Off-Target Effects of Drugs that Disrupt Human Mitochondrial DNA Maintenance

Young, Matthew J.

doi:10.3389/fmolb.2017.00074

Cited by 57 publications

(48 citation statements)

References 132 publications

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“…Another study investigated HIV‐positive patients who developed neuropathy 6‐10 weeks after starting zalcitabine, and this investigation found mitochondrial alterations and significantly reduced mtDNA copy number in nerve biopsy samples (Dalakas, Semino‐Mora, & Leon‐Monzon, ). Additionally, cell culture, animal model, and biochemical studies have demonstrated that mitochondrial toxicity can result from NRTIs blocking the mtDNA replication and repair machinery (Young, ). Recently, Southern blotting served as a powerful tool to characterize and identify the human degradosome, the mitochondrial machinery that quickly degrades mtDNA harboring double‐stranded breaks (Peeva et al., ).…”

Section: Commentarymentioning

confidence: 99%

“…Evidence supports that mitochondria are targeted by environmental toxicants that disrupt mtDNA maintenance, and that chemical exposures can cause an increase or decrease in mtDNA copy number (Meyer et al., ). mtDNA depletion can be a side effect in human immunodeficiency virus (HIV)–infected subjects treated with nucleoside reverse transcriptase inhibitors (NRTIs; Young, ). Mitochondrial toxicity from NRTIs mimics phenotypes of mitochondrial disease, such as mitochondrial myopathy, or other clinical manifestations (Koczor & Lewis, ).…”

Section: Introductionmentioning

confidence: 99%

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Analysis of Human Mitochondrial DNA Content by Southern Blotting and Nonradioactive Probe Hybridization

Wheeler

Young

2019

CP Toxicology

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A single cell can contain several thousand copies of the mitochondrial DNA genome or mtDNA. Tools for assessing mtDNA content are necessary for clinical and toxicological research, as mtDNA depletion is linked to genetic disease and drug toxicity. For instance, mtDNA depletion syndromes are typically fatal childhood disorders that are characterized by severe declines in mtDNA content in affected tissues. Mitochondrial toxicity and mtDNA depletion have also been reported in human immunodeficiency virus–infected patients treated with certain nucleoside reverse transcriptase inhibitors. Further, cell culture studies have demonstrated that exposure to oxidative stress stimulates mtDNA degradation. Here we outline a Southern blot and nonradioactive digoxigenin‐labeled probe hybridization method to estimate mtDNA content in human genomic DNA samples. © 2019 by John Wiley & Sons, Inc.

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Section: Commentarymentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Analysis of Human Mitochondrial DNA Content by Southern Blotting and Nonradioactive Probe Hybridization

Wheeler

Young

2019

CP Toxicology

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“…This hypothesis stems from the evidence that NRTIs inhibit HIV-1 reverse transcriptase as well as eukaryotic pol-γ (the mtDNA replicase that also possesses reverse transcriptase activity) [155]. In the early times of HIV epidemic, NRTIs, including azidothymidine (AZT), didanosine (ddI), and abacavir (ABC) [156-160] were proven to be able to reduce telomerase activity and TL in vitro.…”

Section: Effect Of Art On Telomerase Activity Of T Cellsmentioning

confidence: 99%

Beneficial and Detrimental Effects of Antiretroviral Therapy on HIV-Associated Immunosenescence

Franzese¹,

Barbaccia²,

Bonmassar³

et al. 2018

Chemotherapy

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Since the introduction of highly active antiretroviral therapy more than 2 decades ago, HIV-related deaths have dramatically decreased and HIV infection has become a chronic disease. Due to the inability of antiretroviral drugs to eradicate the virus, treatment of HIV infection requires a systemic lifelong therapy. However, even when successfully treated, HIV patients still show increased incidence of age-associated co-morbidities compared with uninfected individuals. Virus- induced immunosenescence, a process characterized by a progressive decline of immune system function, contributes to the premature ageing observed in HIV patients. Although antiretroviral therapy has significantly improved both the quality and length of patient lives, the life expectancy of treated patients is still shorter compared with that of uninfected individuals. In particular, while antiretroviral therapy can contrast some features of HIV-associated immunosenescence, several anti-HIV agents may themselves contribute to other aspects of immune ageing. Moreover, older HIV patients tend to have a worse immunological response to the antiviral therapy. In this review we will examine the available evidence on the role of antiretroviral therapy in the control of the main features regulating immunosenescence.

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“…121,155 Though at first nucleoside reverse transcriptase inhibitors (NRTIs) were supposed to be genotoxic, mutagenic and oncogenic due to their ability to incorporate into nuclear DNA and directly inhibit cellular DNA polymerases, 114,117,156,157 the subsequent clinical studies have shown no clear correlation between NRTIs and cancer (see above). In fact, in vitro studies have shown, that NRTIs might also possess anticancer activity, [158][159][160] which is probably associated with their capacity to inhibit DNA repair, 161 induce mitochondrial toxicity, 162 apoptosis, modulate activity and expression of endogenous reverse transcriptase encoded by the long interspersed nuclear element-1 (LINE-1). 158 LINE-1 propagation throughout the DNA may play a role in genome instability, mutagenesis and contribute to carcinogenesis.…”

Section: Preclinical Antineoplastic Activity Of Haart Drugsmentioning

confidence: 99%

HIV‐1, HAART and cancer: A complex relationship

Шмакова

Germini

Vassetzky

2019

Intl Journal of Cancer

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HIV infected people are at higher risk of developing cancer, although it is globally diminished in the era of highly active antiretroviral treatment (HAART). Recently, antioncogenic properties of some HAART drugs were discovered. We discuss the role of HAART in the prevention and improvement of treatment outcomes of cancers in HIV‐infected people. We describe different trends in HAART–cancer relationships: cancer‐predisposing as well as cancer‐preventing. We cover the roles of particular drug regimens in cancer prevention. We also describe the causes of cancer treatment with HAART drugs in HIV‐negative people, including ongoing clinical studies that may directly point to a possible independent anti‐oncogenic activity of HAART drugs. We conclude that despite potent antioncogenic activities of every class of HAART drugs reported in preclinical models, the evidence to date indicates that their independent clinical impact in HIV‐infected people is limited. Improved cancer prevention strategies besides HAART are needed to reduce HIV‐cancer‐related mortality.

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Off-Target Effects of Drugs that Disrupt Human Mitochondrial DNA Maintenance

Cited by 57 publications

References 132 publications

Analysis of Human Mitochondrial DNA Content by Southern Blotting and Nonradioactive Probe Hybridization

Analysis of Human Mitochondrial DNA Content by Southern Blotting and Nonradioactive Probe Hybridization

Beneficial and Detrimental Effects of Antiretroviral Therapy on HIV-Associated Immunosenescence

HIV‐1, HAART and cancer: A complex relationship

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