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Journal Update September 2003

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Title: Journal Update September 2003

1
Journal UpdateSeptember 2003

Michael Rotblatt, MD
Soma Wali, MD

2
Topics Today

Tx of opiate addiction
HTN, proteinuria and non-diabetic kidney disease
Pharmaceutical Update

3
Case 1

31 y.o. M supermarket manager is admitted to your
ward service for LE cellulitis
Upon questioning, he admits to injecting IV
heroin
Hed like to quit the habit, but doesnt want the
stigma of going to a drug abuse clinic
He asks if theres anything you can do to help
him, as hes heard of a new drug that can be
prescribed by general physicians for drug detox

4
Background

1914 Harrison Narcotic Drug Act
Illegal for physicians to prescribe narcotics for
the tx of opioid dependence
Exception methadone (and LAAM) through regulated
programs (Schedule II triplicates)
2000 Drug Addiction Treatment Act
Allows Schedule III, IV, or V narcotics (that
have been FDA approved for such use) to be
prescribed for medically supervised detox
(tapering) or maintenance
Oct. 2002
FDA approved buprenorphine and the combination
buprenorphine/naloxone (DEA III) for detox or
maintenance

5
Background

Buprenorphine narcotic for mod-severe pain
partial mu-receptor agonist
max effective dose 60-70 mg methadone
mixed agonist/antagonist
Mean half-life 36 hrs
Buprenorphine naloxone (narcan)
reduces drug diversion to IVDU (crushing and
injecting IV) since naloxone IV -- withdrawal sxs

6
Fudalla et al. Office-Based Treatment of Opiate
Addiction with a SL-Tablet Formulation of
Buprenorphine and Naloxone. NEJM Sept. 4, 2003
349949-58

Multicenter, randomized, placebo-controlled trial
to assess the safety and efficacy of SL
buprenorphine (and buprenorphine/naloxone) in an
office-base setting

7
Methods

Enrolled adults with opiate dependence (DSM-IV)
Exclusions
Pregnant, nursing, abnl liver labs, Axis I Psych
d/o, methadone/LAAM/naltrexone w/in 2 wks
Study visits in a physicians office
Remote from drug detox/maintenance clinics

8
Methods

DBPCT x 4 wks
Clinic visits daily (M-F) - given pill on that
day
Pts randomized 3 groups
buprenorphine 16mg SL qd
buprenorphine 16mg/naloxone 4mg SL qd
Placebo qd
Open-label safety phase x 1 yr
Clinic visits daily x 2 wks, then up to a 10 dy
supply
buprenorphine/naloxone - up to 24/6 mg qd

9
Outcome Measurements

DBCT
Primary outcomes
of opiate - urine tests (urine samples 3x/wk)
Subjects self-reported cravings for opiates (100
pt. VAS)
Secondary outcomes
Overall status by subject and physician
VAS - worse - no change - better
of urine tests - for other drugs of abuse
Subject retention, adverse events...
Open-Label (urine tests results available)
Outcomes labs, PE, adverse events

10
Results

DBCT
Goal to enroll 384 subjects
After 323 subjects enrolled and 243 (82)
completed the trial, study terminated early
Primary outcomes - urine test cravings
Buprenorphine 20.7 62 -- 33
Bupren/naloxone 17.8 62 -- 30
Placebo 5.8 65 -- 55
(p
Secondary outcomes
Better overall status with study drugs, well
tolerated

11
Results

Open-Label - buprenorphine/naloxone
472 subjects assessed for safety
261 6 months
Most serious AEs
Increases in ALT, AST, LDH in 10 subjects
8/10 with viral hepatitis
urine tests - for opiates
35 ---- 67 (4 weeks -- 1 year)

12
Authors Conclusion

Both buprenorphine alone and buprenorphine
combined with naloxone provide safe and effective
treatment of opiate-addicted persons in an
office-based setting

13
Study Limitations

DBCT biased for poor results (opiate-free)
Short duration (one month)
Fixed dose (individual titration not permitted)
Clinicians blind to urine test results
Biased for better results
Expertise and resources of the study
investigators (not usual clinic physicians)
Did not mimic current use for buprenorphine
prescribing (
needs
Daily (DBCT) or

