Structural Characterization of Mucin O-Glycosylation May Provide Important Information to Help Prevent Colorectal Tumor Recurrence.

Adriana Mihalache,Jean-François Delplanque,Bélinda Ringot-Destrez,Cindy Wavelet,Sophie Groux-Degroote,Bertrand Nunes,Catherine Robbe-Masselot,Renaud Léonard,Pierre Gosset

doi:10.3389/fonc.2015.00217

Abstract

Although colorectal cancer is a preventable and curable disease if early stage tumors are removed, it still represents the second cause of cancer-related death worldwide. Surgical resection is the only curative treatment but once operated the patient is either subjected to adjuvant chemotherapy or not, depending on the invasiveness of the cancer and risks of recurrence. In this context, we investigated, by mass spectrometry (MS), alterations in the repertoire of glycosylation of mucins from colorectal tumors of various stages, grades, and recurrence status. Tumors were also compared with their counterparts in resection margins from the same patients and with healthy controls. The obtained data showed an important decrease in the level of expression of sialylated core 3-based O-glycans in tumors correlated with an increase in sialylated core 1 structures. No correlation was established between stages of the tumor samples and mucin O-glycosylation. However, with the notable exception of sialyl Tn antigens, tumors with recurrence presented a milder alteration of glycosylation profile than tumors without recurrence. These results suggest that mucin O-glycans from tumors with recurrence might mimic a healthier physiological situation, hence deceiving the immune defense system.

Highlights

Colorectal cancer (CRC) is the second leading cause of cancer-related death in the Western world [1]
To investigate potential differences in the profile of glycosylation of colon mucins during malignant transformation, colorectal tumor tissues were collected from 10 patients with tumors of different stages and grades (Table 1)
The ion at m/z 691, corresponding to the sialyl Tn antigen increased from 5.9% of total O-glycans in stage II, 6% in stage III, and 10.7% in stage IV

Summary

Introduction

Colorectal cancer (CRC) is the second leading cause of cancer-related death in the Western world [1]. It arises as the result of an accumulation of genetic and epigenetic alterations leading to transformation of normal colonic epithelium to invasive adenocarcinomas, due to disorders in cell proliferation and differentiation [2]. Metastatic CRC is frequently associated with recurrences within 5 years after surgery. In this context, there is an urgent need to identify biomarkers for early detection of CRC, to follow tumor development during the course of therapy and to predict recurrence

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Conclusion