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951.
The results of comparing the solutions of the direct task of electroencephalography on a spherical model and a spherical model
with one nonuniformity are discussed. The nonuniformity was simulated by two parabolas situated on the same axis of symmetry
and crossing the boundary of the gray and the white matter. The region between the larger and the smaller parabolas had the
physical characteristics of the gray matter, and the region inside the smaller parabola had the characteristics of the cerebrospinal
fluid. The task was to find a combination of parameters (distance between the dipole and the nonuniformity, angle of rotation
of the dipole relative to the nonuniformity, sizes of the dipole and the nonuniformity, etc.) that provides the maximum effect
of the difference of potentials on the outer surface of the scalp in the spherical model with one nonuniformity and the spherical
model. The influence of the points of grounding on the value of the effect was analyzed (ground only at the right ear and
ground at both ears). The data obtained show that a maximum difference of potentials is reached at the positions of dipoles
close to tangential relative to the scalp surface. 相似文献
952.
Han Dai Lauren Kustigian David Carney April Case Thomas Considine Basil P. Hubbard Robert B. Perni Thomas V. Riera Bruce Szczepankiewicz George P. Vlasuk Ross L. Stein 《The Journal of biological chemistry》2010,285(43):32695-32703
SIRT1 is a protein deacetylase that has emerged as a therapeutic target for the development of activators to treat diseases of aging. SIRT1-activating compounds (STACs) have been developed that produce biological effects consistent with direct SIRT1 activation. At the molecular level, the mechanism by which STACs activate SIRT1 remains elusive. In the studies reported herein, the mechanism of SIRT1 activation is examined using representative compounds chosen from a collection of STACs. These studies reveal that activation of SIRT1 by STACs is strongly dependent on structural features of the peptide substrate. Significantly, and in contrast to studies reporting that peptides must bear a fluorophore for their deacetylation to be accelerated, we find that some STACs can accelerate the SIRT1-catalyzed deacetylation of specific unlabeled peptides composed only of natural amino acids. These results, together with others of this study, are at odds with a recent claim that complex formation between STACs and fluorophore-labeled peptides plays a role in the activation of SIRT1 (Pacholec, M., Chrunyk, B., Cunningham, D., Flynn, D., Griffith, D., Griffor, M., Loulakis, P., Pabst, B., Qiu, X., Stockman, B., Thanabal, V., Varghese, A., Ward, J., Withka, J., and Ahn, K. (2010) J. Biol. Chem. 285, 8340–8351). Rather, the data suggest that STACs interact directly with SIRT1 and activate SIRT1-catalyzed deacetylation through an allosteric mechanism. 相似文献
953.
A. G. Kursanov R. V. Lisin S. Yu. Khamzin A. A. Balakin Yu. L. Protsenko O. E. Solovyova 《Biophysics》2016,61(5):759-764
The results of numerical simulations and physiological experiments that assessed the dependence of the intramyocardial slow force response under an afterload in the heterogeneous myocardium are described. Muscle duplexes of our design were used as the simplest experimental and theoretical models of the heterogeneous myocardium. It is shown that the degree of the slow force response increases with an afterload and the time of the stimulation delay between the elements of the duplex. This effect is explainable by an increase in the time of the mechanical interaction between the duplex elements in the isometric phase of contraction. This leads to changes in individual contractility, the configuration of the action potential, and the kinetic characteristics of intracellular calcium in cardiomyocytes of interacting muscles. 相似文献
954.
Juliette J. Kahle George P. Souroullas Peng Yu Fabian Zohren Yoontae Lee Chad A. Shaw Huda Y. Zoghbi Margaret A. Goodell 《PLoS genetics》2013,9(3)
Hematopoietic stem cells (HSCs) are rare quiescent cells that continuously replenish the cellular components of the peripheral blood. Observing that the ataxia-associated gene Ataxin-1-like (Atxn1L) was highly expressed in HSCs, we examined its role in HSC function through in vitro and in vivo assays. Mice lacking Atxn1L had greater numbers of HSCs that regenerated the blood more quickly than their wild-type counterparts. Molecular analyses indicated Atxn1L null HSCs had gene expression changes that regulate a program consistent with their higher level of proliferation, suggesting that Atxn1L is a novel regulator of HSC quiescence. To determine if additional brain-associated genes were candidates for hematologic regulation, we examined genes encoding proteins from autism- and ataxia-associated protein–protein interaction networks for their representation in hematopoietic cell populations. The interactomes were found to be highly enriched for proteins encoded by genes specifically expressed in HSCs relative to their differentiated progeny. Our data suggest a heretofore unappreciated similarity between regulatory modules in the brain and HSCs, offering a new strategy for novel gene discovery in both systems. 相似文献
955.
