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1 Medication for Opioid Use Disorder Melissa B. Weimer, DO, MCR, FASAM Assistant Professor of Medicine Medical Director, Yale Addiction Medicine Consult Service Yale University School of Medicine 1

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Page 1: Medication for Opioid Use Disorder… · • In 1947, approved in US as analgesic and antitussive • In 1960s, first utilization as medication to treat OUD by Dr. Vincent Dole of

1

Medication for Opioid Use Disorder

Melissa B. Weimer, DO, MCR, FASAM Assistant Professor of Medicine

Medical Director, Yale Addiction Medicine Consult Service

Yale University School of Medicine

1

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2

Melissa Weimer Disclosures

• Dr. Weimer has received monetary honorarium on one occasion from Indivior related to speaking about opioid dependence and pain only.

The contents of this activity may include discussion of off label or investigative drug uses. The faculty is aware that is their responsibility to disclose this information.

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3

Target Audience

• The overarching goal of PCSS-MAT is to make

available the most effective medication treatments

to serve patients in a variety of settings, including

primary care, psychiatric care, and pain

management settings.

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4

Educational Objectives

• At the conclusion of this activity participants should be able to:

Identify the rationale for using medications to treat opioid use disorder

Describe effective medications for treating opioid use disorder

Explain the unique properties of methadone, buprenorphine, and naltrexone

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5

Case

• Jane is a 23 year old female with chronic low back pain from a motor vehicle accident at

age 16 who presents to your office asking for help to stop using IV heroin.

• She has been using opioids daily for about 4 years. She started using illicit prescription

opioids, then switched to IV heroin daily about 2 years ago when she could no longer

afford illicit opioid pills.

• She has attempted non-medication-based addiction treatment in the past and quickly

relapsed.

• She also drinks approximately 14 alcoholic drinks per week, but has never had alcohol

withdrawal symptoms when she stops drinking. She feels that she could easily stop

drinking alcohol. She denies other drug use.

• She denies other mental health or medical issues, but has had two opioid overdoses in

the past year.

• She lives with her parents who are supportive of her. She is on probation for possession

of opioids.

• She reports opioid withdrawal symptoms including anxiety, restlessness, nausea,

stomach cramping, and diarrhea. Her vital signs and physical exam are normal except

for gooseflesh, dilated pupils, and bilateral upper extremity track marks.

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6

Case Questions

• Is medication for opioid use disorder (OUD) indicated for this

patient?

• What additional work up or evaluation is needed to decide

upon medication for this patient?

• Which medication to treat OUD is most appropriate for this

patient?

• How will you address the concomitant alcohol use?

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7

Substance Use Disorder:

A Chronic Relapsing Disorder

McLellan, Lewis, O’Brien & Kleber (2000) JAMA, 284: 1689-1695.

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8

Stages of the Addiction Cycle

Volkow, et al, NEJM. 2016

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9

Substance Use Disorder: DSM-5

(>2 items in 12 month period)

1. Failure to fulfill responsibilities ✓

2. Use in physically hazardous situations ✓

3. Legal problems was in DSM-IV but it was replaced with Craving in DSM-5.

4. Social/interpersonal problems ✓

5. Use larger amounts/longer than intended ✓

6. Cannot cut down ✓

7. ↑ time spent to get, use, and recover ✓

8. Give up or ↓ other important parts of life ✓

9. Ongoing use despite problems ✓

10. Tolerance* ✓

11. Withdrawal* ✓

Mild=2-3

Mod=4-5

Severe=6+

DS

M-I

V A

bu

se

D

SM

-IV

: D

ep

en

de

nce

*10 and 11 do

not count if opioid

is prescribed

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10

Purpose of Medication for OUD

• Allow reestablishment of homeostasis of the reward pathways in the brain away from substances

• Restore emotional and decision-making capacities

• Control symptoms of opioid withdrawal

• Suppress opioid cravings

• Block the reinforcing effects of ongoing opioid use

• Promote and facilitate patient engagement in recovery-oriented activities

• Coupled with behavioral interventions

Enhance the salience of natural, healthy rewards

Reduce stress reactivity and negative emotional state

Improve self-regulation

Increase avoidance of relapse triggers

Volkow, et al, NEJM. 2016

ASAM National Practice Guideline, June 1, 2015.

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11

Goals of Medication for OUD

• Reduce mortality

All cause and drug-related

• Reduce associated morbidity

Transmission of blood-borne viruses

Infectious complications from IV drug use

• Reduce and/or discontinue opioid use

• Increase retention in addiction treatment

• Improve general health and well-being

• Reduce drug-related crime

Volkow, et al, NEJM. 2016

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12

Access to medication remains a key barrier

to reduction in mortality from opioid use

Williams, Bisaga. Health Affairs, 2017.

