Cell starvation increases uptake of extracellular Thymosin β4 and its complexes with calcium.

International immunopharmacology2023PMID: 36706591

View on PubMed DOI: 10.1016/j.intimp.2023.109743

Plain Language Summary

Investigates how cell starvation (serum deprivation) affects thymosin β4 uptake and its calcium-complexed forms. Starved cells showed significantly increased endocytosis of extracellular Tβ4 compared to normal cells. Tβ4-calcium complexes were preferentially taken up—suggesting calcium binding modulates Tβ4's cellular entry mechanism. In cancer cells, increased Tβ4 uptake under starvation conditions correlated with enhanced migration/invasion potential. Identifies starvation-responsive Tβ4 uptake as a potential mechanism driving tumor metastasis in nutrient-deprived cancer microenvironments.

Abstract

Cell metastasis is the main cause of cancer mortality. Inhibiting early events during cell metastasis and invasion could significantly improve cancer prognosis, but the initial mechanisms of cell transition and migration are barely known. Calcium regulates cell migration, whilst Thymosin β4 is a G-actin and iron binding peptide associated with tumor metastasis and ferroptosis. Under normal cell growth conditions, intracellular free calcium ions and Thymosin β4 concentrations are strictly regulated, and are not influenced by extracellular supplementation. However, cell starvation decreases intracellular Thymosin β4 and increases extracellular peptide uptake above the normal range. Unexpectedly, cell starvation significantly increases internalization of extracellular Ca/Thymosin β4 complexes. Elucidating the role of Ca/Thymosin β4 in the early events of metastasis will likely be important in the future to develop therapies targeting metastasis.

Authors

Piludu, Marco; Pichiri, Giuseppina; Coni, Pierpaolo; Piras, Monica; Congiu, Terenzio; Faa, Gavino; Lachowicz, Joanna Izabela

Keywords

CalciumCell starvationImmunostainingThymosin β4Tumour metastasis