Publication date: Oct 01, 2024
Neurologic post-COVID-19 condition (PCC), or long COVID, symptoms of fatigue and cognitive dysfunction continue to affect millions of people who have been infected with SARS-CoV-2. There currently are no effective evidence-based therapies available for treating neurologic PCC. To assess the effects of lithium aspartate therapy on PCC fatigue and cognitive dysfunction. A randomized, double-blind, placebo-controlled trial (RCT) enrolling participants in a neurology clinic from November 28, 2022, to June 29, 2023, with 3 weeks of follow-up, was conducted. Subsequently, an open-label lithium dose-finding study with 6 weeks of follow-up was performed among the same participants enrolled in the RCT. Eligible individuals needed to report new, bothersome fatigue or cognitive dysfunction persisting for more than 4 weeks after a self-reported positive test for COVID-19, Fatigue Severity Scale-7 (FSS-7) or Brain Fog Severity Scale (BFSS) score of 28 or greater, Beck Depression Inventory-II score less than 24, and no history of a condition known to cause fatigue or cognitive dysfunction. All participants in the RCT were eligible for the dose-finding study, except for those who responded to the placebo. Intention-to-treat analysis was used. Lithium aspartate, 10 to 15 mg/d, or identically appearing placebo for 3 weeks followed by open-label lithium aspartate, 10 to 15 mg/d, for 2 weeks. In the subsequent dose-finding study, open-label lithium aspartate dosages up to 45 mg/d for 6 weeks were given. Change in sum of FSS-7 and BFSS scores. The scores for each measure range from 7 to 49, with higher scores indicating more severe symptoms. Secondary outcomes included changes from baseline in the scores of additional questionnaires. Fifty-two participants were enrolled (30 [58%] males; mean [SD] age, 58. 54 [14. 34] years) and 26 were randomized to treatment with lithium aspartate (10 females) and 26 to placebo (12 female). Two participants assigned to lithium aspartate were lost to follow-up and none withdrew. No adverse events were attributable to lithium therapy. There were no significant intergroup differences for the primary outcome (-3. 6; 95% CI, -16. 6 to 9. 5; Pā=ā. 59) or any secondary outcomes. Among 3 patients completing a subsequent dose-finding study, open-label lithium aspartate, 40 to 45 mg/d, was associated with numerically greater reductions in fatigue and cognitive dysfunction scores than 15 mg/d, particularly in 2 patients with serum lithium levels of 0. 18 and 0. 49 mEq/L compared with 1 patient with a level of 0. 10 mEq/L. In this RCT, therapy with lithium aspartate, 10 to 15 mg/d, was ineffective for neurologic PCC fatigue and cognitive dysfunction. Another RCT is required to assess the potential benefits of higher lithium dosages for treating neurologic PCC. ClinicalTrials. gov Identifier: NCT05618587 and NCT06108297.
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Semantics
Type | Source | Name |
---|---|---|
disease | MESH | Long COVID |
disease | MESH | Cognitive Dysfunction |
disease | MESH | COVID-19 |
drug | DRUGBANK | Factor IX Complex (Human) |
disease | MESH | Brain Fog |
disease | MESH | Depression |
disease | IDO | history |
disease | MESH | lost to follow-up |
disease | MESH | Infectious Diseases |
disease | IDO | intervention |
disease | MESH | bipolar disorder |
disease | MESH | neuroinflammation |
disease | MESH | Parkinson disease |
pathway | KEGG | Parkinson disease |
drug | DRUGBANK | Water |
disease | MESH | Anxiety Disorder |
disease | MESH | Insomnia |
drug | DRUGBANK | Tropicamide |
drug | DRUGBANK | Microcrystalline cellulose |
drug | DRUGBANK | Lithium carbonate |
disease | MESH | cancers |
disease | MESH | brain inflammation |
drug | DRUGBANK | L-Aspartic Acid |