The Comparative Pharmacokinetics of Physical Manipulation by Crushing of Xtampza
            <sup>®</sup>
            ER Compared with OxyContin
            <sup>®</sup>

Brennan, Michael J.; Kopecky, Ernest A.; Marseilles, Ann; O’Connor, Melinda; Fleming, Alison B.

doi:10.2217/pmt-2017-0030

Cited by 6 publications

(16 citation statements)

References 16 publications

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“…Table 1 summarizes the abuse-deterrence claims from the prescribing information for commercially available abuse-deterrent opioids [18][19][20][21][34][35][36][37][38][39][40][41][42][43][44][45][46][47][48][49][50]. All abuse-deterrent opioid labels include a statement saying that abuse (by oral, intranasal and/or IV routes) is still possible.…”

Section: Identifying and Interpreting Information On Abuse Deterrence In Product Labelsmentioning

confidence: 99%

Abuse-Deterrent Opioid Analgesics: A Guide for Clinicians

Carinci

2020

Pain Manag.

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The US FDA has encouraged the development of abuse-deterrent formulations (ADFs) of opioid analgesics as one component in a comprehensive effort to combat prescription opioid abuse. Guidance issued by the FDA outlines three types of premarket studies for evaluating abuse deterrence: laboratory-based in vitro manipulation and extraction studies, pharmacokinetic studies and human abuse potential studies. After approval, postmarket studies are needed to evaluate the impact of an ADF product on abuse in real-world settings. This review summarizes the regulatory issues involved in the development of ADF opioids and clarifies abuse-deterrence claims in product labels, in order to assist clinicians in critically evaluating the available evidence pertaining to the abuse-deterrent features of opioid analgesics.

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Section: Identifying and Interpreting Information On Abuse Deterrence In Product Labelsmentioning

confidence: 99%

Abuse-Deterrent Opioid Analgesics: A Guide for Clinicians

Carinci

2020

Pain Manag.

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“…Premarket in vitro and in vivo testing of Xtampza ER is well documented and demonstrates the difficulties in manipulating the product as well as the product's pharmacokinetic profile and human abuse potential. [7][8][9][10][11][12][13][14] Published postmarket data is limited to a recent publication comparing Xtampza ER to IR oxycodone, other ADF ER opioids, and non-ADF ER opioids which suggested that Xtampza ER has low relative abuse rates and low relative likelihood of non-oral use. 15 While these results were consistent across several data sources, additional real-world data are needed to further understand the relative risk of abuse of currently available opioid medications.…”

Section: Introductionmentioning

confidence: 99%

Nonmedical Use of Xtampza® ER and Other Oxycodone Medications in Adults Evaluated for Substance Abuse Treatment: Real-World Data from the Addiction Severity Index-Multimedia Version (ASI-MV®)

Green¹,

Robbins²,

Govoni³

et al. 2021

JPR

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Purpose The purpose of this study was to evaluate real-world data related to past 30-day nonmedical use (NMU) and routes of administration of Xtampza ® ER and comparator oxycodone medications in the US as captured within the Addiction Severity Index-Multimedia Version ® (ASI-MV ® ). Methods Data were collected from July 2016 through December 2019 from 647 centers located in 44 states using the ASI-MV, a clinical instrument used to evaluate substance use and treatment planning. Demographic characteristics were assessed using Pearson’s chi-square test for categorical data and quarterly NMU rates were calculated. Distribution of route of administration was studied using a proportional reporting ratio (PRR) analysis. Results Of 192,810 assessments, 42,279 (21.9%) indicated past 30-day NMU of at least one prescription opioid, including Xtampza ER (N=73, 0.2%), other oxycodone ER (n=3802, 9.0%) and oxycodone IR (n=14,579, 34.5%). All quarterly Xtampza ER NMU rates per 100 ASI-MV assessments were significantly lower than those for other oxycodone ER and oxycodone IR. Overall, quarterly Xtampza ER NMU drug utilization adjusted rates were significantly lower than quarterly rates observed for other oxycodone ER NMU but not consistently significantly lower than oxycodone IR NMU. Although not all statistically significant, all ratios from the PRR analysis were less than 1.0, indicating that rates of use of any alternate route, any non-oral route, snorting, and injecting were higher for other oxycodone ER and oxycodone IR than for Xtampza ER. Conclusion Xtampza ER had significantly lower rates of NMU than other oxycodone ER products and oxycodone IR products, as well as significantly lower rates of non-oral NMU than oxycodone IR products, in a population of individuals seeking substance abuse treatment. Understanding risks associated with different opioid medications is important for prescribers as they manage risks of opioid misuse and abuse with effective pain therapy.

