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从苏铁种子中鉴定和表征具有 DNA 结合特性的杀菌和促凋亡肽。

Identification and characterization of a bactericidal and proapoptotic peptide from Cycas revoluta seeds with DNA binding properties.

机构信息

Department of Internal Medicine, University of Texas Medical Branch, Galveston, Texas 77555, USA.

出版信息

J Cell Biochem. 2012 Jan;113(1):184-93. doi: 10.1002/jcb.23343.

DOI:10.1002/jcb.23343
PMID:21882228
Abstract

Nowadays, novel pharmacies have been screened from plants. Among them are the peptides, which show multiple biotechnological activities. In this report, a small peptide (Ala-Trp-Lys-Leu-Phe-Asp-Asp-Gly-Val) with a molecular mass of 1,050 Da was purified from Cycas revoluta seeds by using reversed-phase liquid chromatography. This peptide shows clear deleterious effects against human epidermoid cancer (Hep2) and colon carcinoma cells (HCT15). It caused inhibition of cancer cell proliferation and further disruption of nucleosome structures, inducing apoptosis by direct DNA binding. A remarkable antibacterial activity was also observed in this same peptide. Nevertheless, no significant lysis of normal RBC cells was observed in the presence of peptide. Additionally, an acetylation at the N-termini portion is able to reduce both activities. Bioinformatics tools were also utilized for construction of a three-dimensional model showing a single amphipathic helix. Since in vitro binding studies show that the target of this peptide seems to be DNA, theoretical docking studies were also performed to better understand the interaction between peptide and nucleic acids and also to shed some light on the acetyl group role. Firstly, binding studies showed that affinity contacts basically occur due to electrostatic attraction. The complex peptide-ssDNA was clearly oriented by residues Ala(1), Lys(3), and Asp(6), which form several hydrogen bonds that are able to stabilize the complex. When acetyl was added, hydrogen bonds are broken, reducing the peptide affinity. In summary, it seems that information here provided could be used to design a novel derivative of this peptide which a clear therapeutic potential.

摘要

如今,新型药物已从植物中筛选出来。其中包括具有多种生物技术活性的肽。在本报告中,一种分子量为 1050Da 的小肽(Ala-Trp-Lys-Leu-Phe-Asp-Asp-Gly-Val)从苏铁种子中通过反相液相色谱法被分离出来。该肽对人表皮样癌细胞(Hep2)和结肠癌细胞(HCT15)具有明显的杀伤作用。它通过直接与 DNA 结合诱导细胞凋亡,导致癌细胞增殖受到抑制和核小体结构进一步破坏。该肽还具有显著的抗菌活性。然而,在存在肽的情况下,未观察到正常 RBC 细胞的显著裂解。此外,N 末端的乙酰化能够降低这两种活性。生物信息学工具也被用于构建一个三维模型,显示出单一的两亲性螺旋。由于体外结合研究表明,该肽的靶标似乎是 DNA,因此还进行了理论对接研究,以更好地理解肽与核酸之间的相互作用,并阐明乙酰基的作用。首先,结合研究表明,亲和力接触主要是由于静电吸引。复合物肽-ssDNA 被残基 Ala(1)、Lys(3)和 Asp(6)明显定向,它们形成几个氢键,能够稳定复合物。当加入乙酰基时,氢键被打破,降低了肽的亲和力。总之,这里提供的信息似乎可以用于设计这种肽的新型衍生物,具有明确的治疗潜力。

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