DOAJ Open Access 2024

Macrophages as Potential Therapeutic Targets in Acute Myeloid Leukemia

Oana Mesaros Madalina Onciul Emilia Matei Corina Joldes Laura Jimbu +4 lainnya

Abstrak

Acute myeloid leukemia (AML) is a heterogenous malignant hemopathy, and although new drugs have emerged recently, current treatment options still show limited efficacy. Therapy resistance remains a major concern due to its contribution to treatment failure, disease relapse, and increased mortality among patients. The underlying mechanisms of resistance to therapy are not fully understood, and it is crucial to address this challenge to improve therapy. Macrophages are immune cells found within the bone marrow microenvironment (BMME), of critical importance for leukemia development and progression. One defining feature of macrophages is their plasticity, which allows them to adapt to the variations in the microenvironment. While this adaptability is advantageous during wound healing, it can also be exploited in cancer scenarios. Thus, clinical and preclinical investigations that target macrophages as a therapeutic strategy appear promising. Existing research indicates that targeting macrophages could enhance the effectiveness of current AML treatments. This review addresses the importance of macrophages as therapeutic targets including relevant drugs investigated in clinical trials such as pexidartinib, magrolimab or bexmarilimab, but also provides new insights into lesser-known therapies, like macrophage receptor with a collagenous structure (MACRO) inhibitors and Toll-like receptor (TLR) agonists.

Topik & Kata Kunci

Penulis (9)

O

Oana Mesaros

M

Madalina Onciul

E

Emilia Matei

C

Corina Joldes

L

Laura Jimbu

A

Alexandra Neaga

O

Oana Serban

M

Mihnea Zdrenghea

A

Ana Maria Nanut

Format Sitasi

Mesaros, O., Onciul, M., Matei, E., Joldes, C., Jimbu, L., Neaga, A. et al. (2024). Macrophages as Potential Therapeutic Targets in Acute Myeloid Leukemia. https://doi.org/10.3390/biomedicines12102306

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Informasi Jurnal
Tahun Terbit
2024
Sumber Database
DOAJ
DOI
10.3390/biomedicines12102306
Akses
Open Access ✓