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81.
82.
Effects of computerized guidelines for managing heart disease in primary care 总被引:1,自引:0,他引:1 下载免费PDF全文
Tierney WM Overhage JM Murray MD Harris LE Zhou XH Eckert GJ Smith FE Nienaber N McDonald CJ Wolinsky FD 《Journal of general internal medicine》2003,18(12):967-976
BACKGROUND: Electronic information systems have been proposed as one means to reduce medical errors of commission (doing the wrong thing) and omission (not providing indicated care). OBJECTIVE: To assess the effects of computer-based cardiac care suggestions. DESIGN: A randomized, controlled trial targeting primary care physicians and pharmacists. SUBJECTS: A total of 706 outpatients with heart failure and/or ischemic heart disease. INTERVENTIONS: Evidence-based cardiac care suggestions, approved by a panel of local cardiologists and general internists, were displayed to physicians and pharmacists as they cared for enrolled patients. MEASUREMENTS: Adherence with the care suggestions, generic and condition-specific quality of life, acute exacerbations of their cardiac disease, medication compliance, health care costs, satisfaction with care, and physicians' attitudes toward guidelines. RESULTS: Subjects were followed for 1 year during which they made 3,419 primary care visits and were eligible for 2,609 separate cardiac care suggestions. The intervention had no effect on physicians' adherence to the care suggestions (23% for intervention patients vs 22% for controls). There were no intervention-control differences in quality of life, medication compliance, health care utilization, costs, or satisfaction with care. Physicians viewed guidelines as providing helpful information but constraining their practice and not helpful in making decisions for individual patients. CONCLUSIONS: Care suggestions generated by a sophisticated electronic medical record system failed to improve adherence to accepted practice guidelines or outcomes for patients with heart disease. Future studies must weigh the benefits and costs of different (and perhaps more Draconian) methods of affecting clinician behavior. 相似文献
83.
U Meckler W F Caspary T Clement P Herzog B Lembcke B Limberg A el Mouaaouy G Nippel P Reuss W B Schwerk 《Zeitschrift für Gastroenterologie》1991,29(7):355-359
Sonography is adding a new dimension to diagnosis of Crohn's disease: the analysis of the transmural and peri-intestinal manifestations of the chronic inflammation. Distortions in the structure of intestinal wall are recognizable, the impact on transport of intestinal content can be judged, penetration of inflammation into the bowel surrounding as fistula, abscess, mesenteriitis und peritonitis is safely seen. Differential diagnosis on a strictly sonographic basis is difficult. The paper represents the results of an expert meeting held at the University of Frankfurt/M. 相似文献
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Sarah N. Lauder Emma Jones Kathryn Smart Anja Bloom Anwen S. Williams James P. Hindley Beatrice Ondondo Philip R. Taylor Mathew Clement Ceri Fielding Andrew J. Godkin Simon A. Jones Awen M. Gallimore 《European journal of immunology》2013,43(10):2613-2625
Balancing the generation of immune responses capable of controlling virus replication with those causing immunopathology is critical for the survival of the host and resolution of influenza‐induced inflammation. Based on the capacity of interleukin‐6 (IL‐6) to govern both optimal T‐cell responses and inflammatory resolution, we hypothesised that IL‐6 plays an important role in maintaining this balance. Comparison of innate and adaptive immune responses in influenza‐infected wild‐type control and IL‐6‐deficient mice revealed striking differences in virus clearance, lung immunopathology and generation of heterosubtypic immunity. Mice lacking IL?6 displayed a profound defect in their ability to mount an anti‐viral T‐cell response. Failure to adequately control virus was further associated with an enhanced infiltration of inflammatory monocytes into the lung and an elevated production of the pro‐inflammatory cytokines, IFN‐α and TNF‐α. These events were associated with severe lung damage, characterised by profound vascular leakage and death. Our data highlight an essential role for IL‐6 in orchestrating anti‐viral immunity through an ability to limit inflammation, promote protective adaptive immune responses and prevent fatal immunopathology. 相似文献
86.
Boris Klempa Tatjana Avsic-Zupanc Jan Clement Tamara K. Dzagurova Heikki Henttonen Paul Heyman Ferenc Jakab Detlev H. Kruger Piet Maes Anna Papa Evgeniy A. Tkachenko Rainer G. Ulrich Olli Vapalahti Antti Vaheri 《Archives of virology》2013,158(3):521-529
Dobrava-Belgrade virus (DOBV) is a human pathogen that has evolved in, and is hosted by, mice of several species of the genus Apodemus. We propose a subdivision of the species Dobrava-Belgrade virus into four related genotypes – Dobrava, Kurkino, Saaremaa, and Sochi – that show characteristic differences in their phylogeny, specific host reservoirs, geographical distribution, and pathogenicity for humans. 相似文献
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88.
