March 3, 2026Open Access

Sepsis induces long-term reprogramming of human HSPCs and drives myeloid dysregulation in sepsis survivors

Key Points

Long-term reprogramming of human hematopoietic stem and progenitor cells (HSPCs) drives myeloid dysregulation.
Sepsis survivors exhibit altered immune memory that may impact their overall immune response.
Assessment of immune alterations in this population reveals potential therapeutic avenues to explore.
Identifying specific reprogramming pathways in HSPCs may guide better management of sepsis long-term outcomes.

Abstract

Together, these findings suggest that sepsis induces lasting reprogramming in HSPCs leading to myeloid progeny with altered immune memory that might drive immune dysregulation in survivors. These data open avenues to explore potential targets to better manage long-term immune alterations in sepsis survivors.

Sepsis induces long-term reprogramming of human HSPCs and drives myeloid dysregulation in sepsis survivors

Key Points

Abstract

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