Helix-distorting DNA lesions, for example UV-induced cyclopyrimidine dimes T∩T) are recognized throughout the genome by the protein complex XPC-HR23B. Lesion recognition is facilitated by the DDB complex (DDB1 and XPE/DDB2) specifically in the case of DNA damage caused by UV radiation. DDB is part of the Cul4A complex, which ubiquitylates XPC, leading to its stable association with damaged DNA. This subpathway of NER is called global genome NER (GG-NER). Lesions on the transcribed strand of DNA, which block RNA polymerase II-mediated transcription, activate transcription-coupled NER (TC-NER). TC-NER is facilitated by CSB, CSA and XAB2. Either XPC in GG-NER or CSB and CSA in TC-NER recruit the transcription factor TFIIH to the site of damage. XPG stabilizes TFIIH. The XPB and XPD subunits of TFIIH are helicases that unwind the DNA around the lesion. XPA and RPA then bind and stabilize this unwound intermediate and recruit XPF-ERCC1. This endonuclease incises the damaged strand of DNA 5’ to the lesion, while XPG makes the 3’ incision. The lesion is removed in a single-stranded oligonucleotide, leaving behind a gap, which is filled by the replication machinery comprised of polymerase δ and ε, PCNA, RPA and RFC. The DNA backbone is sealed by DNA Ligase I or DNA Ligase 3-XRCC1.