Inhibition of Glutamate‐to‐Glutathione Flux Promotes Tumor Antigen Presentation in Colorectal Cancer Cells (Journal Article) (2025)

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    • MLA

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      Yu, Tao, Van_der_Jeught, Kevin, Zhu, Haiqi, Zhou, Zhuolong, Sharma, Samantha, Liu, Sheng, Eyvani, Haniyeh, So, Ka Man, Singh, Naresh, Wang, Jia, Sandusky, George E, Liu, Yunlong, Opyrchal, Mateusz, Cao, Sha, Wan, Jun, Zhang, Chi, and Zhang, Xinna. Inhibition of Glutamate‐to‐Glutathione Flux Promotes Tumor Antigen Presentation in Colorectal Cancer Cells. Retrieved from https://par.nsf.gov/biblio/10580208. Advanced Science 12.1 Web. doi:10.1002/advs.202310308.

    • APA

      Cite: APA Format

      Yu, Tao, Van_der_Jeught, Kevin, Zhu, Haiqi, Zhou, Zhuolong, Sharma, Samantha, Liu, Sheng, Eyvani, Haniyeh, So, Ka Man, Singh, Naresh, Wang, Jia, Sandusky, George E, Liu, Yunlong, Opyrchal, Mateusz, Cao, Sha, Wan, Jun, Zhang, Chi, & Zhang, Xinna. Inhibition of Glutamate‐to‐Glutathione Flux Promotes Tumor Antigen Presentation in Colorectal Cancer Cells. Advanced Science, 12 (1). Retrieved from https://par.nsf.gov/biblio/10580208. https://doi.org/10.1002/advs.202310308

    • Chicago

      Cite: Chicago Format

      Yu, Tao, Van_der_Jeught, Kevin, Zhu, Haiqi, Zhou, Zhuolong, Sharma, Samantha, Liu, Sheng, Eyvani, Haniyeh, So, Ka Man, Singh, Naresh, Wang, Jia, Sandusky, George E, Liu, Yunlong, Opyrchal, Mateusz, Cao, Sha, Wan, Jun, Zhang, Chi, and Zhang, Xinna. "Inhibition of Glutamate‐to‐Glutathione Flux Promotes Tumor Antigen Presentation in Colorectal Cancer Cells". Advanced Science 12 (1). Country unknown/Code not available: Wiley. https://doi.org/10.1002/advs.202310308. https://par.nsf.gov/biblio/10580208.

    • BibTeX

      Cite: BibTeX Format

      @article{osti_10580208,
      place = {Country unknown/Code not available}, title = {Inhibition of Glutamate‐to‐Glutathione Flux Promotes Tumor Antigen Presentation in Colorectal Cancer Cells}, url = {https://par.nsf.gov/biblio/10580208}, DOI = {10.1002/advs.202310308}, abstractNote = {Abstract Colorectal cancer (CRC) cells display remarkable adaptability, orchestrating metabolic changes that confer growth advantages, pro‐tumor microenvironment, and therapeutic resistance. One such metabolic change occurs in glutamine metabolism. Colorectal tumors with high glutaminase (GLS) expression exhibited reduced T cell infiltration and cytotoxicity, leading to poor clinical outcomes. However, depletion of GLS in CRC cells has minimal effect on tumor growth in immunocompromised mice. By contrast, remarkable inhibition of tumor growth is observed in immunocompetent mice when GLS is knocked down. It is found that GLS knockdown in CRC cells enhanced the cytotoxicity of tumor‐specific T cells. Furthermore, the single‐cell flux estimation analysis (scFEA) of glutamine metabolism revealed that glutamate‐to‐glutathione (Glu‐GSH) flux, downstream of GLS, rather than Glu‐to‐2‐oxoglutarate flux plays a key role in regulating the immune response of CRC cells in the tumor. Mechanistically, inhibition of the Glu‐GSH flux activated reactive oxygen species (ROS)‐related signaling pathways in tumor cells, thereby increasing the tumor immunogenicity by promoting the activity of the immunoproteasome. The combinatorial therapy of Glu‐GSH flux inhibitor and anti‐PD‐1 antibody exhibited a superior tumor growth inhibitory effect compared to either monotherapy. Taken together, the study provides the first evidence pointing to Glu‐GSH flux as a potential therapeutic target for CRC immunotherapy.}, journal = {Advanced Science}, volume = {12}, number = {1}, publisher = {Wiley}, author = {Yu, Tao and Van_der_Jeught, Kevin and Zhu, Haiqi and Zhou, Zhuolong and Sharma, Samantha and Liu, Sheng and Eyvani, Haniyeh and So, Ka Man and Singh, Naresh and Wang, Jia and Sandusky, George E and Liu, Yunlong and Opyrchal, Mateusz and Cao, Sha and Wan, Jun and Zhang, Chi and Zhang, Xinna}, }

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Inhibition of Glutamate‐to‐Glutathione Flux Promotes Tumor Antigen Presentation in Colorectal Cancer Cells (Journal Article) (2025)
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