Abstract
Astrocytes, the most abundant cells of the CNS are believed to play vital roles in brain development and functioning, providing trophic support to neurons and eliciting CNS responses to pathogens/injury. During HIV infection of the CNS, glial activation and infection play major roles in generating the immune activation, a process which, in turn, leads to release of neurotoxic mediators (viral and cellular). Accompanying the activation and proliferation of astroglia is also recruitment of mononuclear phagocytes across the endothelium. Regulated signal transduction pathways finely control all these processes. While earlier believed to support only abortive HIV infection, astrocytes are now recognized to be active participants of productive viral replication. Following infection and/or exposure to viral proteins released from neighboring infected cells, astrocytes become activated and elicit release of inflammatory mediators, such as cytokines, chemokines and growth factors, that are toxic not only for neurons but also for neighboring cells around astrocytes within the CNS. This cascade of inflammation triggers the ensuing neuropathogenesis associated with HIV-1. The normally neuroprotective role of astrocytes thus transforms into a functionally deleterious function, with the ultimate result of disrupted CNS homeostasis. The current review is an attempt to summarize the cellular signal transduction pathways critical for astrocyte activation and inflammation involved in HIV-1 associated dementia
Keywords: HIV, Astrocytes, cell signalling, signal transduction, CNS, astrocyte inflammation, astrogliosis, inflammatroy mediators, HAD, neurodegenerative syndrome
Current Signal Transduction Therapy
Title: Signal Transduction in HIV Protein-Treated Astrocytes
Volume: 7 Issue: 1
Author(s): Honghong Yao, Crystal Bethel-Brown, Lu Yang, Yu Cai, Marlene Kanmogne, Vikas Mudgapalli, Natasha Fields and Shilpa Buch
Affiliation:
Keywords: HIV, Astrocytes, cell signalling, signal transduction, CNS, astrocyte inflammation, astrogliosis, inflammatroy mediators, HAD, neurodegenerative syndrome
Abstract: Astrocytes, the most abundant cells of the CNS are believed to play vital roles in brain development and functioning, providing trophic support to neurons and eliciting CNS responses to pathogens/injury. During HIV infection of the CNS, glial activation and infection play major roles in generating the immune activation, a process which, in turn, leads to release of neurotoxic mediators (viral and cellular). Accompanying the activation and proliferation of astroglia is also recruitment of mononuclear phagocytes across the endothelium. Regulated signal transduction pathways finely control all these processes. While earlier believed to support only abortive HIV infection, astrocytes are now recognized to be active participants of productive viral replication. Following infection and/or exposure to viral proteins released from neighboring infected cells, astrocytes become activated and elicit release of inflammatory mediators, such as cytokines, chemokines and growth factors, that are toxic not only for neurons but also for neighboring cells around astrocytes within the CNS. This cascade of inflammation triggers the ensuing neuropathogenesis associated with HIV-1. The normally neuroprotective role of astrocytes thus transforms into a functionally deleterious function, with the ultimate result of disrupted CNS homeostasis. The current review is an attempt to summarize the cellular signal transduction pathways critical for astrocyte activation and inflammation involved in HIV-1 associated dementia
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Cite this article as:
Yao Honghong, Bethel-Brown Crystal, Yang Lu, Cai Yu, Kanmogne Marlene, Mudgapalli Vikas, Fields Natasha and Buch Shilpa, Signal Transduction in HIV Protein-Treated Astrocytes, Current Signal Transduction Therapy 2012; 7 (1) . https://dx.doi.org/10.2174/157436212799278070
DOI https://dx.doi.org/10.2174/157436212799278070 |
Print ISSN 1574-3624 |
Publisher Name Bentham Science Publisher |
Online ISSN 2212-389X |

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