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51.
The tetanic (tta; X.-52.6) mutation has been isolated on the basis of its sensitivity to extradoses of the normal Shaker gene complex (ShC) where the K+ channel la is encoded. The mutant shows up to threefold elevation of the membrane bound protein phosphatase type 1 (PP1) activity in body extracts, probably due to reduced levels of the PP1 specific inhibitor 2 (I-2). By contrast, PP1 activity in the head is only half of the normal value. In addition, tta fails to perform normally in a negative reinforcement olfactory paradigm. The functional relationships between phosphorylation, K+ currents, phosphatase activity and modulation of synaptic activity during learning and memory are discussed in the light of their possible genetic links. 相似文献
52.
G. B. Gurrola R. Molinar-Rode M. Sitges A. Bayon L. D. Possani 《Journal of neural transmission (Vienna, Austria : 1996)》1989,75(1):11-20
Summary A nonapeptide Thr-Ile-Ile-Asn-Val-Lys-Cys-Thr-Ser (NTX1–9) and a decapeptide Met-Asn-Gly-Lys-Cys-Lys-Cys-Tyr-Asn-Asn (NTX30–39) corresponding to the N-terminal and C-terminal sequences respectively of Noxiustoxin (NTX) were synthesized by the solid phase method of Merrifield (1963). The first synthetic peptide (NTX1–9) was shown to be toxic to mice independently of the route of administration: intraperitoneally, subcutaneously or intraventricularly (100–200 g/20 g mouse weight). The second (NTX30–39) was not toxic even at higher dose (400 g/20 g mouse). When the effects of the peptide NTX1–9 and of the authentic toxin (Noxiustoxin) were studied on the liberation of [3H] 4-aminobutyric acid (3H-GABA) from mouse synaptosomes, both gave essentially the same results, except that peptide NTX1–9 was needed at higher concentration. Synthetic peptide NTX30–39 had no effect in the same preparation at even higher doses. The GABA release produced by toxic peptide NTX1–9 was not affected by tetrodotoxin but was completely abolished by the presence of the K+ ionophore valinomycin, mimicking the effect of native NTX in the same system (Sitges et al., 1986). These results indicate that the toxic active site of Noxiustoxin is possibly located in or near the N-terminal amino acid portion of the molecule.Abbreviations used BOC
amino acids ter-butyloxycarbonyl-amino acids
- BOC
amino acid-PAM-resin ter-butyloxycarbonyl-aminoacyl-4-(oxymethyl)-phenacetamidomethyl-resin
- GABA 4
aminobutyric acid
- HPLC
high performance liquid chromatography
- MSA
mouse serum albumin
- NTX
Noxiustoxin
- NTX
(numbers) synthetic peptides with amino acid sequences of NTX at position start (first number) to position end (second number) of the sequence according to Fig. 1
- TTX
tetrodotoxin
Supported in part by the Mexican Council of Science and Technology (CONACyT), grants PVT/QF/NAL/84/2182, PVT/AI/NAL/85/3029 to L.D.P.; PCSACNA 022640 to A.B. A patent request claiming rights on the use of synthetic NTX and related peptides was presented in Washington, DC (U.S.A.), Serial number 07/132,169, filing date December 14, 1987. 相似文献
53.
A. K. Mir H. Berthold G. E. Scholtysik J. R. Fozard 《Naunyn-Schmiedeberg's archives of pharmacology》1989,340(4):424-430
Summary The present experiments were carried out to investigate the cardiovascular effects of endothelin 1 (ET) in pithed spontaneously hypertensive (SH) rats and to evaluate its mechanism of action. The results show that ET (0.1 – 3 nmol/kg i.v.) is a powerful vasoconstrictor agent in the pithed rat. However, at a dose of 3 nmol/kg i.v. all the pithed animals died following a gradual decrease in mean arterial blood pressure and pulse pressure and changes in the form of the electrocardiogram (ECG). The predominant feature of the change in the ECG was a progressive decrease in the amplitude of the T wave resulting in a depression of the curve representing repolarization. Investigations in isolated perfused SH rat hearts showed that ET powerfully reduces coronary flow concentration-dependently (IC50 2.1 ±0.3 nM) an effect associated with sinus bradycardia and a decrease in coronary pressure amplitude. No overt ECG changes were seen. Control experiments with mechanical flow restriction suggest that bradycardia is a consequence of reduced coronary flow and that the ECG changes observed in vivo can be explained on the basis of coronary insufficiency and resulting myocardial hypoxia. Vasoconstrictor responses to angiotensin II (0.4 g/kg i.v.), phenylephrine (8 g/kg i.v.) and ET (0.5 nmol/kg i.v.) were antagonised by around 70% by isradipine (0.03 mg/kg i.a.). The results suggest that endothelin-induced vasoconstriction may involve receptor operated channel activation and opening of voltage sensitive Ca2+ channels.Send offprint requests to A. K. Mir at the above address 相似文献
54.
