Synthetic Lethality Targeting Polθ
TLDR
The authors discuss the current state of knowledge on Polθ as a potential target for synthetic lethality-based anticancer therapies and suggests it is a promising target in the treatment of tumors harboring deficiencies in homologous recombination repair (HRR).Abstract:
Research studies regarding synthetic lethality (SL) in human cells are primarily motivated by the potential of this phenomenon to be an effective, but at the same time, safe to the patient’s anti-cancer chemotherapy. Among the factors that are targets for the induction of the synthetic lethality effect, those involved in DNA repair seem to be the most relevant. Specifically, when mutation in one of the canonical DNA double-strand break (DSB) repair pathways occurs, which is a frequent event in cancer cells, the alternative pathways may be a promising target for the elimination of abnormal cells. Currently, inhibiting RAD52 and/or PARP1 in the tumor cells that are deficient in the canonical repair pathways has been the potential target for inducing the effect of synthetic lethality. Unfortunately, the development of resistance to commonly used PARP1 inhibitors (PARPi) represents the greatest obstacle to working out a successful treatment protocol. DNA polymerase theta (Polθ), encoded by the POLQ gene, plays a key role in an alternative DSB repair pathway—theta-mediated end joining (TMEJ). Thus, it is a promising target in the treatment of tumors harboring deficiencies in homologous recombination repair (HRR), where its inhibition can induce SL. In this review, the authors discuss the current state of knowledge on Polθ as a potential target for synthetic lethality-based anticancer therapies.read more
Citations
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DNA polymerase theta protects leukemia cells from metabolic-induced DNA damage.
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Small Molecules Targeting DNA Polymerase Theta (POLθ) as Promising Synthetic Lethal Agents for Precision Cancer Therapy
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TL;DR: The first proof of concept for the effectiveness of synthetic lethality (SL) was provided by the approval of poly(ADP-ribose)polymerase inhibitors, which exploit a SL interaction in BRCA-deficient cells, although their use is limited by resistance as discussed by the authors .
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Polθ Inhibition: An Anticancer Therapy for HR-Deficient Tumours
TL;DR: In this paper , the authors describe the significance of DNA polymerase theta and the Polθ-mediated TMEJ pathway and summarize the current state-of-the-art inhibitors and emphasize the promising role of Pol θ as a therapeutic target.
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G. Farinea,V. Crespi,Angela Listì,Luisella Righi,Paolo Bironzo,Alessandra Merlini,Umberto Malapelle,Silvia Novello,Giorgio V. Scagliotti,Francesco Passiglia +9 more
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