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11.
Influence of Surfactants on Lipase Fat Digestion in a Model Gastro-intestinal System 总被引:1,自引:0,他引:1
Pedro M. Reis Thomas W. Raab Jean Y. Chuat Martin E. Leser Reinhard Miller Heribert J. Watzke Krister Holmberg 《Food biophysics》2008,3(4):370-381
In the present study, we use a model gastro-intestinal system to study the influence of different food-grade surface-active
molecules (Sn-2 monopalmitin, β-lactoglobulin, or lysophosphatodylcholine) on lipase activity. The interfacial activity of
lipase and surfactants are assessed with the pendant drop technique, a commonly used tensiometry instrument. A mathematical
model is adopted which enables quantitative determination of the composition of the water–oil interface as a function of bulk
surfactant concentration in the water–oil mixtures. Our results show a decrease in gastric lipolysis when interfacially active
molecules are incorporated into a food matrix. However, only the Sn-2 monopalmitin caused a systematic decrease in triglyceride
hydrolysis throughout the gastro-intestinal tract. This effect is most likely due to exclusion of both lipase and triglyceride
from the water–oil interface together with a probable saturation of the solubilization capacity of bile with monoglycerides.
Addition of β-lactoglobulin or lysophopholipids increased the hydrolysis of fat after the gastric phase. These results can
be attributed to an increasing interfacial area with lipase and substrate present at the interface. Otherwise, β-lactoglobulin,
or lysophopholipids reduced fat hydrolysis in the stomach. From the mathematical modeling of the interface composition, we
can conclude that Sn-2 monopalmitin can desorb lipase from the interface, which, together with exclusion of substrate from
the interface, explains the gradually decreased triglyceride hydrolysis that occurs during the digestion. Our results provide
a biophysics approach on lipolysis that can bring new insights into the problem of fat uptake. 相似文献
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Corinna Stefanie Weber Katrina Hainz Tekalign Deressa Helen Strandt Douglas Florindo Pinheiro Roberta Mittermair Jennifer Pizarro Pesado Josef Thalhamer Peter Hammerl Angelika Stoecklinger 《PloS one》2015,10(6)
The skin accommodates multiple dendritic cell (DC) subsets with remarkable functional diversity. Immune reactions are initiated and modulated by the triggering of DC by pathogen-associated or endogenous danger signals. In contrast to these processes, the influence of intrinsic features of protein antigens on the strength and type of immune responses is much less understood. Therefore, we investigated the involvement of distinct DC subsets in immune reactions against two structurally different model antigens, E. coli beta-galactosidase (betaGal) and chicken ovalbumin (OVA) under otherwise identical conditions. After epicutaneous administration of the respective DNA vaccines with a gene gun, wild type mice induced robust immune responses against both antigens. However, ablation of langerin+ DC almost abolished IgG1 and cytotoxic T lymphocytes against betaGal but enhanced T cell and antibody responses against OVA. We identified epidermal Langerhans cells (LC) as the subset responsible for the suppression of anti-OVA reactions and found regulatory T cells critically involved in this process. In contrast, reactions against betaGal were not affected by the selective elimination of LC, indicating that this antigen required a different langerin+ DC subset. The opposing findings obtained with OVA and betaGal vaccines were not due to immune-modulating activities of either the plasmid DNA or the antigen gene products, nor did the differential cellular localization, size or dose of the two proteins account for the opposite effects. Thus, skin-borne protein antigens may be differentially handled by distinct DC subsets, and, in this way, intrinsic features of the antigen can participate in immune modulation. 相似文献
15.
Gerhard Pichler Po-Yin Cheung Corinna Binder Megan O’Reilly Bernhard Schwaberger Khalid Aziz Berndt Urlesberger Georg M. Schm?lzer 《PloS one》2014,9(12)
Objective
To describe temporal changes in systolic, diastolic, and mean blood pressure (SBP, DBP, and MBP, respectively) in term and preterm infants immediately after birth.Methods
Prospective observational two-center study. In term infants SBP, DBP, and MBP were assessed non-invasively every minute for the first 15 minutes, and in preterm infants every minute for the first 15 minutes, as well as at 20, 25, 30, 45, and 60 minutes after birth. Regression analyses were performed by gender and respiratory support in all neonates; and by mode of delivery, cord clamping time, and development of ultrasound-detected brain injury in preterm neonates.Results
Term infants (n = 54) had a mean (SD) birth weight of 3298 (442) g and gestational age of 38 (1) weeks, and preterm infants (n = 94) weighed 1340 (672) g and were 30 (3) weeks gestation. Term infants’ SBP, DBP and MBP within the first 15 minutes after birth were independent of gender or respiratory support. Linear mixed regression analysis showed that preterm infants, who were female, born vaginally, had delayed cord clamping and did not require positive pressure ventilation nor develop periventricular injury or ventriculomegaly, had significantly higher SBP, DBP, and MBP at some measurement points within the first hour after birth.Conclusions
We present novel reference ranges of BP immediately after birth in a cohort of term and preterm neonates. They may aid in optimization of cardiovascular support during early transition at all gestations. 相似文献16.
