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高分辨率质谱驱动的昆虫免疫中肽类危险信号的发现。

High-resolution mass spectrometry driven discovery of peptidic danger signals in insect immunity.

机构信息

Institute of Inorganic and Analytical Chemistry, Justus Liebig University, Giessen, Germany.

出版信息

PLoS One. 2013 Nov 26;8(11):e80406. doi: 10.1371/journal.pone.0080406. eCollection 2013.

Abstract

The 'danger model' is an alternative concept for immune response postulating that the immune system reacts to entities that do damage (danger associated molecular patterns, DAMP) and not only to entities that are foreign (pathogen-associated molecular patterns, PAMP) as proposed by classical immunology concepts. In this study we used Galleria mellonella to validate the danger model in insects. Hemolymph of G. mellonella was digested with thermolysin (as a representative for virulence-associated metalloproteinases produced by humanpathogens) followed by chromatographic fractionation. Immune-stimulatory activity was tested by measuring lysozyme activity with the lytic zone assays against Micrococcus luteus cell wall components. Peptides were analyzed by nano-scale liquid chromatography coupled to high-resolution Fourier transform mass spectrometers. Addressing the lack of a genome sequence we complemented the rudimentary NCBI protein database with a recently established transcriptome and de novo sequencing methods for peptide identification. This approach led to identification of 127 peptides, 9 of which were identified in bioactive fractions. Detailed MS/MS experiments in comparison with synthetic analogues confirmed the amino acid sequence of all 9 peptides. To test the potential of these putative danger signals to induce immune responses we injected the synthetic analogues into G. mellonella and monitored the anti-bacterial activity against living Micrococcus luteus. Six out of 9 peptides identified in the bioactive fractions exhibited immune-stimulatory activity when injected. Hence, we provide evidence that small peptides resulting from thermolysin-mediated digestion of hemolymph proteins function as endogenous danger signals which can set the immune system into alarm. Consequently, our study indicates that the danger model also plays a role in insect immunity.

摘要

“危险模型”是一种免疫反应的替代概念,它假设免疫系统对造成损伤的实体(危险相关分子模式,DAMP)作出反应,而不仅仅是对异物(病原体相关分子模式,PAMP)作出反应,这与经典免疫学概念不同。在这项研究中,我们使用家蚕来验证昆虫中的危险模型。用胰凝乳蛋白酶消化家蚕的血淋巴(作为人类病原体产生的与毒力相关的金属蛋白酶的代表),然后进行色谱分离。通过用溶菌酶活性测定法(裂解区测定法)检测对微球菌细胞壁成分的溶菌酶活性来测试免疫刺激活性。使用纳升液相色谱法与高分辨率傅里叶变换质谱仪联用分析肽。针对缺乏基因组序列的问题,我们使用最近建立的转录组和从头测序方法来补充基本的 NCBI 蛋白质数据库,以进行肽鉴定。这种方法导致鉴定出 127 个肽,其中 9 个在生物活性级分中被鉴定出来。与合成类似物的详细 MS/MS 实验证实了所有 9 个肽的氨基酸序列。为了测试这些潜在的危险信号诱导免疫反应的潜力,我们将合成类似物注射到家蚕中,并监测对活微球菌的抗菌活性。在生物活性级分中鉴定出的 9 个肽中的 6 个在注射时表现出免疫刺激活性。因此,我们提供了证据表明,来自血淋巴蛋白的胰凝乳蛋白酶介导消化产生的小肽作为内源性危险信号,可以使免疫系统进入警报状态。因此,我们的研究表明,危险模型在昆虫免疫中也发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1cd7/3841204/d66ab8d9da1f/pone.0080406.g001.jpg

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