Inhibition of matrix metalloproteinases by HIV-1 integrase strand transfer inhibitors

Foster, Emma G.; Palermo, Nicholas Y.; Liu, Yutong; Edagwa, Benson; Gendelman, Howard Eliot; Bade, Aditya N.

doi:10.3389/ftox.2023.1113032

Cited by 3 publications

(4 citation statements)

References 81 publications

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“…One of the gene subsets most commonly downregulated across INSTIs were those associated with extracellular matrix interactions and cell motility, including ADAM metallopeptidases, laminins and collagens, and C3 and CXCL12 , classic pro-inflammatory genes with known roles in neural structure and development ( Figures 6A–C, E ). These observations are consistent with a recent report relating integrase inhibitors’ ability to impair matrix metalloproteinase function with the frequent–yet inconclusive–clinical reports of structural defects in the developing CNS when exposed to INSTIs in utero ( Xu et al, 2017 ; Bade et al, 2021 ; Foster et al, 2022 , 2023 ; Zizioli et al, 2023 ). The majority of the significant differentially expressed genes altered by EVG were shared with RAL ( Figure 6D ), and several of the unique RAL genes also involved morphogenesis and TGF-β signaling.…”

Section: Resultssupporting

confidence: 91%

“…MEA experiments indicated that EVG had a greater impact on cell viability than RAL, as previously reported in rodent models (Stern et al, 2018b;Smith et al, 2022). The shared transcriptomic trend of downregulated ECM-associated genes is the first demonstration in neurons of matrix interaction deficits consistent with those INSTIIs induced in myeloid cells, and may be particularly relevant in a developing neuronal model (Bade et al, 2021;Foster et al, 2023). In LPS-treated microglia supernatant experiments, drastic reduction of coordinated firing was consistent with down regulation of AMPA and NMDA receptor genes, which has been previously reported in CNS cells exposed to LPS-induced inflammation (Pellegrini-Giampietro et al, 1994;Zubareva et al, 2020).…”

Section: Discussionsupporting

confidence: 80%

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Human iPSC-derived neurons reveal NMDAR-independent dysfunction following HIV-associated insults

Starr,

Nickoloff-Bybel,

Abedalthaqafi

et al. 2024

Front. Mol. Neurosci.

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The central nervous system encounters a number of challenges following HIV infection, leading to increased risk for a collection of neurocognitive symptoms clinically classified as HIV-associated neurocognitive disorders (HAND). Studies attempting to identify causal mechanisms and potential therapeutic interventions have historically relied on primary rodent neurons, but a number of recent reports take advantage of iPSC-derived neurons in order to study these mechanisms in a readily reproducible, human model. We found that iPSC-derived neurons differentiated via an inducible neurogenin-2 transcription factor were resistant to gross toxicity from a number of HIV-associated insults previously reported to be toxic in rodent models, including HIV-infected myeloid cell supernatants and the integrase inhibitor antiretroviral drug, elvitegravir. Further examination of these cultures revealed robust resistance to NMDA receptor-mediated toxicity. We then performed a comparative analysis of iPSC neurons exposed to integrase inhibitors and activated microglial supernatants to study sub-cytotoxic alterations in micro electrode array (MEA)-measured neuronal activity and gene expression, identifying extracellular matrix interaction/morphogenesis as the most consistently altered pathways across HIV-associated insults. These findings illustrate that HIV-associated insults dysregulate human neuronal activity and organization even in the absence of gross NMDA-mediated neurotoxicity, which has important implications on the effects of these insults in neurodevelopment and on the interpretation of primary vs. iPSC in vitro neuronal studies.

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Section: Resultssupporting

confidence: 91%

Section: Discussionsupporting

confidence: 80%

Human iPSC-derived neurons reveal NMDAR-independent dysfunction following HIV-associated insults

Starr,

Nickoloff-Bybel,

Abedalthaqafi

et al. 2024

Front. Mol. Neurosci.

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“… 37 , 38 Higher homocysteine levels have been reported in people living with HIV, although specific investigations in the context of DTG use are lacking. 35 DTG has also been shown to inhibit matrix metalloproteinases (MMPs), 39 , 40 which play an important role in a wide range of developmental processes including vascular remodelling, angiogenesis, and establishment of the blood–brain barrier. 41 , 42 …”

Section: Discussionmentioning

confidence: 99%

Folate deficiency increases the incidence of dolutegravir-associated foetal defects in a mouse pregnancy model

Mohan,

Nguyen,

MacKenzie

et al. 2023

eBioMedicine

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“…ARVs reduce mother-to-child-transmission of HIV ( Schnoll et al, 2021 ) and drugs that produce synapse loss might have neurodevelopmental consequences ( Foster et al, 2023 ). Umbilical cord-to-maternal plasma concentration ratios for BIC, ETV, and NFV are 1.46, 0.52, and 0.19, respectively ( Mulligan et al, 2016 ; Eke et al, 2019 ; Bukkems et al, 2021 ).…”

Section: Discussionmentioning

confidence: 99%

Antiretroviral drugs from multiple classes induce loss of excitatory synapses between hippocampal neurons in culture

McMullan,

Gansemer,

Thayer

2024

Front. Pharmacol.

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Introduction: Antiretroviral (ARV) drugs have improved prognoses for people living with HIV. However, HIV-associated neurocognitive disorders (HAND) persist despite undetectable viral loads. Some ARVs have been linked to neuropsychiatric effects that may contribute to HAND. Synapse loss correlates with cognitive decline in HAND and synaptic deficits may contribute to the neuropsychiatric effects of ARV drugs.Methods: Using an automated high content assay, rat hippocampal neurons in culture expressing PSD95-eGFP to label glutamatergic synapses and mCherry to fill neuronal structures were imaged before and after treatment with 25 clinically used ARVs.Results and Discussion: At a concentration of 10 μM the protease inhibitors nelfinavir and saquinavir, the non-nucleoside reverse transcriptase inhibitors etravirine and the 8-OH metabolite of efavirenz, the integrase inhibitor bictegravir, and the capsid inhibitor lenacapavir produced synaptic toxicity. Only lenacapavir produced synapse loss at the nanomolar concentrations estimated free in the plasma, although all 4 ARV drugs induced synapse loss at Cmax. Evaluation of combination therapies did not reveal synergistic synaptic toxicity. Synapse loss developed fully by 24 h and persisted for at least 3 days. Bictegravir-induced synapse loss required activation of voltage-gated Ca2+ channels and bictegravir, etravirine, and lenacapavir produced synapse loss by an excitotoxic mechanism. These results indicate that select ARV drugs might contribute to neuropsychiatric effects in combination with drugs that bind serum proteins or in disease states in which synaptic function is altered. The high content imaging assay used here provides an efficient means to evaluate new drugs and drug combinations for potential CNS toxicity.

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Inhibition of matrix metalloproteinases by HIV-1 integrase strand transfer inhibitors

Cited by 3 publications

References 81 publications

Human iPSC-derived neurons reveal NMDAR-independent dysfunction following HIV-associated insults

Human iPSC-derived neurons reveal NMDAR-independent dysfunction following HIV-associated insults

Folate deficiency increases the incidence of dolutegravir-associated foetal defects in a mouse pregnancy model

Antiretroviral drugs from multiple classes induce loss of excitatory synapses between hippocampal neurons in culture

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