Английская Википедия:Buprenorphine/naloxone

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Шаблон:Short description Шаблон:Cs1 config Шаблон:Distinguish Шаблон:Infobox drug

Buprenorphine/naloxone, sold under the brand name Suboxone among others, is a fixed-dose combination medication that includes buprenorphine and naloxone.[1] It is used to treat opioid use disorder, and reduces the mortality of opioid use disorder by 50% (by reducing the risk of overdose on full-agonist opioids such as heroin or fentanyl).[1][2][3] It relieves cravings to use and withdrawal symptoms.[4] Buprenorphine/Шаблон:Shynaloxone is available for use in two different forms, under the tongue or in the cheek.[5]

Side effects may include respiratory depression (decreased breathing), small pupils, sleepiness, and low blood pressure.[1] The risk of overdose with buprenorphine/Шаблон:Shynaloxone (unless combined with other sedating substances) is exceedingly low, and lower than with methadone,[4] but people are more likely to stop treatment on buprenorphine/Шаблон:Shynaloxone than methadone.[4] Buprenorphine (like methadone) is a treatment option during pregnancy.

At lower doses, buprenorphine results in the usual opioid effects; high doses beyond a certain level do not result in greater effects.[6] This is believed to result in a lower risk of overdose than some other opioids.[6] Naloxone is an opioid antagonist that competes with and blocks the effect of other opioids (including buprenorphine) if given by injection.[1] Naloxone is poorly absorbed when taken by mouth and is added to decrease the risk that people will misuse the medication by injection.[5] Misuse by injection or use in the nose still occurs, and more recently the efficacy of naloxone in preventing misuse by injection has been brought into question and preparations including naloxone could even be less safe than preparations containing solely buprenorphine.[1][7] Rates of misuse in the U.S. appear to be lower than with other opioids.[8]

The combination formulation was approved for medical use in the U.S. in 2002,[1][8][9] and in the European Union in 2017.[10] A generic version was approved in the U.S. in 2018.[11] In 2019, it was the 272nd most commonly prescribed medication in the U.S., with more than 1Шаблон:Nbspmillion prescriptions.[12]

Medical uses

Файл:Suboxone.jpg
Sublingual tablets
Файл:Suboxone SL Tabs.jpg
Film (package)

Buprenorphine/Шаблон:Shynaloxone is used for the treatment of opioid use disorder.[13] Long-term outcomes are generally better with use of buprenorphine/Шаблон:Shynaloxone than attempts at stopping opioid use altogether.[4] This includes a lower risk of overdose with medication use.[4] Due to the high binding affinity and low activation at the opioid receptor, cravings and withdrawal for opioids are decreased while preventing a person from getting high and relapsing on another opioid. The combination of the two medications is preferred over buprenorphine alone for maintenance treatment due to the presence of naloxone in the formulation, which is believed to help discourage intravenous use.[13] However, the belief that the addition of naloxone provides this benefit has been called into question, and posters on drug-related online forums have stated that they were able to attain a high by injecting preparations of buprenorphine despite being combined with naloxone.[7]

Buprenorphine/Шаблон:Shynaloxone has been found to be effective for treating opioid dependence, and serves as a recommended first-line medication according to the U.S. National Institute on Drug Abuse.[8] The medication is an effective maintenance therapy for opioid dependence and has generally similar efficacy to methadone. Both Шаблон:NowrapШаблон:Tspbuprenorphine/Шаблон:Shynaloxone and Шаблон:NowrapШаблон:Tspare substantially more effective than abstinence-based treatment.[4][14] Prescribers need a Drug Addiction Treatment Act (DATA 2000) waiver to prescribe buprenorphine/Шаблон:Shynalaxone for opioid dependence.[15]

Because it may be prescribed out of an office setting (as opposed to methadone, which requires specialized centers), buprenorphine/naloxone allows people more freedom of administration. It also thus comes with more risks in this vulnerable population. Buprenorphine/Шаблон:Shynaloxone may be recommended for socially stable people who use opioids who cannot retrieve medications from a center daily, who have another condition requiring regular primary care visits, or who have jobs or daily lives that require they maintain all their faculties and cannot take a sedating medication.[4] Buprenorphine/Шаблон:Shynaloxone is also recommended over methadone for people who at high risk of methadone toxicity, such as the elderly, those taking high doses of benzodiazepines or other sedating substances, concomitant alcohol use disorder, those with a lower level of opioid tolerance, and those at high risk of prolonged QT interval. It is also helpful to use the medication in combination with psychosocial support and counseling.[1][16]

