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Advances In HIV Treatment: HAART And Its Complications

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Advances In HIV Treatment: HAART And Its Complications Amy V. Kindrick, M.D., M.P.H. National HIV/AIDS Clinicians Consultation Center April 26, 2003 – PowerPoint PPT presentation

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Title: Advances In HIV Treatment: HAART And Its Complications

1
Advances In HIV Treatment HAART And Its
Complications

Amy V. Kindrick, M.D., M.P.H.
National HIV/AIDS Clinicians Consultation Center
April 26, 2003

2
Overview

New concepts and strategies in HIV antiretroviral
therapy
Long-term toxicities of ARV therapy
New and investigational ARV agents
New strategies for OI management
Common management challenges

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9
Typical CD4 Response to HAART
10
Challenges of HAART

Complexity
Toxicity
Accessibility
Incomplete efficacy
Viral resistance

11
Whats a Clinician to Do?

Expanding number of agents adds complexity
Minimal clinical experience when drugs released
adds toxicity risk
Shortage of outcomes data adds uncertainty

12
New ARV Treatment Strategies and Concepts

Adherence to treatment
ARV resistance and resistance testing
Interrupting ARV therapy
Treating primary HIV infection

13
Adherence

Drugs dont work if people dont take them.
C. Everett Koop

14
Reasons for Non-Adherence Clinician vs Patient
Views
Chesney M. Adherence to antiretroviral therapy.
12th World AIDS Conference, 1998 Geneva. Lecture
281
15
Viral Suppression And Adherence By Refill Records
N 504 pts on HAART
Achieving lt500 copies/mL
Adherence, by prescription refill
Montessori, V, et al. XII International
Conference on AIDS, Durban, South Africa, 2000.
Abstract MoPpD1056.
16
Measuring Adherence Electronic Bottle Caps

Caps harbor chips that register each time a
bottle is opened or closed

MEMScaps, Aardex Corp.
17
Viral Suppression And Adherence By MEMS
Patients with HIV RNAlt400 copies/mL,
PI adherence, (electronic bottle caps)

Paterson, et al. 6th Conference on Retroviruses
and Opportunistic Infections 1999 Chicago, IL.
Abstract 92.
18
Adherence and AIDS-Free Survival
10 adherence difference 21 reduction in risk
of AIDS
1.00
0.75
Proportion AIDS-Free
0.50
0.25
P .0012
0.00
0
5
10
15
20
25
30
Months from entry
Bangsberg D, et al. AIDS. 2001151181
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Why Does HAART Fail?
21
ARV Resistance
22
What Is Resistance?

Viral replication in the presence of drug pressure

23
Basic Pharmacology Principles
Cmax
Drug Level
Cmin
IC90
Area of Potential HIV Replication
IC50
Dosing Interval
Time
Dose
Dose
24
How Does Resistance Develop?

High replication and transcription error rates
generate mutant HIV variants
Spontaneously generated variants often contain
mutations that confer survival advantage in the
presence of antiretroviral agents
Poor adherence or suboptimal regimens can lead to
resistance and viral breakthrough

25
HIV-1 Quasi Species in Untreated and Treated HIV
InfectionHeterogeneity vs. Selection of
Resistant Strains
acute
chronic
AIDS
Plasma viremia
Time
V. Simon, MD
26
Development of Drug Resistance
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Antiretroviral Resistance Testing

Goals
Improve virologic control and immunologic benefit
Minimize exposure to ineffective agents
Options
Genotype
Phenotype
Virtual phenotype

31
Definitions

Genotype
Virus nucleotide sequence from which a proteins
amino acids can be deduced
Mutations reported as change in the deduced amino
acid sequence, e.g., Met184Val
Specific mutations confer phenotypic resistance
The phenotype is always derived from the genotype
Phenotype
Relative growth of the virus in the presenceof
different drug concentrations
Usually reported as the drug concentration that
inhibits virus replication by 50 (IC50), or the
fold increase in IC50

32
Genotype Vs Phenotype
Strengths
Weaknesses
33
HIV Drug Resistance Assays DHHS Recommendations
Recommended
Optional
Not Generally Recommended
34
Resistance Testing Factors

Cost
Time
Access
Technical limitations
Thresholds
Partial resistance
Mutations yet to be identified
New drugs
Different sequence regions for old drugs
Uncertain clinical impact

35
Complications Of HIV And ARV Therapy
36
Long-Term Complications of HIV and ARV Therapy

Body habitus changes
Insulin resistance/hyperglycemia/diabetes
Hyperlipidemia
Lactic acidosis
Hepatic steatosis
Osteopenia
Avascular necrosis

