Parallel single-cell metabolic analysis and extracellular vesicle profiling reveal vulnerabilities with prognostic significance in acute myeloid leukemia.

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作者:Forte Dorian, Pellegrino Roberto Maria, Falvo Paolo, Garcia-Gonzalez Paulina, Alabed Husam B R, Maltoni Filippo, Lombardi Davide, Bruno Samantha, Barone Martina, Pasini Federico, Fabbri Francesco, Vannini Ivan, Donati Benedetta, Cristiano Gianluca, Sartor Chiara, Ronzoni Simona, Ciarrocchi Alessia, Buratta Sandra, Urbanelli Lorena, Emiliani Carla, Soverini Simona, Catani Lucia, Bertolini Francesco, Argüello Rafael José, Cavo Michele, Curti Antonio
Acute myeloid leukemia (AML) is an aggressive disease with a high relapse rate. In this study, we map the metabolic profile of CD34(+)(CD38(low/-)) AML cells and the extracellular vesicle signatures in circulation from AML patients at diagnosis. CD34(+) AML cells display high antioxidant glutathione levels and enhanced mitochondrial functionality, both associated with poor clinical outcomes. Although CD34(+) AML cells are highly dependent on glucose oxidation and glycolysis for energy, those from intermediate- and adverse-risk patients reveal increased mitochondrial dependence. Extracellular vesicles from AML are mainly enriched in stem cell markers and express antioxidant GPX3, with their profiles showing potential prognostic value. Extracellular vesicles enhance mitochondrial functionality and dependence on CD34(+) AML cells via the glutathione/GPX4 axis. Notably, extracellular vesicles from adverse-risk patients enhance leukemia cell engraftment in vivo. Here, we show a potential noninvasive approach based on liquid 'cell-extracellular vesicle' biopsy toward a redefined metabolic stratification in AML.

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