ANGPTL4 T266M variant is associated with reduced cancer invasiveness

摘要

Abstract Angiopoietin-like 4 (ANGPTL4) is a secretory protein that can be cleaved to form an N-terminal and a C-terminal protein. Studies performed thus far have linked ANGPTL4 to several cancer-related and metabolic processes. Notably, several point mutations in the C-terminal ANGPTL4 (cANGPTL4) have been reported, although no studies have been performed that ascribed these mutations to cancer-related and metabolic processes. In this study, we compared the characteristics of tumors with and without wild-type (wt) cANGPTL4 and tumors with cANGPTL4 bearing the T266M mutation (T266M cANGPTL4). We found that T266M cANGPTL4 bound to integrin α5β1 with a reduced affinity compared to wt, leading to weaker activation of downstream signaling molecules. The mutant tumors exhibited impaired proliferation, anoikis resistance, and migratory capability and had reduced adenylate energy charge. Further investigations also revealed that cANGPTL4 regulated the expression of Glut2. These findings may explain the differences in the tumor characteristics and energy metabolism observed with the cANGPTL4 T266M mutation compared to tumors without the mutation. Highlights ? Coding T266M cANGPTL4 variant exhibited reduced affinity for integrin. ? Cancer cells with T266M cANGPTL4 have attenuated glucose uptake and invasiveness. ? cANGPTL4 regulates Glut2 expression to affect the level of adenylate energy charge. ? MALDI-MSI imaging reveals energy charge hotspots within tumor xenografts. ]]>