High risk of hypoxemic COVID-19 pneumonia in myasthenia gravis patients with type I IFN autoantibodies
Gervais, A.; Marchal, A.; Maillard, A.; Le Voyer, T.; Rosain, J.; Philipot, Q.; Bizien, L.; Peel, J.; Cederholm, A.; Migaud, M.; Pons, S.; Saker, K.; Laforet, P.; Aubart, M.; Gitiaux, C.; Biggs, C.; Leon Lopez, R.; Souvannanorath, S.; Tard, C.; Nadaj Pakleza, A.; Grapperon, A.-M.; Heming, N.; Annane, D.; Verschueren, A.; Attarian, S.; Bigaut, K.; Hankiewicz, K.; Kouton, L.; Villar-Quiles, R.-N.; Cauquil, C.; Fleury, M.-C.; Rocher, E.; Nicolas, G.; de Paula Estephan, E.; da Penha Ananias Morita, M.; Zanoteli, E.; Saied, Z.; Rachdi, A.; Rim, A.; Belal, S.; Ben Sassi, S.; Hubers, A.; Faure, E.; D
Show abstract
Patients with myasthenia gravis (MG) may produce autoantibodies neutralizing type I interferons (AAN-I-IFN), which have been shown to underlie severe viral diseases, including critical COVID-19 pneumonia, in patients without MG. We studied an international cohort of 85 unvaccinated SARS-CoV-2-infected MG patients with no antiviral treatment. Hypoxemic pneumonia occurred in 48 of these patients, including 22 (45.8%) with AAN-I-IFN, which neutralized both IFN-2 and IFN-{omega} in 14 (29.2%) patients. Six (16.2%) of the remaining 37 patients had AAN-I-IFN, which neutralized both IFN-2 and IFN-{omega} in three patients. The risk of hypoxemic pneumonia was greater in MG patients with AAN-I-IFN neutralizing 10 ng/mL of both IFN-2 and IFN-{omega} (odds ratio and 95% confidence interval (OR [95% CI]): 12.7 [2.1-78.9], p=0. 0010) or IFN-2 at any dose (4.7 [1.5-15.0], p=0.0054) than in those without such autoantibodies. The risk of AAN-I-IFN production was much higher in MG patients than in the general population (28.9 [10.8-77.7], p=4.9x10-27). Fourteen patients had thymoma, which increased the risk of AAN-I-IFN (64% versus 27%, (OR [95% CI]: 5.6 [1.6-19.4], p=0.0050) and hypoxemic pneumonia (9.2 [1.9-44.2]; p=0.0019). Thymoma is, thus, associated with a higher risk of producing AAN-I-IFN, and these autoantibodies are associated with a higher risk of developing life-threatening COVID-19 pneumonia in patients with MG.
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