Philippon Héloïse, Brochier-Armanet Céline, Perrière Guy
Laboratoire de Biométrie et Biologie Evolutive, UMR CNRS 5558, Université Claude Bernard - Lyon 1, 43 bd. du 11 Novembre 1918, Villeurbanne, 69622, France.
BMC Evol Biol. 2015 Oct 19;15:226. doi: 10.1186/s12862-015-0498-7.
Phosphatidylinositol-3-kinases (PI3Ks) are a family of eukaryotic enzymes modifying phosphoinositides in phosphatidylinositols-3-phosphate. Located upstream of the AKT/mTOR signalling pathway, PI3Ks activate secondary messengers of extracellular signals. They are involved in many critical cellular processes such as cell survival, angiogenesis and autophagy. PI3K family is divided into three classes, including 14 human homologs. While class II enzymes are composed of a single catalytic subunit, class I and III also contain regulatory subunits. Here we present an in-depth phylogenetic analysis of all PI3K proteins.
We confirmed that PI3K catalytic subunits form a monophyletic group, whereas regulatory subunits form three distinct groups. The phylogeny of the catalytic subunits indicates that they underwent two major duplications during their evolutionary history: the most ancient arose in the Last Eukaryotic Common Ancestor (LECA) and led to the emergence of class III and class I/II, while the second - that led to the separation between class I and II - occurred later, in the ancestor of Unikonta (i.e., the clade grouping Amoebozoa, Fungi, and Metazoa). These two major events were followed by many lineage specific duplications in particular in vertebrates, but also in various protist lineages. Major loss events were also detected in Vidiriplantae and Fungi. For the regulatory subunits, we identified homologs of class III in all eukaryotic groups indicating that, for this class, both the catalytic and the regulatory subunits were presents in LECA. In contrast, homologs of the regulatory class I have a more recent origin.
The phylogenetic analysis of the PI3K shed a new light on the evolutionary history of these enzymes. We found that LECA already contained a PI3K class III composed of a catalytic and a regulatory subunit. Absence of class II regulatory subunits and the recent origin of class I regulatory subunits is puzzling given that the class I/II catalytic subunit was present in LECA and has been conserved in most present-day eukaryotic lineages. We also found surprising major loss and duplication events in various eukaryotic lineages. Given the functional specificity of PI3K proteins, this suggests dynamic adaptation during the diversification of eukaryotes.
磷脂酰肌醇-3-激酶(PI3Ks)是一类真核酶,可修饰磷脂酰肌醇-3-磷酸中的磷酸肌醇。PI3Ks位于AKT/mTOR信号通路的上游,可激活细胞外信号的二级信使。它们参与许多关键的细胞过程,如细胞存活、血管生成和自噬。PI3K家族分为三类,包括14种人类同源物。II类酶由单个催化亚基组成,而I类和III类还包含调节亚基。在此,我们对所有PI3K蛋白进行了深入的系统发育分析。
我们证实PI3K催化亚基形成一个单系群,而调节亚基形成三个不同的群。催化亚基的系统发育表明,它们在进化历史中经历了两次主要的复制:最古老的一次发生在最后的真核生物共同祖先(LECA)中,导致了III类和I/II类的出现,而第二次——导致I类和II类分离的那次——发生在单鞭毛生物祖先中(即包括变形虫、真菌和后生动物的进化枝)。这两次主要事件之后是许多特定谱系的复制,特别是在脊椎动物中,但也在各种原生生物谱系中。在维管植物和真菌中也检测到了主要的丢失事件。对于调节亚基,我们在所有真核生物类群中都鉴定出了III类的同源物,这表明对于该类而言,催化亚基和调节亚基在LECA中都已存在。相比之下,I类调节亚基的同源物起源较晚。
PI3K的系统发育分析为这些酶的进化历史提供了新的线索。我们发现LECA已经包含了由催化亚基和调节亚基组成的III类PI3K。鉴于I/II类催化亚基存在于LECA中并在大多数现代真核生物谱系中得以保留,II类调节亚基的缺失以及I类调节亚基的近期起源令人费解。我们还在各种真核生物谱系中发现了惊人的主要丢失和复制事件。鉴于PI3K蛋白的功能特异性,这表明在真核生物多样化过程中存在动态适应。
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