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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00000672
Other study ID # ACTG 118
Secondary ID 070V1AI454-007
Status Completed
Phase Phase 2
First received November 2, 1999
Last updated March 11, 2011

Study information

Verified date October 1994
Source National Institute of Allergy and Infectious Diseases (NIAID)
Contact n/a
Is FDA regulated No
Health authority United States: Federal Government
Study type Interventional

Clinical Trial Summary

AMENDED: 8/29/90 Inclusion of asymptomatic patients with CD4 counts less than 200 cells/mm3. Standardization of baseline evaluation schedule to allow 14 days prior to study dosing. Reduction in frequency and intensity of follow-up evaluations. Standardization of study endpoints. Inclusion of toxicity scoring and management for amylase and triglyceride elevations. Clarification of concomitant medication use. Original design: To determine the effectiveness of didanosine (ddI) in patients with AIDS or advanced AIDS related complex (ARC) who have documented hematologic intolerance to zidovudine (AZT) therapy. To determine if the efficacy of ddI increases with increasing doses.

AZT is effective in reducing mortality in patients with AIDS who receive the drug after the first episode of Pneumocystis carinii pneumonia (PCP) and in patients with advanced ARC. However, AZT therapy has been associated with significant toxicities. In addition, the effectiveness of AZT appears to decrease during the second and third years of therapy. For these reasons, the development of alternative therapy that would be at least as effective but less toxic is of great importance. The drug ddI is an antiviral agent that inhibits replication (reproduction) of HIV with less apparent toxicity than AZT. The major dose-limiting toxicities found in the Phase I studies have been pains in the feet and legs of 2 patients initially receiving 12 mg/kg/day and 12 patients receiving daily doses of 25.8 to 51.2 mg/kg; symptoms began 8 to 27 weeks after initiating ddI treatment. These neuropathy-like symptoms have generally not been associated with significant abnormalities in nerve conduction studies and patients have reported marked improvement in symptoms within 1 to 2 weeks of discontinuing ddI. Some patients have resumed ddI treatment at a reduced dose after resolution of their symptoms. Studies indicate that ddI remains active in the body for at least 12 hours. This indicates that benefits of ddI might be achieved with a low frequency of drug administration.


Description:

AZT is effective in reducing mortality in patients with AIDS who receive the drug after the first episode of Pneumocystis carinii pneumonia (PCP) and in patients with advanced ARC. However, AZT therapy has been associated with significant toxicities. In addition, the effectiveness of AZT appears to decrease during the second and third years of therapy. For these reasons, the development of alternative therapy that would be at least as effective but less toxic is of great importance. The drug ddI is an antiviral agent that inhibits replication (reproduction) of HIV with less apparent toxicity than AZT. The major dose-limiting toxicities found in the Phase I studies have been pains in the feet and legs of 2 patients initially receiving 12 mg/kg/day and 12 patients receiving daily doses of 25.8 to 51.2 mg/kg; symptoms began 8 to 27 weeks after initiating ddI treatment. These neuropathy-like symptoms have generally not been associated with significant abnormalities in nerve conduction studies and patients have reported marked improvement in symptoms within 1 to 2 weeks of discontinuing ddI. Some patients have resumed ddI treatment at a reduced dose after resolution of their symptoms. Studies indicate that ddI remains active in the body for at least 12 hours. This indicates that benefits of ddI might be achieved with a low frequency of drug administration.

Patients are randomized to one of three ddI treatment groups; within each group, doses will be adjusted according to patient's weight at study entry. Stratification is by diagnosis of AIDS or AIDS related complex (ARC) and Medical Center. Data will be tabulated for the Data and Safety Monitoring Board at 3 month intervals.


Recruitment information / eligibility

Status Completed
Enrollment 660
Est. completion date
Est. primary completion date February 1993
Accepts healthy volunteers No
Gender Both
Age group 12 Years and older
Eligibility Inclusion Criteria

Concurrent Medication:

Required:

- Aerosolized pentamidine (300 mg every 4 weeks). In the event of physiological intolerance, alternative PCP prophylaxis may be trimethoprim/sulfamethoxazole 1 DS tab per day or dapsone 50 - 100 mg per day.

