Letter to the Editor—Response to “Opioid-related xylazine toxicity manifesting as myonecrosis, rhabdomyolysis, multifocal ischemic cerebral infarcts, and cerebral edema”

Anthony Spadaro MD, MPH, Jennifer S. Love MD, Lewis S. Nelson MD, MBA, Howard A. Greller MD
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Abstract

To the Editors,

We commend the authors on their presentation of “Opioid-related xylazine toxicity manifesting as myonecrosis, rhabdomyolysis, multifocal ischemic cerebral infarcts, and cerebral edema”.1

However, we have significant concerns regarding their attribution of the adverse effects to xylazine. The case description is identical to that of a hypoxic, multiorgan system insult resulting from an opioid overdose, including liver injury, rhabdomyolysis, and cerebral infarcts. While the authors appropriately note that the unregulated fentanyl supply is increasingly adulterated with xylazine, “xylazine overdose” is currently always a xylazine–fentanyl overdose.2 Therefore, the contribution of fentanyl in overdose victims cannot be overlooked or underestimated, and especially given hearing loss, it is far more likely that the patient's injuries were due to fentanyl.3

The authors hypothesize that xylazine toxicity resulted in hemodynamic changes that contributed to microvascular constriction and infarcts. They cite animal studies or case studies of intentional xylazine overdose, which are not clinically analogous to human exposure to fentanyl adulterated with xylazine. Interestingly, patients with consequential xylazine-adulterated fentanyl exposures may be relatively hemodynamically stable. In a study of patients with such overdoses in whom xylazine was detected, there was no increase in the incidence or degree of bradycardia, coma, or need for ventilatory support.4 In fact, xylazine-exposed patients had lower rates of cardiopulmonary arrest. A potential explanation for this finding is that due to the addition of xylazine to the street product, they were exposed to less fentanyl overall.

The authors rely on urine drug screen (UDS) results to support that xylazine is the cause of the patient's presentation. Fentanyl and xylazine were detected on the UDS; however, there was no quantitative measurement of either fentanyl or xylazine to explain their relative contributions to the outcome. Regardless, because the detection window of a xylazine UDS is not known, it is not possible to know the time of last use or the temporal relationship between xylazine-adulterated fentanyl use and the development of clinical effects. There may be utility in adding xylazine to a UDS for epidemiological or research purposes or for educating patients on the contents of the unregulated drug supply, but there is no clear clinical utility for the management of patients with acute drug intoxication. Furthermore, the xylazine UDS may lead to premature diagnostic closure with a time-sensitive conditions, such as altered mental status.5 Although the emergence of xylazine in the unregulated drug supply is a public health concern, it should not distract from the fact that fentanyl is the major contributor to drug overdose deaths and that ventilatory support and naloxone remain the treatments of choice.

The authors declare they have no conflicts of interest.

The authors received no specific funding for this work.

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致编辑的信--对 "表现为肌坏死、横纹肌溶解、多灶性缺血性脑梗塞和脑水肿的阿片类药物相关恶性肿瘤 "的回应
致编辑:我们赞赏作者对 "阿片类药物相关的恶嗪中毒表现为肌坏死、横纹肌溶解、多灶性缺血性脑梗塞和脑水肿 "的描述1。然而,我们对作者将不良反应归咎于恶嗪的做法表示严重关切。病例描述与阿片类药物过量导致的缺氧性多器官系统损伤相同,包括肝损伤、横纹肌溶解和脑梗塞。虽然作者恰当地指出,不受管制的芬太尼供应越来越多地掺入了异丙嗪,但 "异丙嗪过量 "目前总是异丙嗪-芬太尼过量。因此,不能忽视或低估芬太尼在过量用药受害者中的作用,尤其是考虑到听力损失,患者的伤害更有可能是由芬太尼引起的。3 作者假设,异丙嗪中毒导致血液动力学变化,从而造成微血管收缩和梗塞。他们引用了动物实验或故意过量使用异丙嗪的病例研究,但这些实验在临床上并不能与人类接触掺有异丙嗪的芬太尼相提并论。有趣的是,因此而暴露于掺有异丙嗪的芬太尼的患者血流动力学可能相对稳定。在一项针对此类过量用药且检测出含有异丙嗪的患者的研究中,心动过缓、昏迷或呼吸支持需求的发生率或程度都没有增加。作者根据尿液药物筛查(UDS)结果来证明患者发病的原因是二甲嗪。UDS 中检测到了芬太尼和异丙嗪;但没有对芬太尼或异丙嗪进行定量测量,因此无法解释它们对结果的相对影响。无论如何,由于不知道 UDS 的检测窗口,因此无法知道最后一次使用的时间,也无法知道使用掺有异丙嗪的芬太尼与出现临床效应之间的时间关系。为了流行病学或研究目的,或为了教育病人了解不受管制的药物供应的内容,在 UDS 中加入异丙嗪可能有用,但对于急性药物中毒病人的管理没有明确的临床用途。此外,在精神状态改变等时效性较强的情况下,使用二甲苯嗪 UDS 可能会导致诊断过早结束。5 虽然二甲苯嗪出现在不受管制的药物供应中是一个公共卫生问题,但这不应分散人们的注意力,因为芬太尼是药物过量致死的主要原因,而通气支持和纳洛酮仍是首选治疗方法。
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