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Evaluation
of Indinavir/Ritonavir Versus Saquinavir/Ritonavir in HIV Patients:
The MaxCmin-1 Trial
Although HIV and Hepatitis.com has reported on these study
data several times, presented
most recently at the 5th Lipodystrophy Workshop in Paris (July
9-11, 2003), complete results of this randomized, multi-center,
phase IV trial appear in the current issue (September 1, 2003) of
The Journal of infectious Diseases. Following is a summary
review of that article.
The MaxCmin-1
trial was designed to assess whether equivalence exists in efficacy
and safety between Crixivan
(indinavir/IDV) plus Norvir
(ritonavir/RTV) 800/100 mg b.i.d. and Fortovase
(saquinavir/SQV) plus RTV 1000/100 mg b.i.d., in combination with
at least 2 non-PI drugs, with the primary outcome being the incidence
of protocol-defined virological failure.
When this comparative trial started in 2000, the combination of
IDV/RTV 800/100 mg b.i.d. was a commonly used RTV-boosted protease
inhibitor (PI) regimen. A switch to the RTV-boosted regimen was
motivated by poor adherence to IDV 800 mg three times daily (the
FDA-approved IDV dose) as well as by data suggesting the IDV dosing
frequency could be reduced to twice daily. Furthermore, the pharmacokinetic
data also suggested that the RTV-boosted twice-daily regimen might
allow for dropping the fasting requirement for IDV.
There have been a number of studies evaluating use of the double
PI combination of SQV/RTV, primarily in a twice-daily dosing schedule.
In most patients, this regimen is associated with gastrointestinal
adverse events. In addition, there was a concern that in a SQV/RTV
regimen at a dose of 1000/100 b.i.d, only SQV would show virologic
activity, compared to the SQV/RTV 400/400 mg b.i.d. regimen, in
which both drugs had virological activity.
The MaxCmin-1 trial is the first direct comparison of two RTV-boosted
PI regimens.
Patients and Methods
Patients
were primarily white (84%) men (78%) who engaged
in homosexual- or bisexual-risk behavior (49%) with a median age of 39 years. The median CD4
cell count nadir was 110 cells/microliter, the
median CD4 cell count was 277 cells/microliter, and the
median VL was 3.9 log10 copies/mL; 39% of patients had a baseline VL of <400 copies/mL,
and 30% had had a prior clinical AIDS-defining
disease.
At
enrollment, 25% of patients were ART-naive,
14% were ART-experienced but PI-naive, and 61% were PI- experienced. However, only patients with an
equal chance of benefit from and/or risk of
development of treatment-related AEs to the two study PIs at the time of screening could be
randomized.
Randomized
patients, irrespective of whether they started receiving or switched from the assigned treatment, were followed up at baseline (first day of intake of assigned
treatment) and at weeks 4, 12, 24, 36, and
48.
During follow-up visits, the following procedures were
performed: clinical evaluation, safety analyses (hemoglobin; white blood cell, lymphocyte, and platelet counts;
and creatinine, aspartate aminotransferase and/or alanine aminotransferase, bilirubin, and amylase
levels), and viral load (VL) and CD4 cell count measurements.
In
addition, fasting total cholesterol, low-density lipoprotein
(LDL) cholesterol, and total triglyceride levels were measured at baseline and at weeks 4 and
48.
Patients randomized to receive SQV/RTV were allowed to change from the SQV soft-gel formulation (Fortovase) to the hard-gel formulation (Invirase) without this being considered a switch from the assigned treatment.
During the trial, modification of the randomized treatment
was allowed in the case of virological failure
or treatment-limiting toxicities. If available, dose reduction was performed on the basis of therapeutic-drug monitoring. Of note, patients
experiencing virological failure, according to the protocol's definition, were allowed to continue receiving
the assigned treatment at the discretion of
the treating physician.
Definition of Virological, Immunological and Clinical Failure
For patients
entering the study with a VL of <200 copies/mL,
virological failure was defined as a VL of
> or = 200 HIV-1 RNA copies/mL. For patients entering the study with a VL of > or = 200 copies/mL, virological failure was defined as any
increase in HIV-1 RNA load of > or = 0.5
logs and/or a VL of > or = 50,000 HIV-1
RNA copies/mL at week 4, > or = 5000 copies/mL at week 12, or > or = 200 copies/mL at week 24 or thereafter.
Immunological failure was defined as a decrease in the CD4
cell count of >50% from the baseline level,
provided that the baseline CD4 cell count was
>150 cells/microliter. For patients with a baseline CD4 cell count of 100  150 cells/microliter,
immunological failure was defined as a CD4
cell count of <50 cells/microliter and, for patients
with baseline CD4 cell count of <100 cells/microliter,
immunological failure was defined as a CD4 cell
count of <25 cells/microliter.
