Mitochondrial Protease ClpP is a Target for the Anticancer Compounds ONC201 and Related Analogues

Graves, Paul R.; Aponte‐Collazo, Lucas J.; Fennell, Emily M.J.; Graves, Adam C.; Hale, Andrew; Dicheva, Nedyalka; Herring, Laura E.; Gilbert, Samuel F.; East, Michael P.; McDonald, Ian M.; Lockett, Matthew R.; Ashamalla, Hani; Moorman, Nathaniel J.; Karanewsky, Donald S.; Iwanowicz, Edwin J.; Holmuhamedov, Ekhson; Graves, Lee M.

doi:10.1021/acschembio.9b00222

Cited by 131 publications

(226 citation statements)

References 39 publications

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“…Compared to ADEP1, a known activator of bacterial ClpP and human CLPP (Brötz-Oesterhelt et al 2005;Wong et al 2018), the imipridones were at least 20-fold more potent in these in vitro assays ( Figure S1D). These results demonstrate that ONC201 and ONC212 inhibit human cell proliferation by inducing unregulated CLPP proteolytic activity, as recently shown in other studies (Graves et al 2019;Ishizawa et al 2019).…”

Section: Onc201 and Onc212 Activate Clppsupporting

confidence: 90%

“…CLPX also performs chaperone functions independently of CLPP, as it promotes heme biosynthesis and enhances the DNA-binding activity of TFAM, a mitochondrial transcription factor (Kasashima et al 2012;Yien et al 2017). TFAM itself was also depleted in response to ONC212, in agreement with previous studies in other cell lines (Greer et al 2018;Graves et al 2019). Consistent with previous reports of mitochondrial defects caused by ONC201 treatment in various cell lines (Greer et al 2018;Ishizawa et al 2019), we found that both ONC201 and ONC212, but not an inactive isomer of ONC201, caused a collapse of mitochondrial membrane potential and an increase in mitochondrial reactive oxygen species levels in NALM-6 cells ( Figure S3).…”

Section: Effect Of Clpp Activation On the Human Proteomesupporting

confidence: 88%

“…HRP-conjugated goat anti-rabbit or goat anti-mouse (Jackson ImmunoResearch Laboratories) secondary antibodies were detected with Ultrascence Western Substrate (FroggaBio) and imaged on a ChemiDoc MP (Bio-Rad, Hercules, CA). In vitro degradation assays were performed with purified recombinant human CLPP (Profoldin) or E. coli ClpP (Li et al 2010) at 37°in 384-well plates in triplicate using fluorescein isothiocyanate (FITC)-labeled casein (FITC-casein) or N-acetyl-Trp-Leu-Ala-7-amino-4-methylcoumarin (Ac-WLA-AMC) substrates (Graves et al 2019). Fluorescence intensity was measured at l ex /l em of 485/528 or 350/460 nm for FITC-casein and Ac-WLA-AMC, respectively.…”

Section: Protein Analysis and Enzyme Assaysmentioning

confidence: 99%

“…Cell biological characterization suggests that ONC201 disrupts mitochondrial function and that cancer cells that do not depend on mitochondrial respiration are ONC201-insensitive (Greer et al 2018). It has recently been shown that ONC201 and other imipridones directly bind and activate CLPP in the absence of CLPX, resulting in the degradation of selected mitochondrial proteins and loss of mitochondrial integrity (Graves et al 2019;Ishizawa et al 2019).…”

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confidence: 99%

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Imipridone Anticancer Compounds Ectopically Activate the ClpP Protease and Represent a New Scaffold for Antibiotic Development

et al. 2020

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Systematic genetic interaction profiles can reveal the mechanisms-of-action of bioactive compounds. The imipridone ONC201, which is currently in cancer clinical trials, has been ascribed a variety of different targets. To investigate the genetic dependencies of imipridone action, we screened a genome-wide clustered regularly interspaced short palindromic repeats (CRISPR) knockout library in the presence of either ONC201 or its more potent analog ONC212. Loss of the mitochondrial matrix protease CLPP or the mitochondrial intermediate peptidase MIPEP conferred strong resistance to both compounds. Biochemical and surrogate genetic assays showed that impridones directly activate CLPP and that MIPEP is necessary for proteolytic maturation of CLPP into a catalytically competent form. Quantitative proteomic analysis of cells treated with ONC212 revealed degradation of many mitochondrial as well as nonmitochondrial proteins. Prompted by the conservation of ClpP from bacteria to humans, we found that the imipridones also activate ClpP from Escherichia coli, Bacillus subtilis, and Staphylococcus aureus in biochemical and genetic assays. ONC212 and acyldepsipeptide-4 (ADEP4), a known activator of bacterial ClpP, caused similar proteome-wide degradation profiles in S. aureus. ONC212 suppressed the proliferation of a number of Gram-positive (S. aureus, B. subtilis, and Enterococcus faecium) and Gram-negative species (E. coli and Neisseria gonorrhoeae). Moreover, ONC212 enhanced the ability of rifampin to eradicate antibiotic-tolerant S. aureus persister cells. These results reveal the genetic dependencies of imipridone action in human cells and identify the imipridone scaffold as a new entry point for antibiotic development.

