Hydroxychloroquine-azithromycin, doubase C, and QTc prolongation in congolese patients with COVID-19: Myth or reality?

Brady Madioko Makanzu, Jean-Robert Makulo, Madone Ndona Mandina, Dimosi Roger Wumba, Murielle Mashi Longokolo, Hippolyte Situakibanza, Ossam Odio, Donat Sonzi Mangala, Constantin Mihigo Bashengezi, Benjamin Kabwe Mwilambwe, Gilbert Kabanda Kurhenga, Benjamin Longo-Mbenza, Roger Mwimba Mbungu
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Abstract

Background: QTc interval prolongation with an increased risk of torsade de pointes (Tsd) has been described in coronavirus disease 2019 (COVID-19) patients treated with hydroxychloroquine (HCQ) and azithromycin (AZI) in Western countries. In the DR Congo, few studies have evaluated the safety of this association or proposed new molecules.

Aim: To determine the incidence of QTc prolongation and Tsd in COVID-19 patients treated with HCQ-AZIs vs doubase C (new molecule).

Methods: In present randomized clinical trial, we have included patients with mild or moderate COVID-19 treated with either HCQ-AZI or doubase C. Electrocardiogram (ECG) changes on day 14 of randomization were determined based on pretreatment tracing. Prolonged QTc was defined as ≥ 500 ms on day 14 or an increase of ≥ 80 ms compared to pretreatment tracing. Patients with cardiac disease, those undergoing other treatments likely to prolong QTc, and those with disturbed ECG tracings were excluded from the study.

Results: The study included 258 patients (mean age 41 ± 15 years; 52% men; 3.4% diabetics, 11.1% hypertensive). Mild and moderate COVID-19 were found in 93.5% and 6.5% of patients, respectively. At baseline, all patients had normal sinus rhythm, a mean heart rate 78 ± 13/min, mean PR space 170 ± 28 ms, mean QRS 76 ± 13 ms, and mean QTc 405 ± 30 ms. No complaints suggesting cardiac involvement were reported during or after treatment. Only four patients (1.5%) experienced QTc interval prolongation beyond 500 ms. Similarly, only five patients (1.9%) had an increase in the QTc interval of more than 80 ms. QTc prolongation was more significant in younger patients, those with high viral load at baseline, and those receiving HCQ-AZI (P < 0.05). None of the patients developed Tsd.

Conclusion: QTc prolongation without Tsd was observed at a lower frequency in patients treated with HCQ-AZI vs doubase C. The absence of comorbidities and concurrent use of other products that are likely to cause arrhythmia may explain our results.

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COVID-19刚果患者的羟氯喹-阿奇霉素、双酶C和QTc延长:神话还是现实?
背景:在西方国家,接受羟氯喹(HCQ)和阿奇霉素(AZI)治疗的2019年冠状病毒病(COVID-19)患者中出现了QTc间期延长并增加了心搏过速(Tsd)的风险。在刚果(金),很少有研究对这种关联或新分子的安全性进行评估。目的:确定接受HCQ-AZIs与双酶C(新分子)治疗的COVID-19患者QTc延长和Tsd的发生率:在本随机临床试验中,我们纳入了接受HCQ-AZI或doubase C治疗的轻度或中度COVID-19患者。QTc延长的定义是:第14天QTc≥500毫秒,或与治疗前描记相比QTc增加≥80毫秒。研究排除了心脏病患者、正在接受其他可能导致 QTc 延长的治疗的患者以及心电图描记紊乱的患者:研究共纳入 258 名患者(平均年龄 41 ± 15 岁;52% 为男性;3.4% 为糖尿病患者,11.1% 为高血压患者)。发现轻度和中度 COVID-19 的患者分别占 93.5%和 6.5%。基线时,所有患者的窦性心律正常,平均心率(78±13)/分钟,平均 PR 间期(170±28)毫秒,平均 QRS(76±13)毫秒,平均 QTc(405±30)毫秒。在治疗期间或治疗后,均未出现心脏受累的主诉。只有四名患者(1.5%)的 QTc 间期延长超过 500 毫秒。同样,只有五名患者(1.9%)的 QTc 间期延长超过 80 毫秒。QTc延长在年轻患者、基线病毒载量高的患者和接受HCQ-AZI治疗的患者中更为显著(P < 0.05)。没有一名患者出现 Tsd:没有合并症和同时使用其他可能导致心律失常的产品可能是我们得出结论的原因。
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