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The Twitter hashtag that put a spotlight on racism in academia 期刊论文
NATURE, 2020, 582 (7812) : 327-327
作者:  Lee, Yang;  Warne, Tony;  Nehme, Rony;  Pandey, Shubhi;  Dwivedi-Agnihotri, Hemlata;  Chaturvedi, Madhu;  Edwards, Patricia C.;  Garcia-Nafria, Javier;  Leslie, Andrew G. W.;  Shukla, Arun K.;  Tate, Christopher G.
收藏  |  浏览/下载:23/0  |  提交时间:2020/07/03
Brain control of humoral immune responses amenable to behavioural modulation 期刊论文
NATURE, 2020, 581 (7807)
作者:  Yang, C. H.;  Leon, R. C. C.;  Hwang, J. C. C.;  Saraiva, A.;  Tanttu, T.;  Huang, W.;  Lemyre, J. Camirand;  Chan, K. W.;  Tan, K. Y.;  Hudson, F. E.;  Itoh, K. M.;  Morello, A.;  Pioro-Ladriere, M.;  Laucht, A.;  Dzurak, A. S.
收藏  |  浏览/下载:12/0  |  提交时间:2020/07/03

It has been speculated that brain activities might directly control adaptive immune responses in lymphoid organs, although there is little evidence for this. Here we show that splenic denervation in mice specifically compromises the formation of plasma cells during a T cell-dependent but not T cell-independent immune response. Splenic nerve activity enhances plasma cell production in a manner that requires B-cell responsiveness to acetylcholine mediated by the alpha 9 nicotinic receptor, and T cells that express choline acetyl transferase(1,2) probably act as a relay between the noradrenergic nerve and acetylcholine-responding B cells. We show that neurons in the central nucleus of the amygdala (CeA) and the paraventricular nucleus (PVN) that express corticotropin-releasing hormone (CRH) are connected to the splenic nerve  ablation or pharmacogenetic inhibition of these neurons reduces plasma cell formation, whereas pharmacogenetic activation of these neurons increases plasma cell abundance after immunization. In a newly developed behaviour regimen, mice are made to stand on an elevated platform, leading to activation of CeA and PVN CRH neurons and increased plasma cell formation. In immunized mice, the elevated platform regimen induces an increase in antigen-specific IgG antibodies in a manner that depends on CRH neurons in the CeA and PVN, an intact splenic nerve, and B cell expression of the alpha 9 acetylcholine receptor. By identifying a specific brain-spleen neural connection that autonomically enhances humoral responses and demonstrating immune stimulation by a bodily behaviour, our study reveals brain control of adaptive immunity and suggests the possibility to enhance immunocompetency by behavioural intervention.


Neuronal activities in the central amygdala and paraventricular nucleus are transmitted via the splenic nerve to increase plasma cell formation after immunization, and this process can be behaviourally enhanced in mice.