Allowed:

- Chronic suppressive treatment for toxoplasmosis, Pneumocystis carinii pneumonia (PCP), cryptococcal meningitis, herpes simplex virus, cytomegalovirus, coccidioidomycosis, and histoplasmosis (absorption of ketoconazole or dapsone may be inhibited if given at the same time as the buffered solution of ddI, and should be taken 2 hours before or 2 hours after taking ddI; oral acidifying agents are not allowed). Isoniazid is permitted only if no acceptable alternative therapy is available. Metronidazole may be used for single courses not to exceed 14 days within consecutive 90 day intervals, the first of which begins at the initiation of the study. Erythropoietin for patients under the relevant treatment IND. Intravenous acyclovir for short courses of therapy.

Patients must:

- Have documented hematologic intolerance to zidovudine (AZT).

- Have the diagnosis of AIDS or advanced AIDS related complex (ARC).

- Have ended treatment for acute Pneumocystis carinii pneumonia (PCP) at least 2 weeks before study entry.

Have previous intolerance on at least two courses of AZT therapy (one of which must have been at daily doses of 500 mg of AZT or less).

- Be able to provide informed consent (and/or guardian as appropriate).

- Be available for follow-up for at least 6 months.

- Have baseline laboratory values as measured within 7 days before initial drug dosing.

- Allowed:

- Development of new opportunistic infections during the study - patients remain in the protocol.

Prior Medication:

Required:

- Prior use and intolerance to zidovudine (AZT).

- Allowed:

- Intralesional agents.

Exclusion Criteria

Co-existing Condition:

Patients with the following are excluded:

- Presence of Kaposi's sarcoma (KS) with known or suspected visceral disease or where KS requires chemotherapy.

- Active AIDS defining opportunistic infections not specifically allowed.

- Intractable diarrhea.

- Stage 2 AIDS-dementia complex.

- History of intolerance to aerosolized pentamidine.

- Grade 2 neuropathy, based on the Neuropathy Targeted Symptom Questionnaire, or any moderate abnormality indicative of peripheral neuropathy, particularly impaired sensation of sharp pain, light touch, or vibration in the lower extremities, distal extremity weakness, or distal extremity hyporeflexia.

- Prior history of acute or chronic pancreatitis.

- History of seizures within past 2 years or currently requiring anticonvulsants for control.

- Any other clinical conditions or prior therapy which, in the opinion of the investigator, would make the patient unsuitable for study or unable to comply with the dosing requirements.

Concurrent Medication:

Excluded:

- Isoniazid (INH).

Patients with the following are excluded:

- Active AIDS-defining opportunistic infections not specifically allowed.

- Intractable diarrhea.

- AIDS-dementia complex = or > stage 2.

- History of intolerance to aerosolized pentamidine. Grade 2 neuropathy, based on the Neuropathy Targeted Symptom Questionnaire, or any moderate abnormality indicative of peripheral neuropathy, particularly impaired sensation of sharp pain, light touch, or vibration in the lower extremities, distal extremity weakness, or distal extremity hyporeflexia.

- Prior history of acute or chronic pancreatitis.

- History of seizures within past 2 years or currently requiring anticonvulsants for control.

- Any other clinical conditions or prior therapy which, in the opinion of the investigator, would make the patient unsuitable for study or unable to comply with the dosing requirements.

- Previous participation in any Phase I ddI study.

- Life expectancy < 6 months.

Prior Medication:

Excluded:

- Chronic therapy for cytomegalovirus infection with ganciclovir.

- ddI.

- d4T.

- ddC.

Excluded within 2 weeks of study entry:

- Zidovudine (AZT).

Excluded within 1 month of study entry:

- Therapy with any other antiretroviral drug or investigational agent not specifically allowed, including interferon and immunomodulating drugs.

- Ganciclovir.

- Neurotoxic drugs.

Excluded within 3 months of study entry:

- Ribavirin.

- Cytotoxic anticancer therapy.

Prior Treatment:

Excluded within 2 weeks of study randomization:

- Transfusion.

Active alcohol or drug abuse that is sufficient, in investigator's opinion, to prevent adequate compliance with study therapy.

