journal
https://read.qxmd.com/read/38609529/accelerating-data-sharing-and-reuse-in-volume-electron-microscopy
#1
JOURNAL ARTICLE
Kirk James Czymmek, Ilya Belevich, Johanna Bischof, Aastha Mathur, Lucy Collinson, Eija Jokitalo
No abstract text is available yet for this article.
April 12, 2024: Nature Cell Biology
https://read.qxmd.com/read/38605144/a-crispri-a-screening-platform-to-study-cellular-nutrient-transport-in-diverse-microenvironments
#2
JOURNAL ARTICLE
Christopher Chidley, Alicia M Darnell, Benjamin L Gaudio, Evan C Lien, Anna M Barbeau, Matthew G Vander Heiden, Peter K Sorger
Blocking the import of nutrients essential for cancer cell proliferation represents a therapeutic opportunity, but it is unclear which transporters to target. Here we report a CRISPR interference/activation screening platform to systematically interrogate the contribution of nutrient transporters to support cancer cell proliferation in environments ranging from standard culture media to tumours. We applied this platform to identify the transporters of amino acids in leukaemia cells and found that amino acid transport involves high bidirectional flux dependent on the microenvironment composition...
April 11, 2024: Nature Cell Biology
https://read.qxmd.com/read/38600237/tissue-pressure-and-yap-during-organogenesis
#3
JOURNAL ARTICLE
Qian Xu, Thomas G H Diekwisch
No abstract text is available yet for this article.
April 10, 2024: Nature Cell Biology
https://read.qxmd.com/read/38600236/transcription-coupled-dna-protein-crosslink-repair-by-csb-and-crl4-csa-mediated-degradation
#4
JOURNAL ARTICLE
Marjolein van Sluis, Qing Yu, Melanie van der Woude, Camila Gonzalo-Hansen, Shannon C Dealy, Roel C Janssens, Hedda B Somsen, Anisha R Ramadhin, Dick H W Dekkers, Hannah Lena Wienecke, Joris J P G Demmers, Anja Raams, Carlota Davó-Martínez, Diana A Llerena Schiffmacher, Marvin van Toorn, David Häckes, Karen L Thijssen, Di Zhou, Judith G Lammers, Alex Pines, Wim Vermeulen, Joris Pothof, Jeroen A A Demmers, Debbie L C van den Berg, Hannes Lans, Jurgen A Marteijn
DNA-protein crosslinks (DPCs) arise from enzymatic intermediates, metabolism or chemicals like chemotherapeutics. DPCs are highly cytotoxic as they impede DNA-based processes such as replication, which is counteracted through proteolysis-mediated DPC removal by spartan (SPRTN) or the proteasome. However, whether DPCs affect transcription and how transcription-blocking DPCs are repaired remains largely unknown. Here we show that DPCs severely impede RNA polymerase II-mediated transcription and are preferentially repaired in active genes by transcription-coupled DPC (TC-DPC) repair...
April 10, 2024: Nature Cell Biology
https://read.qxmd.com/read/38600235/transcription-coupled-repair-of-dna-protein-cross-links-depends-on-csa-and-csb
#5
JOURNAL ARTICLE
Christopher J Carnie, Aleida C Acampora, Aldo S Bader, Chimeg Erdenebat, Shubo Zhao, Elnatan Bitensky, Diana van den Heuvel, Avital Parnas, Vipul Gupta, Giuseppina D'Alessandro, Matylda Sczaniecka-Clift, Pedro Weickert, Fatih Aygenli, Maximilian J Götz, Jacqueline Cordes, Isabel Esain-Garcia, Larry Melidis, Annelotte P Wondergem, Simon Lam, Maria S Robles, Shankar Balasubramanian, Sheera Adar, Martijn S Luijsterburg, Stephen P Jackson, Julian Stingele
Covalent DNA-protein cross-links (DPCs) are toxic DNA lesions that block replication and require repair by multiple pathways. Whether transcription blockage contributes to the toxicity of DPCs and how cells respond when RNA polymerases stall at DPCs is unknown. Here we find that DPC formation arrests transcription and induces ubiquitylation and degradation of RNA polymerase II. Using genetic screens and a method for the genome-wide mapping of DNA-protein adducts, DPC sequencing, we discover that Cockayne syndrome (CS) proteins CSB and CSA provide resistance to DPC-inducing agents by promoting DPC repair in actively transcribed genes...
