2018
DOI: 10.1093/jac/dkx511
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Phenotypic analysis of HIV-1 E157Q integrase polymorphism and impact on virological outcome in patients initiating an integrase inhibitor-based regimen

Abstract: Assessment of virological response in 39 patients initiating an INI-based regimen with E157Q-mutated virus, in combination with phenotypic analysis, suggests that particular attention should be paid to antiretroviral-naive patients and dolutegravir should be preferentially used in these patients.

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Cited by 40 publications
(25 citation statements)
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“…Similarly, although L74M and E157Q individually have minimal effect on the susceptibility to INSTIs, a combination of L74M and E157Q with other INSTIs RAMs result in reduced susceptibility to INSTIs. In fact, patients harboring viruses with L74M [61] or E157Q [64] mutations in addition to other integrase RAMs showed reduced susceptibility to DTG.…”
Section: Discussionmentioning
confidence: 99%
See 1 more Smart Citation
“…Similarly, although L74M and E157Q individually have minimal effect on the susceptibility to INSTIs, a combination of L74M and E157Q with other INSTIs RAMs result in reduced susceptibility to INSTIs. In fact, patients harboring viruses with L74M [61] or E157Q [64] mutations in addition to other integrase RAMs showed reduced susceptibility to DTG.…”
Section: Discussionmentioning
confidence: 99%
“…In summary, the current study of integrase and nef viral sequences from 345 HIV-infected Cameroonians showed only 2 subjects with INSTIs major RAMs, but several subjects with INSTIs accessory RAMs and polymorphic mutations, including 10 subjects harboring viruses that simultaneously had two different INSTIs accessory RAMs. Individually, INSTIs accessory RAMs do not have major effects on susceptibility to INSTIs, but the simultaneous presence of several accessory mutations or their presence in combination with other mutations has been associated with reduced susceptibility to INSTIs, increased viral fitness and virologic failure [40,[60][61][62][63][64][65]. With the current worldwide push to expand the use of DTG/INSTIs-based ART, it is inevitable that some patients on these regimens could experience virologic failure at some point during the course of their treatment.…”
Section: Discussionmentioning
confidence: 99%
“…Integrase E157Q substitution has been described as a polymorphism present in 2.4% of viral sequences obtained from cART-naïve patients in the ARCA Italian database and in 5.0% in the last French transmitted drug resistance survey study [ 3 , 24 ]. A recent study of the French ANRS AC11 virology network conducted on 8528 integrase sequences from INI-naïve patients showed that the overall prevalence of E157Q polymorphism was 2.7% and its distribution among HIV-1 subtypes was 1.7%, 5.6% and 2.2% in B, CRF02_AG and others non-B subtypes, respectively [ 25 ].…”
Section: E157q Integrase Mutationmentioning
confidence: 99%
“…These in vitro phenotypic data are in accordance with the recent findings of the Italian study using similar phenotypic assays [ 3 ]. However, we observed a slight increase of FC to EVG at 1.9 and 2.4 in the presence of E157Q in B and CRF02_AG contexts, respectively [ 25 ]. Thus, E157Q polymorphism does not seem to impact phenotypic susceptibility to RAL or DTG, in contrast a potential low-level resistance, especially in the context of CRF02_AG recombinant, was observed for EVG.…”
Section: E157q Integrase Mutationmentioning
confidence: 99%
“…11 E157Q, which was detected in 3/158 (1.8%) patients in our study, has been reported to have no impact on phenotypic susceptibility to dolutegravir when expressed alone. 12 However, when E157Q is expressed in combination with R263K, it has been reported to increase dolutegravir resistance mediated by R263K. 13 The importance of naturally occurring polymorphisms at codons 97 and 157 in the subsequent development of resistance to dolutegravir in Tanzanian settings should therefore be investigated with strategic longitudinal studies.…”
mentioning
confidence: 99%