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1.
Yimei Li Matt Hall Brian T. Fisher Alix E. Seif Yuan-Shung Huang Rochelle Bagatell Kelly D. Getz Todd A. Alonzo Robert B. Gerbing Lillian Sung Peter C. Adamson Alan Gamis Richard Aplenc 《PloS one》2015,10(11)
Purpose
Clinical trials data from National Cancer Institute (NCI)-funded cooperative oncology group trials could be enhanced by merging with external data sources. Merging without direct patient identifiers would provide additional patient privacy protections. We sought to develop and validate a matching algorithm that uses only indirect patient identifiers.Methods
We merged the data from two Phase III Children’s Oncology Group (COG) trials for de novo acute myeloid leukemia (AML) with the Pediatric Health Information Systems (PHIS). We developed a stepwise matching algorithm that used indirect identifiers including treatment site, gender, birth year, birth month, enrollment year and enrollment month. Results from the stepwise algorithm were compared against the direct merge method that used date of birth, treatment site, and gender. The indirect merge algorithm was developed on AAML0531 and validated on AAML1031.Results
Of 415 patients enrolled on the AAML0531 trial at PHIS centers, we successfully matched 378 (91.1%) patients using the indirect stepwise algorithm. Comparison to the direct merge result suggested that 362 (95.7%) matches identified by the indirect merge algorithm were concordant with the direct merge result. When validating the indirect stepwise algorithm using the AAML1031 trial, we successfully matched 157 out of 165 patients (95.2%) and 150 (95.5%) of the indirectly merged matches were concordant with the directly merged matches.Conclusions
These data demonstrate that patients enrolled on COG clinical trials can be successfully merged with PHIS administrative data using a stepwise algorithm based on indirect patient identifiers. The merged data sets can be used as a platform for comparative effectiveness and cost effectiveness studies. 相似文献2.
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Martin L. Adamson 《Systematic parasitology》1981,3(4):209-216
Summary
Rhigonema infecta (Leidy, 1849) Christie & Cobb, 1927, a member of the family Rhigonematidae sensu Théodoridès, 1965, is redescribed from the diplopod Narceus annularis from Sharbot Lake and Long Point, Ontario, Canada. R. infecta is most similar to R. subtruncatum Dollfus, 1952 but differs from this species in possessing four rather than three post-cloacal papillae in the male. Rhigonematids have been affiliated with members of the order Oxyurida by most authors but study of R. infecta suggests that rhigonematids should be placed in their own order, the Rhigonematida. Members of the order Rhigonematida are characterized by: two spicules in the male; H-shaped excretory system; are round to oval sperms; thick and smooth egg-shell; apparently lacking a uterine layer; and development in the egg involving no moults and resulting in a long, thin, coiled larva. In contrast, oxyuridans have a single spicule, the excretory system is X-shaped, the sperm is comet-shaped and the egg-shell has a prominent striated uterine layer. Development in the egg involves at least one and probably two moults and results in a short, robust, uncoiled larva. ac]19810310 相似文献
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Intact plants and isolated leaves of Zostera capricornii Martens ex Aschers were transferred from daylight to darkness. Substantial amounts of chloropyll a and b continued to accumulate in immature and mature tissue in the same ratio as in the light and were incorporated into chlorophyll-protein complexes in the thylakoids. A small amount of protochlorophyllide also accumulated in immature tissue in the dark. Proplastids and immature chloroplasts continued to develop into mature chloroplasts in the dark in the normal manner but prolamellar bodies, which are a conspicuous feature of immature chloroplasts, took longer to disperse than in the light. Protochlorophyllide accumulation and prolamellar-body formation were not correlated. The results indicate that Zostera has a genetic capacity for dark chlorophyll synthesis which is expressed in immature and mature leaf tissue and enables this plant to continue synthesising chlorophyll and assembling chloroplasts at night.Abbreviations Chl
chlorophyll
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T
o
time of transfer to darkness 相似文献
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V C Broudy J M Harlan J W Adamson 《Journal of immunology (Baltimore, Md. : 1950)》1987,138(12):4298-4302
Tumor necrosis factor-alpha/cachectin (TNF-alpha) and tumor necrosis factor-beta/lymphotoxin (TNF-beta) are inflammatory mediators with similar spectrums of cytotoxic activity against tumors in vitro and in vivo. We compared the effect of purified recombinant human TNF-alpha and TNF-beta on neutrophil adhesion molecule expression and hematopoietic growth factor production by cultured human umbilical vein endothelial cells. Endothelial cells acquired adhesive properties for neutrophils after a 4-hr incubation with as little as 5 U/ml TNF-alpha. TNF-alpha stimulated a dose-dependent increase in endothelial cell adhesiveness for neutrophils, with a maximal effect at 250 U/ml. In contrast, TNF-beta did not enhance endothelial-dependent neutrophil adherence until a concentration of 600 to 1200 U/ml was reached. Endothelial cells cultured for 24 hr with TNF-alpha, 10 to 1,000 U/ml, released hematopoietic colony-stimulating activity. TNF-beta failed to augment growth factor production by endothelial cells at any concentration tested. Inhibitor assays showed that the absence of detectable colony-stimulating activity was not due to direct inhibition of colony growth by TNF-beta or to release of hematopoietic inhibitors by the TNF-beta-stimulated endothelial cells. Purified natural TNF-beta was similar to recombinant TNF-beta in its effect on neutrophil adhesion molecule expression and growth factor production by endothelial cells. These results indicate that the two immunomodulatory proteins TNF-alpha and TNF-beta differ in their effects on a common target tissue. TNF-beta, which retains tumoricidal properties, shows fewer proinflammatory activities on cultured endothelial cells than TNF-alpha in vitro. 相似文献
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