In generalized myasthenia gravis (gMG), the therapeutic rationale for complement C5 inhibition is grounded in a well-defined immunopathological cascade.
Immunoglobulins are the central effector molecules of adaptive humoral immunity. They are produced by B cells and their terminally differentiated plasma cells and contribute to pathogen clearance, maintenance of immune homeostasis, and the development of immunopathology through a dual ...
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