Department of Physiology, Center for Biomedical Engineering and Technology, University of Maryland School of Medicine, Baltimore, MD 20201, USA.
Int J Mol Sci. 2021 Feb 8;22(4):1685. doi: 10.3390/ijms22041685.
The evolution of the eukaryotic cell from the primal endosymbiotic event involved a complex series of adaptations driven primarily by energy optimization. Transfer of genes from endosymbiont to host and concomitant expansion (by infolding) of the endosymbiont's chemiosmotic membrane greatly increased output of adenosine triphosphate (ATP) and placed selective pressure on the membrane at the host-endosymbiont interface to sustain the energy advantage. It is hypothesized that critical functions at this interface (metabolite exchange, polypeptide import, barrier integrity to proteins and DNA) were managed by a precursor β-barrel protein ("pβB") from which the voltage-dependent anion-selective channel (VDAC) descended. VDAC's role as hub for disparate and increasingly complex processes suggests an adaptability that likely springs from a feature inherited from pβB, retained because of important advantages conferred. It is proposed that this property is the remarkable structural flexibility evidenced in VDAC's gating mechanism, a possible origin of which is discussed.
真核细胞从原始内共生事件的进化涉及一系列复杂的适应,主要由能量优化驱动。内共生体基因向宿主的转移和内共生体化学渗透膜的伴随扩张(通过内折)极大地增加了三磷酸腺苷(ATP)的产量,并对宿主-内共生体界面处的膜施加了选择性压力,以维持这种能量优势。据推测,在这个界面上的关键功能(代谢物交换、多肽导入、蛋白质和 DNA 的屏障完整性)是由前体β-桶蛋白(“pβB”)管理的,电压依赖性阴离子选择性通道(VDAC)由此衍生。VDAC 作为不同且越来越复杂的过程的中心的作用表明了一种适应性,这种适应性可能源于从 pβB 继承的特征,因为赋予了重要的优势而得以保留。有人提出,这种特性是 VDAC 门控机制中明显的结构灵活性的证据,对此进行了讨论。
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