Involvement of Toso in activation of monocytes, macrophages, and granulocytes

Lang, Karl S.; Lang, Philipp A.; Meryk, Andreas; Pandyra, Aleksandra A.; Boucher, Louis-Martin; Pozdeev, Vitaly I.; Tusche, Michael W.; Göthert, Joachim R.; Haight, Jillian; Wakeham, Andrew; You-Ten, Annick; McIlwain, David R.; Merches, Katja; Khairnar, Vishal; Recher, Mike; Nolan, Garry P.; Hitoshi, Yasumichi; Funkner, Pauline; Navarini, Alexander A.; Verschoor, Admar; Shaabani, Namir; Honke, Nadine; Penn, Linda Z.; Ohashi, Pamela S.; Häussinger, Dieter; Lee, Kyeong-Hee; Mak, Tak W.

doi:10.1073/pnas.1222264110

Cited by 61 publications

(79 citation statements)

References 35 publications

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“…The FcμR expression began at the early immature B cell stage in bone marrow and continued through to plasmablast stage of differentiation, accompanied by transient down-modulation during GC reactions 6 . Contrary to this, Lang et al recently reported that Ly6G + bone marrow granulocytes and Mφs expressed FcμR at extremely low density on their cell surface 57 . Strangely, Ly6G - bone marrow cells which should contain a significant number of FcμR-expressing B cells, were negative with their B68 mAb 57 .…”

Section: Potential Functionsmentioning

confidence: 84%

“…Contrary to this, Lang et al recently reported that Ly6G + bone marrow granulocytes and Mφs expressed FcμR at extremely low density on their cell surface 57 . Strangely, Ly6G - bone marrow cells which should contain a significant number of FcμR-expressing B cells, were negative with their B68 mAb 57 . In this regard, we reexamined extensively and found that none of our mAbs reacted specifically with the cell surface of these phagocytes and that FcμR transcripts were clearly detectable in B-lineage cells but not in the double sorted Ly6G + granulocytes or in Rag1 -deficient splenocytes, which were devoid of B and T cells but contained abundant granulocytes and Mφs, even after 35 cycles of amplification 6, 58 .…”

Section: Potential Functionsmentioning

confidence: 84%

“…Fcmr KO mice have been independently generated by two laboratories, our collaborator Hiroshi Ohno at RIKEN in Yokohama and Tak Mak at Ontario Cancer Institute in Toronto, and recently have been characterized by four different groups of investigators and there are clear differences in the reported phenotypes 6, 57, 59, 60 . Although the basis for these discrepancies requires further investigations, it might be due to different strategies for gene targeting [ i.e., deletion of exon 2 to 4 6, 59 versus exon 2 to 8 57, 60 and the absence 6, 59 versus presence of the Neo gene 57, 60 in the mouse genome] or to other differences in mouse ages, environments including intestinal flora or reagents used.…”

Section: Potential Functionsmentioning

confidence: 99%

“…Although the basis for these discrepancies requires further investigations, it might be due to different strategies for gene targeting [ i.e., deletion of exon 2 to 4 6, 59 versus exon 2 to 8 57, 60 and the absence 6, 59 versus presence of the Neo gene 57, 60 in the mouse genome] or to other differences in mouse ages, environments including intestinal flora or reagents used. Nevertheless, the abnormal phenotypes commonly observed (in at least two laboratories) in Fcmr KO mice are: ( i ) increase in pre-immune serum IgM 6, 59 , ( ii ) alterations in B cell subpopulations 6, 59, 54 , ( iii ) dysregulation of humoral immune responses 6, 59, 54 , ( iv ) impairment of B cell proliferation upon ligation of BCR in vitro 59, 60 , and ( v ) predisposition to autoantibody production 6, 59, 54 .…”

Section: Potential Functionsmentioning

confidence: 99%

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The Long Elusive IgM Fc Receptor, FcμR

et al. 2014

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IgM exists as both a monomer on the surface of B cells and a pentamer secreted by plasma cells. Both preimmune “natural” and antigen-induced “immune” IgM antibodies are important for protective immunity and for immune regulation of autoimmune processes by recognizing pathogens and self-antigens. Effector proteins interacting with the Fc portion of IgM, such as complement and complement receptors, have thus far been proposed but fail to fully account for the IgM-mediated protection and regulation. A major reason for this deficit in our understanding of IgM function seems to be lack of data on a long elusive Fc receptor for IgM (FcμR). We have recently identified a bona fide FcμR in both humans and mice. In this article we briefly review what we have learned so far about FcμR.

