Your search keyword '"631/337/384/2568"' showing total 2 results

1. A disease-linked lncRNA mutation in RNase MRP inhibits ribosome synthesis

Author

Nic Robertson, Vadim Shchepachev, David Wright, Tomasz W. Turowski, Christos Spanos, Aleksandra Helwak, Rose Zamoyska, David Tollervey, Shchepachev, Vadim [0000-0001-8551-5940], Turowski, Tomasz W [0000-0002-7052-8682], Spanos, Christos [0000-0002-4376-8242], Zamoyska, Rose [0000-0001-9816-2638], Tollervey, David [0000-0003-2894-2772], and Apollo - University of Cambridge Repository

Subjects

RNA Folding, Ribosomopathy, T-Lymphocytes, General Physics and Astronomy, 13, medicine.disease_cause, Ribosome, RNA Precursors, 42/41, Mitochondrial ribosome, Cells, Cultured, Mice, Knockout, Mutation, Multidisciplinary, Chemistry, article, Cell biology, 13/31, 631/337/384/2568, RNA, Long Noncoding, 631/80/304, Primary Immunodeficiency Diseases, Science, 631/250/2502, 38/90, 13/106, Osteochondrodysplasias, General Biochemistry, Genetics and Molecular Biology, 38, 38/91, Endoribonucleases, 631/208/200, medicine, Animals, Humans, Hirschsprung Disease, RRNA processing, Gene, Cell Proliferation, Base Sequence, 82/58, RNA, General Chemistry, Fibroblasts, 49, Mice, Inbred C57BL, RNase MRP, RNA, Ribosomal, 631/1647/2017/2003, K562 Cells, Ribosomes, Hair

Abstract

RMRP encodes a non-coding RNA forming the core of the RNase MRP ribonucleoprotein complex. Mutations cause Cartilage Hair Hypoplasia (CHH), characterized by skeletal abnormalities and impaired T cell activation. Yeast RNase MRP cleaves a specific site in the pre-ribosomal RNA (pre-rRNA) during ribosome synthesis. CRISPR-mediated disruption of RMRP in human cells lines caused growth arrest, with pre-rRNA accumulation. Here, we analyzed disease-relevant primary cells, showing that mutations in RMRP impair mouse T cell activation and delay pre-rRNA processing. Patient-derived human fibroblasts with CHH-linked mutations showed similar pre-rRNA processing delay. Human cells engineered with the most common CHH mutation (70AG in RMRP) show specifically impaired pre-rRNA processing, resulting in reduced mature rRNA and a reduced ratio of cytosolic to mitochondrial ribosomes. Moreover, the 70AG mutation caused a reduction in intact RNase MRP complexes. Together, these results indicate that CHH is a ribosomopathy, and the first processing-specific human disorder to be described.HighlightsMutations in RMRP lncRNA impair pre-rRNA processing and T cell activationPatient derived fibroblasts show impaired pre-rRNA processingCells with the most common disease-linked mutation have specific processing defectsCytoplasmic ribosomes and intact RNase MRP complexes are also reduced in these cells

Published

2021

2. A high-content RNAi screen reveals multiple roles for long noncoding RNAs in cell division

Author

Fanni Gergely, Jasmin Mangei, John C. Marioni, Patrice Mascalchi, Chris Bakal, Duncan T. Odom, Christina Ernst, Alexis R. Barr, Aisling M. Redmond, Vicky Bousgouni, Lovorka Stojic, Aaron T. L. Lun, Stojic, Lovorka [0000-0001-6691-3396], Lun, Aaron T. L. [0000-0002-3564-4813], Redmond, Aisling M. [0000-0001-9070-1780], Barr, Alexis R. [0000-0002-6684-8114], Bakal, Chris [0000-0002-0413-6744], Odom, Duncan T. [0000-0001-6201-5599], Gergely, Fanni [0000-0002-2441-8095], Apollo - University of Cambridge Repository, Lun, Aaron TL [0000-0002-3564-4813], Redmond, Aisling M [0000-0001-9070-1780], Barr, Alexis R [0000-0002-6684-8114], Odom, Duncan T [0000-0001-6201-5599], and Lun, Aaron T L [0000-0002-3564-4813]

Subjects

0301 basic medicine, binding, Cell division, General Physics and Astronomy, comparative genomics, 13, 14, 631/337/641/1655, Transcriptome, Chromosome segregation, 0302 clinical medicine, RNA interference, lcsh:Science, 0303 health sciences, Multidisciplinary, 030302 biochemistry & molecular biology, High-throughput screening, Cell biology, Multidisciplinary Sciences, spindle-assembly checkpoint, 631/337/384/2568, Science & Technology - Other Topics, RNA Interference, RNA, Long Noncoding, Cell Division, Cell type, Science, Mitosis, gene repression, Biology, General Biochemistry, Genetics and Molecular Biology, Article, 38, 38/91, 14/32, 03 medical and health sciences, Microtubule, expression, 38/89, 631/208/200, Humans, 030304 developmental biology, Science & Technology, microtubule organization, Proteins, General Chemistry, mitotic block, 49, High-Throughput Screening Assays, Gene regulation, 030104 developmental biology, tubulin, 14/63, Long non-coding RNAs, lcsh:Q, tppp/p25, 631/1647/2163, protein, 030217 neurology & neurosurgery, Cytokinesis, HeLa Cells

Abstract

Genome stability relies on proper coordination of mitosis and cytokinesis, where dynamic microtubules capture and faithfully segregate chromosomes into daughter cells. With a high-content RNAi imaging screen targeting more than 2,000 human lncRNAs, we identify numerous lncRNAs involved in key steps of cell division such as chromosome segregation, mitotic duration and cytokinesis. Here, we provide evidence that the chromatin-associated lncRNA, linc00899, leads to robust mitotic delay upon its depletion in multiple cell types. We perform transcriptome analysis of linc00899-depleted cells and identify the neuronal microtubule-binding protein, TPPP/p25, as a target of linc00899. We further show that linc00899 binds TPPP/p25 and suppresses its transcription. In cells depleted of linc00899, upregulation of TPPP/p25 alters microtubule dynamics and delays mitosis. Overall, our comprehensive screen uncovers several lncRNAs involved in genome stability and reveals a lncRNA that controls microtubule behaviour with functional implications beyond cell division., Long noncoding RNAs (lncRNAs) regulate key steps of cell division. Here, the authors perform a comprehensive RNAi imaging screen targeting more than 2,000 human lncRNAs, and suggest a role of chromatin-associated linc00899 in regulation of cell division by suppressing the transcription of microtubule-binding protein TPPP/p25.

Published

2019