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61.
The aberrant features of the genus Daubentonia, such as the superficially rodent-like dentition, the globose and foreshortened brain case, and the filiform third manual digit have long been known. But the current assessment of the genus as lemuriform, and within that group as closest to the indriids, depends upon greater weight being placed upon other characteristics such as the cranial arterial pattern, the molariform teeth, and the developmental characteristics of the dentition. Prior multivariate morphometric studies have shown that though the shoulder structure of Daubentonia is uniquely different from that of all other primates, the structure of its pelvis may not be especially different from that of many relatively non-specialized primates. A large series of studies have been summated here in which many different anatomical regions (shoulder, arm, forearm, forelimb as a whole, pelvis, femur, hindlimb as a whole, forelimb and hindlimb combined, and total bodily proportions including limbs, trunk, and head) have been characterized osteometrically in a wide range of primate genera. The resulting data sets have been studied by discriminant function analyses. The differences that have been found are large enough that it can be confidently asserted that in its postcranial skeleton, Daubentonia is more different from the primates as a whole than is any other primate genus. These differences are big enough that their statistical and biological significance is not at all in doubt, notwithstanding the very small numbers of available specimens of this rare genus. They are so great that functional implications exist though they cannot, in our present state of knowledge of the habits of the genus, be ascribed with any certainty. They are so great indeed, paralleling the enormous differences of Daubentonia from other primates in its dentition, skull and cheiridia, that we may prefer to keep open minds about its taxonomic placement.  相似文献   
62.
The central nervous system of the shiverer mouse is known to be severely deficient in myelin. Animals heterozygous for this autosomal-recessive mutation were crossed, and the myelin proteins were examined in the brains and spinal cords of shiverers and unaffected littermates among the offspring. In the brains and spinal cords of nine of the 14 unaffected littermates examined, the quantities of the myelin basic and proteolipid proteins were lower than normal. Furthermore, in the brains of heterozygotes 33 to ~ 150 days old, the myelin basic and proteolipid proteins were reduced in amount, compared to wild-type controls; the myelin basic protein was also present in subnormal amounts in the spinal cords from heterozygous animals at the ages of 17 to 150 days. More severe reductions in the quantities of the myelin proteins were observed in central nervous system tissue from homozygous shiverer mice, and the quantity of the myelin proteolipid protein in the central nervous system of the shiverer mouse, expressed as a ratio to the control value at each age, underwent a developmental decline. In heterozygotes, as well as shiverers, the peripheral nerves were also deficient in the P1 and Pr proteins, which are the same as the basic proteins in rodent central nervous system myelin. The findings regarding heterozygotes suggest that the defective primary gene product in the shiverer mouse could be the myelin basic protein itself or a protein required for a rate-limiting step in the processing of the myelin basic protein.  相似文献   
63.
The cerebellar hypoplasia induced by hereditary hyperbilirubinemia in the Gunn rat was analyzed neurochemically and immunohistochemically. The antiserum against myelin basic protein was used to visualize the arborization of the fibers in the cerebellum. Arborization was very scarce in the affected lobes of the homozygous (jj) cerebellum. Na,K-ATPase activity did not show significant differences between the jj and the control (Jj) cerebellum. The concentration of norepinephrine in the jj cerebellum was about 1.5 times that of the control. However, the activation ratio of the Na,K-ATPase by norepinephrine and other catecholamines such as dopamine and isoproterenol was about twice as high as the basal activity, and no significant difference was observed between the jj and the Jj cerebella. The glutamic acid decarboxylase activity of the jj cerebellum did not differ significantly from that of the control.  相似文献   
64.
Cytogenetic and electrophoretic analyses on 2n = 28 strains ofAsphodelus cerasiferus strongly suggest that the basic number x = 14 of the genusAsphodelus is of secondary polyploid origin from x = 7.  相似文献   
65.
Sylvie Secretan 《Geobios》1980,13(3):411-433
Are the Eumalacostraca issued from a model of Crustacea which the carapace would have disapeared later on in some of them, and persisted in others, or from one without carapace that some of its decendants would have acquired? In the two instances this ancestor would goes far back, seeing that, already, in the Devonian, Syncarida, Stomatopoda, Phyllocarida and Eocarida were differenciated. With regard to the preliminary survey on a fine material of Syncarida from the Stephanian of the region of Autun, comparisons between two models of Crustaceans from which the cephalon includes only sensorial and gnathal segments, without adjunction of any thoracic metamere, allow to specify the notion of carapace, and to surround the question. The great oldness of the origin of the phyla possessing or not possessing a carapace seems to exclude the hypothesis of a passing over from one model to the other and suggests a representation of the common ancestor which have to be searched in the Cambrian period.  相似文献   
66.
