| Literature DB >> 28958617 |
Maria Laura Martin1, Zhaoshi Zeng2, Mohammad Adileh2, Adrian Jacobo3, Christy Li4, Efsevia Vakiani5, Guoqiang Hua6, Lixing Zhang7, Adriana Haimovitz-Friedman8, Zvi Fuks8, Richard Kolesnick9, Philip B Paty10.
Abstract
Stem cells of the small and large intestine are marked by expression of the Wnt target gene LGR5, a leucine-rich-repeat-containing G protein-coupled receptor. Previous studies reported increased expression of LGR5 in human colorectal cancer (CRC) compared to normal tissue either by immunohistochemistry or in situ hybridization (ISH). However, as these studies were semi-quantitative they did not provide a numerical estimate of the magnitude of this effect. While we confirm that LGR5+ cells are exclusively located at the base of normal human small and large intestinal crypts, representing approximately 6% of total crypt cells, we show this cell population is 10-fold expanded in all grades of CRC, representing as much as 70% of the cells of tumor crypt-like structures. This expansion of the LGR5 compartment coincides with maintenance of crypt-like glandular structure (adenomas, and well and moderately differentiated adenocarcinomas), and is reduced in poorly differentiated CRC, where crypt-like glandular architecture is lost, accompanied by reduced epithelial terminal differentiation. Altogether these results indicate that LGR5+ cell expansion is a hallmark of CRC tumorigenesis occurring during progression to adenoma, supporting CRC as a stem cell disease with implications for CRC therapy.Entities:
Keywords: Colorectal cancer; In situ hybridization; LGR5(+); Stem cells
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Year: 2017 PMID: 28958617 PMCID: PMC5766032 DOI: 10.1016/j.cellsig.2017.09.018
Source DB: PubMed Journal: Cell Signal ISSN: 0898-6568 Impact factor: 4.315