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Integrin α6 mediates the drug resistance of acute lymphoblastic B-cell leukemia. | LitMetric

AI Article Synopsis

  • Resistance to multimodal chemotherapy in acute lymphoblastic leukemia (ALL) is partly caused by adhesion-mediated drug resistance, with integrin α6 playing a key role.
  • The anti-human α6-blocking antibody P5G10 has been shown to induce apoptosis in primary ALL cells and enhance their sensitivity to chemotherapy and tyrosine kinase inhibitors both in vitro and in vivo.
  • Deleting α6 in ALL cells leads to increased apoptosis and improved treatment outcomes when combined with tyrosine kinase inhibitors, suggesting that targeting α6 could be an effective therapeutic strategy for ALL.

Article Abstract

Resistance to multimodal chemotherapy continues to limit the prognosis of acute lymphoblastic leukemia (ALL). This occurs in part through a process called adhesion-mediated drug resistance, which depends on ALL cell adhesion to the stroma through adhesion molecules, including integrins. Integrin α6 has been implicated in minimal residual disease in ALL and in the migration of ALL cells to the central nervous system. However, it has not been evaluated in the context of chemotherapeutic resistance. Here, we show that the anti-human α6-blocking Ab P5G10 induces apoptosis in primary ALL cells in vitro and sensitizes primary ALL cells to chemotherapy or tyrosine kinase inhibition in vitro and in vivo. We further analyzed the underlying mechanism of α6-associated apoptosis using a conditional knockout model of α6 in murine BCR-ABL1+ B-cell ALL cells and showed that α6-deficient ALL cells underwent apoptosis. In vivo deletion of α6 in combination with tyrosine kinase inhibitor (TKI) treatment was more effective in eradicating ALL than treatment with a TKI (nilotinib) alone. Proteomic analysis revealed that α6 deletion in murine ALL was associated with changes in Src signaling, including the upregulation of phosphorylated Lyn (pTyr507) and Fyn (pTyr530). Thus, our data support α6 as a novel therapeutic target for ALL.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7357190PMC
http://dx.doi.org/10.1182/blood.2019001417DOI Listing

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