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Structure and catalytic mechanism of a human triacylglycerol-synthesis enzyme 期刊论文
NATURE, 2020, 581 (7808) : 323-+
作者:  Nikoo, Mohammad Samizadeh;  Jafari, Armin;  Perera, Nirmana;  Zhu, Minghua;  Santoruvo, Giovanni;  Matioli, Elison
收藏  |  浏览/下载:19/0  |  提交时间:2020/07/03

Triacylglycerols store metabolic energy in organisms and have industrial uses as foods and fuels. Excessive accumulation of triacylglycerols in humans causes obesity and is associated with metabolic diseases(1). Triacylglycerol synthesis is catalysed by acyl-CoA diacylglycerol acyltransferase (DGAT) enzymes(2-4), the structures and catalytic mechanisms of which remain unknown. Here we determined the structure of dimeric human DGAT1, a member of the membrane-bound O-acyltransferase (MBOAT) family, by cryo-electron microscopy at approximately 3.0 angstrom resolution. DGAT1 forms a homodimer through N-terminal segments and a hydrophobic interface, with putative active sites within the membrane region. A structure obtained with oleoyl-CoA substrate resolved at approximately 3.2 angstrom shows that the CoA moiety binds DGAT1 on the cytosolic side and the acyl group lies deep within a hydrophobic channel, positioning the acyl-CoA thioester bond near an invariant catalytic histidine residue. The reaction centre is located inside a large cavity, which opens laterally to the membrane bilayer, providing lipid access to the active site. A lipid-like density-possibly representing an acyl-acceptor molecule-is located within the reaction centre, orthogonal to acyl-CoA. Insights provided by the DGAT1 structures, together with mutagenesis and functional studies, provide the basis for a model of the catalysis of triacylglycerol synthesis by DGAT.


Cryo-electron microscopy structures and functional and mutagenesis studies provide insights into the catalysis of triacylglycerol synthesis by human acyl-CoA diacylglycerol acyltransferase at its intramembrane active site.


  
Late-stage oxidative C(sp(3))-H methylation 期刊论文
NATURE, 2020, 580 (7805) : 621-+
作者:  Fessler, Evelyn;  Eckl, Eva-Maria;  Schmitt, Sabine;  Mancilla, Igor Alves;  Meyer-Bender, Matthias F.;  Hanf, Monika;  Philippou-Massier, Julia;  Krebs, Stefan;  Zischka, Hans;  Jae, Lucas T.
收藏  |  浏览/下载:46/0  |  提交时间:2020/07/03

Frequently referred to as the '  magic methyl effect'  , the installation of methyl groups-especially adjacent (alpha) to heteroatoms-has been shown to dramatically increase the potency of biologically active molecules(1-3). However, existing methylation methods show limited scope and have not been demonstrated in complex settings(1). Here we report a regioselective and chemoselective oxidative C(sp(3))-H methylation method that is compatible with late-stage functionalization of drug scaffolds and natural products. This combines a highly site-selective and chemoselective C-H hydroxylation with a mild, functional-group-tolerant methylation. Using a small-molecule manganese catalyst, Mn(CF3PDP), at low loading (at a substrate/catalyst ratio of 200) affords targeted C-H hydroxylation on heterocyclic cores, while preserving electron-neutral and electron-rich aryls. Fluorine- or Lewis-acid-assisted formation of reactive iminium or oxonium intermediates enables the use of a mildly nucleophilic organoaluminium methylating reagent that preserves other electrophilic functionalities on the substrate. We show this late-stage C(sp(3))-H methylation on 41 substrates housing 16 different medicinally important cores that include electron-rich aryls, heterocycles, carbonyls and amines. Eighteen pharmacologically relevant molecules with competing sites-including drugs (for example, tedizolid) and natural products-are methylated site-selectively at the most electron rich, least sterically hindered position. We demonstrate the syntheses of two magic methyl substrates-an inverse agonist for the nuclear receptor RORc and an antagonist of the sphingosine-1-phosphate receptor-1-via late-stage methylation from the drug or its advanced precursor. We also show a remote methylation of the B-ring carbocycle of an abiraterone analogue. The ability to methylate such complex molecules at late stages will reduce synthetic effort and thereby expedite broader exploration of the magic methyl effect in pursuit of new small-molecule therapeutics and chemical probes.


