Use of new antiretroviral drugs and classes in Bahia, Brazil: a real life experience on salvage therapy of AIDS patients

Brites, Carlos; Nóbrega, Isabella; Netto, Eduardo Martins

doi:10.1016/j.bjid.2015.03.005

ABSTRACT

Antiretroviral therapy has significantly evolved in the last decade, with an increasing number of new drugs and classes. Currently, even heavily experienced patients can be successfully treated with new regimens. In Brazil, the recent incorporation of some new antiretroviral drugs made it possible to suppress HIV plasma viremia in most treated patients, with significant benefits in terms of quality of life and survival. However, little has been published on outcomes of patients under new drugs-based regimens. We reviewed the safety and efficacy of antiretroviral regimens using recently introduced drugs in Bahia. Our results confirm that patients using darunavir, raltegravir, enfuvirtide, or etravirine presented with a high rate of virological suppression without significant adverse events, after one year of follow-up.

Keywords:
HIV; Antiretroviral; Salvage therapy

One of the most important problems in the treatment of HIV-1 infected patients has been the development of resistance to antiretroviral (ARV) drugs. In the early HAART era, patients exposed to multiple ARV regimens usually presented with a broad spectrum of drug resistance, making it difficult to define a fully suppressive ARV regimen. The absence of effective treatment usually led to disease progression and death.¹1 . Pennings PS. HIV drug resistance: problems and perspectives. Infect Dis Rep. 2013;5 Suppl. 1:e5. The development of new drugs and classes of ARV dramatically modified the scenario of salvage therapy for patients previously exposed to multiple regimens. Several studies provided strong evidence that even patients with complex drug resistance profile could be successfully treated with a regimen that include new, active ARV drugs.²2 . Fernández- Montero JV, Barreiro P, Soriano V. HIV protease inhibitors: recent clinical trials and recommendations on use. Expert Opin Pharmacother. 2009;10:1615-29. ³3 . McKinnell JA, Lin HY, Nevin CN, et al. Early virologic suppression with three-class experienced patients: 24- week effectiveness in the darunavir outcomes study. AIDS. 2009;23:1539-46. ⁴4 . Makinson A, Reynes J. The fusion inhibitor enfuvirtide in recent antiretroviral strategies. Curr Opin HIV AIDS. 2009;4:150-8. ⁵5 . Gazzola L, Cicconi P, Ripamonti D, et al. Efficacy and safety of darunavir/ritonavir plus etravirine dual regimen in antiretroviral therapy- experienced patients: a multicenter clinical experience. HIV Clin Trials. 2014;15:140-50. ^and ⁶6 . Eron JJ, Cooper DA, Steigbigel RT, et al. Efficacy and safety of raltegravir for treatment of HIV for 5 years in the BENCHMRK studies: final results of two randomised, placebo- controlled trials. Lancet Infect Dis. 2013;13:587-96.

Brazil recently provided access to new ARV drugs like ritonavir-boosted darunavir (DRV/r), raltegravir (RAL), etravirine (ETV), and maraviroc (MRV). However, the Brazilian AIDS Program established several rules to use these new ARV drugs, which are available only as "third line" options. There is scarce information on the outcomes of patients treated with these new drugs/classes in developing countries. In the present work we evaluated the impact of new drugs use on viral suppression, and its tolerability by patients with a history of previous failures to multiple regimens.

We reviewed the Bahia state's central pharmacy registry to identify the first patients who used darunavir/ritonavir (DRV/r), enfuvirtide (ENF), raltegravir (RAL), etravirine (ETV) or maraviroc (MVC) up to August 2011. After identification of all patients who used or were in use of these ARV drugs, we reviewed the medical records to evaluate clinical characteristics, virological response, and tolerability of ARV regimens containing these new drugs.

We compared CD4 counts and plasma HIV-1 RNA viral loads at the moment of initiation of ARV regimens containing one or more of these new drugs, and 6 and 12 months thereafter. The proportion of patients with undetectable viral load was compared at each time-point, as well as the change in CD4 count. Adherence to therapy was also evaluated, and the frequency of adverse events was recorded.