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13

Opioid Maintenance

Treatment and Mortality

Adjusting for heroin purity

and the number of

methadone patients, there

was a statistically

significant inverse

relationship between

heroin overdose deaths

and patients treated with

buprenorphine (P = .002).

Schwartz et al AJPH 2013

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14

Medication for OUD

• Methadone

Opioid Treatment Program

• Buprenorphine

Office-Based

Opioid Treatment Program

• Naltrexone

Office-Based

Opioid Treatment Program

• Counseling mandatory for methadone; ability to refer to counseling

necessary for buprenorphine; optional for naltrexone but encouraged.

• All medical modalities require medication management

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Opioid (mu) Receptor Activity for Medications

treating Opioid Use Disorder

no drug high dose

Medication Dose

low dose

% Mu

Receptor

Intrinsic

Activity

0

10

20

30

40

50

60

70

80

90

100

Full Agonist: Methadone

Antagonist: Naltrexone

Partial Agonist: Buprenorphine

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16

Medication Efficacy for

Opioid Use Disorder

All cause

Mortality

Treatment

Retention

Any Opioid

Use

HIV or HCV

Transmission

Criminal

Activity

Methadone

(n=4)a,c

(n=6)a

(n=6)a

(n=34)b

(n=2)a

Buprenorphine

(n=2)a,c

(n=4)a

(n=2)a

(n=6)b

(n=2)a

Oral

Naltrexone

No data

(n=3)d

(n=3)d No data

(n=2)d

Extended

Release

Naltrexone

(n=1)e

(n=6)e-j

(n=6)e-j No data

(n=1)g

aMattick RP, et al. Cochrane Database Syst Rev 2014; bGowing, L et al. Cochrane Database Syst Rev 2011 cSordo, et al. BMJ 2017 dMinozzi S, et al. Cochrane Database Syst Rev 2011; eReece, AS. J Addict Dise 2010 fKrupitsky E et al. Lancet. 2011,

gComer SD et al. Arch Gen Psychiatry 2006, hLee J et al, NEJM, 2016. iTanum L et al. JAMA Psych, 2017

jLee, et al. X:BOT. Lancet, 2018

(n = number of studies)

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17

Methadone

• Developed in 1930s during WWII as an alternative to

morphine

• In 1947, approved in US as analgesic and antitussive

• In 1960s, first utilization as medication to treat OUD by

Dr. Vincent Dole of Rockefeller University

• 1971, first federal program for methadone maintenance

treatment

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18

Methadone

• Full opioid agonist indicated to treat opioid use disorder

• Long and variable elimination half-life

15-150 hours

• Federal regulation requires dispensing in a licensed

opioid treatment program (OTP)

Exceptions: hospitals

• OTPs integrate counseling into the treatment paradigm

• Specific Eligibility Criteria

• Typical effective dose range is 60-100mg per day, may

need to be higher in some patients

Mattick Cochrane Rev 2013

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19

Methadone

• >40 years of data support 1,2

Safety

Sustained opioid abstinence

Treatment retention

Reduced IV Drug Use risk behaviors

Reduced transmission of HIV and HCV

• But…

Requires careful monitoring

Increased risk of mortality in first 2 weeks of treatment due to unique and complex pharmacokinetics

Prolongs QTc3,4

− 23% of patients by 16 weeks of treatment4

Multiple drug-drug interactions5

1 Kreek Addict Dis 2010 2 Mattick Cochrane Rev 2014 3 Chou, J Pain 2014 4 Wedam Arch Intern Med 2007 5 McCance-Katz Am J Addict 2009

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20

Mortality Risk During and After

Methadone Treatment

0

5

10

15

20

25

30

35

40

Methadone - all cause mortality Methadone - overdose risk

Mortality rates/1000 person years (95% CI)

In treatment Out of treatment

Sordo, et al. BMJ 2017.

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21

Methadone:

Contraindications and Precautions

Contraindications Precautions

Hypersensitivity

Concurrent use of other CNS depressants

including alcohol, other opioids,

benzodiazepines

Respiratory depression (e.g.

severe COPD, severe OSA, etc) Liver disease

Hypercapnia

Drug interactions with medications

metabolized by cytochrome p450

-CYP34A, CYP2B6, CYP2C19, CTY2C9,

CYP2D6

Paralytic ileus Electrocardiogram (ECG) QTc > 450ms*

ECG QTc > 500ms*

*Pretreatment and annual ECG screening recommended

Chou, J Pain 2014

ASAM National Practice Guideline, June 1, 2015.