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Section: Onc201 and Onc212 Activate Clppsupporting

confidence: 90%

Section: Effect Of Clpp Activation On the Human Proteomesupporting

confidence: 88%

Section: Protein Analysis and Enzyme Assaysmentioning

confidence: 99%

mentioning

confidence: 99%

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Imipridone Anticancer Compounds Ectopically Activate the ClpP Protease and Represent a New Scaffold for Antibiotic Development

et al. 2020

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“…Follow-up studies discovered that ONC201 did not directly activate TRAIL in all of the cancer cells in which it was effective but was impairing mitochondrial function [75]. Recent data from two studies identified the target of ONC201 as being the mitochondrial CLPP protease which is activated by ONC201 and results in increased cancer cell killing [76,77].…”

Section: Toxic Effects Of Pharmacological Agents On Mitochondrial Funmentioning

confidence: 99%

Impact of pharmacological agents on mitochondrial function: a growing opportunity?

Stoker

Newport

Hulit³

et al. 2019

Biochemical Society Transactions

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Present-day drug therapies provide clear beneficial effects as many diseases can be driven into remission and the symptoms of others can be efficiently managed; however, the success of many drugs is limited due to both patient non-compliance and adverse off-target or toxicity-induced effects. There is emerging evidence that many of these side effects are caused by drug-induced impairment of mitochondrial function and eventual mitochondrial dysfunction. It is imperative to understand how and why drug-induced side effects occur and how mitochondrial function is affected. In an aging population, age-associated drug toxicity is another key area of focus as the majority of patients on medication are older. Therefore, with an aging population possessing subtle or even more dramatic individual differences in mitochondrial function, there is a growing necessity to identify and understand early on potentially significant drug-associated off-target effects and toxicity issues. This will not only reduce the number of unwanted side effects linked to mitochondrial toxicity but also identify useful mitochondrial-modulating agents. Mechanistically, many successful drug classes including diabetic treatments, antibiotics, chemotherapies and antiviral agents have been linked to mitochondrial targeted effects. This is a growing area, with research to repurpose current medications affecting mitochondrial function being assessed in cancer, the immune system and neurodegenerative disorders including Parkinson's disease. Here, we review the effects that pharmacological agents have on mitochondrial function and explore the opportunities from these effects as potential disease treatments. Our focus will be on cancer treatment and immune modulation.

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Structure of Staphylococcus aureus ClpP Bound to the Covalent Active‐Site Inhibitor Cystargolide A

Illigmann,

Vielberg,

Lakemeyer

et al. 2023

Angewandte Chemie

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The caseinolytic protease is a highly conserved serine protease, crucial to prokaryotic and eukaryotic protein homeostasis, and a promising antibacterial and anticancer drug target. Herein, we describe the potent cystargolides as the first natural β‐lactone inhibitors of the proteolytic core ClpP. Based on the discovery of two clpP genes next to the cystargolide biosynthetic gene cluster in Kitasatospora cystarginea, we explored ClpP as a potential cystargolide target. We show the inhibition of Staphylococcus aureus ClpP by cystargolide A and B by different biochemical methods in vitro. Synthesis of semisynthetic derivatives and probes with improved cell penetration allowed us to confirm ClpP as a specific target in S. aureus cells and to demonstrate the anti‐virulence activity of this natural product class. Crystal structures show cystargolide A covalently bound to all 14 active sites of ClpP from S. aureus, Aquifex aeolicus, and Photorhabdus laumondii, and reveal the molecular mechanism of ClpP inhibition by β‐lactones, the predominant class of ClpP inhibitors.

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Mitochondrial Protease ClpP is a Target for the Anticancer Compounds ONC201 and Related Analogues

Cited by 131 publications

References 39 publications

Imipridone Anticancer Compounds Ectopically Activate the ClpP Protease and Represent a New Scaffold for Antibiotic Development

Imipridone Anticancer Compounds Ectopically Activate the ClpP Protease and Represent a New Scaffold for Antibiotic Development

Impact of pharmacological agents on mitochondrial function: a growing opportunity?

Structure of Staphylococcus aureus ClpP Bound to the Covalent Active‐Site Inhibitor Cystargolide A

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