PHF8PHD finger protein 8
Autism Reports / Total Reports
5 / 13Rare Variants / Common Variants
33 / 0Aliases
PHF8, RP13-444K19.2, JHDM1F, MRXSSD, ZNF422Associated Syndromes
-Chromosome Band
Xp11.22Associated Disorders
IDRelevance to Autism
An in-frame deletion variant in PHF8 was found to segregate with high-functioning autism without other clinical features in a multiplex ASD family (Nava et al., 2012). Mutations in this gene are associated with a syndromic form of X-linked intellectual disability (Siderius type X-linked syndromic mental retardation; OMIM 300263); behavioral abnormalities and stereotypic movements have been observed in some individuals with this disorder (Laumonnier et al., 2005; Abidi et al., 2007; Koivisto et al., 2007; Redin et al., 2014; Deciphering Developmental Disorders Study 2015). Sobering et al., 2022 presented 16 individuals with Siderious X-linked intellectual disability syndrome caused by loss-of-function variants in the PHF8 gene from 11 families and found that all affected individuals exhibited developmental delay, and all but two had borderline to severe intellectual disability, autism spectrum disorder (ASD) was reported in seven of these individuals.
Molecular Function
The protein encoded by this gene is a histone lysine demethylase that preferentially acts on histones in the monomethyl or dimethyl states. The encoded protein requires Fe(2+) ion, 2-oxoglutarate, and oxygen for its catalytic activity. The protein has an N-terminal PHD finger and a central Jumonji C domain. This gene is thought to function as a transcription activator. Defects in this gene are a cause of syndromic X-linked Siderius type intellectual disability (MRXSSD).
External Links
SFARI Genomic Platforms
Reports related to PHF8 (13 Reports)
| # | Type | Title | Author, Year | Autism Report | Associated Disorders |
|---|---|---|---|---|---|
| 1 | Highly Cited | Mutations in PHF8 are associated with X linked mental retardation and cleft lip/cleft palate | Laumonnier F , et al. (2005) | No | - |
| 2 | Support | A novel mutation in the PHF8 gene is associated with X-linked mental retardation with cleft lip/cleft palate | Abidi F , et al. (2007) | No | - |
| 3 | Support | Screening of mutations in the PHF8 gene and identification of a novel mutation in a Finnish family with XLMR and cleft lip/cleft palate | Koivisto AM , et al. (2007) | No | - |
| 4 | Primary | Analysis of the chromosome X exome in patients with autism spectrum disorders identified novel candidate genes, including TMLHE | Nava C , et al. (2012) | Yes | ID |
| 5 | Support | Efficient strategy for the molecular diagnosis of intellectual disability using targeted high-throughput sequencing | Redin C , et al. (2014) | No | - |
| 6 | Support | Large-scale discovery of novel genetic causes of developmental disorders | Deciphering Developmental Disorders Study (2014) | No | Microcephaly |
| 7 | Recent Recommendation | JMJD-1.2/PHF8 controls axon guidance by regulating Hedgehog-like signaling | Riveiro AR , et al. (2017) | No | - |
| 8 | Support | Characterization of intellectual disability and autism comorbidity through gene panel sequencing | Aspromonte MC , et al. (2019) | Yes | - |
| 9 | Support | Targeted Next-Generation Sequencing in Patients with Suggestive X-Linked Intellectual Disability | Ibarluzea N , et al. (2020) | No | - |
| 10 | Support | A recurrent PJA1 variant in trigonocephaly and neurodevelopmental disorders | Suzuki T et al. (2020) | Yes | - |
| 11 | Support | - | Balan S et al. (2021) | Yes | - |
| 12 | Support | - | Bruno LP et al. (2021) | Yes | - |
| 13 | Recent Recommendation | - | Sobering AK et al. (2022) | No | ASD, ADHD, epilepsy/seizures |
Rare Variants (33)
| Status | Allele Change | Residue Change | Variant Type | Inheritance Pattern | Parental Transmission | Family Type | PubMed ID | Author, Year |
|---|---|---|---|---|---|---|---|---|
