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991.
Polyacrylamide gel electrophoresis of the RNAs of influenza A viruses was performed under conditions in which each of the eight RNA segments of influenza A/PR/8/34 (H0N1) virus migrates differently from the equivalent segments of influenza A/Hong Kong/8/68 (H3N2) virus. As reported previously [Palese, P. and Schulman, J. L. Proc. Nat. Acad. Sci. USA73, 2142–2146 (1976)], analysis of RNA patterns of recombinant viruses derived from these two parents permitted the identification of the fourth RNA segment (the slowest-moving RNA segment is counted as #1) of each virus as the gene coding for hemagglutinin, and the fifth segment of Hong Kong virus and the sixth segment of PR8 virus as the genes for the respective neuraminidases. Three more genes have been identified by correlating migration patterns of RNAs with protein patterns of recombinant viruses on gradient polyacrylamide gels. The slowest-moving band (RNA 1) is the gene coding for the third largest influenza virus protein (P3). RNA segment 2 codes for the largest protein (Pl), and the P2 protein is coded for by RNA segment 3. 相似文献
992.
Daniel J. Kruger Peter Hutchison Matthew G. Monroe Thomas Reischl Susan Morrel‐Samuels 《Journal of community psychology》2007,35(4):483-498
This study develops an explanatory framework for fear of neighborhood crime based on respondents' social context and local rates of assault injuries. Rates of assault injuries within zip codes are based on hospital discharge records. We find that only four variables have a significant unique contribution to fear of crime: respondent's sex, perceptions of neighborhood social capital, and the rates of struck by/against assault injuries for the 10–24 and 50+ age groups. We also find that the perception of neighborhood social capital moderates the impact of assault injury rates on fear of crime; those who perceive a high level of neighborhood social capital exhibit less sensitivity to assault injury rates. We include a map of assault injury rates and fear of crime by ZIP Code and describe the community context related to our results. © 2007 Wiley Periodicals, Inc. J Comm Psychol 35: 483–498, 2007. 相似文献
993.
Dr. H. H. Funkenstein Peter Winter 《Experimental brain research. Experimentelle Hirnforschung. Expérimentation cérébrale》1973,18(5):464-488
Summary The responses of single units in the superior temporal gyrus of awake squirrel monkeys to tone pips, noise, clicks, and frequency-modulated sounds were recorded with extracellular microelectrodes. A majority of the units responded to acoustic stimulation, pure tone pips being the most effective in terms of the percentage of units responding (71%). No simple catalogue of response types could be elicited. Units varied in terms of the combinations of stimuli to which they were responsive, the frequency range over which pure tones were effective, and the temporal pattern of discharge to different frequencies and different types of stimuli. A substantial majority of units gave precise timed responses to the onset or offset of the stimuli, while a few introduced long delays between the stimulus and the response. With regard to the area studied, acoustic units could be found between stereotaxic coordinates A3 and A10, both on the lateral surface of the hemisphere and in the superior temporal plane, as well as in the caudal insular region. No precise tonotopic organization could be discerned.Peter Winter died in a skiing accident in March, 1972. 相似文献
994.
A newly developed noninvasive tissue reflectance oximeter utilizes 5 light emitting diodes operating at the wavelengths of 0.635, 0.665, 0.795, 0.910, and 0.955 μ, and photodiodes to sample the tissue reflectance spectra. Since the tissue reflectance is affected by changes in both hemoglobin content (Hb T) and hemoglobin oxygen saturation (OS T),Hb T is first determined using the reflectance at 0.795 μ. The hemoglobinOS T is then estimated using the reflectances at the 5 wavelengths in conjunction with the diffuse reflectance equation which has previously been verified applicable to tissue reflectance oximetry. A quantitative estimation of bothHb T andOS T in intestinal mucosa of dogs obtained using this instrument showed thatHb T values agreed fairly well with those of others and that the standard errors ofOS T were around 5.0% inOS as compared with theOS values of blood samples for minimized arterial-venousOS differences. The continuous on-line measurement ofHb T andOS T should be possible using the reflectance technique and should be valuable for clinical evaluation of the patients. 相似文献
995.