Available forms

Buprenorphine/naloxone is available in sublingual formulations (that is, products that are dissolved under the tongue). There is no evidence that the tablet formulation is easier to divert and use in ways other than intended by the prescriber compared to the film formulation, or that the tablet formulation has a higher risk for accidental ingestion by children.[17] There are various pharmacokinetic differences between sublingual formulations.[18]

Contraindications

Contraindications are severe respiratory or liver impairment and acute alcoholism.[16] There are limited accounts of cross-reactivity with opioids, but there is a possibility.[19] Serious central nervous system (CNS) and respiratory depression may also occur with concurrent use of CNS depressants, ingesting alcohol, or other CNS-depressing factors while on buprenorphine/Шаблон:Shynaloxone.

Adverse effects

Side effects are similar to those of buprenorphine and other opioids.[16] In addition, naloxone can induce withdrawal symptoms in people who are chemically dependent on opioids.[16] The most common side effects (in order of most to least common) of sublingual tablets include headaches, opioid withdrawal syndrome, pain, nausea, increased sweating, and difficulty sleeping.[20] The most common side effects seen in film formulations are tongue pain, decreased sensation and redness in the mouth, headache, nausea, vomiting, excessive sweating, constipation, signs and symptoms of opioid withdrawal, sleeping difficulties, pain, and swelling of the extremities.[1] Post-approval, the most frequently reported side effects of buprenorphine/naloxone in sublingual strip form (i.e. Suboxone strips) are peripheral edema, stomatitis, glossitis, blistering of the mouth, and mouth ulcers (mouth sores).[21][22] Use of buprenorphine/naloxone may also increase the risk of developing certain dental problems (including tooth decay and tooth loss).[23][24][25]

Buprenorphine/naloxone has a milder side effect profile than methadone and limited respiratory effects, due to both agonist/antagonist effects. But buprenorphine/Шаблон:Shynaloxone may be less safe than methadone in people with stable liver disease, since it can elevate liver enzymes.[26]

Dependence and withdrawal

Шаблон:Further When taken in excess, buprenorphine/naloxone can produce dysphoric symptoms for non opioid-dependent/tolerant people because buprenorphine is a partial opioid agonist. The sublingual formulation of the buprenorphine/Шаблон:Shynaloxone combination was designed to reduce the potential to inject the medication in comparison to buprenorphine alone. If the combination is taken sublingually, as directed, the addition of naloxone does not diminish buprenorphine's effects. When an opioid-dependent person dissolves and injects a combination sublingual tablet, it is believed that a withdrawal effect may be triggered because of naloxone's high parenteral bioavailability.[27] However, the efficacy of naloxone in preventing misuse by injection has more recently been brought into question and preparations including naloxone could even be less safe than preparations containing solely buprenorphine.[7] While this mechanism may act to deter intravenous injection, the Suboxone formulation can still produce an opioid agonist "high" if used sublingually by non-dependent persons, leading to opioid dependence.[27][28]

Interactions

Buprenorphine's sedating/narcotic effect is increased by other sedating substances, such as other opioids, benzodiazepines, first-generation antihistamines, alcohol, and antipsychotics. Opioids and especially benzodiazepines also increase the risk of potentially lethal respiratory depression.[16]

Strong inhibitors of the liver enzyme CYP3A4, such as ketoconazole, moderately increase buprenorphine concentrations; CYP3A4 inducers can theoretically decrease concentrations of buprenorphine.[1][16]

Pharmacology

Файл:Buprenorphine-naloxone action at opioid receptor.png
A theoretical model of activity: buprenorphine/naloxone at opioid receptor when taken sublingually (top) versus when injected intravenously (bottom).
Файл:Buprenorphine is a Partial Agonist at the µ-Opioid Receptor.png
Buprenorphine as a partial agonist: Buprenorphine cannot fully activate the µ-opioid receptor even when the dose is escalated. This is demonstrated as a plateau in the concentration-response curve. Opioids like morphine (natural) or leu-enkephalin (endogenous in the body) produce a greater maximum response. Tramadol is a partial agonist with intermediate activity between buprenorphine and full agonists. A full description of buprenorphine with naloxone pharmacology can be found at https://www.youtube.com/watch?v=_y8DGjkP1so

Mechanism of action

Buprenorphine binds strongly to opioid receptors and acts as a pain-reducing medication in the central nervous system (CNS). It binds to the μ-opioid receptor with high affinity, which produces the analgesic effects in the CNS. It is a partial μ-opioid receptor agonist and a weak κ-opioid receptor antagonist. As a partial agonist, buprenorphine binds and activates the opioid receptors, but has only partial efficacy at the receptor relative to a full agonist, even at maximal receptor occupancy. It is thus well-suited to treat opioid dependence, as it produces milder effects on the opioid receptor with lower dependence and habit-forming potential.