Mean age for patients included in this study was 41.2 ± 11.9 years. Around two-thirds (60%) were male, and black/racially mixed (68%). Only 17% described themselves as white, while 15% were of other ethnic groups. The mean number of previous ARV regimens was 4.8 ± 3.3. Mean HIV-1 RNA plasma viral load was 4.6 ± 1.3 log copies/mL, while mean CD4+ cell count was 273 ± 32 cells/mm³. As expected in a subpopulation of patients with long-term treatment history, most of them had a previous diagnosis of infectious and non-infectious comorbidities. Table 1 shows the main health problems detected in this population.

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Table 1 -
Clinical characteristics of 194 patients who started an ARV regimen containing new ARV drugs.

We identified a total of 546 medical prescriptions of at least one of these new ARV, distributed between the four referral centers in Salvador city, Bahia, Brazil, and several smaller cities in Bahia. Table 2summarizes the number of prescriptions of each ARV drug. Due to the limited access to medical charts from other institutions, we focused the review on medical records of two main referral centers for AIDS care in Bahia, namely Centro de Ensino, Diagnóstico, Assistencia e Pesquisa (CEDAP) and Complexo Hospitalar Prof. Edgard Santos (C-HUPES), at the Federal University of Bahia Hospital. Together, these two institutions concentrate about two-thirds of the total number of patients in the state. Thus, a total of 246 patients had their records selected for review. However, 52 of them were excluded, because their medical charts were incomplete, with many missing information. The remaining 194 (79%) patients were included in this analysis. Of note, only 15 (6%) patients were in use of three new ARV (DRV/r + RAL + ETV in nine cases, RAL + DRV/r + ENF in six cases).

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Table 2 -
Number of medical prescriptions for new drugs in the study's period.

After six months of therapy with the new drugs 71.1% of patients had HIV-1 RNA plasma viral load below the limit of detection (50 copies/mL), and after 12 months this rate increased to 74.7%. Mean CD4+ cell count at month six was 377 ± 274 cells/mm³(net gain from baseline of 104 cells/m³⁾, raising to 476 ± 282 cells after 12 months (additional gain of 99 cells/mm³, p < 0.001 for both values, compared to baseline). Mean HIV-1 RNA plasma viral load (log₁₀copies/mL) was 4.6 ± 1.3 at baseline, decreased to 1.7 ± 1.2 at six months, and to 1.7 ± 1.2 at 12 months (p < 0.001 for comparison with baseline values for both time-points). Table 3 details laboratory characteristics of patients at diagnosis, at therapy baseline, and 6/12 months after salvage regimen had been introduced.

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Table 3 -
Mean HIV-1 RNA plasma viral load (PVL) and CD4/8 count at baseline, pre-therapy, and 6/12 months post therapy with new drugs.

The main adverse events reported by patients are summarized in Table 4. Of note, gastrointestinal complaints were the most commonly detected problems: nausea or diarrhea was reported by 10.7% of patients. Local pain, the most frequent adverse event related to ENF, was detected in 20/39 (64%) of patients on ENF. Optimal (100%) self-reported adherence rate to new ARV regimen was 71%. Laboratory parameters were similar after six and 12 months, compared to baseline values, except for creatinine (variation from 0.9 to 1.0 after six months and from 1.0 to 1.1 after 12 months, (p < 0.01 for comparison of both time-points with baseline), and for HDL cholesterol, which showed a mean decrease of 4 mg at six and 12 months when compared to baseline values (p = 0.04). No significant variations were observed in liver enzymes, lipids other than HDL cholesterol, hemoglobin or glucose.

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Table 4 -
Frequency of adverse events among patients in use of new antiretroviral drugs.

Forty-seven patients (19%) had their ARV regimens changed, after starting a regimen containing at least one new drug. In 21 cases, switch was motivated by adverse events, but virological failure also contributed to regimen change in 20 patients. The remaining six patients had discontinued therapy for other reasons.

Virological response to ART regimens including new antiretroviral drugs/classes for salvage therapy was very high (72%), as evaluated after six months of therapy. This high response rate even increased (79%) after 12 months of follow-up, demonstrating great virological efficacy in heavily experienced patients. Moreover, the new regimens were well tolerated, and adherence level was high, which certainly contributed to these responses.

