| Literature DB >> 29652830 |
Ugo Testa1, Elvira Pelosi2, Germana Castelli3.
Abstract
Colon cancer is the third most common cancer worldwide. Most colorectal cancer occurrences are sporadic, not related to genetic predisposition or family history; however, 20-30% of patients with colorectal cancer have a family history of colorectal cancer and 5% of these tumors arise in the setting of a Mendelian inheritance syndrome. In many patients, the development of a colorectal cancer is preceded by a benign neoplastic lesion: either an adenomatous polyp or a serrated polyp. Studies carried out in the last years have characterized the main molecular alterations occurring in colorectal cancers, showing that the tumor of each patient displays from two to eight driver mutations. The ensemble of molecular studies, including gene expression studies, has led to two proposed classifications of colorectal cancers, with the identification of four/five non-overlapping groups. The homeostasis of the rapidly renewing intestinal epithelium is ensured by few stem cells present at the level of the base of intestinal crypts. Various experimental evidence suggests that colorectal cancers may derive from the malignant transformation of intestinal stem cells or of intestinal cells that acquire stem cell properties following malignant transformation. Colon cancer stem cells seem to be involved in tumor chemoresistance, radioresistance and relapse.Entities:
Keywords: adenomatous polyp; cancer stem cells; colorectal cancer; gene expression profiling; gene sequencing; serrated polyp; tumor xenotrasplantation assay
Year: 2018 PMID: 29652830 PMCID: PMC6024750 DOI: 10.3390/medsci6020031
Source DB: PubMed Journal: Med Sci (Basel) ISSN: 2076-3271