Naloxone is a pure opioid antagonist that competes with opioid molecules in the CNS and prevents them from binding to the opioid receptors.[14] Naloxone's binding affinity is highest for the μ-opioid receptor, then the δ-opioid receptor, and lowest for the κ-opioid receptor.[29] Naloxone has poor bioavailability, and is rapidly inactivated following oral administration.[30] When injected, it exerts its full effects.

The principle behind its function as a deterrent is as follows: when taken sublingually as prescribed, buprenorphine's effects at the opioid receptor dominate, while naloxone's effects are negligible due to the low oral absorption. But when someone attempts to misuse the medication via either injection or inhalation, the naloxone is intended to act as an antagonist and either reduce the opioid's euphoric effects or even precipitate withdrawal in those dependent on opioids.[14] This helps reduce the potential for deviating from the prescriber's intended use relative to buprenorphine, though it does not eradicate it.[31] One reason that naloxone might have limited efficacy as an abuse deterrent is that buprenorphine binds more tightly to the mu-opioid receptor than naloxone.[31]

Pharmacokinetics

There are small differences in the pharmacokinetics between different sublingual buprenorphine/Шаблон:Shynaloxone products.[18] These differences may require changes in dose when a person switches from one product to another.[18] The buprenorphine/Шаблон:Shynaloxone sublingual film (e.g. trade name Suboxone) achieves higher buprenorphine maximum plasma concentrations (Cmax) and area under the curve (AUC, a measure of total drug exposure) than the original buprenorphine/Шаблон:Shynaloxone sublingual tablets at equal doses.[18] For example, at a buprenorphine/Шаблон:Shynaloxone dose of 8 mg/2 mg, the buprenorphine Cmax after a single dose of the original tablet formulation is around 3 ng/mL whereas that of the 8 mg/2 mg film formulation is around 3.55 ng/mL.[18] The Zubsolv trade name sublingual tablets have higher buprenorphine bioavailability than the original sublingual tablets, while the Bunavail trade name buccal films have the highest bioavailability.[18] For example, a single dose of Bunavail 4.2 mg/0.7 mg achieves a Cmax around 3.41 ng/mL.[18]

Buprenorphine

Шаблон:Main Buprenorphine is metabolized by the liver, primarily via the cytochrome P450 (CYP) isozyme CYP3A4, into norbuprenorphine. The glucuronidation of buprenorphine is primarily carried out by the UDP-glucuronosyltransferases (UGTs) UGT1A1 and UGT2B7, while norbuprenorphine is glucuronidated by UGT1A1 and UGT1A3. These glucuronides are then eliminated mainly through excretion into bile. The elimination half-life of buprenorphine is 20 to 73 hours (mean 37 hours). Due to the mainly hepatic elimination, there is no risk of accumulation in people with kidney problems.[32]

Naloxone

Шаблон:Main Naloxone is extensively inactivated by first-pass metabolism in the liver, meaning that use of buprenorphine/Шаблон:Shynaloxone as prescribed should not lead to active naloxone in the blood (which, as an opioid antagonist, would reverse the effect of buprenorphine or other opioids).

Society and culture

Cost

While the cost of the medication buprenorphine/Шаблон:Shynaloxone is greater than buprenorphine alone, one analysis predicted the overall costs would be less in the United States due to a lower risk of misuse.[33]

Access in the United States

Before the Drug Addiction Treatment Act of 2000 (DATA), physicians were not allowed to prescribe narcotics to treat opioid dependence. People with narcotic dependence had to go to registered clinics to receive treatment. With DATA, Suboxone was the first medication approved for office-based treatment for opioid dependence.[5] Suboxone has thus become widely used as a replacement for methadone as it can be prescribed by doctors in their offices, while methadone can only be provided at specialized addiction centers, of which there are a limited number, often making access difficult. Integrating Medication-Assisted Treatment into outpatient primary care practices improves patient access to Suboxone.[34] Some physicians are also leading a movement to begin prescribing it out of the emergency department (ED), as some small studies have shown ED-initiated Suboxone to be effective with people more likely to remain in addiction treatment compared to those either referred to addiction treatment programs or those receiving just a brief intervention in the department.[35][36]