Study Design

Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
Didanosine


Locations

Country Name City State
Puerto Rico San Juan Veterans Administration Med Ctr San Juan
United States Johns Hopkins Hosp Baltimore Maryland
United States Beth Israel Deaconess - West Campus Boston Massachusetts
United States Beth Israel Deaconess Med Ctr Boston Massachusetts
United States Boston Med Ctr Boston Massachusetts
United States Harvard (Massachusetts Gen Hosp) Boston Massachusetts
United States Bronx Municipal Hosp Ctr/Jacobi Med Ctr Bronx New York
United States Bronx Veterans Administration / Mount Sinai Hosp Bronx New York
United States Jack Weiler Hosp / Bronx Municipal Hosp Bronx New York
United States Montefiore Med Ctr / Bronx Municipal Hosp Bronx New York
United States SUNY / Erie County Med Ctr at Buffalo Buffalo New York
United States Univ of North Carolina Chapel Hill North Carolina
United States Northwestern Univ Med School Chicago Illinois
United States Holmes Hosp / Univ of Cincinnati Med Ctr Cincinnati Ohio
United States Univ Hosp of Cleveland / Case Western Reserve Univ Cleveland Ohio
United States Ohio State Univ Hosp Clinic Columbus Ohio
United States Mountain States Regional Hemophilia Ctr / Univ of Colorado Denver Colorado
United States Univ of Colorado Health Sciences Ctr Denver Colorado
United States Duke Univ Med Ctr Durham North Carolina
United States City Hosp Ctr at Elmhurst / Mount Sinai Hosp Elmhurst New York
United States G E Morey Jr Fort Lauderdale Florida
United States Univ TX Galveston Med Branch Galveston Texas
United States Milton S Hershey Med Ctr Hershey Pennsylvania
United States Edward Hines Veterans Administration Hosp Hines Illinois
United States Hermann Hosp / Univ Texas Health Science Ctr Houston Texas
United States Texas Children's Hosp / Baylor Univ Houston Texas
United States Indiana Univ Hosp Indianapolis Indiana
United States Univ of Tennessee / E Tennessee Comprehensive Hemophilia Ctr Knoxville Tennessee
United States Cedars Sinai / UCLA Med Ctr Los Angeles California
United States Harbor - UCLA Med Ctr / UCLA School of Medicine Los Angeles California
United States Los Angeles County - USC Med Ctr Los Angeles California
United States UCLA Med Ctr / Pediatric Los Angeles California
United States Univ of Miami School of Medicine Miami Florida
United States Great Lakes Hemophilia Foundation Milwaukee Wisconsin
United States Univ of Minnesota Minneapolis Minnesota
United States Louisiana Comprehensive Hemophilia Care Ctr New Orleans Louisiana
United States Louisiana State Univ Med Ctr / Tulane Med School New Orleans Louisiana
United States Tulane Univ School of Medicine New Orleans Louisiana
United States Bellevue Hosp / New York Univ Med Ctr New York New York
United States Beth Israel Med Ctr / Peter Krueger Clinic New York New York
United States Mem Sloan - Kettering Cancer Ctr New York New York
United States Mount Sinai Hemophilia Ctr / Mount Sinai Med Ctr New York New York
United States Mount Sinai Med Ctr New York New York
United States Saint Luke's - Roosevelt Hosp Ctr New York New York
United States Nebraska Regional Hemophilia Ctr Omaha Nebraska
United States Palo Alto Veterans Adm Med Ctr / Stanford Univ Palo Alto California
United States Univ of Pennsylvania Philadelphia Pennsylvania
United States Hemophilia Ctr of Western PA / Univ of Pittsburgh Pittsburgh Pennsylvania
United States Univ of Pittsburgh Med School Pittsburgh Pennsylvania
United States Univ of Rochester Medical Center Rochester New York
United States Univ of Utah School of Medicine Salt Lake City Utah
United States Univ of California / San Diego Treatment Ctr San Diego California
United States Univ of Washington Seattle Washington
United States Baystate Med Ctr of Springfield Springfield Massachusetts
United States Stanford Univ School of Medicine Stanford California
United States SUNY - Stony Brook Stony Brook New York
United States Olive View Med Ctr Sylmar California
United States Sepulveda Veterans Adm Med Ctr / Olive View Med Ctr Sylmar California
United States SUNY / State Univ of New York Syracuse New York
United States Univ of South Florida Tampa Florida
United States Harbor UCLA Med Ctr Torrance California
United States George Washington Univ Med Ctr Washington District of Columbia
United States Julio Arroyo West Columbia South Carolina
United States Univ of Kansas School of Medicine Wichita Kansas
United States Bowman Gray School of Medicine / Wake Forest Univ Winston-Salem North Carolina
United States Med Ctr of Central Massachusetts Worcester Massachusetts
United States Univ of Massachusetts Med Ctr Worcester Massachusetts

