Different levels of Ras activity can specify distinct transcriptional and morphological consequences in early Drosophila embryos

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JOURNAL ARTICLES

Different levels of Ras activity can specify distinct transcriptional and morphological consequences in early Drosophila embryos

S Greenwood and G Struhl
Howard Hughes Medical Institute, and Department of Genetics and Development, Columbia University College of Physicians and Surgeons, New York, NY 10032, USA.

The terminal portions of the Drosophila body pattern are specified by the localized activity of the receptor tyrosine kinase Torso (Tor) at each pole of the early embryo. Tor activity elicits the transcription of two 'gap' genes, tailless (tll) and huckebein (hkb), in overlapping but distinct domains by stimulating the Ras signal transduction pathway. Here, we show that quantitative variations in the level of Ras activity can specify qualitatively distinct transcriptional and morphological responses. Low levels of Ras activity at the posterior pole direct tll but not hkb transcription; higher levels drive transcription of both genes. Correspondingly, low levels of Ras activity specify a limited subset of posterior terminal structures, whereas higher levels specify a larger subset. However, we also show that the response to Ras activity is not uniform along the body. Instead, levels of Ras activity which suffice to drive tll and hkb transcription at the posterior pole fail to drive their expression in more central portions of the body, apparently due to repression by other gap gene products. We conclude that tll and hkb transcription, as well as the terminal structures, are specified by two inputs: a gradient of Ras activity which emanates from the pole, and the opposing influence of more centrally deployed gap genes which repress the response to Ras.

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				A. Stathopoulos and M. Levine Linear signaling in the Toll-Dorsal pathway of Drosophila: activated Pelle kinase specifies all threshold outputs of gene expression while the bHLH protein Twist specifies a subset Development, March 9, 2003; 129(14): 3411 - 3419. [Abstract] [Full Text] [PDF]

				D. del Alamo, J. Terriente, and F. J. Diaz-Benjumea Spitz/EGFr signalling via the Ras/MAPK pathway mediates the induction of bract cells in Drosophila legs Development, March 6, 2003; 129(8): 1975 - 1982. [Abstract] [Full Text] [PDF]

				C. Dossenbach, S. Rock, and M. Affolter Specificity of FGF signaling in cell migration in Drosophila Development, November 15, 2001; 128(22): 4563 - 4572. [Abstract] [Full Text] [PDF]

				K. Radke, K. Johnson, R. Guo, A. Davidson, and L. Ambrosio Drosophila-Raf Acts to Elaborate Dorsoventral Pattern in the Ectoderm of Developing Embryos Genetics, November 1, 2001; 159(3): 1031 - 1044. [Abstract] [Full Text] [PDF]

				K Halfar, C Rommel, H Stocker, and E Hafen Ras controls growth, survival and differentiation in the Drosophila eye by different thresholds of MAP kinase activity Development, January 5, 2001; 128(9): 1687 - 1696. [Abstract] [PDF]

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