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861.
CM Sorensen I Giese TH Braunstein JC Brasen M Salomonsson NH Holstein-Rathlou 《American journal of physiology. Renal physiology》2012,303(6):F855-F863
Connexins in renal arterioles affect autoregulation of arteriolar tonus and renal blood flow and are believed to be involved in the transmission of the tubuloglomerular feedback (TGF) response across the cells of the juxtaglomerular apparatus. Connexin40 (Cx40) also plays a significant role in the regulation of renin secretion. We investigated the effect of deleting the Cx40 gene on autoregulation of afferent arteriolar diameter in response to acute changes in renal perfusion pressure. The experiments were performed using the isolated blood perfused juxtamedullary nephron preparation in kidneys obtained from wild-type or Cx40 knockout mice. Renal perfusion pressure was increased in steps from 75 to 155 mmHg, and the response in afferent arteriolar diameter was measured. Hereafter, a papillectomy was performed to inhibit TGF, and the pressure steps were repeated. Conduction of intercellular Ca(2+) changes in response to local electrical stimulation was examined in isolated interlobular arteries and afferent arterioles from wild-type or Cx40 knockout mice. Cx40 knockout mice had an impaired autoregulatory response to acute changes in renal perfusion pressure compared with wild-type mice. Inhibition of TGF by papillectomy significantly reduced autoregulation of afferent arteriolar diameter in wild-type mice. In Cx40 knockout mice, papillectomy did not affect the autoregulatory response, indicating that these mice have no functional TGF. Also, Cx40 knockout mice showed no conduction of intercellular Ca(2+) changes in response to local electrical stimulation of interlobular arteries, whereas the Ca(2+) response to norepinephrine was unaffected. These results suggest that Cx40 plays a significant role in the renal autoregulatory response of preglomerular resistance vessels. 相似文献
862.
Beck R. Frydenborg Cory J. Krediet Max Teplitski Kim B. Ritchie 《Microbial ecology》2014,67(2):392-401
Bacteria living within the surface mucus layer of corals compete for nutrients and space. A number of stresses affect the outcome of this competition. The interactions between native microorganisms and opportunistic pathogens largely determine the coral holobiont's overall health and fitness. In this study, we tested the hypothesis that commensal bacteria isolated from the mucus layer of a healthy elkhorn coral, Acropora palmata, are capable of inhibition of opportunistic pathogens, Vibrio shiloi AK1 and Vibrio coralliilyticus. These vibrios are known to cause disease in corals and their virulence is temperature dependent. Elevated temperature (30 °C) increased the cell numbers of one commensal and both Vibrio pathogens in monocultures. We further tested the hypothesis that elevated temperature favors pathogenic organisms by simultaneously increasing the fitness of vibrios and decreasing the fitness of commensals by measuring growth of each species within a co-culture over the course of 1 week. In competition experiments between vibrios and commensals, the proportion of Vibrio spp. increased significantly under elevated temperature. We finished by investigating several temperature–dependent mechanisms that could influence co-culture differences via changes in competitive fitness. The ability of Vibrio spp. to utilize glycoproteins found in A. palmata mucus increased or remained stable when exposed to elevated temperature, while commensals' tended to decrease utilization. In both vibrios and commensals, protease activity increased at 30 °C, while chiA expression increased under elevated temperatures for Vibrio spp. These results provide insight into potential mechanisms through which elevated temperature may select for pathogenic bacterial dominance and lead to disease or a decrease in coral fitness. 相似文献
863.
864.
Max Stolpe 《Journal of Ornithology》1935,83(1):115-128
Ohne Zusammenfassung 相似文献
865.
Abstract The main distribution area of the Chameleon in Turkey is the Aegean and the Mediterranean regions, however, records are also available from the Marmara region and from southeast Anatolia. 相似文献
866.
867.
