Inhibitors of PARP: Number crunching and structure gazing

Proceedings of the National Academy of Sciences, Год журнала: 2022, Номер 119(11)

Опубликована: Март 8, 2022

SignificancePARP is an important target in the treatment of cancers, particularly patients with breast, ovarian, or prostate cancer that have compromised homologous recombination repair (i.e., BRCA

Язык: Английский

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HPF1-dependent histone ADP-ribosylation triggers chromatin relaxation to promote the recruitment of repair factors at sites of DNA damage

Nature Structural & Molecular Biology, Год журнала: 2023, Номер 30(5), С. 678 - 691

Опубликована: Апрель 27, 2023

Язык: Английский

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PARP1: Structural insights and pharmacological targets for inhibition

DNA repair, Год журнала: 2021, Номер 103, С. 103125 - 103125

Опубликована: Апрель 15, 2021

Poly(ADP-ribose) polymerase 1 (PARP1, also known as ADPRT1) is a multifunctional human ADP-ribosyltransferase. It plays role in multiple DNA repair pathways, including the base excision (BER), non-homologous end joining (NHEJ), homologous recombination (HR), and Okazaki-fragment processing pathways. In response to strand breaks, PARP1 covalently attaches ADP-ribose moieties arginine, glutamate, aspartate, cysteine, lysine, serine acceptor sites on both itself other proteins. This signal recruits proteins site of damage. binding these enhances ADP-ribosylation via allosteric communication between distant catalytic domains. this review, we provide general overview emphasize novel potential approaches for pharmacological inhibition. Clinical inhibitors bind pocket, where they directly interfere with ADP-ribosylation. Some may further enhance potency by "trapping" an mechanism, though proposed mode action remains controversial. are used clinically treat some cancers, but resistance common, so urgently needed. One approach be design small molecules that at inter-domain interfaces essential allostery. To illustrate points, review includes instructive videos showing structures mechanisms.

Язык: Английский

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HPF1 and nucleosomes mediate a dramatic switch in activity of PARP1 from polymerase to hydrolase

eLife, Год журнала: 2021, Номер 10

Опубликована: Март 8, 2021

Poly(ADP-ribose) polymerase 1 (PARP1) is an important player in the response to DNA damage. Recently, Histone PARylation Factor (HPF1) was shown be a critical modulator of activity PARP1 by facilitating histones and redirecting target amino acid specificity from acidic serine residues. Here, we investigate mechanism specific consequences HPF1-mediated using nucleosomes as both activators substrates for PARP1. HPF1 provides that catalytic base Glu284 substantially redirect such become primary recipients PAR chains. Surprisingly, partitions most reaction product free ADP-ribose (ADPR), resulting much shorter chains compared reactions absence HPF1. This switch hydrolase has implications PARP1-mediated damage raises interesting new questions about role intracellular ADPR depletion NAD + .

Язык: Английский

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HPF1 dynamically controls the PARP1/2 balance between initiating and elongating ADP-ribose modifications

Nature Communications, Год журнала: 2021, Номер 12(1)

Опубликована: Ноя. 18, 2021

PARP1 and PARP2 produce poly(ADP-ribose) in response to DNA breaks. HPF1 regulates PARP1/2 catalytic output, most notably permitting serine modification with ADP-ribose. However, is substantially more abundant cells than HPF1, challenging whether can pervasively modulate PARP1. Here, we show biochemically that efficiently output at sub-stoichiometric ratios matching their relative cellular abundances. rapidly associates/dissociates from multiple molecules, initiating before initiates on glutamate/aspartate, accelerating initiation be comparable elongation reactions forming poly(ADP-ribose). This "hit run" mechanism ensures contributions during do not persist interfere PAR chain elongation. We provide structural insights into HPF1/PARP1 assembled a break, assess impact retention DNA. Our data support the prevalence of serine-ADP-ribose efficiency required for an acute damage response.

Язык: Английский

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PARP1: Liaison of Chromatin Remodeling and Transcription

Cancers, Год журнала: 2022, Номер 14(17), С. 4162 - 4162

Опубликована: Авг. 27, 2022

Poly(ADP-ribosyl)ation (PARylation) is a covalent post-translational modification and plays key role in the immediate response of cells to stress signals. Poly(ADP-ribose) polymerase 1 (PARP1), founding member PARP superfamily, synthesizes long branched polymers ADP-ribose (PAR) onto acceptor proteins, thereby modulating their function local surrounding. PARP1 most prominent PARPs responsible for production about 90% PAR cell. Therefore, PARylation play pleotropic wide range cellular processes, such as DNA repair genomic stability, cell death, chromatin remodeling, inflammatory gene transcription. has DNA-binding catalytic activities that are important repair, yet also modulate conformation transcription, which can be independent damage response. homeostasis have been implicated multiple diseases, including inflammation, stroke, diabetes cancer. Studies molecular action biological provide basis development pharmaceutic strategies clinical applications. This review focuses primarily on regulation remodeling transcriptional activation.

Язык: Английский

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Captured snapshots of PARP1 in the active state reveal the mechanics of PARP1 allostery

Molecular Cell, Год журнала: 2022, Номер 82(16), С. 2939 - 2951.e5

Опубликована: Июль 5, 2022

Язык: Английский

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

Science Advances, Год журнала: 2022, Номер 8(36)

Опубликована: Сен. 7, 2022

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

Язык: Английский

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Updated protein domain annotation of the PARP protein family sheds new light on biological function

Nucleic Acids Research, Год журнала: 2023, Номер 51(15), С. 8217 - 8236

Опубликована: Июнь 3, 2023

AlphaFold2 and related computational tools have greatly aided studies of structural biology through their ability to accurately predict protein structures. In the present work, we explored AF2 models 17 canonical members human PARP family supplemented this analysis with new experiments an overview recent published data. proteins are typically involved in modification nucleic acids mono or poly(ADP-ribosyl)ation, but function can be modulated by presence various auxiliary domains. Our provides a comprehensive view structured domains long intrinsically disordered regions within PARPs, offering revised basis for understanding these proteins. Among other functional insights, study model PARP1 domain dynamics DNA-free DNA-bound states enhances connection between ADP-ribosylation RNA ubiquitin-like modifications predicting putative RNA-binding E2-related RWD certain PARPs. line bioinformatic analysis, demonstrate first time PARP14's capability activity vitro. While our insights align existing experimental data probably accurate, they need further validation experiments.

Язык: Английский

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Clinical PARP inhibitors allosterically induce PARP2 retention on DNA

Science Advances, Год журнала: 2023, Номер 9(12)

Опубликована: Март 24, 2023

PARP1 and PARP2 detect DNA breaks, which activates their catalytic production of poly(ADP-ribose) that recruits repair factors contributes to PARP1/2 release from DNA. PARP inhibitors (PARPi) are used in cancer treatment target activity, interfering with increasing persistence on damage. In addition, certain PARPi exert allosteric effects increase retention However, no clinical exhibit this behavior toward PARP1. contrast, we show an effect retains breaks a manner depends communication between the binding regions. Using mutant mimics inhibitor effect, observed increased at cellular damage sites. The AZD5305 also exhibited clear reverse PARP2. Our results can help explain toxicity suggest ways improve moving forward.

Язык: Английский

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