High cortactin expression in B-cell acute lymphoblastic leukemia is associated with increased transendothelial migration and bone marrow relapse

B细胞急性淋巴细胞白血病中高表达的皮质肌动蛋白与跨内皮迁移增加和骨髓复发相关

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作者:Martha Velázquez-Avila ,Juan Carlos Balandrán ,Dalia Ramírez-Ramírez ,Mirella Velázquez-Avila ,Antonio Sandoval ,Alfonso Felipe-López ,Porfirio Nava ,José Antonio Alvarado-Moreno ,David Dozal ,Jessica L Prieto-Chávez ,Matthias Schaks ,Klemens Rottner ,Elisa Dorantes-Acosta ,Briceida López-Martínez ,Michael Schnoor # ,Rosana Pelayo #

Abstract

Cancer is a major cause of death in children worldwide, with B-lineage cell acute lymphoblastic leukemia (B-ALL) being the most frequent childhood malignancy. Relapse, treatment failure and organ infiltration worsen the prognosis, warranting a better understanding of the implicated mechanisms. Cortactin is an actin-binding protein involved in cell adhesion and migration that is overexpressed in many solid tumors and in adult B-cell chronic lymphocytic leukemia. Here, we investigated cortactin expression and potential impact on infiltration and disease prognosis in childhood B-ALL. B-ALL cell lines and precursor cells from bone marrow (BM) and cerebrospinal fluid (CSF) of B-ALL patients indeed overexpressed cortactin. In CXCL12-induced transendothelial migration assays, transmigrated B-ALL cells had highest cortactin expression. In xenotransplantation models, only cortactinhigh-leukemic cells infiltrated lungs, brain, and testis; and they colonized more easily hypoxic BM organoids. Importantly, cortactin-depleted B-ALL cells were significantly less efficient in transendothelial migration, organ infiltration and BM colonization. Clinical data highlighted a significant correlation between high cortactin levels and BM relapse in drug-resistant high-risk B-ALL patients. Our results emphasize the importance of cortactin in B-ALL organ infiltration and BM relapse and its potential as diagnostic tool to identify high-risk patients and optimize their treatments.

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