Assessing Drug-Induced Mitochondrial Toxicity in Cardiomyocytes: Implications for Preclinical Cardiac Safety Evaluation

Tang, Xiaoli; Wang, Zengwu; Hu, Shengshou; Zhou, Bingying

doi:10.3390/pharmaceutics14071313

Cited by 14 publications

(13 citation statements)

References 400 publications

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“…In this review, we attempted to emphasize the complexity of mitochondrial effects of the therapeutic armamentarium currently used in cardiovascular diseases as promising prospects for future translational research into safety pharmacology and drug development. The need for the assessment of mitochondrial toxicity by means of modern testing platforms should be included in preclinical safety pharmacology in order to prevent drug attrition during development, and also decrease the risk of side-/off target deleterious effects, has been recently emphasized by a comprehensive review [ 325 ]. While the concept of ”clinical trial in a dish” for drug development is strongly supported by the pharmaceutical industry [ 326 ], it has to be mentioned that it will never be able to appropriately recapitulate the complexity of the clinical situation where both disease and ageing-related neurohormonal activation/impaired signaling occur.…”

Section: Discussionmentioning

confidence: 99%

Mitochondrial Effects of Common Cardiovascular Medications: The Good, the Bad and the Mixed

Bețiu

Noveanu

Hâncu

et al. 2022

IJMS

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Mitochondria are central organelles in the homeostasis of the cardiovascular system via the integration of several physiological processes, such as ATP generation via oxidative phosphorylation, synthesis/exchange of metabolites, calcium sequestration, reactive oxygen species (ROS) production/buffering and control of cellular survival/death. Mitochondrial impairment has been widely recognized as a central pathomechanism of almost all cardiovascular diseases, rendering these organelles important therapeutic targets. Mitochondrial dysfunction has been reported to occur in the setting of drug-induced toxicity in several tissues and organs, including the heart. Members of the drug classes currently used in the therapeutics of cardiovascular pathologies have been reported to both support and undermine mitochondrial function. For the latter case, mitochondrial toxicity is the consequence of drug interference (direct or off-target effects) with mitochondrial respiration/energy conversion, DNA replication, ROS production and detoxification, cell death signaling and mitochondrial dynamics. The present narrative review aims to summarize the beneficial and deleterious mitochondrial effects of common cardiovascular medications as described in various experimental models and identify those for which evidence for both types of effects is available in the literature.

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Section: Discussionmentioning

confidence: 99%

Mitochondrial Effects of Common Cardiovascular Medications: The Good, the Bad and the Mixed

Bețiu

Noveanu

Hâncu

et al. 2022

IJMS

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“…Oncological drugs are reported to cause structural damage to mitochondria, including downregulated ferroptosis, accumulation of lipid peroxides, mitochondrial swelling, cristae disappearance, and matrix cavitation, as found in research with the oncological medicine doxorubicin (DOX) (Tadokoro et al, 2020;Tang et al, 2022). Related to mitochondrial complexes, zoniporide, naproxen, dronedarone, and mubritinib inhibit complex I (Tang et al, 2022). Complex II is compromised by propranolol and atenolol.…”

Section: The Impact Of Modern Life On the Warburg Effect And Mitochon...mentioning

confidence: 99%

“…Modern life puts a real burden on the normal functioning of mitochondria in multiple organs. Factors such as sitting time ( Nogueira Silva Lima et al, 2021 ), high-calorie diet ( Nogueira Silva Lima et al, 2021 ), sleep disturbance ( Saner et al, 2021 ), and alcohol abuse ( Wang et al, 2010 ) and factors that are hardly evitable such as environmental pollution ( Grytting et al, 2022 ), light pollution ( Grytting et al, 2022 ) diesel exhaust and the use of multiple medicines, including NAISDs ( Tang et al, 2022 ), can produce a state of low-grade inflammation (LGI) associated with many chronic diseases ( de Punder and Pruimboom, 2015a ). LGI and mitochondrial dysfunction are two cross-connected mechanisms.…”

