Antitumor efficacy of PARP inhibitors in homologous recombination deficient carcinomas

Yi, Tianjin; Feng, Yi; Sundaram, Ravi; Tie, Yan; Zheng, Heng; Qian, Yanping; You, Di; Yi, Tao; Wang, Ping; Zhao, Xia

doi:10.1002/ijc.32143

Cited by 24 publications

(13 citation statements)

References 29 publications

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“…Multiple cancer therapies, such as DNA damage-inflicting irradiation or chemotherapy, are aimed at this vulnerability, however, emerging treatment strategies are aimed to take advantage of disturbed DNA repair systems that may be present in different tumour types. For instance, treatment with PARP inhibitors, which results in increased numbers of doublestrand DNA breaks (DSBs), is clinically effective in carcinomas that are deficient in homologous recombination (HR) 2 , the major error-free pathway that repairs DSBs by predominantly using the sister chromatid as a undamaged template for repair. Careful assessment of the repair capacity of tumour cells can thus influence treatment choice but can also prevent overtreatment, if upfront analysis would predict treatment unresponsiveness.…”

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confidence: 99%

BRCA1-associated structural variations are a consequence of polymerase theta-mediated end-joining

et al. 2020

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Failure to preserve the integrity of the genome is a hallmark of cancer. Recent studies have revealed that loss of the capacity to repair DNA breaks via homologous recombination (HR) results in a mutational profile termed BRCAness. The enzymatic activity that repairs HR substrates in BRCA-deficient conditions to produce this profile is currently unknown. We here show that the mutational landscape of BRCA1 deficiency in C. elegans closely resembles that of BRCA1-deficient tumours. We identify polymerase theta-mediated end-joining (TMEJ) to be responsible: knocking out polq-1 suppresses the accumulation of deletions and tandem duplications in brc-1 and brd-1 animals. We find no additional backup repair in HR and TMEJ compromised animals; non-homologous end-joining does not affect BRCAness. The notion that TMEJ acts as an alternative to HR, promoting the genome alteration of HR-deficient cells, supports the idea that polymerase theta is a promising therapeutic target for HR-deficient tumours.

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confidence: 99%

BRCA1-associated structural variations are a consequence of polymerase theta-mediated end-joining

et al. 2020

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“…Thus, PARP inhibition, as described by us for CDDP could induce cancer cell apoptosis by ROS‐mediated p53 activation. Consistently with this evidence, as pointed by Yi et al, a phase II clinical trial in gastric cancer showed an increased benefit by PARP inhibitors in patients presenting a functionally compromised ataxia‐telangiectasia mutated protein (ATM) . At this regard, it should be highlighted that ATM not only interferes with DNA repair but also modulates redox stress; in fact, cells lacking wild‐type ATM are prone to ROS accumulation and oxidative stress.…”

Section: Main Mechanisms Of Cancer Cell Death Mediated By the Parp Inmentioning

confidence: 59%

Section: Main Mechanisms Of Cancer Cell Death Mediated By the Parp Inmentioning

confidence: 99%

“…As reviewed by Yi et al ., clinical evaluation of PARP inhibitors in different trials and settings highlighted the role of mutations in DNA repair mechanisms as a prerequisite for a significant therapeutic efficacy. However, Yi et al . themselves found that the efficacy of PARP inhibitors, even weaker, is maintained also in the non‐BRCA and non‐HRD cancers, especially in combination regimens.…”

Section: Main Mechanisms Of Cancer Cell Death Mediated By the Parp Inmentioning

confidence: 99%

“…Finally, we believe that when discussing the benefit of PARP inhibitor, both in HRD‐ and non‐HRD‐mutated cancer, both if used alone or in combination (i.e., with alkylating agents such as temozolomide), as reviewed by Yi et al ., it should be important to note that these drugs not only affect DNA repair mechanisms in cancer cells, but they also act through different mechanisms (Table ) involving, in particular, the modulation of the energy metabolism, ATP synthesis and oxidative stress, which may contribute to their efficacy and synergism with other drugs. These pleiotropic activities mediated by PARP inhibitors could also provide new approaches for their use in several cancers that are resistant to current therapeutics.…”

Section: Main Mechanisms Of Cancer Cell Death Mediated By the Parp Inmentioning

confidence: 99%

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Antitumor efficacy of PARP inhibitors in homologous recombination deficient carcinomas

Cited by 24 publications

References 29 publications

BRCA1-associated structural variations are a consequence of polymerase theta-mediated end-joining

BRCA1-associated structural variations are a consequence of polymerase theta-mediated end-joining

The mechanism of cancer cell death by PARP inhibitors goes beyond DNA damage alone

Poly(ADP-ribose) polymerase (PARP) inhibitors for the treatment of ovarian cancer

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