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YearIMPACT-FACTOR
2022  1,200
2021  1,540
2020  1,374
2019  1,023
2018  0,932
2017  0,977
2016  0,799
2015  0,662
2014  0,740
2013  0,739
2012  0,637
2011  0,658
2010  0,654
2009  0,570
2008  0,849
2007  0,805
2006  0,330
2005  0,435
2004  0,623
2003  0,567
2002  0,641
2001  0,490
2000  0,477
1999  0,762
1998  0,785
1997  0,507
1996  0,518
1995  0,502
Vol 56(2022) N 2 p. 251-256; DOI 10.1134/S0026893322020066 Full Text

E. Iscan1,2*, G. Karakülah1,2, U. Ekin1,2, M. Ozturk1,3, H. Uzuner1,2, A. Suner4

TAp73α is Upregulated in the Most Common Human Cancers

1Izmir Biomedicine and Genome Center, Izmir, Turkey
2Izmir International Biomedicine and Genome Institute, Dokuz Eylul University, Izmir, 35330 Turkey
3Faculty of Medicine, Izmir Tinaztepe University, Izmir, Turkey
4Department of Biostatistics and Medical Informatics, Faculty of Medicine, Ege University, Izmir, 35100 Turkey

*evin.iscan@deu.edu.tr
Received - 2021-04-07; Revised - 2021-06-14; Accepted - 2021-07-19

The transcription factor p73 is a member of the p53 tumor suppressor gene family and one of the key regulators of apoptosis. TP73 gene encodes two protein isoforms classes with diverse functions, TAp73 and DNp73, and TAp73 expression in tumor tissues is altered. Unlike the TP53 gene, TP73 is not mutated in cancers. Here, we sought to explore the expression of p73 isoforms across eight major cancer types using the publicly available data deposited at the GDC data portal and the TSVdb database. Our results showed that TAp73α is overexpressed in breast invasive carcinoma, stomach adenocarcinoma, lung squamous cell carcinoma, colon adenocarcinoma, and esophageal carcinoma tumors, whereas the expression of DNp73 isoforms is downregulated in breast invasive carcinoma (DNp73α,β,γ), Prostate Adenocarcinoma (DNp73β), Lung Adenocarcinoma (DNp73α), Lung Squamous Cell Carcinoma (DNp73α) tumors. In summary, this study revealed that TAp73α has higher expression than the DNp73 isoforms in several cancer types.

p73, cancer, TCGA splicing variants analysis



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