A brief overview of mechanisms of mitochondrial toxicity from NRTIs

Kohler, James J.; Lewis, William

doi:10.1002/em.20223

Cited by 143 publications

(110 citation statements)

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“…The DNA pol-␥ hypothesis 2 has been developed and refined throughout the years 1,47 to help define events in acquired mtDNA depletion caused by antiretroviral nucleosides for AIDS. 28 Pharmacological and cellular events that relate to abundance of phosphorylated NRTIs and normal mtDNA precursors in the intramitochondrial compartment were considered important initially but now are becoming crucial biological factors in understanding the downstream events in inhibition of DNA pol-␥ and in resultant mtDNA depletion.…”

Section: Discussionmentioning

confidence: 99%

Targeted Transgenic Overexpression of Mitochondrial Thymidine Kinase (TK2) Alters Mitochondrial DNA (mtDNA) and Mitochondrial Polypeptide Abundance

Hosseini

Kohler

Haase

et al. 2007

The American Journal of Pathology

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Mitochondrial toxicity limits nucleoside reverse transcriptase inhibitors (NRTIs) for acquired immune deficiency syndrome. NRTI triphosphates, the active moieties, inhibit human immunodeficiency virus reverse transcriptase and eukaryotic mitochondrial DNA polymerase pol-␥. NRTI phosphorylation seems to correlate with mitochondrial toxicity, but experimental evidence is lacking. Transgenic mice (TGs) with cardiac overexpression of thymidine kinase isoforms (mitochondrial TK2 and cytoplasmic TK1) were used to study NRTI mitochondrial toxicity. Echocardiography and nuclear magnetic resonance imaging defined cardiac performance and structure. TK gene copy and enzyme activity, mitochondrial (mt) DNA and polypeptide abundance, succinate dehydrogenase and cytochrome oxidase histochemistry, and electron microscopy correlated with transgenesis, mitochondrial structure, and biogenesis. Antiretroviral combinations simulated therapy. Untreated hTK1 or TK2 TGs exhibited normal left ventricle mass. In TK2 TGs, cardiac TK2 gene copy doubled, activity increased 300-fold, and mtDNA abundance doubled. Abundance of the 17-kd subunit of complex I, succinate dehydrogenase histochemical activity, and cristae density increased. NRTIs increased left ventricle mass 20% in TK2 TGs. TK activity increased 3 logs in hTK1 TGs, but no cardiac phenotype resulted. NRTIs abrogated functional effects of transgenically increased TK2 activity but had no effect on TK2 mtDNA abundance. Thus, NRTI mitochondrial phosphorylation by TK2 is integral to clinical NRTI mitochondrial toxicity.

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Section: Discussionmentioning

confidence: 99%

Targeted Transgenic Overexpression of Mitochondrial Thymidine Kinase (TK2) Alters Mitochondrial DNA (mtDNA) and Mitochondrial Polypeptide Abundance

Hosseini

Kohler

Haase

et al. 2007

The American Journal of Pathology

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“…[3] The 140 kDa catalytic protein is translated from the 22 exons of the POLG1 gene on chromosome 15q25, and possesses both polymerase and 3´ -5´ exonuclease activities. [4] Primary mutations in the POLG1 gene lead to secondary defects in the maintenance of the mitochondrial genome, depletion of mtDNA, [5,6] damage to oxidative phosphorylation [6] and elevation of serum lactate, [5,7] thus making the POLG1 gene a strong candidate for NRTI-induced mitochondrial-toxicity-related disorders such as hyperlactataemia. Literature reports from developed countries suggest an incidence rate for SHL of 5 -10/1 000 patients per year on NRTIs and 1/1 000 patients per year for the very severe form (LA), which is associated with a high expected mortality.…”

Section: Researchmentioning

confidence: 99%

Mutations of mtDNA polymerase-γ and hyperlactataemia in the HIV-infected Zulu population of South Africa

et al. 2016

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Background. Mitochondrial toxicity, particularly symptomatic hyperlactataemia or lactic acidosis (SHL/LA), has been attributed to the use of nucleoside reverse transcriptase inhibitors (NRTIs), possibly because of their capacity to impede human mitochondrial DNA polymerase-γ (POLG), which is responsible for the replication of mitochondrial DNA. Objective. To determine whether known monogenic POLG1 polymorphisms could be linked with the unexpectedly high incidence of SHL/ LA observed in HIV-infected Zulu-speaking patients exposed to the NRTIs stavudine or zidovudine in their antiretroviral therapy. Methods. One hundred and sixteen patients from Edendale Hospital, Pietermaritzburg, South Africa, participated in the study between March and August 2014. Fifty-nine symptomatic cases were compared with 57 non-symptomatic controls on stavudine for ≥24 months. Among the symptomatic patients, 13 had SHL with measured lactate between 3.0 and 4.99 mmol/L, and 46 had LA with a lactate level ≥5 mmol/L. Genomic DNA from 113 samples was used for subsequent allelic discrimination polymerase chain reaction screening for the R964C and E1143G single-nucleotide polymorphisms of POLG1. Sequencing was performed for 40/113 randomly selected samples for confirmation of the genotyping results. Results. Neither of the two known POLG1 mutations was observed. The cases presented with SHL/LA between 4 and 18 months on stavudine. Females (70.4%) were significantly (p<0.001) more likely to be cases (adjusted odds ratio 24.24, 95% CI 5.14 -114.25) compared with males. Conclusion. This study has shown that our sample of the Zulu-speaking population does not exhibit a genetic predisposition to SHL/LA associated with known monogenic POLG1 mutations, indicating another possible predisposing factor for increased risk of SHL/LA.

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“…The emergence of these strains along with the severe NRTI/NtRTI-associated side effects, including lactic acidosis, lipoatrophy, and peripheral neuropathy, usually necessitates changes in the regimen, which can include switching ARVs, adding more ARVs, and/or adjusting dosing (Kohler and Lewis 2007). Interestingly, individual NRTIs/NtRTIs are associated with specific side effects.…”

Section: Side Effectsmentioning

confidence: 99%

“…For example, d4T, and to a lesser extent, AZT, are associated with lipoatrophy, while TDF does not appear to cause this particular side effect. Peripheral neuropathy, which manifests in approximately 40% patients on cART, is associated with regimens that include d4T (Kohler and Lewis 2007). On the other hand, TDF is associated with increased risk of nephropathy and loss of bone density (Duarte-Rojo and Heathcote 2010).…”

Section: Side Effectsmentioning

confidence: 99%