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101.
Sarva Mangala Praveena Siti Shapor Siraj Ahmad Zaharin Aris 《Reviews in Environmental Science and Biotechnology》2012,11(1):27-39
Coral reefs in Malaysia are about 4,006 km2 with over 550 species contributed to nation’s economy. Coral reefs studies and threats in Malaysia have been reviewed briefly.
Perspectives are addressed as coral reefs studies, threats, gaps and future studies. Coral reefs in Malaysia are being damaged
at an increasing rate where it faces natural and anthropogenic stresses. Excellent summaries are available in terms of coral
reefs cover throughout Malaysia however scarce in terms of qualitative, quantitative and biogeographical data. There are also
limited studies on heavy metals concentration in corals skeleton studies. Poor to fair conditions of coral reefs in Peninsular
Malaysia is due to increases of sedimentation and tourism impacts. Overfishing and fish blasting were main threats of coral
reefs damage in Sabah. In Sarawak, coral reefs are threatened by high sedimentation and sand mining. The 1998–1999 bleaching
event also affected coral reefs in Malaysia due to climate change. Gaps in coral reefs studies can be completed by continuous
collaborations between local and international researchers as well as research by local universities. Economic valuation,
policy analysis and community participation are directions in future coral reefs studies in Malaysia. Future studies are to
understand effects of management on coral reefs health and impact of pollution on coral reefs growth with a standard coral
reefs methodology. Established legal systems to reduce threats received by coral reefs are also need to be introduced. Role
of science-driven management with community participation and media mass are also gaps to be highlighted in future studies. 相似文献
102.
Pliatsika P Antoniou A Alexandrou A Panoulis C Kouskouni E Augoulea A Dendrinos S Aravantinos L Creatsa M Lambrinoudaki I 《Gynecological endocrinology : the official journal of the International Society of Gynecological Endocrinology》2012,28(8):655-660
Contradictory results have been reported regarding a relationship between serum lipid levels and bone mineral density. The purpose of this study was to further investigate a possible relationship between those parameters in Greek postmenopausal women. A total of 591 patients followed at a tertiary hospital were examined for seven different lipid factors in relation to dual-emission X-ray absorptiometry measurements at the lumbar spine. Lipoprotein-a was the only lipid measurement that univariately showed an almost significant trend of association with bone mass category (analysis of variance [ANOVA] p value 0.062 for Ln(Lipoprotein-a)). In multiple regression, it was noted that a non-significant negative trend of association of high density lipoprotein (HDL) cholesterol and Apolipoprotein AI with lumbar T-score (p value 0.058 and 0.075, respectively). In age subgroup analysis, Lipoprotein-a and Ln(Lipoprotein-a) presented a negative correlation with lumbar T-score for women with age ≥ 53 years (p value 0.043 and 0.070, respectively), while a negative correlation of HDL and Apolipoprotein AI levels with lumbar T-score remained in women with age < 53 years (p value 0.039 and 0.052, respectively). The findings do not support a strong relationship between lipid levels and bone mass measurements. 相似文献
103.
Measurement of the degree of asymmetry in phylogenetic trees is important because a tree's shape reflects the process by which it has grown. For example, highly asymmetric trees are evidence that species have had different potential for diversification. Of the tree shape measures in the literature, that proposed by Fusco & Cronk (J. theor. Biol.175, 235-243) appears to be particularly useful, because it does not require fully-resolved trees whose terminals are of equal taxonomic rank. The value of the asymmetry or imbalance at a node is intended to be independent of the number of species ultimately descended from the node. In this paper, however, we point out that the value does depend upon species number. We propose two modifications that remove the dependency and so increase the measure's usefulness. We illustrate the use of the modified measures, which are implemented in a freely-available program, MESA. 相似文献
104.
105.
The structure of solutions to a simple spatially dependent population model involving growth and death is investigated. Two
forms of motility of the population are considered: (1) random motion only modeled by a Fickian law, and (2) a directed component
of motion (chemotaxis), included in addition to the random motion. Under certain growth conditions a traveling wave of constant
speed is approached. This speed can be increased by the addition of the chemotaxis with a corresponding increase in the asymptotic
population. Development of initial conditions into a wave is illustrated numerically. 相似文献
106.
107.
