All variants in the LDLR gene

Information The variants shown are described using the NM_000527.4 transcript reference sequence.

2 entries on 1 page. Showing entries 1 - 2.
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Effect     

Exon     

AscendingDNA change (cDNA)     

RNA change     

Protein     

P-domain     

Enzyme activity     

Predict-BioInf     

Classification method     

Clinical classification     

DNA change (genomic) (hg19)     

DNA change (hg38)     

Published as     

ISCN     

DB-ID     

Variant remarks     

Reference     

ClinVar ID     

dbSNP ID     

Origin     

Segregation     

Frequency     

Re-site     

VIP     

Methylation     

Owner     
+?/+? 9 c.1297G>C r.(?) p.(Asp433His) LDL-receptor class B1 - PolyphenII: probably damaging, 0.999, HumVar probably damaging, 0.977; SIFT: Not tolerated, SIFT2 Not tolerated; MutationTaster: disease causing; conservation: 0.982 (Ch, Rh, D, P, B, M, Ra, H, Rb, Ck, X, Z, S) ACGS likely pathogenic g.11224064G>C g.11113388G>C D412H - LDLR_001390 Impared processing and rapid degradation of peptide in Hmz fibroblasts & COS cells PubMed: Miyake 1992 - rs121908036 Germline - not in ExAC, May 2015 - - - Sarah Leigh
+?/+? 9 c.1297G>C r.(?) p.(Asp433His) LDL-receptor class B1 - PolyphenII: probably damaging, 0.999, HumVar probably damaging, 0.977; SIFT: Not tolerated, SIFT2 Not tolerated; MutationTaster: disease causing; conservation: 0.982 (Ch, Rh, D, P, B, M, Ra, H, Rb, Ck, X, Z, S) ACGS likely pathogenic g.11224064G>C g.11113388G>C D412H - LDLR_001390 Segregation reported, Impared processing and rapid degradation of receptor {PMID1446662:Miyake et al 1992 Eur J Biochem 210 1}. PubMed: Mozas 2004 - rs121908036 Germline - not in ExAC, May 2015 - - - Sarah Leigh
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