Novel phenanthridinone inhibitors of poly(adenosine 5′-diphosphate-ribose) synthetase: Potent cytoprotective and antishock agents*

Jagtap, Prakash G.; Soriano, Francisco; Virág, László; Liaudet, Lucas; Mabley, Jon G.; Szabó, Éva; Haskó, György; Marton, Anita; Lorigados, Clara Batista; Gallyas, Ferenc; Sümegi, Balázs; Hoyt, Dale G.; Baloglu, Erkan; VanDuzer, John; Salzman, Andrew L.; Southan, Garry J.; Szabó, Csaba

doi:10.1097/00003246-200205000-00019

Cited by 182 publications

(169 citation statements)

References 44 publications

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“…We further tested the effect of blocking PARP-1 signaling with the pharmacological inhibitor PJ-34 (10 mg/kg intraperitonealy at MCAO onset, Jagtap et al, 2002;Abdelkarim et al, 2001) in ovary-intact WT female mice and obtained results consistent with those from female PARP-1-knockouts (Figure 9). Increased damage was observed in both cortex and striatum of PJ-34-treated mice with corresponding Physiological levels of E2 were restored to ovariectomized (OVX) PARPÀ/À and wild-type (WT) female mice.…”

Section: Pharmacological Inhibition Of Poly-adp Ribose Polymerase Alsmentioning

confidence: 77%

Ischemic Nitric Oxide and Poly (ADP-Ribose) Polymerase-1 in Cerebral Ischemia: Male Toxicity, Female Protection

McCullough

Zeng

Blizzard

et al. 2005

J Cereb Blood Flow Metab

297

326

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It is well established that tissue damage and functional outcome after experimental or clinical stroke are shaped by biologic sex. We investigated the novel hypothesis that ischemic cell death from neuronally derived nitric oxide (NO) or poly-ADP ribose polymerase (PARP-1) activation is sexually dimorphic and that interruption of these molecular death pathways benefits only the male brain. Female neuronal nitric oxide synthase (nNOS) knockout (nNOSÀ/À) mice exhibited exacerbated histological injury after middle cerebral artery occlusion (MCAO) relative to wild-type (WT) females, unlike the protection observed in male nNOSÀ/À littermates. Similarly, treatment with the nNOS inhibitor (7-nitroindozole, 25 mg/kg) increased infarction in female C57Bl6 WT mice, but protected male mice. The mechanism for this sexually specific response is not mediated through changes in protein expression of endothelial NOS or inducible NOS, or differences in intraischemic cerebral blood flow. Unlike male PARP-1 knockouts (PARP1À/À), female PARP1À/À littermates sustained grossly increased ischemic damage relative to sex-matched WT mice. Treatment with a PARP inhibitor (PJ-34, 10 mg/kg) resulted in identical results. Loss of PARP-1 resulted in reversal of the neuroprotective activity by the female sex steroid, 17b estradiol. These data suggest that the previously described cell death pathways involving NO and PARP ischemic neurotoxicity may be operant solely in male brain and that the integrity of nNO/PARP-1 signaling is paradoxically protective in the female.

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Section: Pharmacological Inhibition Of Poly-adp Ribose Polymerase Alsmentioning

confidence: 77%

Ischemic Nitric Oxide and Poly (ADP-Ribose) Polymerase-1 in Cerebral Ischemia: Male Toxicity, Female Protection

McCullough

Zeng

Blizzard

et al. 2005

J Cereb Blood Flow Metab

297

326

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“…Poly(ADP-ribose) polymerase (PARP) is an abundant nuclear enzyme with complex regulatory functions (Hiromatsu et al 1992, De Murcia et al 1994, Menissier-de Murcia et al 1997, Szabó et al 1997b, 1998a, 2000, Le Rhun et al 1998, Rudat et al 1998, De Murcia &Shall 2000, Davidovic et al 2001, Virág & Szabó 2002. Poly(ADPribose) polymerase-1 (PARP-1, EC 2.4.2.30) [also known as poly(ADP-ribose) synthetase (PARS)], the major PARP isoform, is a member of the PARP enzyme family consisting of PARP-1 and many additional, recently identified poly(ADP-ribosylating) enzymes (minor PARP isoforms).…”