Most of the patients received ARV regimens based on the use of RAL and/or DRV/r, a minority being treated with regimens including ETV or ENF. DRV/r plus RAL was the most (58%) used regimen, with/without a third new drug. The main side-effect observed was reaction at the local of ENF injection, followed by gastrointestinal symptoms (nausea/vomiting or diarrhea).

The initial regimens used for salvage therapy were based in only one new, active drug (usually a PI), and resulted in modest outcomes, as it was observed in TORO (ENF), POWER (DRV/r) and RESIST (TPV/r) trials.⁶6 . Eron JJ, Cooper DA, Steigbigel RT, et al. Efficacy and safety of raltegravir for treatment of HIV for 5 years in the BENCHMRK studies: final results of two randomised, placebo- controlled trials. Lancet Infect Dis. 2013;13:587-96. ⁷7 . Reynes J, Arastéh K, Clotet B, et al. TORO: ninety-six-week virologic and immunologic response and safety evaluation of enfuvirtide with an optimized background of antiretrovirals. AIDS Patient Care STDS. 2007;21:533-43. ⁸8 . Arastéh K, Yeni P, Pozniak A, et al. Efficacy and safety of darunavir/ritonavir in treatment- experienced HIV type -1 patients in the POWER 1, 2 and 3 trials at week 96. Antivir Ther. 2009;14:859-64. ^and ⁹9 . Cahn P, Villacian J, Lazzarin A, et al. Ritonavir- boosted tipranavir demonstrates superior efficacy to ritonavir- boosted protease inhibitors in treatment- experienced HIV- infected patients: 24- week results of the RESIST-2 trial. Clin Infect Dis. 2006;43:1347-56. Availability of more recent ARV dramatically changed this scenario. The BENCHMARK trial provided rates of up to 80% success at six months, when at least two new drugs were used.⁶6 . Eron JJ, Cooper DA, Steigbigel RT, et al. Efficacy and safety of raltegravir for treatment of HIV for 5 years in the BENCHMRK studies: final results of two randomised, placebo- controlled trials. Lancet Infect Dis. 2013;13:587-96.Also, there has been a previous trial showing high response rates with DRV/r and ETV, and recent studies showing rates close to 100% in salvage therapy of patients treated with a combination of three new drugs, from different classes.¹⁰10 . Girard PM, Campbell TB, Grinsztejn B, et al. Pooled week 96 results of the phase III DUET-1 and DUET-2 trials of etravirine: further analysis of adverse events and laboratory abnormalities of special interest. HIV Med. 2012;13: 427-35. ¹¹11 . Imaz A, Falcó V, Ribera E. Antiretroviral salvage therapy for multiclass drug-resistant HIV-1-infected patients: from clinical trials to daily clinical practice. AIDS Rev. 2011;13:180-93. ^and ¹²12 . Fagard C, Colin C, Charpentier C, et al. Long -term efficacy and safety of raltegravir, etravirine, and darunavir/ritonavir in treatment- experienced patients: week 96 results from the ANRS 139 TRIO trial. J Acquir Immune Defic Syndr. 2012;59:489-93.

In Brazil, three previous studies evaluated the effectiveness of DRV/r-based salvage regimens for highly experienced patients and found similar results after 48 weeks. Vidal et al. prospectively followed 92 patients who received a DRV/r-based ARV salvage regimen, and reported 83% virological suppression rate.¹³13 . Vidal JE, Song AT, Matos ML, et al. High rate of virologic suppression with darunavir/ritonavir plus optimized background therapy among highly antiretroviral- experienced HIV- infected patients: results of a prospective cohort study in São Paulo, Brazil. Braz J Infect Dis. 2013;17:41-7. Another group published two additional papers, with a similar approach with rates of virological suppression of 73 and 78%.¹⁴14 . Ribeiro KM, Biscione FM, Westin MR, et al. Virologic and immunologic effectiveness of darunavir-based salvage therapy in HIV-1-infected adults in a Brazilian clinical practice setting: results of a multicenter and retrospective cohort study. Braz J Infect Dis. 2014;18:1-7. ^and ¹⁵15 . Biscione FM, Westin MR, Ribeiro KM, et al. Virologic and immunologic effectiveness at 48 weeks of darunavir-ritonavir-based regimens in treatment- experienced persons living with HIV-1 infection in clinical practice: a multicenter Brazilian cohort. J Int Assoc Provid AIDS Care. 2014;13:63-8. All of these studies followed a common strategy (DRV/r-based regiments plus optimized backbone) with very close results to those found in our study.

