The PARP inhibitor olaparib exerts beneficial effects in mice subjected to cecal ligature and puncture and in cells subjected to oxidative stress without impairing DNA integrity: A potential opportunity for repurposing a clinically used oncological drug for the experimental therapy of sepsis

Ahmad, Akbar; Vieira, Juliana de Camargo; Mello, Aline Haas de; Lima, Thaís Martins de; Ariga, Suely Kubo; Barbeiro, Denise Frediani; Barbeiro, Hermes Vieira; Szczesny, Bartosz; Törő, Gábor; Druzhyna, Nadiya; Randi, Elisa B.; Marcatti, Michela; Toliver‐Kinsky, Tracy; Kiss, András; Liaudet, Lucas; Salomão, Reinaldo; Soriano, Francisco; Szabó, Csaba

doi:10.1016/j.phrs.2019.104263

Cited by 21 publications

(38 citation statements)

References 63 publications

(84 reference statements)

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“…As discussed previously ( 17 , 81 ), the effective dose of the clinically approved PARP inhibitors in nononcological models is significantly lower than the doses of the same agents in oncology, most likely due to the fact that in nononcological models a partial inhibition of PARP is sufficient to exert therapeutic effects. Thus, it will be possible to find effective doses of olaparib for the therapy of nononcological conditions (in particular, in disease conditions in which the patients do not have any baseline defect in DNA-repair pathways, such as ALI) in which a partial inhibition of PARP exerts beneficial effects without interfering with DNA repair and DNA integrity.…”

Section: The Therapeutic Efficacy Of Parp Inhibitors In Alimentioning

confidence: 93%

“…The preclinical data demonstrating the efficacy of the clinically approved PARP inhibitor olaparib (or 4-(3-{[4-(cyclopropylcarbonyl)piperazin-1-yl]carbonyl}-4-fluorobenzyl)phthalazin-1(2H)-one; marketed as Lynparza) in various experimental models of lung injury and/or various forms of critical illness ( 70 , 72 , 80 , 81 , 83 , 84 ) are especially relevant from the translational standpoint. Olaparib (similar to the PARP inhibitors of other classes) improves pulmonary inflammation, counteracts pulmonary extravasation, reduces oxidative stress, and improves antioxidant status in the lung in various experimental models of ALI ( 70 , 72 , 80 , 83 ) and, importantly, also exerts beneficial effects against the ALI-associated central-nervous-system dysfunction (e.g., cognitive defects) ( 83 ).…”

Section: The Therapeutic Efficacy Of Parp Inhibitors In Alimentioning

confidence: 99%

“…Olaparib also exerts beneficial effects in other animal models that have a significant pulmonary-injury component and/or systemic hyperinflammatory component, including asthma models ( 72 , 74 ), a pulmonary inflammation/emphysema model ( 80 ), and murine models of acute burn injury and pancreatitis ( 84 , 90 ). In a murine model of sepsis (induced by CLP), olaparib improved survival and exerted beneficial effects on inflammatory-mediator production and immune-cell balance, but in this model, no significant pulmonary injury was noted, and olaparib had no effect on the various pulmonary parameters investigated ( 81 ).…”

Section: The Therapeutic Efficacy Of Parp Inhibitors In Alimentioning

confidence: 99%

“…Thus, it will be possible to find effective doses of olaparib for the therapy of nononcological conditions (in particular, in disease conditions in which the patients do not have any baseline defect in DNA-repair pathways, such as ALI) in which a partial inhibition of PARP exerts beneficial effects without interfering with DNA repair and DNA integrity. Indeed, in a CLP model, in which the efficacy and safety of olaparib were simultaneously assessed, olaparib (at the effective dose range of 6–30 mg/kg/d), olaparib beneficially modulated the cytokine and immune status of the animals and improved survival but did not exert any adverse effects on mitochondrial or nuclear DNA integrity in various tissues, including the lung ( 81 ). In a second study, in which the effect of PARP inhibition in a critical illness was assessed not only on efficacy parameters but also on DNA injury, the PARP inhibitor used (INO-1001, 4 mg/kg) provided hemodynamic stabilization in a porcine model of thoracic aortic cross-clamping–induced ischemia/reperfusion, without worsening the DNA damage in peripheral blood lymphocytes ( 91 ).…”

Section: The Therapeutic Efficacy Of Parp Inhibitors In Alimentioning

confidence: 99%

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Poly(ADP-Ribose) Polymerase Inhibition in Acute Lung Injury. A Reemerging Concept

