The impact of phosphatidylserine exposure on cancer cell membranes on the activity of the anticancer peptide HB43.

IF 5.5 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
FEBS Journal Pub Date : 2022-04-01 Epub Date: 2021-11-20 DOI:10.1111/febs.16276
Claudia Herrera-León, Francisco Ramos-Martín, Viviane Antonietti, Pascal Sonnet, Nicola D'Amelio
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引用次数: 6

Abstract

HB43 (FAKLLAKLAKKLL) is a synthetic peptide active against cell lines derived from breast, colon, melanoma, lung, prostate, and cervical cancers. Despite its remarkable spectrum of activity, the mechanism of action at the molecular level has never been investigated, preventing further optimization of its selectivity. The alternation of charged and hydrophobic residues suggests amphipathicity, but the formation of alpha-helical structure seems discouraged by its short length and the large number of positively charged residues. Using different biophysical and in silico approaches we show that HB43 is completely unstructured in solution but assumes alpha-helical conformation in the presence of DPC micelles and liposomes exposing phosphatidylserine (PS) used as mimics of cancer cell membranes. Membrane permeabilization assays demonstrate that the interaction leads to the preferential destabilization of PS-containing vesicles with respect to PC-containing ones, here used as noncancerous cell mimics. ssNMR reveals that HB43 is able to fluidify the internal structure of cancer-cell mimicking liposomes while MD simulations show its internalization in such bilayers. This is achieved by the formation of specific interactions between the lysine side chains and the carboxylate group of phosphatidylserine and/or the phosphate oxygen atoms of targeted phospholipids, which could catalyze the formation of the alpha helix required for internalization. With the aim of better understanding the peptide biocompatibility and the additional antibacterial activity, the interaction with noncancerous cell mimicking liposomes exposing phosphatidylcholine (PC) and bacterial mimicking bilayers exposing phosphatidylglycerol (PG) is also described.

暴露于肿瘤细胞膜上的磷脂酰丝氨酸对抗癌肽HB43活性的影响。
HB43 (FAKLLAKLAKKLL)是一种合成肽,对来自乳腺癌、结肠癌、黑色素瘤、肺癌、前列腺癌和宫颈癌的细胞系有活性。尽管其具有显著的活性谱,但在分子水平上的作用机制从未被研究过,这阻碍了其选择性的进一步优化。带电残基和疏水残基的交替显示了两亲性,但由于其长度短和带正电残基数量多,似乎不利于α -螺旋结构的形成。使用不同的生物物理和硅方法,我们表明HB43在溶液中完全非结构化,但在DPC胶束和脂质体存在时呈现α -螺旋构象,暴露磷脂酰丝氨酸(PS)用作癌细胞膜的模拟物。膜渗透试验表明,这种相互作用导致含有ps的囊泡相对于含有pc的囊泡优先失稳,这里用作非癌细胞模拟物。ssNMR显示HB43能够流化癌细胞模拟脂质体的内部结构,而MD模拟显示其内化在这种双层中。这是通过赖氨酸侧链与磷脂酰丝氨酸的羧酸基团和/或目标磷脂的磷酸氧原子之间形成特定的相互作用来实现的,这可以催化内化所需的α螺旋的形成。为了更好地了解肽的生物相容性和额外的抗菌活性,还描述了与暴露磷脂酰胆碱(PC)的非癌细胞模拟脂质体和暴露磷脂酰甘油(PG)的细菌模拟双层的相互作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
FEBS Journal
FEBS Journal 生物-生化与分子生物学
CiteScore
11.70
自引率
1.90%
发文量
375
审稿时长
1 months
期刊介绍: The FEBS Journal is an international journal devoted to the rapid publication of full-length papers covering a wide range of topics in any area of the molecular life sciences. The criteria for acceptance are originality and high quality research, which will provide novel perspectives in a specific area of research, and will be of interest to our broad readership. The journal does not accept papers that describe the expression of specific genes and proteins or test the effect of a drug or reagent, without presenting any biological significance. Papers describing bioinformatics, modelling or structural studies of specific systems or molecules should include experimental data.
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