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981.
Dane J. Genther MD Joshua Betz MS Sheila Pratt PhD Kathryn R. Martin PhD MPH Tamara B. Harris MD MS Suzanne Satterfield MD DrPH Douglas C. Bauer MD Anne B. Newman MD MPH Eleanor M. Simonsick PhD Frank R. Lin MD PhD the Health Aging Body Composition Study 《Journal of the American Geriatrics Society》2015,63(6):1146-1152
982.
Spear GT Kersh E Guenthner P Vishwanathan SA Gilbert D Zariffard MR Mirmonsef P Landay A Zheng L Gillevet P 《AIDS research and human retroviruses》2012,28(10):1244-1249
Abstract Vaginal bacterial communities play an important role in human health and have been shown to influence HIV infection. Pigtailed macaques (Macaca nemestrina) are used as an animal model of HIV vaginal infection of women. Since the bacterial microbiota could influence retrovirus infection of pigtailed macaques, the genital microbiota in 10 cycling macaques was determined by pyrosequencing. The microbiota of all macaques was polymicrobial with a median of 13 distinct genera. Strikingly, the genera Sneathia and Fusobacterium, both in the phylum Fusobacteria, accounted for 18.9% and 13.3% of sequences while the next most frequent were Prevotella (5.6%), Porphyromonas (4.1%), Atopobium (3.6%), and Parvimonas (2.6%). Sequences corresponding to Lactobacillus comprised only 2.2% of sequences on average and were essentially all L. amylovorus. Longitudinal sampling of the 10 macaques over an 8-week period, which spanned at least one full ovulatory cycle, showed a generally stable presence of the major types of bacteria with some exceptions. These studies show that the microbiota of the pigtailed macaques is substantially dissimilar to that found in most healthy humans, where the genital microbiota is usually dominated by Lactobacillus sp. The polymicrobial makeup of the macaque bacterial populations, the paucity of lactobacilli, and the specific types of bacteria present suggest that the pigtailed macaque microbiota could influence vaginal retrovirus infection. 相似文献
983.
Demichelis F Setlur SR Banerjee S Chakravarty D Chen JY Chen CX Huang J Beltran H Oldridge DA Kitabayashi N Stenzel B Schaefer G Horninger W Bektic J Chinnaiyan AM Goldenberg S Siddiqui J Regan MM Kearney M Soong TD Rickman DS Elemento O Wei JT Scherr DS Sanda MA Bartsch G Lee C Klocker H Rubin MA 《Proceedings of the National Academy of Sciences of the United States of America》2012,109(17):6686-6691
984.
985.
Douglas P. Munoz Brian D. Corneil 《Experimental brain research. Experimentelle Hirnforschung. Expérimentation cérébrale》1995,103(1):168-173
We examined the processes controlling selective orientation, specifically the processes required for generating saccadic eye movements in humans. Before a saccadic eye movement can be initiated, active visual fixation must be disengaged from the current point of fixation and a new target selected. We investigated whether these neural processes occur independently or interactively by devising a simple, multimodal choice reaction task in which subjects were asked to direct their gaze away from a central visual fixation target to an eccentric visual target while ignoring a simultaneous auditory distractor. Subjects had more difficulty suppressing incorrect movements toward the distractor when the fixation target was extinguished prior to onset of the eccentric target than when the fixation target remained illuminated during eccentric target presentation. Subjects with the shortest saccadic reaction times produced the most incorrect movements. These results support a recent hypothesis suggesting that the processes of disengaging active visual fixation and selecting a new saccade target are interrelated and arise, at least in part, from a change of activity within the superior colliculus. 相似文献
986.
Burr J. Loew MD FASGE Douglas A. Howell MD Michael K. Sanders MD David J. Desilets MD Paul P. Kortan MD FASGE Gary R. May MD FASGE Raj J. Shah MD Yang K. Chen MD FASGE Willis G. Parsons MD Robert H. Hawes MD Peter B. Cotton MD FASGE Adam A. Slivka MD FASGE Jawad Ahmad MD Glen A. Lehman MD FASGE Stuart Sherman MD FASGE Horst Neuhaus MD Brigitte M. Schumacher MD 《Gastrointestinal endoscopy》2009,70(3):445-453
987.
