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71.
Identification of Cytokinins of Root Nodules of the Garden Pea, Pisum sativum L 总被引:4,自引:3,他引:1
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Five cytokinin activities which induced soybean callus proliferation were detected in ethanol extracts of root nodules of the garden pea (Pisum sativum L., cv. Little Marvel). The most active factors among them were identified as zeatin and its riboside on the basis of their mobility on thin layer chromatography in three solvent systems. Smaller activities of zeatin ribotide, isopentenyladenine and its riboside were also detected. Cytokinin activity gradually decreased with the cultivation period, but no qualitative change in the active compounds was found. 相似文献
72.
Romeu Cardoso Guimarães 《Origins of life and evolution of the biosphere》2011,41(4):357-371
An investigation of the biosynthesis pathways producing glycine and serine was necessary to clarify an apparent inconsistency
between the self-referential model (SRM) for the formation of the genetic code and the model of coevolution of encodings and
of amino acid biosynthesis routes. According to the SRM proposal, glycine was the first amino acid encoded, followed by serine.
The coevolution model does not state precisely which the first encodings were, only presenting a list of about ten early assignments
including the derivation of glycine from serine—this being derived from the glycolysis intermediate glycerate, which reverses
the order proposed by the self-referential model. Our search identified the glycine-serine pathway of syntheses based on one-carbon
sources, involving activities of the glycine decarboxylase complex and its associated serine hydroxymethyltransferase, which
is consistent with the order proposed by the self-referential model and supports its rationale for the origin of the genetic
code: protein synthesis was developed inside an early metabolic system, serving the function of a sink of amino acids; the
first peptides were glycine-rich and fit for the function of building the early ribonucleoproteins; glycine consumption in
proteins drove the fixation of the glycine-serine pathway. 相似文献
73.
Catarina Macedo-Silva Vera Miranda-Gonalves Ana Lameirinhas Joana Lencart Alexandre Pereira Joo Lobo Rita Guimares Ana Teresa Martins Rui Henrique Isabel Bravo Carmen Jernimo 《Cell death & disease》2020,11(12)
Esophageal squamous cell carcinoma (ESCC), the most frequent esophageal cancer (EC) subtype, entails dismal prognosis. Hypoxia, a common feature of advanced ESCC, is involved in resistance to radiotherapy (RT). RT response in hypoxia might be modulated through epigenetic mechanisms, constituting novel targets to improve patient outcome. Post-translational methylation in histone can be partially modulated by histone lysine demethylases (KDMs), which specifically removes methyl groups in certain lysine residues. KDMs deregulation was associated with tumor aggressiveness and therapy failure. Thus, we sought to unveil the role of Jumonji C domain histone lysine demethylases (JmjC-KDMs) in ESCC radioresistance acquisition. The effectiveness of RT upon ESCC cells under hypoxic conditions was assessed by colony formation assay. KDM3A/KDM6B expression, and respective H3K9me2 and H3K27me3 target marks, were evaluated by RT-qPCR, Western blot, and immunofluorescence. Effect of JmjC-KDM inhibitor IOX1, as well as KDM3A knockdown, in in vitro functional cell behavior and RT response was assessed in ESCC under hypoxic conditions. In vivo effect of combined IOX1 and ionizing radiation treatment was evaluated in ESCC cells using CAM assay. KDM3A, KDM6B, HIF-1α, and CAIX immunoexpression was assessed in primary ESCC and normal esophagus. Herein, we found that hypoxia promoted ESCC radioresistance through increased KDM3A/KDM6B expression, enhancing cell survival and migration and decreasing DNA damage and apoptosis, in vitro. Exposure to IOX1 reverted these features, increasing ESCC radiosensitivity and decreasing ESCC microtumors size, in vivo. KDM3A was upregulated in ESCC tissues compared to the normal esophagus, associating and colocalizing with hypoxic markers (HIF-1α and CAIX). Therefore, KDM3A upregulation in ESCC cell lines and primary tumors associated with hypoxia, playing a critical role in EC aggressiveness and radioresistance. KDM3A targeting, concomitant with conventional RT, constitutes a promising strategy to improve ESCC patients’ survival.Subject terms: Predictive markers, Cancer 相似文献
74.