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22

Buprenorphine/Naloxone Film or Tablet

(4:1 combination)

• First FDA approval in 2002 for OUD treatment

• Partial opioid agonist, Schedule 3

• Transmucosal film or tablet

• Dosing

Once daily

Alternative dosing: every other day or thrice weekly also effective

Off label: twice daily or three times daily

• 24mg/day usually the highest effective dose

• Ceiling Effect* with lower opioid overdose risk

• Office based prescribing by MDs, DOs, PAs, or NPs with DEA waiver or “X license”

Treat up to 30 patients the first year, then up to 100 patients

Can apply to prescribe up to 275 patients if certain requirements met

*Ceiling effect does not apply to children where unintentional exposure can lead to death

SAMHSA TIP 63: https://store.samhsa.gov/system/files/sma18-5063pt3.pdf

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23

Rationale for Buprenorphine/Naloxone

Combination

• Naloxone present in attempt to decrease misuse or

diversion

• Naloxone is mostly inactive unless injected

Very low bioavailability of naloxone when medication

used sublingually

If patient opioid dependent and not in opioid withdrawal,

injection of buprenorphine/naloxone can precipitate

withdrawal

If patient in opioid withdrawal, injection of

buprenorphine/naloxone can have euphorogenic or

opioid withdrawal relieving effects

SAMHSA TIP 63: https://store.samhsa.gov/system/files/sma18-5063pt3.pdf

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24

Commercially Available Transmucosal

Buprenorphine Formulations for the

Treatment of OUD

Buprenorphine/

Naloxone Suboxone® Buprenorphine Zubsolv® Bunavail®

Formulation SL Tablets SL Film SL Tablets SL Tablets

Mucous

Membrane

Film

Dosages

Available

2/0.5mg

8/2mg

2/0.5mg

4/1mg

8/2mg

12/3mg

2mg

8mg

1.4/0.36mg

2.9/0.71mg

5.7/1.4mg

8.6/2.1mg

11.4/2.9mg

2.1/0.3mg

4.2/0.7mg

6.3/1mg

Concomitant

Naloxone Yes Yes No Yes Yes

SL = Sublingual

Belbuca®, Buprenex®, and Butrans® are not indicated for treatment of opioid dependence or opioid use disorder

Fudin, J, 2016

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25

Buprenorphine:

Contraindications and Precautions

Contraindications Precautions

Hypersensitivity

Concurrent use of other CNS

depressants including alcohol, other

opioids, benzodiazepines

Patient not already on

buprenorphine and undergoing

a procedure where full agonist

treatment is needed*

Precipitated withdrawal due to full

agonist opioid use

Severe liver impairment

*Patients can have acute pain addressed while on buprenorphine treatment. Refer to PCSS Core

Pain Curriculum for more information.

ASAM National Practice Guideline, June 1, 2015.

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26

Buprenorphine Implant

(Probuphine®)

• FDA approved in 2016

• Indication: Treatment of OUD in patients who have been clinically

stabilized on transmucosal buprenorphine 8 mg/day or less.

• Medication consists of 4 implants (80mg/implant) surgically inserted

into the subdermal region of the upper arm that release

buprenorphine for 6 months.

• At steady state (after 4 weeks), comparable to trough

buprenorphine plasma levels produced by daily sublingual

buprenorphine doses of 8mg or less.

• To prescribe, insert or remove medication, providers must complete

a live training program.

SAMHSA TIP 63: https://store.samhsa.gov/system/files/sma18-5063pt3.pdf

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27

Buprenorphine Implant

Probuphine®

Responder Rate Implant SL B/X P Value NNT

Primary Analysis

• 4 of 6 month

without illicit

opioid use

81/84 (96.4%) 78/89 (87.6%) <0.001 11.4

Secondary Analysis

• 6 month illicit

opioid abstinence 72/84 (85.7%) 64/89 (71.9%) 0.03 7.3

• 177 randomized; 166 completed (93.8% retention)

Rosenthal, Lofwall et al. JAMA. 2016. 316(3):282-290

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28

Buprenorphine Depot Injection

(Sublocade®)

• FDA approval obtained November 2017

Moderate to severe OUD treatment

• Monthly subcutaneous abdominal injection

Minimum 7 days of transmucosal buprenorphine treatment first

• Two doses

300mg/1.5mL and 100mg/0.5mL

• Two dosing options based on current evidence

300mg/1.5mL x 6 months

300mg/1.5mL x 2 months, followed by 100mg/0.5mL x 4 months

• Peak buprenorphine concentrations occur ~24 hrs after injection

• Steady state achieved in 4 to 6 months

• After discontinuation, patients may have detectable plasma levels for 12 months or longer

