AI Article Synopsis

  • Leukemia can lead to tumor-like growths called myeloid sarcomas (MS) when cells accumulate outside of the bone marrow, especially in the brain, making treatment difficult due to limited drug effectiveness and resistance.
  • A new 3D in vitro model, created using brain-derived hydrogel, effectively mimics intracranial MS, allowing researchers to study how leukemia cells behave in a brain-like environment.
  • The study found that leukemia cells in this model undergo significant changes, including increased dormant stem cells and drug resistance, highlighting ferroptosis suppression as a key feature that could guide future targeted therapies.

Article Abstract

Leukemia circulates in the bloodstream and induces various symptoms and complications. Occasionally, these cells accumulate in non-marrow tissues, forming a tumor-like myeloid sarcoma (MS). When the blast-stage leukemia cells invade the brain parenchyma, intracranial MS occurs, leading to a challenging prognosis owing to the limited penetration of cytostatic drugs into the brain and the development of drug resistance. The scarcity of tissue samples from MS makes understanding the phenotypic changes occurring in leukemia cells within the brain environment challenging, thereby hindering development of effective treatment strategies for intracranial MS. This study presents a novel 3D in vitro model mimicking intracranial MS, employing a hydrogel scaffold derived from the brain-decellularized extracellular matrix in which suspended leukemia cells are embedded, simulating the formation of tumor masses in the brain parenchyma. This model reveals marked phenotypic changes in leukemia cells, including altered survival, proliferation, differentiation, and cell cycle regulation. Notably, proportion of dormant leukemia stem cells increases and expression of multidrug resistance genes is upregulated, leading to imatinib resistance, mirroring the pathological features of in vivo MS tissue. Furthermore, suppression of ferroptosis is identified as an important characteristic of intracranial MS, providing valuable insights for the development of targeted therapeutic strategies.

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Source
http://dx.doi.org/10.1002/adhm.202304371DOI Listing

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