| Literature DB >> 23965959 |
Dora Colussi1, Giovanni Brandi, Franco Bazzoli, Luigi Ricciardiello.
Abstract
Research conducted during the past 30 years has increased our understanding of the mechanisms involved in colorectal cancer initiation and development. The findings have demonstrated the existence of at least three pathways: chromosomal instability, microsatellite instability and CpG island methylator phenotype. Importantly, new studies have shown that inflammation and microRNAs contribute to colorectal carcinogenesis. Recent data have demonstrated that several genetic and epigenetic changes are important in determining patient prognosis and survival. Furthermore, some of these mechanisms are related to patients' response to drugs, such as aspirin, which could be used for both chemoprevention and treatment in specific settings. Thus, in the near future, we could be able to predict disease behavior based on molecular markers found on tumors, and direct the best treatment options for patients.Entities:
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Year: 2013 PMID: 23965959 PMCID: PMC3759916 DOI: 10.3390/ijms140816365
Source DB: PubMed Journal: Int J Mol Sci ISSN: 1422-0067 Impact factor: 5.923
Molecular markers and implications for disease behavior.
| Gene | Effect on disease | Ref. |
|---|---|---|
| Poor prognosis | [ | |
| Metastatic disease; poor prognosis; increased cancer specific mortality | [ | |
| Better survival among p-ERK positive | [ | |
| Better survival among non obese | [ | |
| Better survival for patients >60 yrs | [ | |
| Increased cancer specific mortality | [ | |
| Loss in non MSI → decreased survival | [ | |
| Increased survival among chronic aspirin users | [ | |
| Young age of onset and increased cancer and overall mortality | [ | |
| High colorectal cancer-specific mortality | [ | |
| High colorectal cancer and overall mortality | [ | |
| Better prognosis and survival than CIN/MSS | [ | |
| Low colon cancer and overall mortality | [ | |
| High cancer-specific mortality | [ | |
| Low colon cancer-specific mortality | [ | |
| Poor survival among caucasians with stage IV and poor survival in blacks with stages I and II CRC | [ | |
| Poor prognosis in patients with stage IV CRC | [ | |
| Increased risk of CRC development, lower risk among those taking aspirin | [ | |
| Increased risk of CRC development, advanced CRC stage, and a worse prognosis | [ | |
| Association with increased risk of colorectal cancer, in particular in lean individuals | [ |