Protocol 104

OUTLINE OF PROTOCOL AVEG 104/ACTG PROTOCOL 235

PHASE I SAFETY AND IMMUNOGENICITY TRIAL OF MN RGP12-/HIV-1 VACCINE IN HIV INFECTED, PREGNANT WOMEN [GENENTECH]

Subjects: Pregnant women who are HIV infected but without AIDS-defining illness and with CD4 lymphocyte counts of 400/mm³ or above. In addition, they must have no special obstetrical risks. Their infants, although not directly immunized, will participate in the study during follow-up after delivery. Maternal therapy with zidovudine (ZDV) will not be a contraindication to participation in the trial.

Schema: Control versus 300 µg MN rgp120/HIV-1 vaccine beginning from week 16 through week 24 of gestation with monthly booster injections concluding at end of pregnancy for a total of at most 5 immunizations. Placebo controls will receive an equal number of injections. Mothers and infants are followed through 18 months after the end of pregnancy. Vaccinees were originally given the option of booster immunizations at 3, 6, 9 and 12 months after delivery; the optional immunizations were discontinued on 12/09/94.

Group A (16 volunteers)	300 µg MN rgp120/HIV-1
Group B (8 volunteers)	Placebo control
A total of 26 volunteers were enrolled

ACCRUAL, IMMUNIZATIONS AND FOLLOW-UP COMPLETED

Product Description: CHO cell-derived HIV-1 MN rgp120 in alum [Genentech]

Time Period: First volunteer enrolled on 05/27/93 and the last on 01/04/95; follow-up of approximately 24 months for mothers; infant follow-up extended to approximately 24 months of age for special CTL study.

Clinical Sites: Johns Hopkins University, Saint Louis University, University of Rochester, University of Washington, Vanderbilt University, University of California at San Francisco Pediatric ACTU

AVEG Clinical Coordination: University of Rochester for University of California at San Francisco

Study Chairs: Peter Wright, Vanderbilt University and John Lambert, Johns Hopkins University

INCLUSION CRITERIA

Without clinical criteria for a diagnosis of AIDS (Appendix B), but with proven HIV-1 infection documented by ELISA and one other confirmatory test such as Western Blot or culture. Generalized lymphadenopathy does not preclude entry into the trial.
Proven pregnancy in a woman between the ages of 16 and 40 years of age inclusive, and between the 16th and 24th week of gestation inclusive at the time of the first immunization. Use of ZDV will be prescribed by the attending obstetrician, and women on ZDV may be included in the trial.
History and physical examination compatible with a normal course of pregnancy. No obstetrical high risk factors other than HIV infection identified on screening. The woman must intend to continue the pregnancy to delivery and agree to being followed by the AVEU for the duration of the study.
The mother must be able to provide informed consent. In accordance with Federal regulations the father of the fetus (if available after a reasonable attempt to contact him) must also provide informed consent.
Acceptable entry laboratory parameters defined as:
- Hematocrit >28%
- Platelets >100,000/mm³
- Total WBC >3000 cells/mm³
- Creatinine <1.5 mg/dl
- Baseline CD4 cells >400 cells/mm³
- SGPT <3 times upper limit of normal
NOTE: Baseline CD4 count will be the average of all determinations performed during the preceding month, or a minimum of two determinations one week apart.

EXCLUSION CRITERIA

Known hypersensitivity to a component of the vaccine
Systemic manifestations related to HIV other than HIV-induced lymphadenopathy
HIV p24 >30 pg/ml
Current use of illicit drugs or known chronic alcohol use. Subjects who have used illicit drugs, and are actively participating in a treatment program (such as methadone maintenance) may be included
Evidence of fetal abnormality at screening ultrasound (sonogram)
Evidence of maternal risk factors including insulin dependent diabetes, moderate to severe hypertension, repeated fetal wastage (>3), Rh-sensitization or other blood group alloimmunization, severe renal disease, previous infants with malformations or other factors obstetrically judged to constitute a special risk of spontaneous abortion or premature birth
Intent to breast feed
Subjects may not have received antiretroviral or immunomodulating agent other than ZDV within 90 days of entry into the study or during pregnancy [Treatment with Acyclovir will not be exclusionary]
Evidence of active syphilis in the mother
Positive circulating hepatitis B surface antigen

STUDY GOALS

Primary Objective

To evaluate the safety of the candidate vaccine in asymptomatic, HIV-1 infected pregnant women.

Secondary Objectives

To evaluate the immunogenicity of the candidate vaccine in asymptomatic, HIV-1 infected pregnant women, and the passive acquisition of vaccine-specific antibody in the infant.
To evaluate the effects of the candidate vaccine on course of pregnancy, and outcome in infant. The study is not designed as an efficacy trial. It should establish the feasibility of maternal immunization and allow assessment of the potential benefit of vaccination in a primary or additive role in subsequent efficacy trials.
To evaluate the long term safety (18 months postpartum) of the candidate vaccine in women who received the vaccine during pregnancy.
To evaluate the long term immunogenicity and safety of the candidate vaccine in women given postpartum immunizations.