HIV Infections Clinical Trial
To conduct a multicenter epidemiologic study of the human retroviruses HIV-1, HIV-2, HTLV-I, and HTLV-II in volunteer blood donors from areas of the United States that were reportedly at high and medium or low risk for HIV. Also, to determine the prevalence of retrovirus seropositivity in first time blood donors; and the rate of retrovirus seroconversion in repeat blood donors as a measure of incidence of infection; to ascertain risk factors for antibody-positive donors; to characterize the blood donor population by geographic location, age, sex, race/ethnicity, and donation history to permit analysis on prevalence, incidence, and risk factors; to identify recipients of retrovirus-positive blood units and conduct clinical and laboratory follow-up of these recipients; and to establish a blood specimen repository for long-term storage of specimens from study donors and recipients for future testing.
BACKGROUND:
HIV is known to be transmissible by blood, blood components, or plasma derivatives. The risk
of contracting HIV infection from blood transfusion has been greatly reduced in the United
States by implementing stringent criteria for donor acceptance, HIV antibody screening, and
new methods of virus inactivation in coagulation factor concentrates. There are additional
human retroviruses, however, that may pose a threat to the safety of the nation's blood
supply.
The human T-cell lymphotropic retroviruses share many properties, including a preferred
tropism for certain lymphocytes and similar modes of transmission. They also differ
significantly from each other and on this basis are divided into two distinct groups: the
human T-cell lymphocytropic viruses (HTLVs) and the human immunodeficiency viruses (HIVs).
HTLV-I, a transforming virus, is the prototype of the first group (HTLVs). It is associated
with adult T-cell leukemia (ATL) and is thought to be involved in a central nervous system
disorder referred to as tropical spastic paraparesis. This group also includes HTLV-II,
which is associated with a T-cell malignancy different from ATL. A newly isolated human
retrovirus, termed HTLV-V, may be the etiologic agent of cutaneous T-cell lymphoma/leukemia,
and may also be added to this group. HIV, previously known as HTLV-III or lymphadenopathy
virus (LAV), a nontransforming virus, causes acquired immunodeficiency syndrome (AIDS) and
is the prototype of the second group (HIVs). New members of this group of nontransforming
human retroviruses were isolated from individuals in different countries of Africa. LAV-2,
also referred to as HIV-2, was isolated from two AIDS patients in Africa, and the first case
of AIDS in the United States caused by HIV-2 was reported in January, 1988. A third member
of this group, HIV-3, was detected in Africa.
Although the HTLV family of retroviruses is distinct from the HIV family, both groups of
viruses infect human T4 (CD4) lymphocytes preferentially and alter the host's T-cell
functions. Whereas HTLV-I or HTLV-II primarily induce transformation and proliferation of T
Lymphocytes and cause T-cell lymphoma/leukemia in humans, HIV and HIV-2 induce T-cell
cytopathology that leads to depletion of CD4 cells.
The spread of HIV by blood transfusion represents a highly efficient mode of transmission.
Blood components from donors with antibody to HIV have been shown to transmit the virus with
frequencies of greater than 90 percent. Packed red blood cells, platelets, or fresh frozen
plasma are all equally effective in transmitting the virus to recipients. It is highly
likely, therefore, that recipients who receive blood from donors with antibody to HIV will
themselves become infected with the virus. Fortunately, the likelihood of such an occurrence
in the United States is now rare due to the implementation of screening procedures and other
safeguards. When the study was initiated in 1989, there was a growing concern, however, that
human retroviruses other than HIV might threaten the safety of the United States blood
supply.
DESIGN NARRATIVE:
Blood donors were asked to participate in this multicenter study. Seropositive donors were
notified of test results, counseled, and invited to join the follow-up study. Data collected
during the first interview included such items as possible exposures to persons with
retroviral infection, sexual preferences and contacts, marital history, intravenous drug
use, occupation, travel, knowledge of AIDS and routes of HIV transmission. At subsequent
visits a blood specimen was collected for laboratory testing and an assessment made of
changes in behavior to reduce the risk of virus transmission.
To calculate incidence and prevalence rates, each center identified the appropriate study
population for analysis purposes in collaboration with the coordinating center. For
prevalence calculations, the study population consisted of donors at all centers who
indicated that they had never donated blood previously. To calculate incidence, the study
population consisted of donors who had donated previously in the same center. The incidence
of retroviral infections was assessed annually in years three through five. Clinical
follow-up of all subjects concluded 48 months after the beginning of enrollment. A blood
profile for each center was required to calculate denominator values for incidence and
prevalence determinations. The blood profile, or donor demographic characterization
consisted of information regarding total donor volume with respect to donation status; new
or repeat donor, and if repeat, the time of last donation; age; sex; and race.
An adjunct to the study was the development of repositories of plasma and cell samples from
infected donors and negative controls collected at the same time. A potential byproduct of
these repositories will be the ability in future years to retrospectively search the REDS
frozen repository file for new retroviruses which may appear in the United States
population.
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