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Section: Potential Functionsmentioning

confidence: 84%

Section: Potential Functionsmentioning

confidence: 84%

Section: Potential Functionsmentioning

confidence: 99%

Section: Potential Functionsmentioning

confidence: 99%

See 2 more Smart Citations

The Long Elusive IgM Fc Receptor, FcμR

et al. 2014

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“…The Journal of Immunology, 2015, 194: 4055-4057. Two laboratories (Ohno and Mak) had generated Fcmr/ Toso-deficient mice, and from 2012 to 2015 four groups of investigators independently characterized their phenotypes (11)(12)(13)(14)(15)(16)(17)(18)(19). Clear differences in the reported phenotypes, in addition to the cellular distribution of FcmR/Toso, were evident but are not discussed in this article because they are not directly related to the topic of this meeting.…”

Section: Nomenclature Of Toso Fas Apoptosis Inhibitory Molecule 3 Amentioning

confidence: 99%

Nomenclature of Toso, Fas Apoptosis Inhibitory Molecule 3, and IgM FcR

Kubagawa

Carroll

Jacob

et al. 2015

The Journal of Immunology

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Hiromi Kubagawa and John E. Coligan coordinated an online meeting to define an appropriate nomenclature for the cell surface glycoprotein presently designated by different names: Toso, Fas apoptosis inhibitory molecule 3 (FAIM3), and IgM FcR (FcμR). FAIM3 and Faim3 are the currently approved symbols for the human and mouse genes, respectively, in the National Center for Biotechnology Information, Ensembl, and other databases. However, recent functional results reported by several groups of investigators strongly support a recommendation for renaming FAIM3/Faim3 as FCMR/Fcmr, a name better reflecting its physiological function as the FcR for IgM. Participants included 12 investigators involved in studying Toso/FAIM3(Faim3)/FμR, representatives from the Human Genome Nomenclature Committee (Ruth Seal) and the Mouse Genome Nomenclature Committee (Monica McAndrews), and an observer from the IgM research field (Michael Carroll). In this article, we provide a brief background of the key research on the Toso/FAIM3(Faim3)/FcμR proteins, focusing on the ligand specificity and functional activity, followed by a brief summary of discussion about adopting a single name for this molecule and its gene and a resulting recommendation for genome nomenclature committees.

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Identification of the Fc‐alpha/mu receptor in Xenopus provides insight into the emergence of the poly‐Ig receptor (pIgR) and mucosal Ig transport

et al. 2021

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The polyimmunoglobulin receptor (pIgR) transcytoses J chain-containing antibodies through mucosal epithelia. In mammals, two cis-duplicates of PIGR, FCMR, and FCAMR, flank the PIGR gene. A PIGR duplication is first found in amphibians, previously annotated as PIGR2 (herein xlFCAMR), and is expressed by APCs. We demonstrate that xlFcamR is the equivalent of mammalian FcamR. It has been assumed that pIgR is the oldest member of this family, yet our data could not distinguish whether PIGR or FCAMR emerged first; however, FCMR was the last family member to emerge. Interestingly, bony fish "pIgR" is not an orthologue of tetrapod pIgR, and possibly acquired its function via convergent evolution. PIGR/FCAMR/FCMR are members of a larger superfamily, including TREM, CD300, and NKp44, which we name the "double-disulfide Ig superfamily" (ddIgSF). Domains related to each ddIgSF family were identified in cartilaginous fish (sharks, chimeras) and encoded in a single gene cluster syntenic to the human pIgR locus. Thus, the ddIgSF families date back to the earliest antibody-based adaptive immunity, but apparently not before. Finally, our data strongly suggest that the J chain arose in evolution only for Ig multimerization. This study provides a framework for further studies of pIgR and the ddIgSF in vertebrates.

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Involvement of Toso in activation of monocytes, macrophages, and granulocytes

Cited by 61 publications

References 35 publications

The Long Elusive IgM Fc Receptor, FcμR

The Long Elusive IgM Fc Receptor, FcμR

Nomenclature of Toso, Fas Apoptosis Inhibitory Molecule 3, and IgM FcR

Identification of the Fc‐alpha/mu receptor in Xenopus provides insight into the emergence of the poly‐Ig receptor (pIgR) and mucosal Ig transport

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