Table 1.
Results of linkage analyses of replicate 4 using redefined affection status.
| Results from linkage analyses | Type of marker set | |||
| STR-7.5 cM | SNP-3 cM | SNP-1 cM | SNP-0.3 cM | |
| Information contenta | 0.90 | 0.79 | 0.87 | 0.96 |
| Two-point LOD scoreb | 3.91 | 2.22 | 2.22 | 3.19 |
| Multipoint Zmax/NPL p-valuesc | ||||
| GENEHUNTER | ||||
| NPL p-value | 0.000021 | 0.0026 | 3.23e-06 | 2.16e-07 |
| Multipoint HLOD (α) | 3.65 (1.00) | 2.45 (0.96) | 5.93 (1.00) | 6.36 (1.00) |
| MERLIN | ||||
| NPL p-value | <0.00001 | 0.00004 | <0.00001 | <0.00001 |
| SIMWALK2 | ||||
| NPL p-value | 0.0001 | 0.0066 | 0.0012 | NDe |
| SIBPAL | ||||
| p-value | 5.8 × 10-7 | 9.5 × 10-8 | 4.8 × 10-6 | 7.0 × 10-7 |
| 1-LOD interval (cM)d | 5.23 | 12.55 | 8.16 | 7.54 |
aAveraged information content estimated from all markers on STR, SNP-1 cM, SNP-0.3 cM marker sets and the telomeric 50 markers on SNP-3 cM map using the entropy function in MERLIN.
bReflected the highest LOD scores obtained at the telomeric region.
cLinkage signal at the telomeric region of chromosome 3 was successfully detected by all marker panels. LOD scores and p-values reflected the most significant results for each panel.
dEstimated from multipoint LOD-score curves obtained from GENEHUNTER analyses.
eNot determined because of the failure in convergence.