TY  - GEN
T1  - me98 is a new allele of rad-54
AU  - Roelens, Baptiste
AU  - Zawadzki, Karl A
AU  - Villeneuve, Anne M
DO  - 10.17912/micropub.biology.000108
UR  - http://beta.micropublication.org/journals/biology/micropub-biology-000108/
AB  - We isolated the me98 mutant in a genetic screen for C. elegans mutants with an altered number of GFP::COSA-1 foci, which mark the sites of crossovers in wild-type C. elegans germ cells (Rosu et al. 2013). After multiple rounds of outcrossing, we confirmed that the me98 mutant is defective in meiotic prophase as i) chromosomes in diakinesis oocytes appear partially decondensed and structurally compromised (Fig. 1A), ii) me98 fails to form the six GFP::COSA-1 foci observed in wild-type late pachytene meiocytes (Fig. 1B) and iii) me98 accumulates RAD-51 foci during the course of meiotic prophase (Fig. 1C). Further, 100% of eggs laid by me98 mutant hermaphrodites are inviable. These defects are reminiscent of those caused by the previously-described rad-54(ok615) mutation (Mets and Meyer 2009), and sequencing of the rad-54 locus in me98 mutants revealed the presence of a 13bp deletion in the second exon of the annotated transcript (I:9065652 to I:9065664 of WS269). This lesion creates a frameshift that would result in premature termination of translation in the third exon (of seventeen) of the predicted transcript (Fig. 1D), suggesting that it is likely a null allele. Of note, the previously described rad-54 loss-of-function allele, ok615, is an insertion/deletion that also affects the neighboring gene snx-3 (Fig 1E). As gonads of rad-54(me98) mutants appear overall healthier than those in the ok615 mutant, me98 could be a valuable tool to analyze the specific function of rad-54.
PY  - 2019
JO  - microPublication Biology
ER  -