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利用蛋白质组学方法揭示 对吸血和感染 的反应。

Using Proteomic Approaches to Unravel the Response of to Blood Feeding and Infection With .

机构信息

Laboratory of Immunoparasitology, Department of Pathology, Reproduction and One Health, Faculdade de Ciências Agrárias e Veterinárias, Universidade Estadual Paulista (FCAV/UNESP), Jaboticabal, Brazil.

Intracellular Pathogens Research Laboratory, Department of Clinical Sciences, The Comparative Medicine Institute, College of Veterinary Medicine, North Carolina State University, Raleigh, NC, United States.

出版信息

Front Cell Infect Microbiol. 2022 Jan 28;12:828082. doi: 10.3389/fcimb.2022.828082. eCollection 2022.

Abstract

Among the -borne pathogens, , the main aetiological agent of cat scratch disease (CSD), is of increasing comparative biomedical importance. Despite the importance of as an emergent pathogen, prevention of the diseases caused by this agent in cats, dogs and humans mostly relies on the use of ectoparasiticides. A vaccine targeting both flea fitness and pathogen competence is an attractive choice requiring the identification of flea proteins/metabolites with a dual effect. Even though recent developments in vector and pathogen -omics have advanced the understanding of the genetic factors and molecular pathways involved at the tick-pathogen interface, leading to discovery of candidate protective antigens, only a few studies have focused on the interaction between fleas and flea-borne pathogens. Taking into account the period of time needed for replication in flea digestive tract, the present study investigated flea-differentially abundant proteins (FDAP) in unfed fleas, fleas fed on uninfected cats, and fleas fed on -infected cats at 24 hours and 9 days after the beginning of blood feeding. Proteomics approaches were designed and implemented to interrogate differentially expressed proteins, so as to gain a better understanding of proteomic changes associated with the initial transmission period (24 hour timepoint) and a subsequent time point 9 days after blood ingestion and flea infection. As a result, serine proteases, ribosomal proteins, proteasome subunit α-type, juvenile hormone epoxide hydrolase 1, vitellogenin C, allantoinase, phosphoenolpyruvate carboxykinase, succinic semialdehyde dehydrogenase, glycinamide ribotide transformylase, secreted salivary acid phosphatase had high abundance in response of blood feeding and/or infection by . In contrast, high abundance of serpin-1, arginine kinase, ribosomal proteins, peritrophin-like protein, and FS-H/FSI antigen family member 3 was strongly associated with unfed cat fleas. Findings from this study provide insights into proteomic response of cat fleas to infected and uninfected blood meal, as well as response to invading over an infection time course, thus helping understand the complex interactions between cat fleas and at protein levels.

摘要

在虫媒病原体中,主要的猫抓病(CSD)病因,越来越具有比较生物医学的重要性。尽管作为一种新兴病原体的重要性,但预防这种病原体在猫、狗和人类中引起的疾病主要依赖于寄生虫防治药物的使用。针对跳蚤适应性和病原体能力的疫苗是一个有吸引力的选择,需要鉴定具有双重作用的跳蚤蛋白/代谢物。尽管最近在载体和病原体基因组学方面的进展提高了对蜱-病原体界面涉及的遗传因素和分子途径的理解,从而发现了候选保护性抗原,但只有少数研究集中在跳蚤和跳蚤传播病原体之间的相互作用上。考虑到在跳蚤消化道中复制所需的时间,本研究调查了未进食跳蚤、未感染猫喂食的跳蚤和感染后 24 小时和 9 天后感染猫喂食的跳蚤中丰度不同的跳蚤蛋白(FDAP)。设计并实施了蛋白质组学方法来检测差异表达的蛋白质,以更好地了解与初始传播期(24 小时时间点)和随后的时间点(感染后 9 天)相关的蛋白质组变化。结果表明,丝氨酸蛋白酶、核糖体蛋白、蛋白酶体亚基 α 型、保幼激素环氧化物水解酶 1、卵黄蛋白 C、尿囊素酶、磷酸烯醇丙酮酸羧激酶、琥珀酸半醛脱氢酶、甘氨酰胺核糖核苷酸转化酶、分泌唾液酸磷酸酶在响应血液摄取和/或感染时高度丰富。相比之下,丝氨酸蛋白酶抑制剂 1、精氨酸激酶、核糖体蛋白、围食膜蛋白样蛋白和 FS-H/FSI 抗原家族成员 3 的高丰度与未进食的猫跳蚤强烈相关。本研究的结果提供了有关猫跳蚤对感染和未感染的血液餐的蛋白质组反应以及对感染过程中入侵的反应的见解,从而有助于从蛋白质水平理解猫跳蚤和之间的复杂相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d583/8831700/f2c6f818162a/fcimb-12-828082-g001.jpg

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