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101.
目的应用超声手段探测儿童颈动脉内膜-中层厚度(IMT),探讨其与儿童肥胖类型的关系。方法依体质指数(BMI)、腰围身高比(WHtR)标准,入组外周性肥胖组160名(A组),内脏性肥胖150名(B组),正常体重儿童160名(正常对照组);应用超声手段探测各组儿童内脏脂肪厚度(VFT)和颈动脉内膜-中层厚度,比较3组间各项检测参数。结果内脏肥胖组VFT、IMT均高于外周性肥胖组及正常组,差异具有统计学意义(P〈0.05);外周性肥胖组VFT、IMT与正常组相似,差异没有显著性。结论IMT与肥胖类型相关,内脏性肥胖儿童VFT、IMT增加。实时超声检查技术为研究儿童肥胖类型提供了一种新的检测手段。 相似文献
102.
Melatonin seems to be an important stimulatory factor of the immune system. This indolamine is capable of inducing activation of leukocytes. Tissue leukocyte infiltration is a key feature of inflammatory and immune responses; however, there is no information about the effect of melatonin on leukocyte chemotaxis. Therefore, the aim of this study was to examine the in vitro and in vivo effects of melatonin on leukocyte chemotaxis, on modulation of leukocyte chemotaxis to other chemoattractants and on the in vivo induction of leukocyte chemokines. Neutrophils and mononuclear leukocytes (PBMC) were isolated by a discontinuous gradient on Hystopaque. Chemotaxis was performed in blind well Boyden's chambers. In vivo chemotaxis was determined after intraperitoneal injection of melatonin into rats. Leukocyte chemotactic response and leukocyte chemokine expression were determined in human volunteers treated with 20 mg daily of melatonin. Increased neutrophils and PBMC chemotaxis in response to 1.2 nm melatonin was observed in vitro. Peritoneal leukocytes were found increased after melatonin injection. Humans treated with melatonin showed an increased neutrophil chemotactic response to a physiological chemoattractant and increased expression of intracellular chemokines; however, decreased chemotactic response and no chemokine expression were observed in PBMC. These data suggest that melatonin could have a relevant role during the tissue leukocyte infiltration in inflammatory and immune responses. 相似文献
103.
Schmidt JM Rincon F Fernandez A Resor C Kowalski RG Claassen J Connolly ES Fitzsimmons BF Mayer SA 《Neurocritical care》2007,7(1):10-17
Background
Cerebral infarction is a common complication of aneurysmal subarachnoid hemorrhage (SAH), but usually occurs several days after onset as a complication of vasospasm or aneurysm repair. The frequency, causes, and clinical impact of acute infarction associated with the primary hemorrhage are poorly understood. 相似文献104.
目的 探讨应用非每日千伏级锥形束CT(KVCBCT)校位能否改善摆位误差对鼻咽癌调强放疗(IMRT)剂量分布影响。方法 对14例行根治性IMRT的鼻咽癌患者治疗开始后连续5次用KVCBCT检测摆位误差,并将其均值作为系统误差预测值,若其>1.5 mm则在第6次离线校位。假设通过移床能完全校正系统误差,那么从第6次起实际各方向摆位误差值加上离线校位值可得到未行校位时的摆位误差值,在治疗计划系统中通过等中心移位重新计算剂量来模拟应用非每日校位策略前后摆位误差所致的剂量变化。结果 对10例系统误差预测值>1.5 mm者摆位误差明显降低了靶区剂量:98%大体肿瘤体积(GTV)所接受剂量(GTV-D98)平均减少3.8Gy(Z=-2.81,P=0.005),原发灶临床靶体积(CTVns) D95( CTVns-D95)平均减少4.8Gy(Z=-1.96,P=0.050),高危CTV1 -D95平均减少1.0Gy(Z=-2.82,P=0.005),低危CTV2-D95减少不明显(Z=-0.13,P=0.900)。应用非每日校位后明显减少了摆位误差的三维方向位移总量,均值从3.6 mm减少为2.6mm(t=2.00,P=0.000),GTV-D98平均增加3.8 Gy(Z=-2.70,P=0.007),CTVns-D95平均增加5.0Gy(Z=-2.15,P=0.030),CTV1 -D95平均增加0.9Gy(Z=-2.80,P=0.005),减少了危及器官剂量增加>3%、5%患者比例。结论 应用非每日KVCBCT校位能有效减少摆位误差对鼻咽癌IMRT剂量分布的不利影响。 相似文献
105.
