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101.
102.
Xin Xiong Yan Hao Kan Sun Jiaxing Li Xia Li Bibhudatta Mishra Pushpanjali Soppina Chunlai Wu Richard I. Hume Catherine A. Collins 《PLoS biology》2012,10(12)
Axonal degeneration is a hallmark of many neuropathies, neurodegenerative diseases, and injuries. Here, using a Drosophila injury model, we have identified a highly conserved E3 ubiquitin ligase, Highwire (Hiw), as an important regulator of axonal and synaptic degeneration. Mutations in hiw strongly inhibit Wallerian degeneration in multiple neuron types and developmental stages. This new phenotype is mediated by a new downstream target of Hiw: the NAD+ biosynthetic enzyme nicotinamide mononucleotide adenyltransferase (Nmnat), which acts in parallel to a previously known target of Hiw, the Wallenda dileucine zipper kinase (Wnd/DLK) MAPKKK. Hiw promotes a rapid disappearance of Nmnat protein in the distal stump after injury. An increased level of Nmnat protein in hiw mutants is both required and sufficient to inhibit degeneration. Ectopically expressed mouse Nmnat2 is also subject to regulation by Hiw in distal axons and synapses. These findings implicate an important role for endogenous Nmnat and its regulation, via a conserved mechanism, in the initiation of axonal degeneration. Through independent regulation of Wnd/DLK, whose function is required for proximal axons to regenerate, Hiw plays a central role in coordinating both regenerative and degenerative responses to axonal injury. 相似文献
103.
The iab-7 polycomb response element maps to a nucleosome-free region of chromatin and requires both GAGA and pleiohomeotic for silencing activity 总被引:1,自引:0,他引:1 下载免费PDF全文
Mishra RK Mihaly J Barges S Spierer A Karch F Hagstrom K Schweinsberg SE Schedl P 《Molecular and cellular biology》2001,21(4):1311-1318
104.
Sushil Kumar Swati Chaudhary Vishakha Sharma Renu Kumari Raghvendra Kumar Mishra Arvind Kumar Debjani Roy Choudhury Ruchi Jha Anupama Priyadarshini Arun Kumar 《Journal of genetics》2010,89(2):201-211
To understand the role of INSECATUS (INS) gene in pea, the leaf blades of wild-type, ins mutant and seven other genotypes, constructed by recombining ins with uni-tac, af, tl and mfp gene mutations, were quantitatively compared. The ins was inherited as a recessive mutant allele and expressed its phenotype in proximal leaflets of full size leaf blades. In
ins leaflets, the midvein development was arrested in distal domain and a cleft was formed in lamina above this point. There
was change in the identity of ins leaflets such that the intercalary interrupted midvein bore a leaf blade. Such adventitious blades in ins, ins tl and ins tl mfp were like the distal segment of respective main leaf blade. The ins phenotype was not seen in ins af and ins af uni-tac genotypes. There was epistasis of uni-tac over ins. The ins, tl and mfp mutations interacted synergistically to produce highly pronounced ins phenotype in the ins tl mfp triple mutant. The role(s) of INS in leaf-blade organogenesis are: positive regulation of vascular patterning in leaflets, repression of UNI activity in leaflet
primordia for ectopic growth and in leaf-blade primordium for indeterminate growth of rachis, delimitation of proximal leaflet
domain and together with TL and MFP homeostasis for meristematic activity in leaflet primordia. The variant apically bifid
shape of the affected ins leaflets demonstrated that the leaflet shape is dependent on the venation pattern. 相似文献
105.
Maurice Okello Sanjay Mishra Malik Nishonov Vasu Nair 《Bioorganic & medicinal chemistry letters》2013,23(14):4112-4116
While some examples are known of integrase inhibitors that exhibit potent anti-HIV activity, there are very few cases reported of integrase inhibitors that show significant differences in anti-HIV activity that result from distinctions in cis- and trans-configurations as well as enantiomeric stereostructure. We describe here the design and synthesis of two enantiomeric trans-hydroxycyclopentyl carboxamides which exhibit notable difference in anti-HIV activity. This difference is explained through their binding interactions within the active site of the HIV-1 integrase intasome. The more active enantiomer 3 (EC50 25 nM) was relatively stable in human liver microsomes. Kinetic data revealed that its impact on key cytochrome P450 isozymes, as either an inhibitor or an activator, was minor, suggesting a favorable CYP profile. 相似文献
106.
