MCP-1 LEVELS AND ATYPICAL LYMPHOCYTES IN EARLY FEVER OF DENGUE VIRUS INFECTION WITH NON-STRUCTURAL PROTEIN 1 (NS-1) ANTIGEN TEST IN dr DARSONO HOSPITAL, PACITAN

Indah Agustiningrum, J. Nugraha, Hartono Kahar
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引用次数: 1

Abstract

Dengue infection caused by DENV and transmitted by mosquitoes Aedes aegypti and Aedes albopictus is a major health problem in the world, including Indonesia. Clinical manifestations of dengue infection are very widely, from asymptomatic until dengue shock syndrome (DSS). DENV will attack macrophages and dendritic cells (DC) and replicate them. Monocytes are mac rophages in the blood (±10% leukocytes). Macrophages produce cytokines and chemokines such as monocyte chemotactic protein-1 (MCP-1)/CCL2 .  The monocytes that are infected with DENV will express MCP-1, which will increase the permeability of vascular endothelial cells so that they have a risk of developing DHF/DSS. Macrophages and DC secrete NS1 proteins, which are the co-factors that are needed for viral replication and can be detected in the early phase of fever. The increased MCP-1 levels in dengue infection followed by an increase in the number of atypical lymphocytes indicate the arrival of macrophages and monocytes to the site of inflammation which triggers proliferation rather than lymphocytes. This is an observational analytical study with a cross-sectional design to determine the MCP-1 level in dengue infection patients with 1st until the 4th day of fever and the presence of atypical lymphocytes. Dengue infection was determined by rapid tests NS1 positive or negative and MCP-1 levels were measured using by ELISA sandwich method.MCP-1 level of sixty patients dengue infection NS-1 rapid positive or negative with 2nd until 4rt fever were significantly higher than healthy subjects (420.263±158,496vs29, 475±23.443;p=0.000), but there was no significant difference in subjects with DF, DHF or DSS ( 436,47 ± 2 25 ,5 9  vs 42 2 ,7 7 ± 1 7 0, 55 vs  448, 50 ± 117,39; p =0. 8 44). Atypicallymphosite differ s significantly in healthy subjects than subjects infected with DENV  an average of 2% (p= 0,000) . In conclusion, this shows the arrival of macrophages and monocytes to the site of inflammation, which triggers the proliferation of lymphocytes.
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用非结构蛋白1 (NS-1)抗原检测登革病毒感染早期发热的MCP-1水平和非典型淋巴细胞
由登革热病毒引起并由埃及伊蚊和白纹伊蚊传播的登革热感染是包括印度尼西亚在内的世界上的一个主要卫生问题。登革热感染的临床表现非常广泛,从无症状到登革休克综合征(DSS)。DENV会攻击巨噬细胞和树突状细胞(DC)并复制它们。单核细胞是血液中的巨噬细胞(±10%的白细胞)。巨噬细胞产生细胞因子和趋化因子,如单核细胞趋化蛋白-1 (MCP-1)/CCL2。感染DENV的单核细胞会表达MCP-1, MCP-1会增加血管内皮细胞的通透性,使它们有发生DHF/DSS的风险。巨噬细胞和DC分泌NS1蛋白,这是病毒复制所需的辅助因子,可在发热早期检测到。登革热感染中MCP-1水平升高,随后非典型淋巴细胞数量增加,这表明巨噬细胞和单核细胞到达触发增殖的炎症部位,而不是淋巴细胞。这是一项横断面设计的观察性分析研究,旨在确定登革热感染患者发烧第1天至第4天并存在非典型淋巴细胞的MCP-1水平。采用快速检测法检测登革热感染NS1阳性或阴性,ELISA夹心法检测MCP-1水平。60例登革热感染NS-1快速阳性或阴性伴2 ~ 4rt发热的患者MCP-1水平均显著高于健康组(420.263±158,496vs 29,475±23.443;p=0.000),而DF、DHF和DSS组的MCP-1水平差异无统计学意义(436,47±2,25,5 9 vs 42,7 7±17,0,55 vs 448,50±117,39;p = 0。8 44)。非典型淋巴体在健康受试者中与DENV感染受试者的差异显著,平均为2% (p= 0000)。综上所述,这表明巨噬细胞和单核细胞到达炎症部位,触发淋巴细胞的增殖。
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