Author: Patel, Oneel; Chinni, Vidyasagar; Elâ€Khoury, John; Perera, Marlon; Neto, Ary S.; McDonald, Christine; See, Emily; Jones, Daryl; Bolton, Damien; Bellomo, Rinaldo; Trubiano, Jason; Ischia, Joseph
Title: A pilot doubleâ€blind safety and feasibility randomized controlled trial of highâ€dose intravenous zinc in hospitalized COVIDâ€19 patients Cord-id: ixjye9vg Document date: 2021_3_9
ID: ixjye9vg
Snippet: Zinc inhibits replication of the SARSâ€CoV virus. We aimed to evaluate the safety, feasibility, and biological effect of administering highâ€dose intravenous zinc (HDIVZn) to patients with COVIDâ€19. We performed a Phase IIa doubleâ€blind, randomized controlled trial to compare HDIVZn to placebo in hospitalized patients with COVIDâ€19. We administered trial treatment per day for a maximum of 7 days until either death or hospital discharge. We measured zinc concentration at baseline and duri
Document: Zinc inhibits replication of the SARSâ€CoV virus. We aimed to evaluate the safety, feasibility, and biological effect of administering highâ€dose intravenous zinc (HDIVZn) to patients with COVIDâ€19. We performed a Phase IIa doubleâ€blind, randomized controlled trial to compare HDIVZn to placebo in hospitalized patients with COVIDâ€19. We administered trial treatment per day for a maximum of 7 days until either death or hospital discharge. We measured zinc concentration at baseline and during treatment and observed patients for any significant side effects. For eligible patients, we randomized and administered treatment to 33 adult participants to either HDIVZn (n = 15) or placebo (n = 18). We observed no serious adverse events throughout the study for a total of 94 HDIVZn administrations. However, three participants in the HDIVZn group reported infusion site irritation. Mean serum zinc on Day 1 in the placebo, and the HDIVZn group was 6.9 ± 1.1 and 7.7 ± 1.6 µmol/l, respectively, consistent with zinc deficiency. HDIVZn, but not placebo, increased serum zinc levels above the deficiency cutoff of 10.7 µmol/l (p < .001) on Day 6. Our study did not reach its target enrollment because stringent public health measures markedly reduced patient hospitalizations. Hospitalized COVIDâ€19 patients demonstrated zinc deficiency. This can be corrected with HDIVZn. Such treatment appears safe, feasible, and only associated with minimal peripheral infusion site irritation. This pilot study justifies further investigation of this treatment in COVIDâ€19 patients.
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