Currently, the availability of a large number of ARV drugs makes it possible to choose the best regimen for treating experienced patients failing therapy, with a high likelihood of sustainable virological response. In addition, the newer classes have also a very good safety profile, reducing the risks of lower adherence/lower response due to adverse events.¹¹11 . Imaz A, Falcó V, Ribera E. Antiretroviral salvage therapy for multiclass drug-resistant HIV-1-infected patients: from clinical trials to daily clinical practice. AIDS Rev. 2011;13:180-93.

In conclusion, the real life experience here described demonstrates that virological response of heavily pre-treated patients can be as high as that found in clinical trials. The use of newer drugs and classes makes it easier to treat such patients, who present with highly resistant HIV-1 strains, in comparison to the early HAART era. In addition, the favorable safety profile of these drugs ensures a high level of adherence to therapy, with no significant clinical or laboratory abnormalities.

Acknowledgment

This study was supported by a grant from Departamento de DST/AIDS e Hepatites Virais, Ministério da Saúde, Brasil/UNESCO.

References

¹
Pennings PS. HIV drug resistance: problems and perspectives. Infect Dis Rep. 2013;5 Suppl. 1:e5.
²
Fernández- Montero JV, Barreiro P, Soriano V. HIV protease inhibitors: recent clinical trials and recommendations on use. Expert Opin Pharmacother. 2009;10:1615-29.
³
McKinnell JA, Lin HY, Nevin CN, et al. Early virologic suppression with three-class experienced patients: 24- week effectiveness in the darunavir outcomes study. AIDS. 2009;23:1539-46.
⁴
Makinson A, Reynes J. The fusion inhibitor enfuvirtide in recent antiretroviral strategies. Curr Opin HIV AIDS. 2009;4:150-8.
⁵
Gazzola L, Cicconi P, Ripamonti D, et al. Efficacy and safety of darunavir/ritonavir plus etravirine dual regimen in antiretroviral therapy- experienced patients: a multicenter clinical experience. HIV Clin Trials. 2014;15:140-50.
⁶
Eron JJ, Cooper DA, Steigbigel RT, et al. Efficacy and safety of raltegravir for treatment of HIV for 5 years in the BENCHMRK studies: final results of two randomised, placebo- controlled trials. Lancet Infect Dis. 2013;13:587-96.
⁷
Reynes J, Arastéh K, Clotet B, et al. TORO: ninety-six-week virologic and immunologic response and safety evaluation of enfuvirtide with an optimized background of antiretrovirals. AIDS Patient Care STDS. 2007;21:533-43.
⁸
Arastéh K, Yeni P, Pozniak A, et al. Efficacy and safety of darunavir/ritonavir in treatment- experienced HIV type -1 patients in the POWER 1, 2 and 3 trials at week 96. Antivir Ther. 2009;14:859-64.
⁹
Cahn P, Villacian J, Lazzarin A, et al. Ritonavir- boosted tipranavir demonstrates superior efficacy to ritonavir- boosted protease inhibitors in treatment- experienced HIV- infected patients: 24- week results of the RESIST-2 trial. Clin Infect Dis. 2006;43:1347-56.
¹⁰
Girard PM, Campbell TB, Grinsztejn B, et al. Pooled week 96 results of the phase III DUET-1 and DUET-2 trials of etravirine: further analysis of adverse events and laboratory abnormalities of special interest. HIV Med. 2012;13: 427-35.
¹¹
Imaz A, Falcó V, Ribera E. Antiretroviral salvage therapy for multiclass drug-resistant HIV-1-infected patients: from clinical trials to daily clinical practice. AIDS Rev. 2011;13:180-93.
¹²
Fagard C, Colin C, Charpentier C, et al. Long -term efficacy and safety of raltegravir, etravirine, and darunavir/ritonavir in treatment- experienced patients: week 96 results from the ANRS 139 TRIO trial. J Acquir Immune Defic Syndr. 2012;59:489-93.
¹³
Vidal JE, Song AT, Matos ML, et al. High rate of virologic suppression with darunavir/ritonavir plus optimized background therapy among highly antiretroviral- experienced HIV- infected patients: results of a prospective cohort study in São Paulo, Brazil. Braz J Infect Dis. 2013;17:41-7.
¹⁴
Ribeiro KM, Biscione FM, Westin MR, et al. Virologic and immunologic effectiveness of darunavir-based salvage therapy in HIV-1-infected adults in a Brazilian clinical practice setting: results of a multicenter and retrospective cohort study. Braz J Infect Dis. 2014;18:1-7.
¹⁵
Biscione FM, Westin MR, Ribeiro KM, et al. Virologic and immunologic effectiveness at 48 weeks of darunavir-ritonavir-based regimens in treatment- experienced persons living with HIV-1 infection in clinical practice: a multicenter Brazilian cohort. J Int Assoc Provid AIDS Care. 2014;13:63-8.

