Dynamics of the human antibody repertoire after B cell depletion in systemic sclerosis
Charles F. A. de Bourcy(Stanford University), Cornelia L. Dekker(Stanford University), Mark M. Davis(Howard Hughes Medical Institute), Mark R. Nicolls(VA Palo Alto Health Care System), Stephen R. Quake(Chan Zuckerberg Initiative (United States))
Cited by 55Open Access
Abstract
) proportion with reduced mutation loads and an expanded proportion of highly antibody-secreting cells. Disease signatures pertaining to IGHV2-5 segment usage, IgD proportions, and mutation loads were temporarily reversed after B cell depletion. Analyzing the time course of B cell depletion, we find that the kinetics of naïve replenishment are predictable from baseline measurements alone, that release of plasma cells into the periphery can precede naïve replenishment, and that modes of B cell receptor diversity are highly elastic. Our findings reveal humoral immune signatures of SSc-PAH and uncover determinism in the effects of B cell depletion on the antibody repertoire.
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