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卵黄蛋白原家族基因的表达不会延长果蝇的寿命或繁殖力。

Vitellogenin family gene expression does not increase Drosophila lifespan or fecundity.

作者信息

Ren Yingxue, Hughes Kimberly A

机构信息

Department of Biological Science, Florida State University, Tallahassee, FL 32306, USA.

出版信息

F1000Res. 2014 Jun 10;3:125. doi: 10.12688/f1000research.3975.1. eCollection 2014.

Abstract

One of the most striking patterns in comparative biology is the negative correlation between lifespan and fecundity observed in comparisons among species. This pattern is consistent with the idea that organisms need to allocate a fixed energy budget among competing demands of growth, development, reproduction and somatic maintenance. However, exceptions to this pattern have been observed in many social insects, including ants, bees, and termites.  In honey bees ( Apis mellifera), Vitellogenin ( Vg), a yolk protein precursor, has been implicated in mediating the long lifespan and high fecundity of queen bees. To determine if Vg-like proteins can regulate lifespan in insects generally, we examined the effects of expression of Apis Vg and Drosophila CG31150 (a Vg-like gene recently identified as cv-d) on Drosophila melanogaster lifespan and fecundity using the RU486-inducible GeneSwitch system. For all genotypes tested, overexpression of Vg and CG31150 decreased Drosophila lifespan and did not affect total or age-specific fecundity. We also detected an apparent effect of the GeneSwitch system itself, wherein RU486 exposure (or the GAL4 expression it induces) led to a significant increase in longevity and decrease in fecundity in our fly strains. This result is consistent with the pattern reported in a recent meta-analysis of Drosophila aging studies, where transgenic constructs of the UAS/GAL4 expression system that should have no effect (e.g. an uninduced GeneSwitch) significantly extended lifespan in some genetic backgrounds. Our results suggest that Vg-family genes are not major regulators of Drosophila life history traits, and highlight the importance of using appropriate controls in aging studies.

摘要

比较生物学中最显著的模式之一是在物种间比较时观察到的寿命与繁殖力之间的负相关。这种模式与生物体需要在生长、发育、繁殖和体细胞维持等相互竞争的需求之间分配固定能量预算的观点一致。然而,在包括蚂蚁、蜜蜂和白蚁在内的许多社会性昆虫中都观察到了这种模式的例外情况。在蜜蜂(西方蜜蜂)中,卵黄原蛋白(Vg),一种卵黄蛋白前体,被认为在介导蜂王的长寿和高繁殖力方面发挥作用。为了确定Vg样蛋白是否一般能调节昆虫的寿命,我们使用RU486诱导型基因开关系统研究了西方蜜蜂Vg和果蝇CG31150(最近被鉴定为cv-d的一个Vg样基因)的表达对黑腹果蝇寿命和繁殖力的影响。对于所有测试的基因型,Vg和CG31150的过表达降低了果蝇的寿命,并且不影响总繁殖力或特定年龄的繁殖力。我们还检测到了基因开关系统本身的明显影响,其中在我们的果蝇品系中,暴露于RU486(或其诱导的GAL4表达)导致寿命显著增加和繁殖力下降。这一结果与最近一项果蝇衰老研究的荟萃分析中报道的模式一致,在该分析中,本应无作用的UAS/GAL4表达系统的转基因构建体(例如未诱导的基因开关)在某些遗传背景下显著延长了寿命。我们的结果表明,Vg家族基因不是果蝇生活史特征的主要调节因子,并强调了在衰老研究中使用适当对照的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a26b/4111121/737e2da15e07/f1000research-3-4260-g0000.jpg

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