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Endorsing cellular competitiveness in aberrant epithelium of oral submucous fibrosis progression: neighbourhood analysis of immunohistochemical attributes
Authors:Anji?Anura  author-information"  >  author-information__contact u-icon-before"  >  mailto:anji.anura@gmail.com"   title="  anji.anura@gmail.com"   itemprop="  email"   data-track="  click"   data-track-action="  Email author"   data-track-label="  "  >Email author,Anees?Kazi,Mousumi?Pal,Ranjan?Rashmi?Paul,Sanghamitra?Sengupta,Jyotirmoy?Chatterjee
Affiliation:1.School of Medical Science and Technology,Indian Institute of Technology Kharagpur,Kharagpur,India;2.Chair for Computer Aided Medical Procedures and Augmented Reality, Fakul?tfür Informatik,TechnischeUniversit?t München,Garchingbei München,Germany;3.Guru Nanak Institute of Dental Science and Research,Kolkata,India;4.Department of Biochemistry,University of Calcutta,Kolkata,India;5.Center for Stem Cell Research (A Unit of inStem, Bengaluru),Vellore,India
Abstract:Epithelial abnormality during the transformation of oral submucous fibrosis (OSF) into oral squamous cell carcinoma has been well studied and documented. However, the differential contribution of atrophy and hyperplasia for malignant potentiality of OSF is yet to be resolved. Existing diagnostic conjectures lack precise diagnostic attributes which may be effectively resolved by substantiation of specific molecular pathology signatures. Present study elucidates existence of cellular competitiveness in OSF conditions using computer-assisted neighbourhood analysis in quantitative immunohistochemistry (IHC) framework. The concept of field cancerization was contributory in finding correspondence among neighbouring cells of epithelial layers with reference to differential expression of cardinal cancer-related genes [c-Myc (oncogene), p53 (tumour suppressor), and HIF-1α (hypoxia regulator)] which are known to be important sensors in recognizing cellular competitive interface. Our analyses indicate that different states of OSF condition may be associated with different forms of competitiveness within epithelial neighbouring cells which might be responsible to shape the present and future of the pre-malignant condition. Analytical findings indicated association of atrophic epithelium with stress-driven competitive environment having low c-Myc, high-p53, and stable HIF-1α (the looser cells) which undergo apoptosis. Whereas, the cells with high c-Myc+ (winner cells) give rise to hyperplastic epithelium via possible mutation in p53. The epithelial dysplasia plausibly occurs due to clonal expansion of c-Myc and p53 positive supercompetitor cells. Present study proposes quantitative IHC along with neighbourhood analysis which might help us to dig deeper on to the interaction among epithelial cell population to provide a better understanding of field cancerization and malignant transformation of pre-malignancy.
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