揭示信息:对裸鼹鼠比较基因组学的洞察。

Kaitlyn N Lewis, Ilya Soifer, Eugene Melamud, Margaret Roy, R Scott McIsaac, Matthew Hibbs, Rochelle Buffenstein
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引用次数: 34

摘要

动物已经进化到能够在不同的环境中生存,甚至茁壮成长。遗传适应可能间接地创造了表型,也导致了更长的寿命。这种现象的一个例子是超常长寿的裸鼹鼠。这种严格意义上的地下啮齿动物能够耐受缺氧、高碳酸血症和土壤毒素。裸鼹鼠还表现出对癌症的明显抵抗力,而且随着哺乳动物年龄的增长,许多生理特征也会逐渐减弱。阐明导致其独特表型的机制将有助于更好地理解地下生态生理学和衰老生物学。在这方面,比较基因组学可能是一个有用的工具。自2011年裸鼹鼠基因组组装发表以来,对基因组和转录组数据的分析使人们能够更清楚地了解鼹鼠的进化史,并提出可能解释该物种异常长寿和独特健康特征的分子途径(例如nrf2信号激活和DNA损伤修复机制)。然而,仔细审查和重新分析表明,一些已确定的特征是由于对裸鼹鼠基因组的不正确或不精确的注释和组装造成的。此外,当分析包括其他更密切相关的物种时,一些结论(例如,与抗癌和无毛有关的基因)被拒绝。我们描述了更好的研究设计,改进的基因组测序技术,以及新的生物信息学和数据分析工具的结合将如何改善比较基因组学,并最终弥合传统模型和非模式生物之间的差距。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Unraveling the message: insights into comparative genomics of the naked mole-rat.

Unraveling the message: insights into comparative genomics of the naked mole-rat.

Unraveling the message: insights into comparative genomics of the naked mole-rat.

Unraveling the message: insights into comparative genomics of the naked mole-rat.

Animals have evolved to survive, and even thrive, in different environments. Genetic adaptations may have indirectly created phenotypes that also resulted in a longer lifespan. One example of this phenomenon is the preternaturally long-lived naked mole-rat. This strictly subterranean rodent tolerates hypoxia, hypercapnia, and soil-based toxins. Naked mole-rats also exhibit pronounced resistance to cancer and an attenuated decline of many physiological characteristics that often decline as mammals age. Elucidating mechanisms that give rise to their unique phenotypes will lead to better understanding of subterranean ecophysiology and biology of aging. Comparative genomics could be a useful tool in this regard. Since the publication of a naked mole-rat genome assembly in 2011, analyses of genomic and transcriptomic data have enabled a clearer understanding of mole-rat evolutionary history and suggested molecular pathways (e.g., NRF2-signaling activation and DNA damage repair mechanisms) that may explain the extraordinarily longevity and unique health traits of this species. However, careful scrutiny and re-analysis suggest that some identified features result from incorrect or imprecise annotation and assembly of the naked mole-rat genome: in addition, some of these conclusions (e.g., genes involved in cancer resistance and hairlessness) are rejected when the analysis includes additional, more closely related species. We describe how the combination of better study design, improved genomic sequencing techniques, and new bioinformatic and data analytical tools will improve comparative genomics and ultimately bridge the gap between traditional model and nonmodel organisms.

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