April 10, 2024: Nature Cell Biology
https://read.qxmd.com/read/38600234/endogenous-aldehyde-induced-dna-protein-crosslinks-are-resolved-by-transcription-coupled-repair
#6
JOURNAL ARTICLE
Yasuyoshi Oka, Yuka Nakazawa, Mayuko Shimada, Tomoo Ogi
DNA-protein crosslinks (DPCs) induced by aldehydes interfere with replication and transcription. Hereditary deficiencies in DPC repair and aldehyde clearance processes cause progeria, including Ruijs-Aalfs syndrome (RJALS) and AMeD syndrome (AMeDS) in humans. Although the elimination of DPC during replication has been well established, how cells overcome DPC lesions in transcription remains elusive. Here we show that endogenous aldehyde-induced DPC roadblocks are efficiently resolved by transcription-coupled repair (TCR)...
April 10, 2024: Nature Cell Biology
https://read.qxmd.com/read/38600233/adding-a-transcription-coupled-repair-pathway
#7
JOURNAL ARTICLE
Marco Saponaro
No abstract text is available yet for this article.
April 10, 2024: Nature Cell Biology
https://read.qxmd.com/read/38594588/fatty-acyl-coenzyme-a-activates-mitochondrial-division-through-oligomerization-of-mid49-and-mid51
#8
JOURNAL ARTICLE
Ao Liu, Frieda Kage, Asan F Abdulkareem, Mac Pholo Aguirre-Huamani, Gracie Sapp, Halil Aydin, Henry N Higgs
Mitochondrial fission occurs in many cellular processes, but the regulation of fission is poorly understood. We show that long-chain acyl-coenzyme A (LCACA) activates two related mitochondrial fission proteins, MiD49 and MiD51, by inducing their oligomerization, which activates their ability to stimulate the DRP1 GTPase. The 1:1 stoichiometry of LCACA:MiD in the oligomer suggests interaction in the previously identified nucleotide-binding pocket, and a point mutation in this pocket reduces LCACA binding and LCACA-induced oligomerization for MiD51...
April 9, 2024: Nature Cell Biology
https://read.qxmd.com/read/38594587/cd32-captures-committed-haemogenic-endothelial-cells-during-human-embryonic-development
#9
JOURNAL ARTICLE
Rebecca Scarfò, Lauren N Randolph, Monah Abou Alezz, Mahassen El Khoury, Amélie Gersch, Zhong-Yin Li, Stephanie A Luff, Andrea Tavosanis, Giulia Ferrari Ramondo, Sara Valsoni, Sara Cascione, Emma Didelon, Laura Passerini, Giada Amodio, Chiara Brandas, Anna Villa, Silvia Gregori, Ivan Merelli, Jean-Noël Freund, Christopher M Sturgeon, Manuela Tavian, Andrea Ditadi
During embryonic development, blood cells emerge from specialized endothelial cells, named haemogenic endothelial cells (HECs). As HECs are rare and only transiently found in early developing embryos, it remains difficult to distinguish them from endothelial cells. Here we performed transcriptomic analysis of 28- to 32-day human embryos and observed that the expression of Fc receptor CD32 (FCGR2B) is highly enriched in the endothelial cell population that contains HECs. Functional analyses using human embryonic and human pluripotent stem cell-derived endothelial cells revealed that robust multilineage haematopoietic potential is harboured within CD32+ endothelial cells and showed that 90% of CD32+ endothelial cells are bona fide HECs...
April 9, 2024: Nature Cell Biology
https://read.qxmd.com/read/38589534/transcription-bodies-regulate-gene-expression-by-sequestering-cdk9
#10
JOURNAL ARTICLE
Martino Ugolini, Maciej A Kerlin, Ksenia Kuznetsova, Haruka Oda, Hiroshi Kimura, Nadine L Vastenhouw
The localization of transcriptional activity in specialized transcription bodies is a hallmark of gene expression in eukaryotic cells. It remains unclear, however, if and how transcription bodies affect gene expression. Here we disrupted the formation of two prominent endogenous transcription bodies that mark the onset of zygotic transcription in zebrafish embryos and analysed the effect on gene expression using enriched SLAM-seq and live-cell imaging. We find that the disruption of transcription bodies results in the misregulation of hundreds of genes...