SAMHSA TIP 63: https://store.samhsa.gov/system/files/sma18-5063pt3.pdf

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29

Buprenorphine Depot Injection

(Sublocade®)

• One Phase 3 trial completed1

• Low proportion of people with significant adverse effects

• Primary endpoint = mean % abstinence1

41-43% treatment arm vs 5% for placebo (p<0.0001)

• Secondary endpoint = treatment success (80% urine

samples free of opioids) 1

28-29% treatment arm vs 2% placebo (p<0.0001)

1Late-Breaking Research Oral Session at CPDD 79th

Annual Scientific Meeting 2017. http://cpdd.org/meetings/2017-meeting-information/

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30 Treatment duration (days)

Re

ma

inin

g in

tre

atm

en

t (

nr)

0

5

10

15

20

0 50 100 150 200 250 300 350

Treatment Retention: Buprenorphine Detoxification vs. Maintenance

Maintenance: 75% Abstinent at 1 year

0% mortality

HR = 58.7, p .0001

Kakko, Lancet 2003

Detoxification: 0% Abstinent at 1 year

20% mortality

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Mortality Risk During and After

Buprenorphine Treatment

0

2

4

6

8

10

12

Buprenorphine - all cause mortality Buprenorphine - overdose risk

Mortality rates/1000 person years (95% CI)

In treatment Out of treatment

Sordo, et al. BMJ 2017.

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Buprenorphine vs. Methadone Treatment Retention

Perc

ent

Reta

ined

0

20

40

60

80

100

1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17

20% Low dose

methadone (20mg)

58% Buprenorphine

73% High dose

methadone (60-

100mg)

Study Week Johnson NEMJ 2000

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Buprenorphine vs. Methadone Opiate Urine Results

Mean %

Negative

Study Week

40% Buprenorphine

80

1 3 5 7 9 11 13 15 17

0

20

40

60

100

19% Low dose

methadone

39% High dose

methadone

Johnson NEMJ 2000

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34

Oral Naltrexone

• Opioid antagonist: blocks all opioid receptors

• Two formulations: Oral and Intramuscular

• Oral Naltrexone FDA approved in 1984 for blockade of effects of administered opioids

Dose is 50mg daily

Alternative dosing = dose three times a week with two 100mg-doses followed by 150mg dose

Not widely used to treat OUD because low rates of patient acceptance, difficulty with initiation, and high rates of medication nonadherence

Cochrane Review did not find oral naltrexone superior to placebo or no medication in treatment retention and illicit opioid use

SAMHSA TIP 63: https://store.samhsa.gov/system/files/sma18-5063pt3.pdf

Minozzi S, et al. Cochrane Database Syst Rev 2011

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Extended-Release (XR)

Naltrexone: Intramuscular Injection

• FDA approved 2010 for treatment of opioid use disorder following medically supervised withdrawal

• 380mg administered intramuscularly once every 4 weeks

Some people may metabolize quickly and need injection in 21 days

• Consider in

Patients who have failed agonist treatment

Patients confined to environments that do not allow for medication treatments

Patients who do not have access to agonist treatment

Patients with high risk of diversion

Patients who are highly motivated and willing to taper off opioid agonists

Patients who do not want to be treated with an agonist

Patients with concomitant opioid and alcohol use disorder

Comer, S, Cunningham, C, et al. (2015)

ASAM The National Practice Guideline For the Use of

Medications in the Treatment of Addiction Involving Opioid Use.

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XR-Naltrexone

• Requires patient to be fully abstinent from opioids

Short acting opioids = 5-7 days abstinent

Long acting opioids = 7-10 days abstinent

Confirm opioid abstinence with urine drug test and/or naloxone

challenge*

• Few drug-drug interactions

• Induction delays and non-adherence may reduce overall effectiveness

Comer, S, Cunningham, C, et al. (2015)

ASAM The National Practice Guideline For the Use of

Medications in the Treatment of Addiction Involving Opioid Use.

