Abstract
Several studies have suggested that the autoantibodies (autoAbs) against muscle acetylcholine receptor (AChR) of myasthenia gravis (MG) patients are the main pathogenic factor in MG; however, this belief has not yet been confirmed with direct observations. Although animals immunized with AChR or injected with anti-AChR monoclonal Abs, or with crude human MG Ig fractions exhibit MG symptoms, the pathogenic role of isolated anti-AChR autoAbs, and, more importantly, the absence of pathogenic factor(s) in the autoAb-depleted MG sera has not yet been shown by in vivo studies. Using recombinant extracellular domains of the human AChR α and β subunits, we have isolated autoAbs from the sera of four MG patients. The ability of these isolated anti-subunit Abs and of the Ab-depleted sera to passively transfer experimental autoimmune MG in Lewis rats was investigated. We found that the isolated anti-subunit Abs were at least as efficient as the corresponding whole sera or whole Ig in causing experimental MG. Abs to both α- and β-subunit were pathogenic although the anti-α-subunit were much more efficient than the anti-β-subunit ones. Interestingly, the autoAb-depleted sera were free of pathogenic activity. The later suggests that the myasthenogenic potency of the studied anti-AChR MG sera is totally due to their anti-AChR autoAbs, and therefore selective elimination of the anti-AChR autoAbs from MG patients may be an efficient therapy for MG.
Highlights
Myasthenia gravis (MG) is considered the classical organ specific, autoantibody-mediated, and T cell dependent human autoimmune disease [1,2,3,4,5,6]
In order to select potent MG sera, first we screened over 100 MG sera for binding to both rat and human acetylcholine receptor (AChR) by RIA
We found that the MG sera showed varying degree of Ab cross-reactivity between the two AChR species
Summary
Myasthenia gravis (MG) is considered the classical organ specific, autoantibody-mediated, and T cell dependent human autoimmune disease [1,2,3,4,5,6]. MG is associated with autoantibodies (autoAbs) against the acetylcholine receptor (AChR) of the neuromuscular junction (NMJ). These autoAbs are found in approximately 85% of the patients with generalized MG (AChRMG) [1,2], while the remaining ,15% of MG patients have autoAbs to additional NMJ proteins: MuSK (Muscle-Specific Kinase) [7,8,9] and LRP4 (lipoprotein receptor-related protein) [10,11] or not yet detectable autoAbs [12]. MG patients are suffering from fatigability and weakness of skeletal muscles, usually due to destruction of the AChRs in the NMJ [2,3,4,13]. Muscle AChRs bear one binding site per a-subunit for acetylcholine (ACh), the neurotransmitter which is responsible for the transmission of the nerve impulse to the muscle fibers [14,15]
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