摘要

Mapping markers from linkage data continues to be a task performed in many, genetic epidemiological studies. Data collected in a study may be used to refine published map estimates and a study may use markers that do not appear in an), published map. Furthermore, inaccuracies in meiotic maps can Seriously bias linkage findings. To make best use of the available marker information, multilocus linkage analyses are performed. However, two computational issues greatly limit the number of markers currently mapped jointly; the number of candidate marker orders increases exponentially with marker number and computing exact multilocus likelihoods on general pedigrees is computationally demanding In this article, a new Markov chain Monte Carlo (MCMC approach that solves both these computational problems is presented. The MCMC approach allows many markers to be mapped jointly, using data observed on general pedigrees with unobserved individuals. The performance Of the new mapping procedure is demonstrated through the analysis of simulated and real data. The MCMC procedure performs extremely well, even when there are millions of candidate orders, and gives results superior to those of CRI-MAP.

  • 出版日期2005-10