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脂滴控制果蝇胚胎的母体组蛋白供应。

Lipid droplets control the maternal histone supply of Drosophila embryos.

机构信息

Department of Biology, University of Rochester, Rochester, NY 14627, USA.

出版信息

Curr Biol. 2012 Nov 20;22(22):2104-13. doi: 10.1016/j.cub.2012.09.018. Epub 2012 Oct 18.

Abstract

BACKGROUND

Histones are essential for chromatin packing, yet free histones not incorporated into chromatin are toxic. While in most cells multiple regulatory mechanisms prevent accumulation of excess histones, early Drosophila embryos contain massive extranuclear histone stores, thought to be essential for development. Excess histones H2A, H2B, and H2Av are bound to lipid droplets, ubiquitous fat storage organelles especially abundant in embryos. It has been proposed that sequestration on lipid droplets allows safe transient storage of supernumerary histones.

RESULTS

Here, we critically test this sequestration hypothesis. We find that histones are anchored to lipid droplets via the previously uncharacterized protein Jabba: Jabba localizes to droplets, coimmunoprecipitates with histones, and is necessary to recruit histones to droplets. Jabba mutants lack the maternal H2A, H2B, and H2Av deposits altogether; presumably, these deposits are eliminated unless sequestered on droplets. Jabba mutant embryos compensate for this histone deficit by translating maternal histone mRNAs. However, when histone expression is mildly compromised, the maternal histone protein deposits are essential for proper early mitoses and for viability.

CONCLUSIONS

A growing number of proteins from other cellular compartments have been found to transiently associate with lipid droplets. Our studies provide the first insight into mechanism and functional relevance of this sequestration. We conclude that sequestration on lipid droplets allows embryos to build up extranuclear histone stores and provides histones for chromatin assembly during times of high demand. This work reveals a novel aspect of histone metabolism and establishes lipid droplets as functional storage sites for unstable or detrimental proteins.

摘要

背景

组蛋白对于染色质包装至关重要,但未结合到染色质中的游离组蛋白是有毒的。虽然在大多数细胞中,多种调控机制可以防止积累过多的组蛋白,但早期果蝇胚胎中含有大量的核外组蛋白储存库,这些储存库被认为对发育是必需的。多余的组蛋白 H2A、H2B 和 H2Av 与脂滴结合,脂滴是普遍存在的脂肪储存细胞器,在胚胎中尤为丰富。有人提出,将组蛋白隔离在脂滴上可以安全地暂时储存多余的组蛋白。

结果

在这里,我们对这种隔离假说进行了严格的检验。我们发现组蛋白通过以前未被表征的蛋白 Jabba 锚定在脂滴上:Jabba 定位于脂滴,与组蛋白共免疫沉淀,并且是将组蛋白募集到脂滴上所必需的。Jabba 突变体完全缺乏母源 H2A、H2B 和 H2Av 沉积;推测这些沉积物被消除,除非隔离在脂滴上。Jabba 突变体胚胎通过翻译母源组蛋白 mRNA 来补偿这种组蛋白缺陷。然而,当组蛋白表达受到轻微损害时,母源组蛋白蛋白沉积对于正常的早期有丝分裂和生存是必需的。

结论

越来越多来自其他细胞区室的蛋白质被发现与脂滴短暂相关。我们的研究首次提供了对这种隔离机制和功能相关性的深入了解。我们的结论是,脂滴上的隔离允许胚胎建立核外组蛋白储存库,并在高需求时为染色质组装提供组蛋白。这项工作揭示了组蛋白代谢的一个新方面,并确立了脂滴作为不稳定或有害蛋白质的功能性储存场所。

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