hTERT gene amplification and increased mRNA expression in central nervous system embryonal tumors
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Fan X Wang Y Kratz J Brat DJ Robitaille Y Moghrabi A Perlman EJ Dang CV Burger PC Eberhart CG 《The American journal of pathology》2003,162(6):1763-1769
High-level gains at 5p15, a chromosomal region including the human telomerase catalytic protein subunit (hTERT) gene, have been documented in several medulloblastomas. We therefore analyzed hTERT gene dosage in a group of medulloblastomas and other embryonal brain tumors using differential PCR. Amplification of the hTERT locus was detected in 15 of 36 (42%) tumors examined. To correlate gene amplification with message level, we used real-time quantitative PCR to measure hTERT mRNA in 50 embryonal brain tumors. hTERT mRNA was detected in all but one of these cases, and mRNA level correlated significantly with gene dosage (r = 0.82). Log-rank analysis of survival data revealed a trend toward poor clinical outcomes in patients with medulloblastomas containing high hTERT mRNA levels, but clinical follow-up was relatively short and the association was not statistically significant (P = 0.078). Comparative genomic hybridization was used to further analyze the tumor with the greatest hTERT gene dosage and mRNA level, a recurrent medulloepithelioma. hTERT was amplified in the recurrent tumor but not in the primary lesion, suggesting this locus can be involved in tumor progression. Our data indicate that hTERT gene amplification is relatively common in embryonal brain tumors, and that increased expression of hTERT mRNA may be associated with biologically aggressive tumor behavior. 相似文献
996.
Association analysis of 5-HTTLPR variants, 5-HT2a receptor gene 102T/C polymorphism and migraine 总被引:3,自引:0,他引:3
Juhasz G Zsombok T Laszik A Gonda X Sotonyi P Faludi G Bagdy G 《Journal of neurogenetics》2003,17(2-3):231-240
It is well known that migraine has a strong genetic component, although the type and number of genes involved is not yet clear. There is evidence to suggest that serotonin-related genes participate in the pathogenesis of migraine. Previous studies have shown that gender differences influence the serotonergic neurotransmission and, in addition, the migraine prevalence is higher in females than males. Therefore, we investigated the functional polymorphism in the upstream regulatory region of the serotonin transporter gene (5-HTTLPR) and the 102T/C polymorphism of the 5-HT2A receptor gene in the Hungarian female population. These genes were analysed in 126 migraine sufferers (with or without aura)and 101 unrelated healthy controls using case control design. A borderline association (chi2 = 3.84, df = 1, p = 0.049; OR = 1.45, 95% CI = 1.00-2.12) between 5-HTTLPR short (S) allele and migraine was found. No significant difference between migraine sufferers and controls was observed for the 102T/C polymorphism of 5-HT2A receptor gene. Furthermore, there was no significant interaction between5-HTTLPR and 102T/C polymorphisms in our study population. In conclusion, our results support that the genetic susceptibility of migraine may be associated with a locus at or near the 5-HT transporter gene. 相似文献
997.
The issue of antibiotic resistance in Helicobacter pylori is of particular concern and has become an important factor leading to eradication failure. This paper reports the prevalence of primary resistance to clarithromycin, amoxicillin, metronidazole and tetracycline among H. pylori isolates in the north-eastern part of Germany. A total of 1644 clinical H. pylori isolates was investigated over a period of 6 years from 1995 to 2000. The MICs were determined by the Etest. The overall rate of primary resistance was 26.2% for metronidazole and 2.2% for clarithromycin. No significant changes in the resistance rates during the period of investigation were observed. No isolate was resistant to amoxicillin or tetracycline. PCR-RFLP analysis for the detection of point mutations associated with clarithromycin resistance was performed with 36 H. pylori isolates. The A --> G transition mutation at position 2143 was detected in 19 H. pylori isolates (52.8%), whereas the mutation at position 2142 was found in 13 isolates (36.1%). 相似文献
998.