Stephenie Paine-Saunders Beth L Viviano Aris N Economides Scott Saunders 《The Journal of biological chemistry》2002,277(3):2089-2096
Bone morphogenetic proteins (BMPs) are expressed broadly and regulate a diverse array of developmental events in vivo. Essential to many of these functions is the establishment of activity gradients of BMP, which provide positional information that influences cell fates. Secreted polypeptides, such as Noggin, bind BMPs and inhibit their function by preventing interaction with receptors on the cell surface. These BMP antagonists are assumed to be diffusible and therefore potentially important in the establishment of BMP activity gradients in vivo. Nothing is known, however, about the potential interactions between Noggin and components of the cell surface or extracellular matrix that might limit its diffusion. We have found that Noggin binds strongly to heparin in vitro, and to heparan sulfate proteoglycans on the surface of cultured cells. Noggin is detected only on the surface of cells that express heparan sulfate, can be specifically displaced from cells by heparin, and can be directly cross-linked to a cell surface proteoglycan in culture. Heparan sulfate-bound Noggin remains functional and can bind BMP4 at the plasma membrane. A Noggin mutant with a deletion in a putative heparin binding domain has reduced binding to heparin and does not bind to the cell surface but has preserved BMP binding and antagonist functions. Our results imply that interactions between Noggin and heparan sulfate proteoglycans in vivo regulate diffusion and therefore the formation of gradients of BMP activity. 相似文献
108.
109.
Tpl-2/Cot and COX-2 in breast cancer 总被引:1,自引:0,他引:1
Krcova Z Ehrmann J Krejci V Eliopoulos A Kolar Z 《Biomedical papers of the Medical Faculty of the University Palacky, Olomouc, Czechoslovakia》2008,152(1):21-25
Background: Breast cancer is the most common cancer in women worldwide and although mortality (129 000/year) stagnates, incidence (370 000/year) is increasing. In addition to histological type, grade, stage, hormonal and c-erbB2 status there is therefore a strong need for new and reliable prognostic and predictive factors. Methods and results: This minireview focuses on two potential prognostic and predictive candidates Tpl2/Cot and COX-2 and summarise information about them. Conclusion: Tumor progression locus 2 (Tpl2/Cot) is a serine/threonine protein kinase belonging to the family of MAP3 kinases. Activated Tpl2/Cot leads to induction of ERK1/2, JNK, NF-kappaB and p38MAPK pathways. The first study on Tpl2/Cot mRNA in breast cancer showed its increase in 40 % of cases of breast cancer but no available data exist on protein expression. Cyclo-oxygenase 2 (COX-2) is inducible by growth and inflammatory factors and contributes to the development of various tumours. Expression of COX-2 in breast cancer varied from 5-100 % in reviewed papers with significantly higher values in poorly differentiated tumours. Tpl2/Cot and COX-2 have their importance in different intracellular pathways and some of these are involved in cancer development. Briefly, the results from recent studies suggest that Tpl2/Cot and COX-2 could be prognostic factors in breast cancer. 相似文献
110.
Katsoulakou E Tiliakos M Papaefstathiou G Terzis A Raptopoulou C Geromichalos G Papazisis K Papi R Pantazaki A Kyriakidis D Cordopatis P Manessi-Zoupa E 《Journal of inorganic biochemistry》2008,102(7):1397-1405
Two new organotin(IV) complexes with dianionic dipeptides containing the α-aminoisobutyryl residue (Aib) as ligands are described. The solid complexes [(n-Bu)2Sn(H−1LA)] · 2MeOH (1 · 2MeOH) (LAH = H-Aib-L-Leu-OH) and [(n-Bu)2Sn(H−1LB)] · MeOH (2 · MeOH) (LBH = H-Aib-L-Ala-OH) have been isolated and characterized by single-crystal X-ray crystallography and spectroscopic techniques (H−1L2− is the dianionic form of the corresponding dipeptide). Complexes 1 · 2MeOH and 2 · MeOH are monomeric with similar molecular structures. The doubly deprotonated dipeptide behaves as a N(amino), N(peptide), O(carboxylate) ligand and binds to the SnIV atom. The five-coordinate metal ion has a distorted trigonal bipyramidal geometry. A different network of intermolecular hydrogen bonds in each compound results in very dissimilar supramolecular features. The IR, far-IR, Raman and 119Sn NMR data are discussed in terms of the nature of bonding and known structures. The antibacterial and antiproliferative activities as well as the effect of the new compounds on pDNA were examined. Complexes 1 and 2 are active against the gram-positive bacteria Bacillus subtilis and Bacillus cereus. The IC50 values reveal that the two compounds express promising cytotoxic activity in vitro against a series of cell lines. 相似文献