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本文引用的文献

1
Relapsing thrombotic microangiopathy and intravenous sustained-release oxycodone.复发性血栓性微血管病与静脉注射缓释羟考酮
Clin Kidney J. 2016 Aug;9(4):580-2. doi: 10.1093/ckj/sfw039. Epub 2016 May 30.
2
THROMBOTIC MICROANGIOPATHY ASSOCIATED WITH OPANA ER INTRAVENOUS ABUSE A Case Report.与奥施康定静脉滥用相关的血栓性微血管病 病例报告
J Med Liban. 2016 Jan-Mar;64(1):40-2. doi: 10.12816/0023831.
3
A Proactive Response to Prescription Opioid Abuse.对处方阿片类药物滥用的积极应对措施。
N Engl J Med. 2016 Apr 14;374(15):1480-5. doi: 10.1056/NEJMsr1601307. Epub 2016 Feb 4.
4
Hemoglobinuria-related acute kidney injury is driven by intrarenal oxidative reactions triggering a heme toxicity response.血红蛋白尿相关性急性肾损伤是由触发血红素毒性反应的肾内氧化反应驱动的。
Cell Death Dis. 2016 Jan 21;7(1):e2064. doi: 10.1038/cddis.2015.392.
5
Increases in Drug and Opioid Overdose Deaths--United States, 2000-2014.药物和阿片类药物过量死亡人数增加 - 美国,2000-2014 年。
MMWR Morb Mortal Wkly Rep. 2016 Jan 1;64(50-51):1378-82. doi: 10.15585/mmwr.mm6450a3.
6
Haptoglobin Preserves Vascular Nitric Oxide Signaling during Hemolysis.触珠蛋白在溶血过程中可维持血管一氧化氮信号传导。
Am J Respir Crit Care Med. 2016 May 15;193(10):1111-22. doi: 10.1164/rccm.201510-2058OC.
7
Rapamycin protects against gentamicin-induced acute kidney injury via autophagy in mini-pig models.在小型猪模型中,雷帕霉素通过自噬作用预防庆大霉素诱导的急性肾损伤。
Sci Rep. 2015 Jun 8;5:11256. doi: 10.1038/srep11256.
8
Community Outbreak of HIV Infection Linked to Injection Drug Use of Oxymorphone--Indiana, 2015.2015年印第安纳州与注射使用羟考酮相关的艾滋病毒感染社区疫情
MMWR Morb Mortal Wkly Rep. 2015 May 1;64(16):443-4.
9
Intravenous OxyContin-associated thrombotic microangiopathy treated successfully without plasma exchange.静脉注射奥施康定相关血栓性微血管病未经血浆置换成功治愈。
Med J Aust. 2015 Apr 6;202(6):330-1. doi: 10.5694/mja14.01125.
10
Haptoglobin, hemopexin, and related defense pathways-basic science, clinical perspectives, and drug development.触珠蛋白、血红素结合蛋白及相关防御途径:基础科学、临床观点与药物研发。
Front Physiol. 2014 Oct 28;5:415. doi: 10.3389/fphys.2014.00415. eCollection 2014.

与静脉注射滥用奥施康定缓释片相关的血栓性微血管病的机制研究。

A mechanistic investigation of thrombotic microangiopathy associated with IV abuse of Opana ER.

作者信息

Hunt Ryan, Yalamanoglu Ayla, Tumlin James, Schiller Tal, Baek Jin Hyen, Wu Andrew, Fogo Agnes B, Yang Haichun, Wong Edward, Miller Peter, Buehler Paul W, Kimchi-Sarfaty Chava

机构信息

Division of Plasma Protein Therapeutics, Office of Tissues and Advanced Therapies and.

Division of Blood Components and Devices, Office of Blood Research and Review, Center for Biologics Evaluation and Research, US Food and Drug Administration, Silver Spring, MD.

出版信息

Blood. 2017 Feb 16;129(7):896-905. doi: 10.1182/blood-2016-08-736579. Epub 2016 Nov 18.

DOI:10.1182/blood-2016-08-736579
PMID:27864296
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5314814/
Abstract

Since 2012, a number of case reports have described the occurrence of thrombotic microangiopathy (TMA) following IV abuse of extended-release oxymorphone hydrochloride (Opana ER), an oral opioid for long-term treatment of chronic pain. Here, we present unique clinical features of 3 patients and investigate IV exposure to the tablet's inert ingredients as a possible causal mechanism. Guinea pigs were used as an animal model to understand the hematopathologic and nephrotoxic potential of the inert ingredient mixture (termed here as PEO+) which primarily contains high-molecular-weight polyethylene oxide (HMW PEO). Microangiopathic hemolytic anemia, thrombocytopenia, and acute kidney injury were found in a group of 3 patients following recent injection of adulterated extended-release oxymorphone tablets. Varying degrees of cardiac involvement and retinal ischemia occurred, with TMA evident on kidney biopsy. A TMA-like state also developed in guinea pigs IV administered PEO+. Acute tubular and glomerular renal injury was accompanied by nonheme iron deposition and hypoxia-inducible factor-1α upregulation in the renal cortex. Similar outcomes were observed following dosing with HMW PEO alone. IV exposure to the inert ingredients in reformulated extended-release oxymorphone can elicit TMA. Although prescription opioid abuse shows geographic variation, all physicians should be highly inquisitive of IV drug abuse when presented with cases of TMA.

摘要

自2012年以来,已有多篇病例报告描述了静脉注射滥用盐酸羟考酮缓释片(奥施康定)后发生血栓性微血管病(TMA)的情况,奥施康定是一种用于长期治疗慢性疼痛的口服阿片类药物。在此,我们介绍3例患者的独特临床特征,并调查静脉接触该片剂的惰性成分作为一种可能的致病机制。使用豚鼠作为动物模型,以了解主要含有高分子量聚环氧乙烷(HMW PEO)的惰性成分混合物(在此称为PEO+)的血液病理学和肾毒性潜力。在一组近期注射掺假盐酸羟考酮缓释片的3例患者中发现了微血管病性溶血性贫血、血小板减少和急性肾损伤。出现了不同程度的心脏受累和视网膜缺血,肾活检显示有TMA。静脉注射PEO+的豚鼠也出现了类似TMA的状态。急性肾小管和肾小球肾损伤伴有肾皮质非血红素铁沉积和缺氧诱导因子-1α上调。单独给予HMW PEO后也观察到类似结果。静脉接触重新配方的盐酸羟考酮缓释片中的惰性成分可引发TMA。尽管处方阿片类药物滥用存在地域差异,但所有医生在面对TMA病例时都应高度怀疑静脉药物滥用情况。