| c.*1101G>A | - | missense_variant | Unknown | - | - | 34262135 | Balan S et al. (2021) | |
| c.529T>A | p.Ser177Thr | stop_gained | De novo | - | - | 17594395 | Abidi F , et al. (2007) | |
| c.264C>A | p.Asn88Lys | missense_variant | Unknown | - | - | 34262135 | Balan S et al. (2021) | |
| c.1627-1G>A | - | splice_site_variant | De novo | - | - | 35469323 | Sobering AK et al. (2022) | |
| c.*1112G>C | - | missense_variant | Familial | Maternal | - | 34262135 | Balan S et al. (2021) | |
| c.2475G>C | p.Glu825Asp | missense_variant | Unknown | - | - | 34262135 | Balan S et al. (2021) | |
| c.704+1G>A | - | splice_site_variant | De novo | - | Simplex | 35469323 | Sobering AK et al. (2022) | |
| c.124G>T | p.Val42Leu | missense_variant | Familial | Maternal | - | 34262135 | Balan S et al. (2021) | |
| c.2239G>A | p.Glu747Lys | missense_variant | Familial | Maternal | - | 34262135 | Balan S et al. (2021) | |
| c.1249+5G>C | - | splice_site_variant | Familial | Maternal | Simplex | 25167861 | Redin C , et al. (2014) | |
| - | p.Gly316_Arg380del | inframe_deletion | Familial | Maternal | - | 35469323 | Sobering AK et al. (2022) | |
| c.143A>G | p.Tyr48Cys | missense_variant | Familial | Maternal | - | 35469323 | Sobering AK et al. (2022) | |
| c.808C>T | p.Arg270Cys | missense_variant | Familial | Maternal | - | 35469323 | Sobering AK et al. (2022) | |
| c.2190_2192del | p.Leu731del | inframe_deletion | De novo | - | Simplex | 34948243 | Bruno LP et al. (2021) | |
| c.1150G>A | p.Glu384Lys | missense_variant | Familial | Maternal | - | 35469323 | Sobering AK et al. (2022) | |
| c.1731-2A>G | - | splice_site_variant | Familial | Maternal | Simplex | 35469323 | Sobering AK et al. (2022) | |
| c.252C>A | p.Tyr84Ter | stop_gained | Familial | Maternal | Simplex | 31906484 | Ibarluzea N , et al. (2020) | |
| c.862C>T | p.Gln288Ter | stop_gained | Familial | Maternal | Multiplex | 35469323 | Sobering AK et al. (2022) | |
| c.2794T>C | p.Cys932Arg | missense_variant | Familial | Maternal | - | 31209962 | Aspromonte MC , et al. (2019) | |
| c.2972A>G | p.Asn991Ser | missense_variant | Familial | Maternal | Simplex | 32530565 | Suzuki T et al. (2020) | |
| c.846dup | p.His283SerfsTer3 | frameshift_variant | Familial | Maternal | - | 35469323 | Sobering AK et al. (2022) | |
| c.257C>T | p.Thr86Met | missense_variant | Familial | Maternal | Multiplex | 35469323 | Sobering AK et al. (2022) | |
| c.294-1820_597-603del | - | inframe_deletion | Familial | Maternal | Simplex | 35469323 | Sobering AK et al. (2022) | |
| c.2868dup | p.Thr957HisfsTer19 | frameshift_variant | Familial | Maternal | - | 35469323 | Sobering AK et al. (2022) | |
| c.836C>T | p.Phe279Ser | missense_variant | Familial | Maternal | Multiplex | 17661819 | Koivisto AM , et al. (2007) | |
| c.2904_2906del | p.Ser969del | inframe_deletion | Familial | Maternal | Multiplex | 23092983 | Nava C , et al. (2012) | |
| c.1027C>T | p.Gln343Ter | stop_gained | Familial | Maternal | Extended multiplex | 35469323 | Sobering AK et al. (2022) | |
| c.631C>T | p.Arg211Ter | stop_gained | Familial | Maternal | Multi-generational | 16199551 | Laumonnier F , et al. (2005) | |
| c.2073_2074insTG | p.Glu692TrpfsTer174 | frameshift_variant | De novo | - | Simplex | 35469323 | Sobering AK et al. (2022) | |
| c.2104del | p.Glu702ArgfsTer163 | frameshift_variant | Familial | Maternal | Simplex | 35469323 | Sobering AK et al. (2022) | |
| del(ACAGGTCTTCCC) | - | splice_site_variant | Familial | Maternal | Multi-generational | 16199551 | Laumonnier F , et al. (2005) | |
| c.1731-2A>G | - | splice_site_variant | Familial | Maternal | Multiplex (monozygotic twins) | 35469323 | Sobering AK et al. (2022) | |
| c.738dup | p.Arg247SerfsTer17 | frameshift_variant | Familial | Maternal | Multi-generational | 25533962 | Deciphering Developmental Disorders Study (2014) |
Common Variants
No common variants reported.
