YAP1 |
- 1
Haplo
Score - 0
Triplo
Score
Gene Facts External Data Attribution
- HGNC Symbol
- YAP1 (HGNC:16262) HGNC Entrez Ensembl OMIM UCSC Uniprot GeneReviews LOVD LSDB ClinVar
- HGNC Name
- Yes1 associated transcriptional regulator
- Gene type
- protein-coding gene
- Locus type
- gene with protein product
- Previous symbols
- No previous names found
- Alias symbols
- YAP65, YAP-1
- %HI
- 9.76(Read more about the DECIPHER Haploinsufficiency Index)
- pLI
- 1(Read more about gnomAD pLI score)
- LOEUF
- 0.21(Read more about gnomAD LOEUF score)
- Cytoband
- 11q22.1
- Genomic Coordinates
-
GRCh37/hg19: chr11:101981178-102104155 NCBI Ensembl UCSC GRCh38/hg38: chr11:102110447-102233424 NCBI Ensembl UCSC - MANE Select Transcript
- NM_001130145.3 ENST00000282441.10 (Read more about MANE Select)
- Function
- Transcriptional regulator which can act both as a coactivator and a corepressor and is the critical downstream regulatory target in the Hippo signaling pathway that plays a pivotal role in organ size control and tumor suppression by restricting proliferation and promoting apoptosis (PubMed:17974916, PubMed:18280240, PubMed:18579750, PubMed:21364637, PubMed:30447097). The core of this pathway is composed of a kinase cascade wherein STK3/MST2 and STK4/MST1, in complex with its regulatory protein S... (Source: Uniprot)
Dosage Sensitivity Summary (Gene)
Dosage ID:
ISCA-36611
ClinGen Curation ID:
CCID:008123
Curation Status:
Complete
Issue Type:
Dosage Curation -
Gene
Haploinsufficiency:
Little Evidence for Haploinsufficiency
(1)
Triplosensitivity:
No Evidence for Triplosensitivity
(0)
Last Evaluated:
11/13/2014
Haploinsufficiency (HI) Score Details
HI Score:
1
HI Evidence Strength:
Little Evidence for Haploinsufficiency
(Disclaimer)
HI Disease:
- uveal coloboma-cleft lip and palate-intellectual disability Monarch
HI Evidence:
-
PUBMED:
24462371
Williamson et al. (2014) described two families with optic fissure closure defects (OFCD) with loss of function (LOF) mutations in YAP1: Family 1305 [c.370c>T(p.Arg124*)] mutation was present in 4 family members affected with coloboma (which is typically due to an OFCD) and inherited from the unaffected grandfather. Family 132 [c.1066G>T(p.Glu356*)] mutation proband presented with bilateral OFCD and is part of a family with an autosomal dominant disorder with OFCDs, cleft lip with or without palate, intellectual disability, hematuria(without renal impairment or dysplasia) and sensorineural hearing loss. All 13 affected members carry the nonsense mutation but present with variable features of the syndrome. LOD score for the segregation of nonsense mutations in family 1305 and 132 was 4.2. Another family has been reported with phenotype similar to Family 132 in which YAP1 mutation could not be identified. No other LOF mutations in YAP1 were detected in 700 non-coloboma exomes in UK10K rare disease group or NHLBI exome sequencing project exome variant server (EVS). The UK10K coloboma exome data did not identify any missense mutation that were not also present in EVS. Array data from 210 individuals with eye malformations identified one individual with bilateral OFCDs and intellectual disability with a 29 Mb de novo deletion (chr11:84,886,352-113,918,790) that included YAP1 as well as 434 other genes. A re-evaluation of 336 unrelated OFCD affected individuals (not overlapped with patients for exome sequencing) identified three missense mutations in YAP1: One did not segregate with the OFCD phenotype, two had no family history of eye malformation or parental follow up. Complete inactivation of YAP1 in mice results in developmental arrest at 8.5 days leading to multisystem defects including yolk sac vasculogenesis and embryonic axis elongation. In mice, site and stage specific expression in mouse embryos shows expression otic vesicle, brain stem, in eye and distal optic cup and overlying surface of ectoderm, brain and in both maxillary and frontonasal components of primary palate. In humans, an attempt to quantify YAP1 in two control lymphoblastoid cell lines (LCL) and LCL from proband in Family 132 was not detectable. Differences in phenotype between the two families was suggested to be caused by alternative transcriptional start site. Mutation in Family 132 was in coding sequence of all transcriptscoming from either TSS. Family 1305 mutation was found in the 5'UTR rather than coding sequence and thus thought to be invisible to NMD. However, they were unable to test differential effect on NMD becuase there was no access to direct cell lines or tissues.
HI Evidence Comments:
Though both families are reported to have colobomas, given the discrepancy in phenotype between the two families reported in Williamson et al. 2014, we are giving this gene a haploinsufficiency score of 1; additional information is needed to clarify the role of this gene in optic fissure closure defects.
Triplosensitivity (TS) Score Details
TS Score:
0
TS Evidence Strength:
No Evidence for Triplosensitivity (Disclaimer)
Genomic View
Select assembly:
(NC_000011.9)
(NC_000011.10)