Janine Jason Lennox K. Archibald Okey C. Nwanyanwu Anne L. Sowell Ian Buchanan Joshua Larned Michael Bell Peter N. Kazembe Hamish Dobbie William R. Jarvis 《Clinical and Vaccine Immunology : CVI》2002,9(3):616-621
In animal studies, vitamin A deficiency induces a shift from type 2 (humoral) to type 1 (cellular) cytokines; there are no similar data for humans. Control of human immunodeficiency virus (HIV) and Mycobacterium tuberculosis infections requires type 1 cytokine (cellular) immunity. These infections and vitamin A deficiency are highly prevalent in Africa. We therefore examined the interactions among serum vitamin A levels, immune parameters, HIV infection status, Mycobacterium bovis BCG vaccine scarring (as an indicator of a type 1 cytokine profile), and clinical findings for 70 hospitalized children in Malawi, Africa. Directly conjugated monoclonal antibodies and flow cytometry were used to assess cell-specific cytokine production by peripheral blood monocytes and lymphocyte subpopulations. The statistical techniques employed included nonparametric statistics and logistic regression analyses. Thirty percent of the participants had severe vitamin A deficiency (<10 μg/dl), 34% had moderate deficiency (10 to <20 μg/dl), and 36% had normal levels (≥20 μg/dl). Vitamin A levels were lower for HIV-positive than for HIV-negative children (median, 10 and 17 μg/dl, respectively). Vitamin A-deficient children (<20 μg/dl) were more likely than non-vitamin A-deficient children to have higher proportions of natural killer (NK) cells (median, 8.3 and 5.2%, respectively) and lower ratios of interleukin-10-producing monocytes to tumor necrosis factor alpha-producing monocytes after induction (median, 1.0 and 2.3, respectively). Vitamin A-deficient children were also more likely than non-vitamin A-deficient children to exhibit respiratory symptoms (47% versus 12%) and visible BCG vaccine scars (83% versus 48%), which are indicative of a type 1 response to vaccination. Vitamin A status did not vary with gender, age, incidence of malaria parasitemia, blood culture positivity, or rates of mortality (6% of vitamin A-deficient children died versus 20% of non-vitamin A-deficient children). Lower vitamin A levels were associated with a relative type 1 cytokine dominance and proportionately more NK cells, both of which may be somewhat beneficial to persons who are exposed to HIV, M. tuberculosis, or other type 1 pathogens. 相似文献
999.
Rapid pulsed-field gel electrophoresis protocol for subtyping of Campylobacter jejuni 总被引:7,自引:0,他引:7
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Ribot EM Fitzgerald C Kubota K Swaminathan B Barrett TJ 《Journal of clinical microbiology》2001,39(5):1889-1894
We developed a rapid pulsed-field gel electrophoresis (PFGE) protocol for subtyping Campylobacter isolates based on the standardized protocols used by PulseNet laboratories for the subtyping of other food-borne bacterial pathogens. Various combinations of buffers, reagents, reaction conditions (e.g., cell suspension concentration, lysis time, lysis temperature, and restriction enzyme concentration), and electrophoretic parameters were evaluated in an effort to devise a protocol that is simple, rapid, and robust. PFGE analysis of Campylobacter isolates can be completed in 24 to 30 h using this protocol, whereas the most widely used current protocols require 3 to 4 days to complete. Comparison of PFGE patterns obtained in six laboratories showed that subtyping results obtained using this protocol are highly reproducible. 相似文献
1000.
目的 在白人群体中 ,导致人类补体第 8成份 β亚基缺陷的分子基础主要是在编码 β亚基基因的第 9外显子上发生碱基 C→ T的突变 ,从而形成终止密码 ,导致 C8β亚基不能完全合成。国外学者在两例 C8β亚基完全缺失的患者家系研究中 ,发现这两例β亚基缺失个体只是第 9外显子上碱基 C→ T突变的杂合子 ,现进一步寻找这两例 C8β亚基完全缺失的分子遗传学机理。方法 对两例 C8β亚基完全缺失患者的 C8β编码基因的全部 11个外显子的 PCR扩增产物进行 DNA测序分析并与正常人 DNA序列进行对比。结果 两例完全性 C8β亚基缺失患者的蛋白质编码基因中 ,分别在第 3外显子的 2 98和 388位置发现了 C→T突变 ,同时对这两个突变位点的家系分析也证实 ,位于第 3外显子上的这两个突变位点是独立于第 9外显子的突变而遗传。结论 所发现的两个突变位点均能形成终止密码而导致 C8β亚基合成提前终止 ,因此这两例患者 C8β亚基完全缺失的分子遗传学机理是由于编码 C8β亚基的基因在第 3和第 9外显子上同时发生了点突变 ,进而形成终止密码造成 C8β亚基合成终止所致。 相似文献