Forty years of cisplatin-based chemotherapy in muscle-invasive bladder cancer: are we understanding how, who and when?
Julian SchardtBeat RothRoland SeilerPublished in: World journal of urology (2018)
We elaborate biomarkers at the methylation, DNA, RNA and protein levels and give their current status in clinical trials and/or their implementation in daily clinical practice. In particular, detection of alterations in DNA damage repair pathways as well as molecular subtypes seems to be a promising method for identifying responders to NAC. Furthermore, we illustrate liquid-based biomarkers. Circulating tumor DNA (ctDNA) in patient blood and urine appear to offer an elegant way for biological characterization of MIBC. Recent data show that the presence of ctDNA is limited in patients with localized MIBC being considered for NAC. At this disease stage, ctDNA in patient urine may be more promising for the genomic characterization of MIBC. However, ctDNA in blood or urine has not yet been rigorously investigated in this clinical context.
Keyphrases
- circulating tumor
- cell free
- circulating tumor cells
- dna damage
- clinical trial
- muscle invasive bladder cancer
- transcription factor
- current status
- clinical practice
- case report
- primary care
- oxidative stress
- physical activity
- electronic health record
- dna methylation
- ionic liquid
- genome wide
- dna repair
- copy number
- phase ii
- big data
- randomized controlled trial
- open label
- amino acid
- locally advanced
- high resolution
- artificial intelligence
- label free
- double blind