| 收费全文 | 1371280篇 |
| 免费 | 102211篇 |
| 国内免费 | 4733篇 |
| 耳鼻咽喉 | 17292篇 |
| 儿科学 | 44805篇 |
| 妇产科学 | 36979篇 |
| 基础医学 | 202393篇 |
| 口腔科学 | 36766篇 |
| 临床医学 | 132342篇 |
| 内科学 | 266323篇 |
| 皮肤病学 | 27478篇 |
| 神经病学 | 114767篇 |
| 特种医学 | 49155篇 |
| 外国民族医学 | 368篇 |
| 外科学 | 188479篇 |
| 综合类 | 29953篇 |
| 现状与发展 | 1篇 |
| 一般理论 | 474篇 |
| 预防医学 | 117540篇 |
| 眼科学 | 29961篇 |
| 药学 | 101315篇 |
| 12篇 | |
| 中国医学 | 3607篇 |
| 肿瘤学 | 78214篇 |
| 2021年 | 12024篇 |
| 2019年 | 12753篇 |
| 2018年 | 17889篇 |
| 2017年 | 13259篇 |
| 2016年 | 14133篇 |
| 2015年 | 16084篇 |
| 2014年 | 21905篇 |
| 2013年 | 33675篇 |
| 2012年 | 46964篇 |
| 2011年 | 49920篇 |
| 2010年 | 28635篇 |
| 2009年 | 25910篇 |
| 2008年 | 44993篇 |
| 2007年 | 47394篇 |
| 2006年 | 47239篇 |
| 2005年 | 45711篇 |
| 2004年 | 43534篇 |
| 2003年 | 41316篇 |
| 2002年 | 39980篇 |
| 2001年 | 61892篇 |
| 2000年 | 63761篇 |
| 1999年 | 53055篇 |
| 1998年 | 14839篇 |
| 1997年 | 13450篇 |
| 1996年 | 13295篇 |
| 1995年 | 12622篇 |
| 1994年 | 11733篇 |
| 1993年 | 11036篇 |
| 1992年 | 41721篇 |
| 1991年 | 40879篇 |
| 1990年 | 39557篇 |
| 1989年 | 37436篇 |
| 1988年 | 34664篇 |
| 1987年 | 33767篇 |
| 1986年 | 32212篇 |
| 1985年 | 30704篇 |
| 1984年 | 23086篇 |
| 1983年 | 19632篇 |
| 1982年 | 11782篇 |
| 1979年 | 20825篇 |
| 1978年 | 14831篇 |
| 1977年 | 12080篇 |
| 1976年 | 11894篇 |
| 1975年 | 12129篇 |
| 1974年 | 14810篇 |
| 1973年 | 14488篇 |
| 1972年 | 13361篇 |
| 1971年 | 12431篇 |
| 1970年 | 11494篇 |
| 1969年 | 10421篇 |
Background
Since recent reports have shown that (-)-Epigallocatechin-3-gallate (EGCG) could be used for treating proliferative and inflammatory disorders, we explored its use for the management of corneal chemical burns.Materials and methods
Initially, EGCG was assayed on the rabbit corneal epithelial cell line RCE1(5T5) to establish the best testing conditions, and to avoid unwanted outcomes in the experimental animals. Then, we studied its effects on cell proliferation, cell cycle progression and cell differentiation. Afterwards, we instilled EGCG in experimental grade II corneal alkali burns in mice, three times a day up to 21 days, and evaluated by slit lamp examination and histological sections of corneal epithelial, corneal endothelial and stromal edema, as well as the presence of inflammatory cells and neovascularization.Results
EGCG reduced cell growth and led to a decline in the proportion of proliferative cells in a concentration dependent manner. At 10 μM, EGCG promoted cell differentiation, an effect not related with apoptosis or cytotoxicity. When 10 μM EGCG was instilled in corneal alkali burns in mice three times a day up to 21 days, EGCG significantly reduced corneal opacity and neovascularization. The improved clinical appearance of the cornea was associated to a controlled epithelial growth; epithelial morphology was similar to that observed in normal epithelium and contrasted with the hyperproliferative, desquamating epithelium observed in control burn wounds. EGCG reduced corneal, stromal and endothelial edema, and wound inflammation.Conclusion
This work constitutes the first evidence for the use of EGCG in the acute phase of a corneal alkali burn, representing a possible novel alternative to improve patient outcomes as an add-on therapy. 相似文献Method: Socio-demographics, early-life adversity (ELA), individual quality of life (iQoL), and mental and physical health of 270 individuals (Mage = 66.82 years, 71.5% female) were assessed. Polynomial regressions and mediation analyses were conducted.