ZHENG LianBin LI YongLan XI HuanJiu YU KeLi LU ShunHua SHI Rui WEN YouFeng BAO JingPing ZHANG XingHua LI YuLing REN Fu XU GuoChang 《中国科学:生命科学英文版》2015,58(2):215-217,1,3
<正>Dear Editor,Shortly after initiating the"Physical Anthropological Research on Han Chinese"research project,we applied uniform sampling methods as well as methods and instruments of measurement to obtain a complete set of measurements of physical anthropological indicators among Han populations across China.Among these measurements,body stature was a key indicator.Currently,there should be reliable 相似文献
956.
L. B. Piotrovskiy E. V. Litasova M. A. Dumpis D. N. Nikolaev E. E. Yakovleva O. A. Dravolina A. Yu. Bespalov 《Doklady. Biochemistry and biophysics》2016,468(1):173-175
The present report describes development of hexamethonium complexes based on fullerene C60. Hexamethonium has a limited penetration into CNS and therefore can antagonize central effects of nicotine only when given at high doses. In the present studies conducted in laboratory rodents, intraperitoneal administration of hexamethonium-fullerene complexes blocked effects of nicotine (convulsions and locomotor stimulation). When compared to equimolar doses of hexamethonium, complexes of hexamethonium with derivatives of fullerene C60 were 40 times more potent indicating an enhanced ability to interact with central nicotine receptors. Thus, fullerene C60 derivatives should be explored further as potential carrier systems for polar drug delivery into CNS. 相似文献
957.
958.
959.
Autophagy induction by xanthoangelol exhibits anti‐metastatic activities in hepatocellular carcinoma
Xiuwei Yang Jing Xie Xiaoxiao Liu Zichao Li Kun Fang Luying Zhang Mei Han Zhuang Zhang Zhi Gong Xuezhu Lin Xianzhou Shi Hui Gao Kui Lu 《Cell biochemistry and function》2019,37(3):128-138
Xanthoangelol (XAG), a prenylated chalcone isolated from the Japanese herb Angelica keiskei Koidzumi, has been reported to exhibit antineoplastic properties. However, the specific anti‐tumor activity of XAG in human hepatocellular carcinoma (HCC), and the relevant mechanisms are not known. Herein, we evaluated the effect of XAG against HCC in vitro and in vivo. Although XAG treatment did not significantly reduce the viability of the Hep3B and Huh7 cell lines, it suppressed cell migration, invasion, and EMT. This anti‐metastatic effect of XAG was due to induction of autophagy, because treatment with the autophagy inhibitor 3‐methyadenine (3‐MA) or knockdown of the pro‐autophagy Beclin‐1 effectively abrogated the XAG‐induced suppression of metastasis. Mechanistically, XAG induced autophagy via activation of the AMPK/mTOR signaling pathway, and XAG treatment dramatically increased the expression of p‐AMPK while decreasing p‐mTOR expression. In addition, blocking AMPK/mTOR axis with compound C abrogated the autophagy‐mediated inhibition of metastasis. The murine model of HCC metastasis also showed that XAG effectively reduced the number of metastatic pulmonary nodules. Taken together, our results revealed that autophagy via the activation of AMPK/mTOR pathway is essential for the anti‐metastatic effect of XAG against HCC. These findings not only contribute to our understanding of the anti‐tumor activity of XAG but also provide a basis for its clinical application in HCC. Before this study, evidence of XAG on HCC was purely anecdotal; present study provides the first comprehensive assessments of XAG on HCC metastasis and investigates its underlying mechanism. Results suggest that XAG exerts anti‐metastatic properties against HCC through inducing autophagy which is mediated by the activation of AMPK/mTOR signaling pathway. This research extends our knowledge about the antineoplastic properties of XAG and suggests that induction autophagy may represent future treatment strategies for metastatic HCC. 相似文献
960.
Journal of Ichthyology - Information on stone cockscomb Alectrias alectrolophus diet in Avacha Bay (eastern Kamchatka) are presented, and seasonal, local, age, and interannual changes in the... 相似文献