CD5L is a canonical component of circulatory IgM

Author:

Oskam NienkeORCID,den Boer Maurits A.ORCID,Lukassen Marie V.,Heer Pleuni Ooijevaar-de,Veth Tim S.,Mierlo Gerard van,Lai Szu-Hsueh,Derksen Ninotska I.L.,Yin Victor C.ORCID,Streutker Marij,Franc Vojtech,Siborova Marta,Damen Mirjam,Kos Dorien,Barendregt Arjan,Bondt AlbertORCID,Goudoever Johannes B. vanORCID,Haas Carla J.C.,Aerts Piet C.,Muts Remy M.,Rooijakkers Suzan H.M.ORCID,Vidarsson GesturORCID,Rispens TheoORCID,Heck Albert J.R.ORCID

Abstract

AbstractImmunoglobulin M (IgM) is an evolutionary conserved key component of humoral immunity, and the first antibody isotype to emerge during an immune response. IgM is a large (1 MDa), multimeric protein, for which both hexameric and pentameric structures have been described, the latter additionally containing a joining (J) chain. Using a combination of single-particle mass spectrometry and mass photometry, proteomics and immunochemical assays, we here demonstrate that circulatory (serum) IgM exclusively exists as a complex of J-chain-containing pentamers covalently bound to the small CD5 antigen-like (CD5L, 36 kDa) protein. In sharp contrast, secretory IgM in saliva and milk is principally devoid of CD5L. Unlike IgM itself, CD5L is not produced by B cells, implying that it associates with IgM in the extracellular space. We demonstrate that CD5L integration has functional implications, i.e., it diminishes IgM binding to two of its receptors, the FcαµR and the polymeric Immunoglobulin receptor (pIgR). On the other hand, binding to FcµR as well as complement activation via C1q seem unaffected by CD5L integration. Taken together, we redefine the composition of circulatory IgM as a J-chain containing pentamer, always in complex with CD5L.

Publisher

Cold Spring Harbor Laboratory

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