Results: Significant inverse U-shaped associations were found between ELA and iQoL (β = ?.59, p = .005) and between ELA and mental health (β = ?.64, p = .002), but not between ELA and physical health. Furthermore, mental health significantly mediated the relationship between ELA and iQoL (b = ?.84, BCa CI [?1.66, ?.27]).
Conclusion: Highest level of individual quality of life (i.e. successful aging) was related to a moderate amount of ELA. Additionally, mental health significantly mediated this relationship. These findings suggest that some amount of ELA could be beneficial for successful aging. Resource-focused interventions are needed to improve health and promote successful aging for an underdetected, at-risk subgroup with low early-life adversity. 相似文献
Background
Rosacea is a chronic inflammatory skin condition whose etiology has been linked to mast cells and the antimicrobial peptide cathelicidin LL-37. Individuals with refractory disease have demonstrated clinical benefit with periodic injections of onabotulinum toxin, but the mechanism of action is unknown.Objectives
To investigate the molecular mechanism by which botulinum toxin improves rosacea lesions.Methods
Primary human and murine mast cells were pretreated with onabotulinum toxin A or B or control. Mast cell degranulation was evaluated by β-hexosaminidase activity. Expression of botulinum toxin receptor Sv2 was measured by qPCR. The presence of SNAP-25 and VAMP2 was established by immunofluorescence. In vivo rosacea model was established by intradermally injecting LL-37 with or without onabotulinum toxin A pretreatment. Mast cell degranulation was assessed in vivo by histologic counts. Rosacea biomarkers were analyzed by qPCR of mouse skin sections.Results
Onabotulinum toxin A and B inhibited compound 48/80-induced degranulation of both human and murine mast cells. Expression of Sv2 was established in mouse mast cells. Onabotulinum toxin A and B increased cleaved SNAP-25 and decreased VAMP2 staining in mast cells respectively. In mice, injection of onabotulinum toxin A significantly reduced LL-37-induced skin erythema, mast cell degranulation, and mRNA expression of rosacea biomarkers.Conclusions
These findings suggest that onabotulinum toxin reduces rosacea-associated skin inflammation by directly inhibiting mast cell degranulation. Periodic applications of onabotulinum toxin may be an effective therapy for refractory rosacea and deserves further study. 相似文献Methods: Tumour and surrounding tissue were modeled by elliptical two- and three-dimensional computational phantoms having six different nanoparticle distributions. Nanoparticles were modeled as point heat sources having amplitude-dependent loss power. The total number of nanoparticles was fixed, and their spatial distribution and heat output were varied. Heat transfer was computed by solving the Pennes’ bioheat equation using finite element methods (FEM) with temperature-dependent blood perfusion. Local temperature was regulated using a proportional-integral-derivative (PID) controller. Tissue temperature, thermal dose and tissue damage were calculated. The required minimum thermal dose delivered to the tumor was kept constant, and heating power was adjusted for comparison of both the heating methods.
Results: Modulated power heating produced lower and more homogeneous temperature distributions than did constant power heating for all studied nanoparticle distributions. For a concentrated nanoparticle distribution, located off-center within the tumor, the maximum temperatures inside the tumor were 16% lower for modulated power heating when compared to constant power heating. This resulted in less damage to surrounding normal tissue. Modulated power heating reached target thermal doses up to nine-fold more rapidly when compared to constant power heating.
Conclusions: Controlling the temperature at the tumor-healthy tissue boundary by modulating the heating power of magnetic nanoparticles demonstrably compensates for a variable nanoparticle distribution to deliver effective treatment. 相似文献