  
Neuronal programming by microbiota regulates intestinal physiology 期刊论文
NATURE, 2020, 578 (7794) : 284-+
作者:  Li, Yilong;  Roberts, Nicola D.;  Wala, Jeremiah A.;  Shapira, Ofer;  Schumacher, Steven E.;  Kumar, Kiran;  Khurana, Ekta;  Waszak, Sebastian;  Korbel, Jan O.;  Haber, James E.;  Imielinski, Marcin;  Weischenfeldt, Joachim;  Beroukhim, Rameen;  Campbell, Peter J.;  Akdemir, Kadir C.;  Alvarez, Eva G.;  Baez-Ortega, Adrian;  Boutros, Paul C.;  Bowtell, David D. L.;  Brors, Benedikt;  Burns, Kathleen H.;  Chan, Kin;  Chen, Ken;  Cortes-Ciriano, Isidro;  Dueso-Barroso, Ana;  Dunford, Andrew J.;  Edwards, Paul A.;  Estivill, Xavier;  Etemadmoghadam, Dariush;  Feuerbach, Lars;  Fink, J. Lynn;  Frenkel-Morgenstern, Milana;  Garsed, Dale W.;  Gerstein, Mark;  Gordenin, Dmitry A.;  Haan, David;  Hess, Julian M.;  Hutter, Barbara;  Jones, David T. W.;  Ju, Young Seok;  Kazanov, Marat D.;  Klimczak, Leszek J.;  Koh, Youngil;  Lee, Eunjung Alice;  Lee, Jake June-Koo;  Lynch, Andy G.;  Macintyre, Geoff;  Markowetz, Florian;  Martincorena, Inigo;  Martinez-Fundichely, Alexander;  Meyerson, Matthew;  Miyano, Satoru;  Nakagawa, Hidewaki;  Navarro, Fabio C. P.;  Ossowski, Stephan;  Park, Peter J.;  Pearson, John, V;  Puiggros, Montserrat;  Rippe, Karsten;  Roberts, Steven A.;  Rodriguez-Martin, Bernardo;  Scully, Ralph;  Shackleton, Mark;  Sidiropoulos, Nikos;  Sieverling, Lina;  Stewart, Chip;  Torrents, David;  Tubio, Jose M. C.;  Villasante, Izar;  Waddell, Nicola;  Yang, Lixing;  Yao, Xiaotong;  Yoon, Sung-Soo;  Zamora, Jorge;  Zhang, Cheng-Zhong
收藏  |  浏览/下载:40/0  |  提交时间:2020/07/03

Neural control of the function of visceral organs is essential for homeostasis and health. Intestinal peristalsis is critical for digestive physiology and host defence, and is often dysregulated in gastrointestinal disorders(1). Luminal factors, such as diet and microbiota, regulate neurogenic programs of gut motility(2-5), but the underlying molecular mechanisms remain unclear. Here we show that the transcription factor aryl hydrocarbon receptor (AHR) functions as a biosensor in intestinal neural circuits, linking their functional output to the microbial environment of the gut lumen. Using nuclear RNA sequencing of mouse enteric neurons that represent distinct intestinal segments and microbiota states, we demonstrate that the intrinsic neural networks of the colon exhibit unique transcriptional profiles that are controlled by the combined effects of host genetic programs and microbial colonization. Microbiota-induced expression of AHR in neurons of the distal gastrointestinal tract enables these neurons to respond to the luminal environment and to induce expression of neuron-specific effector mechanisms. Neuron-specific deletion of Ahr, or constitutive overexpression of its negative feedback regulator CYP1A1, results in reduced peristaltic activity of the colon, similar to that observed in microbiota-depleted mice. Finally, expression of Ahr in the enteric neurons of mice treated with antibiotics partially restores intestinal motility. Together, our experiments identify AHR signalling in enteric neurons as a regulatory node that integrates the luminal environment with the physiological output of intestinal neural circuits to maintain gut homeostasis and health.


In a mouse model, aryl hydrocarbon receptor signalling in enteric neurons is revealed as a mechanism that helps to maintain gut homeostasis by integrating the luminal environment with the physiology of intestinal neural circuits.


