从感染三角瘤血淋巴中分离的两种具有抗菌活性的速激肽相关肽。

Microbiology insights Pub Date : 2020-07-31 eCollection Date: 2020-01-01 DOI:10.1177/1178636120933635
Laura Cristina Lima Diniz, Flávio Lopes Alves, Antonio Miranda, Pedro Ismael da Silva Junior
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引用次数: 7

摘要

抗菌肽和抗菌蛋白(AMPs)是一种可以与微生物细胞相互作用并导致膜破坏或细胞内分子相互作用和死亡的分子。一些具有抗菌作用的分子还表现出其他生物活性。其中一个代表双重活动的蛋白质组是速激蛋白家族。速激肽(Tachykinins, TKs)在脊椎动物中形成一个具有一致的c端区(F-X-G-Y-R-NH2)的神经肽家族。无脊椎动物TKs和tk相关肽(TKRPs)是在无脊椎动物中发现的与TKs具有高度同源性且具有相似生物学效应的亚家族。其中一些分子已经被描述,但关于半翅目物种中TKRP的报道有限。通过反相高效液相色谱、生物测定和质谱分析,分离出两个抗菌分子,并鉴定为TKRPs,分别命名为TRP1-TINF和TRP2-TINF (tachykinin-related peptides I和II from T. infestans)。TRP1-TINF是具有9个氨基酸残基的随机二级结构肽。它对氨基肽酶降解敏感,主要对黄体微球菌(32 μM)有活性。TRP2-TINF是一种10个氨基酸的肽,具有310螺旋的二级结构,易被羧肽酶降解。对铜绿假单胞菌和大肠杆菌(45 μM)均有较强的抑菌活性。两种分子对人红细胞均无毒性,在浓度为1000 μM时对Vero细胞均有轻微毒性。该研究首次对具有抗菌活性的TKRPs进行了描述,有助于更广泛地了解昆虫的生理和药理相关分子。
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Two Tachykinin-Related Peptides with Antimicrobial Activity Isolated from Triatoma infestans Hemolymph.

Antimicrobial peptides and proteins (AMPs) are molecules that can interact with microbial cells and lead to membrane disruption or intracellular molecule interactions and death. Several molecules with antimicrobial effects also present other biological activities. One such protein group representing the duplicity of activities is the tachykinin family. Tachykinins (TKs) form a family of neuropeptides in vertebrates with a consensus C-terminal region (F-X-G-Y-R-NH2). Invertebrate TKs and TK-related peptides (TKRPs) are subfamilies found in invertebrates that present high homology with TKs and have similar biological effects. Several of these molecules have already been described but reports of TKRP in Hemiptera species are limited. By analyzing the Triatoma infestans hemolymph by reversed-phase high-performance liquid chromatography, biological assays, and mass spectrometry, two antimicrobial molecules were isolated and identified as TKRPs, which we named as TRP1-TINF and TRP2-TINF (tachykinin-related peptides I and II from T. infestans). TRP1-TINF is a random secondary structure peptide with 9 amino acid residues. It is susceptible to aminopeptidases degradation and is active mainly against Micrococcus luteus (32 μM). TRP2-TINF is a 10-amino acid peptide with a 310 helix secondary structure and is susceptible to carboxypeptidases degradation. It has major antimicrobial activity against both Pseudomonas aeruginosa and Escherichia coli (45 μM). Neither molecule is toxic to human erythrocytes and both present minor toxicity toward Vero cells at a concentration of 1000 μM. As the first description of TKRPs with antimicrobial activity in T. infestans, this work contributes to the wider comprehension of the insects' physiology and describes pharmacological relevant molecules.

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