/18665 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).

Original Source

Larsen Cumulative Evidence Score

Score 64

Ranking 23/461 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.

Original Source

Zhang D Score

Score 0.43666272912927

Ranking 1066/20870 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.

Original Source

External PIN Data

BioGRID Human Protein Reference Database

Interaction Table

Interactor Symbol	Interactor Name	Interactor Organism	Interactor Type	Entrez ID	Uniprot ID
TMEM171	Transmembrane protein 171	Human	Protein Binding	134285	Q8WVE6

Human Gene Module / Chromosome 1 / POGZ

POGZPogo transposable element with ZNF domain

SFARI Gene Score

Autism Reports / Total Reports

Rare Variants / Common Variants

EAGLE Score

Aliases

Associated Syndromes

Chromosome Band

Associated Disorders

Genetic Category

Relevance to Autism

Molecular Function

External Links

Human

Mouse

Fruit fly

SFARI Genomic Platforms

Reports related to POGZ (64 Reports)

Rare Variants (204)

Common Variants

SFARI Gene score

High Confidence, Syndromic

Score Delta: Score remained at 1S

criteria met

High Confidence

Syndromic

1/1/2021

Score remained at 1

Description

Reports Added

10/1/2020

Score remained at 1

Description

Reports Added

4/1/2020

Score remained at 1

Description

Reports Added

1/1/2020

Score remained at 1

Description

Reports Added

10/1/2019

Score remained at 1

New Scoring Scheme

Description

Reports Added

7/1/2019

Score remained at 1S

Description

Reports Added

4/1/2019

Score remained at 1S

Description

Reports Added

1/1/2019

Score remained at 1S

Description

Reports Added

10/1/2018

Score remained at 1S

Description

Reports Added

4/1/2017

Score remained at 1S

Description

Reports Added

1/1/2017

Score remained at 1S

Description

Reports Added

10/1/2016

Score remained at 1S

Description

Reports Added

7/1/2016

Score remained at 1S

Description

Reports Added