SFARI Gene score
Syndromic
An in-frame deletion variant in PHF8 was found to segregate with high-functioning autism without other clinical features in a multiplex ASD family (Nava et al., 2012). Mutations in this gene are associated with a syndromic form of X-linked intellectual disability (Siderius type X-linked syndromic mental retardation; OMIM 300263); behavioral abnormalities and stereotypic movements have been observed in some individuals with this disorder (Laumonnier et al., 2005; Abidi et al., 2007; Koivisto et al., 2007; Redin et al., 2014; Deciphering Developmental Disorders Study 2015).
Score Delta: Score remained at S
criteria met
See SFARI Gene'scoring criteriaThe 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."
7/1/2020
Score remained at S
Description
An in-frame deletion variant in PHF8 was found to segregate with high-functioning autism without other clinical features in a multiplex ASD family (Nava et al., 2012). Mutations in this gene are associated with a syndromic form of X-linked intellectual disability (Siderius type X-linked syndromic mental retardation; OMIM 300263); behavioral abnormalities and stereotypic movements have been observed in some individuals with this disorder (Laumonnier et al., 2005; Abidi et al., 2007; Koivisto et al., 2007; Redin et al., 2014; Deciphering Developmental Disorders Study 2015).
1/1/2020
Score remained at S
Description
An in-frame deletion variant in PHF8 was found to segregate with high-functioning autism without other clinical features in a multiplex ASD family (Nava et al., 2012). Mutations in this gene are associated with a syndromic form of X-linked intellectual disability (Siderius type X-linked syndromic mental retardation; OMIM 300263); behavioral abnormalities and stereotypic movements have been observed in some individuals with this disorder (Laumonnier et al., 2005; Abidi et al., 2007; Koivisto et al., 2007; Redin et al., 2014; Deciphering Developmental Disorders Study 2015).
10/1/2019
Score remained at S
New Scoring Scheme
Description
An in-frame deletion variant in PHF8 was found to segregate with high-functioning autism without other clinical features in a multiplex ASD family (Nava et al., 2012). Mutations in this gene are associated with a syndromic form of X-linked intellectual disability (Siderius type X-linked syndromic mental retardation; OMIM 300263); behavioral abnormalities and stereotypic movements have been observed in some individuals with this disorder (Laumonnier et al., 2005; Abidi et al., 2007; Koivisto et al., 2007; Redin et al., 2014; Deciphering Developmental Disorders Study 2015).
Reports Added
[New Scoring Scheme]7/1/2019
Score remained at S
Description
An in-frame deletion variant in PHF8 was found to segregate with high-functioning autism without other clinical features in a multiplex ASD family (Nava et al., 2012). Mutations in this gene are associated with a syndromic form of X-linked intellectual disability (Siderius type X-linked syndromic mental retardation; OMIM 300263); behavioral abnormalities and stereotypic movements have been observed in some individuals with this disorder (Laumonnier et al., 2005; Abidi et al., 2007; Koivisto et al., 2007; Redin et al., 2014; Deciphering Developmental Disorders Study 2015).
Krishnan Probability Score
Score 0.49502600193412
Ranking 3268/25841 scored genes
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ExAC Score
Score 0.99823985258815
Ranking 1218/18225 scored genes
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Sanders TADA Score
Score 0.94235519684495
Ranking 15275/18665 scored genes
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Larsen Cumulative Evidence Score
Score 5
Ranking 288/461 scored genes
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Zhang D Score
Score 0.54398739843134
Ranking 265/20870 scored genes
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External PIN Data
Interactome
- Protein Binding
- DNA Binding
- RNA Binding
- Protein Modification
- Direct Regulation
- ASD-Linked Genes
Interaction Table
| Interactor Symbol | Interactor Name | Interactor Organism | Interactor Type | Entrez ID | Uniprot ID |
|---|---|---|---|---|---|
| CDC26 | cell division cycle 26 | Human | Protein Binding | 246184 | Q8NHZ8 |