Mitochondria-targeted peptides prevent on contrast-induced acute kidney injury in the rats with hypercholesterolemia

Duan, Shao‐Bin; Yang, Shikun; Zhou, Qing; Pan, Peng; Zhang, Hui; Liu, Fang; Xu, Xin

doi:10.3109/0886022x.2013.815107

Cited by 21 publications

(19 citation statements)

References 23 publications

(27 reference statements)

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“…In a recent report, both SS-31 and SS-20 significantly reduced oxidative stress and renal injury in rats given diatrizoate. 76 These studies highlight the number of drug-induced toxicities that appear to be mediated by mitochondrial impairment and suggest that SS-31 can significantly protect against such toxicities caused by diverse chemical compounds.…”

Section: Protection Against Herbicide-and Drug-induced Mitochondrial mentioning

confidence: 97%

Serendipity and the Discovery of Novel Compounds That Restore Mitochondrial Plasticity

Szeto

Birk

2014

Clin Pharmacol Ther

156

144

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The mitochondrial electron transport chain (ETC) plays a central role in energy generation in the cell. Mitochondrial dysfunctions diminish adenosine triphosphate (ATP) production and result in insufficient energy to maintain cell function. As energy output declines, the most energetic tissues are preferentially affected. To satisfy cellular energy demands, the mitochondrial ETC needs to be able to elevate its capacity to produce ATP at times of increased metabolic demand or decreased fuel supply. This mitochondrial plasticity is reduced in many age-associated diseases. In this review, we describe the serendipitous discovery of a novel class of compounds that selectively target cardiolipin on the inner mitochondrial membrane to optimize efficiency of the ETC and thereby restore cellular bioenergetics in aging and diverse disease models, without any effect on the normal healthy organism. The first of these compounds, SS-31, is currently in multiple clinical trials.

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Section: Protection Against Herbicide-and Drug-induced Mitochondrial mentioning

confidence: 97%

Serendipity and the Discovery of Novel Compounds That Restore Mitochondrial Plasticity

Szeto

Birk

2014

Clin Pharmacol Ther

156

144

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“…This review will concentrate on the most recent findings and those preclinical studies that have provided the rationale for clinical trials with SS‐31. In addition to studies described in detail below, SS‐31 has been reported to be beneficial for chronic kidney disease, metabolic syndrome, neurodegenerative diseases and drug‐induced mitochondrial toxicity (Petri et al ., ; Mizuguchi et al ., ; Anderson et al ., ; Yang et al ., ; Duan et al ., ; Huang et al ., ; Toyama et al ., ). It should be pointed out that SS‐31 is also referred to as MTP‐131 or Bendavia in the literature.…”

Section: Therapeutic Potential Of Ss‐31 In Age‐associated Diseasesmentioning

confidence: 99%

First‐in‐class cardiolipin‐protective compound as a therapeutic agent to restore mitochondrial bioenergetics

Szeto

2014

British J Pharmacology

427

390

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A decline in energy is common in aging, and the restoration of mitochondrial bioenergetics may offer a common approach for the treatment of numerous age‐associated diseases. Cardiolipin is a unique phospholipid that is exclusively expressed on the inner mitochondrial membrane where it plays an important structural role in cristae formation and the organization of the respiratory complexes into supercomplexes for optimal oxidative phosphorylation. The interaction between cardiolipin and cytochrome c determines whether cytochrome c acts as an electron carrier or peroxidase. Cardiolipin peroxidation and depletion have been reported in a variety of pathological conditions associated with energy deficiency, and cardiolipin has been identified as a target for drug development. This review focuses on the discovery and development of the first cardiolipin‐protective compound as a therapeutic agent. SS‐31 is a member of the Szeto‐Schiller (SS) peptides known to selectively target the inner mitochondrial membrane. SS‐31 binds selectively to cardiolipin via electrostatic and hydrophobic interactions. By interacting with cardiolipin, SS‐31 prevents cardiolipin from converting cytochrome c into a peroxidase while protecting its electron carrying function. As a result, SS‐31 protects the structure of mitochondrial cristae and promotes oxidative phosphorylation. SS‐31 represents a new class of compounds that can recharge the cellular powerhouse and restore bioenergetics. Extensive animal studies have shown that targeting such a fundamental mechanism can benefit highly complex diseases that share a common pathogenesis of bioenergetics failure. This review summarizes the mechanisms of action and therapeutic potential of SS‐31 and provides an update of its clinical development programme. Linked Articles This article is part of a themed issue on Mitochondrial Pharmacology: Energy, Injury & Beyond. To view the other articles in this issue visit http://dx.doi.org/10.1111/bph.2014.171.issue-8

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“…SS-31 pretreatment also serves a protective role against hypoxia-/reoxygenation-induced apoptosis of human renal tubular epithelial cells, partly by suppression of p66Shc (Zhao et al 2013), a gene that encodes for an adaptor protein that regulates oxidative stress and apoptosis. Moreover, intraperitoneal injections of SS-31 in rats alleviate contrast-induced AKI, primarily due to an antioxidant action (Duan et al 2013). …”

Section: Renal Mitochondrial Targetingmentioning

confidence: 99%

The Emerging Role of Mitochondrial Targeting in Kidney Disease

Eirin

Lerman

2016

Handbook of Experimental Pharmacology

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Renal disease affects millions of people worldwide, imposing an enormous financial burden for health-care systems. Recent evidence suggests that mitochondria play an important role in the pathogenesis of different forms of renal disease, including genetic defects, acute kidney injury, chronic kidney disease, aging, renal tumors, and transplant nephropathy. Renal mitochondrial abnormalities and dysfunction affect several cellular pathways, leading to increased oxidative stress, apoptosis, microvascular loss, and fibrosis, all of which compromise renal function. Over recent years, compounds that specifically target mitochondria have emerged as promising therapeutic options for patients with renal disease. Although the most compelling evidence is based on preclinical studies, several compounds are currently being tested in clinical trials. This chapter provides an overview of the involvement of mitochondrial dysfunction in renal disease and summarizes the current knowledge on mitochondria-targeted strategies to attenuate renal disease.

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Mitochondria-targeted peptides prevent on contrast-induced acute kidney injury in the rats with hypercholesterolemia

Cited by 21 publications

References 23 publications

Serendipity and the Discovery of Novel Compounds That Restore Mitochondrial Plasticity

Serendipity and the Discovery of Novel Compounds That Restore Mitochondrial Plasticity

First‐in‐class cardiolipin‐protective compound as a therapeutic agent to restore mitochondrial bioenergetics

The Emerging Role of Mitochondrial Targeting in Kidney Disease

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