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排序方式: 共有10000条查询结果,搜索用时 15 毫秒
981.
Kanako Iwasaki Tomoyuki Fujiyama Shinya Nakata Minjeong Park Chika Miyoshi Noriko Hotta-Hirashima Aya Ikkyu Miyo Kakizaki Fumihiro Sugiyama Seiya Mizuno Manabu Abe Kenji Sakimura Satoru Takahashi Hiromasa Funato Masashi Yanagisawa 《The Journal of neuroscience》2021,41(12):2733
Sleep is regulated in a homeostatic manner. Sleep deprivation increases sleep need, which is compensated mainly by increased EEG δ power during non-rapid eye movement sleep (NREMS) and, to a lesser extent, by increased sleep amount. Although genetic factors determine the constitutive level of sleep need and sleep amount in mice and humans, the molecular entity behind sleep need remains unknown. Recently, we found that a gain-of-function Sleepy (Slp) mutation in the salt-inducible kinase 3 (Sik3) gene, which produces the mutant SIK3(SLP) protein, leads to an increase in NREMS EEG δ power and sleep amount. Since Sik3Slp mice express SIK3(SLP) in various types of cells in the brain as well as multiple peripheral tissues from the embryonic stage, the cell type and developmental stage responsible for the sleep phenotype in Sik3Slp mice remain to be elucidated. Here, we generated two mouse lines, synapsin1CreERT2 and Sik3ex13flox mice, which enable inducible Cre-mediated, conditional expression of SIK3(SLP) in neurons on tamoxifen administration. Administration of tamoxifen to synapsin1CreERT2 mice during late infancy resulted in higher recombination efficiency than administration during adolescence. SIK3(SLP) expression after late infancy increased NREMS and NREMS δ power in male synapsin1CreERT2; Sik3ex13flox/+ mice. The expression of SIK3(SLP) after adolescence led to a higher NREMS δ power without a significant change in NREMS amounts. Thus, neuron-specific expression of SIK3(SLP) after late infancy is sufficient to increase sleep.SIGNIFICANCE STATEMENT The propensity to accumulate sleep need during wakefulness and to dissipate it during sleep underlies the homeostatic regulation of sleep. However, little is known about the developmental stage and cell types involved in determining the homeostatic regulation of sleep. Here, we show that Sik3Slp allele induction in mature neurons in late infancy is sufficient to increase non-rapid eye movement sleep amount and non-rapid eye movement sleep δ power. SIK3 signaling in neurons constitutes an intracellular mechanism to increase sleep. 相似文献
982.
Thomas Klopstock MD Aleksandar Videnovic MD Almut Turid Bischoff MD Cecilia Bonnet MD Laura Cif MD Cynthia Comella MD Marta Correa-Vela MD Maria L. Escolar MD Jamie L. Fraser MD Victoria Gonzalez MD Neal Hermanowicz MD Robert Jech MD Hyder A. Jinnah MD Tomasz Kmiec MD Anthony Lang MD Maria J. Martí MD Saadet Mercimek-Andrews MD Migvis Monduy MD Graeme A.M. Nimmo MBBS Belen Perez-Dueñas MD Helle Cecilie Viekilde Pfeiffer MD Lluis Planellas MD Emmanuel Roze MD Nivedita Thakur MD Laura Tochen MD Nora Vanegas-Arroyave MD Giovanna Zorzi MD Colleen Burns PhD Feriandas Greblikas MD 《Movement disorders》2021,36(6):1342-1352
983.
984.
