Incidental Mutation 'N/A - 287:Sorl1'

• ID: 168
• Institutional Source: Beutler Lab
• Gene Symbol: Sorl1
• Ensembl Gene: ENSMUSG00000049313
• Gene Name: sortilin-related receptor, LDLR class A repeats-containing
• Synonyms: Sorla, mSorLA, LR11, 2900010L19Rik
• Essential gene?: Possibly non essential (E-score: 0.319)
• Stock #: N/A - 287 of strain 287
• Status: Validated
• Chromosome: 9
• Chromosomal Location: 41876016-42035593 bp(-) (GRCm39)
• Type of Mutation: nonsense
• DNA Base Change (assembly): A to T at 41952892 bp (GRCm39)
• Zygosity: Homozygous
• Amino Acid Change: Cysteine to Stop codon at position 716 (C716*)
• Ref Sequence: ENSEMBL: ENSMUSP00000058613
• Gene Model: predicted gene model for transcript(s): [ENSMUST00000060989]
• AlphaFold: O88307
• Predicted Effect: probably null; Transcript: ENSMUST00000060989; AA Change: C716*
• SMART Domains: Protein: ENSMUSP00000058613; Gene: ENSMUSG00000049313; AA Change: C716*

Domain	Start	End	E-Value	Type
signal peptide	1	28	N/A	INTRINSIC
VPS10	124	757	N/A	SMART
LY	780	822	9.33e-6	SMART
LY	824	866	2.38e-12	SMART
LY	867	912	1.87e-5	SMART
LY	913	953	1.08e-10	SMART
LY	954	993	5.43e0	SMART
EGF_like	1020	1072	2.8e1	SMART
LDLa	1077	1114	1.76e-14	SMART
LDLa	1116	1155	5.34e-14	SMART
LDLa	1157	1194	1.67e-15	SMART
EGF_like	1198	1236	4.93e1	SMART
LDLa	1198	1237	3.83e-15	SMART
LDLa	1238	1273	1.99e-13	SMART
LDLa	1274	1317	2.53e-6	SMART
LDLa	1324	1361	4.34e-14	SMART
LDLa	1367	1405	1.14e-13	SMART
LDLa	1418	1455	3.34e-15	SMART
LDLa	1470	1508	1.09e-10	SMART
LDLa	1513	1551	1.09e-10	SMART
FN3	1555	1638	4.19e-4	SMART
FN3	1651	1732	7.23e-8	SMART
FN3	1747	1830	4.8e0	SMART
FN3	1842	1920	3e1	SMART
FN3	1933	2016	6.01e-5	SMART
FN3	2025	2107	2.03e-2	SMART
transmembrane domain	2137	2159	N/A	INTRINSIC
low complexity region	2188	2199	N/A	INTRINSIC

• Meta Mutation Damage Score: 0.9755
• Coding Region Coverage:
  • 1x: 88.3%
  • 3x: 72.3%
• Validation Efficiency: 81% (138/170)
• MGI Phenotype: FUNCTION: [Summary is not available for the mouse gene. This summary is for the human ortholog.] This gene encodes a mosaic protein that belongs to at least two families: the vacuolar protein sorting 10 (VPS10) domain-containing receptor family, and the low density lipoprotein receptor (LDLR) family. The encoded protein also contains fibronectin type III repeats and an epidermal growth factor repeat. The encoded preproprotein is proteolytically processed to generate the mature receptor, which likely plays roles in endocytosis and sorting. Mutations in this gene may be associated with Alzheimer's disease. [provided by RefSeq, Feb 2016] ; PHENOTYPE: Homozygous mutation of this gene results in decreased femoral artery intimal thickness after cuff placement and abolished angiotensin II stimulated vascular smooth muscle migration and attachment. Two other alleles show an increase in beta-amyloid deposits or peptide in the brain. [provided by MGI curators]
• Allele List at MGI:

  All alleles(15) : Targeted, knock-out(2) Gene trapped(13)

• Posted On: 2010-04-08

Nature of Mutation

DNA sequencing using the SOLiD technique identified a T to A transversion at position 2324 of the Sorl1 transcript in exon 4 of 4 total exons.  Four transcripts of the Sorl1 gene are displayed on Ensembl. The mutated nucleotide introduces a premature stop codon at cysteine 716 of the encoded protein. The mutation has been confirmed by DNA sequencing using the Sanger method (Figure 1).

Protein Function and Prediction

The Sorl1 gene encodes a 2215 amino acid single-pass type I membrane protein that is likely to be a multifunctional endocytic receptor implicated in the uptake of lipoproteins and proteases. The Sortilin-related receptor or sorting protein-related receptor (sorLA) binds LDL, the major cholesterol-carrying lipoprotein of plasma, and transports it into cells by endocytosis. It is abundantly expressed in brain and detectable in kidney, spleen, skeletal muscle and lung. SorLA contains five BNR repeats, five LDL-receptor class B repeats, eleven LDL-receptor class A domains, six fibronectin type III domains, and one EGF-like domain. All of these domains are extracellular (Uniprot O88307). Homozygotes for a targeted null allele are generally normal, but exhibit increased beta-amyloid levels and display deficiencies in angiotensin II-induced vascular smooth muscle cell migration.

 

The C716X change truncates the protein after the fifth BNR repeat and prior to the first LDL-receptor class B repeat.