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Paracrine orchestration of intestinal tumorigenesis by a mesenchymal niche 期刊论文
NATURE, 2020, 580 (7804) : 524-+
作者:  Poore, Gregory D.;  Kopylova, Evguenia;  Zhu, Qiyun;  Carpenter, Carolina;  Fraraccio, Serena;  Wandro, Stephen;  Kosciolek, Tomasz;  Janssen, Stefan;  Metcalf, Jessica;  Song, Se Jin;  Kanbar, Jad;  Miller-Montgomery, Sandrine;  Heaton, Robert;  Mckay, Rana;  Patel, Sandip Pravin;  Swafford, Austin D.;  Knight, Rob
收藏  |  浏览/下载:40/0  |  提交时间:2020/07/03

The initiation of an intestinal tumour is a probabilistic process that depends on the competition between mutant and normal epithelial stem cells in crypts(1). Intestinal stem cells are closely associated with a diverse but poorly characterized network of mesenchymal cell types(2,3). However, whether the physiological mesenchymal microenvironment of mutant stem cells affects tumour initiation remains unknown. Here we provide in vivo evidence that the mesenchymal niche controls tumour initiation in trans. By characterizing the heterogeneity of the intestinal mesenchyme using single-cell RNA-sequencing analysis, we identified a population of rare pericryptal Ptgs2-expressing fibroblasts that constitutively process arachidonic acid into highly labile prostaglandin E-2 (PGE(2)). Specific ablation of Ptgs2 in fibroblasts was sufficient to prevent tumour initiation in two different models of sporadic, autochthonous tumorigenesis. Mechanistically, single-cell RNA-sequencing analyses of a mesenchymal niche model showed that fibroblast-derived PGE(2) drives the expansion omicron f a population of Sca-1(+) reserve-like stem cells. These express a strong regenerative/tumorigenic program, driven by the Hippo pathway effector Yap. In vivo, Yap is indispensable for Sca-1(+) cell expansion and early tumour initiation and displays a nuclear localization in both mouse and human adenomas. Using organoid experiments, we identified a molecular mechanism whereby PGE(2) promotes Yap dephosphorylation, nuclear translocation and transcriptional activity by signalling through the receptor Ptger4. Epithelial-specific ablation of Ptger4 misdirected the regenerative reprogramming of stem cells and prevented Sca-1(+) cell expansion and sporadic tumour initiation in mutant mice, thereby demonstrating the robust paracrine control of tumour-initiating stem cells by PGE(2)-Ptger4. Analyses of patient-derived organoids established that PGE(2)-PTGER4 also regulates stem-cell function in humans. Our study demonstrates that initiation of colorectal cancer is orchestrated by the mesenchymal niche and reveals a mechanism by which rare pericryptal Ptgs2-expressing fibroblasts exert paracrine control over tumour-initiating stem cells via the druggable PGE(2)-Ptger4-Yap signalling axis.


Single-cell RNA-sequencing analysis of intestinal mesenchyme identified a population of fibroblasts that produce prostaglandin E-2, which, when disrupted, prevented initiation of intestinal tumours.


  
Construction of a human cell landscape at single-cell level 期刊论文
NATURE, 2020, 581 (7808) : 303-+
作者:  Han, Yan;  Reyes, Alexis A.;  Malik, Sara;  He, Yuan
收藏  |  浏览/下载:12/0  |  提交时间:2020/07/03

Single-cell analysis is a valuable tool for dissecting cellular heterogeneity in complex systems(1). However, a comprehensive single-cell atlas has not been achieved for humans. Here we use single-cell mRNA sequencing to determine the cell-type composition of all major human organs and construct a scheme for the human cell landscape (HCL). We have uncovered a single-cell hierarchy for many tissues that have not been well characterized. We established a '  single-cell HCL analysis'  pipeline that helps to define human cell identity. Finally, we performed a single-cell comparative analysis of landscapes from human and mouse to identify conserved genetic networks. We found that stem and progenitor cells exhibit strong transcriptomic stochasticity, whereas differentiated cells are more distinct. Our results provide a useful resource for the study of human biology.


Single-cell RNA sequencing is used to generate a dataset covering all major human organs in both adult and fetal stages, enabling comparison with similar datasets for mouse tissues.


  
Nitrogen deposition outweighs climatic variability in driving annual growth rate of canopy beech trees: Evidence from long-term growth reconstruction across a geographic gradient 期刊论文
GLOBAL CHANGE BIOLOGY, 2018, 24 (7) : 2898-2912
作者:  Gentilesca, Tiziana;  Rita, Angelo;  Brunetti, Michele;  Giammarchi, Francesco;  Leonardi, Stefano;  Magnani, Federico;  van Noije, Twan;  Tonon, Giustino;  Borghetti, Marco
收藏  |  浏览/下载:5/0  |  提交时间:2019/04/09
age  climate change  Fagus sylvatica L  forest  height growth  nitrogen deposition  stem analysis  volume growth  
Carbon stock classification for tropical forests in Brazil: Understanding the effect of stand and climate variables 期刊论文
FOREST ECOLOGY AND MANAGEMENT, 2017, 404
作者:  David, Hassan Camil;  Gomes de Araujo, Emanuel Jose;  Morais, Vinicius Augusto;  Soares Scolforo, Jose Roberto;  Marques, Jair Mendes;  Netto, Sylvio Pellico;  MacFarlane, David W.
收藏  |  浏览/下载:8/0  |  提交时间:2019/04/09
Discriminant analysis  Stem carbon  Temperature and precipitation  Mean diameter and height  Brazilian biomes  
Vulnerability to forest loss through altered postfire recovery dynamics in a warming climate in the Klamath Mountains 期刊论文
GLOBAL CHANGE BIOLOGY, 2017, 23 (10)
作者:  Tepley, Alan J.;  Thompson, Jonathan R.;  Epstein, Howard E.;  Anderson-Teixeira, Kristina J.
收藏  |  浏览/下载:5/0  |  提交时间:2019/04/09
Douglas-fir  forest resilience  Klamath Mountains  postfire recruitment  propagule pressure  reburn  stem analysis  tipping point  tree regeneration  
Steps Toward a Formative Evaluation of NSDL 科技报告
来源:Rand Corporation. 出版年: 2011
作者:  Tora K. Bikson;  Nidhi Kalra;  Lionel A. Galway;  Grace Agnew
收藏  |  浏览/下载:4/0  |  提交时间:2019/04/05
STEM Education  Educational Technology  Program Evaluation  Databases and Data Collection, Analysis and Processing