2000HIVTrained: 2000HIV Trained Innate Immunity in HIV Elite Controllers

Sponsor

Radboud University Medical Center (Other)

Overall Status

Active, not recruiting

CT.gov ID

NCT04968717

Collaborator

Erasmus Medical Center (Other), Onze Lieve Vrouwe Gasthuis (Other), Elisabeth-TweeSteden Ziekenhuis (Other)

109

Enrollment

Locations

Anticipated Duration (Months)

36.3

Patients Per Site

2.3

Patients Per Site Per Month

Study Details

Study Description

Brief Summary

Some individuals are able to spontaneously control HIV replication, the so-called 'elite controllers' (ECs). ECs are crucial for our understanding of HIV infection. While there is more and more evidence pointing towards a role of the innate immune system in elite control, no research has been performed on the role of innate trained immunity in elite control of HIV.

In this cross-sectional case-control study, we will study this role of trained immunity in HIV elite control by comparing ECs both to a non-HIV-infected first-degree relative, and to HIV patients who are not elite controllers. In addition, we will study whether HIV itself can induce a trained innate immunity phenotype.

Condition or Disease	Intervention/Treatment	Phase
HIV-1-infection

Detailed Description

Rationale:

It remains unknown how some individuals spontaneously control HIV in the absence of antiretroviral medication, called HIV 'elite controllers' (ECs). ECs have been absolutely crucial to our current understanding of control of HIV replication. While research has mainly focused on the adaptive immune system, there is a vast amount of evidence indicating that the innate immune system is essential to HIV elite control.

Trained innate immunity can be expressed in terms of enhanced responsiveness of innate immune cells to a repeated trigger. This occurs through epigenetic remodeling after exposure to certain stimuli, such as beta-glucan, lipopolysaccharide (LPS) or the bacillus Calmette-Guérin (BCG) vaccine. Innate training results in an altered gene expression and metabolic reqiring on a cellular level, resulting in greater resistance against subsequent infection.

Both the impact of trained immunity on HIV infections and vice versa, the impact of HIV on trained immunity, are unknown. Our hypothesis is that ECs are natural hyper-responders to innate immune training triggers and that this aids in the HIV elite control phenotype.

Objectives:

(Primary) Investigate if a trained immunity profile in innate immune cells plays a role in HIV elite control.
(Secondary) Determine the immune phenotypes that distinguish family members of HIV elite controllers from family members of people living with HIV who have never been controllers.
(Secondary) Determine whether HIV can induce a long-term functional and transcriptional program in innate immune cells similar to trained immunity.

Study design:

Cross-sectional case-control study.

For the primary objective, HIV elite controllers will be compared to ART-suppressed HIV patients who never have been elite controllers and first-degree relatives of HIV elite controllers will be compared to first-degree relatives of ART-suppressed HIV patients who have never been elite controllers.

For the secondary objectives, first, a system biology approach will be used in the comparison above. To determine the role of HIV in trained innate immunity we will compare people living with HIV (both controllers as non-controllers) to their respective family members.

Study Design

Study Type:

Observational

Actual Enrollment :

109 participants

Observational Model:

Case-Control

Time Perspective:

Cross-Sectional

Official Title:

2000HIV Trained Innate Immunity in HIV Elite Controllers

Actual Study Start Date :

Aug 2, 2021

Actual Primary Completion Date :

Oct 27, 2021

Anticipated Study Completion Date :

Dec 1, 2022

Arms and Interventions

Arm	Intervention/Treatment
HIV elite controllers Non-viremic elite controller: HIV-positive , > 1 year without cART AND with >3 consecutive HIV-RNA < 75 copies/ml spanning >12 months AND stable CD4> 500 cells/uL.(i.e. >75% of measurements) OR on cART, but before start cART > 1 year without cART AND with >3 consecutive HIV-RNA < 75 copies/ml spanning >12 months AND stable CD4> 500 cells/uL. (i.e. >75% of measurements) Viremic elite controller: HIV-positive >5 year without cART AND with always HIV-RNA >50-10.000 copies/ml AND always CD4> 500 cells/uL. OR on cART, but before start cART >5 year without cART AND with always HIV-RNA >50-10.000 copies/ml AND always CD4> 500 cells/uL
First-degree relatives of HIV elite controllers
cART-treated non-controller HIV patients
First-degree relatives of cART-treated non-controller HIV patients

