ANRS 12372 MODERATO Study

Study Description

Brief Summary

MODERATO is a phase III, open-label, randomized, multicenter, non-inferiority trial conducted in West and Central Africa (Cameroon, Côte d'Ivoire, Burkina Faso).

HIV-1 infected adults receiving first line ART with TDF+XTC+EFV virologically suppressed will be recruited and followed during 100 weeks.

The objective is to assess the non-inferiority of a strategy consisting of switching to a dual maintenance therapy (DTG+ 3TC or ATV/r+3TC), comparing to WHO standard first line regimen (TDF+3TC+EFV), in terms of virological success at 96 weeks

Detailed Description

In HIV-1 infected adults receiving first line ART with TDF+XTC+EFV virologically suppressed (viral load < detection limit of the technique used) for at least two years: to assess the non-inferiority of a strategy consisting of switching to a dual maintenance therapy (DTG+ 3TC or ATV/r+3TC), comparing to WHO standard first line regimen (TDF+3TC+EFV), in terms of virological success at 96 weeks, in Cameroon, Côte d'Ivoire and Burkina Faso.

This is a trial including two strategies (dual maintenance therapy and triple reference therapy) and three ART regimens (DTG+3TC and ATV/r+3TC used in the maintenance strategy and TDF+3TC+EFV used in the reference strategy).

The primary analysis will compare the two strategies. Secondary analyses will compare the three ART regimens two by two.

In order to make these secondary analyses possible, participants will be randomly assigned, at inclusion, to each of the three ART regimens (arm 1: DTG+3TC; arm 2: ATV/r+3TC; arm 3: TDF+3TC+EFV). The maintenance strategy will include arm 1 and 2. The reference strategy will include arm 3

Number of participants : 600 (200 in each ART regimen, ie 400 in the dual maintenance therapy strategy and 200 in the triple therapy reference strategy)

The primary endpoint is treatment success, as defined by using the FDA snapshot algorithm :

patients who are still continuing the assigned strategy and whose last available plasma HIV-1 RNA in the the window analysis (90 to 102 weeks) is <50 copies/ml at the end of the window analysis (90 to 102 weeks)

Study Design

Outcome Measures

Primary Outcome Measures

1. The treatment success [90 to 102 weeks]

   The proportion of patients who are still continuing the assigned strategy and whose last available plasma HIV-1 RNA in the the window analysis is <50 copies/ml at the end of the window analysis

Secondary Outcome Measures

1. Failure combined endpoint [Between Day 0 and Week 96]

   Percentage of participants who reach the following combined endpoint : "new drug-resistant resistance mutations observed", "decline of at least 20% in creatinine clearance" and "occurrence of at least one grade 3-4 neuropsychiatric disorder"

2. Plasma HIV-1 RNA [Between Day 0 and Week 96]

   Evolution of plasma HIV-1 RNA

3. Virological success [Between Day 0 and Week 96]

   Evolution of the percentage of participants with virological success (VL< 50 copies/Ml)

4. CD4 lymphocyte [Between Day 0 and Week 96]

   Evolution of CD4 lymphocyte absolute count and percentage

5. Virological failure and new resistance mutations [Week 48 and Week 96]

   Percentage of participants with virological failure and new resistance mutations

6. New HIV-1 drug resistance mutations [Week 48 and Week 96]

   Profile of new HIV-1 drug resistance mutations observed in participants with virological failure

7. WHO stage 3-4 morbidity [Between Day 0 and Week 96]

   Incidence of WHO stage 3-4 morbidity ( AIDS events and non AIDS severe morbidity)

8. ANRS grade 3-4 overall morbidity [Between Day 0 and Week 96]

   Incidence of ANRS grade 3-4 overall morbidity (toxicity)

