CD4-Independent Infection of Astrocytes by Human Immunodeficiency Virus Type 1: Requirement for the Human Mannose Receptor

Liu, Ying; Liu, Hao; Kim, Byung Oh; Gattone, Vincent H.; Li, Jinliang; Nath, Avindra; Blum, Janice S.; He, Johnny J.

doi:10.1128/jvi.78.8.4120-4133.2004

Cited by 178 publications

(133 citation statements)

References 82 publications

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“…The fate of HIV-1 upon binding to MR, as for other foreign antigens, is internalization and entry into the endocytic pathway of a variety of antigen-presenting cells as shown in immature MDDCs (43), dermal dendritic cells (24), MDMs (31,44), and astrocytes (45). Where DC-SIGN and MR are co-expressed on dermal DCs, HIV binding and entry probably occurs primarily via DC-SIGN.…”

Section: Discussionmentioning

confidence: 99%

Oligomerization of the Macrophage Mannose Receptor Enhances gp120-mediated Binding of HIV-1

Lai

Bernhard

Turville

et al. 2009

Journal of Biological Chemistry

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C-type lectin receptors expressed on the surface of dendritic cells and macrophages are able to bind glycoproteins of microbial pathogens via mannose, fucose, and N-acetylglucosamine. Langerin on Langerhans cells, dendritic cell-specific intercellular adhesion molecule 3-grabbing nonintegrin on dendritic cells, and mannose receptor (MR) on dendritic cells and macrophages bind the human immunodeficiency virus (HIV) envelope protein gp120 principally via high mannose oligosaccharides. These C-type lectin receptors can also oligomerize to facilitate enhanced ligand binding. This study examined the effect of oligomerization of MR on its ability to bind to mannan, monomeric gp120, native trimeric gp140, and HIV type 1 BaL. Mass spectrometry analysis of crosslinked MR showed homodimerization on the surface of primary monocyte-derived dendritic cells and macrophages. Both monomeric and dimeric MR were precipitated by mannan, but only the dimeric form was co-immunoprecipitated by gp120. These results were confirmed independently by flow cytometry analysis of soluble monomeric and trimeric HIV envelope and a cellular HIV virion capture assay. As expected, mannan bound to the carbohydrate recognition domains of MR dimers mostly in a calcium-dependent fashion. Unexpectedly, gp120-mediated binding of HIV to dimers on MR-transfected Rat-6 cells and macrophages was not calcium-dependent, was only partially blocked by mannan, and was also partially inhibited by N-acetylgalactosamine 4-sulfate. Thus gp120-mediated HIV binding occurs via the calcium-dependent, non-calcium-dependent carbohydrate recognition domains and the cysteine-rich domain at the C terminus of MR dimers, presenting a much broader target for potential inhibitors of gp120-MR binding.

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Section: Discussionmentioning

confidence: 99%

Oligomerization of the Macrophage Mannose Receptor Enhances gp120-mediated Binding of HIV-1

Lai

Bernhard

Turville

et al. 2009

Journal of Biological Chemistry

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“…For example, mannan-binding lectin, a soluble innate immune lectin, binds to influenza A virus and leads directly to virus inactivation (43). In contrast, another mannose-binding human lectin, macrophage mannose receptor (MMR) potentiates HIV binding to target cells (44)(45)(46), and MMR can also potentiate infection of macrophages by influenza virus (47), so that different mannose-binding lectins can bind to viruses to either reduce or potentiate infection. Considering the long-standing evolutionary relationship between virus and host, it is not entirely surprising that viruses have learned to co-opt host innate immune defenses for increased target cell entry and replication.…”

Section: Discussionmentioning

confidence: 99%

Timing of Galectin-1 Exposure Differentially Modulates Nipah Virus Entry and Syncytium Formation in Endothelial Cells

