Incidental Mutation 'IGL01983:Pon3'

• ID: 183527
• Institutional Source: Australian Phenomics Network
• Gene Symbol: Pon3
• Ensembl Gene: ENSMUSG00000029759
• Gene Name: paraoxonase 3
• Essential gene?: Essential (E-score: 1.000)
• Stock #: IGL01983
• Chromosome: 6
• Chromosomal Location: 5220852-5256286 bp(-) (GRCm39)
• Type of Mutation: missense
• DNA Base Change (assembly): A to G at 5240974 bp (GRCm39)
• Zygosity: Heterozygous
• Amino Acid Change: Leucine to Serine at position 69 (L69S)
• Ref Sequence: ENSEMBL: ENSMUSP00000031773
• Gene Model: predicted gene model for transcript(s): [ENSMUST00000031773] [ENSMUST00000125686] [ENSMUST00000129344]
• AlphaFold: Q62087
• Predicted Effect: probably damaging; Transcript: ENSMUST00000031773; AA Change: L69S; PolyPhen 2 Score 1.000 (Sensitivity: 0.00; Specificity: 1.00)
• SMART Domains: Protein: ENSMUSP00000031773; Gene: ENSMUSG00000029759; AA Change: L69S

Domain	Start	End	E-Value	Type
Pfam:SGL	84	304	8.8e-9	PFAM
Pfam:Arylesterase	167	252	2.5e-43	PFAM
Pfam:Str_synth	184	250	3e-8	PFAM

• Predicted Effect: probably benign; Transcript: ENSMUST00000125686
• SMART Domains: Protein: ENSMUSP00000135603; Gene: ENSMUSG00000029759

Domain	Start	End	E-Value	Type
Pfam:Arylesterase	94	135	9.1e-20	PFAM

• Predicted Effect: probably benign; Transcript: ENSMUST00000129344
• SMART Domains: Protein: ENSMUSP00000118137; Gene: ENSMUSG00000029759

Domain	Start	End	E-Value	Type
PDB:4HHQ|A	1	67	3e-17	PDB

• Predicted Effect: noncoding transcript; Transcript: ENSMUST00000156848
• Predicted Effect: noncoding transcript; Transcript: ENSMUST00000176948
• SMART Domains: Protein: ENSMUSP00000135554; Gene: ENSMUSG00000029759

Domain	Start	End	E-Value	Type
PDB:3SRG|A	3	90	1e-33	PDB

• MGI Phenotype: FUNCTION: [Summary is not available for the mouse gene. This summary is for the human ortholog.] This gene is a member of the paraoxonase family and lies in a cluster on chromosome 7 with the other two family members. The encoded protein is secreted into the bloodstream and associates with high-density lipoprotein (HDL). The protein also rapidly hydrolyzes lactones and can inhibit the oxidation of low-density lipoprotein (LDL), a function that is believed to slow the initiation and progression of atherosclerosis. Alternatively spliced variants which encode different protein isoforms have been described; however, only one has been fully characterized. [provided by RefSeq, Jul 2008] ; PHENOTYPE: Homozygotes for a null allele show prenatal and postnatal lethality. Homozygotes for a different null allele are viable but show altered lipid and bile acid metabolism, impaired mitochondrial respiration, and increased susceptibility to diet-induced atherosclerosis, gallstone formation, and obesity. [provided by MGI curators]
• Posted On: 2014-05-07