The site of function of the Y chromosome in Drosophila melanogaster males

Summary The Y chromosome is essential for fertility in D. melanogaster males. An analysis of 126 pal-induced Y chromosome mosaics indicated that its function is only required in the germ line of fertile males. This analysis also showed that approximately 1/4 of all pal-induced Y chromosome mosaics had an XO/XYY constitution and hence that they resulted from somatic nondisjunction. Preliminary evidence suggests that pal-induced somatic nondisjunction can occur at the second or subsequent cleavage divisions.     

Dopa decarboxylase from Drosophila melanogaster

Summary Dopa decarboxylase (EC 4.1.1.26) has been purified to near homogeneity from mature larvae of Drosophila melanogaster. The enzyme has a molecular weight of 113,000 measured by sucrose gradient sedimentation and 102,000 measured by variable porosity acrylamide gel electrophoresis. Electrophoresis under denaturing conditions revealed the enzyme consists of two subunits of molecular weight 54,000. The affinity of the enzyme for L-dopa is 30-fold greater than for L-tyrosine. Activity is strongly inhibited by heavy metal ions and the sulfhydryl reagent N-ethylmaleimide. N-acetyl dopamine acts as a competitive inhibitor of the enzyme.Antibodies were elicited against the purified enzyme and measurements of the amount of cross-reacting material (CRM) in two groups of mutants were made. The first group comprised the recessive lethal mutants l(2)amd. Heterozygous mutant stocks are hypersensitive to -methyl dopa, an inhibitor of dopa decarboxylase. These stocks were found to have nearly normal amounts of CRM and enzyme activity.A second group of recessive lethal mutants, characterized by lower levels of dopa decarboxylase, was also analysed. These mutants, designated l(2) Ddc, as heterozygotes exhibited CRM levels between 25 and 75% of normal. Although they are alleles at a single locus, they were classifiable into three distinct groups whose properties readily could be ascribed to a homodimeric structure of the enzyme. This structure would also account for the pattern of intracistronic complementation exhibited by the mutants. Finally, the severity of the mutant defects, as judged by our measurements of CRM and activity, closely parallels that deduced from their complementation pattern. We conclude that these mutations are lesions in the structural gene for dopa decarboxylase.     

Homology between Drosophila melanogaster and Escherichia coli ribosomal proteins

Summary Antibodies raised against D. melanogaster ribosomal proteins were used to examine possible structural relationships between eukaryotic and prokaryotic ribosomal proteins. The antisera were raised against either groups of ribosomal proteins or purified individual ribosomal proteins from D. melanogaster. The specificity of each antiserum was confirmed and the identity of the homologous E. coli ribosomal protein was determined by immunochemical methods. Immuno-overlay assays indicated that the antiserum against the D. melanogaster small subunit protein S14 (anti-S14) was highly specific for protein S14. In addition, anti-S14 showed a cross-reaction with total E. coli ribosomal proteins in Ouchterlony double immunodiffusion assays and with only E. coli protein S6 in immuno-overlay assays. From these and other experiments with adsorption of anti-S14 with individual purified proteins, the E. coli protein homologous to the D. melanogaster protein S14 was established as protein S6.     

Ethyl methanesulfonate-induced mutants in the Y chromosome of Drosophila melanogaster

Male sterility mutants have been induced in the Y chromosome by treatment with ethyl methanesulfonate. Complementation tests with deficient Y chromosome tester stocks revealed that many of the mutant Y chromosomes were deficient for more than one male fertility locus. Cytological analysis showed that in two cases of multiple deficiency the long arm of the Y chromosome was grossly reduced in size. Several of the mutant Y chromosomes were sensitive to the temperature at which males were reared, males being partially fertile when reared at 18° and sterile when reared at 25°.     

Third chromosome suppressor of position-effect variegation loci in Drosophila melanogaster

Summary As a result of a genetic analysis of 63 third chromosome suppressor mutations of position-effect variegation 12 different loci showing dominant suppression have been identified and their map positions determined. A compilcation of the genetic data available for each suppressor locus is given. The strong suppressor effects of the mutations have been quantified by measurements of white variegation inw ^m4h /w ^m4h ,w ^m4h /Y andw ^m4h /O flies. Mutant alleles of three loci were found in these studies to dominate over the strong enhancer effect of complete loss of the Y chromosome. Most of the identified loci suppressing position-effect variegation represent essential genetic funtions; only three loci represent nonessential functions. Mutations of two loci display recessive butyrate sensitivity and lethal interaction with the heterochromatic Y chromosome suggesting that these genes affect chromosomal condensation. Studies with deficiencies and triploids revealed that most of the loci represent haplo-abnormal suppressor functions. The use of the isolated mutant material for genetic, developmental and molecular studies of processes connected with gene inactivation in position-effect variegation is discussed.Dedicated to Prof. H.J. Becker on the occasion of his 6th birthday     

The genetics of dopa decarboxylase in Drosophila melanogaster

Summary Data on 46 mutations in the structural gene, Ddc. for dopa decarboxylase and 33 mutations in the methyl dopa hypersensitive gene, 1(2)amd, in Drosophila melanogaster are presented including information on their isolation, their effects on DDC activity, and their sensitivity to dietary methyl dopa. Intragenic complementation of both loci is documented, the effects of heteroallelic complementing heterozygosity on DDC activity, in vitro thermolability of DDC, and on temperature sensitive viability are presented. Data are marshalled to support rejection of the hypothesis that Ddc mutations and 1(2)amd, mutations are lesions in a single gene.     