  
Live-animal imaging of native haematopoietic stem and progenitor cells 期刊论文
NATURE, 2020, 578 (7794) : 278-+
作者:  Gerstung, Moritz;  Jolly, Clemency;  Leshchiner, Ignaty;  Dentro, Stefan C.;  Gonzalez, Santiago;  Rosebrock, Daniel;  Mitchell, Thomas J.;  Rubanova, Yulia;  Anur, Pavana;  Yu, Kaixian;  Tarabichi, Maxime;  Deshwar, Amit;  Wintersinger, Jeff;  Kleinheinz, Kortine;  Vazquez-Garcia, Ignacio;  Haase, Kerstin;  Jerman, Lara;  Sengupta, Subhajit;  Macintyre, Geoff;  Malikic, Salem;  Donmez, Nilgun;  Livitz, Dimitri G.;  Cmero, Marek;  Demeulemeester, Jonas;  Schumacher, Steven;  Fan, Yu;  Yao, Xiaotong;  Lee, Juhee;  Schlesner, Matthias;  Boutros, Paul C.;  Bowtell, David D.;  Zhu, Hongtu;  Getz, Gad;  Imielinski, Marcin;  Beroukhim, Rameen;  Sahinalp, S. Cenk;  Ji, Yuan;  Peifer, Martin;  Markowetz, Florian;  Mustonen, Ville;  Yuan, Ke;  Wang, Wenyi;  Morris, Quaid D.;  Spellman, Paul T.;  Wedge, David C.;  Van Loo, Peter;  Deshwar, Amit G.;  Adams, David J.;  Campbell, Peter J.;  Cao, Shaolong;  Christie, Elizabeth L.;  Cun, Yupeng;  Dawson, Kevin J.;  Drews, Ruben M.;  Eils, Roland;  Fittall, Matthew;  Garsed, Dale W.;  Ha, Gavin;  Lee-Six, Henry;  Martincorena, Inigo;  Oesper, Layla;  Peto, Myron;  Raphael, Benjamin J.;  Salcedo, Adriana;  Shi, Ruian;  Shin, Seung Jun;  Spiro, Oliver;  Stein, Lincoln D.;  Vembu, Shankar;  Wheeler, David A.;  Yang, Tsun-Po
收藏  |  浏览/下载:15/0  |  提交时间:2020/07/03

The biology of haematopoietic stem cells (HSCs) has predominantly been studied under transplantation conditions(1,2). It has been particularly challenging to study dynamic HSC behaviour, given that the visualization of HSCs in the native niche in live animals has not, to our knowledge, been achieved. Here we describe a dual genetic strategy in mice that restricts reporter labelling to a subset of the most quiescent long-term HSCs (LT-HSCs) and that is compatible with current intravital imaging approaches in the calvarial bone marrow(3-5). We show that this subset of LT-HSCs resides close to both sinusoidal blood vessels and the endosteal surface. By contrast, multipotent progenitor cells (MPPs) show greater variation in distance from the endosteum and are more likely to be associated with transition zone vessels. LT-HSCs are not found in bone marrow niches with the deepest hypoxia and instead are found in hypoxic environments similar to those of MPPs. In vivo time-lapse imaging revealed that LT-HSCs at steady-state show limited motility. Activated LT-HSCs show heterogeneous responses, with some cells becoming highly motile and a fraction of HSCs expanding clonally within spatially restricted domains. These domains have defined characteristics, as HSC expansion is found almost exclusively in a subset of bone marrow cavities with bone-remodelling activity. By contrast, cavities with low bone-resorbing activity do not harbour expanding HSCs. These findings point to previously unknown heterogeneity within the bone marrow microenvironment, imposed by the stages of bone turnover. Our approach enables the direct visualization of HSC behaviours and dissection of heterogeneity in HSC niches.


A dual genetic strategy enables the labelling and in vivo imaging of native long-term haematopoietic stem cells in the mouse calvarial bone marrow.


