Abnormalities in cell proliferation and apico-basal cell polarity are separable in Drosophila lgl mutant clones in the developing eye |
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Authors: | Grzeschik Nicola A Amin Nancy Secombe Julie Brumby Anthony M Richardson Helena E |
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Affiliation: | a Peter MacCallum Cancer Center, Melbourne, Victoria, Australia b Anatomy and Cell Biology Department, University of Melbourne, Melbourne, Victoria, Australia c Genetics Department, University of Adelaide, Adelaide, South Australia, Australia |
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Abstract: | In homozygous mutants of Drosophila lethal-2-giant larvae (lgl), tissues lose apico-basal cell polarity and exhibit ectopic proliferation. Here, we use clonal analysis in the developing eye to investigate the effect of lgl null mutations in the context of surrounding wild-type tissue. lgl− clones in the larval eye disc exhibit ectopic expression of the G1-S regulator, Cyclin E, and ectopic proliferation, but do not lose apico-basal cell polarity. Decreasing the perdurance of Lgl protein in larval eye disc clones, by forcing extra proliferation of lgl− tissue (using a Minute background), leads to a loss in cell polarity and to more extreme ectopic cell proliferation. Later in development at the pupal stage, lgl mutant photoreceptor cells show aberrant apico-basal cell polarity, but this is not associated with ectopic proliferation, presumably because cells are differentiated. Thus in a clonal context, the ectopic proliferation and cell polarity defects of lgl− mutants are separable. Furthermore, lgl− mosaic eye discs have alterations in the normal patterns of apoptosis: in larval discs some lgl− and wild-type cells at the clonal boundary undergo apoptosis and are excluded from the epithelia, but apoptosis is decreased elsewhere in the disc, and in pupal retinas lgl− tissue shows less apoptosis. |
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Keywords: | Drosophila Eye development Proliferation Apico-basal cell polarity Apoptosis lgl cyclin E |
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