A manganese-catalysed oxidative C(sp(3))-H methylation method allows a methyl group to be selectively installed into medicinally important heterocycles, providing a way to improve pharmaceuticals and better understand the '  magic methyl effect'  .


  
Alpine grassland plants grow earlier and faster but biomass remains unchanged over 35 years of climate change 期刊论文
ECOLOGY LETTERS, 2020, 23 (4) : 701-710
作者:  Wang, Hao;  Liu, Huiying;  Cao, Guangmin;  Ma, Zhiyuan;  Li, Yikang;  Zhang, Fawei;  Zhao, Xia;  Zhao, Xinquan;  Jiang, Lin;  Sanders, Nathan J.;  Classen, Aimee T.;  He, Jin-Sheng
收藏  |  浏览/下载:5/0  |  提交时间:2020/07/02
alpine grassland  biomass production  climate warming  ecosystem function  functional group composition  phenology  plant growth  the Tibetan Plateau  
Effect of present and past landscape structures on the species richness and composition of ground beetles (Coleoptera: Carabidae) and spiders (Araneae) in a dynamic landscape 期刊论文
LANDSCAPE AND URBAN PLANNING, 2019, 192
作者:  Duan, Meichun;  Liu, Yunhui;  Li, Xiang;  Wu, Panlong;  Hu, Wenhao;  Zhang, Feng;  Shi, Hongliang;  Yu, Zhenrong;  Baudry, Jacques
收藏  |  浏览/下载:11/0  |  提交时间:2020/02/17
Ecological traits  Functional group  Landscape dynamic  Land use change  Land use history  
Effects of native deer on invasive earthworms depend on earthworm functional feeding group and correlate with earthworm body size 期刊论文
FOREST ECOLOGY AND MANAGEMENT, 2019, 435: 180-186
作者:  Cope, Colin G.;  Burns, Jean H.
收藏  |  浏览/下载:6/0  |  提交时间:2019/04/09
Aboveground-belowground interactions  Body size  Functional group  Invasion  White-tailed deer  
Forest conversion from Norway spruce to European beech increases species richness and functional structure of aboveground macrofungal communities 期刊论文
FOREST ECOLOGY AND MANAGEMENT, 2019, 432: 522-533
作者:  Heine, Peggy;  Hausen, Jonas;  Ottermanns, Richard;  Schaeffer, Andreas;  Ross-Nickoll, Martina
收藏  |  浏览/下载:6/0  |  提交时间:2019/04/09
Norway spruce forest conversion  European beech  Macrofungal species richness  Community composition  Functional group  Close-to-nature management  
Short-term effects of alternative thinning treatments on the richness, abundance and composition of epixylic bryophytes, lichens, and vascular plants in conifer plantations at microhabitat and stand scales 期刊论文
FOREST ECOLOGY AND MANAGEMENT, 2018, 415: 106-117
作者:  Haughian, Sean R.
收藏  |  浏览/下载:4/0  |  提交时间:2019/04/09
Functional group  Liverwort  Moss  Woody debris  Biodiversity  Acadian forest  
Investigating the biodiversity of the forest strata: The importance of vertical stratification to the activity and development of saproxylic beetles in managed temperate deciduous forests 期刊论文
FOREST ECOLOGY AND MANAGEMENT, 2017, 402
作者:  Plewa, Radoslaw;  Jaworski, Tomasz;  Hilszczanski, Jacek;  Horak, Jakub
收藏  |  浏览/下载:0/0  |  提交时间:2019/04/09
Forest canopy  Functional group  Functional trait  Guild  Oak stands  Red-list index