BackgroundThere is no specific serum-based biomarker for the diagnosis or prognosis of
relapsing-remitting multiple sclerosis (RRMS).ObjectiveWe investigated whether levels of IgM antibodies to
Glc(α1,4)Glc(α) (GAGA4) or to a panel of four
glucose-based glycans could differentiate MS from other neurological
diseases (OND) or predict risk of early relapse following first presentation
(FP) of RRMS.MethodsRetrospective analysis of 440 sera samples of three cohorts: A) FP-RRMS (n =
44), OND (n = 44); B) FP-RRMS (n = 167), OND (n = 85); and C) FP (n = 100).
Anti-GAGA4 IgM levels were measured by enzyme immunoassay in cohort-A and
cohort-B. Cohort-C IgM antibodies to glucosebased glycan panel were measured
by immunofluorescence.ResultsFP-RRMS had higher levels of anti-GAGA4 IgM than OND patients (cohort-A, P =
0.01; cohort-B, P = 0.0001). Sensitivity and specificity were 27% and 97%
for cohort-A; and 26% and 90% for cohort-B, respectively. In cohort-C, 58
patients experienced early relapse (<24 months), 31 had late
relapse (≥24 months), and 11 did not experience second attack
during follow-up. Kaplan– Meier curves demonstrated decrease in
time to next relapse for patients positive for the antibody panel (P = 0.02,
log rank).ConclusionsSerum anti-GAGA4 IgM discerns FP-RRMS patients from OND patients. Higher
levels of serum anti-α-glucose IgM in FP patients predict
imminent early relapse.
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