Hiv Clinical Trial
Official title:
Impact of Antiretroviral Treatment and Predictors in Subjects With Extremely Low HIV-1 Reservoir: Optimization of New Cure Strategies
The main purpose of this study is to unravel the mechanisms by which the "Low Viral Reservoir Treated" patients (LoViReT) maintain extremely low HIV-1 DNA levels despite having initiated cART during chronic HIV-1 infection. This group may have specific and different clinical, virological and immunogenetical characteristics, compared to patients with regular reservoir size, which might be useful to design new and more effective treatment approaches.
Combination antiretroviral therapy (cART) is highly successful suppressing HIV-1 replication
and clinical progression in infected patients. However, it does not hamper the establishment
of viral reservoirs, generating latently infected cells that provoke a quick rebound of HIV
viremia after treatment interruption. Different strategies to tackle HIV-1 reservoirs have
been suggested during last years with limited success. Actually, the few cases of described
HIV-1 functional cure are found in elite and post-treatment controllers. Thus, some patients
with regular HIV progression can control replication spontaneously, most of them after
receiving cART during primary HIV-1 infection. Indeed, the "Mississippi baby", who was
treated 36h after birth, had sustained undetectable viremia for 27 months after treatment
interruption. Recently, it has also been proven in successfully treated patients that low
proviral reservoir is related to better HIV-1 control after treatment discontinuation. Thus,
the identification of patients with lower latent reservoir in chronic infection will allow
unveiling potential mechanisms to achieve a functional cure after cART withdrawal.
Our center in Badalona allocates a biological sample collection containing 72,000 specimens
from HIV-1-infected subjects. Samples from 319 patients under suppressive cART for more than
3 years have been screened using the high sensitive BioRad droplet digital Polymerase Chain
Reaction platform (ddPCR). Among the screened patients, a cohort of 20 "Low Viral Reservoir
Treated" patients (LoViReT) with extremely low or undetectable HIV-1 DNA levels in peripheral
blood despite having initiated cART during chronic HIV-1 infection have been established,
which is expected to be increased up to 40 patients. Discovering the factors that reduce HIV
reservoir and make LoViReT patients maintain extremely low levels of proviral HIV-1 DNA will
open new treatment strategies based on maintaining the reservoir to the lowest levels beside
the regular clinical marker of viral load. In addition, a further second step of controlled
cART interruption can be designed to evaluate the real impact of harboring extremely low
levels of latent reservoir for further functional HIV cure.
To unravel the mechanisms by which the LoViReT cohort maintain extremely low HIV-1 DNA levels
despite having initiated cART during chronic HIV-1 infection, this cohort will be studied
from different points of view. All the results will be compared to a control group of 40
individuals with standard levels of total HIV DNA (reservoir). Three mayor aims will be
addressed to then extrapolate our results to larger chronic HIV-1-infected populations:
- To investigate the role of cART on the suppression of the HIV reservoir in the LoViReT
patients, compared to controls. To address this objective, a longitudinal analysis of
proviral HIV DNA for each patient will be performed, including time points previous to
cART. In total, 200 samples will be analyzed and dynamic models will be built for the
two different levels of reservoir establishment. General immune phenotype of cellular
populations, including also activation markers, will be also assessed in all time
points.
- To investigate the integrity of HIV sequences in the LoViReT patients and its
relationship with pathogenesis, in comparison to controls. Genotypic HIV tropism and the
full viral genome will be analyzed through sequencing from DNA of patients' Peripheral
Blood Mononuclear Cells (PBMC). Fresh blood samples will be taken from the 40 LoViReT
and 40 control patients in the study. In addition, for those exerting virus production,
viral isolates will be used to analyze viral replication capacity and cell pathogenesis.
- To investigate the role of immune-genetic factors that along with cART contribute to
reduce the HIV reservoirs in the LoViReT patients. Functional T-cell response will be
measured isolating CD8 T cells and measuring the inhibition capacity for HIV replication
in each patient. Specific HIV-related CD8 T-cell interferon production will be also
evaluated under epitope stimulus. Other progression associated genetic factors as Human
Leukocyte Antigen (HLA) type, and CCR5, CCR2 and SIGLEC-1 Single Nucleotide
Polymorphisms (SNPs) will be also explored.
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