Susan H. Williams Christopher J. Vinyard Kenneth E. Glander Max Deffenbaugh Mark F. Teaford Cynthia L. Thompson 《International journal of primatology》2008,29(6):1441-1453
In vivo laboratory-based studies describing jaw-muscle activity and mandibular bone strain during mastication provide the empirical
basis for most evolutionary hypotheses linking primate masticatory apparatus form to diet. However, the laboratory data pose
a potential problem for testing predictions of these hypotheses because estimates of masticatory function and performance
recorded in the laboratory may lack the appropriate ecological context for understanding adaptation and evolution. For example,
in laboratory studies researchers elicit rhythmic chewing using foods that may differ significantly from the diets of wild
primates. Because the textural and mechanical properties of foods influence jaw-muscle activity and the resulting strains,
chewing behaviors studied in the laboratory may not adequately reflect chewing behaviors of primates feeding in their natural
habitats. To circumvent this limitation of laboratory-based studies of primate mastication, we developed a system for recording
jaw-muscle electromyograms (EMGs) from free-ranging primates so that researchers can conduct studies of primate jaw-muscle
function in vivo in the field. We used the system to record jaw-muscle EMGs from mantled howlers (Alouatta palliata) at Hacienda La Pacifica, Costa Rica. These are the first EMGs recorded from a noncaptive primate feeding in its natural
habitat. Further refinements of the system will allow long-term EMG data collection so that researchers can correlate jaw-muscle
function with food mechanical properties and behavioral observations. In addition to furthering understanding of primate feeding
biology, our work will foster improved adaptive hypotheses explaining the evolution of primate jaw form. 相似文献
868.
P. Veeraraghavan Ramachandran Daniel R. Nicponski Hari N.G. Nair Matthew A. Helppi Pravin D. Gagare C. Max Schmidt Michele T. Yip-Schneider 《Bioorganic & medicinal chemistry letters》2013,23(24):6911-6914
Aminated α-methylene-γ-butyrolactones, which are readily synthesized with facile control of the diastereoisomerism, provide an economical and commercially-viable alternative to the use of aminated natural products. These aminoloactones, which exhibit excellent activity against three pancreatic cancer cell lines when measured at 10 μM—Panc-1, MIA PaCa-2, and BxPC-3—and are comparable to or better than parthenolide and dimethylaminoparthenolide (DMAPT, LC-1). It has also been shown that there is an effect on the biological activity depending on the identity of the amine. 相似文献
869.
870.
René Hoehn Tanja Zeller Virginie J. M. Verhoeven Franz Grus Max Adler Roger C. Wolfs André G. Uitterlinden Rapha?le Castagne Arne Schillert Caroline C. W. Klaver Norbert Pfeiffer Alireza Mirshahi 《Human genetics》2012,131(11):1783-1793
Central corneal thickness (CCT) has become an endophenotype of major interest for the genetically complex disorder glaucoma. CCT has a high heritability, and thin CCT is an independent risk factor for the diagnosis and progression of open-angle glaucoma. Genome-wide association studies thus provide genetic loci associated with CCT and potentially related to open-angle glaucoma. The distribution of CCT and prevalence of glaucoma in population-based studies have demonstrated ethnic differences suggesting ethnic-dependent variations in the genetic determinants of CCT. We conducted a genome-wide association study in Caucasians (n?=?3,931) from the Gutenberg Health Study (Germany) followed by replication of 30 genome-wide significant SNPs or SNPs of interest (P?<?10?5) in the Rotterdam Study (The Netherlands, n?=?1,418). In a combined analysis, we confirmed quantitative trait loci on chromosomes 9q34 and 16q24 for association with CCT. On chromosome 16q24, the locus is located in an intergenic region near the ZNF469 gene (top SNP: rs9938149, P?=?1.45?×?10?12). ZNF469 missense mutation is involved in a syndrome with very thin cornea (brittle cornea syndrome). The second locus on chromosome 9q34 represents the intergenic region between the RXRA and COL5A1 gene (top SNP: rs3132306, P?=?2.71?×?10?10). Collagen type 5 determines the diameter of the corneal collagen fibrils. In our Caucasian population-based GWA study, we reinforce the involvement of collagen-related genes influencing CCT in Caucasians. We could not confirm the collagen type 8 locus on chromosome 1 as reported in Asian studies. 相似文献