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| HIV
Resistance Testing Consultation Service Report |
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Case
#005:
Potential Antiretroviral Strategies for Salvage
Therapy
(May 21, 2001)
Panel
Clinician:
Jody Lawrence, MD
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Panel Members: |
Richard
Aranow, MD
George W. Beatty, MD, MPH
Steven G. Deeks, MD
Betty J. Dong, Pharm.D
Amy V. Kindrick, MD
Jody Lawrence, MD
Michael
L. Lim, Pharm.D (11/00-6/01)
John Stansell, MD (3/01-6/01)
Jason Tokumoto, MD
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History
Resistance Test Findings
Interpretations/Implications for Treatment
Recommendations |
Project
Director: |
Ronald
H. Goldschmidt, MD |
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Disclaimer:
This information has been developed solely as an educational resource for health
care professionals interested in HIV care and research. The information presented
represents the views of the Panel members only and not necessarily those
of the National HIV/AIDS Clinicians' Consultation Center's HIV Telephone
Consultation Service (Warmline), the Positive Health Program at San Francisco
General Hospital, or sponsoring organizations. Resistance testing can help
identify whether certain drugs or classes of drugs might be ineffective,
but cannot establish which drugs will be effective. Furthermore, test results
can be inaccurate and interpretation of tests is not yet standardized. Because
of the many factors involved in treatment decisions when resistant virus
is present, the antiretroviral regimens and the therapeutic strategies discussed
are not the only possible options and might be different from current Practice
Guidelines. Other sources of information on resistance testing, such as clinical
HIV websites, can be of help. Health care professionals should consult the
HIV Telephone Consultation Service (Warmline) or HIV experts in their community
before using any of the recommended therapeutic regimens or strategies in
this document.
Consultation:
Consultation
is available to California AIDS Drug Assistance
Program providers through the California State Office of AIDS
Voucher Program by calling the HRSA/ AIDS ETC National HIV Telephone
Consultation Service (Warmline) at 1/800/933-3413. The HIV Resistance
Testing Consultation Service is supported by a grant from the
California State Office of AIDS through the Pacific AIDS Education
and Training Center. |
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| History/Clinical Course |
A
36 -year -old man with a history of IVDU presented to his
current primary care provider in November
1996 with a CD4 count of 13cells/mm3 and a viral load (VL)
of 186,000. The patient initially was treated with indinavir
(IDV) plus lamivudine (3TC) and zidovudine (AZT) but subsequently
failed therapy and was placed on nevirapine (NVP) plus nelfinavir
(NFV) plus stavudine (d4T) plus didanosine (ddI) with the response
below. The patient was initially non-adherent. However, he
did not show a VL response even during a period of documented
good adherence to the treatment. While on this last regimen,
he developed elevations in his liver function tests which was
associated with nausea, vomiting, and abdominal pain. These
symptoms were not associated with ETOH use. This prompted the
primary care provider to obtain a genotype and stop all antiretroviral
treatment until symptoms resolved. The patient has no history
of opportunistic infections or viral hepatitis but he does
have peripheral neuropathy.
Date |
Regimen |
CD4 |
VL |
11/96 |
Baseline (pre-treatment) |
13 |
186,000 |
11/96 – 12/97 |
AZT, 3TC, IDV (1st regimen) |
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12/97 |
|
20 |
100,000 |
12/97 – 10/31/00 |
d4T, ddI, NFV, NVP (2nd
regimen) |
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8/98 |
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188,000 |
10/99 |
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110,000 |
6/00 |
patient admitted non-adherence |
84 |
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8/00 |
entered adherence study
with 98% adherence (pill ct, phone) |
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10/31/00 |
developed increased LFTs
with nausea + abdominal pain, stopped all ARVs, got genotype |
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|
11/00 |
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77 |
112K |
Current medications: Azithromycin, Bactrim, Ultram, and Marinol Back to Top  |
| Resistance
Test Findings |
Key Mutations
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| NRT |
M41L, A62V, L74V, V75T, L210W, T215Y |
| NNRTI |
K103N, Y181C |
| PI |
M46I, G73S/A, V77I, L90M |
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| Interpretation/Implications
for Treatment |
This patient is significantly immunocompromised
with a CD4 count that has been persistently less than 100 for
the last 3 years. He has limited treatment options based on
his prior exposure with treatment failures to multiple antiretroviral
drugs, including agents from all three major classes of currently
available HIV drugs.
Previous antiretroviral exposure by class include the following:
PI: Nelfinavir, Indinavir
NNRTI: Nevirapine
NRTI: AZT, ddI, d4T, 3TC
The genotypic resistance pattern
indicates likely reduced sensitivity to the following:
1. Protease inhibitors (PI): saquinavir, nelfinavir, indinavir,
ritonavir, lopinavir , amprenavir
The mutation L90M is thought to confer fairly broad class resistance
to protease inhibitors. The mutation 46 is a major resistance
mutation for indinavir and is commonly seen in resistance to
other protease inhibitors as well. The mutation 73 is primarily
seen in resistance to indinavir, saquinavir, and lopinavir.
The mutation at 77 is commonly seen with general protease inhibitor
exposure and may represent a polymorphism or contribute to
resistance when added to other mutational changes.
