RT Journal Article SR Electronic T1 Clinical utility of AQP4-IgG titers and measures of complement-mediated cell killing in NMOSD JF Neurology - Neuroimmunology Neuroinflammation JO Neurol Neuroimmunol Neuroinflamm FD Lippincott Williams & Wilkins SP e727 DO 10.1212/NXI.0000000000000727 VO 7 IS 4 A1 Jitprapaikulsan, Jiraporn A1 Fryer, James P. A1 Majed, Masoud A1 Smith, Carin Y. A1 Jenkins, Sarah M. A1 Cabre, Philippe A1 Hinson, Shannon R. A1 Weinshenker, Brian G. A1 Mandrekar, Jay A1 Chen, John J. A1 Lucchinetti, Claudia F. A1 Jiao, Yujuan A1 Segan, Jessica A1 Schmeling, John E. A1 Mills, John A1 Flanagan, Eoin P. A1 McKeon, Andrew A1 Pittock, Sean J. YR 2020 UL http://nn.neurology.org/content/7/4/e727.abstract AB Objective To investigate whether aquaporin-4–immunoglobulin G (AQP4-IgG) titers and measures of complement-mediated cell killing are clinically useful to predict the occurrence of relapse, relapse severity, and/or disability in neuromyelitis optica spectrum disorder (NMOSD).Methods We studied 336 serial serum specimens from 82 AQP4-lgG–seropositive patients. NMOSD activity at blood draw was defined as preattack (24 [7.1%], drawn within 30 days preceding an attack), attack (108 [32.1%], drawn on attack onset or within 30 days after), or remission (199 [59.2%], drawn >90 days after attack onset and >30 days preceding a relapse). For each specimen, we documented the attack type and severity and immunotherapy status. Complement-mediated cell killing was quantitated by flow cytometry using an M23-AQP4 cell-based assay.Results The estimated logarithmic means of AQP4-IgG titers in preattack, attack, and remission samples were 3.302, 3.657, and 3.458, respectively, p = 0.21. Analyses of 81 attack/remission pairs in 42 patients showed no significant titer differences (3.736 vs 3.472, p = 0.15). Analyses of 13 preattack/attack pairs in 9 patients showed no significant titer differences (3.994 vs 3.889, p = 0.67). Of 5 patients who converted to seronegative status, 2 continued to have attacks. Titers for major and minor attacks (n = 70) were not significantly different (3.905 vs 3.676, p = 0.47). Similarly, measures (titers) of complement-mediated cell killing were not significantly associated with disease course, attack severity, or disability at 5 years.Conclusions and relevance AQP4-IgG titer and complement-mediated cell killing lack significant prognostic or predictive utility in NMOSD. Although titers may drop in the setting of immunotherapy, seroconversion to negative status does not preclude ongoing clinical attacks.Classification of evidence This study provides Class II evidence that in patients with NMOSD, AQP4-IgG titers and measures of complement-mediated cell killing activity do not predict relapses, relapse severity, or disability.AChR=acetylcholine receptor; AQP4=aquaporin-4; EDSS=Expanded Disability Status Scale; GEE=generalized estimating equation; HSCT=hematopoietic stem cell transplantation; IgG=immunoglobulin G; IVMP=IV methylprednisolone; NMDAR=NMDA receptor; NMOSD=neuromyelitis optica spectrum disorder; ON=optic neuritis; PI=propidium iodide; PLEX=plasma exchange; TM=transverse myelitis