Chromatin Stability as a Target for Cancer Treatment.
Katerina V GurovaPublished in: BioEssays : news and reviews in molecular, cellular and developmental biology (2019)
In this essay, I propose that DNA-binding anti-cancer drugs work more via chromatin disruption than DNA damage. Success of long-awaited drugs targeting cancer-specific drivers is limited by the heterogeneity of tumors. Therefore, chemotherapy acting via universal targets (e.g., DNA) is still the mainstream treatment for cancer. Nevertheless, the problem with targeting DNA is insufficient efficacy due to high toxicity. I propose that this problem stems from the presumption that DNA damage is critical for the anti-cancer activity of these drugs. DNA in cells exists as chromatin, and many DNA-targeting drugs alter chromatin structure by destabilizing nucleosomes and inducing histone eviction from chromatin. This effect has been largely ignored because DNA damage is seen as the major reason for anti-cancer activity. I discuss how DNA-binding molecules destabilize chromatin, why this effect is more toxic to tumoral than normal cells, and why cells die as a result of chromatin destabilization.
Keyphrases
- dna damage
- dna binding
- transcription factor
- induced apoptosis
- oxidative stress
- dna repair
- circulating tumor
- gene expression
- cell cycle arrest
- cell free
- single molecule
- genome wide
- cancer therapy
- papillary thyroid
- dna methylation
- endoplasmic reticulum stress
- squamous cell carcinoma
- drug induced
- single cell
- locally advanced
- pi k akt
- lymph node metastasis