Ab. Mongey et al., Acetylation status is associated with serological changes but not clinically significant disease in patients receiving procainamide, J RHEUMATOL, 26(8), 1999, pp. 1721-1726
Objective. Autoantibodies occur in the majority of patients receiving proca
inamide (PA) for more than one year. Slow acetylator status has been propos
ed to predispose to their development. We previously reported the results o
f serological evaluation of 52 asymptomatic patients receiving PA. The aims
of this study were to follow these patients to determine the incidence of
drug related lupus (DRL) and serologic changes in patients receiving longte
rm PA therapy, and to evaluate the possible effect of acetylator status on
the development of PA autoimmunity.
Methods, Fifty-two patients receiving PA were reevaluated after a mean of 3
1.5 months. Antinuclear antibodies and antibodies to histones, dsDNA, and p
olyadenylic acid (PolyA) were assayed, Acetylator status was determined by
phenotyping and genotyping methods. Five additional patients referred with
a diagnosis of DRL were also evaluated.
Results. Autoantibodies were detected in the majority of patients still rec
eiving PA and in some patients in whom PA had been discontinued, Slow acety
lator status correlated with IgG antibodies to the H2A-2B dimer complex, Ac
etylator status did not correlate with PA dose. Seven of the 9 patients wit
h PA related lupus were fast acetylators.
Conclusion. Most patients receiving PA have autoantibodies that may persist
after discontinuation of PA, Despite persistently high frequency of autoan
tibodies the majority of these patients did not develop DRL. Slow acetylato
r status correlated with IgG antibodies to H2A-2B but was not a risk factor
for the development of PA related lupus.