Surface CD81 supports leukemia stem cell function and reveals a therapeutic vulnerability in acute myeloid leukemia
Summary
Relapse remains the leading cause of mortality in acute myeloid leukemia (AML), largely due to the persistence of therapy-resistant leukemia stem cells (LSCs). However, surface determinants that sustain LSC function and disease aggressiveness remain incompletely defined. Here, we identify the tetraspanin CD81 as a regulator of LSC function, progression and treatment resistance in AML. Analysis of retrospective patient cohorts revealed that high CD81 surface expression is associated with re
Content
# Surface CD81 supports leukemia stem cell function and reveals a therapeutic vulnerability in acute myeloid leukemia
*Published: 2026 Apr 21*
Relapse remains the leading cause of mortality in acute myeloid leukemia (AML),
largely due to the persistence of therapy-resistant leukemia stem cells (LSCs).
However, surface determinants that sustain LSC function and disease
aggressiveness remain incompletely defined. Here, we identify the tetraspanin
CD81 as a regulator of LSC function, progression and treatment resistance in
AML. Analysis of retrospective patient cohorts revealed that high CD81 surface
expression is associated with relapse and adverse clinical outcomes in
non-core-binding factor AML. Functional studies demonstrated that elevated CD81
expression promotes chemoresistance and enhances leukemic engraftment in
immunodeficient mouse models. In vivo gain- and loss-of-function approaches
further established that CD81 drives increased leukemia burden and aggressive
disease behavior. Notably, CD81 was enriched within LSC-containing
subpopulations, where its expression supported LSC maintenance and resistance to
chemotherapy. Mechanistically, CD81 promotes chemoresistance and leukemic
aggressiveness through pathways linked to LAPTM4B-mediated STAT3 signaling and
enhanced adhesion-dependent cellular interactions. These effects were
accompanied by increased migration, invasion, and formation of filopodia-like
membrane protrusions. Importantly, therapeutic immunotargeting of CD81
significantly reduced leukemic burden while exhibiting a manageable toxicity
profile in preclinical models. Collectively, these findings establish CD81 as a
clinically relevant surface marker associated with AML relapse and identify
CD81-dependent signaling as a therapeutic vulnerability for targeting LSCs and
preventing disease recurrence.
DOI: 10.1038/s41392-026-02697-2