Section: Poly(adp-ribose) Polymerase and Its Activationmentioning

confidence: 99%

“…Numerous overviews and monographs appeared in recent years about the structure and functions of PARP (Szabó et al 1998a, 2000, Virág & Szabó 2002, Zhang 2002. PARP is a DNA damage sensor and signaling molecule and binds to both single-and double stranded DNA breaks, becomes activated, forms homodimers and initiates an energy-consuming cycle by transferring ADP ribose units from NAD + onto nuclear acceptor proteins such as histones, transcriptional factors, DNA replication factors and signaling molecules (AP-1, DNA-PK, NFkB, Oct-1, p53) with PARP itself being the major acceptor.…”

Section: Poly(adp-ribose) Polymerase and Its Activationmentioning

confidence: 99%

“…In case of the histones, this process leads to electrostatic repulsion between DNA and loosening up the chromatin structure thereby making genes more accessible for gene transcription (Oikawa et al 1980, Poirier et al 1982, Park et al 1983, Satoh & Lindahl 1992, Lautier et al 1993, Herceg et al 2001. The effect of PARP on the function of these proteins is carried out by non-covalent protein-protein interactions and by covalent poly(ADP-ribosylation) (for review see Virág & Szabó 2002). Poly(ADP-ribosylation) is a dynamic process as the polymer is rapidly degraded by two enzymes: poly(ADP-ribose) glycohydrolase (PARG) and ADP-ribosyl protein lyase.…”

Section: Poly(adp-ribose) Polymerase and Its Activationmentioning

confidence: 99%

“…When activated by DNA breaks, PARP initiates an energy-consuming cycle resulting in the depletion of NAD + and ATP, slowing the rate of glycolysis and mitochondrial respiration, eventually leading to cellular dysfunction and necrotic cell death. Necrosis is the least desirable form of cell death as the cellular content is released into the tissue exposing neighboring cells to proteases and various pro-inflammatory factors, thereby triggering positive feedback pathways of inflammatory tissue injury (Virág & Szabó 2002). PARP-overactivation induced necrosis is also related to intracellular acidification (Herceg et al 2001, Affar et al 2002.…”

Section: Poly(adp-ribose) Polymerase and Its Activationmentioning

confidence: 99%

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The pathogenesis of diabetic complications: the role of DNA injury and poly(ADP-ribose) polymerase activation in peroxynitrite-mediated cytotoxicity

Kiss

Szabó

2005

Mem. Inst. Oswaldo Cruz

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PARP Inhibitors As Anticancer Agents

Costantino

Pellicciari

2010

Burger's Medicinal Chemistry and Drug Discovery

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Poly(ADP‐ribosyl)ation is posttranslation covalent modification, which is operated by a family of enzymes whose founding member, named PARP‐1, has been involved in a variety of physiological as well as pathological processes. In particular, PARP‐1 is activated by DNA‐strand breaks, and is a key component of the DNA repairing machinery thus acting as a caretaker of genomic stability. Over the last decade, many evidence have accumulated suggesting that PARP inhibitors may find utility as cotherapy with DNA damaging agents in many preclinical models of cancer, and also as monotherapy in some important DNA repair defective tumors. These findings are now translating into clinically useful agents that are undergoing clinical trials. In this chapter, we review the diversity of the PARP family, the significance of poly(ADP‐ribosyl)ation in DNA repairing and the mechanism of PARP inhibitors in cancer therapy. Finally, an overview of the most promising PARP inhibitors under clinical evaluation is given.

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Novel phenanthridinone inhibitors of poly(adenosine 5′-diphosphate-ribose) synthetase: Potent cytoprotective and antishock agents*

Abstract: The novel series of phenanthridinone PARS inhibitors have potent cytoprotective effects in vitro and significant protective effects in shock and reperfusion injury in rodent models in vivo.

Cited by 182 publications

References 44 publications

Ischemic Nitric Oxide and Poly (ADP-Ribose) Polymerase-1 in Cerebral Ischemia: Male Toxicity, Female Protection

Ischemic Nitric Oxide and Poly (ADP-Ribose) Polymerase-1 in Cerebral Ischemia: Male Toxicity, Female Protection

The pathogenesis of diabetic complications: the role of DNA injury and poly(ADP-ribose) polymerase activation in peroxynitrite-mediated cytotoxicity

PARP Inhibitors As Anticancer Agents

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