All
cases of suspected immunological failure were confirmed
by a second CD4 cell count measurement performed
at least 1 week later. Once reconfirmed, the
time of immunological failure was defined as the
time of the first measurement that met the
failure criteria. Clinical failure was defined as the development of a new AIDS-defining disease
or as the relapse of an AIDS-defining disease
that had been successfully treated previously.
Power Calculation and Statistics
The
trial was powered to show equivalence between the
study arms, with an 80% chance that the 95%
confidence interval (CI) for the difference in
virological failure rates would exclude a difference of >15% in either direction. This was based on a sample size of 150 patients/arm and an
underlying failure rate of 20% in both arms.
The primary population for analysis was the intention-to-treat/exposed
(ITT/e) population, including all randomized patients
who had taken at least one dose of the assigned
treatment. This analysis is also termed the
"ITT switch included" analysis. In the other protocol-stipulated analysis, switching from
the assigned treatment constituted failure (ITT/e/switch
= failure [ITT/e/s]). In both analyses, patients
who withdrew consent, who were lost to follow-up,
or who died, constituted failure, and the time
of failure was the time of the event (whichever
came first). Some patients withdrew their consent
during follow-up but permitted reporting of laboratory data measured as part of their routine care. For these patients, withdrawn consent did not constitute (virological) failure.
Results
Complete week-48 follow-up data were available for 285 (93%) of the 306 patients who initiated the assigned treatment, 202 (66%) of whom continued to receive the assigned treatment. No difference was seen
between the 2 study arms in the rate of patients lost to follow-up (7%).
The
104 patients who prematurely switched from the
assigned treatment did so primarily because of nonfatal,
clinical AEs (n = 67). Among the 104 patients,
no significant differences were observed between
the study arms in the proportion of patients
who switched treatment regimens.
Nine
patients switched from IDV/RTV to SQV/RTV, and 4
patients switched from SQV/RTV to IDV/RTV. There was a significantly higher percentage of patients
in the IDV/RTV arm (41%) than in the SQV/RTV arm (27%) who prematurely switched from the assigned treatment. This difference was driven by patients who discontinued the randomized treatment because
of a nonfatal, clinical AE (28% of patients
assigned to IDV/RTV arm vs. 15% in the SQV/RTV
arm).
Of
the nonfatal, clinical AEs that led to patients'
switching from the assigned treatment, 66% were
of grade 1 or 2. More renal, skin and hair,
and gastrointestinal AEs were observed in
patients in the IDV/RTV arm. Twenty-two patients reduced the dose of the assigned treatment during follow-up (21 in the IDV/RTV arm and 1 in the
SQV/RTV arm).
Virological, Immunological and Clinical Outcomes
The primary efficacy outcome, rate of virological failure,
was seen in 77 (25%) of 306 patients, with no difference between the study arms. The median VL at the time of failure was 2279 copies/mL,
slightly higher in the IDV/RTV arm (3857 copies/mL)
than in the SQV/RTV arm (881 copies/mL) (P
= .40). The difference between the 2 study
arms in the proportion of patients experiencing virological failure was 2.2% (95% CI, -2.8% to 7.2%), with a higher proportion of protocol-defined
virological failures in the IDV/RTV arm.
Using
a Farrington-Manning equivalence test, the investigators
found sufficient evidence at the 5% level
of significance to claim that the difference
in success rates between the 2 treatments is
<15% (P < .0048).
The
higher discontinuation rate in the IDV/RTV arm resulted
in a significantly higher virological failure rate in this arm in the ITT/e/s analysis. No difference
was seen between the study arms in the during-treatment
analysis.
Only
6 patients experienced immunological failure (4
in the IDV/RTV arm and 2 in the SQV/RTV arm).
An increase of > or = 100 CD4 cells/microliter
at any time during follow-up was seen in 181
patients, at a median of 98 days. There was
no significant difference between the study
arms in the number of patients or time to an increase
of > or = 100 CD4 cells/microliter.
Clinical failure was seen in 23 patients after a median
of 80 days (13 patients classed as CDC category
B, 7 patients classed as CDC category C, and
3 deaths); of these clinical failures, 14
(4 patients classed as CDC category C and
1 death) were observed in the IDV/RTV arm,
and 9 (3 patients classed as CDC category
C and 2 deaths) were observed in the SQV/RTV
arm.
