Graduate School of Pharmaceutical Sciences , The University of Tokyo , 7-3-1 Hongo, Bunkyo-ku , Tokyo 113-0033 , Japan.
J Am Chem Soc. 2018 Aug 22;140(33):10602-10611. doi: 10.1021/jacs.8b06755. Epub 2018 Aug 7.
Polytheonamide B (1) is a unique peptide natural product because of its extremely complex structure, a channel-forming ability in vitro, and the extremely potent cytotoxicity. The 48-mer sequence of 1 comprises alternating d,l-amino acids and possesses an array of sterically bulky β-tetrasubstituted and hydrogen bond forming residues. These unusual structural features are believed to drive 1 to fold into a 4.5 nm long tube, form a transmembrane ion channel at the plasma membrane, and exert cytotoxicity. Despite its potential biological application, however, multiple substitutions by these unusual residues significantly heightened the synthetic challenges, impeding the solid-phase peptide synthesis (SPPS) of 1. In this study, we first addressed the synthesis problem by extensive optimization of various factors of the SPPS. Adaptation of a new protective group strategy allowed for elongation of a 37-mer peptide on resin, to which an N-terminal 11-mer fragment was condensed. Removal of the 18 protective groups and resin gave rise to 1 in excellent overall yield (4.5%, 76 steps from 17). The SPPS protocol is operationally simple and was proven easily amenable to total synthesis of the fluorescent 48-mer probe 2. Synthetic 1 and 2 were utilized for analysis of their cellular behavior. Reflecting its ion-channel function, the addition of 1 to MCF-7 cells rapidly diminished a potential across the plasma membrane. Furthermore, fluorescence imaging study revealed that 1 and 2 were also internalized into the cells, accumulating in acidic lysosomes and neutralizing the lysosomal pH gradient. These new findings indicated that 1 is capable of exerting two functions upon causing apoptotic cell death of mammalian cells: It induces free cation transport across the plasma as well as lysosomal membranes. The present chemical and biological studies provide valuable information for the design and synthesis of polytheonamide-based molecules with more potent and selective biological activities.
聚醚酰胺 B(1)是一种独特的肽天然产物,因为其具有极其复杂的结构、体外形成通道的能力和极其强烈的细胞毒性。1 的 48 -mer 序列由交替的 d,l-氨基酸组成,并且具有一系列空间庞大的β-四取代和氢键形成残基。这些不寻常的结构特征被认为促使 1 折叠成一个 4.5nm 长的管,在质膜上形成跨膜离子通道,并发挥细胞毒性。然而,尽管具有潜在的生物学应用,但这些不寻常残基的多次取代极大地增加了合成挑战,阻碍了 1 的固相肽合成(SPPS)。在这项研究中,我们首先通过对 SPPS 的各种因素进行广泛优化来解决合成问题。适应一种新的保护基团策略允许在树脂上延长 37-mer 肽,然后将其与 N-端 11-mer 片段缩合。去除 18 个保护基团和树脂得到 1,总收率优异(从 17 开始,76 步,4.5%)。SPPS 方案操作简单,已被证明易于进行荧光 48-mer 探针 2 的全合成。合成的 1 和 2 用于分析它们的细胞行为。反映其离子通道功能,1 被添加到 MCF-7 细胞中后,迅速降低质膜两侧的电位。此外,荧光成像研究表明 1 和 2 也被内化到细胞中,在酸性溶酶体中积累并中和溶酶体 pH 梯度。这些新发现表明,1 在导致哺乳动物细胞凋亡性细胞死亡时能够发挥两种功能:它诱导阳离子自由跨膜以及溶酶体膜的运输。这些新的化学和生物学研究为设计和合成具有更强和更选择性生物活性的聚醚酰胺类分子提供了有价值的信息。