  
Tropical cyclone sensitivities to CO2 doubling: roles of atmospheric resolution, synoptic variability and background climate changes 期刊论文
CLIMATE DYNAMICS, 2019, 53: 5999-6033
作者:  Vecchi, Gabriel A.;  Delworth, Thomas L.;  Murakami, Hiroyuki;  Underwood, Seth D.;  Wittenberg, Andrew T.;  Zeng, Fanrong;  Zhang, Wei;  Baldwin, Jane W.;  Bhatia, Kieran T.;  Cooke, William;  He, Jie;  Kapnick, Sarah B.;  Knutson, Thomas R.;  Villarini, Gabriele;  van der Wiel, Karin;  Anderson, Whit;  Balaji, V.;  Chen, Jan-Huey;  Dixon, Keith W.;  Gudgel, Rich;  Harris, Lucas M.;  Jia, Liwei;  Johnson, Nathaniel C.;  Lin, Shian-Jiann;  Liu, Maofeng;  Ng, Ching Ho Justin;  Rosati, Anthony;  Smith, James A.;  Yang, Xiaosong
收藏  |  浏览/下载:13/0  |  提交时间:2019/11/27
Magnetic Weyl semimetal phase in a Kagome crystal 期刊论文
SCIENCE, 2019, 365 (6459) : 1282-+
作者:  Liu, D. F.;  Liang, A. J.;  Liu, E. K.;  Xu, Q. N.;  Li, Y. W.;  Chen, C.;  Pei, D.;  Shi, W. J.;  Mo, S. K.;  Dudin, P.;  Kim, T.;  Cacho, C.;  Li, G.;  Sun, Y.;  Yang, L. X.;  Liu, Z. K.;  Parkin, S. S. P.;  Felser, C.;  Chen, Y. L.
收藏  |  浏览/下载:10/0  |  提交时间:2019/11/27
Seasonal climatic effects and feedbacks of anthropogenic heat release due to global energy consumption with CAM5 期刊论文
CLIMATE DYNAMICS, 2019, 52 (11) : 6377-6390
作者:  Chen, Bing;  Wu, C.;  Liu, X.;  Chen, L.;  Wu, Jian;  Yang, H.;  Luo, Tao;  Wu, Xue;  Jiang, Yiquan;  Jiang, Lei;  Brown, H. Y.;  Lu, Z.;  Fan, W.;  Lin, G.;  Sun, Bo;  Wu, M.
收藏  |  浏览/下载:18/0  |  提交时间:2019/11/26
Anthropogenic heat release  Climatic effect  Climate feedback  Climate change  
Climate-driven reduction of genetic variation in plant phenology alters soil communities and nutrient pools 期刊论文
GLOBAL CHANGE BIOLOGY, 2019, 25 (4) : 1514-1528
作者:  Ware, Ian M.;  Van Nuland, Michael E.;  Schweitzer, Jennifer A.;  Yang, Zamin;  Schadt, Christopher W.;  Sidak-Loftis, Lindsay C.;  Stone, Nathan E.;  Busch, Joseph D.;  Wagner, David M.;  Bailey, Joseph K.
收藏  |  浏览/下载:9/0  |  提交时间:2019/04/09
climate  ecosystem dynamics  genetic divergence  intraspecific variation  phenology  Populus  
Natural, incidental, and engineered nanomaterials and their impacts on the Earth system 期刊论文
SCIENCE, 2019, 363 (6434) : 1414-+
作者:  Hochella, Michael F., Jr.;  Mogk, David W.;  Ranville, James;  Allen, Irving C.;  Luther, George W.;  Marr, Linsey C.;  McGrail, B. Peter;  Murayama, Mitsu;  Qafoku, Nikolla P.;  Rosso, Kevin M.;  Sahai, Nita;  Schroeder, Paul A.;  Vikesland, Peter;  Westerhoff, Paul;  Yang, Yi
收藏  |  浏览/下载:9/0  |  提交时间:2019/11/27
A sea change in our view of overturning in the subpolar North Atlantic 期刊论文
SCIENCE, 2019, 363 (6426) : 516-+
作者:  Lozier, M. S.;  Li, F.;  Bacon, S.;  Bahr, F.;  Bower, A. S.;  Cunningham, S. A.;  de Jong, M. F.;  de Steur, L.;  deYoung, B.;  Fischer, J.;  Gary, S. F.;  Greenan, B. J. W.;  Holliday, N. P.;  Houk, A.;  Houpert, L.;  Inall, M. E.;  Johns, W. E.;  Johnson, H. L.;  Johnson, C.;  Karstensen, J.;  Koman, G.;  Le Bras, I. A.;  Lin, X.;  Mackay, N.;  Marshall, D. P.;  Mercier, H.;  Oltmanns, M.;  Pickart, R. S.;  Ramsey, A. L.;  Rayner, D.;  Straneo, F.;  Thierry, V.;  Torres, D. J.;  Williams, R. G.;  Wilson, C.;  Yang, J.;  Yashayaev, I.;  Zhao, J.
收藏  |  浏览/下载:9/0  |  提交时间:2019/11/27