April 8, 2024: Nature Cell Biology
https://read.qxmd.com/read/38589533/judith-campisi-1948-2024
#11
EDITORIAL
Simon Melov, Birgit Schilling, Lisa M Ellerby, Pankaj Kapahi
No abstract text is available yet for this article.
April 8, 2024: Nature Cell Biology
https://read.qxmd.com/read/38589532/transcriptional-bodies-manage-tight-resources
#12
JOURNAL ARTICLE
Natalia Stec, Adam Klosin
No abstract text is available yet for this article.
April 8, 2024: Nature Cell Biology
https://read.qxmd.com/read/38589531/a-lipid-atlas-of-human-and-mouse-immune-cells-provides-insights-into-ferroptosis-susceptibility
#13
JOURNAL ARTICLE
Pooranee K Morgan, Gerard Pernes, Kevin Huynh, Corey Giles, Sudip Paul, Adam Alexander T Smith, Natalie A Mellett, Amy Liang, Tilly van Buuren-Milne, Camilla Bertuzzo Veiga, Thomas J C Collins, Yangsong Xu, Man K S Lee, T Michael De Silva, Peter J Meikle, Graeme I Lancaster, Andrew J Murphy
The cellular lipidome comprises thousands of unique lipid species. Here, using mass spectrometry-based targeted lipidomics, we characterize the lipid landscape of human and mouse immune cells ( www.cellularlipidatlas.com ). Using this resource, we show that immune cells have unique lipidomic signatures and that processes such as activation, maturation and development impact immune cell lipid composition. To demonstrate the potential of this resource to provide insights into immune cell biology, we determine how a cell-specific lipid trait-differences in the abundance of polyunsaturated fatty acid-containing glycerophospholipids (PUFA-PLs)-influences immune cell biology...
April 8, 2024: Nature Cell Biology
https://read.qxmd.com/read/38589530/lipidomes-define-immune-cell-identity
#14
JOURNAL ARTICLE
Kandice R Levental, Whitney S Henry
No abstract text is available yet for this article.
April 8, 2024: Nature Cell Biology
https://read.qxmd.com/read/38570617/proliferation-driven-mechanical-compression-induces-signalling-centre-formation-during-mammalian-organ-development
#15
JOURNAL ARTICLE
Neha Pincha Shroff, Pengfei Xu, Sangwoo Kim, Elijah R Shelton, Ben J Gross, Yucen Liu, Carlos O Gomez, Qianlin Ye, Tingsheng Yu Drennon, Jimmy K Hu, Jeremy B A Green, Otger Campàs, Ophir D Klein
Localized sources of morphogens, called signalling centres, play a fundamental role in coordinating tissue growth and cell fate specification during organogenesis. However, how these signalling centres are established in tissues during embryonic development is still unclear. Here we show that the main signalling centre orchestrating development of rodent incisors, the enamel knot (EK), is specified by a cell proliferation-driven buildup in compressive stresses (mechanical pressure) in the tissue. Direct mechanical measurements indicate that the stresses generated by cell proliferation are resisted by the surrounding tissue, creating a circular pattern of mechanical anisotropy with a region of high compressive stress at its centre that becomes the EK...
April 3, 2024: Nature Cell Biology
https://read.qxmd.com/read/38561547/glucose-controls-lipolysis-through-golgi-ptdins4p-mediated-regulation-of-atgl
#16
JOURNAL ARTICLE
Lianggong Ding, Florian Huwyler, Fen Long, Wu Yang, Jonas Binz, Kendra Wernlé, Matthias Pfister, Manuel Klug, Miroslav Balaz, Barbara Ukropcova, Jozef Ukropec, Chunyan Wu, Tongtong Wang, Min Gao, Pierre-Alain Clavien, Philipp Dutkowski, Mark W Tibbitt, Christian Wolfrum
Metabolic crosstalk of the major nutrients glucose, amino acids and fatty acids (FAs) ensures systemic metabolic homeostasis. The coordination between the supply of glucose and FAs to meet various physiological demands is especially important as improper nutrient levels lead to metabolic disorders, such as diabetes and metabolic dysfunction-associated steatohepatitis (MASH). In response to the oscillations in blood glucose levels, lipolysis is thought to be mainly regulated hormonally to control FA liberation from lipid droplets by insulin, catecholamine and glucagon...