目的:分析总结食管癌切除胸腹二区淋巴结清扫的手术疗效。方法:回顾分析1986年2月~2007年12月我院对中下段食管癌和上段食管癌分别采用Ivor—Lewis术式,即上腹正中、右胸后外侧二切口切除及Akiyama术式.即右胸后外侧、上腹正中、左颈部三切口切除,并作胸腹二区淋巴结清扫治疗胸段食管癌1690例的临床资料,总结胸腹二区淋巴结转移的发生率并随访1、3、5年的生存率。结果:全组手术切除率为97.86%(1690/1727)。全组有淋巴结转移782例,占46.27%,其中胸部淋巴结转移占38.93%(658/1690),腹部淋巴结转移占25.92%(438/1690),胸部淋巴结转移发生于最上纵隔位于气管食管沟及喉返神经旁占20.47%(346/1690),术后共有178例发生230例次各种并发症,总的并发症的发生率为13.6%(230/1690),其中肺部并发症为第一位,占34.3%,心律失常占17.4%,喉返神经损伤发生率为8.7%,吻合口瘘发生率为1.7%。术后1、3、5年的生存率分别为88.2%(1161/1316)、63.5%(634/998)和51.8%(331/639)。无淋巴结转移的5年生存率为65.2%(219/336),有淋巴结转移的5年生存率为32.3%(102/316)。结论:Ivor-Lewis术式和Akiyama术式胸腹腔有良好的显露,淋巴结清扫彻底、方便,尤其对右侧最上纵隔沿喉返神经旁淋巴结清扫便利。特别对有淋巴结转移的食管癌患者行胸、腹二区淋巴结清扫十分必要,能明显提高术后5年生存率。 相似文献
106.
107.
108.
The kinetic occipital (KO) region in man: an fMRI study 总被引:10,自引:8,他引:2
Van Oostende S; Sunaert S; Van Hecke P; Marchal G; Orban GA 《Cerebral cortex (New York, N.Y. : 1991)》1997,7(7):690-701
We used functional magnetic resonance imaging to explore, in individual
subjects, the properties of the kinetic occipital (KO) region, which
previous position emission tomography studies have shown to be involved in
the processing of kinetic boundaries. The KO region was significantly
activated in 23/25 subjects tested in the subtraction of uniform motion
from kinetic gratings. The KO region is genuinely specialized for
processing kinetic boundaries since it is significantly more activated by
kinetic gratings than by luminance-defined gratings, uniform motion or
transparent motion. This leaves only the kinetic boundaries, created by
discontinuities in motion direction, as the specific stimulus aspect,
activating the KO region. The KO region is anatomically and functionally
distinct from areas MT/V5, V3 and V3A. It also has minimal overlap with the
lateral occipital (LO) region. The selective activation of the KO region is
robust and relatively immune to changes in stimulus size, spatial frequency
and type of kinetic boundary. These results strongly argue for the view
that the KO region is a new, separate, functional region in human occipital
cortex.
相似文献
109.
Electron microscopic evidence of persistent chlamydial infection following treatment 总被引:4,自引:0,他引:4
EY Bragina † MA Gomberg ‡ GA Dmitriev† 《Journal of the European Academy of Dermatology and Venereology》2001,15(5):405-409
Chlamydia trachomatis infections of the female and male genital tracts are often asymptomatic and, thus, tend to become persistent. In the persistent state the typical Chlamydia life cycle is arrested and standard antibiotic regimens do not always eradicate this infection. We sought to relate treatment failures in men and women with persistent chlamydial genital tract infections to electron microscopic evidence of chlamydial persistence and with atypical morphological forms of the organism. Of 16 patients with chlamydial persistence following azithromycin treatment, morphological variants of this organism were observed by electron microscopy from one endocervical sample and one male urethral sample. We document the presence of intracellular inclusions containing only reticulate bodies, extracellular monomembrane and polymembrane phagosomes containing elementary bodies and reticulate bodies with abnormal outer membranes in the process of dividing extracellularly. These observations parallel previous in vitro studies of chlamydial persistence under adverse conditions. This capacity of C. trachomatis to undergo atypical morphological alterations in vivo may contribute to its persistence and relative resistance to antibiotics. 相似文献
110.
Adjuvant pretreatment with alum protects neonatal mice in sepsis through myeloid cell activation
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J. C. Rincon A. L. Cuenca S. L. Raymond B. Mathias D. C. Nacionales R. Ungaro P. A. Efron J. L. Wynn L. L. Moldawer S. D. Larson 《Clinical and experimental immunology》2018,191(3):268-278
The high mortality in neonatal sepsis has been related to both quantitative and qualitative differences in host protective immunity. Pretreatment strategies to prevent sepsis have received inadequate consideration, especially in the premature neonate, where outcomes from sepsis are so dismal. Aluminium salts‐based adjuvants (alum) are used currently in many paediatric vaccines, but their use as an innate immune stimulant alone has not been well studied. We asked whether pretreatment with alum adjuvant alone could improve outcome and host innate immunity in neonatal mice given polymicrobial sepsis. Subcutaneous alum pretreatment improves survival to polymicrobial sepsis in both wild‐type and T and B cell‐deficient neonatal mice, but not in caspase‐1/11 null mice. Moreover, alum increases peritoneal macrophage and neutrophil phagocytosis, and decreases bacterial colonization in the peritoneum. Bone marrow‐derived neutrophils from alum‐pretreated neonates produce more neutrophil extracellular traps (NETs) and exhibit increased expression of neutrophil elastase (NE) after in‐vitro stimulation with phorbol esters. In addition, alum pretreatment increases bone marrow and splenic haematopoietic stem cell expansion following sepsis. Pretreatment of neonatal mice with an alum‐based adjuvant can stimulate multiple innate immune cell functions and improve survival. These novel findings suggest a therapeutic pathway for the use of existing alum‐based adjuvants for preventing sepsis in premature infants. 相似文献