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HIV的复制能力、细胞病变效应及细胞嗜性

Replicative capacity, cytopathic effect and cell tropism of HIV.

作者信息

Fenyö E M, Albert J, Asjö B

机构信息

Department of Virology, Karolinska Institute, Stockholm, Sweden.

出版信息

AIDS. 1989;3 Suppl 1:S5-12. doi: 10.1097/00002030-198901001-00002.

Abstract

Naturally occurring HIV variants show distinct biologic features that correspond to the severity of HIV infection. Virus from asymptomatic HIV carriers or individuals with mild disease replicates slowly and inefficiently in the patients' peripheral blood mononuclear cell cultures. Attempts to passage these viruses in CD4-positive cell lines usually fail or result in transient replication only. In contrast, viruses from patients with severe immunodeficiency replicate rapidly and efficiently in peripheral blood mononuclear cell cultures as well as cell lines: hence the designation slow/low and rapid/high, respectively. These two groups of viruses can also be distinguished by the type of cytopathogenicity exerted in peripheral blood mononuclear cells. Rapid/high viruses are characterized by extensive syncytia formation, whereas syncytia are rarely seen with slow/low viruses. Instead cultures infected with slow/low viruses show signs of cell death or no cytopathic changes at all. It has also been observed that shift from the slow/low type of virus to rapid/high may occur in the same individual over time. Whether this change signals the emergence of HIV variants with increased virulence or reflects the damage to the immune system that can no longer control virus replication remains to be seen. Rapid/high and slow/low viruses can also be distinguished by cell tropism when tested in a model system on indicator cell lines of T-lymphoid or monocytoid origin. Infection by rapid/high viruses activates chloramphenicol acetyl transferase in both T-lymphoid and monocytoid indicator cells, whereas slow/low viruses activate chloramphenicol acetyl transferase only in monocytoid cell lines. A difference between slow/low and rapid/high viruses cannot be demonstrated in fresh normal macrophage cultures, since most isolates can be successfully passaged in macrophages. Whether the viruses that infect macrophages are truly macrophage-tropic or dual-tropic, and infect macrophages and lymphocytes with equal efficiency, remains to be studied.

摘要

天然存在的HIV变体具有与HIV感染严重程度相对应的独特生物学特征。来自无症状HIV携带者或轻症患者的病毒在患者外周血单核细胞培养物中复制缓慢且效率低下。试图使这些病毒在CD4阳性细胞系中传代通常会失败,或者仅导致短暂复制。相比之下,来自严重免疫缺陷患者的病毒在外周血单核细胞培养物以及细胞系中复制迅速且高效:因此分别被称为慢/低和快/高。这两组病毒也可以通过在外周血单核细胞中产生的细胞病变类型来区分。快/高病毒的特征是广泛形成合胞体,而慢/低病毒很少见到合胞体。相反,感染慢/低病毒的培养物显示细胞死亡迹象或根本没有细胞病变变化。还观察到,随着时间的推移,同一个体中可能会出现从慢/低型病毒向快/高型病毒的转变。这种变化是预示着毒力增强的HIV变体出现,还是反映了免疫系统对病毒复制失去控制的损伤,仍有待观察。在T淋巴细胞或单核细胞来源的指示细胞系模型系统中进行测试时,快/高和慢/低病毒也可以通过细胞嗜性来区分。快/高病毒感染可激活T淋巴细胞和单核细胞指示细胞中的氯霉素乙酰转移酶,而慢/低病毒仅在单核细胞系中激活氯霉素乙酰转移酶。在新鲜的正常巨噬细胞培养物中无法证明慢/低和快/高病毒之间的差异,因为大多数分离株都可以在巨噬细胞中成功传代。感染巨噬细胞的病毒是真正具有巨噬细胞嗜性还是双嗜性,以及是否能以相同效率感染巨噬细胞和淋巴细胞,仍有待研究。

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