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荔湾区HIV感染者/AIDS患者生存质量与相关耻辱调查 总被引:1,自引:0,他引:1
目的了解广州市荔湾区HIV感染者与艾滋病患者的生活质量和耻辱现状,分析其相关的影响因素。方法通过一对一问卷调查方法,采用一般情况问卷、MOS-HIV量表和Berger-HIV耻辱量表对72例HIV感染者/AIDS患者进行调查,其中收回有效问卷56份,对其生活质量和相关耻辱进行典型相关分析。结果典型相关分析结果显示,耻辱量表中影响较大的因素是个人耻辱(X1),载荷量是-0.761;生存质量量表中影响较大的是情绪(Y9),载荷量是0.952。个人耻辱与情绪呈负相关(相关系数为0.727,P〈0.05)。结论HIV/AIDS患者的个人耻辱感越强,其情绪就越差。 相似文献
957.
Tsutomu Takahashi Stephen J. Wood Bridget Soulsby Ryoichiro Tanino Michael T.H. Wong Patrick D. McGorry Michio Suzuki Dennis Velakoulis Christos Pantelis 《Progress in neuro-psychopharmacology & biological psychiatry》2009
Volume reductions of the insular cortex have been described in schizophrenia, but it remains unclear whether other psychotic disorders such as affective psychosis also exhibit insular cortex abnormalities. In this study, we used magnetic resonance imaging to investigate the gray matter volume of the anterior (short) and posterior (long) insular cortices in 162 first-episode patients with various psychotic disorders (46 schizophrenia, 57 schizophreniform disorder, 34 affective psychosis, and 25 other psychoses) and 62 age- and gender-matched healthy comparison subjects. Patients with schizophrenia showed bilateral volume reduction of the anterior and posterior insular cortices compared with controls, but the remaining first-episode psychosis subgroups had normal insular volumes. The volumes of these insular subregions were significantly smaller in schizophrenia patients than in patients with schizophreniform disorder or affective psychoses. There was no association between the insular cortex volume and daily dosage or type of antipsychotic medication in any patient group. These findings suggest that the widespread volume reduction of the insular cortex is specific to established schizophrenia, implicating its role in the neurobiology of clinical characteristics associated with schizophrenia. 相似文献
958.
Gabriel Miltenberger-Miltenyi Thomas Schwarzbraun Wolfgang N L?scher Julia Wanschitz Christian Windpassinger Hans-Christoph Duba Rainer Seidl Gerhard Albrecht Helga Weirich-Schwaiger Heinz Zoller Gerd Utermann Michaela Auer-Grumbach Andreas R Janecke 《European journal of human genetics : EJHG》2009,17(9):1154-1159
Duplication within the chromosome 17p11.2 (CMT1Adup), peripheral myelin protein 22 (PMP22), myelin protein zero (MPZ) and gap junction β1-protein (GJB1) gene mutations are frequent causes of the Charcot-Marie-Tooth disease (CMT). A large number of mutations in these genes are listed in databases. Sequence variants identified in patients are frequently reported as mutations without further evaluation. We analyzed 250 consecutively recruited unrelated Austrian CMT patients for CMT1Adup by microsatellite marker typing, real-time PCR or MLPA, and found 79 duplications (31.6%). The coding regions of the PMP22, MPZ and GJB1 genes were analyzed by direct sequencing in the remaining patients; 28 patients showed mutations, 14 of which were novel. We scored the pathogenicity of novel missense mutations by segregation studies and by their exclusion in control samples. Our comprehensive literature study found that up to 60% of the reported mutations in these genes had not been evaluated regarding their pathogenicity, and the PANTHER bioinformatics tool was used to score novel and published missense variants. The PANTHER program scored known polymorphisms as such, but scored ∼82–88% only of the published and novel mutations as most likely deleterious. Mutations associated with axonal CMT were less likely to be classified as deleterious, and the PMP22 S72L mutation repeatedly associated with severe CMT was classified as a polymorphism using default parameters. Our data suggest that this in silico analysis tool could be useful for assessing the functional impact of DNA variations only as a complementary approach. The CMT1Adup, GJB1, MPZ and PMP22 mutation frequencies were in the range of those described in other CMT patient collectives with different ethnical backgrounds. 相似文献
959.