*Naloxone Challenge:

Use to assess lack of physical opioid dependence

Usually involves injection (IV, IM, or SQ) of

Short-acting NALOXONE to test opioid abstinence

See TIP 63 for more information

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XR-Naltrexone

• Efficacious for opioid abstinence compared to placebo

Comer: 60 U.S. people who use heroin at 8 weeks1

Krupitsky: 250 Russian people who use heroin at 24

wks2

− % Opioid Abstinent XR-Naltrexone 45 (35.7%) vs

Placebo 25 (22.8%)

− RR 1.58, 95% CI (1.06 – 2.36), p = 0.0224

− NNT 7.8

− Fair quality study, high attrition, young white males

only

1 Comer Arch Gen Psych 2006 2 Krupitsky Lancet 2011

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38

XR-Naltrexone to Prevent Opioid

Relapse in Criminal Justice Offenders

• Open-label, randomized, controlled effectiveness trial

• Compared six monthly injections of XR-NTX with usual treatment (brief counseling and referrals for community treatment programs)

• Study population: adult ex-prisoners who had a history of opioid dependence

• Primary endpoint: opioid relapse

Lee JD et al. N Engl J Med 2016;374:1232-1242

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39

After 6 months

Time to relapse:

10.5 weeks Naltrexone

5.0 weeks Usual

Treatment

Opioid Relapse Event:

43% Naltrexone

64% Usual Treatment

Overdoses:

0 Naltrexone

7 Usual Treatment

Lee JD et al. N Engl J Med 2016;374:1232-1242

Kaplan–Meier Curves for Relapse-free Survival

XR-Naltrexone to Prevent Opioid

Relapse in Criminal Justice Offenders

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40

XR-Naltrexone:

Contraindications and Precautions

Contraindications Precautions

Hypersensitivity Vulnerability to overdose

Patient currently physically

dependent on opioids – will

develop severe precipitated opioid

withdrawal

Injection site reactions associated with

injectable naltrexone

Patient receiving opioid analgesics Risk of hepatotoxicity

Patients in acute opioid withdrawal Monitor for development of depression

and suicidality

Thrombocytopenia or coagulation

disorder – injection bleeding risk

ASAM National Practice Guideline, June 1, 2015.

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41

XR-Naltrexone Compared to

Buprenorphine

• Tanum, et al, 2017: Open label RCT

159 patients randomized / 105 completed study

Inpatient detox setting

12 weeks follow up

Primary Outcomes: retention in treatment, group proportion of opioid-negative UDTs, days of use of heroin or other opioids

XR-NRT non-inferior to buprenorphine (relatively low dose) for treatment retention and decreasing opioid use at 12 weeks

− Lower use of heroin or other opioids in XR-NRT group

• Secondary outcomes: XR-NRT superior to buprenorphine on reduction in heroin craving, reduction of insomnia, satisfaction with treatment, life satisfaction, and reduction of pain. No difference in anxiety or depression

Tanum L et al. JAMA Psych, 2017

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42

X:BOT Trial (XR-Naltrexone

Compared to Buprenorphine)

• Lee, et al, 2018: Comparative Effectiveness RCT

570 patients randomized / 474 completed

8 INpatient detoxification/residential treatment programs

around the US

− Sites utilizing non-opioid detox had better success with

XR-NRT induction

24 weeks of follow up

Primary outcome: “time to relapse”

− 7 consecutive use days

− 4 consecutive use weeks

− Beginning no earlier than 21 days post-randomization

Lee, et al. X:BOT. Lancet, 2018

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X:BOT Trial (XR-Naltrexone

Compared to Buprenorphine)

• Patients were less likely to be inducted on XR-NTX, less likely to relapse if they received buprenorphine.

• Once started on medication, a statistically significant difference was not observed btw medications.

Lee, et al. X:BOT. Lancet, 2018

Outcome XR-NXT (n=283) BUP-NX (n=287) Treatment Effect*

Number of patients

Inducted to study

medication (ITT)

204 (72%) 270 (94%) OR 0.61, 0.09-0.28

P<0.0001

Weeks Relapse-free

survival (ITT) 8.4 (3-23.4) 14.4 (5.1-23.4)

HR 1.36, 1.10-1.68

P=0.0040

24-week relapse rates

(ITT) 65% 57%

OR=1.44, 1.02-2.01

P=0.04

XR-NRT (n=204) BUP-NX (n=270)

Weeks Relapse-free

survival Per-protocol 20.4 (5.4-23.4) 15.2 (5.7-23.4)

HR 0.92, 0.71-1.18

P=0.49

24-week relapse rates

per-protocol 52% 56%

OR=0.87, 0.60-1.25

P=0.44

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44

Models of Care Treating

Patients with OUD

• Office-based buprenorphine

therapy

• Buprenorphine HIV

evaluation and support

collaborative model

• One-stop shop model

• Integrated prenatal care and

MAT

• Hub and spoke model

• Medicaid health home model

• Project ECHO

• Collaborative opioid

prescribing model

• Nurse care manager model

• ED initiation of buprenorphine

• Inpatient initiation of MAT

• Southern Oregon model

Chou R, et al. Agency for Healthcare Research and Quality (US); 2016

Dec. (Technical Briefs, No. 28.) Report No.: 16(17)-EHC039-EF.

Korthuis, et al. Annals of Internal Medicine, 2017.

