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171.
生物医药领域近年来发展迅猛,多肽类药物因其生物学活性高、毒性小、生物相容性好等优势,在肿瘤治疗、细胞活性模拟、抗体检测等领域展开广泛应用,多肽的检测分析也成为研究的一大热点。传统的色谱法、溶剂沉淀法、离心超滤法和固相萃取法对多肽能够展现富集效果,但富集的效率往往不够理想。近年来,以有机框架材料为代表的纳米材料,在气体吸附、荧光、传感和催化等领域展开了广泛应用。有机框架材料凭借着独特的结构尺寸,成为了一类理想的生物吸附剂。由于其具有表面可修饰性,能够大大提高对多肽的富集效率。本文着重介绍近5年来金属-有机框架材料(metalorganic frameworks,MOFs)和共价-有机框架(covalent-organic frameworks,COFs)在多肽富集中的应用。 相似文献
172.
木波罗种子脱水敏感性与膜脂过氧化的研究 总被引:2,自引:0,他引:2
刚采收的木波罗种子含水量为58.6%。随着含水量下降,种子的发芽率和发芽指数迅速下降,种子对脱水非常敏感,是典型的顽拗性种。自然脱水时,种子胚轴和子叶中超氧物歧化酶的活性先上升,然后下降,丙二醛和脂质氢过氧化物的含量显著增加。其脱水敏感性的原因可能是当种子脱水时,植物酶SOD的活性下降,膜脂过氧化作用加强,从而使膜的结构和功能受到破坏,种子生活力丧失。 相似文献
173.
美味猕猴桃子叶愈伤组织的原生质体培养和再生植株 总被引:12,自引:0,他引:12
从B_5和NN-69培养基(含1mg/L 2,4-D)上分别选出美味猕猴桃子叶愈伤组织系A_(11)B_2和A_(16)N_1。在B_5原生质体培养基中,A_(11)B_2的原生质体再生细胞形成小细胞团;在NN-69原生质体培养基中,A_(16)N_1的原生质体再生细胞能持续分裂形成愈伤组织。经过分步诱导再生,获得A_(16)N_1原生质体再生植株。 相似文献
174.
175.
镇海棘螈(Echinotriton chinhaiensis)为国家一级重点保护野生动物,其种群面临着生境退化及丧失的重要威胁。产卵是决定镇海棘螈种群数量增长的关键环节之一,了解其产卵选择的微生境偏好可以更有针对性地保护该物种。本研究旨在确定影响镇海棘螈产卵场微生境选择的关键环境变量,同时为该物种的产卵生境保护、改造和重建提供科学基础。本文于2021年3-5月(繁殖期)在浙江省宁波市北仑区林场对镇海棘螈产卵位点(n=105)与非产卵位点(n=70)处的18个微生境变量进行调查。采用拟合优度卡方检验判断3种无序分类变量的差异性,并利用生境喜好系数对生境选择性进行分析。采用二元逻辑斯蒂回归模型对15个数值型变量进行分析,确定影响镇海棘螈产卵微生境选择的关键变量。结果显示镇海棘螈繁殖期间对产卵场微生境有明显偏好,通常产卵于朝向水坑、落叶层较厚(5.19±0.18 cm)、坡度较陡(18.64°±1.18°)和土壤含水量较低(33.51%±1.87%)的土壤基质上。此外,在大型遮蔽物中,镇海棘螈偏好选择体积较小的石块和乔木(2,994.63±316.17 cm3)作为遮蔽... 相似文献
176.
动物群落是构成城市绿地生态系统的关键要素,声景作为野生动物重要的生态信息,掌握其时空变化及其影响因素,对于指导城市绿地景观设计与生物多样性保护具有重要意义。本文以Web of Science数据库的核心合集2005–2022年收录的67篇研究文献为对象,综合梳理与分析了城市绿地动物声景的时空模式及其驱动因素。城市绿地动物声景在空间上表现出环境空间梯度和植被空间结构的差异,动物声音多样性随海拔、纬度、城市化程度的降低以及植被类型和高度的增加呈现升高趋势。时间尺度呈现出昼夜、季节和年度变化差异,表现为鸟类在黎明和黄昏合唱、昆虫和两栖动物在夜间鸣叫以及季节性和年度性发声规律等。影响城市动物声景模式的因素主要包括植被、环境、人为干扰和动物自身驱动等。动物声景作为当前声景生态学研究的热点之一,面临大时空尺度演变规律研究不足、动物声景分析有限等挑战,建议未来着重开展多时空尺度变化规律研究、创新动物声景分析方法、定量解析影响因素及其响应机制、建立全球动物声景数据库等。 相似文献
177.
