2D-DIGE-Based Proteomic Profiling with Validations Identifies Vimentin as a Secretory Biomarker Useful for Early Detection and Poor Prognosis in Oral Cancers

Author:

Sivagnanam Ananthi1ORCID,Shyamsundar Vidyarani2ORCID,Kesavan Pallavi1ORCID,Krishnamurthy Arvind3ORCID,Thangaraj Soundara Viveka1ORCID,Venugopal Divyambika Catakapatri4ORCID,Kasirajan Hemashree5,Ramani Pratibha5,Sarma Vinutha Rachapudi6ORCID,Ramshankar Vijayalakshmi1ORCID

Affiliation:

1. Department of Preventive Oncology (Research), Cancer Institute (WIA), Adyar, Chennai, 600020 Tamil Nadu, India

2. Centre for Oral Cancer Prevention and Research, Sree Balaji Dental College and Hospital, Pallikaranai, Chennai, 600100 Tamil Nadu, India

3. Department of Surgical Oncology, Cancer Institute (WIA), Adyar, Chennai, 600020 Tamil Nadu, India

4. Department of Oral Medicine and Radiology, Sri Ramachandra Institute of Higher Education and Research (DU), Porur, 600016, Chennai, Tamil Nadu, India

5. Department of Oral Pathology and Maxillofacial Pathology, Saveetha Dental College, Velappanchavadi, 600077, Chennai, Tamil Nadu, India

6. Public Health Foundation of India, New Delhi 110017, India

Abstract

Oral tongue squamous cell carcinoma (OTSCC) is an aggressive cancer with high morbidity and mortality rates, despite multimodality management. There are currently no clinically relevant molecular markers that identify patients at higher risk of recurrence and failure. We undertook 2D-DIGE proteomic profiling to study the differentially expressed proteins in OTSCC evaluating their role in prognosis. 2D-DIGE coupled with tandem mass spectrometry was performed on tissues obtained from early staged OTSCC along with its paired apparently adjacent normal tissue samples ( n = 10 ). Top upregulated protein was validated using immunohistochemistry ( n = 345 ), comprising of retrospective early stage OTSCC ( n = 150 ) and prospective series of oral precancers, normal, and oral cancers ( n = 195 ). Saliva samples collected from oral cancer and precancer samples were analyzed by ELISA ( n = 146 ). We found statistically significant differential expression in 151 proteins out of 700 proteins quantified. Top ten differentially regulated proteins were identified using mass spectrometry analysis. We found vimentin, the mesenchymal protein, to be the most upregulated protein in tongue tumor tissues compared to adjacent apparent normal tissues. Vimentin was found to be significantly overexpressed in oral precancers along with cancers compared to normal tissues. The vimentin expression correlated significantly with differentiated states of oral precancers and cancers. Vimentin was also detected at significantly higher levels in saliva collected from oral precancer and cancer patients compared to normal healthy volunteers. Validation of vimentin in an independent series of retrospective early staged OTSCC showed that the vimentin expression is significantly associated with treatment failures and poorer DFS. The vimentin expression is useful as both poor prognostic and early detection marker in oral cancer. Vimentin detection in saliva can be a diagnostic test to detect oral precancers that may have malignant potential, needing closer follow-up, and disease monitoring.

Funder

Government of India

Publisher

Hindawi Limited

Subject

Oncology

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