DNA Damage-Inducing Anticancer Therapies: From Global to Precision Damage

Reuvers, Thom G. A.; Kanaar, Roland; Nonnekens, Julie

doi:10.3390/cancers12082098

Cited by 59 publications

(52 citation statements)

References 149 publications

(181 reference statements)

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“…In the same model, shikonin caused DNA damage [ 142 ] ( Table S4 ), as observed in several cancer cells in vitro [ 142 , 159 , 160 ] ( Table 2 ), thus configuring itself as a possible mutagen compound. This aspect is certainly to be taken into account in the evaluation of the toxicological profile of shikonin, even if it is worth noting that the antitumor activity of several anticancer drugs is based on DNA-damage induction [ 161 ]. In BALB/c nude mouse xenograft model of human osteosarcoma, shikonin reduced tumor growth, increased RIP1/3 expression, and reduced lung metastasis thus suggesting an antimetastatic activity for shikonin [ 138 ] ( Table S4 ).…”

Section: Necroptosismentioning

confidence: 99%

“…However, attention must be paid since the role of necroptosis in cancer metastatization is controversial. Strilic et al reported that tumor cells-induced necroptosis of endothelial cells promotes cancer cells extravasation and metastatization through interaction with DR6 (death receptor 6) [ 162 ], hence showing that necroptosis could promote cancer cell metastatization [ 161 ]…”

Section: Necroptosismentioning

confidence: 99%

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Natural Products as Inducers of Non-Canonical Cell Death: A Weapon against Cancer

Greco

Catanzaro

Fimognari

2021

Cancers

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Apoptosis has been considered the main mechanism induced by cancer chemotherapeutic drugs for a long time. This paradigm is currently evolving and changing, as increasing evidence pointed out that antitumor agents could trigger various non-canonical or non-apoptotic cell death types. A considerable number of antitumor drugs derive from natural sources, both in their naturally occurring form or as synthetic derivatives. Therefore, it is not surprising that several natural compounds have been explored for their ability to induce non-canonical cell death. The aim of this review is to highlight the potential antitumor effects of natural products as ferroptosis, necroptosis, or pyroptosis inducers. Natural products have proven to be promising non-canonical cell death inducers, capable of overcoming cancer cells resistance to apoptosis. However, as discussed in this review, they often lack a full characterization of their antitumor activity together with an in-depth investigation of their toxicological profile.

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Section: Necroptosismentioning

confidence: 99%

Section: Necroptosismentioning

confidence: 99%

Natural Products as Inducers of Non-Canonical Cell Death: A Weapon against Cancer

Greco

Catanzaro

Fimognari

2021

Cancers

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“…Cytotoxic chemotherapy causes severe DNA damage directly by induction of breaks or indirectly due to the formation of reactive oxygen species (ROS) and ultimately induce cell death 34,35 . In responses to DNA damage, cells recruit DNA repair factors to upregulate mutagenic repair pathways that to maintain survival 36 .…”

Section: Discussionmentioning

confidence: 99%

Metformin Sensitizes Osteosarcoma Cells to Chemotherapy Through IGF-1R/miR-610/FEN1 Pathway

Dong¹,

Zhu³

et al. 2021

Preprint

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Background: Due to constitutive or acquired non-sensitive to cytotoxic agents, the prognosis of osteosarcoma remains unfavorable. It’s has been proved that metformin could enhance the chemosensitivity of cancer cells to anticancer drugs. A novel finding states that IGF-1R involves in cancer chemoresistance, However, whether IGF-1R play a role in metformin-induced osteosarcoma chemosensitivity is incompletely understood. Hence, the current study aimed to elucidate the role of metformin in OS cell chemosensitivity modulation to identify the underlying mechanism of metformin regulating the IGF-1R/miR-610/FEN1 signaling.Methods: Immunohistochemistry and qRT-PCR were used to evaluate the expression pattern of IGF-1R, miR-610 and FEN1 in osteosarcoma and paired normal tissues. Western blot and qRT-PCR were performed to determine changes in expression of key molecules in the IGF-1R/miR-610/FEN1 signaling pathway after various treatments. The direct modulation between miR-610 and FEN1 was monitored by luciferase reporter assay. Osteosarcoma cell sensitivity to chemotherapy was detected by MTS assay. In vivo experiments were conducted to further verify the role of the metformin in the chemosensitivity modulation of OS cells to ADM.Results: We found that IGF-1R, miR-610 and FEN1 were abberently expressed in osteosarcoma, and participated in apoptosis modulation (p < 0.05). We found that this effect was abated by metformin treatment. Luciferase reporter assays confirmed that FEN1 is a direct target of miR-610. Moreover, we observed that metformin treatment decreased IGF-1R and FEN1, but elevated miR-610 expression. Metformin sensitized OS cells to cytotoxic agents, while overexpression of FEN1 compromised the sensitizing effects of metformin partly. Furthermore, metformin was observed to enforce the ADM treatment effect in nude mice xenograft models.Conclusions: Overall, metformin enhanced the sensitivity of OS cells to cytotoxic agents via the IGF-1R/miR-610/FEN1 signaling axis, highlighting the capacity of metformin as an adjunct to the chemotherapy of OS.

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“…To maintain genomic integrity of normal cells, damaged DNA induces checkpoints (e.g. p53-p21)-controlled cell cycle arrest until that DNA repair is achieved or cell death is launched (25). Under this premise, malignant cells might sustain in G0 phase by activating other epigenetics or genetics-dependent quiescence programs (26).…”

Section: Discussionmentioning

confidence: 99%

Gene Panel of Persister Cells as a Prognostic Indicator for Tumor Repopulation After Radiation

et al. 2020

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Tumor repopulation during cycles of radiotherapy limits the radio-response in ensuing cycles and causes failure of treatment. It is thus of vital importance to unveil the mechanisms underlying tumor repopulating cells. Increasing evidence suggests that a subpopulation of drug-tolerant persister cancer cells (DTPs) could survive the cytotoxic treatment and resume to propagate. Whether these persister cells contribute to development of radio-resistance remains elusive. Based on the genetic profiling of DTPs by integrating datasets from Gene Expression Omnibus database, this study aimed to provide novel insights into tumor-repopulation mediated radio-resistance and identify predictive biomarkers for radio-response in clinic. A prognostic risk index, grounded on four persister genes (LYNX1, SYNPO, GADD45B, and PDLIM1), was constructed in non-small-cell lung cancer patients from The Cancer Genome Atlas Program (TCGA) using stepwise Cox regression analysis. Weighted gene co-expression network analysis further confirmed the interaction among persister-gene based risk score, radio-response and overall survival time. In addition, the predictive role of risk index was validated in vitro and in other types of TCGA patients. Gene set enrichment analysis was performed to decipher the possible biological signaling, which indicated that two forces behind persister cells, stress response and survival adaptation, might fuel the tumor repopulation after radiation. Targeting these persister cells may represent a new prognostic and therapeutic approach to enhance radio-response and prevent radio-resistance induced by tumor repopulation.

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DNA Damage-Inducing Anticancer Therapies: From Global to Precision Damage

Cited by 59 publications

References 149 publications

Natural Products as Inducers of Non-Canonical Cell Death: A Weapon against Cancer

Natural Products as Inducers of Non-Canonical Cell Death: A Weapon against Cancer

Metformin Sensitizes Osteosarcoma Cells to Chemotherapy Through IGF-1R/miR-610/FEN1 Pathway

Gene Panel of Persister Cells as a Prognostic Indicator for Tumor Repopulation After Radiation

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