《Journal of medical engineering & technology》2013,37(4):292-306
AbstractA comparative study of three computer-aided classification (CAC) systems for characterization of focal hepatic lesions (FHLs), such as cyst, hemangioma (HEM), hepatocellular carcinoma (HCC) and metastatic carcinoma (MET), along with normal (NOR) liver tissue is carried out in the present work. In order to develop efficient CAC systems a comprehensive and representative dataset consisting of B-mode ultrasound images with (1) typical and atypical cases of cyst, HEM and MET lesions, (2) small and large HCC lesions and (3) NOR liver cases have been used for designing K-nearest neighbour (KNN), probabilistic neural network (PNN) and a back propagation neural network (BPNN) classifiers. For differential diagnosis between atypical FHLs, expert radiologists often visualize the textural characteristics of regions inside and outside the lesion. Accordingly in the present work, texture features and texture ratio features are computed from regions inside and outside the lesions. A feature set consisting of 208 texture features (i.e. 104 texture features and 104 texture ratio features) is subjected to principal component analysis (PCA) for dimensionality reduction; it is observed that maximum accuracy of 87.7% is obtained for a PCA-BPNN-based CAC system in comparison to 86.1% and 85% as obtained by PCA-PNN and PCA-KNN-based CAC systems. The sensitivity of the proposed PCA-BPNN based CAC system for NOR, Cyst, HEM, HCC and MET cases is 82.5%, 96%, 93.3%, 90% and 82.2%, respectively. The sensitivity values with respect to typical, atypical, small HCC and large HCC cases are 85.9%, 88.1%, 100% and 87%, respectively. Keeping in view the comprehensive and representative dataset used for designing the classifier, the results obtained by the proposed PCA-BPNN-based CAC system are quite encouraging and indicate its usefulness to assist experienced radiologists for interpretation and diagnosis of FHLs. 相似文献
985.
986.
Xuelin Zhang Chengzhi He Chunya He Baofu Chen Yanxia Liu Min Kong Chunguo Wang Lizhong Lin Yan Dong Haihui Sheng 《Pathology, research and practice》2013
Esophageal squamous cell carcinoma (ESCC) is one of the most common tumors worldwide, with a high malignant degree and poor prognosis. The present study aims to investigate the relationship between pyruvate kinase M2 (PKM2) expression and the prognosis of patients with ESCC. The expression of PKM2 in 86 cases of esophageal carcinoma tissues was tested using immunohistochemistry. The relationship between PKM2 expression and clinical pathological parameters, and their effects on the prognosis of patients with ESCC were analyzed. The expression levels of PKM2 in both cytoplasm and nucleus of ESCC tissues were significantly higher than those in paracancerous tissues (P = 6.73 × 10−9 and 4.32 × 10−6, respectively). The Kaplan–Meier analysis showed that nuclear PKM2 expression was closely related to the survival of patients with ESCC (P = 0.005). Patients with high PKM2 expression in the nucleus had significantly shorter survival times than those with low PKM2 expression in the nucleus (hazard ratio for death, 2.358; 95% confidence interval, 1.156–4.812; P = 0.018). No other significant difference was found between PMK2 expression and clinico-pathological features of ESCC patients (all P > 0.05). In conclusion, high PKM2 expression in the nucleus is essential in the pathogenic process of ESCC and may be used to predict the prognosis of patients with ESCC. 相似文献
987.
988.
目的 淀粉样前体蛋白(APP)基因是与痴呆症发生发展相关的重要基因,利用APP基因敲除小鼠探讨铝诱导的认知障碍损伤,及APP对中
毒性认知障碍损伤的作用。方法 3月龄同窝阴性小鼠分为野生对照组(WT)和铝处理组(WT+Al),APP敲除小鼠分为模型对照组(APP-/- )和
模型处理组(APP-/- +Al),每组10只。铝处理组在粮食中加入相应剂量的乳酸铝,同窝阴性小鼠和APP-/-小鼠给予常规鼠粮作为对照,乳酸
铝处理8周后进行水迷宫实验。HE染色观察小鼠脑组织神经病理改变;Western blotting检测糖原合成激酶3β(GSK-3β)和Caspase-3的活性变
化。结果 与WT相比,WT+Al小鼠在原平台区域停留时间和穿越原平台区域次数减少了28.1%和18.8%,而APP-/- +Al小鼠在原平台区域停留时间
和穿越原平台区域次数减少了44.1%和51%。Western blotting显示,WT+Al小鼠和APP-/-+Al小鼠脑组织中p-GSK-3β分别减少了17.4%和46.4%。结论 APP基因敲除促进铝诱导的神经毒性和学习记忆损伤。APP基因敲除导致GSK-3β的磷酸化水平降低、活性增高。由于GSK-3β活性增加对痴呆症具有促进作用,推测APP通过抑制GSK-3β活性在痴呆症发生过程中发挥保护效应。 相似文献
989.