G Henderson A Duncan M Kromberg J Roberts F Sim G Vafidis 《BMJ (Clinical research ed.)》1990,300(6731):1076
75.
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77.
Rezende Renan de Souza Kroth Nádia Capitanio Bruna Maria Lima-Rezende Cássia Alves Cassol Angélica Soligo Cozzer Gilberto Dinis Baldissera Ronei Breaux Jennifer Ann Albeny-Simões Daniel 《Limnology》2020,21(3):275-285
Limnology - Aquatic macroinvertebrate communities are dependent on intrinsic environmental characteristics and biological interactions in microhabitat systems. We investigated the... 相似文献
78.
Acetylation changes tau interactome to degrade tau in Alzheimer’s disease animal and organoid models
Heesun Choi Haeng Jun Kim Jinhee Yang Sehyun Chae Wonik Lee Sunwoo Chung Jisoo Kim Hyunjung Choi Hyeseung Song Chang Kon Lee Jae Hyun Jun Yong Jae Lee Kyunghyeon Lee Semi Kim Hye‐ri Sim Young Il Choi Keun Ho Ryu Jong‐Chan Park Dongjoon Lee Sun‐Ho Han Daehee Hwang Jangbeen Kyung Inhee Mook‐Jung 《Aging cell》2020,19(1)
Alzheimer's disease (AD) is an age‐related neurodegenerative disease. The most common pathological hallmarks are amyloid plaques and neurofibrillary tangles in the brain. In the brains of patients with AD, pathological tau is abnormally accumulated causing neuronal loss, synaptic dysfunction, and cognitive decline. We found a histone deacetylase 6 (HDAC6) inhibitor, CKD‐504, changed the tau interactome dramatically to degrade pathological tau not only in AD animal model (ADLPAPT) brains containing both amyloid plaques and neurofibrillary tangles but also in AD patient‐derived brain organoids. Acetylated tau recruited chaperone proteins such as Hsp40, Hsp70, and Hsp110, and this complex bound to novel tau E3 ligases including UBE2O and RNF14. This complex degraded pathological tau through proteasomal pathway. We also identified the responsible acetylation sites on tau. These dramatic tau‐interactome changes may result in tau degradation, leading to the recovery of synaptic pathology and cognitive decline in the ADLPAPT mice. 相似文献
79.
Ingrid S. Garcia Susana A. Teixeira Karine A. Costa Daniele B. D. Marques Gustavo de A. Rodrigues Thaís C. Costa Jos D. Guimares Pamela I. Otto Alysson Saraiva Adriana M. G. Ibelli Maurício E. Canto Haniel C. de Oliveira Mnica C. Ledur Jane de O. Peixoto Simone E. F. Guimares 《Molecular reproduction and development》2020,87(7):819-834
80.
Juliana S. Maldarine Bruno D. A. Sanches Vitria A. Santos gata S. Cabral Maria L. D. Lima Carolina M. Bedolo Marília F. Calmon Paula Rahal Rejane M. Ges Patricia S. L. Vilamaior Sebastio R. Taboga 《Cell biology international》2020,44(6):1341-1352
The development and maintenance of prostate function depend on a fine balance between oestrogen and androgen levels. Finasteride inhibits 5α‐reductase, which is responsible for the conversion of testosterone into its most active form, dihydrotestosterone. Enzymes that metabolize these hormones have a highly relevant role in both the normal prostate metabolism and in the occurrence of pathological conditions. There are few studies on the impact of finasteride on male prostate development and fewer studies on the female prostate and possible intersexual differences. Therefore, we treated male and female gerbils from 7 to 14 days in postnatal life with a high dose of finasteride (500 μg/kg/day); the prostate complexes were then removed and submitted to immunohistochemistry, immunofluorescence and three‐dimensional reconstruction. In addition, hormonal serum dosages were administered. Treatment with finasteride resulted in an increased thickness of the periductal smooth musculature in the prostate of both male and female gerbils, such as well as a reduction in the thickness of developing prostate alveoli in both sexes. In addition, intersexual differences were observed as increased epithelial proliferation and decreases in the number of developing alveoli in females. Together, the data indicate that postnatal exposure to finasteride causes greater changes in the female gerbil prostate than in the male. 相似文献