Requirements for Ectopic Homologous Recombination in Mammalian Somatic Cells

Abstract

Ectopic recombination occurs between DNA sequences that are not in equivalent positions on homologous chromosomes and has beneficial as well as potentially deleterious consequences for the eukaryotic genuine. In the present study, we have examined ectopic recombination in mammalian somatic (murine hybridoma) cells in which a deletion in the μ gene constant (Cμ) region of the endogenous chromosomal immunoglobulin μ gene is corrected by using as a donor an ectopic wild-type Cμ region. Ectopic recombination restores normal immunoglobulin M production in hybridomas. We show that (i) chromosomal μ gene deletions of 600 bp and 4 kb are corrected less efficiently than a deletion of only 2 bp, (ii) the minimum amount of homology required to mediate ectopic recombination is between 1.9 and 4.3 kb, (iii) the frequency of ectopic recombination dues not depend on donor copy number, and (iv) the frequency of ectopic recombination in hybridoma lines in which the donor and recipient Cμ regions are physically connected to each other on the same chromosome can be as much as 4 orders of magnitude higher than it is for the same sequences located on homologous or nonhomologous chromosomes. The results are discussed in terms of a model for ectopic recombination in mammalian somatic cells in which the scanning mechanism that is used to locate a homologous partner operates preferentially in cis.