let-7 Regulates Self Renewal and Tumorigenicity of Breast Cancer Cells

Yu, Fang; Yao, Herui; Zhu, Pengcheng; Zhang, Xiaoqin; Pan, Qiuhui; Gong, Chang; Huang, Yijun; Hu, Xiaoqu; Su, Fengxi; Lieberman, Judy; Song, Erwei

doi:10.1016/j.cell.2007.10.054

Cited by 1,719 publications

(1,598 citation statements)

References 33 publications

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“…Of the four most effective miRNAs identified, let-7c and miR200b belong to the let-7 and miRNA-200s families, respectively, of which the tumour-suppressor roles in TICs have been well appreciated 8,23,46 , while miR-222 and miR-424 were first identified as TIC-suppressing miRNAs despite a tumoursuppressor role of both miRNAs has been identified in a number of cancers other than HCC [47][48][49][50] . Paradoxically, miR-222 was previously regarded as oncogene in some reports because it could enhance some tumour cell growth by targeting CDK inhibitor p27 in vitro, and was found to be upregulated in HCC and some other types of cancers 42,51,52 ; however, its tumourpromoting role was rarely validated in vivo.…”

Section: Discussionmentioning

confidence: 99%

“…In fact, aberrant expression of miRNAs such as let-7, miR-34a, miR-181a, miRNA-130b in TICs has been found in a variety of tumour types. These aberrantly expressed miRNAs play essential roles in the regulation of TIC properties as either TIC suppressors or promoters [20][21][22][23][24] . Moreover, a series of critical signalling pathways involved in the regulation of TIC properties have been uncovered with the identification of the targets of these miRNAs 19,[25][26][27][28] .…”

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confidence: 99%

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PBX3 is targeted by multiple miRNAs and is essential for liver tumour-initiating cells

Han

Zhao

et al. 2015

Nat Commun

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Tumour-initiating cells (TICs) are advocated to constitute the sustaining force to maintain and renew fully established malignancy; however, the molecular mechanisms responsible for these properties are elusive. We previously demonstrated that voltage-gated calcium channel a2d1 subunit marks hepatocellular carcinoma (HCC) TICs. Here we confirm directly that a2d1 is a HCC TIC surface marker, and identify let-7c, miR-200b, miR-222 and miR-424 as suppressors of a2d1 þ HCC TICs. Interestingly, all the four miRNAs synergistically target PBX3, which is sufficient and necessary for the acquisition and maintenance of TIC properties. Moreover, PBX3 drives an essential transcriptional programme, activating the expression of genes critical for HCC TIC stemness including CACNA2D1, EpCAM, SOX2 and NOTCH3. In addition, the expression of CACNA2D1 and PBX3 mRNA is predictive of poor prognosis for HCC patients. Collectively, our study identifies an essential signalling pathway that controls the switch of HCC TIC phenotypes.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

PBX3 is targeted by multiple miRNAs and is essential for liver tumour-initiating cells

Han

Zhao

et al. 2015

Nat Commun

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“…For example, lethal‐7a (let‐7a), one of the founding members in the miRNA family,3 is poorly expressed in human cancers including prostate, breast, and brain cancers, which is decreased by more than threefold in contrast to other healthy tissues. [[qv: 2b,4]] Accordingly, upregulation of let‐7a results in a marked promotion of apoptosis and inhibition of the proliferation and metastasis of cancer cell by silencing KRAS and high‐mobility group AT‐hook 2 (HMGA2) 5. Therefore, miRNA replacement therapies can be employed as a promising treatment strategy if the miRNA can be delivered to cancer cells with high efficiency.…”

Section: Introductionmentioning

confidence: 99%

Rod‐Shaped Active Drug Particles Enable Efficient and Safe Gene Delivery

et al. 2017

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Efficient microRNAs (miRNA) delivery into cells is a promising strategy for disease therapy, but is a major challenge because the available conventional nonviral vectors have significant drawbacks. In particular, after these vectors are entrapped in lysosomes, the escape efficiency of genes from lysosomes into the cytosol is less than 2%. Here, a novel approach for lethal‐7a (let‐7a) replacement therapy using rod‐shaped active pure drug nanoparticles (≈130 nm in length, PNPs) with a dramatically high drug‐loading of ≈300% as vectors is reported. Importantly, unlike other vectors, the developed PNPs/let‐7a complexes (≈178 nm, CNPs) can enter cells and bypass the lysosomal route to localize to the cytosol, achieving efficient intracellular delivery of let‐7a and a 50% reduction in expression of the target protein (KRAS). Also, CNPs prolong the t 1/2 of blood circulation by ≈threefold and increase tumor accumulation by ≈1.5–2‐fold, resulting in significantly improved antitumor efficacies. Additionally, no damage to normal organs is observed following systemic injection of CNPs. In conclusion, rod‐shaped active PNPs enable efficient and safe delivery of miRNA with synergistic treatment for disease. This nanoplatform would also offer a viable strategy for the potent delivery of proteins and peptides in vitro and in vivo.

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“…Since in both studies let-7 miRNA was delivered at the same time as tumorigenesis was initiated, these two studies showed that let-7 can be used as a preventive therapy against lung cancer in the LSL-Kras G12D mice. In a similar experiment using let-7 treatment, Yu et al (2007a) showed that in a xenograft model of breast cancer, tumor-initiating cells, SK-3rd cells infected with lentivirus expressing let-7, developed significantly fewer tumors than cells given the control virus.…”

Section: Mirnas As Therapeuticsmentioning

confidence: 97%