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Microbial bile acid metabolites modulate gut ROR gamma(+) regulatory T cell homeostasis 期刊论文
NATURE, 2020, 577 (7790) : 410-+
作者:  Bhargava, Manjul
收藏  |  浏览/下载:31/0  |  提交时间:2020/07/03

The metabolic pathways encoded by the human gut microbiome constantly interact with host gene products through numerous bioactive molecules(1). Primary bile acids (BAs) are synthesized within hepatocytes and released into the duodenum to facilitate absorption of lipids or fat-soluble vitamins(2). Some BAs (approximately 5%) escape into the colon, where gut commensal bacteria convert them into various intestinal BAs2 that are important hormones that regulate host cholesterol metabolism and energy balance via several nuclear receptors and/or G-protein-coupled receptors(3,4). These receptors have pivotal roles in shaping host innate immune responses(1,5). However, the effect of this host-microorganism biliary network on the adaptive immune system remains poorly characterized. Here we report that both dietary and microbial factors influence the composition of the gut BA pool and modulate an important population of colonic FOXP3(+) regulatory T (T-reg) cells expressing the transcription factor ROR gamma. Genetic abolition of BA metabolic pathways in individual gut symbionts significantly decreases this T-reg cell population. Restoration of the intestinal BA pool increases colonic ROR gamma(+) T-reg cell counts and ameliorates host susceptibility to inflammatory colitis via BA nuclear receptors. Thus, a pan-genomic biliary network interaction between hosts and their bacterial symbionts can control host immunological homeostasis via the resulting metabolites.


  
Informing management decisions for ecological networks, using dynamic models calibrated to noisy time-series data 期刊论文
ECOLOGY LETTERS, 2020, 23 (4) : 607-619
作者:  Adams, Matthew P.;  Sisson, Scott A.;  Helmstedt, Kate J.;  Baker, Christopher M.;  Holden, Matthew H.;  Plein, Michaela;  Holloway, Jacinta;  Mengersen, Kerrie L.;  McDonald-Madden, Eve
收藏  |  浏览/下载:20/0  |  提交时间:2020/07/02
Conservation  decision science  ecological forecasting  ecological modelling  food webs  interaction network  population dynamics  predator-prey interactions  prediction  uncertainty propagation  
Clades of huge phages from across Earth's ecosystems 期刊论文
NATURE, 2020, 578 (7795) : 425-+
作者:  Zhang, Bing;  Ma, Sai;  Rachmin, Inbal;  He, Megan;  Baral, Pankaj;  Choi, Sekyu;  Goncalves, William A.;  Shwartz, Yulia;  Fast, Eva M.;  Su, Yiqun;  Zon, Leonard I.;  Regev, Aviv;  Buenrostro, Jason D.;  Cunha, Thiago M.;  Chiu, Isaac M.
收藏  |  浏览/下载:78/0  |  提交时间:2020/07/03

Bacteriophages typically have small genomes(1) and depend on their bacterial hosts for replication(2). Here we sequenced DNA from diverse ecosystems and found hundreds of phage genomes with lengths of more than 200 kilobases (kb), including a genome of 735 kb, which is-to our knowledge-the largest phage genome to be described to date. Thirty-five genomes were manually curated to completion (circular and no gaps). Expanded genetic repertoires include diverse and previously undescribed CRISPR-Cas systems, transfer RNAs (tRNAs), tRNA synthetases, tRNA-modification enzymes, translation-initiation and elongation factors, and ribosomal proteins. The CRISPR-Cas systems of phages have the capacity to silence host transcription factors and translational genes, potentially as part of a larger interaction network that intercepts translation to redirect biosynthesis to phage-encoded functions. In addition, some phages may repurpose bacterial CRISPR-Cas systems to eliminate competing phages. We phylogenetically define the major clades of huge phages from human and other animal microbiomes, as well as from oceans, lakes, sediments, soils and the built environment. We conclude that the large gene inventories of huge phages reflect a conserved biological strategy, and that the phages are distributed across a broad bacterial host range and across Earth'  s ecosystems.


Genomic analyses of major clades of huge phages sampled from across Earth'  s ecosystems show that they have diverse genetic inventories, including a variety of CRISPR-Cas systems and translation-relevant genes.


  
Structure of the M2 muscarinic receptor-beta-arrestin complex in a lipid nanodisc 期刊论文
NATURE, 2020, 579 (7798) : 297-+
作者:  Gate, David;  Saligrama, Naresha;  Leventhal, Olivia;  Yang, Andrew C.;  Unger, Michael S.;  Middeldorp, Jinte;  Chen, Kelly;  Lehallier, Benoit;  Channappa, Divya;  De Los Santos, Mark B.;  McBride, Alisha;  Pluvinage, John;  Elahi, Fanny;  Tam, Grace Kyin-Ye;  Kim, Yongha;  Greicius, Michael;  Wagner, Anthony D.;  Aigner, Ludwig;  Galasko, Douglas R.;  Davis, Mark M.;  Wyss-Coray, Tony
收藏  |  浏览/下载:39/0  |  提交时间:2020/07/03