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“…17 The effects of drug manipulation on the PK profile of Xtampza ER after oral administration were evaluated in five studies (Table 1). 8,20,[22][23][24] The effects of crushing (based on the most effective crushing methods using household utensils [common household items that crush, cut, or grate by manual or mechanical means] that could be easily accessed by abusers) and chewing (one of the most common prescription opioid tampering methods 16 ) on the PK profile of Xtampza ER capsule contents were compared with the PK profile of IR oxycodone solution in one category 2 study. 20 In addition, the effects of chewing on the PK profile of Xtampza ER were compared with that of crushed IR oxycodone as part of two category 3 (human abuse potential) studies in nondependent, recreational opioid users.…”

Section: Introductionmentioning

confidence: 99%

“…23,24 Two additional category 2 studies compared the effects of crushing on the PK profile of Xtampza ER capsule contents with the PK profile of crushed IR oxycodone and crushed reformulated OxyContin. 8,22 Because food consumption may alter drug availability, FDA guidance recommends modified-release drugs be evaluated under fasted and fed conditions when characterizing bioequivalence. 25 The Xtampza ER PK profile was therefore assessed in fasted 23,24 and fed 8,20,[22][23][24] conditions in these studies, in line with FDA guidance.…”

Section: Introductionmentioning

confidence: 99%

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Effect of physical manipulation on the oral pharmacokinetic profile of Xtampza® ER (oxycodone DETERx® formulation): A review of published studies

Gudin¹

2020

J of Opioid Management

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Opioids can be an effective treatment option for appropriate patients with chronic pain for whom nonpharmacological or nonopioid treatment does not provide adequate pain relief. However, extended-release (ER) opioid formulations, because of their high drug content, are attractive options for nonmedical use and abuse. Xtampza® ER (oxycodone DETERx®) capsules, an ER abuse-deterrent formulation (ADF), contain microspheres that combine oxycodone with inactive ingredients to increase the difficulty of tampering with the ER mechanism. The aim of this article is to review five previously published studies highlighting the impact of physical manipulation (ie, crushing and chewing) on the pharmacokinetic (PK) properties of orally administered Xtampza ER compared with immediate-release (IR) oxycodone and/or reformulated OxyContin® (the first approved oxycodone ER ADF). Across five studies, manipulated (crushed or chewed) Xtampza ER retained an ER PK profile similar to that of intact Xtampza ER, with respect to maximum plasma concentration (Cmax) and time to Cmax. Additionally, bioequivalence was established between manipulated and intact Xtampza ER, based on Cmax and area under the concentration-time curve values in healthy volunteers and nondependent recreational opioid users. In contrast, crushed OxyContin failed to retain the ER PK profile of intact OxyContin and was bioequivalent to IR oxycodone, based on Cmax in healthy volunteers. The retention of ER PK properties when capsule contents are physically manipulated before oral administration suggests Xtampza ER has lower potential to be manipulated for oral abuse when compared with IR oxycodone or OxyContin.

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The Comparative Pharmacokinetics of Physical Manipulation by Crushing of Xtampza ^® ER Compared with OxyContin ^®

Cited by 6 publications

References 16 publications

Abuse-Deterrent Opioid Analgesics: A Guide for Clinicians

Abuse-Deterrent Opioid Analgesics: A Guide for Clinicians

Nonmedical Use of Xtampza® ER and Other Oxycodone Medications in Adults Evaluated for Substance Abuse Treatment: Real-World Data from the Addiction Severity Index-Multimedia Version (ASI-MV®)

Effect of physical manipulation on the oral pharmacokinetic profile of Xtampza® ER (oxycodone DETERx® formulation): A review of published studies

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The Comparative Pharmacokinetics of Physical Manipulation by Crushing of Xtampza ® ER Compared with OxyContin ®

Cited by 6 publications

References 16 publications

Abuse-Deterrent Opioid Analgesics: A Guide for Clinicians

Abuse-Deterrent Opioid Analgesics: A Guide for Clinicians

Nonmedical Use of Xtampza® ER and Other Oxycodone Medications in Adults Evaluated for Substance Abuse Treatment: Real-World Data from the Addiction Severity Index-Multimedia Version (ASI-MV®)

Effect of physical manipulation on the oral pharmacokinetic profile of Xtampza® ER (oxycodone DETERx® formulation): A review of published studies

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The Comparative Pharmacokinetics of Physical Manipulation by Crushing of Xtampza ^® ER Compared with OxyContin ^®