Ailing Jia Yuwen Shi Yuhang Zhang Yuanyuan Diao Baijin Chang Mengcheng Jiang Weipeng Liu Zhidong Qiu Chaomei Fu Ye Qiu 《化学与生物多样性》2023,20(4):e202200949
This study investigated the effect of butanol extract of AS (ASBUE) on atherosclerosis in apolipoprotein E-deficient (ApoE−/−) mice. The mice were administered ASBUE (390 or 130 mg/kg/day) or rosuvastatin (RSV) via oral gavage for eight weeks. In ApoE−/− mice, ASBUE suppressed the abnormal body weight gain and improved serum and liver biochemical indicators. ASBUE remarkably reduced the aortic plaque area, improved liver pathological conditions, and lipid metabolism abnormalities, and altered the intestinal microbiota structure in ApoE−/− mice. In the vascular tissue of ASBUE-treated mice, P-IKKβ, P-NFκB, and P-IκBα levels tended to decrease, while IκB-α increased in high fat-diet-fed atherosclerotic mice. These findings demonstrated the anti-atherosclerotic potential of ASBUE, which is mediated by the interaction between the gut microbiota and lipid metabolism and regulated via the Nuclear Factor-kappa B (NF-κB) pathway. This work paves the groundwork for subsequent studies to develop innovative drugs to treat atherosclerosis. 相似文献
178.
To develop new highly effective anticancer agents derived from naturally occurring stilbene scaffold, in total of 24 indole and indazole-based stilbenes including 17 new compounds were designed according to molecular hybridization strategy and synthesized via Witting reaction. The cytotoxic screening results against human tumor cell lines (K562 cells and MDA-MB-231 cells) showed that indole and indazole-based stilbenes are of great interest for developing anticancer agents as eight derivatives possessed strong antiproliferative activities with IC50 values less than 10 μM, and those synthetic derivatives displayed more higher cytotoxicities against K562 cells than MDA-MB-231 cells. In particular, indole-based stilbene bearing piperidine exhibited the most potent cytotoxicities against both K562 and MDA-MB-231 cells with IC50 values 2.4 μM and 2.18 μM, respectively, along with a remarkable selectivity towards human normal L-02 cells. Together, the results suggested that indole and indazole-based stilbenes are promising anticancer scaffolds worthy of further investigation. 相似文献
179.
Yaomin Luo Xintong Lu Wenrong Ma Yang Xiao Chen Wei Xiaoxia Yuan Yueyue Wu Yunlin Wang Yiman Xiong Xin Yu Xue Wu Siqi He Yayudie Liu Jinjing Wang Qing Wu Hui Zhou Zhen Jiang 《Journal of cellular and molecular medicine》2023,27(22):3591-3600
Long non-coding RNAs (lncRNA) have an extensive role in the progression and chemoresistance of gastric cancer (GC). Deeply study the regulatory role of lncRNAs could provide potential therapeutic targets. The aim of this study is to explore the regulatory role of HOTAIR in the progression and oxaliplatin resistance of GC. The expression of HOTAIR in GC and cell lines were detected by using qRT-PCR. Cell proliferation and apoptosis were analysed by CCK-8, EdU incorporation and flow cytometry. Luciferase reporter assay was used to identify the interaction between HOTAIR and ABCG2 (ATP-binding cassette (ABC) superfamily G member 2, ABCG2) via miR-195-5p. The regulatory functions were verified by using molecular biology experiments. HOTAIR was significantly overexpressed in GC and associated with poor prognosis. Knock-down of HOTAIR inhibited the GC cells proliferation and oxaliplatin resistance, while overexpression of HOTAIR showed opposite functions. Further studies found that HOTAIR acted as a competing endogenous RNA (ceRNA) to absorb miR-195-5p and elevated the expression of ABCG2, which leads to resistance of GC cells to oxaliplatin. Taken together, our findings demonstrated that HOTAIR regulates ABCG2 induced resistance of GC to oxaliplatin through miR-195-5p signalling and illustrate the great potential of developing new therapeutic targets for GC patients. 相似文献
180.
Xuebing Xu Tong Wu Renjie Lin Shengze Zhu Jie Ji Dandan Jin Mengxiang Huang Wenjie Zheng Wenkai Ni Feng Jiang Shihai Xuan Mingbing Xiao 《Journal of cellular and molecular medicine》2023,27(23):3672-3680
The migrasome is a new organelle discovered by Professor Yu Li in 2015. When cells migrate, the membranous organelles that appear at the end of the retraction fibres are migrasomes. With the migration of cells, the retraction fibres which connect migrasomes and cells finally break. The migrasomes detach from the cell and are released into the extracellular space or directly absorbed by the recipient cell. The cytoplasmic contents are first transported to the migrasome and then released from the cell through the migrasome. This release mechanism, which depends on cell migration, is named ‘migracytosis’. The main components of the migrasome are extracellular vesicles after they leave the cell, which are easy to remind people of the current hot topic of exosomes. Exosomes are extracellular vesicles wrapped by the lipid bimolecular layer. With extensive research, exosomes have solved many disease problems. This review summarizes the differences between migrasomes and exosomes in size, composition, property and function, extraction method and regulation mechanism for generation and release. At the same time, it also prospects for the current hotspot of migrasomes, hoping to provide literature support for further research on the generation and release mechanism of migrasomes and their clinical application in the future. 相似文献