The full EM algorithm for the MLEs of QTL effects and positions and their estimated variances in multiple-interval mapping.

The advent of complete genetic linkage maps of DNA markers has made systematic studies of mapping quantitative trait loci (QTL) in experimental organisms feasible. The method of multiple-interval mapping provides an appropriate way for mapping QTL using genetic markers. However, efficient algorithms for the computation involved remain to be developed. In this article, a full EM algorithm for the simultaneous computation of the MLEs of QTL effects and positions is developed. EM-based formulas are derived for computing the observed Fisher information matrix. The full EM algorithm is compared with an ECM algorithm developed by Kao and Zeng (1997, Biometrics 53, 653-665). The validity of the inverted observed Fisher information matrix as an estimate of the variance matrix of the MLEs is demonstrated by a simulation study.