Publication Dates

Publication in this collection
Sep-Oct 2015

History

Received
11 Feb 2015
Accepted
26 Mar 2015

This is an open-access article distributed under the terms of the Creative Commons Attribution License

[1] ¹
Pennings PS. HIV drug resistance: problems and perspectives. Infect Dis Rep. 2013;5 Suppl. 1:e5.

[2] ²
Fernández- Montero JV, Barreiro P, Soriano V. HIV protease inhibitors: recent clinical trials and recommendations on use. Expert Opin Pharmacother. 2009;10:1615-29.

[3] ³
McKinnell JA, Lin HY, Nevin CN, et al. Early virologic suppression with three-class experienced patients: 24- week effectiveness in the darunavir outcomes study. AIDS. 2009;23:1539-46.

[4] ⁴
Makinson A, Reynes J. The fusion inhibitor enfuvirtide in recent antiretroviral strategies. Curr Opin HIV AIDS. 2009;4:150-8.

[5] ⁵
Gazzola L, Cicconi P, Ripamonti D, et al. Efficacy and safety of darunavir/ritonavir plus etravirine dual regimen in antiretroviral therapy- experienced patients: a multicenter clinical experience. HIV Clin Trials. 2014;15:140-50.

[6] ⁶
Eron JJ, Cooper DA, Steigbigel RT, et al. Efficacy and safety of raltegravir for treatment of HIV for 5 years in the BENCHMRK studies: final results of two randomised, placebo- controlled trials. Lancet Infect Dis. 2013;13:587-96.

[7] ⁷
Reynes J, Arastéh K, Clotet B, et al. TORO: ninety-six-week virologic and immunologic response and safety evaluation of enfuvirtide with an optimized background of antiretrovirals. AIDS Patient Care STDS. 2007;21:533-43.

[8] ⁸
Arastéh K, Yeni P, Pozniak A, et al. Efficacy and safety of darunavir/ritonavir in treatment- experienced HIV type -1 patients in the POWER 1, 2 and 3 trials at week 96. Antivir Ther. 2009;14:859-64.

[9] ⁹
Cahn P, Villacian J, Lazzarin A, et al. Ritonavir- boosted tipranavir demonstrates superior efficacy to ritonavir- boosted protease inhibitors in treatment- experienced HIV- infected patients: 24- week results of the RESIST-2 trial. Clin Infect Dis. 2006;43:1347-56.

[10] ¹⁰
Girard PM, Campbell TB, Grinsztejn B, et al. Pooled week 96 results of the phase III DUET-1 and DUET-2 trials of etravirine: further analysis of adverse events and laboratory abnormalities of special interest. HIV Med. 2012;13: 427-35.

[11] ¹¹
Imaz A, Falcó V, Ribera E. Antiretroviral salvage therapy for multiclass drug-resistant HIV-1-infected patients: from clinical trials to daily clinical practice. AIDS Rev. 2011;13:180-93.