April 1, 2024: Nature Cell Biology
https://read.qxmd.com/read/38553595/cyclophilin-a-supports-translation-of-intrinsically-disordered-proteins-and-affects-haematopoietic-stem-cell-ageing
#17
JOURNAL ARTICLE
Laure Maneix, Polina Iakova, Charles G Lee, Shannon E Moree, Xuan Lu, Gandhar K Datar, Cedric T Hill, Eric Spooner, Jordon C K King, David B Sykes, Borja Saez, Bruno Di Stefano, Xi Chen, Daniela S Krause, Ergun Sahin, Francis T F Tsai, Margaret A Goodell, Bradford C Berk, David T Scadden, André Catic
Loss of protein function is a driving force of ageing. We have identified peptidyl-prolyl isomerase A (PPIA or cyclophilin A) as a dominant chaperone in haematopoietic stem and progenitor cells. Depletion of PPIA accelerates stem cell ageing. We found that proteins with intrinsically disordered regions (IDRs) are frequent PPIA substrates. IDRs facilitate interactions with other proteins or nucleic acids and can trigger liquid-liquid phase separation. Over 20% of PPIA substrates are involved in the formation of supramolecular membrane-less organelles...
March 29, 2024: Nature Cell Biology
https://read.qxmd.com/read/38548891/disordered-c-terminal-domain-drives-spatiotemporal-confinement-of-rnapii-to-enhance-search-for-chromatin-targets
#18
JOURNAL ARTICLE
Yick Hin Ling, Ziyang Ye, Chloe Liang, Chuofan Yu, Giho Park, Jeffry L Corden, Carl Wu
Efficient gene expression requires RNA polymerase II (RNAPII) to find chromatin targets precisely in space and time. How RNAPII manages this complex diffusive search in three-dimensional nuclear space remains largely unknown. The disordered carboxy-terminal domain (CTD) of RNAPII, which is essential for recruiting transcription-associated proteins, forms phase-separated droplets in vitro, hinting at a potential role in modulating RNAPII dynamics. In the present study, we use single-molecule tracking and spatiotemporal mapping in living yeast to show that the CTD is required for confining RNAPII diffusion within a subnuclear region enriched for active genes, but without apparent phase separation into condensates...
March 28, 2024: Nature Cell Biology
https://read.qxmd.com/read/38548890/a-cell-fate-decision-map-reveals-abundant-direct-neurogenesis-bypassing-intermediate-progenitors-in-the-human-developing-neocortex
#19
JOURNAL ARTICLE
Laure Coquand, Clarisse Brunet Avalos, Anne-Sophie Macé, Sarah Farcy, Amandine Di Cicco, Marusa Lampic, Ryszard Wimmer, Betina Bessières, Tania Attie-Bitach, Vincent Fraisier, Pierre Sens, Fabien Guimiot, Jean-Baptiste Brault, Alexandre D Baffet
The human neocortex has undergone strong evolutionary expansion, largely due to an increased progenitor population, the basal radial glial cells. These cells are responsible for the production of a diversity of cell types, but the successive cell fate decisions taken by individual progenitors remain unknown. Here we developed a semi-automated live/fixed correlative imaging method to map basal radial glial cell division modes in early fetal tissue and cerebral organoids. Through the live analysis of hundreds of dividing progenitors, we show that basal radial glial cells undergo abundant symmetric amplifying divisions, and frequent self-consuming direct neurogenic divisions, bypassing intermediate progenitors...
March 28, 2024: Nature Cell Biology
https://read.qxmd.com/read/38538837/defective-prelamin-a-processing-promotes-unconventional-necroptosis-driven-by-nuclear-ripk1
#20
JOURNAL ARTICLE
Yuanxin Yang, Jian Zhang, Mingming Lv, Na Cui, Bing Shan, Qi Sun, Lingjie Yan, Mengmeng Zhang, Chengyu Zou, Junying Yuan, Daichao Xu
Defects in the prelamin A processing enzyme caused by loss-of-function mutations in the ZMPSTE24 gene are responsible for a spectrum of progeroid disorders characterized by the accumulation of farnesylated prelamin A. Here we report that defective prelamin A processing triggers nuclear RIPK1-dependent signalling that leads to necroptosis and inflammation. We show that accumulated prelamin A recruits RIPK1 to the nucleus to facilitate its activation upon tumour necrosis factor stimulation in ZMPSTE24-deficient cells...
March 27, 2024: Nature Cell Biology
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