Heppelmann B McDougall JJ 《Experimental brain research. Experimentelle Hirnforschung. Expérimentation cérébrale》2005,167(1):114-118
Synovial joints are complex sensory organs which provide continuous feedback regarding position sense and degree of limb movement.
The transduction mechanisms which convert mechanical forces acting on the joint into an electrochemical signal which can then
be transmitted to the central nervous system are not well understood. The present investigation examined the effect of the
mechanogated ion channel blockers amiloride and gadolinium on knee joint mechanosensitivity. In deeply anaesthetised rats
(sodium thiopental: 100–120 mg/kg, i.p.), single unit extracellular recordings were made from knee joint group III (Aδ) and
group IV (C) primary afferents in response to mechanical rotation of the joint. Afferent firing rate was measured before and
after topical application of either amiloride (0.1 mM, 1 mM) or gadolinium (250 μM) onto the receptive field of the sensory
unit and recording was continued every 10 min up to a total of 50 min. With normal rotation of the knee, joint mechanosensitivity
was significantly reduced by both amiloride (P<0.0001; n=10–21) and gadolinium (P=0.001; n=12) and this effect was sustained throughout the recording period. This investigation provides the first in vivo electrophysiological
evidence that joint mechanotransduction involves the activation of amiloride and gadolinium-sensitive mechanogated ion channels.
Future studies to determine the mechanogated ion channel subtypes present in joints and the modulation of their gating properties
during inflammation may yield novel approaches for the control of arthritis pain.
Funding: JJMcD is funded by the Alberta Heritage Foundation for Medical Research, the Canadian Institutes for Health Research, and
the Arthritis Society of Canada. 相似文献
55.
经络综合导引治疗仪是根据祖国医学的经络学说和养气功理论,应用呼气启动导引,视觉模型提示和穴位电刺激的多因素共同作用,导引气血沿经络运行。主要用于强化瘫痪肢体的康复。该治疗仪以单片微机为程控中心,通过硬件设计和软件开发,实现了呼气触发,视觉提示和位电刺激同步发,16和电极依次选通和数字化幅度调节等多种功能。 相似文献
56.
A. A. Galkin D. A. Sarkisyan E. N. Timin B. I. Khodorov 《Bulletin of experimental biology and medicine》1978,85(2):172-175
Experiments were carried out on isolated strips of guinea pig taenia coli. The smooth muscle was depolarized in a solution with high potassium concentration (120 mM KCl). The effect of papaverine (in concentrations of 10–5 to 3.10–5 g/ml) on the tone and off-response to a prolonged and strong hyperpolarizing current was investigated on the denervated muscle. Papaverine was found: 1) to abolish contractile responses to application of histamine, bradykinin, and acetylcholine; 2) to reduce the tone of the depolarized muscle and abolish the effect of an increase in the Ca++ concentration in the external medium on muscle tone; 3) to have no effect on the amplitude and velocity of the ascending phase of the off-response; 4) to accelerate the descending phase of the off-response. The following hypotheses are put forward to explain the result: 1) in the cell membrane there are chemically excitable calcium channels which are blocked by papaverine; 2) in the membrane there are calcium leakage channels responsible for the maintenance of tone and blocked by papaverine; 3) papaverine has negligible effect on electrically excitable calcium channels.A. V. Vishnevskii Institute of Surgery, Academy of Medical Sciences of the USSR, Moscow. Bio-Inorganic Chemicals BIKhS Research Institute, Kupavna, Moscow Region. (Presented by Academician of the Academy of Medical Sciences of the USSR N. A. Fedorov.) Translated from Byulleten' Éksperimental'noi Biologii i Meditsiny, Vol. 85, No. 2, pp. 177–180, February, 1978. 相似文献
57.
