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豚鼠吸入神经毒剂VX后的急性肺损伤

Acute lung injury following inhalation exposure to nerve agent VX in guinea pigs.

作者信息

Wright Benjamin S, Rezk Peter E, Graham Jacob R, Steele Keith E, Gordon Richard K, Sciuto Alfred M, Nambiar Madhusoodana P

机构信息

Division of Biochemistry, Department of Biochemical Pharmacology, Walter Reed Army Institute of Research, Silver Spring, Maryland 20910, USA.

出版信息

Inhal Toxicol. 2006 May;18(6):437-48. doi: 10.1080/08958370600563847.

Abstract

A microinstillation technique of inhalation exposure was utilized to assess lung injury following chemical warfare nerve agent VX [methylphosphonothioic acid S-(2-[bis(1-methylethyl)amino]ethyl) O-ethyl ester] exposure in guinea pigs. Animals were anesthetized using Telazol-meditomidine, gently intubated, and VX was aerosolized using a microcatheter placed 2 cm above the bifurcation of the trachea. Different doses (50.4 microg/m3, 70.4 micro g/m(m3), 90.4 microg/m(m3)) of VX were administered at 40 pulses/min for 5 min. Dosing of VX was calculated by the volume of aerosol produced per 200 pulses and diluting the agent accordingly. Although the survival rate of animals exposed to different doses of VX was similar to the controls, nearly a 20% weight reduction was observed in exposed animals. After 24 h of recovery, the animals were euthanized and bronchoalveolar lavage (BAL) was performed with oxygen free saline. BAL was centrifuged and separated into BAL fluid (BALF) and BAL cells (BALC) and analyzed for indication of lung injury. The edema by dry/wet weight ratio of the accessory lobe increased 11% in VX-treated animals. BAL cell number was increased in VX-treated animals compared to controls, independent of dosage. Trypan blue viability assay indicated an increase in BAL cell death in 70.4 microg/m(m3) and 90.4 microg/m(m3) VX-exposed animals. Differential cell counting of BALC indicated a decrease in macrophage/monocytes in VX-exposed animals. The total amount of BAL protein increased gradually with the exposed dose of VX and was highest in animals exposed to 90.4 microg/m(m3), indicating that this dose of VX caused lung injury that persisted at 24 h. In addition, histopathology results also suggest that inhalation exposure to VX induces acute lung injury.

摘要

采用微量滴注吸入暴露技术,评估豚鼠在接触化学战神经毒剂VX[甲基硫代膦酸S-(2-[双(1-甲基乙基)氨基]乙基)O-乙酯]后肺部损伤情况。动物使用替来他明-美托咪定麻醉,轻柔插管,通过置于气管分叉上方2 cm处的微导管将VX雾化。以40次脉冲/分钟的频率给予不同剂量(50.4 μg/m³、70.4 μg/m³、90.4 μg/m³)的VX,持续5分钟。VX剂量根据每200次脉冲产生的气溶胶体积计算,并相应稀释该毒剂。尽管接触不同剂量VX的动物存活率与对照组相似,但在暴露动物中观察到体重减轻近20%。恢复24小时后,对动物实施安乐死,并用无氧生理盐水进行支气管肺泡灌洗(BAL)。对BAL进行离心,分离为BAL液(BALF)和BAL细胞(BALC),并分析其肺部损伤指标。VX处理组动物副叶干/湿重比所致水肿增加了11%。与对照组相比,VX处理组动物的BAL细胞数量增加,与剂量无关。台盼蓝活力测定表明,接触70.4 μg/m³和90.4 μg/m³VX的动物BAL细胞死亡增加。BALC的细胞分类计数表明,VX暴露动物的巨噬细胞/单核细胞减少。BAL蛋白总量随VX暴露剂量逐渐增加,在接触90.4 μg/m³的动物中最高,表明该剂量的VX导致了持续24小时的肺部损伤。此外,组织病理学结果也表明,吸入VX可诱发急性肺损伤。

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