A lead selection algorithm was applied to find optimal recording sites for limited lead body surface potential maps. The studied population consisted of a set of 117 lead body surface potential maps recorded from 744 subjects (229, normal; 278, with myocardial infraction [MI]; and 237, with left ventricular hypertrophy [LVH]). One generic lead set derived from all disease groups was found. Also found were 3 disease-specific lead sets (normal, MI, and LVH) and one specific to abnormal subjects (MI and LVH combined). The performance of each lead set in estimating data from other disease groups was largely similar. This was with the exception of leads specific to LVH in the estimation of normal data and normal leads in the estimation of LVH data. Here, the difference was found to be significant (P