ALLELE-SPECIFIC AND HAPLOID-SPECIFIC PRODUCT GENERATED BY ALTERNATIVE SPLICING FROM A MOUSE T-COMPLEX-RESPONDER LOCUS CANDIDATE

MOUSE t haplotypes represent a variant form of chromosome 17 that has evolved the ability to propagate through natural populations by the phenomenon of 'transmission ratio distortion' (TRD), in which heterozygous +/t males transmit their t-carrying chromosome to 95% or more of their offspring 1,2. Although multiple t-associated loci have a role in expression of this phenotype, only one-the t complex responder (Tcr) locus-is responsible for determining which of the two homologues of chromosome 17 will be transmitted at a high ratio 3. A candiate gene (Tcp-10b) for Tcr that is expressed in both meiotic and post-meiotic male germ cells has been cloned 4. But for this candiate gene to function as the haploid effector of TRD, the t-allele of this gene (Tcp-10b(t)) must express a unique product in a haploid-specific manner. Here we show that a change in the splicing pattern of Tcp-10b(t) transcripts occurs during sperm differentiation. This change results in a unique allele-specific and haploid-specific transcript which could encode a variant polypeptide that would fulfil the conditions required of the Tcr effector of TRD.