乙型流感感染期间、恢复期和继发性病毒血症诱导后可能出现肝肾功能障碍。

Journal of Experimental Pathology Pub Date : 1992-01-01
E S Kang, H J Lee, J Boulet, L K Myers, G A Cook, W Bean
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引用次数: 0

摘要

研究了乙型流感病毒感染是否会改变雪貂的肝功能。此外,还探讨了在血清中检测到病毒特异性抗体(Ab)之前产生病毒特异性抗体的可能性。在流感发烧期间,血清钾、阴离子间隙、氨、白蛋白和CPK降低,BUN、肌酐和GGTP水平升高。随着恢复期的结束,电解质、BUN、肌酐恢复正常,FFA、SGPT、CPK水平升高,血清GGTP进一步升高。肝脏脂肪酸(FA)氧化、鸟氨酸转氨基甲酰基酶(OTC)和肉毒碱棕榈酰基转移酶(CPT)活性变化最小,肝脏ATP和总脂质含量保持正常。继发性病毒血症后,血清FFA持续升高,TG降低,CPK升高,SGPT和GGTP水平恢复正常。在肝脏中,FA氧化率和OTC率保持不变,但CPT活性受到抑制,肝脏中ATP含量显著降低。通过聚乙二醇沉淀从微粒体后上清中提取的免疫复合物(IC)蛋白在恢复期和病毒血症动物的肝脏中逐渐增加。虽然恢复期脾脏中恢复的IC蛋白量也会增加,但病毒血症后情况并非如此,因为形成的IC似乎主要由肝脏处理。通过SDS/PAGE分析,IC中鉴定的主要蛋白为IgM和其他病毒蛋白。然而,该病毒蛋白无法通过免疫印迹法对纯化的乙型流感血凝素(HA)和神经氨酸酶(NA)产生的抗体进行验证,这很可能是由于糖蛋白免疫决定因子的吞噬改变。这些发现表明,在流感、恢复期和病毒血症后,几种血清和肝脏成分的浓度发生变化,反映肝脏受累。此外,抗病毒抗体,主要是IgM,似乎是早期产生的,与银的复合物,可以在血清中检测不到Ab的时候被发现隔离在肝脏和脾脏中。
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Potential for hepatic and renal dysfunction during influenza B infection, convalescence, and after induction of secondary viremia.

Whether infection with influenza B virus alters hepatic function was examined in the ferret. Also, the possibility that viral-specific antibodies (Ab) could be produced well before their detection in serum was explored. During the febrile period of influenza, reductions in the serum potassium, anion gap, ammonia, albumin and CPK and elevations of the BUN, creatinine and the GGTP levels occurred. With convalescence, the electrolytes, BUN and creatinine normalized, FFA, SGPT and CPK levels rose and the serum GGTP rose even further. Hepatic fatty acid (FA) oxidation, ornithine transcarbamylase (OTC) and carnitine palmitoyltransferase (CPT) activities were minimally altered and liver ATP and total lipid content remained normal. Following experimental secondary viremia, serum FFA continued to rise, TG decreased and CPK remained elevated while SGPT and GGTP levels normalized. In the liver, FA oxidation and OTC rates remained unchanged but CPT activity was inhibited and the liver content of ATP was significantly reduced. Immune complex (IC) protein recovered from postmicrosomal supernatant fractions by polyethylene glycol precipitation was progressively increased in livers from convalescent and viremic animals. While the amount of IC protein recovered in the spleen also increases during convalescence, this is not the case after viremia when the IC formed seem to be processed largely by the liver. By SDS/PAGE, the major proteins identified in the IC were IgM and other viral proteins. However, the viral proteins could not be validated by immunoblot with Ab produced against purified influenza B hemagglutinin (HA) and neuraminidase (NA) most probably due to phagocytic alterations of glycoprotein immunodeterminants. These findings indicate that during influenza, convalescence and post viremia changes in the concentrations of several serum and liver components occur that reflect hepatic involvement. Also, antiviral Ab, largely IgM, appears to be produced early, complexes with Ag and can be found sequestered in both the liver and spleen at a time when Ab is not detectable in the serum.

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