Dissecting the molecular determinants of clinical PARP1 inhibitor selectivity for tankyrase1

PARP inhibitors (PARPi) have emerged as promising cancer therapeutics capable of targeting specific DNA repair pathways, but their mechanism of action with respect to PARP1-DNA retention remains unclear. Here, we developed single-molecule assays to directly monitor the retention of PARP1 on DNA lesions in real time. Our study reveals a two-step mechanism by which PARPi modulate the retention of PARP1 on DNA lesions, consisting of a primary step of catalytic inhibition via binding competition with NAD + followed by an allosteric modulation of bound PARPi. While clinically relevant PARPi exhibit distinct allosteric modulation activities that can either increase retention of PARP1 on DNA or induce its release, their retention potencies are predominantly determined by their ability to outcompete NAD + binding. These findings provide a mechanistic basis for improved PARPi selection according to their characteristic activities and enable further development of more potent inhibitors.

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“…S13, B and C). These trends are consistent with the dissociation constant values of different PARPi measured by ensemble methods ( 26 , 30 ).…”

Section: Resultssupporting

confidence: 88%

A two-step mechanism governing PARP1-DNA retention by PARP inhibitors

et al. 2022

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“…In order to explore possible anticancer pharmacodynamics profile, docking investigation have been performed. PolyADP-ribose polymerases PARPs (PARP1 [ 50 ] and PARP2 [ 51 ]) were selected for in silico simulations. The highest binding energies and inhibition constants Ki demonstrated compound 4 to both PARPs enzymes ( Table 6 ).…”

Section: Resultsmentioning

confidence: 99%

Development of Novel Pyridine-Thiazole Hybrid Molecules as Potential Anticancer Agents

et al. 2022

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Novel pyridine-thiazole hybrid molecules were synthesized and subjected to physico-chemical characterization and screening of their cytotoxic action towards a panel of cell lines derived from different types of tumors (carcinomas of colon, breast, and lung, glioblastoma and leukemia), and normal human keratinocytes, for comparison. High antiproliferative activity of the 3-(2-fluorophenyl)-1-[4-methyl-2-(pyridin-2-ylamino)-thiazol-5-yl]-propenone 3 and 4-(2-{1-(2-fluorophenyl)-3-[4-methyl-2-(pyridin-2-ylamino)-thiazol-5-yl]-3-oxopropylsulfanyl}-acetylamino)-benzoic acid ethyl ester 4 was revealed. The IC50 of the compound 3 in HL-60 cells of the acute human promyelocytic leukemia was 0.57 µM, while in the pseudo-normal human cell lines, the IC50 of this compound was >50 µM, which suggests that the compounds 3 and 4 might be perspective anticancer agents. The detected selectivity of the derivatives 3 and 4 for cancer cell lines inspired us to study the mechanisms of their cytotoxic action. It was shown that preincubation of tumor cells with Fluzaparib (inhibitor of PARP1) reduced the cytotoxic activity of the derivatives 3 and 4 by more than twice. The ability of these compounds to affect DNA nativity and cause changes in nucleus morphology allows for the suggestion that the mechanism of action of the novel pyridine-thiazole derivatives might be related to inducing the genetic instability in tumor cells.

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“…This effect was confirmed using a concentration-dependent blocking assay, revealing IC 50 values of 14.51 and 23.77 nM for talazoparib and olaparib, respectively (Figure S16). As talazoparib blocked the amount of bound [ 18 F]talazoparib to a significantly greater extent than olaparib, we theorize that this difference represents talazoparib’s ability to bind a wider array of other PARP isoforms, an effect that we plan to investigate further. , …”

Section: Resultsmentioning

confidence: 99%

“…As talazoparib blocked the amount of bound [ 18 F]talazoparib to a significantly greater extent than olaparib, we theorize that this difference represents talazoparib's ability to bind a wider array of other PARP isoforms, an effect that we plan to investigate further. 22,46 In Vivo Evaluation. [ 18 F]Talazoparib was further characterized in vivo in HCC1937 xenograft-bearing mice.…”

Section: ■ Results and Discussionmentioning

confidence: 99%

DoE Optimization Empowers the Automated Preparation of Enantiomerically Pure [¹⁸F]Talazoparib and its In Vivo Evaluation as a PARP Radiotracer

et al. 2021

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Given the clinical potential of poly(ADP-ribose) polymerases (PARP) imaging for the detection and stratification of various cancers, the development of novel PARP imaging probes with improved pharmacological profiles over established PARP imaging agents is warranted. Here, we present a novel 18 F-labeled PARP radiotracer based on the clinically superior PARP inhibitor talazoparib. An automated radiosynthesis of [ 18 F]talazoparib (RCY: 13 ± 3.4%; n = 4) was achieved using a "design of experiments" (DoE) optimized copper-mediated radiofluorination reaction. The chiral product was isolated from the reaction mixture using 2D reversed-phase/chiral radio-HPLC (>99% ee). (8S,9R)-[ 18 F]Talazoparib demonstrated PARP binding in HCC1937 cells in vitro and showed an excellent tumor-to-blood ratio in xenograft-bearing mice (10.2 ± 1.5). Additionally, a favorable pharmacological profile in terms of excretion, metabolism, and target engagement was observed. This synthesis of [ 18 F]talazoparib exemplifies how DoE can enable the radiosyntheses of synthetically challenging radiolabeled compounds of high interest to the imaging community.

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Dissecting the molecular determinants of clinical PARP1 inhibitor selectivity for tankyrase1

Cited by 44 publications

References 38 publications

A two-step mechanism governing PARP1-DNA retention by PARP inhibitors

A two-step mechanism governing PARP1-DNA retention by PARP inhibitors

Development of Novel Pyridine-Thiazole Hybrid Molecules as Potential Anticancer Agents

DoE Optimization Empowers the Automated Preparation of Enantiomerically Pure [¹⁸F]Talazoparib and its In Vivo Evaluation as a PARP Radiotracer

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Dissecting the molecular determinants of clinical PARP1 inhibitor selectivity for tankyrase1

Cited by 44 publications

References 38 publications

A two-step mechanism governing PARP1-DNA retention by PARP inhibitors

A two-step mechanism governing PARP1-DNA retention by PARP inhibitors

Development of Novel Pyridine-Thiazole Hybrid Molecules as Potential Anticancer Agents

DoE Optimization Empowers the Automated Preparation of Enantiomerically Pure [18F]Talazoparib and its In Vivo Evaluation as a PARP Radiotracer

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Product

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DoE Optimization Empowers the Automated Preparation of Enantiomerically Pure [¹⁸F]Talazoparib and its In Vivo Evaluation as a PARP Radiotracer