Nabil Nakhostine Daniel Lamontagne 《Pflügers Archiv : European journal of physiology》1994,428(5-6):526-532
The mechanism of hypoxia-induced coronary vasodilatation was studied in isolated, saline-perfused rabbit hearts under constant flow conditions. Reduction in the perfusion solution PO2 (from 520±6 to 103±9 mm Hg) under control conditions halved the coronary resistance and was accompanied by a significant release of the prostaglandin (PG) 6-keto-PGF1 (from 1.8±0.3 to a maximum of 4.4±0.9 pmol min–1 g–1). The cyclooxygenase inhibitor, diclofenac (1 M), blocked the release of PGI2 and reduced hypoxia-induced vasodilatation (from 47±8% to 25±5%, P<0.05). The relative contribution of adenosine, prostaglandins, and adenosine triphosphate (ATP)-sensitive K+ channel (KATP channel) activation in hypoxia-induced vasodilatation was assessed by comparing the differential change (control response minus response after treatment) in coronary perfusion pressure (CPP) during infusion of 8-phenyltheophylline (8-PT), diclofenac, and glibenclamide, respectively. The differential change in CPP with 8-PT and diclofenac given together (–48 ±7%) was found to be equivalent to the sum of their respective effects (–24±7 and –19±4%, respectively). Glibenclamide (0.3 M) reduced significantly hypoxia-induced vasodilatation (differential change in CPP of –27±6%) as well as the dilator response to 10 M adenosine and to the stable PGI2-analogue, iloprost. Forskolin-induced coronary vasodilatation in arrested hearts was slightly, but significantly, reduced by glibenclamide. Our results suggest that both cyclooxygenase products and adenosine, acting independently and concomitantly, contribute to the dilator response of coronary resistance vessels to hypoxia, in part through the activation of KATP channels. KATP channel activation by prostacyclin and adenosine may involve both cyclic adenosine monophosphate-dependent and independent pathways. 相似文献
58.
目的: 通过通道蛋白特定位点(P266T)突变,观察对ATP敏感性钾通道电生理特性的影响。 方法: 将Kir6.2及其突变子P266T的cDNA导入人胚肾细胞,表达ATP敏感性钾通道,用膜片钳方法研究KATP电生理特性。 结果: KATP(P266T)开放能力是野生型的2倍; KATP(P266T)密度仅是野生型20%; KATP(P266T)对ATP敏感性降低;对pH敏感性增高。 结论: KATP特定位点(P266T)突变可改变KATP电生理特性。 相似文献
59.
Shear stress induced membrane currents and calcium transients in human vascular endothelial cells 总被引:3,自引:0,他引:3
Gero Schwarz Guy Droogmans Bernd Nilius 《Pflügers Archiv : European journal of physiology》1992,421(4):394-396
We have measured membrane currents induced by shear stress together with intracellular calcium signals in endothelial cells from human umbilical cord veins. In the presence of extracellular calcium (Ca2+]o), shear stress induced an inward current at a holding potential of 0 mV which is accompanied by a rise in intracellular Ca2+ ([Ca2+]i). In the absence of extracellular calcium shear stress was unable to evoke a calcium signal but still induced a membrane current. The voltage dependence of the shear stress induced current was obtained from difference currents evoked by linear voltage ramps before and during application of shear stress. Its reversal potential Erev shifted from –2.3±0.8 mV (n=4) in a nominally Ca2+ free solution to +1.5±1.6 mV at 1.5 mM [Ca2+]o (n=4) and to +21.9±4.4 mV (n=7) at 10 mM [Ca2+]o. From our data we conclude that shear stress opens an ion channel that is 12.5±2.9 (n=7) times more permeable for calcium than for sodium or cesium. 相似文献
60.
目的:研究“钙激活的氯通道”成员之一gob-5和粘蛋白基因Muc5ac在小鼠哮喘模型肺部的表达。 方法: 22只清洁级BALB/c小鼠随机分成哮喘组和对照组,用逆转录聚合酶链反应法(RT-PCR)和免疫组化法分别测定肺组织gob-5 mRNA和粘蛋白基因Muc5ac蛋白的表达。 结果: 小鼠哮喘组肺组织gob-5 mRNA表达阳性(0.2297±0.0186,A),而对照组未出现gob-5 mRNA的表达(P<0.01);哮喘组Muc5ac蛋白表达(0.6637±0.0127,A)明显高于对照组(0.2060±0.0179,A)(P<0.01);哮喘组肺组织gob-5 mRNA表达与Muc5ac蛋白表达呈直线正相关(r=0.864, P<0.05)。 结论: Gob-5 mRNA表达的上调可能在哮喘小鼠气道粘液过度分泌中起着关键作用;抑制gob-5的表达将为哮喘的治疗提供新的策略。 相似文献