Joao B. Augusto Nicolas Johner Dipen Shah Sabrina Nordin Kristopher Knott Stefania Rosmini Clement Lau Mashael Alfarih Rebecca Hughes Andreas Seraphim Ravi Vijapurapu Anish Bhuva Linda Lin Natalia Ojrzyńska Tarekegn Geberhiwot Gabriella Captur Uma Ramaswami Richard P. Steeds Mehdi Namdar 《Molecular genetics and metabolism》2021,132(2):S17-S18
89.
Heng Seh Gabriel Tan Kian Chong Lim Jeen Nee Lui Wei Ming Clement Lai Victoria Soo Hoon Yu 《Journal of endodontics》2021,47(2):169-177
IntroductionThe incidence of immediate postobturation pain associated with 2 sealer techniques was compared and potential prognostic factors identified.MethodsPatients referred for endodontic treatment were recruited with informed consent. Root canals were debrided and teeth rendered asymptomatic before random allocation to receive TotalFill BC (FKG Dentaire SA, La Chaux-de-Fonds, Switzerland) or AH Plus sealer (Dentsply Maillefer, Ballaigues, Switzerland). Patients blinded to the sealer reported their postobturation pain experience 1, 3, and 7 days after treatment. Blinded and calibrated assessors independently reviewed treatment quality, sealer extrusion, and radiographic data under standardized conditions.ResultsOne hundred sixty eligible patients (163 teeth, 95.3%) returned their pain diary. No postobturation pain difference was found between the 2 sealers (P > .05), although the AH Plus sealer technique was significantly associated with extrusion beyond the apex (P < .05; odds ratio [OR] = 3.02; 95% confidence interval [CI], 1.39–6.57). Thirty-three (20.6%) patients reported pain on day 1 (median 1 = very mild pain), 16 (10.0%) on day 3 (median 1 = very mild pain), and 9 (5.6%) on day 7 (median 2 = mild pain). The prognostic factors were as follows:(1) moderate/severe preoperative pain (OR = 4.41; 95% CI, 1.42–13.76 on day 3 and OR = 5.16; 95% CI, 1.17–22.78 on day 7),(2) provoked preoperative pain (OR = 4.24; 95% CI, 1.40–12.78 on day 3 and OR = 5.35; 95% CI, 1.27–22.51 on day 7),(3) pulpless tooth (OR = 0.11; 95% CI, 0.02–0.57 on day 3), and(4) sonic activation during treatment (OR = 3.02; 95% CI, 1.39–6.57 on day 1 and OR = 3.01; 95% CI, 1.05–8.59 on day 3).ConclusionsThere was no significant difference in pain experience between teeth filled using AH Plus or TotalFill BC Sealer 1, 3, and 7 days after obturation. Patient- and treatment-related factors could influence postobturation pain. 相似文献
90.
Owen E. Francis Matthew Bendall Solaiappan Manimaran Changjin Hong Nathan L. Clement Eduardo Castro-Nallar Quinn Snell G. Bruce Schaalje Mark J. Clement Keith A. Crandall W. Evan Johnson 《Genome research》2013,23(10):1721-1729
Emerging next-generation sequencing technologies have revolutionized the collection of genomic data for applications in bioforensics, biosurveillance, and for use in clinical settings. However, to make the most of these new data, new methodology needs to be developed that can accommodate large volumes of genetic data in a computationally efficient manner. We present a statistical framework to analyze raw next-generation sequence reads from purified or mixed environmental or targeted infected tissue samples for rapid species identification and strain attribution against a robust database of known biological agents. Our method, Pathoscope, capitalizes on a Bayesian statistical framework that accommodates information on sequence quality, mapping quality, and provides posterior probabilities of matches to a known database of target genomes. Importantly, our approach also incorporates the possibility that multiple species can be present in the sample and considers cases when the sample species/strain is not in the reference database. Furthermore, our approach can accurately discriminate between very closely related strains of the same species with very little coverage of the genome and without the need for multiple alignment steps, extensive homology searches, or genome assembly—which are time-consuming and labor-intensive steps. We demonstrate the utility of our approach on genomic data from purified and in silico “environmental” samples from known bacterial agents impacting human health for accuracy assessment and comparison with other approaches.The accurate and rapid identification of species and strains of pathogens is an essential component of biosurveillance from both human health and biodefense perspectives (Vaidyanathan 2011). For example, misidentification was among the issues that resulted in a 3-wk delay in accurate diagnosis of the recent outbreak of hemorrhagic Escherichia coli being due to strain O104:H4, resulting in over 3800 infections across 13 countries in Europe with 54 deaths (Frank et al. 2011). The most accurate diagnostic information, necessary for species identification and strain attribution, comes from the most refined level of biological data—genomic DNA sequences (Eppinger et al. 2011). Advances in DNA-sequencing technologies allows for the rapid collection of extraordinary amounts of genomic data, yet robust approaches to analyze this volume of data are just developing, from both statistical and algorithmic perspectives.Next-generation sequencing approaches have revolutionized the way we collect DNA sequence data, including for applications in pathology, bioforensics, and