The protease inhibitors most likely to be effective based
on this genotypic resistance pattern are amprenavir and lopinavir.
A phenotype might help to assess whether amprenavir or lopinavir
would be more active in this patient.
2. Non-Nucleoside Reverse Transcriptase
Inhibitors (NNRTI): efavirenz, nevirapine, delavirdine
The mutation at site K103N confers high level cross-resistance
to all the currently FDA-approved NNRTIs (nevirapine, delavirdine,
efavirenz). The mutation at Y181C confers high level resistance
to nevirapine and delavirdine plus moderate to high level resistance
to efavirenz.
3. Nucleoside Reverse Transcriptase Inhibitors (NRTi): AZT,
ddI, ddC, d4T, abacavir
The zidovudine (AZT)” or “thymidine analogue” mutations
(i.e. M41L, 62, L210W, T215Y) are associated with broad NRTI
class resistance. The mutation at L74V is associated with resistance
to ddI/ddC/ABC and the mutation at V75T is associated with
d4T resistance.
Note: although the patient’s HIV
genotypic data obtained on his last treatment regimen does
not show the 184 mutation
associated with 3TC resistance, this mutation was likely present
earlier when the patient experienced treatment failure while
taking 3TC. Therefore low levels of viral populations resistant
to 3TC may remain and may contribute to subsequent resistance
to abacavir (ABC).
Back
to Top |
| Recommendations |
In February 2001, the panel met
and discussed potential antiretroviral strategies for salvage
therapy for this patient. The consensus opinion of the panel
was to treat this patient with a combination of two or more
protease inhibitors plus two or more NRTIs (recycled). Use
of the currently available NNRTIs (nevirapine, delavirdine,
or efavirenz) is not recommended based on the genotypic resistance
pattern indicating cross-resistance to all of these drugs.
Since this patient has a history of peripheral neuropathy,
the panel would be cautious in using d4T and ddI as recycled
agents in the next salvage regimen.
The optimistic goal in this case is to reach full and durable
viral suppression with future regimens. However attaining partial
viral suppression while attempting to prevent further CD4 count
loss may be a more realistic goal until newer drugs are available.
For greater durability of antiviral
response, one would ideally like to include in the new regimen
more
than one new drug to
which the patient’s virus is likely to be sensitive.
If the patient and primary provider wished to await the availability
of an experimental drug through an expanded access program,
the agents currently furthest along in development are tenofovir
and T20. Tenofovir is available through an expanded access
program from Gilead Sciences and is pending FDA approval.
REGIMEN
OPTIONS |
Treatment
Option 1:
Kaletra (Lopinavir+Ritonavir) + Combivir
(AZT+3TC) |
PROs
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CONs
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- simple regimen
- low pill burden
- not associated
with peripheral neuropathy
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Treatment
Option 2:
Kaletra (Lopinavir+Ritonavir) + Trizavir
(AZT+3TC+Abacavir) With or without Tenofovir +/-
T20 (depending on availability) |
PROs
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CONs
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- simple regimen
- low pill burden
- may be more
effective with additional drugs
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- the increased
drug toxicity may outweigh the potential
increase in potency
- T-20 requires
BID injections
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Treatment
Option 3:
Kaletra (Lopinavir+Ritonavir) + Amprenavir
+ either Combivir or Trizavir with or without Tenofovir
+/- T20 (depending on availability) |
PROs
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CONs
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- may be more effective with the combination
of 2 potent PIs (plus ritonavir as a pharmacokinetic
enhancer)
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- drug toxicity
may be substantial with “MegaHAART”
- Added
costs and toxicity with ABC in Trizivir
compared to Combivir.
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DOSING,
MONITORING and FOLLOW-UP RECOMMENDATIONS
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DOSING:
Lopinavir
and ritonavir can be given as a fixed combination
capsule known as Kaletra. Each Kaletra capsule contains
33 mg of ritonavir and 133 mg of lopinavir. The standard
dosage is 3 capsules bid. The panel thought that
amprenavir, when used with the above dose of ritonavir,
should be dosed at 600 mg bid. The manufacturer recommends
750 mg bid amprenavir when used in combination with
Kaletra. The correct dosing of the combination of
amprenavir with Kaletra is unknown.
Combivir and Trizavir
should be given at their standard doses of one
pill bid, respectively.
The dosing of
T-20 and tenofovir would be determined by the
relevant protocols.
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CLINICAL
MONITORING:
After changing
the antiretroviral regimen, it is advisable
to monitor viral load and CD4 count at 1 month,
2 months, and 4-6 months. The patient should
also be monitored closely for changes in blood
lipids, blood glucose, and liver function tests
(LFTs) as PI’s (particularly lopinavir/ritonavir
with regards to lipids) can adversely affect
these values.
When beginning
or restarting abacavir, the patients should
be educated to monitor
for symptoms suggestive
of an abacavir hypersensitivity reaction. Rash,
fever, respiratory symptoms, flu-like symptoms
of malaise and fatigue, and gastrointestinal
symptoms of nausea, vomiting, and abdominal
pain should be aggressively evaluated
per the package
insert. If abacavir hypersensitivity reaction
is suspected, rechallenge should be avoided
since fatalities can occur.
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