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Abnormalities in cell proliferation and apico-basal cell polarity are separable in Drosophila lgl mutant clones in the developing eye
Authors:Grzeschik Nicola A  Amin Nancy  Secombe Julie  Brumby Anthony M  Richardson Helena E
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
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.
Keywords:Drosophila   Eye development   Proliferation   Apico-basal cell polarity   Apoptosis   lgl   cyclin E
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