The development of drug resistance mutations K103N Y181C and G190A in long term Nevirapine-containing antiviral therapy

Antiretroviral therapy (ART) in China started in 2003 [1], at the end of 2011, over 350,000 HIV-infected patients were receiving ART [2]. Chinese national treatment guidelines for ART is: (1) CD4 cell count, 350/mm³ (increased from 200/mm³ in 2008); (2) total lymphocyte count, 1,200/mm³; or (3) World Health Organization (WHO) stage III or IV disease [3]. The first-line regimen included two kinds of Nucleoside Reverse Transcriptase Inhibitors (NRTI) and one kind of Non-Nucleoside Reverse Transcriptase Inhibitor (NNRTI) [4]. Because of very limited antiretroviral drug formulations and lack of adequate laboratory monitoring of ART patients, most patients who initiated ART during the early phase of the free ART program had to stay on the same regimen for a long period of time (maximum for 112 months in my research). For this fact, the research on the development of drug resistance mutations in long-term ART became more and more necessary.

NNRTIs is a crucial component of Chinese ART, it exhibit a longer plasma half-life and a longer duration of detectable levels than nucleoside analog reverse transcriptase inhibitors (NRTIs) [5]. Nevirapine (NVP) is an acceptable first-line NNRTI for HIV-1-infected patients [6] and is known as the most common NNRTI used in the ART regimens of China. In our research, all patients took NVP as NNRTI in their regimens, and were never been stopped and changed.

NVP is a potent NNRTI to fight against HIV, but it has two drawbacks: one, it could cause allergic reactions in approximately 5-14% of users worldwide [7‐9], another one is that NVP has a low genetic barrier; a single mutation can lead to a high-level drug resistance against NVP [10, 11]. Among the NNRTI drug mutation, K103N, Y181C and G190A are the most common mutation associated with resistance to NVP [12, 13]. Even in the patients before ART, Low frequencies of K103N and Y181C are significantly associated with an increased risk of virologic failure [14]. In vitro study, K103N, Y181C and G190A could not provide significant fitness reduction to HIV viruses, variant with these mutations had similar viral replication fitness with the wild type variant [15, 16]. In the past, consider the low fitness reduction and high-level resistance of NNRTI associated mutations, researchers seldom paid attention to the NNRTIs resistant profiles resulting from therapy failure, because a single NNRTI treatment failure always means the second NNRTI therapy failure [17, 18], and in countries with rich ART resources, patients with NNRTI drug resistance mutations would switch to new regimen but in China, a country with limited antiretroviral drugs, patients had to took same NNRTI drug for long time, so the understanding of the development of NNRTI associated mutations became very necessary.

In this essay, we retrospectively studied the development of K103N, Y181C and G190A in long-term ART.

This research was based on a cohort study including 204 patients taking first-line ART therapy since early stage infection. By the end of 2012, the median treatment duration was 86.4 months (77.6-98.0 months), including 46 patients received ART for over 100 months (22.5%). In our research, after the ART treatment for over 72 months, 55.5% patients had their viral load suppressed and 78.6% patients kept CD4 counts over 200 cells/ml. It seems that the first-line ART could still possibly be effective after long-term treatment.

Though the first-line ART is potent method to fight against HIV, but the development of drug resistance could make ART less effective [24‐27]. NNRTI associated drug resistance mutations could compromise the success of NNRTI-containing ART [28‐30]. Among these mutations, K103N Y181C and G190A are the most frequent NNRTI associated drug resistance mutations. In a research on nevirapine-experienced individuals, the frequencies of these mutations were 43%, 46% and 26% respectively [31]. Among the three NNRTI associated mutations, K103N is one of the most clinically important NNRTI resistance mutations; it causes 20- to 50-fold resistance to most available NNRTIs [32, 33]. In phenotypic experiments, K103N, Y181C and G190A were defined as the mutations that have almost the same replication fitness with wild type. The rank of fitness among mutant viruses was as follows: wild type (WT) ≥ Y181C ≥ K103N ≥ G190A ≥ V106A ≥ P236L ≥ G190S [34, 35]. Besides the replication fitness, K103N can persist for a long time in naive patients, over 2 years in a present case report [36]. K103N also can be found in blood mononuclear cell (PBMC) DNA, with no K103N observed in plasma [37, 38]. All the previous research indicated that K103N can steadily exist in plasma and PBMC, and quasispecies with K103N could be more possibly to survive in the surrounding with NVP.

In our research, the result was different with that in vitro study. We found that during the long-term ART treatment, the frequency of K103N, Y181C and G190A were not kept steady, the fact is the frequency of quasispecies with K103N decreased, and could even vanish in SGA sequences, while the proportion of Y181C and G190A could increase from 0% to nearly 100%. This result was also identified in a 204-patinets long-term cohort study.

Based on the results, we estimated that among the three strong NNRTI drug resistance mutations, K103N, Y181C and G190A, there may be some competition process in long-term ART. In the initial period of NVP-containing ART, K103N, Y181C and G190A emerged in different rate among quasispecies which K103N and G190A had a higher rate than Y181C [39]. Consider the fact that three mutations have similar replication fitness and the replication fitness which are associated with mutant prevalence in vivo [40‐42]. Mutation emerged late would develop to the proper proportion associated with its replication fitness, while the proportion of mutation emerged earlier would reduced because the late emerged mutation took part of its dominant role. Then these three mutations would finally break the imbalanced and unequal proportion which was established in initial ART period.

The result of cKa/Ks ratio could provide another support for the competition hypothesis. Among the K103N, Y181C and G190A, they were not always positively correlated with each other, but may turn to negative correlation with the time of receiving ART. It indicated that although in vitro study, the three mutations all had high replication rate and less viral fitness reduction than other NNRTI mutations, variants with these mutations were not so strong in vivo when existed in plasma at same time, they were not always favored by variant under ART pressure. Some competition effect among them may change the frequency of these mutations.

Here is a question according to the research of Jiong Wang [42], the reduced fitness for G190A mutants may not explain the increased frequency of G190A variants over time. It is true that G190A alone can reduce viral fitness, but another research of Jiong Wang [23] found that the variant with K101E + G190S replicated better in the presence of NNRTIs than in the absence of drug, it indicate that mutation K101E may have some effect on the mutant of Codon 190 to enhance the viral fitness. In our study, the frequency of K101E had a similar trend with that of G190A in SGA result, and nearly 30% (3/9, 4/16, 7/23, 10/27) K101E emerged with G190A in standard genotyping result. This may partly explain the question that the increasing of G190A frequency in long-term ART.

The further mechanism and detail of the competition process were remaining unclear; we may need next-generation sequencing and other techniques to go deep in this question. At least we believe this changing of NNRTI mutations is crucial in long-term ART treatment, especially for the country with limited antiviral drugs.