Ujiie M Dickstein DL Carlow DA Jefferies WA 《Microcirculation (New York, N.Y. : 1994)》2003,10(6):463-470
OBJECTIVE: To establish the generality of cerebrovascular pathology frequently observed with Alzheimer disease, we have assessed blood-brain barrier (BBB) integrity using the Alzheimer disease model Tg2576 mice in which cognitive deficits and neuritic plaque formation develop around 10-12 months of age. METHODS: We assessed BBB integrity using well-established methods involving albumin and Evans blue uptake and introduce the use of a novel perfusion protocol using succinimidyl ester of carboxyfluorescein diacetate. RESULTS: BBB permeability is increased in the cerebral cortex of 10-month-old Tg2576 mice preceding Alzheimer disease pathology presentation. Furthermore, when compared with their nontransgenic littermates, 4-month-old Tg2576 mice exhibit compromised BBB integrity in some areas of the cerebral cortex. An age-related increase in albumin uptake by the brains of Tg2576 mice, compared with nontransgenic mice, was also observed. These findings were supported by quantitative Evans blue analysis (p = 0.07, two-way analysis of variance). CONCLUSION: A breakdown of BBB was evident in young 4- to 10-month-old Tg2576 mice. Compromised barrier function could explain the mechanisms of Abeta entry into the brain observed in experimental Alzheimer disease vaccination models. Such structural changes to the BBB caused by elevated Abeta could play a central role in Alzheimer disease development and might define an early point of intervention for designing effective therapy against the disease. 相似文献
988.
The corpus luteum and interstitial tissue in a marsupial,the brushtail possum (Trichosurus vulpecula) 总被引:2,自引:0,他引:2
Eckery DC Juengel JL Whale LJ Thomson BP Lun S McNatty KP 《Molecular and cellular endocrinology》2002,186(1):81-87
Proline-rich tyrosine kinase 2 (Pyk2) expression in prostate epithelium inversely correlated with degree of malignancy of prostate cancers, thus the role of Pyk2 in the regulation of prostate cells proliferation and differentiation was investigate in PC3 cells. Pyk2 can be activated by canonic stimuli such as tumor necrosis factoralpha and lysophosphatidic acid (LPA) in PC3 cells, in addition, LPA stimulated Pyk2 phosphorylation also induced extracellular signal-regulated kinase 1 and 2 activation in these cells. Proliferation of PC3 cell clones (PC3-PKM) expressing a dominant negative kinase-defective Pyk2 mutant is consistently decreased in respect to that of wild type PC3 cells. In addition, PC3-PKM clones underwent total block cell proliferation upon treatment with dibutyryl cAMP. Finally, in the presence of sustained levels of intracellular cAMP, PC3-PKM cells, but not wild type PC3 cells, acquired a neuron-like morphology. Taken together our results suggest that Pyk2 plays a role in the regulation of prostate cell proliferation and, more interestingly, its expression may represents a sensitive marker of prostate state of differentiation. 相似文献
989.
Objective
(1) To determine the effect of active and placebo interferential current on muscle pain sensitivity using an experimental mechanically induced pain model. (2) To evaluate the predictive role of expectations, gender, baseline muscle pain sensitivity, and intervention order on placebo response.Design
Randomized placebo controlled cross-over trial.Setting
University research laboratory.Participants
Forty healthy volunteers (20 females, 20 males).Interventions
Active interferential current, placebo (sham) interferential current, and no treatment/control were applied to the lumbar area on different days.Main outcomes measures
Pressure pain thresholds and placebo response.Results
The two-way ANOVA with repeated measures analysis determined a significant interaction between condition and time (P = 0.002). Pairwise comparisons found differences between active interferential and the control condition at 15 minutes into treatment (mean difference = 0.890 kg/cm2, 95% CI 0.023 to 1.757, P = 0.043) and at 30 minutes into treatment (mean difference = 0.910 kg/cm2, 95% CI 0.078 to 1.742, P = 0.028). The increase in pressure pain thresholds between the active interferential and the control condition (1.12 kg/cm2) was clinically meaningful. Logistic regression analysis showed that the condition sequence order was the only variable that predicted placebo response (odds ratio 9.7; P = 0.028). If a subject started the sequence receiving placebo treatment first, the odds of responding to placebo would be approximately 10 times higher (i.e. 90% probability of being a placebo responder) than that of starting with an active treatment.Conclusions
Active interferential was more efficient than control condition in decreasing muscle pain sensitivity. Placebo interferential was not significantly different from control. Treatment sequence demonstrated a strong association with placebo response. These findings have implications for future research characterizing and identifying placebo responders in physiotherapy. 相似文献990.