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重新思考人类AMY1基因拷贝数变异的淀粉消化假说。

Rethinking the starch digestion hypothesis for AMY1 copy number variation in humans.

作者信息

Fernández Catalina I, Wiley Andrea S

机构信息

Indiana University Bloomington, 701 E. Kirkwood Avenue, Bloomington, Indiana, 47405-7100.

出版信息

Am J Phys Anthropol. 2017 Aug;163(4):645-657. doi: 10.1002/ajpa.23237. Epub 2017 Jun 1.

DOI:10.1002/ajpa.23237
PMID:28568243
Abstract

Alpha-amylase exists across taxonomic kingdoms with a deep evolutionary history of gene duplications that resulted in several α-amylase paralogs. Copy number variation (CNV) in the salivary α-amylase gene (AMY1) exists in many taxa, but among primates, humans appear to have higher average AMY1 copies than nonhuman primates. Additionally, AMY1 CNV in humans has been associated with starch content of diets, and one known function of α-amylase is its involvement in starch digestion. Thus high AMY1 CNV is considered to result from selection favoring more efficient starch digestion in the Homo lineage. Here, we present several lines of evidence that challenge the hypothesis that increased AMY1 CNV is an adaptation to starch consumption. We observe that α- amylase plays a very limited role in starch digestion, with additional steps required for starch digestion and glucose metabolism. Specifically, we note that α-amylase hydrolysis only produces a minute amount of free glucose with further enzymatic digestion and glucose absorption being rate-limiting steps for glucose availability. Indeed α-amylase is nonessential for starch digestion since sucrase-isomaltase and maltase-glucoamylase can hydrolyze whole starch granules while releasing glucose. While higher AMY1 CN and CNV among human populations may result from natural selection, existing evidence does not support starch digestion as the major selective force. We report that in humans α-amylase is expressed in several other tissues where it may have potential roles of evolutionary significance.

摘要

α-淀粉酶存在于各个生物分类界,具有基因复制的深厚进化史,这导致了几个α-淀粉酶旁系同源物的产生。唾液α-淀粉酶基因(AMY1)的拷贝数变异(CNV)存在于许多分类群中,但在灵长类动物中,人类的平均AMY1拷贝数似乎比非人类灵长类动物更高。此外,人类的AMY1 CNV与饮食中的淀粉含量有关,并且α-淀粉酶的一个已知功能是参与淀粉消化。因此,高AMY1 CNV被认为是由于在人类谱系中有利于更高效淀粉消化的选择所致。在这里,我们提出了几条证据,对AMY1 CNV增加是对淀粉消耗的一种适应这一假设提出了挑战。我们观察到α-淀粉酶在淀粉消化中起的作用非常有限,淀粉消化和葡萄糖代谢还需要额外的步骤。具体而言,我们注意到α-淀粉酶水解仅产生极少量的游离葡萄糖,进一步的酶促消化和葡萄糖吸收是葡萄糖可用性的限速步骤。事实上,α-淀粉酶对于淀粉消化并非必不可少,因为蔗糖酶-异麦芽糖酶和麦芽糖酶-葡糖淀粉酶可以水解整个淀粉颗粒并释放葡萄糖。虽然人群中较高的AMY1 CN和CNV可能是自然选择的结果,但现有证据并不支持淀粉消化是主要的选择力量。我们报告说,在人类中,α-淀粉酶在其他几个组织中表达,在这些组织中它可能具有具有进化意义的潜在作用。

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