Garner

Yun

Pernet

et al. 2015

J Virol

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Nipah virus (NiV) is a deadly emerging enveloped paramyxovirus that primarily targets human endothelial cells. Endothelial cells express the innate immune effector galectin-1 that we have previously shown can bind to specific N-glycans on the NiV envelope fusion glycoprotein (F). NiV-F mediates fusion of infected endothelial cells into syncytia, resulting in endothelial disruption and hemorrhage. Galectin-1 is an endogenous carbohydrate-binding protein that binds to specific glycans on NiV-F to reduce endothelial cell fusion, an effect that may reduce pathophysiologic sequelae of NiV infection. However, galectins play multiple roles in regulating host-pathogen interactions; for example, galectins can promote attachment of HIV to T cells and macrophages and attachment of HSV-1 to keratinocytes but can also inhibit influenza entry into airway epithelial cells. Using live Nipah virus, in the present study, we demonstrate that galectin-1 can enhance NiV attachment to and infection of primary human endothelial cells by bridging glycans on the viral envelope to host cell glycoproteins. In order to exhibit an enhancing effect, galectin-1 must be present during the initial phase of virus attachment; in contrast, addition of galectin-1 postinfection results in reduced production of progeny virus and syncytium formation. Thus, galectin-1 can have dual and opposing effects on NiV infection of human endothelial cells. While various roles for galectin family members in microbial-host interactions have been described, we report opposing effects of the same galectin family member on a specific virus, with the timing of exposure during the viral life cycle determining the outcome. IMPORTANCENipah virus is an emerging pathogen that targets endothelial cells lining blood vessels; the high mortality rate (up to 70%) in Nipah virus infections results from destruction of these cells and resulting catastrophic hemorrhage. Host factors that promote or prevent Nipah virus infection are not well understood. Endogenous human lectins, such as galectin-1, can function as pattern recognition receptors to reduce infection and initiate immune responses; however, lectins can also be exploited by microbes to enhance infection of host cells. We found that galectin-1, which is made by inflamed endothelial cells, can both promote Nipah virus infection of endothelial cells by "bridging" the virus to the cell, as well as reduce production of progeny virus and reduce endothelial cell fusion and damage, depending on timing of galectin-1 exposure. This is the first report of spatiotemporal opposing effects of a host lectin for a virus in one type of host cell. N ipah virus (NiV) is an emerging zoonotic paramyxovirus that targets endothelial and neural cells. Infection with NiV can result in a severe encephalitic or respiratory syndrome with case fatality rates ranging from 40 to 100% in humans (1, 2). Although initial outbreaks involved transmission from bats to pigs and then from pigs to humans, more recent outbreaks have been shown to involve...

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“…Microinjections were made over 15 min in 25-50 nl increments until the total volume was injected. Doses and volumes of each agent were chosen according to previous publications (Itoh and Buñag, 1993;Madden et al, 1999;Nattie et al, 2004;Tsutsui et al, 2011;Wilkinson et al, 2011;Talman et al, 2012) and were confirmed in preliminary experiments to produce significant immunofluorescent changes for the targeted cell types over homologous regions of NTS. The pipette was left in the brainstem for an additional 15 min to reduce efflux of fluid from the pipette track.…”

Section: Methodsmentioning

confidence: 99%

“…The relative selectivity of SAP conjugates for specific neuronal types has been shown by others (Wiley andLappi, 1997, 1999;Madden et al, 1999) and was supported by our finding that treatment with SSP-SAP did not lead to loss of neurons with the biosynthetic enzyme, tyrosine hydroxylase (TH), which is essential for norepinephrine synthesis (Lin et al, 2012b). In contrast, injection into the NTS of anti-dopamine ␤-hydroxylase-SAP (anti-DBH-SAP), which led to a significant loss of TH and DBH neurons, while not affecting NTS neurons with the NK1R, also attenuated the arterial baroreflex and caused significant lability of arterial pressure (Talman et al, 2012).…”

Section: Introductionmentioning

confidence: 99%

Astrocytes in the Rat Nucleus Tractus Solitarii Are Critical for Cardiovascular Reflex Control

et al. 2013

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We have shown that an antibody to dopamine-␤-hydroxylase conjugated with saporin (anti-DBH-SAP) damages catecholamine neurons in the nucleus tractus solitarii (NTS) of rat, attenuates arterial baroreflexes, and leads to lability of arterial blood pressure, damage to cardiac myocytes, and, in some animals, sudden death. However, others have shown that injection of 6-hydroxydopamine (6-OHDA), a toxin devoid of saporin, also damaged NTS catecholamine neurons but did not lead to these cardiovascular changes. We found similar cardiovascular changes after injecting a different SAP conjugate to target NTS neurons with neurokinin (NK1) receptors. Because ribosome-inactivating proteins may be toxic to glia, we hypothesized that SAP, a ribosome-inactivating protein, might target glia whose loss could account for physiological changes. We tested this hypothesis by assessing effects on select neurons and on glia in the NTS after exposure to SAP, targeted SAP conjugates, or 6-OHDA. SAP and all SAP conjugates led to loss of immunoreactivity for glial fibrillary acidic protein, a marker for astrocytes, in the NTS while 6-OHDA did not. As reported previously, anti-DBH-SAP selectively killed noradrenergic neurons in the NTS while SAP conjugated to stabilized substance P (SSP-SAP) selectively killed neurons with NK1 receptors. In contrast, SAP produced no demonstrable neuronal damage. All injections led to activation of microglia in the NTS; however, only SAP and its conjugates attenuated cardiovascular reflexes while also producing lability of arterial pressure, damage to cardiac myocytes, and in some animals, sudden death. Thus, NTS astrocytes may play a role in mediating cardiovascular reflex transmission through the NTS.

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CD4-Independent Infection of Astrocytes by Human Immunodeficiency Virus Type 1: Requirement for the Human Mannose Receptor

Cited by 178 publications

References 82 publications

Oligomerization of the Macrophage Mannose Receptor Enhances gp120-mediated Binding of HIV-1

Oligomerization of the Macrophage Mannose Receptor Enhances gp120-mediated Binding of HIV-1

Timing of Galectin-1 Exposure Differentially Modulates Nipah Virus Entry and Syncytium Formation in Endothelial Cells

Astrocytes in the Rat Nucleus Tractus Solitarii Are Critical for Cardiovascular Reflex Control

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