B. Wojciak-Stothard M. Denyer M. Mishra R. A. Brown 《In vitro cellular & developmental biology. Animal》1997,33(2):110-117
Summary This study examined the behavior of rat tendon fibroblasts, baby hamster kidney fibroblasts, macrophage-like P388D1 cells,
and neurons from rat dorsal root ganglia, cultured on fibronectin strands 0.2–5 μm in diameter. We investigated cell spreading,
orientation, formation of focal contacts, the speed of cell movement, and the speed of neurite outgrowth in cells cultured
on fibronectin strands, glass covered with fibronectin, and plain, nontreated glass. Fibronectin strands significantly promoted
cell spreading and caused a marked alignment of all kinds of cells to the direction of the fiber. The fibers caused the alignment
of actin filaments in fibroblasts and focal contacts in fibroblasts and macrophages and increased polymerization of F-actin
in cells. Fibronectin fibers also increased the speed and persistence of cell movement and the rate of neurite outgrowth.
Macrophages grown on fibronectin fibers produced numerous actin-rich microspikes and adopted a polarized, migratory phenotype.
These findings indicate that fibronectin strands, resembling natural components of the extracellular matrix, are more effective
in activating various types of cells than two-dimensional, fibronectin-covered substrata. The results also confirm the suitability
of the three-dimensionally oriented fibronectin form for use in clinical practice. 相似文献
107.
108.
A regulatory role of Wnt signaling pathway in the hematopoietic differentiation of murine embryonic stem cells 总被引:1,自引:0,他引:1
Feng Z Srivastava AS Mishra R Carrier E 《Biochemical and biophysical research communications》2004,324(4):1333-1339
One of the most important issues in stem cell research is to understand the regulatory mechanisms responsible for their differentiation. An extensive understanding of mechanism underlying the process of differentiation is crucial in order to prompt stem cells to perform a particular function after differentiation. To elucidate the molecular mechanisms responsible for the hematopoietic differentiation of embryonic stem cells (ESCs), we investigated murine ES cells for the presence of hematopoietic lineage markers as well as Wnt signaling pathway during treatments with different cytokines alone or in combination with another. Here we report that Wnt/beta-catenin signaling is down-regulated in hematopoietic differentiation of murine ES cells. We also found that differentiation induced by the interleukin-3, interleukin-6, and erythropoietin combinations resulted in high expression of CD3e, CD11b, CD45R/B220, Ly-6G, and TER-119 in differentiated ES cells. A high expression of beta-catenin was observed in two undifferentiated ES cell lines. Gene and protein expression analysis revealed that the members downstream of Wnt in this signaling pathway including beta-catenin, GSK-3beta, Axin, and TCF4 were significantly down-regulated as ES cells differentiated into hematopoietic progenitors. Our results show that the Wnt/beta-catenin signaling pathway plays a role in the hematopoietic differentiation of murine ESCs and also may support beta-catenin as a crucial factor in the maintenance of ES cells in their undifferentiated state. 相似文献
109.
Ismail M. Fareez Siong Meng Lim Nurul Aida Ashyqin Zulkefli Rakesh K. Mishra Kalavathy Ramasamy 《Probiotics and antimicrobial proteins》2018,10(3):543-557
The susceptibility of probiotics to low pH and high temperature has limited their use as nutraceuticals. In this study, enhanced protection of probiotics via microencapsulation was achieved. Lactobacillus plantarum LAB12 were immobilised within polymeric matrix comprised of alginate (Alg) with supplementation of cellulose derivatives (methylcellulose (MC), sodium carboxymethyl cellulose (NaCMC) or hydroxypropyl methylcellulose (HPMC)). L. plantarum LAB12 encapsulated in Alg-HPMC(1.0) and Alg-MC(1.0) elicited improved survivability (91%) in simulated gastric conditions and facilitated maximal release (~100%) in simulated intestinal condition. Alg-HPMC(1.0) and Alg-MC(1.0) significantly reduced (P < 0.05) the viability loss of LAB12 (viability loss <7%) when compared to Alg alone (viability loss <13%) under extreme temperatures (75 and 90 °C). Four-week storage of encapsulated LAB12 at 4 °C yielded viable counts >7 log CFU g?1. Alg-MC and Alg-HPMC improved the survival of LAB12 against simulated gastric condition (9.24 and 9.55 log CFU g?1, respectively), temperature up to 90 °C (9.54 and 9.86 log CFU g?1, respectively) and 4-week of storage at 4 °C (8.61 and 9.23 log CFU g?1, respectively) with sustained release of probiotic in intestinal condition (>9 log CFU g?1). These findings strongly suggest the potential of cellulose derivatives supplemented Alg bead as protective micro-transport for probiotic strains. They can be safely incorporated into new functional food or nutraceutical products. 相似文献
110.