IgEb immune complexes activate macrophages through FcγRIV binding

Hirano, Masayuki; Davis, Randall S.; Fine, W. David; Nakamura, Shugo; Shimizu, Kentaro; Yagi, Hirokazu; Kato, Koichi; Stephan, Robert P.; Cooper, Max D.

doi:10.1038/ni1477

Cited by 83 publications

(91 citation statements)

References 46 publications

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“…In contrast, blocking antibodies for the medium affinity receptor FcγRIV resulted in an impaired platelet clearance. Similar results were obtained in human ITP patients where blocking antibodies to FcγRIIIA, which is the human ortholog of murine FcγRIV [23,42], but not to human FcγRI were very efficient in blocking platelet depletion [43][44][45][46]. Thus, FcγRs are instrumental for IgG-mediated platelet depletion for murine and human ITP and are an attractive target for therapeutic intervention.…”

Section: Effector Pathways Involved In Murine Itpsupporting

confidence: 73%

“…The problem here is that a lot of crucial information regarding the mechanism and players involved in IgG-mediated effects have only been identified recently and are still under investigation. For example, the mouse ortholog to human FcγRIIIA has only been identified 4 years ago and is still not fully characterized [42,51]. More importantly, monoclonal antibodies specific for all mouse-activating FcγRs have become available only recently.…”

Section: Effector Cells and Organs Involved In Murine (And Human) Itpmentioning

confidence: 99%

“…Therefore, there are still many open questions with respect to the exact FcγR expression pattern on individual cell types. In the blood, FcγRIII (important for IgG1-mediated platelet depletion) and FcγRIV (important for IgG2a/IgG2b-mediated platelet depletion) are largely expressed on monocytes and neutrophils [18,42]. NK cells, mast cells, eosinophils, and dendritic cells on the other hand largely lack expression of FcγRIV but do express FcγRIII.…”

Section: Effector Cells and Organs Involved In Murine (And Human) Itpmentioning

confidence: 99%

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The role of Fcγ receptors in murine autoimmune thrombocytopenia

et al. 2010

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International audienceImmune thrombocytopenia (ITP) can become a life-threatening condition that requires immediate medical attention. The loss in platelet numbers during ITP can be induced by a variety of triggers. Anti-platelet antibodies of several isotypes and subclasses are a major cause for ITP and are a hallmark of many complex autoimmune diseases such as systemic lupus erythematosus. Mouse models have been important to understand the effector pathways involved in antibody-mediated platelet depletion. Therapeutic interventions based on these results have been proven successful in treating human ITP, thus validating the use of these model systems. One major problem that remains to be answered is which cell populations are crucial for platelet removal. Targeting these cells directly might be a novel therapeutic strategy and will also be important to understand the underlying biological mechanisms

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Section: Effector Pathways Involved In Murine Itpsupporting

confidence: 73%

Section: Effector Cells and Organs Involved In Murine (And Human) Itpmentioning

confidence: 99%

Section: Effector Cells and Organs Involved In Murine (And Human) Itpmentioning

confidence: 99%

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The role of Fcγ receptors in murine autoimmune thrombocytopenia

et al. 2010

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“…S1). During the steady state, FcγRIV is expressed mainly on neutrophils, monocytes, and macrophages (14,15,18,19). To demonstrate deletion of FcγRIV on the protein level, we analyzed FcγRIV expression on neutrophils (expressing Ly6G) and monocytes (Ly6G negative, CD11b positive) in blood, spleen, and bone marrow.…”

Section: Resultsmentioning

confidence: 99%

“…An explanation for these observations was afforded by the identification of the mouse activating FcγRIV, which can bind to IgG2a and IgG2b with intermediate affinity (15). On the basis of protein sequence, genomic localization, and functional studies, mouse FcγRIV seems to be the ortholog to human CD16A, although it has some unique features, such as the capacity to bind to IgE with low affinity, and varies in its cellular expression pattern compared to its human counterpart (14,15,18,19). Using blocking antibodies, it was demonstrated that FcγRIV was essentially involved in IgG2a-and IgG2b-dependent killing of B cells, melanoma metastasis in the lung, and phagocytosis of platelets and red blood cells (11,14,15,(20)(21)(22).…”

mentioning

confidence: 99%

FcγRIV deletion reveals its central role for IgG2a and IgG2b activity in vivo

Nimmerjahn

Lux

Albert

et al. 2010

Proc. Natl. Acad. Sci. U.S.A.

170

156

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Cellular Fcγ receptors are essential for IgG-dependent effector functions in vivo. There is convincing evidence that selective activating Fcγ receptors are responsible for the activity of individual IgG subclasses. Thus, IgG1 activity is absent in FcγRIII-deficient mice, and several studies suggest that the activity of the most potent IgG subclasses, IgG2a and IgG2b, might be dependent on either individual or a combination of activating FcγRs. To study the role of individual activating FcγRs for IgG subclass activity, we generated an FcγRIV-deficient mouse and showed that a variety of IgG2a- and IgG2b-dependent effector functions are impaired in the absence of this activating Fc receptor in models of autoimmunity and antibody-dependent cellular cytotoxicity.

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