Byung Yoon Choi Andrew K. Stewart Anne C. Madeo Shannon P. Pryor Suzanne Lenhard Rick Kittles David Eisenman H. Jeffrey Kim John Niparko James Thomsen Kathleen S. Arnos Walter E. Nance Kelly A. King Christopher K. Zalewski Carmen C. Brewer Thomas Shawker James C. Reynolds John A. Butman Lawrence P. Karniski Seth L. Alper Andrew J. Griffith 《Human mutation》2009,30(4):599-608
Hearing loss with enlargement of the vestibular aqueduct (EVA) can be associated with mutations of the SLC26A4 gene encoding pendrin, a transmembrane Cl?/I?/HCO exchanger. Pendrin's critical transport substrates are thought to be I? in the thyroid gland and HCO in the inner ear. We previously reported that bi‐allelic SLC26A4 mutations are associated with Pendred syndromic EVA whereas one or zero mutant alleles are associated with nonsyndromic EVA. One study proposed a correlation of nonsyndromic EVA with SLC26A4 alleles encoding pendrin with residual transport activity. Here we describe the phenotypes and SLC26A4 genotypes of 47 EVA patients ascertained since our first report of 39 patients. We sought to determine the pathogenic potential of each variant in our full cohort of 86 patients. We evaluated the trafficking of 11 missense pendrin products expressed in COS‐7 cells. Products that targeted to the plasma membrane were expressed in Xenopus oocytes for measurement of anion exchange activity. p.F335L, p.C565Y, p.L597S, p.M775T, and p.R776C had Cl?/I? and Cl?/HCO exchange rate constants that ranged from 13 to 93% of wild type values. p.F335L, p.L597S, p.M775T and p.R776C are typically found as mono‐allelic variants in nonsyndromic EVA. The high normal control carrier rate for p.L597S indicates it is a coincidentally detected nonpathogenic variant in this context. We observed moderate differential effects of hypo‐functional variants upon exchange of HCO versus I? but their magnitude does not support a causal association with nonsyndromic EVA. However, these alleles could be pathogenic in trans configuration with a mutant allele in Pendred syndrome. Hum Mutat 0, 1–10, 2009. © 2009 Wiley‐Liss, Inc. 相似文献
960.
Martina Cesani Alessia Capotondo Tiziana Plati Lucia Sergi Sergi Francesca Fumagalli Maria Grazia Roncarolo Luigi Naldini Giancarlo Comi Maria Sessa Alessandra Biffi 《Human mutation》2009,30(10):E936-E945
Metachromatic Leukodystrophy (MLD) is a rare inherited lysosomal storage disorder caused by the deficiency of Arylsulfatase A (ARSA). The disease manifests itself with a broad spectrum of clinical variants, all characterized by progressive neurodegeneration in the central and peripheral nervous systems. The correlation between mutations in the ARSA gene, residual enzymatic activity associated with the mutated alleles and patients' phenotype, which has been extensively drawn for common ARSA mutations, has recently been expanded to rare ones. In this context, functional studies on the rare allelic variances acquire particular relevance for patients' prognostic evaluation. Here we have characterized eight newly identified ARSA mutations, through lentiviral vector‐based expression studies on cell lines and ARSA defective murine fibroblasts. In each case, the residual activity associated with the new mutant allele correlates well with the patient's phenotype. Therefore, our results confirm the importance of functional characterization of mutant alleles for a precise genotype‐based classification and definition of prognosis in MLD patients, which is particularly relevant for pre‐symptomatic diagnosis. © 2009 Wiley‐Liss, Inc. 相似文献