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45

What is Medication Management?

• Treatment of opioid withdrawal

• Medication initiation

• Evaluation for safety and effectiveness

• Confirmation of adherence

Urine drug testing, pill counts, patient report

• Evaluating treatment plan based on patient need and adherence

• Referral for or treatment of mental illness, if needed

• Also involves

Psychosocial needs assessment

Supportive counseling

Case management

Links to existing family supports

Referral to community services

ASAM National Practice Guideline, 2015

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46

Role of Counseling

• Purpose:1

Modify behaviors that maintain or reinforce drug use

Develop coping strategies

Encourage medication adherence

Treat or identify concomitant mental illness that can

complicate SUD or trigger relapse

• Some evidence shows that psychosocial treatment

improves adherence and retention in treatment2-3, but

findings are mixed4-7

1 ASAM National Practice Guideline, 2015 2 Brigham GS, et al, Drug Alcohol Dependence 2014 3 Ruetsch C, et al, Addict Behav, 2012 4 Fiellin, DA, et al, Am J Med 2013 5 Fiellin DA, et al, NEJM 2006 6 Tetrault JM et al, K Subst Abuse Treat 2012 7 Weiss RD et al, Arch Gen Psych 2011

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Effective Counseling Modalities

• Relationship building

• Cognitive behavioral therapies

• Contingency management

• Relapse prevention

• Motivational interviewing

Dutra, et al. Am J Psychiatry, 2008

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48

Case

• Jane is a 23 year old female with chronic low back pain from a motor vehicle accident at

age 16 who presents to your office asking for help to stop using IV heroin.

• She has been using opioids daily for about 4 years. She started using illicit prescription

opioids, then switched to IV heroin daily about 2 years ago when she could no longer afford

illicit opioid pills.

• She has attempted non-medication-based addiction treatment in the past and quickly

relapsed.

• She also drinks approximately 14 alcoholic drinks per week, but has never had alcohol

withdrawal symptoms when she stops drinking. She feels that she could easily stop drinking

alcohol. She denies other drug use.

• She denies other mental health or medical issues, but has had two opioid overdoses in the

past year.

• She lives with her parents who are supportive of her. She is on probation for possession of

opioids.

• She reports opioid withdrawal symptoms including anxiety, restlessness, nausea, stomach

cramping, and diarrhea. Her vital signs and physical exam are normal except for

gooseflesh, dilated pupils, and bilateral upper extremity track marks.

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49

Case Questions

• Is medication indicated for this patient?

Yes

• What additional work up or evaluation is needed to decide upon medication for this patient?

Urine drug screen and pregnancy test

DSM-5 evaluation

General medical evaluation

• How will you address the concomitant alcohol use?

May need to consider medically supervised withdrawal

Structure care to monitor this closely

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50

Pros and Cons of Each Medication

Medication Pros Cons

Buprenorphine

• Quick stabilization of

withdrawal

• May also treat concomitant

pain

• Possible overdose risk with

concomitant alcohol use

Methadone

• Quick stabilization of

withdrawal

• May be more effective to

treat concomitant pain

• Possible overdose risk with

concomitant alcohol use

XR-Naltrexone

• Will treat concomitant

alcohol use disorder

• No risk of withdrawal if

patient is incarcerated

• More severe withdrawal

• Delay in initiation of

treatment

Ultimate choice of medication should be based on patient choice, but access to treatment

program, insurance coverage, and medication access will also likely guide decision.

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51

More Information on

Medication Treatments

https://store.samhsa.gov/

Substance Abuse and Mental Health Services Administration. Medications for Opioid Use Disorder.

Treatment Improvement Protocol (TIP) Series 63, Executive Summary.

HHS Publication No. (SMA) 18-5063EXSUMM. Rockville, MD:

Substance Abuse and Mental Health Services Administration, 2018.

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52

• Brigham GS, Slesnick N, et al. (2014) A randomized pilot clinical trial to evaluate the efficacy of Community Reinforcement and Family Training

for Treatment Retention (CRAFT-T) for improving outcomes for patients completing opioid detoxification. Drug Alcohol Depend;138:240–243.

• Chou, R, et al. (2014) Methadone Safety: A Clinical Practice Guideline From the American Pain Society and College on Problems of Drug

Dependence, in Collaboration With the Heart Rhythm Society. The Journal of Pain, 15 (4): 321 – 337

• Chou R, et al. (2016) Medication-assisted treatment models of care for opioid use disorder in primary care settings [internet]. Rockville, MD:

Agency for Healthcare Research and Quality (US); (Technical Briefs, No. 28.) Report No.: 16(17)-EHC039-EF.

