[No authors listed]
Tâcell lymphoblastic lymphoma (TâLBL) is an aggressive malignancy with poor prognosis due to frequent relapses. Previous studies have reported an association of the disease with abnormal chromosomal rearrangements, DNA copy number alterations and mutations in critical signaling factors, such as those in the Notch1 pathway; however, the molecular mechanisms underlying the development of the disease remain unclear, limiting the development of novel therapies. In the present study, gene expression was detected by qPCR and western blot analysis. Diagnostic analysis was performed by ROC curve. Cell proliferation, invasion and migration were analyzed by cell proliferation and Transwell assays. Gene interactions were analyzed using luciferase reporter assay. In the present study, it was observed that the expression levels of microRNAâ338â3p (miRâ338â3p) were reduced in patient lymphoma tissues and a TâLBL cell line. Upregulation of its expression inhibited the migration and proliferation of cultured TâLBL cells. Bioinformatics analysis of putative target mRNAs of miRâ338â3p identified a direct binding site in the 3'âuntranslated of homeobox A3 (HOXA3). The levels of HOXA3 mRNA and protein were associated with those of miRâ338â3p, and overexpression of HOXA3 promoted the malignant phenotype of TâLBL cells. The results suggested that miRâ338â3p may suppress the development of TâLBL via the downregulation of oncogenic factors, such as HOXA3. The findings indicated that further investigation into miRâ338â3p and the HOXA3 regulatory network may aid the development of novel therapeutic tools.
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