biosurveillance. Given a particular clinical or metagenomic sample, our goal is to identify the specific species, strains, or substrains present in the sample, as well as accurately estimate the proportions of DNA originating from each source genome in the sample. Current approaches for next-gen sequencing usually have read lengths between 25 and 1000 bp; however, these sequencing technologies include error rates that vary by approach and by samples. Such variation is typically less important for species identification given the relatively larger genetic divergences among species than among individuals within species. But for strain attribution, sequencing error has the potential to swamp out discriminatory signal in a data set, necessitating highly sensitive and refined computational models and a robust database for both species identification and strain attribution.Current methods for classifying metagenomic samples rely on one or more of three general approaches: composition or pattern matching (McHardy et al. 2007; Brady and Salzberg 2009; Segata et al. 2012), taxonomic mapping (Huson et al. 2007; Meyer et al. 2008; Monzoorul Haque et al. 2009; Gerlach and Stoye 2011; Patil et al. 2012; Segata et al. 2012), and whole-genome assembly (Kostic et al. 2011; Bhaduri et al. 2012). Composition and pattern-matching algorithms use predetermined patterns in the data, such as taxonomic clade markers (Segata et al. 2012), k-mer frequency, or GC content, often coupled with sophisticated classification algorithms such as support vector machines (McHardy et al. 2007; Patil et al. 2012) or interpolated Markov Models (Brady and Salzberg 2009) to classify reads to the species of interest. These approaches require intensive preprocessing of the genomic database before application. In addition, the classification rule and results can often change dramatically depending on the size and composition of the genome database.Taxonomy-based approaches typically rely on a “lowest common ancestor” approach (Huson et al. 2007), meaning that they identify the most specific taxonomic group for each read. If a read originates from a genomic region that shares homology with other organisms in the database, the read is assigned to the lowest taxonomic group that contains all of the genomes that share the homologous region. These methods are typically highly accurate for higher-level taxonomic levels (e.g., phylum and family), but experience reduced accuracy at lower levels (e.g., species and strain) (Gerlach and Stoye 2011). Furthermore, these approaches are not informative when the reads originate from one or more species or strains that are closely related to each other or different organisms in the database. In these cases, all of the reads can be reassigned to higher-level taxonomies, thus failing to identify the specific species or strains contained in the sample.Assembly-based algorithms can often lead to the most accurate strain identification. However, these methods also require the assembly of a whole genome from a sample, which is a computationally difficult and time-consuming process that requires large numbers of reads to achieve an adequate accuracy—often on the order of 50–100× coverage of the target genome (Schatz et al. 2010). Given current sequencing depths, obtaining this level of coverage is usually possible for purified samples, but coverage levels may not be sufficient for mixed samples or in multiplexed sequencing runs. Assembly approaches are further complicated by the fact that data collection at a crime scene or hospital might include additional environmental components in the biological sample (host genome or naturally occurring bacterial and viral species), thus requiring multiple filtering and alignment steps in order to obtain reads specific to the pathogen of interest.Here we describe an accurate and efficient approach to analyze next-generation sequence data for species identification and strain attribution that capitalizes on a Bayesian statistical framework implemented in the new software package Pathoscope v1.0. Our approach accommodates information on sequence quality, mapping quality, and provides posterior probabilities of matches to a known database of reference genomes. Importantly, our approach incorporates the possibility that multiple species can be present in the sample or that the target strain is not even contained within the reference database. It also accurately discriminates between very closely related strains of the same species with much less than 1× coverage of the genome and without the need for sequence assembly or complex preprocessing of the database or taxonomy. No other method in the literature can identify species or substrains in such a direct and automatic manner and without the need for large numbers of reads. We demonstrate our approach through application to next-generation DNA sequence data from a recent outbreak of the hemorrhagic E. coli (O104:H4) strain in Europe (Frank et al. 2011; Rohde et al. 2011; Turner 2011) and on purified and in silico mixed samples from several other known bacterial agents that impact human health. Software and data examples for our approach are freely available for download at https://sourceforge.net/projects/pathoscope/. 相似文献