Author: Koh, Hui Moon; Chong, Pei Feng; Tan, Ju Nee; Chidambaram, Suresh Kumar; Chua, Hiu Jian
Title: QT prolongation associated with hydroxychloroquine and protease inhibitors in COVIDâ€19 Cord-id: 1z7sm184 Document date: 2021_3_25
ID: 1z7sm184
Snippet: WHAT IS KNOWN AND OBJECTIVE: Hydroxychloroquine and protease inhibitors were widely used as offâ€label treatment options for COVIDâ€19 but the safety data of these drugs among the COVIDâ€19 population are largely lacking. Drugâ€induced QTc prolongation is a known adverse reaction of hydroxychloroquine, especially during chronic treatment. However, when administered concurrently with potential proâ€arrhythmic drugs such as protease inhibitors, the risk of QTc prolongation imposed on these pa
Document: WHAT IS KNOWN AND OBJECTIVE: Hydroxychloroquine and protease inhibitors were widely used as offâ€label treatment options for COVIDâ€19 but the safety data of these drugs among the COVIDâ€19 population are largely lacking. Drugâ€induced QTc prolongation is a known adverse reaction of hydroxychloroquine, especially during chronic treatment. However, when administered concurrently with potential proâ€arrhythmic drugs such as protease inhibitors, the risk of QTc prolongation imposed on these patients is not known. We aim to investigate the incidence of QTc prolongation events and potential factors associated with its occurrence in COVIDâ€19 population. METHODS: We included 446 SARSâ€CoVâ€2 RTâ€PCRâ€positive patients taking at least one treatment drug for COVIDâ€19 within a period of one month (March–April 2020). In addition to COVIDâ€19â€related treatment (HCQ/PI), concomitant drugs with risks of QTc prolongation were considered. We defined QTc prolongation as QTc interval of ≥470 ms in postpubertal males, and ≥480 ms in postpubertal females. RESULTS AND DISCUSSION: QTc prolongation events occurred in 28/446 (6.3%) patients with an incidence rate of 1 case per 100 personâ€days. A total of 26/28 (93%) patients who had prolonged QTc intervals received at least two proâ€QT drugs. Multivariate analysis showed that HCQ and PI combination therapy had five times higher odds of QTc prolongation as compared to HCQâ€only therapy after controlling for age, cardiovascular disease, SIRS and the use of concurrent QTcâ€prolonging agents besides HCQ and/or PI (OR 5.2; 95% CI, 1.11â€24.49; p = 0.036). Independent of drug therapy, presence of SIRS resulted in four times higher odds of QTc prolongation (OR 4.3; 95% CI, 1.66â€11.06; p = 0.003). In HCQâ€PI combination group, having concomitant proâ€QT drugs led to four times higher odds of QTc prolongation (OR 3.8; 95% CI, 1.53â€9.73; p = 0.004). Four patients who had prolonged QTc intervals died but none were cardiacâ€related deaths. WHAT IS NEW AND CONCLUSION: In our cohort, hydroxychloroquine monotherapy had low potential to increase QTc intervals. However, when given concurrently with protease inhibitors which have possible or conditional risk, the odds of QTc prolongation increased fivefold. Interestingly, independent of drug therapy, the presence of systemic inflammatory response syndrome (SIRS) resulted in four times higher odds of QTc prolongation, leading to the postulation that some QTc events seen in COVIDâ€19 patients may be due to the disease itself. ECG monitoring should be continued for at least a week from the initiation of treatment.
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