AI Article Synopsis
- Pirtobrutinib is a non-covalent Bruton's tyrosine kinase (BTK) inhibitor that helps overcome resistance to existing covalent BTK inhibitors in chronic lymphocytic leukemia (CLL), but its resistance mechanisms are not fully understood.
- Researchers created resistant cell models using CRISPR-Cas9 and prolonged drug exposure to evaluate pirtobrutinib resistance, identifying key protein expression changes through advanced analysis techniques.
- The study found that the PI3K/AKT pathway is significantly activated in resistant cells, and using inhibitors targeting this pathway (like CAL101 and MK2206) effectively reduced cell growth and induced cancer cell death, suggesting a potential treatment strategy against resistance.
Article Abstract
Purpose: Pirtobrutinib, a non-covalent Bruton's tyrosine kinase (BTK) inhibitor, has been approved as the first agent to overcome resistance to covalent BTK inhibitors (such as ibrutinib, acalabrutinib, and zanubrutinib). However, the mechanisms of pirtobrutinib resistance in chronic lymphocytic leukemia (CLL) remain poorly understood.
Methods: To investigate pirtobrutinib resistance, we established resistant cell models using BTK knock-out via CRISPR-Cas9 or chronic exposure to pirtobrutinib in MEC-1 cells. These models mimicked intrinsic or acquired resistance, respectively. We then analyzed differential protein expression between wild-type (WT) and resistant MEC-1 cells using Revers Phase Protein microArray (RPPA) and confirmed the findings through Western Blot. Additionally, we evaluated potential drugs to overcome pirtobrutinib resistance by conducting cell proliferation assays, apoptosis studies, and animal experiments using both sensitive and resistant cells.
Results: MEC-1 cells developed resistance to pirtobrutinib either through BTK knock-out or prolonged drug exposure over three months. RPPA analysis revealed significant activation of proteins related to the PI3K/AKT pathway, including AKT and S6, in the resistant cells. Western Blot confirmed increased phosphorylation of AKT and S6 in pirtobrutinib-resistant MEC-1 cells. Notably, both the PI3K inhibitor (CAL101) and the AKT inhibitor (MK2206) effectively reduced cell proliferation and induced apoptosis in the resistant cells. The anti-tumor efficacy of these drugs was mediated by inhibiting the PI3K/AKT pathway. In vivo animal studies further supported the potential of targeting PI3K/AKT to overcome both intrinsic and acquired resistance to pirtobrutinib.
Conclusion: The PI3K/AKT pathway plays a crucial role in both intrinsic and acquired resistance to pirtobrutinib in CLL. Therapeutically targeting this pathway may offer a promising strategy to overcome pirtobrutinib resistance.
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| http://dx.doi.org/10.1016/j.leukres.2024.107548 | DOI Listing |
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