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Literature DB >> 24876273

Targeting RPL39 and MLF2 reduces tumor initiation and metastasis in breast cancer by inhibiting nitric oxide synthase signaling.

Bhuvanesh Dave¹, Sergio Granados-Principal¹, Rui Zhu², Stephen Benz³, Shahrooz Rabizadeh⁴, Patrick Soon-Shiong⁴, Ke-Da Yu⁵, Zhimin Shao⁵, Xiaoxian Li⁶, Michael Gilcrease⁶, Zhao Lai⁷, Yidong Chen⁸, Tim H-M Huang⁹, Haifa Shen¹⁰, Xuewu Liu¹⁰, Mauro Ferrari¹⁰, Ming Zhan², Stephen T C Wong¹¹, Muthiah Kumaraswami¹², Vivek Mittal¹³, Xi Chen¹³, Steven S Gross¹³, Jenny C Chang¹⁴.

Abstract

We previously described a gene signature for breast cancer stem cells (BCSCs) derived from patient biopsies. Selective shRNA knockdown identified ribosomal protein L39 (RPL39) and myeloid leukemia factor 2 (MLF2) as the top candidates that affect BCSC self-renewal. Knockdown of RPL39 and MLF2 by specific siRNA nanoparticles in patient-derived and human cancer xenografts reduced tumor volume and lung metastases with a concomitant decrease in BCSCs. RNA deep sequencing identified damaging mutations in both genes. These mutations were confirmed in patient lung metastases (n = 53) and were statistically associated with shorter median time to pulmonary metastasis. Both genes affect the nitric oxide synthase pathway and are altered by hypoxia. These findings support that extensive tumor heterogeneity exists within primary cancers; distinct subpopulations associated with stem-like properties have increased metastatic potential.

Entities: Disease Gene Species

Mesh：

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Year: 2014 PMID： 24876273 PMCID： PMC4066479 DOI： 10.1073/pnas.1320769111

Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN： 0027-8424 Impact factor: 11.205

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