Department of Biological Sciences, State University of New York at Albany, Albany, NY 12222
Department of Biological Sciences, State University of New York at Albany, Albany, NY 12222.
Proc Natl Acad Sci U S A. 2017 Sep 26;114(39):10491-10496. doi: 10.1073/pnas.1707873114. Epub 2017 Sep 5.
Poison-dart frogs sequester lethal amounts of steroidal alkaloid batrachotoxin (BTX) in their skin as a defense mechanism against predators. BTX targets voltage-gated Na channels and enables them to open persistently. How BTX autoresistance arises in such frogs remains a mystery. The BTX receptor has been delineated along the Na channel inner cavity, which is formed jointly by four S6 transmembrane segments from domains D1 to D4. Within the muscle Na channel, five amino acid (AA) substitutions have been identified at D1/S6 and D4/S6. We therefore investigated the role of these naturally occurring substitutions in BTX autoresistance by introducing them into rat Nav1.4 muscle Na channel, both individually and in combination. Our results showed that combination mutants containing an N1584T substitution all conferred a complete BTX-resistant phenotype when expressed in mammalian HEK293t cells. The single N1584T mutant also retained its functional integrity and became exceptionally resistant to 5 µM BTX, aside from a small residual BTX effect. Single and combination mutants with the other four S6 residues (S429A, I433V, A445D, and V1583I) all remained highly BTX sensitive. These findings, along with diverse BTX phenotypes of N1584K/A/D/T mutant channels, led us to conclude that the conserved N1584 residue is indispensable for BTX actions, probably functioning as an integral part of the BTX receptor. Thus, complete BTX autoresistance found in muscle Na channels could emerge primarily from a single AA substitution (asparagine→threonine) via a single nucleotide mutation (AAC→ACC).
毒镖蛙在皮肤中隔离致死量的甾体生物碱蛙毒素 (BTX),作为防御捕食者的机制。BTX 靶向电压门控 Na 通道,使其持续开放。BTX 自动抗性如何在这些青蛙中出现仍然是一个谜。BTX 受体已沿着 Na 通道内腔进行了描绘,该内腔由来自域 D1 到 D4 的四个 S6 跨膜片段共同形成。在肌肉 Na 通道中,已经在 D1/S6 和 D4/S6 处鉴定出五个氨基酸 (AA) 取代。因此,我们通过将这些天然发生的取代物分别引入大鼠 Nav1.4 肌肉 Na 通道并组合引入来研究它们在 BTX 自动抗性中的作用。我们的结果表明,当在哺乳动物 HEK293t 细胞中表达时,包含 N1584T 取代的组合突变体均赋予完全 BTX 抗性表型。除了残留的小 BTX 效应外,单个 N1584T 突变体也保持其功能完整性并变得异常抵抗 5 µM BTX。具有其他四个 S6 残基(S429A、I433V、A445D 和 V1583I)的单个和组合突变体仍然对 BTX 高度敏感。这些发现以及 N1584K/A/D/T 突变通道的各种 BTX 表型使我们得出结论,保守的 N1584 残基对于 BTX 作用是必不可少的,可能作为 BTX 受体的一个组成部分。因此,在肌肉 Na 通道中发现的完全 BTX 自动抗性主要可能源于单个 AA 取代(天冬酰胺→苏氨酸)通过单个核苷酸突变(AAC→ACC)出现。