The
low number of clinical failures precluded formal statistical analysis. In none of the fatal cases was the death directly related to the assigned treatment: the death in the IDV/RTV arm was due to Castleman disease, and the 2 deaths in the SQV/RTV arm were due to Pneumocystis
carinii pneumonia and hepatitis C end-stage
liver failure.
Adverse Events
Of
the patients exposed to the study medication,
100 (33%) of 306 experienced at least 1 AE
of grade 3 or 4 (65 [41%] in the IDV/RTV
arm vs. 35 [24%] in the SQV/RTV arm. Of these, the treating physician assessed the relationship
to the assigned treatment as being at least
possible in 46 (29%) in the IDV/RTV arm versus
19 (13%) in the SQV/RTV arm. There was a significant difference between the 2 study groups in the distribution by organ system of AEs grade 3 and 4, with a higher number of
renal, dermatological, and gastrointestinal side effects
in the IDV/RTV arm.
Lab Results
The median percentage change from baseline in fasting
total cholesterol, LDL cholesterol, and total
triglyceride is shown in Figure 1 below. Significantly
higher lipid elevations were seen in the IDV/RTV
arm, compared with the SQV/RTV arm, at weeks
4 and 48 (ITT/e analysis).
Figure
1
Median percentage change from baseline in fasting total
cholesterol, low-density lipoprotein (LDL) cholesterol, and total triglyceride levels in the intention-to-treat/exposed
analysis. Nos. within the bars are the no.
of measurements (i.e., patients) at each time
point. IDV, indinavir; RTV, ritonavir; SQV, saquinavir.
No
difference between the study groups was seen in
hematological, renal, or hepatic laboratory parameters,
except for bilirubin levels, which were 10
and 11 micromole/L at baseline in the IDV/RTV
and SQV/RTV arms, respectively (normal range, 4
22 micromole/L).
In the SQV/RTV arm, the bilirubin level did
not change over time, whereas, in the IDV/RTV
arm, it increased to 20 micromole/L at week
4, followed by a decline to 15 micromole/L
at week 48.
Commentary
Equivalence
was observed for efficacy, whereas IDV/RTV led
to an increased risk of treatment-limiting AEs and
AEs of grade 3 and/or 4. As a consequence
of the safety profile of IDV/RTV, fewer patients
continued to receive this treatment throughout the
48 weeks, leading to differences in the efficacy
analyses, in which continuation with study medication influences the outcome. In addition, IDV/RTV was
found to cause a higher risk of elevating
blood levels of lipids and bilirubin.
In
the analysis in which switching from the assigned
treatment is equal to virological failure or
lack of virological suppression, SQV/RTV tended to have superior virological activity than did IDV/RTV.
This result was to be expected, because a
higher proportion of patients in the IDV/RTV
arm switched from the randomized treatment.
The
trial was not designed and did not have the
statistical power to test whether there were
differences in risk of protocol-defined immunological
and clinical failures between the 2 study
arms.
In
the present trial, 21 (13%) of 158 patients
in the IDV/RTV arm reduced the IDV dose. The
trial was not designed to evaluate whether
this strategy lowered the risk of AEs or affected
the efficacy of the treatment, nor was the
sample sufficiently large for formal testing
of these important questions.
Compared
with patients in the SQV/RTV arm, patients
in the IDV/RTV arm had significant increases from
baseline in total cholesterol, LDL cholesterol, and triglyceride levels at weeks 4 and 48. Other drugs (NNRTIs and stavudine) that could potentially
influence these parameters were well balanced
between the 2 groups at baseline.
Therefore, these findings suggest that, relative to SQV/RTV, IDV/RTV affects the lipid metabolism adversely.
Because the same RTV dosing was used in both
arms, it is likely that it is the IDV component that causes lipid levels to increase. However,
another possibility is that the RTV metabolism
is affected differently by IDV, compared with
SQV.
In conclusion, the authors state, “We have found that,
in this open-label study of a heterogeneous patient
population, reflecting the real-life situation, SQV/RTV
has antiretroviral effects comparable to those of IDV/RTV in the doses studied. We observed more treatment-limiting AEs in the IDV/RTV arm, relative
to the SQV/RTV arm, and found that more patients in the SQV/RTV arm remained virologically suppressed
at week 48, probably because of a better toxicity profile.”
09/10/03
Reference
UB Dragsted
and others (for the MaxCmin1 Trial Group). Randomized Trial to Evaluate Indinavir/Ritonavir versus Saquinavir/Ritonavir in Human Immunodeficiency Virus Type 1 Infected Patients: The MaxCmin1 Trial.
The Journal of Infectious Diseases 188:635-642. September 1, 2003.
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