• Comer, S, Cunningham, C, et al. (2015) ASAM The National Practice Guideline For the Use of Medications in the Treatment of Addiction

Involving Opioid Use.

• Comer S, Sullivan, MA. (2006) Injectable, sustained-release naltrexone for the treatment of opioid dependence: a randomized, placebo-

controlled trial. Arch Gen Psychiatry, 63 (2): 210-8.

• Dutra L, Stathopoulou G, et al. (2008) A meta-analytic review of psychosocial interventions for substance use disorders. Am J Psychiatry 165:

179-187.

• Fiellin DA, Barry DT, et al. (2013) A randomized trial of cognitive behavioral therapy in primary care-based buprenorphine. Am J Med.

126:74.e11–74.e17.

• Fiellin DA, Pantalon MV, et al. (2006) Counseling plus buprenorphine-naloxone maintenance therapy for opioid dependence. N Engl J

Med;355:365–374.

• Fudin, J. (2016) A Brief Review of Buprenorphine Products. Pharmacy Times.

• Gowing, L, Farrell, M, et al. (2011) Oral substitution treatment of injecting opioid users for prevention of HIV infection. Cochrane Database of

Systematic Reviews (8): CD004145

• Johnson, R, Chutuape, M, et al. (2000) A comparison of Levomethadyl acetate, Buprenorphine, and Methadone for Opioid Dependence. New

England Journal of Medicine, 343: 1290-1297.

• Kakko,J, Svanborg, K, et al. (2003) 1-year retention and social function after buprenorphine-assisted relapse prevention treatment for heroin

dependence in Sweden: a randomized, placebo controlled trial. Lancet, 361 (9358):662-8.

• Korthuis PT, McCarty D, Weimer M, et al. (2017) Primary Care–Based Models for the Treatment of Opioid Use Disorder: A Scoping Review.

Ann Intern Med;166:268–278.

• Kreek, MJ, Borg, L, et al. (2010) Pharmacotherapy in the treatment of addiction: methadone. J Addict Disease, 29 (2):200-16.

• Krupitsky E, Nunes, E, et al. (2011) Injectable extended-release naltrexone for opioid dependence: a double-blind, placebo-controlled,

multicenter randomized controlled trial. Lancet, 377 (9776): 1506-1513.

References

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53

• Lee J, Friedmann, P, et al. (2016) Extended-release Naltrexone to Prevent Opioid relapse in Criminal Justice Offenders. New England Journal of Medicine.

374 (13): 1232-42.

• Lee J, Nunes, E, Novo, P, et al. (2018) Comparative Effectiveness of extended-release naltrexone versus buprenorphine-naloxone for opioid relapse

prevention (X:BOT): a multicenter, open-label, randomized controlled trial. Lancet 391: 309-314.

• Ling, W, Casadonte, P, et al. Buprenorphine Implants for treatment of opioid dependence a randomized controlled trial. JAMA 304 (14): 1576-83.

• Mattick RP, Breen C, et al. (2009) Methadone maintenance therapy versus no opioid replacement therapy for opioid dependence. Cochrane Database Syst

Review. (3): CD002209.

• Mattick RP, Breen, C, et al. (2014) Buprenorphine maintenance versus placebo or methadone maintenance for opioid dependence. Cochrane Database

Syst Rev. (2): CD002207.

• McCance-Katz, E, Sullivan, E, et al. (2009) Drug Interactions of Clinical Importance among Opioids, Methadone and Buprenorphine, and other frequently

prescribed medications: A Review. Am J Addict, 19 (1): 4-16.

• McLellan, Lewis, et al. (2000) Drug Dependence, a chronic medical illness: Implications for treatment, insurance, and outcomes evaluations. JAMA, 284:

1689-1695.

• Minozzi, S, Amato, L, et al. (2011) Oral naltrexone maintenance treatment for opioid dependence. Cochrane Database Syst Rev: Apr 13;(4):CD001333

• Late-Breaking Research Oral Session at CPDD 79th Annual Scientific Meeting 2017. http://cpdd.org/meetings/2017-meeting-information/

• Reece AS. (2010) Favorable mortality profile of naltrexone implants for opioid addiction. J Addict Dis. 29(1):30-50.

• Rosenthal, Lofwall et al. (2016) Effect of Buprenorphine Implants on Illicit Opioid Use Among Abstinent Adults With Opioid Dependence Treated With

Sublingual Buprenorphine: A Randomized Clinical Trial. JAMA. 316(3):282-290

• Ruetsch C, Tkacz J, et al. (2012) The effect of telephonic patient support on treatment for opioid dependence: outcomes at one year follow-up. Addict

Behav;37:686–689.

