The Noncoding RNA MALAT1 Is a Critical Regulator of the Metastasis Phenotype of Lung Cancer Cells
Tony Gutschner,Monika Hämmerle,Moritz Eißmann,Jeff Hsu,Youngsoo Kim,Gene Hung,Alexey S. Revenko,Gayatri Arun,Marion Stentrup,Matthias Groß,Martin Zörnig,A. Robert MacLeod,David L. Spector,Sven Diederichs +13 more
TLDR
A loss-of-function model unravels the active function of MALAT1 as a regulator of gene expression governing hallmarks of lung cancer metastasis with this ncRNA serving as both predictive marker and therapeutic target.Abstract:
The long non-coding RNA MALAT1, also known as MALAT-1 or NEAT2, is a highly conserved nuclear ncRNA and a predictive marker for metastasis development in lung cancer. To uncover its functional importance, we developed a MALAT1 knockout model in human lung tumor cells by genomically integrating RNA destabilizing elements using Zinc Finger Nucleases. The achieved 1000-fold MALAT1 silencing provides a unique loss-of-function model. Proposed mechanisms of action include regulation of splicing or gene expression. In lung cancer, MALAT1 does not alter alternative splicing but actively regulates gene expression including a set of metastasis-associated genes. Consequently, MALAT1-deficient cells are impaired in migration and form fewer tumor nodules in a mouse xenograft. Antisense oligonucleotides blocking MALAT1 prevent metastasis formation after tumor implantation. Thus, targeting MALAT1 with antisense oligonucleotides provides a potential therapeutic approach to prevent lung cancer metastasis with MALAT1 serving as both, predictive marker and therapeutic target. Lastly, regulating gene expression, but not alternative splicing is the critical function of MALAT1 in lung cancer metastasis. In summary, ten years after the discovery of the lncRNA MALAT1 as a biomarker for lung cancer metastasis, our loss-of-function model unravels the active function of MALAT1 as a regulator of gene expression governing hallmarks of lung cancer metastasis.read more
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Long non-coding RNAs (lncRNAs); roles in tumorigenesis and potentials as biomarkers in cancer diagnosis.
Sajad Varmaziar Najafi,Seyyed Hossein Khatami,Marjan Khorsand,Zeinab Jamali,Zahra Shabaninejad,Mostafa Moazamfard,Jamal Majidpoor,Seyed Mohsen Aghaei Zarch,Ahmad Movahedpour +8 more
TL;DR: In this article , the authors summarized recent advances in the mechanisms and functions of long non-coding RNAs in cancer and discussed their potential uses as biomarkers for the diagnosis and prognosis of cancer.
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Long noncoding RNAs (lncRNAs) in triple negative breast cancer
TL;DR: The advances from the most recent studies of lncRNAs in the predicament of breast cancer, TNBC, are highlighted, especially the functions of specifically selected lnc RNAs, providing clues for the diagnosis and treatments of TNBC.
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LncRNA BRCAT54 inhibits the tumorigenesis of non-small cell lung cancer by binding to RPS9 to transcriptionally regulate JAK-STAT and calcium pathway genes.
Wenhan Yang,Qian Youhui,Kaiping Gao,Wenjing Zheng,Guodong Wu,He Qihan,Qianqian Chen,Yi Song,Liang Wang,Yejun Wang,Peigui Gu,Bin Chen,Rihong Zhai +12 more
TL;DR: A novel lncRNA (BRCAT54), which was significantly up-regulated in preoperative plasma, NSCLC tissues, andNSCLC cells, and its higher expression was associated with better prognosis in patients with NSCLc, and targeting the BRCat54 and RPS9 feedback loop might be a novel therapeutic strategy for NSCLCs.
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Genome-Wide Association Study of Down Syndrome-Associated Atrioventricular Septal Defects
Dhanya Ramachandran,Zhen Zeng,Adam E. Locke,Jennifer G. Mulle,Lora J. H. Bean,Tracie C. Rosser,Kenneth J. Dooley,Clifford L. Cua,George T. Capone,Roger H. Reeves,Cheryl L. Maslen,David J. Cutler,Eleanor Feingold,Stephanie L. Sherman,Michael E. Zwick +14 more
TL;DR: Data are presented from the largest heart study conducted to date on a trisomic background by using a carefully characterized collection of individuals from extreme ends of the phenotypic spectrum to highlight the complex genetic architecture of atrioventricular septal defects even in the highly susceptible Down syndrome population.
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TL;DR: Detailed polling of transcription start and termination sites and analysis of previously unidentified full-length complementary DNAs derived from the mouse genome provide a comprehensive platform for the comparative analysis of mammalian transcriptional regulation in differentiation and development.
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TL;DR: Three potentially functional classes of RNAs have been identified, two of which are syntenically conserved and correlate with the expression state of protein-coding genes and support a highly interleaved organization of the human transcriptome.
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