4.6 Review

The role of transcription factor Yin Yang-1 in colorectal cancer

Journal

CANCER MEDICINE
Volume 12, Issue 10, Pages 11177-11190

Publisher

WILEY
DOI: 10.1002/cam4.5745

Keywords

colorectal cancer; transcription factor; tumor promotion; tumor suppression; Yin Yang-1

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YY1 is highly expressed in colorectal cancer and is widely recognized as an oncogenic factor throughout the course of the disease. Future studies should take the influence of therapeutic regimens into consideration.
BackgroundYin Yang-1 (YY1) is identified as a transcription factor with multiple functions. However, the role of YY1 in tumorigenesis remains controversial and its regulatory effects may depend upon not only cancer types, but also its interacting partners, chromatin structure, and the context in which it acts. It has been detected that YY1 was highly expressed in colorectal cancer (CRC). Intriguingly, many YY1-repressed genes exhibit tumor suppressive potential while YY1 silencing is related to chemotherapy resistance. Therefore, it is crucial to meticulously explore YY1 protein structure and the dynamic alteration of its interactome in each cancer type. This review attempts to describe the structure of YY1, summarize the mechanism that influence the expression level of YY1 and also highlight the recent advances in our understanding of regulatory insights of YY1 functions in CRC. MethodsRelated studies were identified through scoping search of PubMed, Web of science, Scopus and Emhase concerning the terms of colorectal cancer, colorectal carcinoma or CRC with YY1. The retrieval strategy included title, abstract, and keywords with no language limitations. All the included articles were categorized depending on the mechanisms they explored. ResultsIn total, 170 articles were identified for further screening. After removing the duplication, not relevant outcomes and review articles, 34 were finally included in the review. Among them, 10 articles revealed the reasons of YY1 high expression in CRC, 13 articles explored YY1 function in CRC, and 11 articles fell into both aspects. In addition, we also summarized 10 clinical trials concerning the expression and activity of YY1 in various diseases, which offers a hint for future application. ConclusionsYY1 is highly expressed in CRC and broadly recognized as an oncogenic factor during the whole course of CRC. Sporadic controversial views are raised in term of CRC treatment, reminding us that future studies should take the influence of therapeutic regimens into concern.

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