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Cosmc transfection decreases malignant behavior of Tn(+) cells and enhances sensitivity to apoptosis when induced by Apo2L/TRAIL via alteration of O-glycan structure

Cosmc mutations may cause abnormal O-glycosylation and result in Tn antigen expression. In the current study, it was discovered that proliferation and migration of Tn+ cells (Jurkat T and LS174T-Tn(+) cells) with mutant Cosmc decreased after transfected Cosmc, and their sensitivity to apoptosis indu...

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Detalles Bibliográficos
Autores principales: Ding, Ruisong, Hu, Xingyou, Hu, Wen, Du, Zhenzhen, Huang, Panpan, Wang, Mengyang, Sheng, Jiaoyue, Ma, Yanchao, Wang, Ailing, Luan, Xiying, Dong, Menghua, Cao, Qizhi, Zou, Yanfen, Hu, Tao
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8549606/
https://www.ncbi.nlm.nih.gov/pubmed/34644263
http://dx.doi.org/10.18632/aging.203633
Descripción
Sumario:Cosmc mutations may cause abnormal O-glycosylation and result in Tn antigen expression. In the current study, it was discovered that proliferation and migration of Tn+ cells (Jurkat T and LS174T-Tn(+) cells) with mutant Cosmc decreased after transfected Cosmc, and their sensitivity to apoptosis induced by Apo2L/TRAIL increased. Core 1-, 2-, and 3-derived O-glycans were absent in Tn(+) cells. After Cosmc transfection, normal extended core 1-derived O-glycans appeared and were accompanied by increased T-synthase activity. Core 2-derived O-glycans appeared in transfected LS174T-Tn(+) cells, and their structural types and levels were lower than those in LS174T-Tn(−) cells. Core 3-derived O-glycans were present only in LS174T-Tn(−) cells. The activity of C3GnT in LS174T-Tn(+) cells was lower than that in LS174T-Tn(−) cells, and it was absent in Jurkat T cells. Cosmc transfection did not alter C3GnT activity or core 3-derived O-glycans in Jurkat T and LS174T-Tn(+) cells. The results demonstrated that the composition and structure of O-glycans were different among various Tn(+) cells, which not only affected cell malignant behavior but also modulated sensitivity to apoptotic stimuli. Thus, Cosmc transfection may effectively decrease the malignant behavior of Tn(+) tumor cells and enhance their sensitivity to apoptosis when induced by Apo2L/TRAIL through modification of O-glycans.