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621.
Pretreatment effects of different gibberellins, helminthosporicacid, cyclic AMP and Kinetin on subsequent IAA-induced elongationwere tested in cucumber hypocotyl sections. Gibberellin A7 wasmore active than GA3, while gibberellin A3 was almost inactive.Both helminthosporic acid and cyclic AMP mimicked GA3-action,though the degree of their activity was less. Kinetin pretreatmentresulted in marked inhibition of IAA-induced elongation. Thepretreatment effect of GA3 was also reflected in a greater responceof the sections to synthetic auxins. (Received October 6, 1973; ) 相似文献
622.
We predict the virtual trajectories and stiffness ellipses during multijoint arm movements by computer simulations. A two-link manipulator with four single-joint muscles and two double-joint muscles is used as a model of the human arm. Physical parameters of the model are derived from several experimental data. Among them, special emphasis is put on low values of the dynamic hand stiffness recently measured during single joint and multijoint movements. The feedback-error-learning scheme to acquire the inverse dynamics model and the inverse statics model is utilized for this prediction. The virtual trajectories are much more complex than the actual trajectories. This indicates that planning the virtual trajectory is as difficult as solving the inverse dynamics problem for medium and fast movements, and simply falsifies the advocated computational advantage of the virtual trajectory control hypothesis. Thus, we conclude that learning inverse models is essential even in the virtual trajectory control framework. Finally, we propose a new computational model to learn the complicated shape of the virtual trajectories by integrating the virtual trajectory control and the feedback-error-learning scheme. 相似文献
623.
624.
Ayumu Yamashita Yuki Sakai Takashi Yamada Noriaki Yahata Akira Kunimatsu Naohiro Okada Takashi Itahashi Ryuichiro Hashimoto Hiroto Mizuta Naho Ichikawa Masahiro Takamura Go Okada Hirotaka Yamagata Kenichiro Harada Koji Matsuo Saori C. Tanaka Mitsuo Kawato Kiyoto Kasai Nobumasa Kato Hidehiko Takahashi Yasumasa Okamoto Okito Yamashita Hiroshi Imamizu 《PLoS biology》2020,18(12)
Many studies have highlighted the difficulty inherent to the clinical application of fundamental neuroscience knowledge based on machine learning techniques. It is difficult to generalize machine learning brain markers to the data acquired from independent imaging sites, mainly due to large site differences in functional magnetic resonance imaging. We address the difficulty of finding a generalizable marker of major depressive disorder (MDD) that would distinguish patients from healthy controls based on resting-state functional connectivity patterns. For the discovery dataset with 713 participants from 4 imaging sites, we removed site differences using our recently developed harmonization method and developed a machine learning MDD classifier. The classifier achieved an approximately 70% generalization accuracy for an independent validation dataset with 521 participants from 5 different imaging sites. The successful generalization to a perfectly independent dataset acquired from multiple imaging sites is novel and ensures scientific reproducibility and clinical applicability.Biomarkers for psychiatric disorders based on neuroimaging data have yet to be put to practical use. This study overcomes the problems of inter-site differences in fMRI data by using a novel harmonization method, thereby successfully constructing a generalizable brain network marker of major depressive disorder across multiple imaging sites. 相似文献
625.
X.-L. Zhang Y. Komada Yan-Wen Zhou Tong-Xin Chen Haruko Sakai Eiichi Azuma Masaru Ido Minoru Sakurai 《Cancer immunology, immunotherapy : CII》1997,44(1):41-47
Peripheral blood lymphocytes obtained from children with acute lymphoblastic leukemia (ALL) at onset were studied for the
expression of interleukin-2 (IL-2) receptor α-chain (CD25) by two-color flow-cytometric analysis. Stimulated with anti-CD3
monoclonal antibody (mAb) alone, CD25 expression was significantly suppressed in CD4+ T cells from 27 of 48 (56.3%) cases and in CD8+ T cells from 29 of 48 (60.4%) cases. When stimulated with anti-CD3 mAb plus phorbol 12-myristate 13-acetate (PMA), CD25 expression
was clearly restored in certain cases of ALL. When PMA plus ionomycin were used for stimulation of T cells, CD25 was inducible
in a majority of cases. Interestingly CD25 expression upon anti-CD3 mAb stimulation was recovered after complete remission
had been achieved. These observations suggest the presence in ALL children at onset of an in vitro defect in the signal transduction
pathway of the T-cell-receptor/CD3 complex, resulting in inefficient CD25 expression. However, immune-staining analysis indicated
that protein kinase C was normally translocated from the cytosol fraction to the cell membrane fraction. The mobilization
of cytoplasmic free calcium is also normal.
Received: 27 March 1996 / Accepted: 23 December 1996 相似文献