TIRF imaging of Fc gamma receptor microclusters dynamics and signaling on macrophages during frustrated phagocytosis

Lin, Jia-Ren; Kurilova, Svetlana; Scott, Brandon L.; Bosworth, Elizabeth; Iverson, Bradley; Bailey, Elizabeth M.; Hoppe, Adam D.

doi:10.1186/s12865-016-0143-2

Cited by 30 publications

(34 citation statements)

References 37 publications

(43 reference statements)

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“…We tested whether these myosin 1-actin puncta were associated with FcR clusters by transfecting cells with EGFP-FcgRIIA. As has been previously observed, macrophages spreading on IgG formed discrete FcR clusters 41,42 . We found that myo1f and FcgRIIA distinctly colocalized at these structures ( Fig.…”

Section: Myo1e and Myo1f Localize To Fcr-actin Adhesions During Frustsupporting

confidence: 77%

Membrane-cytoskeleton mechanical feedback mediated by myosin-I controls phagocytic efficiency

Barger

Reilly

Shutova

et al. 2018

Preprint

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Phagocytosis of invading pathogens or cellular debris requires a dramatic change in cell shape driven by actin polymerization. For antibody-covered targets, phagocytosis is thought to proceed through the sequential engagement of Fc-receptors on the phagocyte with antibodies on the target surface, leading to the extension and closure of the phagocytic cup around the target. We have found that two actin-dependent molecular motors, class 1 myosins myosin 1e and myosin 1f, are specifically localized to Fc-receptor adhesions and required for efficient phagocytosis of antibody-opsonized targets. Using primary macrophages lacking both myosin 1e and myosin 1f, we found that without the actin-membrane linkage mediated by these myosins, the organization of individual adhesions is compromised, leading to excessive actin polymerization, slower adhesion turnover, and deficient phagocytic internalization. This work identifies a novel role for class 1 myosins in coordinated adhesion turnover during phagocytosis and supports a model for a membrane-tension based feedback mechanism for phagocytic cup closure.

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Section: Myo1e and Myo1f Localize To Fcr-actin Adhesions During Frustsupporting

confidence: 77%

Membrane-cytoskeleton mechanical feedback mediated by myosin-I controls phagocytic efficiency

Barger

Reilly

Shutova

et al. 2018

Preprint

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“…CD14 is one of the most common phagocytic receptors on the surface of macrophages, which is the coreceptor for LPS and can mediate the innate immune response to LPS via MyD88, TIRAP, and TRAF6 . CD64 is one member of the Fc gamma receptor (FcγR) family, which can activate the phagocytosis through recognizing bacteria and viruses opsonized by IgG …”

Section: Discussionmentioning

confidence: 99%

HEV ORF3 downregulatesCD14 and CD64 to impair macrophages phagocytosis through inhibiting JAK/STAT pathway

Lei

Huang

et al. 2019

Journal of Medical Virology

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Hepatitis E virus (HEV) could induce chronic hepatitis and liver failure with high mortality through unknown mechanisms. The previous study showed that the HEV open reading frames 3 (ORF3) could inhibit macrophages inflammatory response. Impaired macrophages phagocytosis was also found in patients infected with HEV and its nucleic acids could be detected in macrophages. To elucidate the role of HEV ORF3 on phagocytosis, the phagocytosis activation was measured by phagocytosis test, flow cytometry, and phalloidin staining. Meanwhile, the expression of key phagocytic receptors and the activation of transduction pathway were investigated by using reverse transcription real‐time quantitative polymerase chain reaction (RT‐qPCR) and Western blot analysis. Results of phagocytosis test showed that the HEV ORF3 could significantly impair the absorption capacity of latex beads. Furthermore, results of RT‐qPCR and Western blot analysis showed that the expression of CD14 and CD64 decreased. Afterward, the present study showed that the activation of Janus kinase‐signal transducer and activator of transcription (JAK/STAT) signaling pathway was inhibited by HEV ORF3 and downregulation of CD14 and CD64 could be reversed by interferon γ, one activator of the JAK1/STAT1 signaling pathway. In conclusion, HEV ORF3 could significantly impair the phagocytosis of macrophage by downregulating expression of CD14 and CD64, which may function by inhibiting the activation of the JAK1/STAT1 signaling pathway.

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“…Following phagocyte contact with IgG-coated surfaces or on supported lipid bilayers, formation of FcγRII nanoclusters suggests activation-driven organization of receptor redistribution ( 75 ). FcγR clusters are localized in front of ruffles on extending pseudopods, with rapid recruitment of Syk to advancing pseudopods and subsequent retrograde movement toward the cell center ( 76 ). PI3K co-localized with actin around FcγR clusters, suggestive of signal propagation from FcγR and consistent with PI3K-dependent control of actin cytoskeletal rearrangements ( 76 ).…”

Section: Molecular Segregation and The Formation Of A Phagocytic “Synmentioning

confidence: 99%

“…FcγR clusters are localized in front of ruffles on extending pseudopods, with rapid recruitment of Syk to advancing pseudopods and subsequent retrograde movement toward the cell center ( 76 ). PI3K co-localized with actin around FcγR clusters, suggestive of signal propagation from FcγR and consistent with PI3K-dependent control of actin cytoskeletal rearrangements ( 76 ).…”

Section: Molecular Segregation and The Formation Of A Phagocytic “Synmentioning

confidence: 99%

The “Phagocytic Synapse” and Clearance of Apoptotic Cells

et al. 2017

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Apoptosis and subsequent phagocytic clearance of apoptotic cells is important for embryonic development, maintenance of tissues that require regular cellular renewal and innate immunity. The timely removal of apoptotic cells prevents progression to secondary necrosis and release of cellular contents, preventing cellular stress and inflammation. In addition, altered phagocyte behavior following apoptotic cell contact and phagocytosis engages an anti-inflammatory phenotype, which impacts upon development and progression of inflammatory and immune responses. Defective apoptotic cell clearance underlies the development of various inflammatory and autoimmune diseases. There is considerable functional redundancy in the receptors that mediate apoptotic cell clearance, highlighting the importance of this process in diverse physiological processes. A single phagocyte may utilize multiple receptor pathways for the efficient capture of apoptotic cells by phagocytes (tethering) and the subsequent initiation of signaling events necessary for internalization. In this review, we will consider the surface alterations and molecular opsonization events associated with apoptosis that may represent a tunable signal that confers distinct intracellular signaling events and hence specific phagocyte responses in a context-dependent manner. Efficient molecular communication between phagocytes and apoptotic targets may require cooperative receptor utilization and the establishment of efferocytic synapse, which acts to stabilize adhesive interactions and facilitate the organization of signaling platforms that are necessary for controlling phagocyte responses.

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TIRF imaging of Fc gamma receptor microclusters dynamics and signaling on macrophages during frustrated phagocytosis

Cited by 30 publications

References 37 publications

Membrane-cytoskeleton mechanical feedback mediated by myosin-I controls phagocytic efficiency

Membrane-cytoskeleton mechanical feedback mediated by myosin-I controls phagocytic efficiency

HEV ORF3 downregulatesCD14 and CD64 to impair macrophages phagocytosis through inhibiting JAK/STAT pathway

The “Phagocytic Synapse” and Clearance of Apoptotic Cells

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