Prevalence and patterns of HIV drug resistance in patients with suspected virological failure in North-Western Tanzania

Author:

Henerico Shimba12ORCID,Mikasi Sello Given2,Kalluvya Samuel Elias3,Brauner Jan M.4,Abdul Seif1,Lyimo Eric5,Desderius Bernard13,Korn Klaus6,van Zyl Gert2ORCID,Jacobs Graeme Brendon2,Preiser Wolfgang2ORCID,Kasang Christa78ORCID

Affiliation:

1. Bugando Medical Centre, Mwanza, United Republic of Tanzania

2. Division of Medical Virology, Faculty of Medicine and Health Sciences, Stellenbosch University/National Health Laboratory Service (NHLS) Tygerberg, South Africa

3. Catholic University of Health and Allied Sciences, Bugando Medical Centre, Mwanza, United Republic of Tanzania

4. Department of Computer Science, University of Oxford, Oxford, UK

5. National Institute of Medical Research, Mwanza, United Republic of Tanzania

6. Institute of Clinical and Molecular Virology, University of Erlangen-Nürnberg, Erlangen, Germany

7. German Leprosy and Tuberculosis Relief Association, Wuerzburg, Germany

8. Medical Mission Institute, Wuerzburg, Germany

Abstract

Abstract Background More than 15 million people in sub-Saharan Africa receive ART. Treatment failure is common, but the role of HIV drug resistance in treatment failure is largely unknown because drug resistance testing is not routinely done. This study determined the prevalence and patterns of HIV drug resistance in patients with suspected virological failure. Materials and methods A single high viral load of >1000 viral RNA copies/mL of plasma at any point during ART was considered as suspected virological failure. HIV-1 RNA was extracted from plasma samples of these patients using the QIAamp Viral RNA kit. The protease and part of the RT regions of the HIV pol gene were characterized. Results Viral load was determined in 317 patients; 64 (20.2%) had suspected virological failure. We successfully genotyped 56 samples; 48 (85.7%) had at least one major resistance-associated mutation (RAM). Common mutations in RT were M184V (75%), T215Y (41.1%), K103N (39.3%), M41L (32.1%), D67DN (30.3%), G190A (28.6%) and A98G (26.8%). No RAMs were detected in ART regimens based on a ritonavir-boosted PI. Conclusions The Tanzanian national guidelines define ‘virological failure’ as two consecutive viral load measurement results, at 3 month intervals, above the WHO threshold (1000 copies/mL). Here, we show that a single viral load above the WHO threshold is associated with high rates of RAMs. This suggests that a single high viral load measurement could be used to predict virological failure and avoid delays in switching patients from first-line to higher genetic barrier second-line regimens.

Funder

Georg Ludwig Rexroth Foundation

Publisher

Oxford University Press (OUP)

Subject

Infectious Diseases,Pharmacology (medical),Pharmacology,Microbiology (medical)

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