Body-weight and chromosome aberrations induced by X-rays in somatic cells of Drosophila melanogaster

Summary Variations in suppression efficiency were observed among nonsense mutations at different locations within the lysozyme gene (e) of T4 phage. The present experiments using three amber mutants in lysozyme gene indicate such variations presumably depend upon the base sequences neighboring to the nonsense mutations.Part of this work is the thesis work of one of the authors (E.A.) and was reported at the Annual Meeting (1968) of Genetic Society of Japan     

Paucimannose N-glycans in Caenorhabditis elegans and Drosophila melanogaster

There is a rich diversity of paucimannose N-glycans in worms and flies, and these may play a role in the survival of these organisms. Although paucimannose N-glycans are not expressed in vertebrates, complex N-glycans may take over some of the functions of paucimannose N-glycans. Identification of the target proteins of β-1,2-N-acetylglucosaminyltransferase I (GnTI) in worms and flies and elucidation of their functions may thus lead to a better understanding of the role of GnTI-dependent glycoproteins in the survival/longevity of both invertebrates and vertebrates.     

The allelic forms of three larval salivary proteins from Drosophila melanogaster

Summary Sodium dodecyl sulphate (SDS) gel electrophoresis shows distinct differences in the number and mobility of the major salivary proteins produced by various stocks of Drosophila melanogaster. Genetic analysis showed that the variation was due to the presence of allelic forms of these proteins and demonstrated the absence of certain types of modifying genes. The variation in the mobility of two non-allelic proteins is so large that it is not possible to group variants of these proteins into specific mobility classes. Some results from the genetic analysis of these variants are of relevance to similar analyses of groups of genes determining related proteins in Drosophila.     

Comparison between rDNA magnification and bb lethal mutation frequencies in Drosophila melanogaster

Summary Unequal mitotic sister strand crossing over has been evoked to explain the occurrence of phenotypically bb ^- males in the progeny of phenotypically bobbed males during magnification. If this is the case, complementary bb ¹ loci should be obtained together with the bb ¹. To test this hypothesis we compared the frequency of bb lethal mutations in the sperms of bb males with the percentage of phenotypically bb ⁺ males obtained during magnification of these bb males. We then compared these values with those occurring in phenotypically bb ⁺ control males. We found that, while the number of bb ⁺ males obtained during magnification, though variable, is high, the bb lethal mutation occurs at a very low frequency in all the genetic conditions, whatever the phenotype of the parental male.     

The action of the Notch locus in Drosophila melanogaster

Summary It is shown that the Notch⁸ deficiency in Drosophila melanogaster affects a number of enzyme activities localized in the mitochondria, such as NADH oxidase (activity of the complete respiratory chain), NADH dehydrogenase (the first step in the respiratory chain before transfer to ubiquinone), Succinate dehydrogenase and -Glycerophosphate dehydrogenase. The experiments reported here do not exclude the possibility of involvement of other genes in the deficiency. The effect of duplications of the Notch locus on NADH oxidase and NADH dehydrogenase suggest that this locus determines the enzyme activities.The dosage effects of the Notch locus on activity suggest that this locus contains the structural genes for these enzymes.     

The sibling species Drosophila melanogaster and Drosophila simulans differ in the expression profile of glutathione S-transferases

Two major forms of glutathione S-transferase are known in Drosophila melanogaster: GST D and GST 2. In the present paper we report the existence of a third major form of glutathione S-transferase in Drosophila simulans. Induction with phenobarbital revealed a different regulation of GST between these species. Despite the fact that these two species are closely related, there was a difference in the expression profile of the enzyme implicated in the detoxification system, suggesting variations in capacity to suit their environment.     

Elements causing hybrid dysgenesis on the second chromosome ofDrosophila melanogaster

Summary Hybrid dysgenesis inDrosophila melanogaster is a syndrome of germline abnormalities including temperature-dependent gonadal dysgenesis (GD sterility), high rates of mutation and male recombination. In theP-M system, hybrid dysgenesis results from interaction between chromosomally-linked factors (P factors) and a particular extrachromosomal state refered to as theM cytotype. TheT007/Cy strain, shown by other authors to induce a high level of mutation and male recombination, is presently studied with respect to gonadal dysgenesis. TheP activity appears mainly linked with theT007 second chromosome and has been essentially mapped to a 0.6 centimorgan long interval, i.e. betweenhk andpr. On the other hand, 14 strains balanced for deficiencies on the left arm of the second chromosome are studied for their relative level ofM cytotype activity.In F1 females, inheriting the same maternal cytotype and the same paternalT007 chromosome, significant differences inGD sterility are found between flies receiving the maternal deficiency and those receiving the alternate non-deleted chromosome. This effect appears only when the chromosomes are deleted for a common region (37F5-38A7), suggesting the presence of elements intervening in the determinism ofGD sterility in this zone. As this region is included in the correspondinghk-pr interval (37C1-38B6), these results state the problem of the nature of the elements located in this interval and two hypotheses are discussed.     

Genetic instability at the cut locus of Drosophila melanogaster induced by the MR-h12 chromosome

Summary Unstable mutations were generated at the cut locus by the MR-h12 factor which induces male recombination. The unstable allele ct ^MR2, containing the MR-transposon in the cut locus is a very powerful mutator producing a number of different viable and lethal mutations both in the cut locus and outside it.I describe several types of mutations: stable reversion to wild type, which were sometimes associated with the appearance of unstable mutations in other loci; of stable deficiencies at the cut locus (lethals); new unstable mutations at different loci with the ct ^MR2 allele conserved; new unstable cut alleles with a phenotype other than that of ct ^MR2. The possible mechanisms of these mutational events are discussed. The genetic system constructed in the present work affords an opportunity for molecular studies of the cut locus and the MR-transposon, as a sequence from the cut locus has recently been cloned (Tchurikov et al. 1981).