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. 1991 Oct 3;353(6343):437-40.
doi: 10.1038/353437a0.

A product of the prune locus of Drosophila is similar to mammalian GTPase-activating protein

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A product of the prune locus of Drosophila is similar to mammalian GTPase-activating protein

D H Teng et al. Nature. .

Abstract

The X-linked prune (pn) eye-colour mutation of Drosophila melanogaster has a highly specific, complementary lethal interaction with the conditional dominant Killer of prune (awdK-pn) mutation. Although awdK-pn flies have no apparent phenotype on their own, pn awdK-pn double mutants die as second or third larval instars. The awd locus encodes a nucleoside diphosphate kinase, an enzyme that catalyses the transfer of high-energy phosphate bonds between nucleoside diphosphates and nucleoside triphosphates, which is essential for the normal development of Drosophila. Analysis of the pn locus has suggested that the complementary DNA, TcD37, encodes a putative pn+ product. Here we report the nucleotide sequence of TcD37 and the similarity of its deduced protein product to the catalytic domain of mammalian GTPase-activating proteins (GAPs); GAPs stimulate the GTPase activity of Ras (ref. 6), which are plasma membrane-bound proteins involved in the regulation of cell proliferation and differentiation. These results suggest that the Drosophila TcD37 protein participates in a biochemical pathway similar to that of Ras and GAPs in mammals and yeast. We propose that the interaction between pn and awd is due to a neomorphic mutation that enhances the ability of AwdK-pn nucleoside diphosphate kinase to induce a regulatory GTPase into a GTP-bound 'on' state, whereas Pn modulates the activity of this GTPase either by switching it to a GDP-bound 'off' state or by interfering with its effector function.

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  • Ras and the awd couple.
    Ruggieri R, McCormick F. Ruggieri R, et al. Nature. 1991 Oct 3;353(6343):390-1. doi: 10.1038/353390a0. Nature. 1991. PMID: 1654523 No abstract available.
  • Prune function?
    Barnes TM, Bürglin TR. Barnes TM, et al. Nature. 1992 Feb 6;355(6360):504-5. doi: 10.1038/355504b0. Nature. 1992. PMID: 1741029 No abstract available.

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