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Phagocytic ability declines with age in adult Drosophila hemocytes

机译:成年果蝇血细胞吞噬能力随年龄下降

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摘要

Most multicellular organisms show a physiological decline in immune function with age. However, little is known about the mechanisms underlying these changes. We examined Drosophila melanogaster, an important model for identifying genes affecting innate immunity and senescence, to explore the role of phagocytosis in age-related immune dysfunction. We characterized the localized response of immune cells at the dorsal vessel to bacterial infection in 1-week- and 5-week-old flies. We developed a quantitative phagocytosis assay for adult Drosophila and utilized this to characterize the effect of age on phagocytosis in transgenic and natural variant lines. We showed that genes necessary for bacterial engulfment in other contexts are also required in adult flies. We found that blood cells from young and old flies initially engulf bacteria equally well, while cells from older flies accumulate phagocytic vesicles and thus are less capable of destroying pathogens. Our results have broad implications for understanding how the breakdown in cellular processes influences immune function with age.
机译:随着年龄的增长,大多数多细胞生物都显示出免疫功能的生理下降。但是,对于这些变化的潜在机制知之甚少。我们研究了果蝇果蝇(Drosophila melanogaster),一种用于鉴定影响先天免疫和衰老的基因的重要模型,以探索吞噬作用在与年龄相关的免疫功能障碍中的作用。我们表征了1周龄和5周龄的苍蝇背侧免疫细胞对细菌感染的局部反应。我们开发了成年果蝇的定量吞噬作用测定法,并利用它来表征年龄对转基因和天然变异系中吞噬作用的影响。我们显示成年果蝇还需要在其他情况下细菌吞噬所需的基因。我们发现,年轻苍蝇和老苍蝇的血细胞最初同样会吞噬细菌,而老苍蝇的细胞会积聚吞噬小泡,因此破坏病原体的能力较弱。我们的结果对于理解细胞过程中的衰老如何影响免疫功能随年龄增长具有广泛意义。

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