TY - JOUR
T1 - Passive transfer models of myasthenia gravis with muscle-specific kinase antibodies
AU - Verschuuren, Jan J. G. M.
AU - Plomp, Jaap J.
AU - Burden, Steve J.
AU - Zhang, Wei
AU - Fillie-Grijpma, Yvonne E.
AU - Stienstra-van Es, Inge E.
AU - Niks, Erik H.
AU - Losen, Mario
AU - van der Maarel, Silvere M.
AU - Huijbers, Maartje G.
PY - 2018/2/1
Y1 - 2018/2/1
N2 - Myasthenia gravis (MG) with antibodies to muscle-specific kinase (MuSK) is characterized by fluctuating fatigable weakness. In MuSK MG, involvement of bulbar muscles, neck, and shoulder and respiratory weakness are more prominent than in acetylcholine receptor (AChR) MG. MuSK autoantibodies are mainly of the IgG4 subclass, and as such are unable to activate complement, have low affinity for Fc receptors, and are functionally monovalent. Therefore, the pathogenicity of IgG4 MuSK autoantibodies was initially questioned. A broad collection of in vitro active immunization and passive transfer models has been developed that have shed light on the pathogenicity of MuSK autoantibodies. Passive transfer studies with purified IgG4 from MuSK MG patients confirmed that IgG4 is sufficient to reproduce clear clinical, electrophysiological, and histological signs of myasthenia. In vitro experiments revealed that MuSK IgG4 autoantibodies preferably bind the first Ig-like domain of MuSK, correlate with disease severity, and interfere with the association between MuSK and low-density lipoprotein receptor-related protein 4 and collagen Q. Some patients have additional IgG1 MuSK autoantibodies, but their role in the disease is unclear. Altogether, this provides a rationale for epitope-specific or IgG4-specific treatment strategies for MuSK MG and emphasizes the importance of the development of different experimental models.
AB - Myasthenia gravis (MG) with antibodies to muscle-specific kinase (MuSK) is characterized by fluctuating fatigable weakness. In MuSK MG, involvement of bulbar muscles, neck, and shoulder and respiratory weakness are more prominent than in acetylcholine receptor (AChR) MG. MuSK autoantibodies are mainly of the IgG4 subclass, and as such are unable to activate complement, have low affinity for Fc receptors, and are functionally monovalent. Therefore, the pathogenicity of IgG4 MuSK autoantibodies was initially questioned. A broad collection of in vitro active immunization and passive transfer models has been developed that have shed light on the pathogenicity of MuSK autoantibodies. Passive transfer studies with purified IgG4 from MuSK MG patients confirmed that IgG4 is sufficient to reproduce clear clinical, electrophysiological, and histological signs of myasthenia. In vitro experiments revealed that MuSK IgG4 autoantibodies preferably bind the first Ig-like domain of MuSK, correlate with disease severity, and interfere with the association between MuSK and low-density lipoprotein receptor-related protein 4 and collagen Q. Some patients have additional IgG1 MuSK autoantibodies, but their role in the disease is unclear. Altogether, this provides a rationale for epitope-specific or IgG4-specific treatment strategies for MuSK MG and emphasizes the importance of the development of different experimental models.
KW - autoimmune
KW - myasthenia gravis
KW - muscle-specific kinase
KW - animal model
KW - passive transfer
KW - ANTI-MUSK ANTIBODIES
KW - ACETYLCHOLINE-RECEPTOR ANTIBODIES
KW - MOUSE NEUROMUSCULAR-JUNCTION
KW - IGG4 AUTOANTIBODIES
KW - MUTATIONS
KW - MICE
KW - IMMUNIZATION
KW - SEVERITY
KW - DOMAIN
KW - PRE
U2 - 10.1111/nyas.13543
DO - 10.1111/nyas.13543
M3 - (Systematic) Review article
C2 - 29356029
SN - 0077-8923
VL - 1413
SP - 111
EP - 118
JO - Annals of the New York Academy of Sciences
JF - Annals of the New York Academy of Sciences
IS - 1
ER -