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HIV感染中细胞激活和病毒传播的多种模式:慢性和潜伏感染细胞在维持病毒复制中的作用。

Multiple modes of cellular activation and virus transmission in HIV infection: a role for chronically and latently infected cells in sustaining viral replication.

作者信息

Grossman Z, Feinberg M B, Paul W E

机构信息

The Office of AIDS Research, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 May 26;95(11):6314-9. doi: 10.1073/pnas.95.11.6314.

Abstract

CD4(+) T cell activation, required for virus replication in these cells, occurs in local microenvironmental domains in transient bursts. Thus, although most HIV originates from short-lived virus-producing cells, it is unlikely that chronic infection is generally sustained in rapid continuous cycles of productive infection as has been proposed. Such continuity of productive infection cycles would depend on efficient long-range transmission of HIV from one set of domains to another, in turn requiring the maintenance of sufficiently high concentrations of cell-free virus across lymphoid tissues at all times. By contrast, long-lived cellular sources of HIV maintain the capacity to infect newly activated cells at close range despite the temporal and spatial discontinuities of activation events. Such proximal activation and transmission (PAT) involving chronically and latently infected cells may be responsible for sustained infection, particularly when viral loads are low. Once CD4 cells are productively infected through PAT, they can infect other activated cells in their immediate vicinity. Such events propagate locally but generally do not spread systemically, unlike in the acute phase of the infection, because of the early establishment of protective anergy. Importantly, antiretroviral drug treatment is likely to differentially impact long-range transmission and PAT.

摘要

CD4(+) T细胞活化是病毒在这些细胞中复制所必需的,它以短暂爆发的形式发生在局部微环境区域。因此,尽管大多数HIV起源于短命的病毒产生细胞,但慢性感染不太可能像所提出的那样通过高效连续的生产性感染循环来维持。这种生产性感染循环的连续性将取决于HIV从一组区域到另一组区域的高效远程传播,这反过来又需要始终在淋巴组织中维持足够高浓度的游离病毒。相比之下,HIV的长寿细胞来源能够在近距离感染新激活的细胞,尽管激活事件存在时间和空间上的间断性。这种涉及慢性和潜伏感染细胞的近端激活和传播(PAT)可能是持续感染的原因,特别是当病毒载量较低时。一旦CD4细胞通过PAT被生产性感染,它们就可以感染其附近的其他激活细胞。由于保护性无反应性的早期建立,这些事件在局部传播,但通常不会像感染急性期那样全身扩散。重要的是,抗逆转录病毒药物治疗可能会对远程传播和PAT产生不同的影响。

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