Dietary palmitic acid inhibits colorectal cancer progression through enhancing bisecting GlcNAc
Lei Lei, Juan Tang, Yuejiao Lv, Bingyi Jia, Wenqing Cai, Shuangshuang Sheng, Keying Li, Zhiwen Shi, Ning Fan, Zengqi Tan, Xiang Li, Feng Guan
Lei Lei, Juan Tang, Yuejiao Lv, Bingyi Jia, Wenqing Cai, Shuangshuang Sheng, Keying Li, Zhiwen Shi, Ning Fan, Zengqi Tan, Xiang Li, Feng Guan
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Research Article Gastroenterology Oncology

Dietary palmitic acid inhibits colorectal cancer progression through enhancing bisecting GlcNAc

Abstract

Glycosylation changes are pivotal in colorectal cancer (CRC) development. The role of bisecting GlcNAc, a specific N-glycosylation type catalyzed by glycosyltransferase MGAT3, in CRC progression remains elusive. Previous studies indicated that dietary interventions can be beneficial for patients with certain congenital disorders of glycosylation. However, the impact of dietary fatty acids, such as palmitic acid (PA), on glycosylation regulation remains largely unclear. Here, we observed markedly decreased levels of bisecting GlcNAc and MGAT3 in colonic tissues of CRC patients. Downregulation of bisecting GlcNAc in CRC cells increased cell proliferation, migration, and invasion, while decreasing apoptosis. Moreover, a PA-rich diet inhibited CRC carcinogenesis in azoxymethane/dextran sodium sulfate–induced CRC mice by elevating bisecting GlcNAc levels. However, in Mgat3fl/fl Villin-Cre mice the inhibitory effects of the PA-rich diet were abolished. Intact glycopeptide analysis revealed that PA enhanced the bisecting GlcNAc modification on desmoglein 2 (DSG2). Additionally, DSG2 was identified to inhibit CRC carcinogenesis through the EGFR/AKT signaling pathway. In conclusion, dietary PA suppresses CRC carcinogenesis by regulating bisecting GlcNAc modification on DSG2, providing a direct mechanistic link between dietary fatty acids and CRC.

Authors

Lei Lei, Juan Tang, Yuejiao Lv, Bingyi Jia, Wenqing Cai, Shuangshuang Sheng, Keying Li, Zhiwen Shi, Ning Fan, Zengqi Tan, Xiang Li, Feng Guan

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Figure 4

PA increases bisecting GlcNAc levels in vitro and in vivo.

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PA increases bisecting GlcNAc levels in vitro and in vivo. HCT116 cells ...
HCT116 cells were treated with PA, OA, LA, or BSA for 48 hours. (A) Bisecting GlcNAc levels assessed by lectin blotting. (B) Apoptosis detected by flow cytometry. (C) Migratory and invasive capacities assessed by Transwell assays. (D) Scheme of the animal experimental design. (E) Measurement of mouse body weight. (F) Quantification of colon tumors in mice (n = 9–12 mice per group). (G) H&E and IHC staining for Pcna, Mgat3, and bisecting GlcNAc in colonic tissues (n = 9–12 mice per group, scale bars: 50 μm). (H) mRNA expression of Mgat3, Pcna, and Mki67 detected by qRT-PCR (n = 8–12 mice per group). (I) Bisecting GlcNAc levels in colonic tissues assessed by lectin blotting. The results are presented as mean ± SEM. Analysis of multiple groups was performed by 1-way ANOVA followed by Tukey’s multiple-comparison test. The cell culture experiments were performed with at least 3 independent repeats. NS, not significant. *P < 0.05; **P < 0.01; ***P < 0.001.