14
Study Limitations

Buprenorphine vs. placebo ???
Better study
Buprenorpine vs. methadone

15
Our Bottom Line

Buprenorphine acts, as expected, like any opioid
narcotic in opiate addicted persons
Used SL with naloxone, it appears safe and
somewhat effective for opiate addicts in
outpatient clinics
More important than these study results is the
change in recent laws and availability of this
drug for physicians

16
Perspective

17 wk study in 270 pts, buprenorphine SL
methadone or LAAM NEJM 20003431290
French experience
Approved methadone in 1993 and buprenorphine in
1996 by any MD -- encouraged buprenorphine
because harder to OD and easier to detox
By 2001, 80,000 French patients taking
buprenorphine, most by general physicians
Deaths from heroin ODs dropped nearly 80 from
1994 to 1999 (566 -- 118)
2 yr study 900 pts txd by general
practitioners found improvements in social status
and decrease in drug abuse

17
Perspective

Concerns about diversion and abuse --
DEA schedule V (1985) -- schedule III
Limit the number of patients each physician can
treat
combination with naloxone
Drug Addiction Treatment Act of 2000
Requires that physicians undergo 8 hrs authorized
training in the use of buprenorphine
Unless already certified in addiction medicine
Register with the SAMHSA
Tx
As of late June, 3000 physicians have undergone
training, only 1900 had applied

18
Perspective

Anecdotally
Patients must be free of opiates x 1-2 dys to
avoid precipitating withdrawal rxns
Dosing should be individualized - pts may even
titrate own doses
Buprenorphine (Subutex(R)) 2, 8 mg SL tabs
With 0.5, 2 mg of naloxone (Suboxone(R))
Cost 300/month (vs. 30/month for methadone)
More information
Substance Abuse and Mental Health Services
Administration (SAMHSA)
Http//buprenorphine.samhsa.gov

19
Case

31 y.o. supermarket manager who is a heroin user,
asking for your help in the clinics with his drug
dependence
Is this patient like those in the study?
Can only prescribe buprenorphine SL if
Taken an authorized 8 hr training course
Registered with SAMHSA
Formulary drug

20
Case 2

42 year old male with h/o HTN, CKD (Cr 1.7),
and no hx of DM presents to your office
Pt states that he is very concerned about his
kidney function and will try anything to make
sure he does not go on HD
He monitors his BP daily and wants to know how
low should his BP be in order to avoid
progression of his kidney disease.

21
Background

In US approximately 5.6 million adults have
Chronic Kidney Disease (CKD).
Many also have HTN, either as a cause or
complication of kidney disease.
HTN and proteinuria occur in most pts with CKD
and are risk factors for faster progression of
Kidney Disease.

22
Definition of CKD

Reduced excretory fxn (estimated GFR ml/min/1.73 m2)
Cr approximately 1.5 in men
Cr approximately 1.4 in women
Presence of urinary findings
Albuminuria 300 mg/d, or
Ratio of 200 mg Alb/g of Cr

23
Goal of Aggressive BP Management

Slow deterioration of renal function
Prevent cardiovascular disease
However Kaplan et al (Lancet, 1998) and others
reported that excessive lowering of BP is
associated with increased risk for cardiovascular
disease.
The role of ACE-I in treatment of HTN
Agent of choice for patients w/ diabetes
Agent of choice for patients w/ CHF
Reduces urinary protein excretion
Reduces progression of CKD in diabetic and
non-diabetics

24
JNC-7 Guidelines for Pts with CKD

Aggressive treatment of HTN to target
BP
BP 1g/d
Does not address whether the target BP should
vary depending on severity of Kidney Disease.
How low should we go?
Can we go too low?