Section: Part Ii: Mitochondrial Dysfunction and Its Involvement In Di...mentioning

confidence: 99%

Mitochondria: It is all about energy

et al. 2023

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Mitochondria play a key role in both health and disease. Their function is not limited to energy production but serves multiple mechanisms varying from iron and calcium homeostasis to the production of hormones and neurotransmitters, such as melatonin. They enable and influence communication at all physical levels through interaction with other organelles, the nucleus, and the outside environment. The literature suggests crosstalk mechanisms between mitochondria and circadian clocks, the gut microbiota, and the immune system. They might even be the hub supporting and integrating activity across all these domains. Hence, they might be the (missing) link in both health and disease. Mitochondrial dysfunction is related to metabolic syndrome, neuronal diseases, cancer, cardiovascular and infectious diseases, and inflammatory disorders. In this regard, diseases such as cancer, Alzheimer’s, Parkinson’s, amyotrophic lateral sclerosis (ALS), chronic fatigue syndrome (CFS), and chronic pain are discussed. This review focuses on understanding the mitochondrial mechanisms of action that allow for the maintenance of mitochondrial health and the pathways toward dysregulated mechanisms. Although mitochondria have allowed us to adapt to changes over the course of evolution, in turn, evolution has shaped mitochondria. Each evolution-based intervention influences mitochondria in its own way. The use of physiological stress triggers tolerance to the stressor, achieving adaptability and resistance. This review describes strategies that could recover mitochondrial functioning in multiple diseases, providing a comprehensive, root-cause-focused, integrative approach to recovering health and treating people suffering from chronic diseases.

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“…BCL2 interacting protein 3 (BNIP3) is essential for arsenic trioxide (As 2 O 3 )-induced autophagy in malignant glioma cells [ 84 ]. As 2 O 3 -induced autophagic cell death involves LC3 and mitochondrial membrane rupture but not caspase activation [ 85 ]. As 2 O 3 is a powerful autophagy inducer that appears to need MAPK kinase (MEK)/extracellular signal-regulated kinase (ERK) pathway activation but not MAPK8/JNK or AKT/mTOR [ 86 ].…”

Section: Targeting Autophagy Modulation To Eliminate Environmental Su...mentioning

confidence: 99%

The Emerging Role of Autophagy as a Target of Environmental Pollutants: An Update on Mechanisms

Rahman

Parvez

et al. 2023

Toxics

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Autophagy is an evolutionarily conserved cellular system crucial for cellular homeostasis that protects cells from a broad range of internal and extracellular stresses. Autophagy decreases metabolic load and toxicity by removing damaged cellular components. Environmental contaminants, particularly industrial substances, can influence autophagic flux by enhancing it as a protective response, preventing it, or converting its protective function into a pro-cell death mechanism. Environmental toxic materials are also notorious for their tendency to bioaccumulate and induce pathophysiological vulnerability. Many environmental pollutants have been found to influence stress which increases autophagy. Increasing autophagy was recently shown to improve stress resistance and reduce genetic damage. Moreover, suppressing autophagy or depleting its resources either increases or decreases toxicity, depending on the circumstances. The essential process of selective autophagy is utilized by mammalian cells in order to eliminate particulate matter, nanoparticles, toxic metals, and smoke exposure without inflicting damage on cytosolic components. Moreover, cigarette smoke and aging are the chief causes of chronic obstructive pulmonary disease (COPD)-emphysema; however, the disease’s molecular mechanism is poorly known. Therefore, understanding the impacts of environmental exposure via autophagy offers new approaches for risk assessment, protection, and preventative actions which will counter the harmful effects of environmental contaminants on human and animal health.

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Assessing Drug-Induced Mitochondrial Toxicity in Cardiomyocytes: Implications for Preclinical Cardiac Safety Evaluation

Cited by 14 publications

References 400 publications

Mitochondrial Effects of Common Cardiovascular Medications: The Good, the Bad and the Mixed

Mitochondrial Effects of Common Cardiovascular Medications: The Good, the Bad and the Mixed

Mitochondria: It is all about energy

The Emerging Role of Autophagy as a Target of Environmental Pollutants: An Update on Mechanisms

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