After activation by an agonist, G-protein-coupled receptors (GPCRs) recruit beta-arrestin, which desensitizes heterotrimeric G-protein signalling and promotes receptor endocytosis(1). Additionally, beta-arrestin directly regulates many cell signalling pathways that can induce cellular responses distinct from that of G proteins(2). In contrast to G proteins, for which there are many high-resolution structures in complex with GPCRs, the molecular mechanisms underlying the interaction of beta-arrestin with GPCRs are much less understood. Here we present a cryo-electron microscopy structure of beta-arrestin 1 (beta arr1) in complex with M2 muscarinic receptor (M2R) reconstituted in lipid nanodiscs. The M2R-beta arr1 complex displays a multimodal network of flexible interactions, including binding of the N domain of beta arr1 to phosphorylated receptor residues and insertion of the finger loop of beta arr1 into the M2R seven-transmembrane bundle, which adopts a conformation similar to that in the M2R-heterotrimeric G(o) protein complex(3). Moreover, the cryo-electron microscopy map reveals that the C-edge of beta arr1 engages the lipid bilayer. Through atomistic simulations and biophysical, biochemical and cellular assays, we show that the C-edge is critical for stable complex formation, beta arr1 recruitment, receptor internalization, and desensitization of G-protein activation. Taken together, these data suggest that the cooperative interactions of beta-arrestin with both the receptor and the phospholipid bilayer contribute to its functional versatility.


  
Forest proximity and lowland mosaic increase robustness of tropical pollination networks in mixed fruit orchards 期刊论文
LANDSCAPE AND URBAN PLANNING, 2019, 192
作者:  Sritongchuay, Tuanjit;  Hughes, Alice C.;  Memmott, Jane;  Bumrungsri, Sara
收藏  |  浏览/下载:34/0  |  提交时间:2020/02/17
Forest proximity  Interaction evenness  Landscape composition  Mixed fruit orchard  Pollination network  Robustness  
Native and alien flower visitors differ in partner fidelity and network integration 期刊论文
ECOLOGY LETTERS, 2019, 22 (8) : 1264-1273
作者:  Trojelsgaard, Kristian;  Heleno, Ruben;  Traveset, Anna
收藏  |  浏览/下载:15/0  |  提交时间:2019/11/27
biotic homogenisation  ecological network  exotic  interaction partner  mutualism  oceanic island  plant  pollinator  species roles  
A highly resolved food web for insect seed predators in a species-rich tropical forest 期刊论文
ECOLOGY LETTERS, 2019, 22 (10) : 1638-1649
作者:  Gripenberg, Sofia;  Basset, Yves;  Lewis, Owen T.;  Terry, J. Christopher D.;  Wright, S. Joseph;  Simon, Indira;  Fernandez, D. Catalina;  Cedeno-Sanchez, Marjorie;  Rivera, Marleny;  Barrios, Hector;  Brown, John W.;  Calderon, Osvaldo;  Cognato, Anthony I.;  Kim, Jorma;  Miller, Scott E.;  Morse, Geoffrey E.;  Pinzon-Navarro, Sara;  Quicke, Donald L. J.;  Robbins, Robert K.;  Salminen, Juha-Pekka;  Vesterinen, Eero
收藏  |  浏览/下载:17/0  |  提交时间:2019/11/27
Apparent competition  Barro Colorado Island  host specialisation  interaction network  Janzen-Connell hypothesis  Panama  plant traits  quantitative food web  seed predation  
Diversity indices for ecological networks: a unifying framework using Hill numbers 期刊论文
ECOLOGY LETTERS, 2019, 22 (4) : 737-747
作者:  Ohlmann, Marc;  39;Connor, Louise
收藏  |  浏览/下载:17/0  |  提交时间:2019/04/09
Hill numbers  interaction network diversity  Metanetwork  species aggregation level  
Microscopic Observations of Pulsating Aurora Associated With Chorus Element Structures: Coordinated Arase Satellite-PWING Observations 期刊论文
GEOPHYSICAL RESEARCH LETTERS, 2018, 45 (22) : 12125-12134
作者:  Ozaki, M.;  Shiokawa, K.;  Miyoshi, Y.;  Hosokawa, K.;  Oyama, S.;  Yagitani, S.;  Kasahara, Y.;  Kasaba, Y.;  Matsuda, S.;  Kataoka, R.;  Ebihara, Y.;  Ogawa, Y.;  Otsuka, Y.;  Kurita, S.;  Moore, R. C.;  Tanaka, Y. -M.;  Nose, M.;  Nagatsuma, T.;  Connors, M.;  Nishitani, N.;  Katoh, Y.;  Hikishima, M.;  Kumamoto, A.;  Tsuchiya, F.;  Kadokura, A.;  Nishiyama, T.;  Inoue, T.;  Imamura, K.;  Matsuoka, A.;  Shinohara, I.
收藏  |  浏览/下载:19/0  |  提交时间:2019/04/09
pulsating aurora  discrete chorus element  wave-particle interaction  Arase satellite  ground-based observation network  
Mapping the imprint of biotic interactions on beta-diversity 期刊论文
ECOLOGY LETTERS, 2018, 21 (11) : 1660-1669
作者:  Ohlmann, Marc;  Mazel, Florent;  Chalmandrier, Loic;  Bec, Stephane;  Coissac, Eric;  Gielly, Ludovic;  Pansu, Johan;  Schilling, Vincent;  Taberlet, Pierre;  Zinger, Lucie;  Chave, Jerome;  Thuiller, Wilfried
收藏  |  浏览/下载:21/0  |  提交时间:2019/04/09
beta-diversity  graphical lasso  graphical model  interaction network  meta-communities  partial correlation networks