Excess Potassium Promotes Autophagy to Maintain the Immunosuppressive Capacity of Myeloid-Derived Suppressor Cells Independent of Arginase 1

Authors

Ramesh Thylur Puttalingaiah, LSU Health Sciences Center - New OrleansFollow
Matthew J. Dean, LSU Health Sciences Center - New OrleansFollow
Liqin Zheng, LSU Health Sciences Center - New OrleansFollow
Phaethon Philbrook, LSU Health Sciences Center - New OrleansFollow
Dorota Wyczechowska, LSU Health Sciences Center - New OrleansFollow
Timothy Kayes, LSU Health Sciences Center - New OrleansFollow
Luis Del Valle, LSU Health Sciences Center - New OrleansFollow
Denise Danos, LSU Health Sciences Center - New OrleansFollow
Maria Dulfary Sanchez-Pino, LSU Health Sciences Center - New OrleansFollow

Document Type

Article

Publication Date

10-19-2024

Publication Title

Cells

Abstract

Potassium ions (K+) are critical electrolytes that regulate multiple functions in immune cells. Recent studies have shown that the elevated concentration of extracellular potassium in the tumor interstitial fluid limits T cell effector function and suppresses the anti-tumor capacity of tumor-associated macrophages (TAMs). The effect of excess potassium on the biology of myeloid-derived suppressor cells (MDSCs), another important immune cell component of the tumor microenvironment (TME), is unknown. Here, we present data showing that increased concentrations of potassium chloride (KCl), as the source of K+ ions, facilitate autophagy by increasing the expression of the autophagosome marker LC3β. Simultaneously, excess potassium ions significantly decrease the expression of arginase I (Arg I) and inducible nitric oxide synthase (iNOS) without reducing the ability of MDSCs to suppress T cell proliferation. Further investigation reveals that excess K+ ions decrease the expression of the transcription factor C/EBP-β and alter the expression of phosphorylated kinases. While excess K+ ions downregulated the expression levels of phospho-AMPKα (pAMPKα), it increased the levels of pAKT and pERK. Additionally, potassium increased mitochondrial respiration as measured by the oxygen consumption rate (OCR). Interestingly, all these alterations induced by K+ ions were abolished by the autophagy inhibitor 3-methyladenine (3-MA). Our results suggest that hyperosmotic stress caused by excess K+ ions regulate the mitochondrial respiration and signaling pathways in MDSCs to trigger the process of autophagy to support MDSCs’ immunosuppressive function by mechanisms independent of Arg I and iNOS. Overall, our in vitro and ex vivo findings offer valuable insights into the adaptations of MDSCs within the K+ ion-rich TME, which has important implications for MDSCs-targeted therapies.

PubMed ID

39451254

Volume

13

Issue

20

Creative Commons License

This work is licensed under a Creative Commons Attribution 4.0 International License.

Recommended Citation

Thylur Puttalingaiah, Ramesh; Dean, Matthew J.; Zheng, Liqin; Philbrook, Phaethon; Wyczechowska, Dorota; Kayes, Timothy; Del Valle, Luis; Danos, Denise; and Sanchez-Pino, Maria Dulfary, "Excess Potassium Promotes Autophagy to Maintain the Immunosuppressive Capacity of Myeloid-Derived Suppressor Cells Independent of Arginase 1" (2024). School of Medicine Faculty Publications. 3203.
https://digitalscholar.lsuhsc.edu/som_facpubs/3203
10.3390/cells13201736