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排序方式: 共有230条查询结果,搜索用时 31 毫秒
221.
Alexia Gómez Ines Sánchez‐Roman Jose Gomez Julia Cruces Ianire Mate Mónica Lopez‐Torres Alba Naudi Manuel Portero‐Otin Reinald Pamplona Monica De la Fuente Gustavo Barja 《Aging cell》2014,13(3):551-560
The membrane fatty acid unsaturation hypothesis of aging and longevity is experimentally tested for the first time in mammals. Lifelong treatment of mice with the β1‐blocker atenolol increased the amount of the extracellular‐signal‐regulated kinase signaling protein and successfully decreased one of the two traits appropriately correlating with animal longevity, the membrane fatty acid unsaturation degree of cardiac and skeletal muscle mitochondria, changing their lipid profile toward that present in much more longer‐lived mammals. This was mainly due to decreases in 22:6n‐3 and increases in 18:1n‐9 fatty acids. The atenolol treatment also lowered visceral adiposity (by 24%), decreased mitochondrial protein oxidative, glycoxidative, and lipoxidative damage in both organs, and lowered oxidative damage in heart mitochondrial DNA. Atenolol also improved various immune (chemotaxis and natural killer activities) and behavioral functions (equilibrium, motor coordination, and muscular vigor). It also totally or partially prevented the aging‐related detrimental changes observed in mitochondrial membrane unsaturation, protein oxidative modifications, and immune and behavioral functions, without changing longevity. The controls reached 3.93 years of age, a substantially higher maximum longevity than the best previously described for this strain (3.0 years). Side effects of the drug could have masked a likely lowering of the endogenous aging rate induced by the decrease in membrane fatty acid unsaturation. We conclude that it is atenolol that failed to increase longevity, and likely not the decrease in membrane unsaturation induced by the drug. 相似文献
222.
A Mahuzier HM Gaudé V Grampa I Anselme F Silbermann M Leroux-Berger D Delacour J Ezan M Montcouquiol S Saunier S Schneider-Maunoury C Vesque 《The Journal of cell biology》2012,198(5):927-940
Cilia are at the core of planar polarity cellular events in many systems. However, the molecular mechanisms by which they influence the polarization process are unclear. Here, we identify the function of the ciliopathy protein Rpgrip1l in planar polarity. In the mouse cochlea and in the zebrafish floor plate, Rpgrip1l was required for positioning the basal body along the planar polarity axis. Rpgrip1l was also essential for stabilizing dishevelled at the cilium base in the zebrafish floor plate and in mammalian renal cells. In rescue experiments, we showed that in the zebrafish floor plate the function of Rpgrip1l in planar polarity was mediated by dishevelled stabilization. In cultured cells, Rpgrip1l participated in a complex with inversin and nephrocystin-4, two ciliopathy proteins known to target dishevelled to the proteasome, and, in this complex, Rpgrip1l prevented dishevelled degradation. We thus uncover a ciliopathy protein complex that finely tunes dishevelled levels, thereby modulating planar cell polarity processes. 相似文献
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Yann Deleye Alexia Karen Cotte Sarah Anissa Hannou Nathalie Hennuyer Lucie Bernard Bruno Derudas Sandrine Caron Vanessa Legry Emmanuelle Vallez Emilie Dorchies Nathalie Martin Steve Lancel Jean Sbastien Annicotte Kadiombo Bantubungi Albin Pourtier Violeta Raverdy Franois Pattou Philippe Lefebvre Corinne Abbadie Bart Staels Joel T. Haas Rjane Paumelle 《The Journal of biological chemistry》2020,295(50):17310
226.
Despite the common assumption that most Haplosclerida are viviparous sponges, this study of the reproductive cycle of Haliclona fulva demonstrates that this species is actually oviparous and gonochoric. Intriguingly, not a single male was recorded in 15 months of sampling. Oogenesis is synchronous, starting in late April and terminating in September. Asexual reproduction is represented by cyclic budding, which occurs from late November to early March. During the season of asexual reproduction, the reproductive effort represents from 0.21% to 1.49% of the parental tissue, with the highest values being recorded in winter. During the season of sexual reproduction, the female reproductive effort ranges 0.05–1.15%, with the highest effort appearing in early summer. However, no significant correlation between reproductive efforts and seawater temperature fluctuations could be detected. We describe the ultrastructural morphogenesis of the buds for the first time in this species. This process is asynchronous, with buds of variable size being attached to the maternal apical surface via a short stalk. Young buds lack any particular anatomical organization, whereas bud maturity is characterized by the development of mesohyl and by the appearance of an increasing number and volume of lacunae in the central part of each bud. At this stage, buds harbor numerous small choanocyte chambers scattered throughout the inner region, and all cell types known from the mesohyl of parental sponges: microgranular cells, granular cells, archaeocytes, endopinacocytes and exopinacocytes, central cells, and sclerocytes. 相似文献
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Krista K. Alexander;Michalis Kentros;Leah G. Helton;Dimitris Tantis-Tapeinos;Timothy J. LeClair;Fredejah T. Royer;Neil J. Grimsey;Alexia V. Polissidis;Eileen J. Kennedy;Hardy J. Rideout; 《Peptide Science》2024,116(6):e24374
Mutations in the gene encoding leucine-rich repeat kinase 2 (LRRK2) are the most common cause of familial Parkinson's disease (PD). The reduced penetrance of mutations in the LRRK2 gene has also led to variants appearing in seemingly sporadic forms of the disease. Kinase inhibition effectively blocks neuronal death and small-molecule Class I inhibitors are proceeding through clinical trials in multiple PD cohorts. The toxic interaction between mutant LRRK2 and FADD lies downstream of its kinase activity and is required to induce neuronal death. The present study aimed to determine whether the FADD-LRRK2 interface could be disrupted and what effects this may have on neuroprotection. A series of constrained peptides were designed to mimic the alpha-helical protein interaction interface between the LRRK2 armadillo region and the death domain of FADD. These peptide-based protein–protein interaction inhibitors significantly reduced this interaction and blocked apoptotic death of primary neurons expressing G2019S-LRRK2. This work has identified novel constrained peptides that disrupt the LRRK2-FADD interface and downregulate mutant LRRK2-induced neuronal death in an allosteric manner, thereby providing a potential alternative therapeutic approach for PD. 相似文献
229.
Alexia Tasca Martin Helmstädter Magdalena Maria Brislinger Maximilian Haas Brian Mitchell Peter Walentek 《Developmental cell》2021,56(4):525-539.e6
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230.
Ashley Castellanos-Jankiewicz Omar Guzmán-Quevedo Valérie S. Fénelon Philippe Zizzari Carmelo Quarta Luigi Bellocchio Anne Tailleux Julie Charton Daniela Fernandois Marcus Henricsson Catherine Piveteau Vincent Simon Camille Allard Sandrine Quemener Valentine Guinot Nathalie Hennuyer Alessia Perino Alexia Duveau Daniela Cota 《Cell metabolism》2021,33(7):1483-1492.e10
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