Szabó

Martins

Liaudet

2020

Am J Respir Cell Mol Biol

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PARP1, the major isoform of a family of ADP-ribosylating enzymes, has been implicated in the regulation of various biological processes including DNA repair, gene transcription, and cell death. The concept that PARP1 becomes activated in acute lung injury (ALI) and that pharmacological inhibition or genetic deletion of this enzyme can provide therapeutic benefits emerged over 20 years ago. The current article provides an overview of the cellular mechanisms involved in the pathogenetic roles of PARP1 in ALI and provides an overview of the preclinical data supporting the efficacy of PARP (poly[ADP-ribose] polymerase) inhibitors. In recent years, several ultrapotent PARP inhibitors have been approved for clinical use (for the therapy of various oncological diseases): these newly-approved PARP inhibitors were recently reported to show efficacy in animal models of ALI. These observations offer the possibility of therapeutic repurposing of these inhibitors for patients with ALI. The current article lays out a potential roadmap for such repurposing efforts. In addition, the article also overviews the scientific basis of potentially applying PARP inhibitors for the experimental therapy of viral ALI, such as coronavirus disease (COVID-19)–associated ALI.

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Section: The Therapeutic Efficacy Of Parp Inhibitors In Alimentioning

confidence: 93%

Section: The Therapeutic Efficacy Of Parp Inhibitors In Alimentioning

confidence: 99%

Section: The Therapeutic Efficacy Of Parp Inhibitors In Alimentioning

confidence: 99%

Section: The Therapeutic Efficacy Of Parp Inhibitors In Alimentioning

confidence: 99%

See 2 more Smart Citations

Poly(ADP-Ribose) Polymerase Inhibition in Acute Lung Injury. A Reemerging Concept

Szabó

Martins

Liaudet

2020

Am J Respir Cell Mol Biol

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“…Cellular bioenergetics was measured by the Extracellular Flux Analysis method as described for various other cell types [10,13]. Cells (15,000/well) were seeded on cell culture microplates and treated with HMPSNE (10, 100, or 300 µM) or its vehicle for 16 h. For analysis of mitochondrial respiration, cells were washed twice with DMEM (pH 7.4) supplemented with L-glutamine (2 mM, Gibco), sodium pyruvate (1 mM, Sigma) and glucose (10 mM, Sigma).…”

Section: Determination Of Cellular Bioenergeticsmentioning

confidence: 99%

Role of 3-Mercaptopyruvate Sulfurtransferase in the Regulation of Proliferation, Migration, and Bioenergetics in Murine Colon Cancer Cells

et al. 2020

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3-mercaptopyruvate sulfurtransferase (3-MST) has emerged as one of the significant sources of biologically active sulfur species in various mammalian cells. The current study was designed to investigate the functional role of 3-MST's catalytic activity in the murine colon cancer cell line CT26. The novel pharmacological 3-MST inhibitor HMPSNE was used to assess cancer cell proliferation, migration and bioenergetics in vitro. Methods included measurements of cell viability (MTT and LDH assays), cell proliferation and in vitro wound healing (IncuCyte) and cellular bioenergetics (Seahorse extracellular flux analysis). 3-MST expression was detected by Western blotting; H 2 S production was measured by the fluorescent dye AzMC. The results show that CT26 cells express 3-MST protein and mRNA, as well as several enzymes involved in H 2 S degradation (TST, ETHE1). Pharmacological inhibition of 3-MST concentration-dependently suppressed H 2 S production and, at 100 and 300 µM, attenuated CT26 proliferation and migration. HMPSNE exerted a bell-shaped effect on several cellular bioenergetic parameters related to oxidative phosphorylation, while other bioenergetic parameters were either unaffected or inhibited at the highest concentration of the inhibitor tested (300 µM). In contrast to 3-MST, the expression of CBS (another H 2 S producing enzyme which has been previously implicated in the regulation of various biological parameters in other tumor cells) was not detectable in CT26 cells and pharmacological inhibition of CBS exerted no significant effects on CT26 proliferation or bioenergetics. In summary, 3-MST catalytic activity significantly contributes to the regulation of cellular proliferation, migration and bioenergetics in CT26 murine colon cancer cells. The current studies identify 3-MST as the principal source of biologically active H 2 S in this cell line.

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Poly (ADP-ribose) polymerase: An Overview of Mechanistic Approaches and Therapeutic Opportunities in the Management of Stroke

et al. 2022

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The PARP inhibitor olaparib exerts beneficial effects in mice subjected to cecal ligature and puncture and in cells subjected to oxidative stress without impairing DNA integrity: A potential opportunity for repurposing a clinically used oncological drug for the experimental therapy of sepsis

Cited by 21 publications

References 63 publications

Poly(ADP-Ribose) Polymerase Inhibition in Acute Lung Injury. A Reemerging Concept

Poly(ADP-Ribose) Polymerase Inhibition in Acute Lung Injury. A Reemerging Concept

Role of 3-Mercaptopyruvate Sulfurtransferase in the Regulation of Proliferation, Migration, and Bioenergetics in Murine Colon Cancer Cells

Poly (ADP-ribose) polymerase: An Overview of Mechanistic Approaches and Therapeutic Opportunities in the Management of Stroke

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