Resistance Database Initiative


HIV Resistance Response Database Initiative is a not-for-profit organisation established in 2002 with the following mission:
To improve the clinical management of HIV infection by developing a large clinical database and bioinformatic techniques that predict accurately any individual's response to any combination of HIV drugs.
The RDI has the following specific goals:
  1. To be an independent repository of HIV resistance and treatment outcome data
  2. To use bioinformatics to explore the relationships between resistance, other clinical and laboratory factors and HIV treatment outcome
  3. To develop and make freely available a system to predict treatment response, as an aid to optimising and individualising the clinical management of HIV infection
The RDI consists of a small executive group based in the UK, an international advisory group of leading HIV/AIDS scientists and clinicians, and an extensive global network of collaborators and data contributors.

Background

is the virus that causes acquired immunodeficiency syndrome, a condition in which the immune system begins to fail, leading to life-threatening opportunistic infections.
There are approximately 25 HIV ‘antiretroviral’ drugs that have been approved for the treatment of HIV infection, from six different classes, based on the point in the HIV life-cycle at which they act.
They are used in combination; typically 3 or more drugs from 2 or more different classes, a form of therapy known as highly active antiretroviral therapy or HAART. The aim of therapy is suppression of the virus to very low, ideally undetectable, levels in the blood this prevents the virus from depleting the immune cells that it preferentially attacks and prevents or delays illness and death.
Despite the expanding availability of these drugs and the impact of their use, treatments continue to fail, often involving to the development of resistance. During drug therapy, low-level virus replication still occurs, particularly when a patient misses a dose. HIV makes errors in copying its genetic material and, if a mutation makes the virus resistant to one or more of the drugs, it may begin to replicate more successfully in the presence of that drug and undermine the effect of the treatment. If this happens then the treatment needs to be changed to re-establish control over the virus.
In well-resourced healthcare settings, when treatment fails a resistance test may be run to predict to which drugs the patient's virus is resistant. The type of test in most common use is the genotype test, which detects mutations in the viral genetic code. This information is then typically interpreted using rules equating individual mutations with resistance against individual drugs. However, there are many different interpretation systems available that do not always agree, the systems only provide categorical results and they do not necessarily relate well to how a patient will respond to a combination of drugs in the clinic.

RDI Overview

The RDI was established in 2002 to pioneer a new approach: to develop computational models using a wide range of laboratory and clinical data collected from thousands of patients treated with HAART all over the world and to use these models to predict how an individual patient will respond to different combinations of drugs.
Key to the success of this approach is the collection of large amounts of data with which to train the models and the use of data from as wide and heterogeneous range of sources as possible to maximise the generalisability of the models’ predictions. In order to achieve this, the RDI set out to involve as many clinics worldwide as possible and to be the single repository for the data required, in an attempt to avoid unnecessary duplication of effort and competition.
As of January 2019, the RDI has collected data from approximately 250,000 patients from dozens of clinics in more than 30 countries. It is probably the largest database of its kind in the world. The data includes demographic information for the patient, and multiple determinations of the amount of virus in the patient's bloodstream, CD4 cells counts, genetic code of the patients virus, and details of the drugs that have been used to treat the patient.
The RDI has used these data to conduct extensive research in order to develop the most accurate system possible for the prediction of treatment response. This research involved the development and comparison of different computational modelling methods including artificial neural networks, support vector machines, random forests and logistical regression.
The predictions of the RDI's models have historically correlated well with the actual changes in virus load of patients in the clinic, typically achieving a correlation co-efficient of 0.7 or more.
Recent models have predicted whether a combination treatment will reduce the level of virus in the patient's bloodstream to undetectable levels with an accuracy of approximately 80%, significantly better than just using a genotype with rules-based interpretation.

HIV-TRePS

In October 2010, following clinical testing in two multinational studies, the RDI made its experimental HIV Treatment Response Prediction System, HIV-TRePS available over the Internet. In January 2011, two clinical studies were published indicating that use of the HIV-TRePS system could lead to clinical and economic benefits. The studies, conducted by expert HIV physicians in the US, Canada and Italy, showed that use of the system was associated with changes of treatment decision to combinations involving fewer drugs overall, which were predicted to result in better virological responses, suggesting that use of the system could potentially improve patient outcomes and reduce the overall number and cost of drugs used.
As clinics in resource-limited settings are often unable to afford genotyping, the RDI has developed models that predict treatment response without the need for a genotype, with only a small loss of accuracy. In July 2011, the RDI made these models available as part of the HIV-TRePS system. This version is aimed particularly at resource-limited settings where genotyping is often not routinely available. The most recent of these models, trained with the largest dataset so far, achieved 80% accuracy, which is comparable to models that use a genotype in their predictions and significantly more accurate than genotyping with rules-based interpretation itself.
HIV-TRePS is now in use in approximately 90 countries as a tool to predict virological response to therapy and avoid treatment failure.
The system has been expanded to enable physicians to include their local drug costs in the modelling. A recent study of data from an Indian cohort demonstrated that the system was able to identify combinations of three locally available drugs with a higher probability of success than the regimen prescribed in the clinic, including those cases where the treatment used in the clinic failed. Moreover, in all these cases some of the alternatives were less costly than the regimen used in the clinic, suggesting that the system could be not only help avoid treatment failure but also reduce costs.

RDI Personnel

RDI Executive

Cohorts: Peter Reiss and Ard van Sighem ; Julio Montaner and Richard Harrigan ; Tobias Rinke de Wit, Raph Hamers and Kim Sigaloff ; Brian Agan, Vincent Marconi and Scott Wegner ; Wataru Sugiura ; Maurizio Zazzi ; Rolf Kaiser and Eugen Schuelter ; Adrian Streinu-Cercel ; Gerardo Alvarez-Uria, Maria-Jesus Perez-Elias,, Tulio de Oliveira,.
Clinics: Jose Gatell and Elisa Lazzari ; Brian Gazzard, Mark Nelson, Anton Pozniak and Sundhiya Mandalia ; Colette Smith ; Lidia Ruiz and Bonaventura Clotet ; Schlomo Staszewski ; Carlo Torti ; H Clifford Lane, Julia A Metcalf and Catherine A Rehm ; Maria-Jesus Perez-Elias ; Stefano Vella and Gabrielle Dettorre ; Andrew Carr, Richard Norris and Karl Hesse ; Dr Emanuel Vlahakis ; Hugo Tempelman and Roos Barth, Robin Wood, Carl Morrow and Dolphina Cogill ; Chris Hoffmann ; Gordana Dragovic ; Ricardo Diaz and Cecilia Sucupira ; Omar Sued and Carina Cesar ; Juan Sierra Madero ; Pachamuthu Balakrishnan and Shanmugam Saravanan.
Clinical trials: Sean Emery and David Cooper ; Carlo Torti ; John Baxter ; Laura Monno and Carlo Torti ; Jose Gatell and Bonventura Clotet ; Gaston Picchio and Marie-Pierre deBethune ; Maria-Jesus Perez-Elias ; Sean Emery, Paul Khabo and Lotty Ledwaba.