Elesclomol restores mitochondrial function in genetic models of copper deficiency

Soma, Shivatheja; Latimer, Andrew J.; Chun, Haarin; Vicary, Alison C.; Timbalia, Shrishiv A.; Boulet, Aren; Rahn, Jennifer J.; Chan, Sherine S.L.; Leary, Scot C.; Kim, Byung-Eun; Gitlin, Jonathan D.; Gohil, Vishal M.

doi:10.1073/pnas.1806296115

Cited by 67 publications

(64 citation statements)

References 31 publications

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“…For example, the copper ionophore elesclomol is an effective anticancer agent that causes oxidative damage to cancer cells by delivering toxic concentrations of copper to the mitochondria (81). More recently, however, low levels of elesclomol were seen to rescue copper deficiency in mammalian cells (82). We therefore tested whether PZ can also have both toxic and beneficial properties by addressing whether, at very low doses, it can rescue copper Figure 5.…”

Section: Pyrithione Zinc Effects On Secreted Sod5 and On C Albicans mentioning

confidence: 99%

Exploiting the vulnerable active site of a copper-only superoxide dismutase to disrupt fungal pathogenesis

Robinett

Culbertson

Peterson

et al. 2019

Journal of Biological Chemistry

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Edited by F. Peter GuengerichCopper-only superoxide dismutases (SODs) represent a new class of SOD enzymes that are exclusively extracellular and unique to fungi and oomycetes. These SODs are essential for virulence of fungal pathogens in pulmonary and disseminated infections, and we show here an additional role for copper-only SODs in promoting survival of fungal biofilms. The opportunistic fungal pathogen Candida albicans expresses three copperonly SODs, and deletion of one of them, SOD5, eradicated candidal biofilms on venous catheters in a rodent model. Fungal copper-only SODs harbor an irregular active site that, unlike their Cu,Zn-SOD counterparts, contains a copper co-factor unusually open to solvent and lacks zinc for stabilizing copper binding, making fungal copper-only SODs highly vulnerable to metal chelators. We found that unlike mammalian Cu,Zn-SOD1, C. albicans SOD5 indeed rapidly loses its copper to metal chelators such as EDTA, and binding constants for Cu(II) predict that copper-only SOD5 has a much lower affinity for copper than does Cu,Zn-SOD1. We screened compounds with a variety of indications and identified several metal-binding compounds, including the ionophore pyrithione zinc (PZ), that effectively inhibit C. albicans SOD5 but not mammalian Cu,Zn-SOD1. We observed that PZ both acts as an ionophore that promotes uptake of toxic metals and inhibits copper-only SODs. The pros and cons of a vulnerable active site for copper-only SODs and the possible exploitation of this vulnerability in antifungal drug design are discussed.

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Section: Pyrithione Zinc Effects On Secreted Sod5 and On C Albicans mentioning

confidence: 99%

Exploiting the vulnerable active site of a copper-only superoxide dismutase to disrupt fungal pathogenesis

Robinett

Culbertson

Peterson

et al. 2019

Journal of Biological Chemistry

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“…Copper(I) released in the mitochondria can react with molecular oxygen generating ROS, which when produced in excess, can cause unmitigated oxidative stress and apoptotic death of cancer cells [14]. While this mechanism of action is consistent with its anticancer activity, it was recently shown that copper(I) released from elesclomol also becomes available for the metalation of CcO [8]. Consistently, low doses of elesclomol were shown to safely but effectively deliver copper to CcO and restore mitochondrial function in genetic models of copper deficiency [8].…”

Section: Elesclomol As a Copper-transporting Therapeutic Agentmentioning

confidence: 99%

“…This 'Trojan-horse' fashion delivery of metals by other lipophilic carrier molecules, such as the iron-transporting hinokitiol, has shown promise in restoring iron levels in preclinical animal models [7]. Using this principle, Soma et al, performed a targeted screen with a number of copper-binding pharmacological agents for their ability to restore respiratory growth in a yeast mutant defective in copper delivery to cytochrome c oxidase (CcO), a mitochondrial cuproenzyme [8]. This screen identified elesclomol as the most potent copper-transporting molecule, which rescued CcO function in a number of in vitro and in vivo models of copper deficiency [8,9].…”

Section: Rationalementioning

confidence: 99%

Repurposing elesclomol, an investigational drug for the treatment of copper metabolism disorders

Gohil

2020

Expert Opinion on Investigational Drugs

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“…Accordingly, treatment of COA6-deficient patient fibroblasts with CuCl 2 revealed partial rescue of the observed COX levels [ 53 ]. Finally, the anticancer drug elesclomol (ES) was proposed to restore COX function by increasing mitochondrial copper content in patient cells with mutations in the COA6 and SCO2 proteins [ 47 , 55 ].…”

Section: Coa6 Is a Cox Assembly Factormentioning

confidence: 99%

What Role Does COA6 Play in Cytochrome C Oxidase Biogenesis: A Metallochaperone or Thiol Oxidoreductase, or Both?

Maghool

Ryan

Maher

2020

IJMS

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Complex IV (cytochrome c oxidase; COX) is the terminal complex of the mitochondrial electron transport chain. Copper is essential for COX assembly, activity, and stability, and is incorporated into the dinuclear CuA and mononuclear CuB sites. Multiple assembly factors play roles in the biogenesis of these sites within COX and the failure of this intricate process, such as through mutations to these factors, disrupts COX assembly and activity. Various studies over the last ten years have revealed that the assembly factor COA6, a small intermembrane space-located protein with a twin CX9C motif, plays a role in the biogenesis of the CuA site. However, how COA6 and its copper binding properties contribute to the assembly of this site has been a controversial area of research. In this review, we summarize our current understanding of the molecular mechanisms by which COA6 participates in COX biogenesis.

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Elesclomol restores mitochondrial function in genetic models of copper deficiency

Cited by 67 publications

References 31 publications

Exploiting the vulnerable active site of a copper-only superoxide dismutase to disrupt fungal pathogenesis

Exploiting the vulnerable active site of a copper-only superoxide dismutase to disrupt fungal pathogenesis

Repurposing elesclomol, an investigational drug for the treatment of copper metabolism disorders

What Role Does COA6 Play in Cytochrome C Oxidase Biogenesis: A Metallochaperone or Thiol Oxidoreductase, or Both?

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