• Samji H, Cescon A, et al. (2013) Closing the Gap: Increases in Life Expectancy among Treated HIV-Positive Individuals in the United States and Canada.

PLoS ONE8(12): e81355.

• Schwartz, R, Gryczynski, J, et al. (2013) Opioid Agonist Treatments and Heroin Overdose Deaths in Baltimore, MD: 1995-2009. American Journal of Public

Health 103 (5): 917-922.

• Sordo, et al. (2017) Mortality Risk during and after opioid substitution treatment: systematic review and meta-analysis of cohort studies. BMJ 357:j1550

• Substance Abuse and Mental Health Services Administration. Medications for Opioid Use Disorder. Treatment Improvement Protocol (TIP) Series 63,

Executive Summary. HHS Publication No. (SMA) 18-5063EXSUMM. Rockville, MD: Substance Abuse and Mental Health Services Administration, 2018.

References

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• Tanum, L, Klemmetsby, K, Latif, Z, et al. (2017) Effectiveness of Injectable Extended-Release Naltrexone vs Daily Buprenorphine-

Naloxone for Opioid Dependence: A Randomized Clinical Noninferiority Trial. JAMA Psych. 74 (12): 1197-1205.

• Tetrault JM, Moore BA, et al. (2012) Brief versus extended counseling along with buprenorphine/naloxone for HIV-infected opioid

dependent patients. J Subst Abuse Treat;43:433–439.

• Walsh, SL, Comer, SD, et al. (2017) Effect of Buprenorphine Weekly Depot (CAM2038) and Hydromorphone Blockade in Individuals With

Opioid Use Disorder: A Randomized Clinical Trial. JAMA Psychiatry;74(9):894-902

• Wedam EF, Bigelow GE, et al. (2007) QT-Interval Effects of Methadone, Levomethadyl, and Buprenorphine in a Randomized Trial. Arch

Intern Med;167(22):2469–2475.

• Weiss RD, Potter JS, Fiellin DA, et al. (2011) Adjunctive counseling during brief and extended buprenorphine-naloxone treatment for

prescription opioid dependence: a 2-phase randomized controlled trial. Arch Gen Psychiatry;68:1238–1246.

• Williams, A, Bisaga, A. (2017) The Opioid Commission Ringing The Right Alarm to Respond To The Overdose Epidemic. Health Affairs

• Volkow, N, Chang, L, et al.(2001) Loss of dopamine transporters in methamphetamine abusers recovers with protracted abstinence. J

Neurosci 21:9414-8

• Volkow, N, Koob, G, et al. (2016) Neurobiological Advances from the Brain Disease Model of Addiction. NEJM 374: 363-71.

References

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PCSS Mentor Program

• PCSS Mentor Program is designed to offer general information to

clinicians about evidence-based clinical practices in prescribing

medications for opioid addiction.

• PCSS mentors are a national network of providers with expertise in

addictions, pain, evidence-based treatment including medication-

assisted treatment.

• 3-tiered approach allows every mentor/mentee relationship to be unique

and catered to the specific needs of the mentee.

• No cost.

For more information visit:

pcssNOW.org/clinical-coaching

55

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PCSS Discussion Forum

Have a clinical question?

56

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Funding for this initiative was made possible (in part) by grant nos. 5U79TI026556-02 and 3U79TI026556-02S1 from SAMHSA. The

views expressed in written conference materials or publications and by speakers and moderators do not necessarily reflect the

official policies of the Department of Health and Human Services; nor does mention of trade names, commercial practices, or

organizations imply endorsement by the U.S. Government.

PCSS-MAT is a collaborative effort led by the American Academy of Addiction Psychiatry (AAAP) in

partnership with the: Addiction Technology Transfer Center (ATTC); American Academy of Family

Physicians (AAFP); American Academy of Neurology (AAN); American Academy of Pain Medicine (AAPM);

American Academy of Pediatrics (AAP); American College of Emergency Physicians (ACEP); American

College of Physicians (ACP); American Dental Association (ADA); American Medical Association (AMA);

American Osteopathic Academy of Addiction Medicine (AOAAM); American Psychiatric Association (APA);

American Psychiatric Nurses Association (APNA); American Society of Addiction Medicine (ASAM);

American Society for Pain Management Nursing (ASPMN); Association for Medical Education and

Research in Substance Abuse (AMERSA); International Nurses Society on Addictions (IntNSA); National

Association of Community Health Centers (NACHC); National Association of Drug Court Professionals

(NADCP), and the Southeast Consortium for Substance Abuse Training (SECSAT).

For more information: www.pcssNOW.org

@PCSSProjects

www.facebook.com/pcssprojects/