Worm Breeder's Gazette 3(1): 17

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Further Studies with the X-linked Lethals

P. Meneely, B. Herman

Figure 1

Among 28,647 F1 progeny of X-irradiated N2 males, we have found 17 
deficiencies of the unc-3 region, and have used these in mapping the 
lethals.  Thirteen of these deficiencies fail to complement all 
mutants in the region.  The map shown is based on the remaining four 
deficiencies and on three-point crosses involving unc-3, 
lethals; the positions found by recombination 
are consistent with the deficiency map.
[See Figure 1]
These fourteen essential genes are defined by twenty-three lethals; 
a fifteenth gene, let-5, is either to the left of unc-3 or to the 
right of let-2.  Three of the lethals have been sent to us by other 
labs; one of these, e1471, provided by Andras Fodor, is the only 
allele of let-15.  The other two alien lethals, e1470 and b246ts, 
provided by Andras and by Judy Kimble respectively, are alleles of let-
2.  Counting these two, we have six alleles of let-2, all of which are 
temperature-sensitive.  For five of the six, the restrictive 
temperature is 20 C; for the sixth, b246, it is 25 C.  Complementation 
at 20 C is complex, with each mutant complementing at least one other; 
all fail to complement at 25 C.
We have also looked at the epistatic interaction between the 
hermaphrodite specific lethal let-7 and the transformer mutants tra-1 
and tra-2.  Homozygotes for let-7 die at about L3, while hemizygous 
males live to adulthood.  Since hemizygous hermaphrodites of the 
genotype unc-3 f1 also die as juveniles, the male 
survival does not appear to be due to having just one let-7 gene.  We 
then checked if the survival was male-specific by using 2X transformer 
males; that is, we made tra/+; unc-3 and 
looked for Unc male self-progeny.  They die at about the same stage as 
the homozygous hermaphrodites, suggesting that the interaction of let-
7 with the transformers is similar to that reported by Hodgkin and 
Brenner for the sex-influenced mutants dpy-21 and dpy-22.  We conclude 
that the action of let-7 is on 2X individuals regardless of sexual 
phenotype, but that the critical region of the X is not the let-7 gene 
itself nor, in fact, any gene in the region deficient in mnDf1.

Figure 1