[12] ¹²
Fagard C, Colin C, Charpentier C, et al. Long -term efficacy and safety of raltegravir, etravirine, and darunavir/ritonavir in treatment- experienced patients: week 96 results from the ANRS 139 TRIO trial. J Acquir Immune Defic Syndr. 2012;59:489-93.

[13] ¹³
Vidal JE, Song AT, Matos ML, et al. High rate of virologic suppression with darunavir/ritonavir plus optimized background therapy among highly antiretroviral- experienced HIV- infected patients: results of a prospective cohort study in São Paulo, Brazil. Braz J Infect Dis. 2013;17:41-7.

[14] ¹⁴
Ribeiro KM, Biscione FM, Westin MR, et al. Virologic and immunologic effectiveness of darunavir-based salvage therapy in HIV-1-infected adults in a Brazilian clinical practice setting: results of a multicenter and retrospective cohort study. Braz J Infect Dis. 2014;18:1-7.

[15] ¹⁵
Biscione FM, Westin MR, Ribeiro KM, et al. Virologic and immunologic effectiveness at 48 weeks of darunavir-ritonavir-based regimens in treatment- experienced persons living with HIV-1 infection in clinical practice: a multicenter Brazilian cohort. J Int Assoc Provid AIDS Care. 2014;13:63-8.

	N	%^*
Male gender	90	64.3

Infectious comorbidity	117	47.5
HCV	12	6.9
HBV	12	6.7
HTLV	5	2.8
TB	58	32.6
AIDS defining infection	60	33.9
CMV	9	5.1
HPV	11	6.2
Syphilis	10	5.6

Non-infectious comorbidities
Obesity	6	3.4
Lipoatrophia	21	11.8
Lypodistrophia	35	19.7
Dyslipidemia	12	6.7
Hypertension	22	12.4
Diabetes	14	7.9

Illicit drugs use	20	14.8
Alcohol	55	36.5
Smoking	38	25.2

Drug	Number of prescriptions for each drug
	RAL (%)	DRV/R (%)	ENF (%)	ETV (%)	Total
RAL	143 (51.8)	111 (40.2)	17 (6.1)	5 (1.8)	276 (100)
DRV/r	111 (40.2)	79 (33.3)	06 (2.8)	06 (2.8)	212 (100)
ENF	17 (46.3)	6 (15.4)	16 (41.0)	0	39 (100)
ETV	05 (26.3)	6 (31.6)	0	8 (42.1)	19 (100)

Total	276 (50.5)	212 (38.8)	39 (7.1)	19 (3.5)	546 (100)

	Mean	SD	Minimum	Maximum	Percentiles
					25	Median	75
First evaluation (at diagnosis)
PLV (log₁₀)	4.73	1.16	1.00	6.99	4.09	4.88	5.56
CD4 (cells/mm³)	276	320	4	2140	56	168	334
CD8 (cells/mm³)	966.9	587.6	51	2556	458	854	1345

Evaluation before introduction of new drugs
PVL (log₁₀)	3.67	1.65	1.00	6.00	2.41	4.30	4.93
CD4 (cells/mm³)	377	274	2	1300	101	242	429
CD8 (cells/mm³)	938.8	599.2	108	2839	514	784	1234

Evaluation after 6 months under new drugs regimen
PVL (log₁₀)	1.73	1.31	1.00	5.64	1.00	1.00	1.99
CD4 (cells/mm³)	394.2	247.7	19	1270	212	338	530
CD8 (cells/mm³)	1145.8	590.4	72	3018	761	1065	1375

Evaluation after 12 months under new drugs regimen
PVL (log₁₀)	1.81	1.44	1.00	5.29	1.00	1.00	2.54
CD4 (cells/mm³)	448.0	272.9	2	1592	295	398	569
CD8 (cells/mm³)	1263.6	601.0	133	2958	782	1182	1777

Adverse events (>3%)	N	%
Nausea/vomiting	13	10.7
Diarrhea	13	10.7
Local pain	25	20.3
Headache	10	8.2
Astenia	4	3.3
Myalgia	6	4.9
Dizziness	6	4.9
Sleep changes	4	3.3
Other	45	23.2
Optimal adherence (self-report)	63	71.6