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171.
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174.
Familial autoimmune myasthenia gravis 总被引:5,自引:0,他引:5
175.
Sumatriptan blocks spreading depression in isolated chick retina 总被引:1,自引:0,他引:1
PA Maranhâo-Filho H Martins-Ferreira MB Vincent LJC Ribeiro SAP Novis 《Cephalalgia : an international journal of headache》1997,17(8):822-825
Spreading depression is a neurohumoral phenomenon that has been related to the pathophysiology of migraine. The recently introduced 5HT1D agonist anti-migraine compound sumatriptan blocks neurogenic extravasation and induces cerebral vasoconstriction, but the actual mechanism of action against migraine remains obscure. Retinal spreading depression (RSD) velocity has been measured in isolated chick retinas in the presence of 0.05-2.00:nM sumatriptan. This drug reversibly blocks RSD in a concentration-dependent manner. Since the preparation is blood-vessel free, this effect must be related to the nervous tissue. 相似文献
176.
Cause of signal loss in MR images of old hemorrhagic lesions 总被引:2,自引:0,他引:2
Old hemorrhagic lesions in the brain are characteristically surrounded by a band of hemosiderin-containing tissue. This region is typically of low signal intensity on long-echo-time (TE) radio-frequency (RF) spin-echo magnetic resonance (MR) images and on gradient-echo MR images. To determine the cause of signal loss in this band, the authors measured the signal that arises from imaging such a region with use of an RF spin-echo technique with a 180 degrees pulse incrementally displaced from TE/2. The incremental loss of signal was small. Using an agar phantom containing iron particles, the authors also showed that signal loss results primarily from diffusion in magnetic gradients. They conclude that most signal loss in the dark band surrounding areas of late-stage hemorrhage arises from diffusion in areas of magnetic inhomogeneity. 相似文献
177.
Massaro A. R. Scivoletto G. Tonali P. 《The Italian Journal of Neurological Sciences》1990,11(6):537-547
Cerebrospinal fluid (CSF) markers are a useful tool for determining disease progression or activity in some neurological disorders
which need parameters both for evaluating treatments and investigating pathobiological evolution in researchoriented follow-up.
A number of CSF proteins are reviewed with data on biological properties, analytical methods, clinical usefulness of: myelin
basic protein, S-100 protein, glial fibrillary acidic protein, neural-cell adhesion molecule, neuron-specific enolase and
others.
Sommario I marcatori liquorali sono un utile strumento per determinare la progressione della malattia ele fasi di attività in alcuni disordini neurologici che necessitano di parametri utili a valutare l’efficacia di un trattamento, o a studiare l’evoluzione patobiologica in follow-up finalizzati alla ricerca. Gli autori passano in rassegna un certo numero di proteine liquorali soffermandosi sulle loro proprietà biologiche, sui metodi analitici, sull’utilizzo a scopi clinici. Vengono prese in considerazione: la proteina basica della mielina, la proteina S-100, la proteina acida gliale fibrillare, la proteina di adesione neuronale N-CAM, la enolasi neurono-specifica e alcune altre.相似文献
178.
JD Carroll M Reidy PA Savundra N Cleave J McAinsh 《Cephalalgia : an international journal of headache》1990,10(2):101-105
A randomized double-blind, cross-over study using treatment periods of 12 weeks with a 2-week washout, comparing two long-acting formulations of propranolol ('Inderal' LA 160 mg daily and Half-'Inderal' LA 80 mg daily) was performed after a placebo run-in of 4 weeks on 51 patients. The study indicated that both long-acting formulations were significantly better than placebo in reducing the frequency of migraine attacks (p less than 0.01). After 12 weeks there was a significantly lower (p = 0.03) frequency of migraine attacks in patients on the higher dose formulation than in those on the lower dose formulation. There was no significant difference in the frequency of side effects produced by the two formulations. 相似文献
179.