Hajime Miyata Soichiro Fushimi Yoko Ota Harry V. Vinters Kaori Adachi Eiji Nanba Tomoyuki Akiyama 《Neuropathology》2021,41(1):58-64
Tuberous sclerosis complex (TSC) is an autosomal dominant hereditary disorder caused by mutations in either TSC1 on chromosome 16 or TSC2 on chromosome 9, clinically characterized mainly by facial angiofibroma, epilepsy, and intellectual disability. Cortical dysplasias, subependymal nodules, and subependymal giant cell astrocytoma are characteristic central nervous system lesions among 11 major features in the current clinical diagnostic criteria for TSC. We encountered an unusual case of genetically confirmed TSC1 presenting with symptomatic West syndrome due to an isolated cortical dysplasia in the left occipital lobe of a six‐month‐old male infant who did not meet the clinical diagnostic criteria for TSC. The patient underwent left occipital lesionectomy at age 11 months and has been seizure‐free for nearly six years since then. Histological examination of the resection specimen revealed cortical neuronal dyslamination with abundant dysmorphic neurons and ballooned cells, consistent with focal cortical dysplasia (FCD) type IIb. However, the lesion was also accompanied by unusual features, including marked calcifications, dense fibrillary gliosis containing abundant Rosenthal fibers, CD34‐positive glial cells with abundant long processes confined to the dysplastic cortex, and multiple nodular lesions occupying the underlying white matter, consisting exclusively of ballooned cell and/or balloon‐like astrocytes with focal calcifications. Genetic testing for TSC1 and TSC2 using the patient's peripheral blood revealed a germline heterozygous mutation in exon 7 (NM_000368.5: c.526dupT, p.Tyr176fs) in TSC1. Isolated FCD with unusual features such as calcification, dense fibrillary gliosis, Rosenthal fibers and/or subependymal nodule‐like lesions in the white matter may indicate the possibility of a cortical tuber even without a clinical diagnosis of TSC. Identification of such histopathological findings has significant implications for early and accurate diagnosis and treatment of TSC, and is likely to serve as an important supplementary feature for the current clinical diagnostic criteria for TSC. 相似文献
990.
《Immunological investigations》2013,42(8):864-875
Background: Systemic lupus erythematosus is one of the autoimmune diseases characterized by multisystem involvement associated with autoantibody and immune complex vasculitis along with endothelial cell damage. Objective: to study the possible role of Angiopoietin- 2 (Ang-2) as a recently highlighted inflammatory and angiogenic mediator in the pathogenesis of SLE and its correlation with the state of another inflammatory marker, P-Selectin, as well as with various markers of the disease activity. Patients and methods: The present study included 3 main groups: active SLE patients (group I), inactive SLE patients (group II) and healthy normal control subjects (group III). Groups I and II were subjected to disease activity assessment using the SLEDAI scoring system and measurement of plasma Ang-2 and P-Selectin by ELISA in addition to various laboratory investigations to assess disease activity as: Complete blood count, ESR, serum creatinine, C3, C4 and 24-h urinary proteins. Results: The mean level of Plasma Ang-2 and P-selectin showed a high significant increase in active group compared to inactive SLE patients and control subjects (p < 0.001).There was a significant positive correlation between Ang-2, P-Selectin, and each of SLEDAI score and 24-h urinary proteins in all SLE patients as well as in the active group, and Ang-2 was a significant independent marker for proteinuria. A significant negative correlation was found between Ang-2, P-Selectin and each of C3, C4. Ang-2 and P-Selectin showed a high sensitivity and specificity in the patients with SLE. Conclusion: Our study suggests that Ang-2 may be a more useful marker than P-Selectin, C3 and C4 in the assessment of disease activity. 相似文献