PARP-2 and PARP-3 are selectively activated by 5′ phosphorylated DNA breaks through an allosteric regulatory mechanism shared with PARP-1

Langelier, Marie-France; Riccio, Amanda A.; Pascal, John M.

doi:10.1093/nar/gku474

Cited by 230 publications

(349 citation statements)

References 40 publications

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“…The DNA-dependent activity of these DDR PARPs requires the presence of a conserved Tyr-Gly-Arg (WGR) domain, which is present in PARPs 1-3 (Langelier et al, 2012;Langelier et al, 2014). In addition to the WGR domain, PARP1, which is perhaps the most structurally complex member of the PARP family, also contains these regulatory domains: the breast cancer susceptibility protein-1 C terminus (BRCT) domain and three zinc finger domains (ZnF1-3) (Figure 2) Steffen et al, 2013).…”

Section: Dna-dependent Parpsmentioning

confidence: 99%

“…PARP1 can also be activated by binding nucleosomes as well as abnormal DNA structures, such as DNA overhangs, hairpins, forks, and cruciform structures Langelier and Pascal, 2013;Langelier et al, 2012Langelier et al, , 2014. Adding further complexity, PARP1 can also be activated by interacting with its binding partners, such as phosphorylated ERK2, thus affecting further downstream signaling cascades or by being modified by a number of posttranslational modifications (Cohen-Armon et al, 2007).…”

Section: Dna-dependent Parpsmentioning

confidence: 99%

“…Two other human DDR PARPs, PARP2 and 3, lack ZnF domains present in PARP1; nevertheless, they can be efficiently activated by DNA breaks directly via their WGR domains (Langelier et al, 2014). It has been shown that PARP2 and PARP3 are selectively activated by 5 0 -phosphorylated breaks.…”

Section: Dna-dependent Parpsmentioning

confidence: 99%

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Structures and Mechanisms of Enzymes Employed in the Synthesis and Degradation of PARP-Dependent Protein ADP-Ribosylation

2015

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The poly(ADP-ribose) polymerases (PARPs) are a major family of enzymes capable of modifying proteins by ADP-ribosylation. Due to the large size and diversity of this family, PARPs affect almost every aspect of cellular life and have fundamental roles in DNA repair, transcription, heat shock and cytoplasmic stress responses, cell division, protein degradation, and much more. In the past decade, our understanding of the PARP enzymatic mechanism and activation, as well as regulation of ADP-ribosylation signals by the readers and erasers of protein ADP-ribosylation, has been significantly advanced by the emergence of new structural data, reviewed herein, which allow for better understanding of the biological roles of this widespread post-translational modification.

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Section: Dna-dependent Parpsmentioning

confidence: 99%

Section: Dna-dependent Parpsmentioning

confidence: 99%

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Structures and Mechanisms of Enzymes Employed in the Synthesis and Degradation of PARP-Dependent Protein ADP-Ribosylation

2015

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“…DNA bağlayan bölge olan N-terminal uç, hasarlı DNA'yı onarmaktan sorumludur. Mer- (15). PARP aktivasyonunun ilişkili olduğu bazı olaylar Tablo 2'de sunulmuştur (16,17).…”

Section: Poli (Adp-riboz) Polimerazlar (Parp'lar)unclassified

A New Approach in Cancer Treatment: Poly(ADP-Ribose) Polymerase-1 Inhibitors

Tok¹,

Kaymakçıoğlu²

2015

MUSBED

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Kanser tedavisinde yeni bir yaklaşım: Poli (ADP-riboz) polimeraz-1 inhibitörleri Genetik materyal olan DNA'da iç ve dış etkenler sonucu hasar oluşabilir. Normal bir hücrede bu hasarı onarabilecek çok sayıda tamir mekanizması vardır. Bunlardan biri de PARP-1 enzimidir. PARP-1, nikotinamid adenin dinükleotidden ADP-riboz yapılarını protein akseptörüne transfer eder. Böylece tek zincir DNA kırıkları onarılır. PARP-1'in inhibisyonu durumunda ise bu tek zincir DNA kırıkları onarılamaz ve çift zincir DNA kırıkları oluşur. Sonuçta hücre nekrozise ya da apoptozise gider. Kanser tedavisinde tümörlü hücrelerin PARP-1 inhibisyonuyla öldürülmesi amaçlanmaktadır. Bu amaçla son on yıl içinde çok sayıda çalışma yapılmış olup, günümüzde faz aşamasında bulunan ve piyasaya sürülmeyi bekleyen PARP-1 inhibitörleri mevcuttur. Bu derlemede, DNA'da oluşan hasarın hangi mekanizmalarla onarıldığı, PARP enzim ailesinin genomik bütünlüğü nasıl koruduğu ve kanser tedavisinde kullanılmak üzere geliştirilmiş PARP-1 inhibitörü kimyasal bileşiklerin yapıları hakkında bilgi verilmiştir.

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“…Recent studies found that PARP-3 could be stimulated by DNA double-strand breaks (DSBs) in vitro and functioned in the same pathway as the poly (ADPribose)-binding protein APLF to accelerate chromosomal DNA DSB repair [9][10][11]. As a result, the absence of PARP3 confers hypersensitivity to anti-tumoral drugs generating DSB [11][12]. However, the underline molecular events remained elusive.…”

Section: Introductionmentioning

confidence: 99%

PARP3 interacts with FoxM1 to confer glioblastoma cell radioresistance

Quan

Song

2015

Tumor Biol.

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Poly(ADP-ribose) polymerase 3 (PARP3), a critical player in cellular response to DNA double-strand breaks (DSBs), plays an essential role in the maintenance of genome integrity. However, the role of PARP3 in tumorigenesis especially in glioblastoma remains largely unknown. In the present study, we found that the mRNA and protein levels of PARP3 were upregulated in primary glioblastoma tissues. Knockdown of PARP3 expression by lentivirus-based shRNA decreased cell glioblastoma proliferation and inhibited tumor growth in vivo by using a xenograft mouse model. Furthermore, we found that silencing the expression of PARP3 resulted in a synergistic radiosensitizing effect when combined with radiotherapy in glioblastoma cell lines. At the molecular level, we found that PARP3 interacted with FoxM1 to enhance its transcriptional activity and conferred glioblastoma cell radioresistance. Thus, our data suggest that PARP3 could be a therapeutic target to overcome radioresistance in glioblastoma.

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PARP-2 and PARP-3 are selectively activated by 5′ phosphorylated DNA breaks through an allosteric regulatory mechanism shared with PARP-1

Cited by 230 publications

References 40 publications

Structures and Mechanisms of Enzymes Employed in the Synthesis and Degradation of PARP-Dependent Protein ADP-Ribosylation

Structures and Mechanisms of Enzymes Employed in the Synthesis and Degradation of PARP-Dependent Protein ADP-Ribosylation

A New Approach in Cancer Treatment: Poly(ADP-Ribose) Polymerase-1 Inhibitors

PARP3 interacts with FoxM1 to confer glioblastoma cell radioresistance

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