4.7 Article

Nuclear-Encoded lncRNA MALAT1 Epigenetically Controls Metabolic Reprogramming in HCC Cells through the Mitophagy Pathway

MOLECULAR THERAPY-NUCLEIC ACIDS (2021)

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Journal

MOLECULAR THERAPY-NUCLEIC ACIDS
Volume 23, Issue -, Pages 264-276

Publisher

CELL PRESS
DOI: 10.1016/j.omtn.2020.09.040

Keywords

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Categories

Medicine, Research & Experimental

Funding

  1. Key Project of Chinese Ministry of Education [311015]
  2. National Basic Research Program of China (973 Program) [2015CB943303]
  3. Nation Key Research and Development Program of China [2016YFC13038000]
  4. Research on Chronic Noncommunicable Diseases Prevention and Control of National Ministry of Science and Technology [2016YFC1303804]
  5. National Health Development Planning Commission Major Disease Prevention and Control of Science and Technology Plan of Action, Cancer Prevention and Control [ZX07C2016004]
  6. National Key R&D Program of China [2018YFA0106902]
  7. National Natural Science Foundation of China [82050003, 32000431, 31430021, 81874052, 81672275, 31871297, 81670143]
  8. Natural Science Foundation of Jilin Province [20150101176JC, 20180101117JC, 20130413010GH]
  9. Provincial Science Fund of Jilin Province Development and Reform Commission [2014N147, 2017C022]
  10. California Institute of Regenerative Medicine (CIRM) grant [RT201942]
  11. Merit Review from the United States Department of Veterans Affairs, Biomedical Laboratory Research and Development Service [BX002905]

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The study revealed that in hepatoma cells, the lncRNA MALAT1 interacts with various loci on mitochondrial DNA, leading to abnormalities in mitochondrial function and subsequently impacting tumor phenotype and pathways related to cellular mitochondria. The findings suggest a critical role of MALAT1 in regulating mitochondrial metabolism and tumor metabolism reprogramming.
Mitochondrial dysfunction is a metabolic hallmark of cancer cells. In search of molecular factors involved in this dysregulation in hepatocellular carcinoma (HCC), we found that the nuclear-encoded long noncoding RNA (lncRNA) MALAT1 (metastasis-associated lung adenocarcinoma transcript 1) was aberrantly enriched in the mitochondria of hepatoma cells. Using RNA reverse transcription-associated trap sequencing (RAT-seq), we showed that MALAT1 interacted with multiple loci on mitochondrial DNA (mtDNA), including D-loop, COX2, ND3, and CYTB genes. MALAT1 knockdown induced alterations in the CpG methylation of mtDNA and in mitochondrial transcriptomes. This was associated with multiple abnormalities in mitochondrial function, including altered mitochondrial structure, low oxidative phosphorylation (OXPHOS), decreased ATP production, reduced mitophagy, decreased mtDNA copy number, and activation of mitochondrial apoptosis. These alterations in mitochondrial metabolism were associated with changes in tumor phenotype and in pathways involved in cell mitophagy, mitochondrial apoptosis, and epigenetic regulation. We further showed that the RNA-shuttling protein HuR and the mitochondria transmembrane protein MTCH2 mediated the transport of MALAT1 in this nuclear-mitochondrial crosstalk. This study provides the first evidence that the nuclear genome-encoded lncRNA MALAT1 functions as a critical epigenetic player in the regulation of mitochondrial metabolism of hepatoma cells, laying the foundation for further clarifying the roles of lncRNAs in tumor metabolic reprogramming.

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