Risky Courtship: Background Contrast,Ornamentation, and Display Behavior of Wolf Spiders Affect Visual Detection by Toad Predators 下载免费PDF全文
David L. Clark Corinna Kizer Zeeff Adam Karson J. Andrew Roberts George W. Uetz 《Ethology : formerly Zeitschrift fur Tierpsychologie》2016,122(5):364-375
Males that search widely for females and perform conspicuous courtship displays run a high risk of being detected by their predators. Therefore, gains in reproductive success might be offset by increased mortality due to predation. Male brush‐legged wolf spiders (Schizocosa ocreata) with larger decorative traits (foreleg tufts) are preferred by females as mates, but are more readily detected by predators. However, predation risk may also be influenced by the interaction between components of signals and the environment in which signaling occurs. Courting male spiders were readily accepted as prey by a sympatric predator, the American toad (Anaxyrus americanus). We used video playback to tease apart the interactive effect between visual signals and the signaling environment on the ability of toads to detect courting spiders as a function of distance, background contrast, the presence or absence of male foreleg tufts, and behavioral activity. The response of toads to video sequences of male spiders was similar to their response to live male spiders. Toad response varied over distance toward spiders displayed against high contrast (sunny) vs. low contrast (shaded) backgrounds. Beyond 30 cm, more toads detected courting male spiders against light, ‘sunny’ backgrounds and detected them faster when compared to the same spider stimulus against darker, ‘shady’ backgrounds. In choice tests, toads oriented more often toward courting males with leg tufts than those without. Toad responses also varied with male spider behavior in that only videos of moving males were attacked. Latency to orient and detection by toads was significantly greater for walking males than courting males, and this effect was most evident at distances between 30 cm and 50 cm. Results supported that courting wolf spiders are at significant risk of predation by visually acute predators. Distance, background contrast, and the presence of foreleg decorations influence detection probability. Thus, the same complex visual signals that make males conspicuous and are preferred by females can make males more vulnerable as prey to toads. 相似文献
17.
Programmed -1 ribosomal frameshift (-1 PRF) allows for alternative reading frames within one mRNA. First found in several viruses, it is now believed to exist in all kingdoms of life. Strong stimulators for -1 PRF are a heptameric slippery site and an RNA pseudoknot. Here, we present a new algorithm KnotInFrame, for the automatic detection of -1 PRF signals from genomic sequences. It finds the frameshifting stimulators by means of a specialized RNA-pseudoknot folding program, fast enough for genome-wide analyses. Evaluations on known -1 PRF signals demonstrate a high sensitivity. 相似文献
18.
Behar DM Metspalu E Kivisild T Achilli A Hadid Y Tzur S Pereira L Amorim A Quintana-Murci L Majamaa K Herrnstadt C Howell N Balanovsky O Kutuev I Pshenichnov A Gurwitz D Bonne-Tamir B Torroni A Villems R Skorecki K 《American journal of human genetics》2006,78(3):487-497
Both the extent and location of the maternal ancestral deme from which the Ashkenazi Jewry arose remain obscure. Here, using complete sequences of the maternally inherited mitochondrial DNA (mtDNA), we show that close to one-half of Ashkenazi Jews, estimated at 8,000,000 people, can be traced back to only 4 women carrying distinct mtDNAs that are virtually absent in other populations, with the important exception of low frequencies among non-Ashkenazi Jews. We conclude that four founding mtDNAs, likely of Near Eastern ancestry, underwent major expansion(s) in Europe within the past millennium. 相似文献
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Kalscheuer VM FitzPatrick D Tommerup N Bugge M Niebuhr E Neumann LM Tzschach A Shoichet SA Menzel C Erdogan F Arkesteijn G Ropers HH Ullmann R 《Human genetics》2007,121(3-4):501-509
We report on three unrelated mentally disabled patients, each carrying a de novo balanced translocation that truncates the
autism susceptibility candidate 2 (AUTS2) gene at 7q11.2. One of our patients shows relatively mild mental retardation; the other two display more profound disorders.
One patient is also physically disabled, exhibiting urogenital and limb malformations in addition to severe mental retardation.
The function of AUTS2 is presently unknown, but it has been shown to be disrupted in monozygotic twins with autism and mental retardation, both
carrying a translocation t(7;20)(q11.2;p11.2) (de la Barra et al. in Rev Chil Pediatr 57:549–554, 1986; Sultana et al. in Genomics 80:129–134, 2002). Given the overlap of this autism/mental retardation (MR) phenotype and the MR-associated disorders in our patients, together
with the fact that mapping of the additional autosomal breakpoints involved did not disclose obvious candidate disease genes,
we ascertain with this study that AUTS2 mutations are clearly linked to autosomal dominant mental retardation. 相似文献