DNA Damage/DNA Repair


The DNA in a human cell receives tens of thousands of damages per day due to both external (exogenous) and internal (endogenous) stress. The exogenous damages are caused by chemical contamination, UV light, ionizing radiation and alkylation/methylation etc, while the endogenous damages are coming from oxidation, alkylation and hydrolysis of bases etc. Since single strand and double strand breaks of DNA will occur after the damage, unrepaired DNA damage leads to cell senescent, apoptosis and malignancies etc. To overcome this threat, cell has developed DNA damage response, to detect DNA damage and mediate its repair.
DNA repair involves multiple mechanisms such as mismatch, base excision, and nucleotide excision repair etc. A group of proteins and pathways are participated in those processes. ATM/ATR kinases and DNA-PK are crucial for the detection of the DNA damage. Chromatin remodelers regulate chromatin accessibility for the DNA repair factors to function. RPA, Rad51 and the fanconi anemia proteins act directly on repairing the DNA damage. p53 network, the RAS GTPase superfamily, and the ubiquitin system also play important part in the DNA damage response. Aberrant DNA damage response is linked to aging, cancer and immune diseases.
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BA4145 SB-429201Summary: SB-429201 is a potent and selective inhibitor. -
BA4146 NCC-149Summary: NCC-149 is a selective inhibitor. -
BA4147 MPT0G211Summary: MPT0G211 is a potent, orally active and selective inhibitor. -
BA4148 HDAC-IN-40Summary: An effective alkoxyamide-based inhibitor. -
BA4150 CG347BSummary: CG347B is a selective inhibitor that is also involved in the synthesis of other metalloenzyme inhibitors. -
BA4151 AES-135Summary: AES-135, a hydroxamic acid-based pan-inhibitor, prolongs survival in an in situ mouse model of pancreatic cancer. -
BA4152 HDAC6-IN-26Summary: An inhibitor -
BA4153 PB131Summary: PB131 is a selective, brain barrier-penetrating inhibitor. -
BA4156 MOCPACSummary: A specific substrate. -
BA4157 PomiferinSummary: An inhibitor

