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破译丽蝇蛹集金小蜂早期滞育的蛋白质组学特征。

Deciphering proteomic signatures of early diapause in Nasonia.

作者信息

Wolschin Florian, Gadau Jürgen

机构信息

School of Life Sciences, Arizona State University, Tempe, Arizona, United States of America.

出版信息

PLoS One. 2009 Jul 28;4(7):e6394. doi: 10.1371/journal.pone.0006394.

Abstract

Insect diapause is an alternative life-history strategy used to increase longevity and survival in harsh environmental conditions. Even though some aspects of diapause are well investigated, broader scale studies that elucidate the global metabolic adjustments required for this remarkable trait, are rare. In order to better understand the metabolic changes during early insect diapause, we used a shotgun proteomics approach on early diapausing and non-diapausing larvae of the recently sequenced hymenopteran model organism Nasonia vitripennis. Our results deliver insights into the molecular underpinnings of diapause in Nasonia and corroborate previously reported diapause-associated features for invertebrates, such as a diapause-dependent abundance change for heat shock and storage proteins. Furthermore, we observed a diapause-dependent switch in enzymes involved in glycerol synthesis and a vastly changed capacity for protein synthesis and degradation. The abundance of structural proteins and proteins involved in protein synthesis decreased with increasing diapause duration, while the abundance of proteins likely involved in diapause maintenance (e.g. ferritins) increased. Only few potentially diapause-specific proteins were identified suggesting that diapause in Nasonia relies to a large extent on a modulation of pre-existing pathways. Studying a diapause syndrome on a proteomic level rather than isolated pathways or physiological networks, has proven to be an efficient and successful avenue to understand molecular mechanisms involved in diapause.

摘要

昆虫滞育是一种可供选择的生活史策略,用于在恶劣环境条件下延长寿命和提高存活率。尽管滞育的某些方面已得到充分研究,但阐明这一显著特征所需的全球代谢调整的更广泛研究却很少见。为了更好地了解昆虫早期滞育期间的代谢变化,我们对最近测序的膜翅目模式生物丽蝇蛹集金小蜂滞育早期和非滞育早期的幼虫采用了鸟枪法蛋白质组学方法。我们的结果揭示了丽蝇蛹集金小蜂滞育的分子基础,并证实了先前报道的无脊椎动物滞育相关特征,如热休克蛋白和储存蛋白的滞育依赖性丰度变化。此外,我们观察到参与甘油合成的酶存在滞育依赖性转变,以及蛋白质合成和降解能力发生了巨大变化。随着滞育持续时间的增加,结构蛋白和参与蛋白质合成的蛋白丰度下降,而可能参与滞育维持的蛋白(如铁蛋白)丰度增加。仅鉴定出少数潜在的滞育特异性蛋白,这表明丽蝇蛹集金小蜂的滞育在很大程度上依赖于对现有途径的调节。事实证明,在蛋白质组水平而非孤立的途径或生理网络上研究滞育综合征,是理解滞育相关分子机制的一种有效且成功的途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/eea8/2712079/15687625fc15/pone.0006394.g001.jpg

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