Table 2.
Association of a burden of rare mutations in the low-density lipoprotein receptor (LDLR) gene with risk for early-onset myocardial infarction
| Mutation set | N cases/controls | T1 cases | T1 controls | % freq cases | % freq controls | OR | P |
|---|---|---|---|---|---|---|---|
| Non-synonymous | 4,703/5,090 | 285 | 208 | 6.1 | 4.1 | 1.5 | 4 × 10−6 |
| Deleterious (PolyPhen) | 4,703/5,090 | 148 | 67 | 3.1 | 1.3 | 2.4 | 1 × 10−11 |
| Deleterious (Broad) | 4,703/5,090 | 243 | 158 | 5.2 | 3.1 | 1.7 | 9 × 10−8 |
| Deleterious (Strict) | 4,703/5,090 | 90 | 23 | 1.9 | 0.45 | 4.2 | 3 × 10−11 |
| Disruptive | 4,703/5,090 | 24 | 2 | 0.51 | 0.039 | 13.0 | 9 × 10−5 |
Summary allele counts and carrier frequencies are shown. Only SNVs and indels with minor allele frequency less than 1% were considered in burden analysis. “Deleterious (PolyPhen)” as defined by nonsense, splice-site, indel frameshift, and missense annotated as “possibly damaging” or “probably damaging” by PolyPhen-2 HumDiv software; “Deleterious (Broad)” as defined by nonsense, splice-site, indel frameshift, and missense annotated as deleterious by at least one of the five protein prediction algorithms of LRT score, MutationTaster, PolyPhen-2 HumDiv, PolyPhen-2 HumVar and SIFT; “Deleterious (Strict)” as defined by nonsense, splice-site, indel frameshift, and missense annotated as deleterious by all five protein prediction algorithms; Disruptive defined as nonsense, splice-site or indel frameshift; T1: Alleles with SNVs or indels with minor allele frequency less than 1%; % freq: percentage of cases or controls carrying a T1 allele; OR: odds ratio.