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住囊虫的3类乙醇脱氢酶为脊索动物视黄酸合成的进化提供了新见解。

Oikopleura dioica alcohol dehydrogenase class 3 provides new insights into the evolution of retinoic acid synthesis in chordates.

作者信息

Cañestro Cristian, Albalat Ricard, Postlethwait John H

机构信息

Institute of Neuroscience, University of Oregon, Eugene, OR 97403, USA.

出版信息

Zoolog Sci. 2010 Feb;27(2):128-33. doi: 10.2108/zsj.27.128.

DOI:10.2108/zsj.27.128
PMID:20141418
Abstract

Enzymes that synthesize retinoic acid (RA) constitute the first level of regulation of RA action. In vertebrates, enzymes of the medium-chain alcohol dehydrogenase (MDR-Adh) family catalyze the first step of the RA synthetic pathway by oxidizing retinol. Among MDR-Adh enzymes, Adh3 is the only member present in non-vertebrates, and whether Adh3 is actually involved in RA biosynthesis remains uncertain. Here, we investigate the MDR-Adh family in Oikopleura dioica, a urochordate representing the sister group to vertebrates. Oikopleura is of special interest because it has lost the classical RA role in development, which relaxed evolutionary constraints to preserve the RA-genetic machinery, leading to the loss of RA-system components. The hypothesis that Adh3 plays a role in RA synthesis predicts that the relaxation of selection in Oikopleura should have led to the loss of Adh3, or changes in residues related to retinol oxidation. The hypothesis also predicts changes in the expression pattern of Oikopleura Adh3 compared to other chordates that preserved RA-signaling. Our results, however, revealed the presence of a highly conserved Adh3 gene in Oikopleura, with no significant changes in functional residues. Our results also revealed that the Oikopleura Adh3 expression remains unchanged in comparison to other non-vertebrate chordates, restricted to specific compartments of the digestive system. Because Adh3 has been highly conserved in an animal that has dismantled the RA system, we conclude that Adh3 preservation is not due to a conserved role in RA synthesis. Thereby, if Adh3 plays a role in RA synthesis in vertebrates, it might be a lineage-specific neofunctionalization.

摘要

合成视黄酸(RA)的酶构成了RA作用的第一级调控。在脊椎动物中,中链醇脱氢酶(MDR-Adh)家族的酶通过氧化视黄醇催化RA合成途径的第一步。在MDR-Adh酶中,Adh3是唯一存在于非脊椎动物中的成员,而Adh3是否实际参与RA生物合成仍不确定。在这里,我们研究了住囊虫中的MDR-Adh家族,住囊虫是一种代表脊椎动物姐妹群的尾索动物。住囊虫特别引人关注,因为它在发育过程中失去了RA的经典作用,这放宽了对保留RA遗传机制的进化限制,导致RA系统成分的丧失。Adh3在RA合成中起作用的假设预测,住囊虫中选择压力的放松应该导致Adh3的丧失,或者与视黄醇氧化相关的残基发生变化。该假设还预测,与保留RA信号的其他脊索动物相比,住囊虫Adh3的表达模式会发生变化。然而,我们的结果显示住囊虫中存在一个高度保守的Adh3基因,其功能残基没有显著变化。我们的结果还显示,与其他非脊椎动物脊索动物相比,住囊虫Adh3的表达保持不变,仅限于消化系统的特定区域。由于Adh3在一个已经拆解RA系统的动物中高度保守,我们得出结论,Adh3的保留并非由于其在RA合成中的保守作用。因此,如果Adh3在脊椎动物的RA合成中起作用,它可能是一种谱系特异性的新功能化。

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