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从大分子复合物的角度探索杂种优势的机制基础。

Exploring the mechanistic bases of heterosis from the perspective of macromolecular complexes.

机构信息

Institut Jacques Monod, CNRS-UMR 7592, Bâtiment Buffon, 15 Rue Hélène Brion, Paris Cedex 13, France.

出版信息

FASEB J. 2011 Feb;25(2):476-82. doi: 10.1096/fj.10-170639. Epub 2010 Nov 9.

Abstract

Heterosis is defined as greater biomass, fertility or other traits in heterozygotes, polyploids or hybrids compared to their genetically divergent (often homozygous) parents. Heterosis was noticed by various civilizations and scientifically reported by Darwin himself. Despite the importance of heterosis, its molecular bases are still enigmatic. Several genetic models have been proposed but fail to give mechanistic insights. Here we show how dominant negative interactions might give rise to heterotic responses. We also explore a biochemical model of gene dosage effects in macromolecular complexes in a similar context. With the help of heuristic examples and computer simulations we find that heterotic individuals display higher allelic diversity and smaller average multimer concentrations than nonheterotic ones. As intuitively expected, the existence of heterosis involving multimeric complexes arises when the inbred parents have on average smaller genetic values than the maximum possible. Despite its simplicity, the dosage model accounts for the puzzling phenomenon of "progressive heterosis" in which polyploids with increasing genetic diversity exhibit progressively greater heterosis.

摘要

杂种优势是指杂合体、多倍体或杂种相对于其遗传上不同的(通常是纯合的)亲本具有更大的生物量、生育力或其他性状。杂种优势被各种文明所注意到,并被达尔文本人从科学上进行了报道。尽管杂种优势很重要,但它的分子基础仍然是神秘的。已经提出了几种遗传模型,但未能提供机械上的见解。在这里,我们展示了显性负相互作用如何产生杂种优势反应。我们还在类似的背景下探索了大分子复合物中基因剂量效应的生化模型。借助启发式示例和计算机模拟,我们发现杂种个体表现出更高的等位基因多样性和更小的平均多聚体浓度,而非杂种个体则表现出更高的等位基因多样性和更小的平均多聚体浓度。正如直观预期的那样,当纯合亲本的遗传值平均小于最大值时,涉及多聚体复合物的杂种优势就会出现。尽管简单,但剂量模型解释了“渐进杂种优势”的令人费解的现象,即遗传多样性增加的多倍体表现出逐渐增强的杂种优势。

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