67.
beta-Endorphin: characteristics of binding sites in the rat brain.   总被引:3,自引:0,他引:3  
Stereospecific binding of human β-endorphin to rat membrane preparations is described for the first time using [3H-Tyr27]-βh-endorphin as the ligand. The binding is time dependent and saturable with respect to βh-endorphin with an apparent dissociation constant of 0.3 nM. Sodium ion (100 mM) elevates this value to 2.5 nM but has no effect on the total number of binding sites present in the membrane preparation. The ability of certain β-endorphin analogs, opiate agonists as well as antagonists to inhibit the binding of βh-endorphin, is presented.  相似文献   
68.
A variety of proteins have been studied for their ability to interact and alter the thermotropic properties of phospholipid bilayer membranes as detected by differential scanning calorimeter. The proteins studied included: basic myelin protein (A1 protein), cytochrome c, major apoprotein of myelin proteolipid (N-2 apoprotein), gramicidin A, polylysine, ribonuclease and hemoglobin. The lipids used for the interactions were dipalmitoylphosphatidylcholine and dipalmitoylphosphatidylglycerol. The interactions were grouped in three categories each having very different effects on the phospholipid phase transition from solid to liquid crystalline. The calorimetric studies were also correlated with data from vesicle permeability and monolayer expansion.Ribonuclease and polylysine which exemplify group 1 interactions, show strong dependence on electrostatic binding. Their effects on lipid bilayers include an increase in the enthalpy of transition (ΔH) accompanied by either an increase or no change in the temperature of transition (Tc). In addition, they show minimal effects on vesicle permeability and monolayer expansion. It was concluded that these interactions represent simple surface binding of the protein on the lipid bilayer without penetration into the hydrocarbon region.Cytochrome c and Al protein, which exemplify group 2 interactions, also show a strong dependence on the presence of net negative charges on the lipid bilayers for their binding. In contrast to the first group, however, they induce a drastic decrease in both Tc and ΔH of the lipid phase transition. Furthermore, they induce a large increase in the permeability of vesicles and a substantial expansion in area of closely packed monolayers at the air-water interface. It was concluded that group 2 interactions represent surface binding followed by partial penetration and/or deformation of the bilayer.Group 3 interactions, shown by proteolipid apoprotein and gramicidin A, were primarily non-polar in character, not requiring electrostatic charges and not inhibited by salt and pH changes. They had no appreciable effect on the Tc but did induce a linear decrease in the magnitude of the ΔH, proportional to the percentage of protein by weight. Membranes containing 50% proteolipid protein still exhibited a thermotropic transition with a ΔH one half that of the pure lipid, and only a small diminution of the size of the cooperative unit. It was concluded that in this case the protein was embedded within the bilayer, associating with a limited number of molecules via non-polar interactions, while the rest of the bilayer was largely unperturbed.  相似文献   
69.
Functional morphology of the caudal skeleton in teleostean fishes   总被引:1,自引:0,他引:1  
The basic function of the caudal skeleton in teleostean fishes is to support the caudal fin, but its parts contribute to this function in somewhat different ways. The main axis for this support is the upturned terminal end of the vertebral column, which ends at the base of the uppermost principal rays. The uroneural struts just ahead of this axis provide support for it. The parts of the caudal skeleton behind and below this upturned axis, the hypurals and parhypural, not only support the caudal rays but also provide a means for differential movements between the upper and lower parts of the fin base. This basic caudal skeleton varies with the position of the fish in the sequence of teleosten evolution, the way in which the fish uses its caudal fin, and to some extent with the shape of the fin.  相似文献   
70.
The application of growth factors (GFs) for treating chronic spinal cord injury (SCI) has been shown to promote axonal regeneration and functional recovery. However, direct administration of GFs is limited by their rapid degradation and dilution at the injured sites. Moreover, SCI recovery is a multifactorial process that requires multiple GFs to participate in tissue regeneration. Based on these facts, controlled delivery of multiple growth factors (GFs) to lesion areas is becoming an attractive strategy for repairing SCI. Presently, we developed a GFs‐based delivery system (called GFs‐HP) that consisted of basic fibroblast growth factor (bFGF), nerve growth factor (NGF) and heparin‐poloxamer (HP) hydrogel through self‐assembly mode. This GFs‐HP was a kind of thermosensitive hydrogel that was suitable for orthotopic administration in vivo. Meanwhile, a 3D porous structure of this hydrogel is commonly used to load large amounts of GFs. After single injection of GFs‐HP into the lesioned spinal cord, the sustained release of NGF and bFGF from HP could significantly improve neuronal survival, axon regeneration, reactive astrogliosis suppression and locomotor recovery, when compared with the treatment of free GFs or HP. Moreover, we also revealed that these neuroprotective and neuroregenerative effects of GFs‐HP were likely through activating the phosphatidylinositol 3 kinase and protein kinase B (PI3K/Akt) and mitogen‐activated protein kinase/extracellular signal‐regulated kinase (MAPK/ERK) signalling pathways. Overall, our work will provide an effective therapeutic strategy for SCI repair.  相似文献   
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