25
Jafar et al, Progression of Chronic Renal
Diseases. The role of BP Control, Proteinuria,
and ACEIAnn Int Med, August 19, 2003

Meta-analysis
Purpose
To determine the levels of BP and urinary protein
excretion associated with the lowest risk for
progression of CKD
In non-diabetics receiving anti-hypertensive
therapy (ACEI and non-ACEI therapies)

26
Method and Study Design

Meta-Analysis conducted by the ACEI in
Progressive Renal Disease (AIPRD) study group
Searched the English language Medline database
for reports evaluating the effects of ACEI on KD
between 1977 and 1999

27
Methods

Study inclusion criteria
RCTs with a minimum of one year follow-up.
Compared effects of antihypertensive regimens
that included ACEI to regimens that did not
include ACEI (or ARBs).
Concomitant anti-hypertensive meds used in both
groups to achieve a target BP
All pts followed at least once / 3 months for
first year and then every 6 months thereafter.

28
Methods (cont.)

Patient inclusion criteria
HTN
Decreased renal function
Patient exclusion criteria
Renal failure (ESRD), obstructive uropathy, RAS
Type I diabetes, Type II diabetes (excluded
later)
CHF
History of transplantation
History of allergy to ACEI
Pregnancy
Active systemic diseases

29
Final Database

Final Database included
11 RCTs of ACEI used to slow progression of KD.
1,860 pts with non-diabetic KD
22,610 visits
Mean during of follow-up was 2.3 years
Range of 1.4 - 3.2 yrs

30
Primary Outcome

Kidney Disease Progression (KDP) defined as
A two fold increase in serum Cr concentration
from baseline, or
Development of Kidney Failure (KF) defined as
initiation of long term dialysis therapy

31
Results for Anti-Hypertensives

311 pts (16.8) experienced KDP (doubling of
serum Cr or KF) in 2.3 years.
124 (13.2) in ACEI group
187 (20.5) on non-ACEI drugs
A total of 176 (9.5) developed KF
70 (7.4) in ACEI group
106 (11.6) on non-ACEI drugs
(Differences are stat. sign. at p0.001)

32
Results for BP

SBP was more related to KDP than DBP
SBP 130 --- increased risk for KDP RR
from 1.83 (SBP 130-139) to 3.14 (SBP 160)
SBP 110-129 --- lowest risk for KDP
SBP increased risk for KDP (RR
2.48)
After adjustment for different levels of SBP and
urine protein excretion, the risk for KDP was
still lower in patients assigned to ACEI

33
Results for Urine Protein Excretion

The lowest RR for KD progression was at urine
protein excretion
1-2 g/d, RR 1.67
2 g/d, RR 2.25
6 g/d, RR 4.77

34
Results for Urine Protein Excretion in relation
to SBP

Urine protein
RR 1 for SBP 110-159
RR 2 for SBP 160
Urine protein 1 g/d
RR 1 for SBP 110-129
RR 4.7 for SBP 130-139
RR 8 for SBP 160

35
Authors Conclusion

SBP 110-129 associated with lowest risk.
SBP
Urine protein excretion lowest risk of KDP
After adjustment for SBP and urine protein
excretion, the risk of KDP was lower in pts
assigned to ACEI therapy

36
Limitations of Study

Usual weaknesses of meta-analyses
e.g., Combining heterogeneous groups
Did not include newer studies after 1999
Blood pressures and protein excretions only a few
times per year (single time points)
Did not address ARBs

37
Perspective

ACEI useful in non diabetic pts w/ CKD
Some patients have partial reduction in
proteinuria w/ ACEI (Kidney Int 2003)
Recent trial suggests added clinical benefits of
combining ACEI and ARB even with SBP of
(Lancet 2003361117)
Systolic HTN in the Elderly data (Young, J Am Soc
Nephrol 200213) SBP is more strongly
associated with KDP than DBP
Animal studies have also shown a higher risk of
KDP with SBP

38
Case 2

42 y.o. M with HTN and non-diabetic CKD wants to
know how low should his BP be in order to avoid
KD progression.
Is this pt like those in the MA?
Bottom Line
Start ACEI if pt is not on it.
Target SBP ideally between 110 and 130.
Consider urine protein measurements periodically
(urine dipstick -- alb/Cr ratio)
Aim to reduce proteinuria to
Target SBP and not DBP

39
Pharmaceutical Update