The inner nuclear membrane protein Lem2 coordinates RNA degradation at the nuclear periphery

被引:0
作者
Lucía Martín Caballero
Matías Capella
Ramón Ramos Barrales
Nikolay Dobrev
Thomas van Emden
Yasuhiro Hirano
Vishnu N. Suma Sreechakram
Sabine Fischer-Burkart
Yasuha Kinugasa
Alicia Nevers
Mathieu Rougemaille
Irmgard Sinning
Tamás Fischer
Yasushi Hiraoka
Sigurd Braun
机构
[1] BioMedical Center (BMC),Graduate School of Frontier Biosciences
[2] Division of Physiological Chemistry,Institute for Genetics
[3] Faculty of Medicine,The John Curtin School of Medical Research
[4] LMU Munich,Instituto de Agrobiotecnología del Litoral, CONICET
[5] International Max Planck Research School for Molecular and Cellular Life Sciences,Centro Andaluz de Biología del Desarrollo (CABD)
[6] Heidelberg University Biochemistry Center (BZH),undefined
[7] Osaka University,undefined
[8] Justus-Liebig-University Giessen,undefined
[9] Université Paris-Saclay,undefined
[10] CEA,undefined
[11] CNRS,undefined
[12] Institute for Integrative Biology of the Cell (I2BC),undefined
[13] The Australian National University,undefined
[14] Universidad Nacional del Litoral,undefined
[15] Universidad Pablo de Olavide-Consejo Superior de Investigaciones Científicas-Junta de Andalucía,undefined
[16] European Molecular Biology Laboratory,undefined
[17] Hamburg Unit,undefined
[18] Regulation for intractable Infectious Diseases,undefined
[19] National Institutes of Biomedical Innovation,undefined
[20] Health and Nutrition,undefined
[21] University Paris-Saclay,undefined
[22] INRAE,undefined
[23] AgroParisTech,undefined
[24] Micalis Institute,undefined
来源
Nature Structural & Molecular Biology | 2022年 / 29卷
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摘要
Transcriptionally silent chromatin often localizes to the nuclear periphery. However, whether the nuclear envelope (NE) is a site for post-transcriptional gene repression is not well understood. Here we demonstrate that Schizosaccharomycespombe Lem2, an NE protein, regulates nuclear-exosome-mediated RNA degradation. Lem2 deletion causes accumulation of RNA precursors and meiotic transcripts and de-localization of an engineered exosome substrate from the nuclear periphery. Lem2 does not directly bind RNA but instead interacts with the exosome-targeting MTREC complex and its human homolog PAXT to promote RNA recruitment. This pathway acts largely independently of nuclear bodies where exosome factors assemble. Nutrient availability modulates Lem2 regulation of meiotic transcripts, implying that this pathway is environmentally responsive. Our work reveals that multiple spatially distinct degradation pathways exist. Among these, Lem2 coordinates RNA surveillance of meiotic transcripts and non-coding RNAs by recruiting exosome co-factors to the nuclear periphery.
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页码:910 / 921
页数:11
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