Abstract B222: Dicer substrate siRNAs to MYC, B-catenin, and other target genes effectively induce in vivo target gene knockdown and tumor inhibition.

Dudek, Henryk; Wortham, Kathleen; Arvan, Rokhand; Shah, Anee; Ying, Bo; Cyr, Wendy A.; Yang, Hailin; Zhou, Wei; Saxena, Utsav; Zhou, Yi; Diwanji, Rohan; Holmes, Ben; Farkiwala, Ruchir; Shah, Aalok; Brown, Bob D.

doi:10.1158/1535-7163.targ-13-b222

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“…Dicer converts inactive hairpin‐structured pre‐miRNA into the active single stranded form, then influence multiple cellular functions . Oncogenic cyclin D1 could promote Dicer, and then induced let‐7 maturation, forming the let‐7/DICER1 and let‐7/cyclin D1 regulatory loop.…”

Section: Discussionmentioning

confidence: 99%

DICER1 regulated let‐7 expression levels in p53‐induced cancer repression requires cyclin D1

Sun

Tang

et al. 2015

J Cellular Molecular Medi

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Let-7 miRNAs act as tumour suppressors by directly binding to the 3′UTRs of downstream gene products. The regulatory role of let-7 in downstream gene expression has gained much interest in the cancer research community, as it controls multiple biological functions and determines cell fates. For example, one target of the let-7 family is cyclin D1, which promotes G0/S cell cycle progression and oncogenesis, was correlated with endoribonuclease DICER1, another target of let-7. Down-regulated let-7 has been identified in many types of tumours, suggesting a feedback loop may exist between let-7 and cyclin D1. A potential player in the proposed feedback relationship is Dicer, a central regulator of miRNA expression through sequence-specific silencing. We first identified that DICER1 is the key downstream gene for cyclin D1-induced let-7 expression. In addition, we found that let-7 miRNAs expression decreased because of the p53-induced cell death response, with deregulated cyclin D1. Our results also showed that cyclin D1 is required for Nutlin-3 and TAX-induced let-7 expression in cancer repression and the cell death response. For the first time, we provide evidence that let-7 and cyclin D1 form a feedback loop in regulating therapy response of cancer cells and cancer stem cells, and importantly, that alteration of let-7 expression, mainly caused by cyclin D1, is a sensitive indicator for better chemotherapies response.

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Section: Discussionmentioning

confidence: 99%