001     145040
005     20250415103927.0
024 7 _ |a 10.1007/s00018-019-03283-2
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024 7 _ |a pmid:31451894
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024 7 _ |a 0014-4754
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024 7 _ |a 1420-682X
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024 7 _ |a 1420-9071
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024 7 _ |a altmetric:65573158
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037 _ _ |a DZNE-2020-00400
041 _ _ |a English
082 _ _ |a 610
100 1 _ |a Sahaboglu, Ayse
|0 P:(DE-HGF)0
|b 0
|e Corresponding author
245 _ _ |a Drug repurposing studies of PARP inhibitors as a new therapy for inherited retinal degeneration.
260 _ _ |a Cham (ZG)
|c 2020
|b Springer International Publishing AG
264 _ 1 |3 online
|2 Crossref
|b Springer Science and Business Media LLC
|c 2019-08-26
264 _ 1 |3 print
|2 Crossref
|b Springer Science and Business Media LLC
|c 2020-06-01
336 7 _ |a article
|2 DRIVER
336 7 _ |a Output Types/Journal article
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336 7 _ |a Journal Article
|b journal
|m journal
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|s 1744706326_27298
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336 7 _ |a ARTICLE
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336 7 _ |a JOURNAL_ARTICLE
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336 7 _ |a Journal Article
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520 _ _ |a The enzyme poly-ADP-ribose-polymerase (PARP) has important roles for many forms of DNA repair and it also participates in transcription, chromatin remodeling and cell death signaling. Currently, some PARP inhibitors are approved for cancer therapy, by means of canceling DNA repair processes and cell division. Drug repurposing is a new and attractive aspect of therapy development that could offer low-cost and accelerated establishment of new treatment options. Excessive PARP activity is also involved in neurodegenerative diseases including the currently untreatable and blinding retinitis pigmentosa group of inherited retinal photoreceptor degenerations. Hence, repurposing of known PARP inhibitors for patients with non-oncological diseases might provide a facilitated route for a novel retinitis pigmentosa therapy. Here, we demonstrate and compare the efficacy of two different PARP inhibitors, BMN-673 and 3-aminobenzamide, by using a well-established retinitis pigmentosa model, the rd1 mouse. Moreover, the mechanistic aspects of the PARP inhibitor-induced protection were also investigated in the present study. Our results showed that rd1 rod photoreceptor cell death was decreased by about 25-40% together with the application of these two PARP inhibitors. The wealth of human clinical data available for BMN-673 highlights a strong potential for a rapid clinical translation into novel retinitis pigmentosa treatments. Remarkably, we have found that the efficacy of 3 aminobenzamide was able to decrease PARylation at the nanomolar level. Our data also provide a link between PARP activity with the Wnt/β-catenin pathway and the major intracellular antioxidant concentrations behind the PARP-dependent retinal degeneration. In addition, molecular modeling studies were integrated with experimental studies for better understanding of the role of PARP1 inhibitors in retinal degeneration.
536 _ _ |a 345 - Population Studies and Genetics (POF3-345)
|0 G:(DE-HGF)POF3-345
|c POF3-345
|f POF III
|x 0
542 _ _ |i 2019-08-26
|2 Crossref
|u http://www.springer.com/tdm
588 _ _ |a Dataset connected to CrossRef, PubMed,
650 _ 7 |a Benzamides
|2 NLM Chemicals
650 _ 7 |a Phthalazines
|2 NLM Chemicals
650 _ 7 |a Poly(ADP-ribose) Polymerase Inhibitors
|2 NLM Chemicals
650 _ 7 |a 3-aminobenzamide
|0 8J365YF1YH
|2 NLM Chemicals
650 _ 7 |a talazoparib
|0 9QHX048FRV
|2 NLM Chemicals
650 _ 7 |a Poly(ADP-ribose) Polymerases
|0 EC 2.4.2.30
|2 NLM Chemicals
650 _ 2 |a Animals
|2 MeSH
650 _ 2 |a Benzamides: therapeutic use
|2 MeSH
650 _ 2 |a Drug Repositioning: methods
|2 MeSH
650 _ 2 |a Humans
|2 MeSH
650 _ 2 |a Mice
|2 MeSH
650 _ 2 |a Phthalazines: therapeutic use
|2 MeSH
650 _ 2 |a Poly(ADP-ribose) Polymerase Inhibitors: therapeutic use
|2 MeSH
650 _ 2 |a Poly(ADP-ribose) Polymerases: metabolism
|2 MeSH
650 _ 2 |a Retina: drug effects
|2 MeSH
650 _ 2 |a Retina: metabolism
|2 MeSH
650 _ 2 |a Retina: pathology
|2 MeSH
650 _ 2 |a Retinal Degeneration: drug therapy
|2 MeSH
650 _ 2 |a Retinal Degeneration: metabolism
|2 MeSH
650 _ 2 |a Retinal Degeneration: pathology
|2 MeSH
650 _ 2 |a Retinitis Pigmentosa: drug therapy
|2 MeSH
650 _ 2 |a Retinitis Pigmentosa: metabolism
|2 MeSH
650 _ 2 |a Retinitis Pigmentosa: pathology
|2 MeSH
700 1 _ |a Miranda, Maria
|b 1
700 1 _ |a Canjuga, Denis
|b 2
700 1 _ |a Avci-Adali, Meltem
|b 3
700 1 _ |a Savytska, Natalia
|0 P:(DE-2719)2812754
|b 4
|u dzne
700 1 _ |a Secer, Enver
|b 5
700 1 _ |a Feria-Pliego, Jessica Abigail
|b 6
700 1 _ |a Kayık, Gülru
|b 7
700 1 _ |a Durdagi, Serdar
|b 8
773 1 8 |a 10.1007/s00018-019-03283-2
|b : Springer Science and Business Media LLC, 2019-08-26
|n 11
|p 2199-2216
|3 journal-article
|2 Crossref
|t Cellular and Molecular Life Sciences
|v 77
|y 2019
|x 1420-682X
773 _ _ |a 10.1007/s00018-019-03283-2
|g Vol. 77, no. 11, p. 2199 - 2216
|0 PERI:(DE-600)1458497-9
|n 11
|p 2199-2216
|t Cellular and molecular life sciences
|v 77
|y 2020
|x 1420-682X
856 4 _ |u https://pub.dzne.de/record/145040/files/DZNE-2020-00400_Restricted.pdf
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910 1 _ |a Deutsches Zentrum für Neurodegenerative Erkrankungen
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LibraryCollectionCLSMajorCLSMinorLanguageAuthor
Marc 21