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A Research Study to See if a Change in Therapy for HIV Infection Can Improve the Immune Response to Treatment

This study has been completed.
Sponsor:
Collaborator:
Abbott
Information provided by:
University of Chicago
ClinicalTrials.gov Identifier:
NCT00145795
First received: September 1, 2005
Last updated: March 21, 2011
Last verified: March 2011
History of Changes
  Purpose

Our goal is to determine if a change in therapy to one containing Kaletra can improve the immune response in patients who have previously been immune partial responders or non-responders. We also are interested in knowing if this agent improves immune response by affecting CD4 + T cell death (apoptosis) or by further inhibiting (preventing) ongoing, low-level, viral replication to levels below detection by current viral load measurements. This will help us understand why immune responses to effective antiretroviral therapy are so different and help determine some possible guidelines for managing patients with poor immune responses.

Hypothesis: Patients with poor immune responses to HAART who receive Kaletra in place of their current PI or NNRTI while continuing their current 2 NRTI backbone will have improved immune response to therapy compared to patients who continue their current regimen.


Condition Intervention Phase
HIV Infections
 Drug: Kaletra + Current Dual NRTI Backbone
Drug: Current Regimen
 Phase 4

Study Type: Interventional
Study Design: Allocation: Randomized
Intervention Model: Crossover Assignment
Masking: Open Label
Primary Purpose: Treatment
Official Title: Randomized Trial of a Switch to a Kaletra + Current Dual NRTI Backbone Versus Continuation of the Current Regimen in Patients With Poor Immune Responses to HAART in Patients With Complete Viral Suppression: A Pilot Study

Resource links provided by NLM:

MedlinePlus related topics: HIV/AIDS
Drug Information available for: Lopinavir
U.S. FDA Resources

Further study details as provided by University of Chicago:

Primary Outcome Measures:
  • Immune reconstitution measured as increase in absolute CD4+ lymphocyte count after 3 and 6 months of therapy [ Time Frame: 3-6 months ] [ Designated as safety issue: No ]

Secondary Outcome Measures:
  • 1.) Rates of ex vivo T cell apoptosis, CD4+, CD8+, both memory and naïve cell populations, 2.) Clinical HIV-related events, and 3.) virologic failure defined as HIV RNA > 2,000 copies/mL [ Time Frame: 3-6 months ] [ Designated as safety issue: No ]

Estimated Enrollment: 40
Study Start Date: April 2004
Study Completion Date: December 2009
Primary Completion Date: June 2009 (Final data collection date for primary outcome measure)
Arms Assigned Interventions
Experimental: 1
Kaletra + Current Dual NRTI Backbone
 Drug: Kaletra + Current Dual NRTI Backbone
study accrual closed
Active Comparator: 2
Current Regimen
 Drug: Current Regimen
study accrual closed

Detailed Description:

To our knowledge our study is the first study showing persistent apoptosis in a subgroup of patients with complete viral suppression in association with poor immune recovery. Immune alterations independent of active viral replication may be responsible. Recent data suggests that immune responses to antiretroviral therapy depend on residual or restored thymic function. Improved CD4+ counts in patients despite virologic treatment failure are associated with greater thymic function, while poor T cell responses despite suppression of HIV are seen with decreased thymic function. Discordant immune responses may also be due to differential effects of particular antiretroviral agents on T cell apoptosis independent of viral suppression. For example, protease inhibitors have been shown to decrease rates of apoptosis of uninfected T cells. Viral replication is never completely suppressed with HAART, even when patients have undetectable plasma HIV RNA. Therefore, varying degrees of low level viral replication or replication in certain cellular compartments may continue to drive T cell apoptosis. Finally, our data suggests that ex vivo rates of PBMC apoptosis could potentially be used predict immune recovery or identify subgroups of patients who may benefit most from changes in HAART or adjunctive immunomodulatory therapies.

At this time, although there are excellent guidelines for how to evaluate and change therapy for patients with virologic failure, there are no recommendation and little data on approaches or strategies to change therapy for patients with poor immune responses. Kaletra (lopinavir/ritonavir) may be of benefit to patients with poor immune responses to HAART despite viral suppression. Kaletra may have greater potency and better suppression of viral replication that is below the level of detection by plasma PCR for HIV-1 RNA. Kaletra also has an excellent pharmacokinetic profile which may result in superior inhibition of T cell apoptosis in vivo.

  Eligibility

Ages Eligible for Study:   18 Years to 75 Years
Genders Eligible for Study:   Both
Accepts Healthy Volunteers:   No
Criteria

Inclusion Criteria:

  • HIV Infection documented CD4+ count within the last 30 days (or drawn with screening labs)
  • Currently on a stable 3-drug HAART regimen including 2 NRTIs for > 6 month VL < 50/mm3 for > 6 months, last within the last 30 days (or drawn with screening labs)
  • Partial immune responder or immune non-responder
  • Age > 18 years
  • Labs (drawn at screening)
  • ALT < 5 X the upper limit of normal (ULN)
  • Total bili < 2 X ULN
  • Creatinine < 2.0 mg/dL

Exclusion Criteria:

  • Prior therapy with Kaletra
  • Known hypersensitivity to Ritonavir
  • Therapy the drugs with potential serious drug interactions: flecainide, propafenone, astemizole, terfenadine, rifampin, dihydroergotamine, ergonovine, ergotamine, metylergonovine, cisapride, pimozide, lovastatin, simvastatin, midazolam, triazolam, and St. John's wart.
  • Pregnancy; breast feeding
  • Current malignancy requiring CT
  • Use of systemic corticosteroids, immunosuppressive, or cytotoxic agents within the last 45 days
  • Fever and/or evidence of an active infectious complication
  • Currently in another interventional clinical trial
  • Receiving IL-2 or any other cytokine or growth factor
  • Enrollment in another interventional clinical trial
  Contacts and Locations
Please refer to this study by its ClinicalTrials.gov identifier: NCT00145795

Locations
United States, Illinois
University of Illinois at Chicago
Chicago, Illinois, United States, 60607
Sponsors and Collaborators
University of Chicago
Abbott
Investigators
Principal Investigator: David Pitrak, MD University of Chicago
  More Information

No publications provided

Responsible Party: David Pitrak, MD, University of Chicago
ClinicalTrials.gov Identifier: NCT00145795     History of Changes
Other Study ID Numbers: 11711B
Study First Received: September 1, 2005
Last Updated: March 21, 2011
Health Authority: United States: Institutional Review Board

Keywords provided by University of Chicago:
HIV
HAART (Highly Active Anti-Retroviral Therapy) partial immune response
no immune response
Treatment Experienced

Additional relevant MeSH terms:
HIV Infections
Acquired Immunodeficiency Syndrome
Lentivirus Infections
Retroviridae Infections
RNA Virus Infections
Virus Diseases
Sexually Transmitted Diseases, Viral
Sexually Transmitted Diseases
Immunologic Deficiency Syndromes
Immune System Diseases
Slow Virus Diseases
 Lopinavir
HIV Protease Inhibitors
Protease Inhibitors
Enzyme Inhibitors
Molecular Mechanisms of Pharmacological Action
Pharmacologic Actions
Anti-HIV Agents
Anti-Retroviral Agents
Antiviral Agents
Anti-Infective Agents
Therapeutic Uses

ClinicalTrials.gov processed this record on May 16, 2013