BACKGROUND: Anecdotal evidence suggests that high-dose intravenous immunoglobulin (IVIG) is useful in the management of human immunodeficiency virus (HIV)-associated thrombocytopenia. STUDY DESIGN AND METHODS: To rigorously evaluate this therapy, a crossover study was designed to compare IVIG, given at 1 g per kg per day for 2 consecutive days each week for 4 weeks, with intravenous saline placebo administered according to the same schedule. Subjects were randomly assigned to receive either IVIG or saline during the first 4 weeks; if IVIG was given, there was a 4-week period of no therapy before beginning placebo administration. Criteria for eligibility were platelet count of less than 50,000 per microL (50 × 10(9)/L), elevated platelet-associated IgG levels, increased megakaryocytes in the bone marrow, and positive HIV antibody test. Twelve patients (11 men, 1 woman) were studied. Seven patients completed the full protocol. Four dropped out: after 2, 5 (2 patients), and 8 weeks that included at least 2 weeks of IVIG. RESULTS: All patients sustained an increase in platelet count in response to IVIG, with increments ranging from 15,000 to 358,000 per microL (15 to 350 × 10(9)/L) (mean, 180,000/microL [180 × 10(9)/L]; median, 174,000/microL [174 × 10(9)/L]). No patient had an increase after placebo infusions. There were no adverse effects of treatment, and weekly chemical analyses showed no new abnormalities except for mild elevations in the serum protein. The duration of responses ranged from 2 to 10 weeks. No patient demonstrated refractoriness to IVIG. CONCLUSION: IVIG consistently raises platelet counts in patients with HIV-associated thrombocytopenia. 相似文献
180.
M. K. Urban MD PhD K. Jules-Elysee MD C. Loughlin PA W. Kelsey BA E. Flynn BA 《HSS journal》2008,4(1):76-80
The diagnosis of a postoperative myocardial infarction (PMI) is important in the orthopedic population because these events
can be associated with significant cardiac morbidity. Plasma troponin I (cTnI) analysis has markedly increased our ability
to detect myocardial damage. Using cTnI analysis for evidence of a PMI, we prospectively assessed all of our patients for
(1) the 1-year incidence of PMI, (2) the clinical consequences of a PMI in relation to the level of the cTnI release, and
(3) 6-month follow-up for cardiac complications. During a 12-month period, patients at risk for perioperative myocardial ischemia
were assessed for a PMI by serum cTnI levels and daily serial ECGs. Patients with cTnI levels above the reference level (≥0.4 ng/ml)
were also assessed for new cardiac regional wall motion abnormalities with an echocardiogram and 6-month postdischarge adverse
cardiac events. Of the 758 patients who were assessed for a PMI, 49 patients had detectable cTnI levels (≥0.4 ng/ml); the
incidence of a PMI was 0.6% of all surgical cases and 6.5% of those patients were at risk for a cardiac event. A PMI was more
common after hip arthroplasty than other orthopedic procedures. Twenty-three patients had a cTnI level >3.0 ng/ml, and 74%
these patients (17/23) had anginal symptoms and/or ischemic ECG changes. Nine of these patients (9/23) had new postoperative
echocardiographic changes, five (5/23) required emergency transfer to a cardiac care unit, and 10 (10/23) had postoperative
cardiac complications. In contrast, 15 patients with levels of cTnI <3.0 ng/ml and without ischemic ECG changes and/or anginal
symptoms had no postoperative cardiac complications. Fourteen patients (14/47) had cardiac complications 6 months after discharge,
including four cardiac deaths, one fatal stroke, and four patients with unstable anginal episodes that required a change in
medical management, and six patients required coronary revascularization. Orthopedic surgical patients with cTnI level <3 ng/ml
and without symptoms or ECG changes suggestive of myocardial ischemia (15/49) may have different risks than those with higher-level
cTn1.
This study was funded by the Department of Anesthesiology, Hospital for Special Surgery, New York, NY. 相似文献