Outcome Measures

Primary Outcome Measures

Direct cytokine responses [24 hour ex vivo experiment]
Isolated monocytes and NK-cells will be stimulated ex vivo with a range of stimuli. Cytokines released in the supernatants will be measured by ELISA.
Cytokine responses after 6-day training [7 day ex vivo experiment]
Isolated monocytes and NK-cells will be trained ex vivo and the innate training effect will be studied after restimulation with an unrelated stimulus on day 7. Cytokines released in the supernatant and intracellularly will be measured by ELISA.
Transcriptome [1 year after sample collection]
RNA in the cells will be analysed to gain a transcriptional signature.
Epigenome [1 year after sample collection]
Epigenetic signatures will be studied by means of ChIP sequencing and ATAC sequencing.
Immune phenotyping [1 year after sample collection]
Circulating cells are phenotyped by menas of elaborate flow cytometry panels.

Other Outcome Measures

Vaccination history [Collected during visit]
All groups
History of contracting COVID19 [Collected during visit]
All groups
Age [Collected during visit]
Only in first-degree relatives. Information on HIV patients already available from 2000HIV study (NCTNCT03994835).
Biological sex [Collected during visit]
Only in first-degree relatives. Information on HIV patients already available from 2000HIV study (NCTNCT03994835).
Medical history [Collected during visit]
Only in first-degree relatives. Information on HIV patients already available from 2000HIV study (NCTNCT03994835).
Medication use [Collected during visit]
Only in first-degree relatives. Information on HIV patients already available from 2000HIV study (NCTNCT03994835).

Eligibility Criteria

Criteria

Ages Eligible for Study:

18 Years and Older

Sexes Eligible for Study:

All

Accepts Healthy Volunteers:

Yes

All participants:

All participants must be ≥18 years of age.
Due to distorting effects on immune parameters and immune responses, participation is either not possible or must be delayed in case of the following:
active hepatitis B/C or signs of acute infections
active or recent malignant condition (i.e. <12 months ago treated)
active systemic auto-immune or auto-inflammatory conditions (such as rheumatoid arthritis, inflammatory bowel disease).
use of immunosuppressive medication
pregnant

HIV elite controllers:

HIV elite controllers in the 2000HIV that have an available first-degree relative. Definition of HIV elite controller is the same as in the 2000HIV, see definition on page 7 of the protocol and in the group description.

ART-suppressed people living with HIV:

As a control group, ART-suppressed people living with HIV in the 2000HIV that have an available first-degree relative will be included.

ART-suppressed people living with HIV need to apply to the following criteria to participate in the 2000HIV: ≥18 years, on cART ≥6 months with an HIV-RNA load <200 copies/mL.

For this 2000HIV-trained study, additional criteria for ART-suppressed people living with

HIV are:

Never applied to controller definition.
At least one documented HIV RNA load >100.000 copies/mL
No documentation of recent HIV acquisition combined with ART initiation in less than 6 months.

Eligible ART-suppressed people living with HIV will be matched by sex and age (max. 5-10 years apart), where possible. Similarity in family members between groups will also be pursued. That is why the HIV elite controllers and their family members will be enrolled first. Thereafter, the ART suppressed people living with HIV and their family members will be recruited and enrolled.

First-degree relatives:

Aside from the criteria for all participants mentioned above, there are no additional criteria for first-degree relatives of participants with HIV. If multiple first-degree relatives are available, siblings are preferred. If no sibling is available, then children

18 years. If no children >18 years, then parents. If there is still multiple options, same-sex will be preferred over different-sex relatives.

Contacts and Locations

Locations

	Site	City	Country	Postal Code
1	OLVG	Amsterdam	Netherlands
2	Radboudumc	Nijmegen	Netherlands	6525GA
3	Erasmus MC	Rotterdam	Netherlands

Sponsors and Collaborators

Radboud University Medical Center
Erasmus Medical Center
Onze Lieve Vrouwe Gasthuis
Elisabeth-TweeSteden Ziekenhuis

Investigators

None specified.

Study Documents (Full-Text)

None provided.

More Information

Publications

None provided.

Responsible Party:

Radboud University Medical Center

ClinicalTrials.gov Identifier:

NCT04968717

Other Study ID Numbers:

NL76999.091.21
2021-7495

First Posted:

Jul 20, 2021

Last Update Posted:

Nov 26, 2021

Last Verified:

Oct 1, 2021

Individual Participant Data (IPD) Sharing Statement:

Undecided

Plan to Share IPD:

Undecided

Studies a U.S. FDA-regulated Drug Product:

Studies a U.S. FDA-regulated Device Product:

Study Results

No Results Posted as of Nov 26, 2021