Phosphatidylserine Exposure Controls Viral Innate Immune Responses by Microglia

Tufail, Yusuf; Cook, Daniela; Fourgeaud, Lawrence; Powers, Colin; Merten, Katharina; Clark, Charles L.; Hoffman, Elizabeth A.; Ngo, Alexander; Sekiguchi, Kohei J.; O’Shea, Clodagh C.; Lemke, Greg; Nimmerjahn, Axel

doi:10.1016/j.neuron.2016.12.021

Cited by 67 publications

(92 citation statements)

References 68 publications

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“…Cells transduced with adenovirus vectors, which expose PtdSer due to the toxicity of viral transduction, were recently shown to be removed by efferocytosis by the interactions between PtdSer, protein S/Gas6, and TAM receptors, resulting in decreased transgene expression of adenoviral vectors (Tufail et al, 2017). Because adenoviruses require cell death for egress (Fields et al, 2013), it is of interest to determine whether protein S/Gas6-mediated efferocytosis can inhibit release of replication-competent adenovirus from infected cells.…”

Section: Discussionmentioning

confidence: 99%

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Protein S and Gas6 induce efferocytosis of HIV-1-infected cells

et al. 2018

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Efferocytosis, the phagocytic clearance of apoptotic cells, can provide host protection against certain types of viruses by mediating phagocytic clearance of infected cells undergoing apoptosis. It is known that HIV-1 induces apoptosis and HIV-1-infected cells are efferocytosed by macrophages, although its molecular mechanisms are unknown. To elucidate the roles that efferocytosis of HIV-1-infected cells play in clearance of infected cells, we sought to identify molecules that mediate these processes. We found that protein S, present in human serum, and its homologue, Gas6, can mediate phagocytosis of HIV-1-infected cells by bridging receptor tyrosine kinase Mer, expressed on macrophages, to phosphatidylserine exposed on infected cells. Efferocytosis of live infected cells was less efficient than dead infected cells; however, a significant fraction of live infected cells were phagocytosed over 12 h. Our results suggest that efferocytosis not only removes dead cells, but may also contribute to macrophage removal of live virus producing cells.

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Section: Discussionmentioning

confidence: 99%

“…Efferocytosis can also play a role in protecting the host from pathogens (Martin et al, 2014; Nainu et al, 2015; Tufail et al, 2017). When cells are infected with certain types of viruses, the cells undergo apoptosis to prevent pathogens from exploiting the host cell machinery.…”

Section: Introductionmentioning

confidence: 99%

Protein S and Gas6 induce efferocytosis of HIV-1-infected cells

et al. 2018

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“…For example, when neurogenic cells in the adult SVZ are BrdU pulse-labeled during cell division, many more healthy BrdU-labeled neurons are present in the olfactory bulb (to which newborn SVZ cells migrate) one month after labeling in Axl −/− Mertk −/− mice than in wild-type [65]. More definitively, adenovirus-transduced astrocytes have been found to transiently externalize PtdSer, and over the course of several days after the transduction, to be phagocytically cleared by activated microglia [66]. This phagocytosis is both TAM- and PtdSer-dependent, since clearance does not occur in either Axl −/− Mertk −/− mutants or when PtdSer externalization is genetically inhibited [66].…”

Section: Biological Phenomena Driven By Ptdser/tam Signalingmentioning

confidence: 99%

“…More definitively, adenovirus-transduced astrocytes have been found to transiently externalize PtdSer, and over the course of several days after the transduction, to be phagocytically cleared by activated microglia [66]. This phagocytosis is both TAM- and PtdSer-dependent, since clearance does not occur in either Axl −/− Mertk −/− mutants or when PtdSer externalization is genetically inhibited [66]. Moreover, in these mutant settings, the non-eaten transduced cells persist as healthy functioning astrocytes for many months [66].…”

Section: Biological Phenomena Driven By Ptdser/tam Signalingmentioning

confidence: 99%

“…This phagocytosis is both TAM- and PtdSer-dependent, since clearance does not occur in either Axl −/− Mertk −/− mutants or when PtdSer externalization is genetically inhibited [66]. Moreover, in these mutant settings, the non-eaten transduced cells persist as healthy functioning astrocytes for many months [66]. These studies are consistent with: (a) earlier analyses of tissue recovery following focal brain ischemia, in which areas (brain volume) of neuronal atrophy are reduced, and recovery is enhanced, in Mertk −/− mice relative to wild-type [67]; and (b) even earlier work in C. elegans embryos, in which genetic inactivation of engulfment (phagocytosis) genes results in the long-term survival of a subset of cells that would otherwise die [68, 69].…”

Section: Biological Phenomena Driven By Ptdser/tam Signalingmentioning

confidence: 99%

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Phosphatidylserine Is the Signal for TAM Receptors and Their Ligands

Lemke

2017

Trends in Biochemical Sciences

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Phagocytic astrocytes: Emerging from the shadows of microglia

Konishi

Koizumi

Kiyama

2022

Glia

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Elimination of dead or live cells take place in both a healthy and diseased central nervous system (CNS). Dying or dead cells are quickly cleared by phagocytosis for the maintenance of a healthy CNS or for recovery after injury. Live cells or parts thereof, such as the synapses and myelin, are appropriately eliminated by phagocytosis to maintain or refine neural networks during development and adulthood. Microglia, the specific population of resident macrophages in the CNS, are classically considered as primary phagocytes; however, astrocytes have also been highlighted as phagocytes in the last decade. Phagocytic targets and receptors are reported to be mostly common between astrocytes and microglia, which raises the question of how astrocytic phagocytosis differs from microglial phagocytosis, and how these two phagocytic systems cooperate. In this review, we address the consequences of astrocytic phagocytosis, particularly focusing on these elusive points.

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Phosphatidylserine Exposure Controls Viral Innate Immune Responses by Microglia

Cited by 67 publications

References 68 publications

Protein S and Gas6 induce efferocytosis of HIV-1-infected cells

Protein S and Gas6 induce efferocytosis of HIV-1-infected cells

Phosphatidylserine Is the Signal for TAM Receptors and Their Ligands

Phagocytic astrocytes: Emerging from the shadows of microglia

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