Distinct requirements for the AP-3 adaptor complex in pigment granule and synaptic vesicle biogenesis in Drosophila melanogaster

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作者
C. Mullins
L. M. Hartnell
J. S. Bonifacino
机构
[1] Cell Biology and Metabolism Branch,
[2] National Institutes of Child Health and Human Development,undefined
[3] National Institutes of Health,undefined
[4] Building 18T/Room 101,undefined
[5] Bethesda,undefined
[6] MD 20892,undefined
[7] USA E-mail: juan@helix.nih.gov Tel.: +1-301-4966368; Fax: +1-301-402-0078,undefined
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Key words AP-3; Biogenesis; Pigment granule; Synaptic vesicle; Drosophila;
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摘要
The AP-3 adaptor protein complex has been implicated in the biogenesis of lysosome-related organelles, such as pigment granules/melanosomes, and synaptic vesicles. Here we compare the relative importance of AP-3 in the biogenesis of these organelles in Drosophila melanogaster. We report that the Drosophila pigmentation mutants orange and ruby carry genetic lesions in the σ3 and β3-adaptin subunits of the AP-3 complex, respectively. Electron microscopy reveals dramatic reductions in the numbers of electron-dense pigment granules in the eyes of these AP-3 mutants. Mutant flies also display greatly reduced levels of pigments housed in these granules. In contrast, electron microscopy of retinula cells reveals numerous synaptic vesicles in both AP-3 mutant and wild-type flies, while behavioral assays show apparently normal locomotor ability of AP-3 mutant larvae. Together, these results demonstrate that Drosophila AP-3 is critical for the biogenesis of pigment granules, but is apparently not essential for formation of a major population of synaptic vesicles in vivo.
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页码:1003 / 1014
页数:11
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