37
Abnormal Fat Redistribution

Syndromes
Abnormal fat accumulation
Buffalo hump
Increased abdominal girth
Increased breast size
Peripheral fat wasting
Sunken cheeks
Thin extremities
Prominent peripheral musculature and veins
Prevalence unknown (est. 2 to 80)
Increased with duration of HIV infection ARV tx
Associated with PI and NRTI use
Mechanism unknown

38
Fat Redistribution Syndromes
39
Cervico-dorsal Fat Pad
40
Central Fat Accumulation
41
Facial Lipoatrophy
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Abnormal Insulin and Glucose Metabolism

Associated with ARVs, especially PIs
Mechanism unclear
?PI inhibition of glut-4 transporter
Risk factors
Older age
African American ethnicity
Clinical syndromes
Insulin resistance
Hyperglycemia
Type 2 diabetes
Treat as usual

44
Hyperlipidemia

Mechanism unknown
Prevalence
Clinical syndromes
Hypertriglyceridemia
Hypercholesterolemia
Mixed
? Impact on CV risk
Manage per AHA guidelines

45
Hyperlipidemia Treatment Considerations

Risk of increased insulin resistance with niacin
Increased risk of myopathy and rhabdomyolysis
Interactions between ARVs and statins
Prefer pravastatin or atorvastatin
Avoid lovastatin and simvastatin
Interactions between statins and fibrates
May respond to ARV change

46
Lactic Acidosis And Hepatic Steatosis

Class toxicity of NRTIs (Black Box warning)
Incidence est. 4/1000 patient-years
Risk factors
Older age
Female gender
ddI, ddC, or d4T use gt 3 months
ddId4T in pregnancy

47
Lactic Acidosis Clinical Presentation

Acute or subacute onset
Varying symptoms, including
Malaise a/o fatigue
Abdominal pain
Nausea a/o vomiting
Anorexia
Hepatomegaly
Breathlessness

Abnormal laboratory values
Elevated serum lactate
Anion gap
Transaminitis
Low serum bicarbonate
Elevated amylase/lipase

48
Management Of Lactic Acidosis

Be alert to symptoms
Stop ARVs if symptomatic and lactate elevated
May consider continuing ARVs if
Symptoms absent or mild
Lactate only minimally elevated (e.g., 2-4
mmol/l)
ddI, d4T can be replaced
Anecdotal treatments for mild disease
L-carnitine
Riboflavin
Thiamine

49
Delayed Onset NRTI Toxicity

Hypothesized due to toxic effects of NRTIs on
human mitochondria
NRTIs inhibit DNA polymerase ? required for mDNA
synthesis
Clinical syndromes
Pancreatitis
Myopathy
Peripheral neuropathy
Bone marrow toxicity
D drugs especially implicated

50
Avascular Necrosis of the Hip
51
Osteopenia and Avascular Necrosis of the Radial
Head
52
Changing TherapyConsiderations

Recent clinical history and physical examination
Two plasma HIV RNA levels
CD4 T cell count
Remaining treatment options

Drug failure or drug toxicity?
Medication adherence
Pharmacology drug interactions
Resistance profile
Patient preference

53
Should Failing HAART Be Stopped?

Better to stay on some ARV regimen than none
Resistance mutations may impair viral fitness
Specific mutations may enhance response to
specific ARV agents
CD4 count gains may be sustained despite
incomplete viral suppression

Deeks, et al. NEJM 2/15/01
54
Antiretroviral Therapy Persistent Uncertainties

When to start
What to start with
When to change
What to change to
When to stop (if ever)

55
ARV Treatment Interruption
56
Treatment Interruption Rationale

Enhance HIV-specific immune response
In primary infection
In chronic infection
Reduce treatment-associated complications
Toxicity
Cost
Treatment fatigue

57
Treatment Interruption Target Groups

ARV treatment fully suppressive
Started during acute infection
Started after infection chronic
ARV treatment not fully suppressive

58
Structured Treatment Interruptions
59
Treatment Interruptions Real Risks And
Theoretical Benefits

Real Risks
Loss of viral suppression
Development of resistance
Repopulation of reservoirs
Acute antiretroviral syndrome
CD4 cell decline
Loss of immune responses
Pharmacokinetic issues
Increased transmission
Disease progression
Death

Theoretical Benefits
Reduced drug exposure
Minimize resistance
Minimize toxicity
Maximize tolerability
Reduced costs
Increased access to drugs
Improved adherence
Better QOL
Enhanced immune function
Long-term viral control off ARVs

60
Structured Treatment Interruptions Conclusions

Still experimental
Rapidly evolving field
Stay tuned!

61
ARVs For Acute HIV Infection
62
Primary HIV Infection Rash
63
Primary HIV Infection Oral Ulcers
64
Natural History of HIV Infection
65
The Berlin Patient
Lisziewicz J et al. NEJM 1999 340 1683-1684.
66
ARV Therapy for Primary Infection