Pharmacogenetics of the Late-Onset Efavirenz Neurotoxicity Syndrome (LENS)

Rensburg, R Van; Nightingale, Sam; Brey, Naeem; Albertyn, C; Kellermann, Tracy; Taljaard, Jantjie; Esterhuizen, Tonya; Sinxadi, Phumla; Decloedt, Eric

doi:10.1093/cid/ciab961

Cited by 14 publications

(19 citation statements)

References 23 publications

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“…T/T genotype is associated with higher plasma and CSF concentrations of EFV (Haas et al, 2004;Nightingale et al, 2016), as well as late onset efavirenz neurotoxicity syndrome (van Rensburg et al, 2021). Further, in silico modeling indicates that measurements of EFV in the CSF likely underrepresent the EFV penetration into the brain (Curley et al, 2017).…”

Section: Discussionmentioning

confidence: 99%

“…Up until 2018, EFV was one component of the first line treatment (WHO, 2018), and is still utilized in resource limited settings. EFV is associated with neurological adverse events, such as dizziness, depression, impaired concentration, disordered sleep, and anxiety (Fumaz et al, 2002;Gutierrez et al, 2005;Romao et al, 2011;Ma et al, 2016;Checa et al, 2020;Hakkers et al, 2020;van Rensburg et al, 2021). Higher plasma concentrations of EFV and its primary metabolite, 8-hydroxyefavirenz (8-OHEFV), have been linked to poorer neurocognitive performance and mood changes (Grilo et al, 2016;Hakkers et al, 2020).…”

Section: Introductionmentioning

confidence: 99%

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Biotransformation of Efavirenz and Proteomic Analysis of Cytochrome P450s and UDP-Glucuronosyltransferases in Mouse, Macaque, and Human Brain-Derived In Vitro Systems

2023

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Antiretroviral drugs such as efavirenz (EFV) are essential to combat HIV infection in the brain, but little is known about how these drugs are metabolized locally. In this study, the cytochrome P450 (P450) and UDP-glucuronosyltransferase (UGT)-dependent metabolism of EFV was probed in brain microsomes from mice, cynomolgus macaques, and humans as well as primary neural cells from C57BL/6N mice. Utilizing ultra-high performance liquid chromatography high resolution mass spectrometry (uHPLC-HRMS), the formation of 8-hydroxyefavirenz (8-OHEFV) from EFV and the glucuronidation of P450-dependent metabolites 8-OHEFV and 8,14dihydroxyefavirenz (8,14-diOHEFV) was observed in brain microsomes from all three species.The direct glucuronidation of EFV, however, was only detected in cynomolgus macaque brain microsomes. In primary neural cells treated with EFV, microglia were the only cell type to exhibit metabolism, forming 8-OHEFV only. In cells treated with the P450-dependent metabolites of EFV, glucuronidation was detected only in cortical neurons and astrocytes, revealing that certain aspects of EFV metabolism are cell-type specific. Untargeted and targeted proteomics experiments were used to identify the P450s and UGTs present in brain microsomes. Eleven P450s and 11 UGTs were detected in human brain microsomes, while seven P450s and 14 UGTs were identified in mouse brain microsomes and 15 and four P450s and UGTs, respectively, were observed in macaque brain microsomes. This was the first time many of these enzymes have been noted in brain microsomes at the protein level. This study indicates the potential for brain metabolism to contribute to pharmacological and toxicological outcomes of EFV in the brain.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Biotransformation of Efavirenz and Proteomic Analysis of Cytochrome P450s and UDP-Glucuronosyltransferases in Mouse, Macaque, and Human Brain-Derived In Vitro Systems

2023

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“…In a study using pharmacokinetic simulations, the efavirenz concentrations in brain tissue were found to be higher compared to plasma or CSF concentrations and in a recent study of patients with late-onset efavirenz toxicity, the 8-hydroxy-efavirenz levels were even decreased. 12 , 25…”

Section: Discussionmentioning

confidence: 99%

“… 11 A recent study of 15 patients with late-onset efavirenz toxicity found that all had polymorphisms of CYP2B6 which result in slower metabolism of efavirenz. 12 Isoniazid inhibits the CYP2A6 enzyme, which is an accessory pathway to metabolise efavirenz. Although usually only a small proportion of efavirenz is metabolised via this enzyme, it becomes more important in slow metabolisers.…”

Section: Discussionmentioning

confidence: 99%

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Late-onset efavirenz toxicity: A descriptive study from Pretoria, South Africa

Munsami

Schutte

Villiers

et al. 2023

Southern African Journal of HIV Medicine

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Background: The neuropsychiatric side effects of efavirenz occur mainly early during treatment and are usually mild. A lesser-known and serious complication is late-onset efavirenz toxicity causing ataxia and encephalopathy. Data regarding this condition are limited.Objectives: We describe the clinical picture of late-onset efavirenz toxicity, investigate co-morbidities and report outcomes.Method: This descriptive study of all patients with late-onset efavirenz toxicity was conducted over three years at Kalafong Provincial Tertiary Hospital, Pretoria, South Africa.Results: Forty consecutive patients were identified. Mean age was 42.1 years, three patients (7.5%) were male and the mean efavirenz level was 49.0 µg/mL (standard deviation [s.d.]: 24.8). Cerebellar ataxia (82.5%) and encephalopathy (47.5%) were the most common presenting features (40.0% had both); four patients presented with psychosis. Presence of encephalopathy and/or cerebellar ataxia was associated with higher efavirenz levels compared with psychosis (52.1 µg/mL, s.d.: 24.1 vs 25.0 µg/mL, s.d.: 17.1). In most patients, symptoms resolved, but four patients (10.0%) died, and one patient remained ataxic.Conclusion: Late-onset efavirenz toxicity typically presented with ataxia and encephalopathy, but psychosis can be the presenting feature. The outcome after withdrawal was good, but the mortality of 10.0% is concerning. Recent changes in guidelines favour dolutegravir, but many patients remain on efavirenz, and awareness of the condition is vital.What this study adds: This large, single-centre study contributes to the limited data of HIV-positive patients with late-onset efavirenz toxicity and emphasises its ongoing relevance in clinical practice.

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