Molecular Therapeutics Research, School of Pharmacy, Queen's University Belfast, Medical Biology Centre, Belfast BT9 7BL, Northern Ireland, UK.
Biochimie. 2013 Sep;95(9):1784-94. doi: 10.1016/j.biochi.2013.06.003. Epub 2013 Jun 14.
Here we report two novel 17-mer amidated linear peptides (TsAP-1 and TsAP-2) whose structures were deduced from cDNAs cloned from a venom-derived cDNA library of the Brazilian yellow scorpion, Tityus serrulatus. Both mature peptides were structurally-characterised following their location in chromatographic fractions of venom and synthetic replicates of each were subjected to a range of biological assays. The peptides were each active against model test micro-organisms but with different potencies. TsAP-1 was of low potency against all three test organisms (MICs 120-160 μM), whereas TsAP-2 was of high potency against the Gram-positive bacterium, Staphylococcus aureus (MIC 5 μM) and the yeast, Candida albicans (10 μM). Haemolytic activity of TsAP-1 was low (4% at 160 μM) and in contrast, that of TsAP-2 was considerably higher (18% at 20 μM). Substitution of four neutral amino acid residues with Lys residues in each peptide had dramatic effects on their antimicrobial potencies and haemolytic activities, particularly those of TsAP-1. The MICs of the enhanced cationic analogue (TsAP-S1) were 2.5 μM for S. aureus/C. albicans and 5 μM for E. coli but with an associated large increase in haemolytic activity (30% at 5 μM). The same Lys residue substitutions in TsAP-2 produced a dramatic effect on its MIC for E. coli lowering this from >320 μM to 5 μM. TsAP-1 was ineffective against three of the five human cancer cell lines tested while TsAP-2 inhibited the growth of all five. Lys residue substitution of both peptides enhanced their potency against all five cell lines with TsAp-S2 being the most potent with IC50 values ranging between 0.83 and 2.0 μM. TsAP-1 and TsAP-2 are novel scorpion venom peptides with broad spectrum antimicrobial and anticancer cell activities the potencies of which can be significantly enhanced by increasing their cationicity.
我们从巴西黄蝎毒液衍生的 cDNA 文库中克隆出两个新型 17 肽酰胺(TsAP-1 和 TsAP-2),并推断出它们的结构。这两种成熟肽在其位于毒液色谱馏分中的位置确定后进行了结构表征,并对每个肽的合成副本进行了一系列生物测定。这些肽都对模型测试微生物具有活性,但效力不同。TsAP-1 对所有三种测试生物的效力都较低(MIC 为 120-160μM),而 TsAP-2 对革兰氏阳性菌金黄色葡萄球菌(MIC 为 5μM)和酵母白色念珠菌(10μM)具有高效力。TsAP-1 的溶血活性较低(160μM 时为 4%),而 TsAP-2 的溶血活性则高得多(20μM 时为 18%)。在每个肽中用 Lys 取代四个中性氨基酸残基对其抗菌效力和溶血活性有显著影响,尤其是 TsAP-1 的。增强的阳离子类似物(TsAP-S1)的 MIC 对金黄色葡萄球菌/白色念珠菌为 2.5μM,对大肠杆菌为 5μM,但溶血活性显著增加(5μM 时为 30%)。在 TsAP-2 中进行相同的 Lys 取代对其 MIC 对大肠杆菌的影响很大,将其从>320μM 降低至 5μM。TsAP-1 对测试的五种人类癌细胞系中的三种无效,而 TsAP-2 则抑制了所有五种的生长。两种肽的 Lys 取代都增强了它们对所有五种细胞系的效力,其中 TsAp-S2 的效力最强,IC50 值在 0.83 和 2.0μM 之间。TsAP-1 和 TsAP-2 是新型的蝎毒液肽,具有广谱的抗菌和抗癌细胞活性,其效力可以通过增加其正电性而显著增强。