Sponsors (2)

Lead Sponsor Collaborator
National Institute of Allergy and Infectious Diseases (NIAID) Bristol-Myers Squibb

Countries where clinical trial is conducted

United States,  Puerto Rico, 

References & Publications (10)

Allan JD, DeGruttola V, Cross A, McLaren C, Seidlin M, Pettinelli C. An efficacy study of 2'3'-dideoxyinosine [ddI](BMY-40900) administered orally twice daily to zidovudine intolerant patients with HIV infection (ACTG 118). The AIDS Clinical Trials Group. Int Conf AIDS. 1993 Jun 6-11;9(1):67 (abstract no WS-B24-2)

Bozzette SA, Hays RD, Berry SH, Kanouse DE. A Perceived Health Index for use in persons with advanced HIV disease: derivation, reliability, and validity. Med Care. 1994 Jul;32(7):716-31. — View Citation

Fichtenbaum CJ, Clifford DB, Powderly WG. Risk factors for dideoxynucleoside-induced toxic neuropathy in patients with the human immunodeficiency virus infection. J Acquir Immune Defic Syndr Hum Retrovirol. 1995 Oct 1;10(2):169-74. — View Citation

Fiscus SA, Heggem-Snow A, Troiani L, Wallmark E, Folds JD, Sheff B, van der Horst CM. Transient high titers of HIV-1 in plasma and progression of disease. J Acquir Immune Defic Syndr Hum Retrovirol. 1995 May 1;9(1):51-7. — View Citation

Grieco MH, McKinley GF, Reddy MM. Effect of 2',3',-dideoxyinosine on HIV P24 antigen, beta2-microglobulin, neopterin,SCD8,SCD4,and SIL2R levels in patients with ARC or AIDS. Int Conf AIDS. 1991 Jun 16-21;7(2):199 (abstract no WB2069)

Kozal MJ, Kroodsma K, Winters MA, Shafer RW, Efron B, Katzenstein DA, Merigan TC. Didanosine resistance in HIV-infected patients switched from zidovudine to didanosine monotherapy. Ann Intern Med. 1994 Aug 15;121(4):263-8. — View Citation

Reddy MM, Winger EE, Hargrove D, McHugh T, McKinley GF, Grieco MH. An improved method for monitoring efficacy of anti-retroviral therapy in HIV-infected individuals: a highly sensitive HIV p24 antigen assay. J Clin Lab Anal. 1992;6(3):125-9. — View Citation

Sharma PL, Chatis PA, Dogon AL, Mayers DL, McCutchan FE, Page C, Crumpacker CS. AZT-related mutation Lys70Arg in reverse transcriptase of human immunodeficiency virus type 1 confers decrease in susceptibility to ddATP in in vitro RT inhibition assay. Virology. 1996 Sep 15;223(2):365-9. Erratum in: Virology 1996 Nov 15;225(2):428. — View Citation

Spino C, Kahn JO, Dolin R, Phair JP. Predictors of survival in HIV-infected persons with 50 or fewer CD4 cells/mm3. J Acquir Immune Defic Syndr Hum Retrovirol. 1997 Aug 15;15(5):346-55. — View Citation

Winger EE, Reddy MM, Hargrove D, McHugh T, McKinley GF, Grieco MH. A sensitive method for monitoring efficacy of anti-retroviral therapy in HIV-infected individuals: a highly sensitive p24 antigen assay. Int Conf AIDS. 1991 Jun 16-21;7(1):31 (abstract no MB38)

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