World Journal of Surgical Oncology (Nov 2012)

Novel cancerization marker, <it>TP53</it>, and its role in distinguishing normal tissue adjacent to cancerous tissue from normal tissue adjacent to benign tissue

  • Liu Guo-Yan,
  • Liu Kun-Hong,
  • Li Yin,
  • Pan Chao,
  • Su Ji-Qin,
  • Liao Hong-Feng,
  • Yv Ren-Xiang,
  • Li Zhao-Hui,
  • Yuan Li,
  • Zhang Huan-Jing,
  • Tzeng Chi-Meng,
  • Xiong Bing

DOI
https://doi.org/10.1186/1477-7819-10-252
Journal volume & issue
Vol. 10, no. 1
p. 252

Abstract

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Abstract Background The histopathological and molecular heterogeneity of normal tissue adjacent to cancerous tissue (NTAC) and normal tissue adjacent to benign tissue (NTAB), and the availability of limited specimens make deciphering the mechanisms of carcinogenesis challenging. Our goal was to identify histogenetic biomarkers that could be reliably used to define a transforming fingerprint using RNA in situ hybridization. Methods We evaluated 15 tumor-related RNA in situ hybridization biomarkers using tumor microarray and samples of seven tumor-adjacent normal tissues from 314 patients. Biomarkers were determined using comprehensive statistical methods (significance of support vector machine-based artificial intelligence and area under curve scoring of classification distribution). Results TP53 was found to be a most reliable index (P -7; area under curve >87%) for distinguishing NTAC from NTAB, according to the results of a significance panel (BCL10, BECN1, BRCA2, FITH, PTCH11 and TP53). Conclusions The genetic alterations in TP53 between NTAC and NTAB may provide new insight into the field of cancerization and tumor transformation.

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