9. ANRS grade 3-4 renal morbidity [Between Day 0 and Week 96]

   Incidence of ANRS grade 3-4 renal morbidity

10. ANRS grade 3-4 neurologic morbidity [Between Day 0 and Week 96]

    Incidence of ANRS grade 3-4 neurologic morbidity

11. ANRS grade 3-4 hepatic morbidity [Between Day 0 and Week 96]

    Incidence of ANRS grade 3-4 hepatic morbidity

12. Creatinine clearance [Between Day 0 and Week 96]

    Evolution of creatinine clearance

13. Grade 1,2,3 or 4 renal disorders [Between Day 0 and Week 96]

    Evolution of the percentage of patients with grade 1,2,3 or 4 renal disorders

14. Grade 1,2,3 or 4 hepatic liver disorders or abnormalities [Between Day 0 and Week 96]

    Evolution of the percentage of patients with grade 1,2,3 or 4 hepatic liver disorders or abnormalities

15. Grade 1,2,3 or 4 CNS disorders [Between Day 0 and Week 96]

    Evolution of the percentage of patients with grade 1,2,3 or 4 CNS disorders

16. Bone mineral density [Between Day 0 and Week 96]

    Evolution of bone mineral density measured using CT bone density scan

17. Adherence to treatment using a self-questionnaire [Between Day 0 and Week 96]

    Evolution of adherence to treatments measured using a self-questionnaire

18. Life quality [Between Day 0 and Week 96]

    Evolution of quality of life measured using the ProQOL questionnaire

19. Symptoms [Between Day 0 and Week 96]

    Evolution of symptoms using the "symptoms experienced" questionnaire

20. ARV drug plasma concentrations in participants with treatment failure [Between Day 0 and Week 96]

    ARV drug plasma concentrations in participants with treatment failure

21. Switched back to triple therapy [Between Day 0 and Week 96]

    Percentage of patients on dual therapy who switched back to triple therapy

22. Cost-effectiveness of the 3 ARV strategies [Week 96]

    Cost-effectiveness of the 3 ARV strategies

Eligibility Criteria

Criteria

Inclusion Criteria:

• HIV-1 infection

• Age of legal majority

• CD4 > 200 cells/mm3 at pre-inclusion

• On stable first-line ART with TDF+XTC+EFV for at least 2 years.

• Absence of past history of virological failure (viral load above the threshold corresponding to the test used); two blips between 50 and 200 copies/ml are allowed.

• At least 2 consecutive HIV-1 RNA < 50 copies/ml within past 2 years, including HIV-1 RNA at pre-inclusion

• Women with pregnancy potential are required to use an effective contraceptive method throughout the study follow up.

• Signed informed consent

Exclusion Criteria:

• HIV-2 infection or HIV-1+2 infection

• CD4 nadir <100 cells/mm3

• Chronic Hepatitis B (HBs Ag positive in the pre-inclusion balance)

• Ongoing active Tuberculosis

• Ongoing severe opportunistic infection

• Ongoing chemotherapy or immunotherapy

• Grade > 2 hemoglobin, neutrophil or platelet disorder

• ALT≥ 3 times the upper limit of normal value

• Creatinine clearance < 50 ml/min (CKD-EPI)

• Allergy to a trial drugs or drug component

• Ongoing pregnancy or Refusal of contraception

• Patient at risk of non-compliance

• Ongoing treatment with a drug that should not be associated with one of the drugs used in the study (cf appendix E page 77)

• Any symptoms or biological findings suggestive of a systemic disorder (renal, hepatic, cardiovascular, pulmonary) or other medical conditions that may interfere with the interpretation of test results or jeopardize the health of patients

Contacts and Locations

Locations

Sponsors and Collaborators

• ANRS, Emerging Infectious Diseases
• Mylan Laboratories

Investigators

• Principal Investigator: Serge P. Eholié, MD, MSc, Pr, Service des Maladies Infectieuses et Tropicales, CHU de Treichville, Abidjan, Côte d'Ivoire
• Principal Investigator: Roland Landman, MD, Institut de Médecine et d'Epidémiologie Appliquée - Hôpital Bichat Claude Bernard, Paris, France
• Study Director: Xavier Anglaret, MD, PhD, Inserm 1219, Université de Bordeaux, France
• Study Chair: Pierre-Marie Girard, MD, PhD, Infectious Diseases Department, University Hospital Saint Antoine, Paris, France

Study Documents (Full-Text)

More Information

Additional Information:

• Sponsor site
• Related Info

Publications