Access to Suboxone can be limited due to varying prior authorization requirements across different insurers. Prior authorization is used by insurance companies to limit certain medications' use by requiring approval before the insurance company will pay for them.[37] This can influence a person's financial access and adherence. Financial access is determined through prior authorization approval, which the prescriber must request before the person can start the medication. The time it takes to have the request approved can delay the person in starting the medication. The prior authorization process can also affect adherence, because the approval is needed for every prescription. This presents the potential for a gap in treatment and withdrawal symptoms as the person waits for approval. Several insurance companies, as well as Medicaid in various states, have removed the use of prior authorization for Suboxone in an attempt to increase access to this treatment.[38]

Controversies

In July 2019, the British company Reckitt Benckiser Group (RB Group) and its current/former affiliated entities (notably Indivior, which split from RB Group in 2014) settled with the US Department of Justice (DOJ) regarding the sale and marketing of brand name Suboxone (buprenorphine/Шаблон:Shynaloxone).[39] The non-prosecution agreement involves RB Group paying up to $1.4 billion, the largest settlement payment in U.S. history involving an opioid-class medication.[39] This record was surpassed in October 2020, when Purdue Pharma reached an $8 billion settlement for claims related to injuries and deaths caused by the opioid epidemic, which includes criminal fines, forfeiture, and civil damages.[40] The 2019 case alleged anti-competitive behavior by RB Group and Indivior surrounding the expiration of their regulatory exclusivity for Suboxone sublingual tablets.[41] The DOJ alleged that RB Group and Indivior employed a product hopping scheme (when a firm ceases production of a product upon expiration of regulatory exclusivity in favor of another product that still has regulatory exclusivity in order to prevent generic manufacturer competition) by misrepresenting that the Suboxone sublingual film formulation was safer than the sublingual tablet formulation because "children are less likely to be accidentally exposed to the film product".[41] There was no scientific evidence for that claim.[17] The company also sponsored a complaint to the FDA, expressing concern that buprenorphine/Шаблон:Shynaloxone sublingual tablets (the very product they formerly produced) were unsafe, requesting that applications for regulatory approval of generic products by other pharmaceutical companies (their competitors) be rejected by the US Food and Drug Administration.[41]

See also

References

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External links

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  1. 1,0 1,1 1,2 1,3 1,4 1,5 1,6 1,7 1,8 Шаблон:Cite web
  2. Шаблон:Cite book
  3. Шаблон:Cite journal
  4. 4,0 4,1 4,2 4,3 4,4 4,5 4,6 Шаблон:Cite journal
  5. 5,0 5,1 5,2 Шаблон:Cite web
  6. 6,0 6,1 Шаблон:Cite journal
  7. 7,0 7,1 7,2 Шаблон:Cite journal
  8. 8,0 8,1 8,2 Шаблон:Cite journal
  9. Шаблон:Cite web
  10. Шаблон:Cite web
  11. Шаблон:Cite press release
  12. Шаблон:Cite web
  13. 13,0 13,1 Шаблон:Cite web
  14. 14,0 14,1 14,2 Шаблон:Cite journal
  15. Шаблон:Cite web
  16. 16,0 16,1 16,2 16,3 16,4 16,5 Шаблон:Cite book
  17. 17,0 17,1 Шаблон:Cite web
  18. 18,0 18,1 18,2 18,3 18,4 18,5 18,6 Шаблон:Cite journal
  19. Шаблон:Cite web
  20. Шаблон:Cite web
  21. Шаблон:Cite web
  22. Шаблон:Cite web
  23. Шаблон:Cite journal
  24. Шаблон:Cite journal
  25. Шаблон:Cite web
  26. Шаблон:Cite journal
  27. 27,0 27,1 Clinical Guidelines for the Use of Buprenorphine in the Treatment of Opioid Addiction. Treatment Improvement Protocol (TIP) 40. Laura McNicholas. US Department of Health and Human Services.
  28. Шаблон:Cite journal
  29. Шаблон:Cite book
  30. Шаблон:Cite news
  31. 31,0 31,1 Шаблон:Cite journal
  32. Шаблон:Cite journal
  33. Шаблон:Cite book
  34. Kirk JK, et al. (2020). "Launching a Medication-Assisted Treatment in an Outpatient Office-Based Practice." Journal of Primary Care & Community Health. https://doi.org/10.1177/2150132720940723
  35. Шаблон:Cite journal
  36. Шаблон:Cite web
  37. Шаблон:Cite web
  38. Шаблон:Cite web
  39. 39,0 39,1 Шаблон:Cite news
  40. Шаблон:Cite web
  41. 41,0 41,1 41,2 Шаблон:Cite web
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