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排序方式: 共有163条查询结果,搜索用时 15 毫秒
1.
Cholera toxin blocks glucagon-mediated inhibition of the liver plasma membrane (Ca2+-Mg2+)-ATPase 总被引:2,自引:0,他引:2
S Lotersztajn C Pavoine A Mallat D Stengel P A Insel F Pecker 《The Journal of biological chemistry》1987,262(7):3114-3117
We have previously shown that liver plasma membrane (Ca2+-Mg2+)-ATPase activity is inhibited by glucagon. To investigate the possible involvement of a GTP-binding (G) protein in this regulation, we have examined the effects of pertussis toxin and cholera toxin on inhibition of (Ca2+-Mg2+)-ATPase by glucagon. Treatment of liver plasma membranes with pertussis toxin did not affect the sensitivity of (Ca2+-Mg2+)-ATPase to the hormone. In contrast, treatment of plasma membranes or prior injection of animals with cholera toxin prevented inhibition of the (Ca2+-Mg2+)-ATPase by glucagon. Even though adenylate cyclase activity was increased by cholera toxin treatment, addition of cyclic AMP did not mimic the effect of cholera toxin in blocking glucagon-mediated inhibition of (Ca2+-Mg2+)-ATPase activity. These data suggest that a cholera toxin-sensitive protein, perhaps Gs or a Gs-like protein, is involved in the regulation of liver (Ca2+-Mg2+)-ATPase activity. The results emphasize the possible role of Gs-like proteins in regulation of enzymes other than adenylate cyclase and suggest that the study of (Ca2+-Mg2+)-ATPase may provide a useful enzymatic system to examine such regulation. 相似文献
2.
D. Stengel J. Parma M. -H. Gannagé N. Roeckel M. -G. Mattei R. Barouki J. Hanoune 《Human genetics》1992,90(1-2):126-130
Summary Recently, we characterized a cDNA clone that encodes a human brain adenylyl cyclase (HBAC1). In the present study, we identified a second population of mRNA suspected to encode a new brain adenylyl cyclase (HBAC2). The amino acid sequence of HBAC2 displays significant homology with HBAC1 in the highly conserved adenylyl cyclase domain (250 aminio acids), found in the 3 cytoplasmic domain of all mammalian adenylyl cyclases. However, outside this domain, the homology is extremely low, suggesting that the corresponding mRNA originates from a different gene. We report here the first chromosomal localization of the adenylyl cyclase genes determined by in situ hybridization of human metaphase chromosomal spreads using human brain cDNA probes specific for each mRNA. The probe corresponding to HBAC1 exhibited a strong specific signal on chromosome 8q24, with a major peak in the band q24.2. In contrast, the HBAC2 probe hybridized to chromosome 5p15, with a major peak in the band p15.3. The two cDNAs hybridized at the two loci without any cross reactivity. Thus, in human brain, a heterogeneous population of adenylyl cyclase mRNAs is expressed, and the corresponding genes might be under the control of independent regulatory mechanisms.Abbreviations C
catalytic part of adenylyl cyclase
- BBAC
bovine brain
- HBAC
human brain
- ROAC
rat olfactory
- RLAC
rat liver
- RTAC
rat testis adenylyl cyclase
- G
guanine nucleotide GTP binding protein (s, stimulatory; i, inhibitory) 相似文献
3.
Michael J. Sofia William T. Jackson Davis L. SaussyJr. Steven A. Silbaugh Larry L. Froelich Sandra L. Cockerham Peter W. Stengel 《Bioorganic & medicinal chemistry letters》1992,2(12)
A series of
-alkoxyphenols containing a tetrazole acid sidechain have been prepared as antagonists of leukotriene B4 receptors. These compounds were tested as receptor antagonists of human neutrophil and guinea pig lung membrane leukotriene B4 receptors. Compounds in this series were found to be up to 18-fold more potent than LY255283. These results indicate that the acyl group of the 1,2,4,5 substituted hydroxyacetophenone class of LTB4 antagonists is not critical to antagonist potency. 相似文献
4.
Peter W. Stengel Penelope A. Pechous Steven A. Silbaugh 《Prostaglandins & other lipid mediators》1987,33(4)
Exposure of conscious guinea pigs to A23187 aerosol produced a concentration-related increase of excised lung gas volume (ELGV),
.
., postmortem pulmonary gas trapping. Measurements of ELGV were highly correlated with
measurements of dynamic compliance (Cdyn) and total pulmonary resistance (RL) and were used as an indication of
airway obstruction. We pretreated guinea pigs intravenously with the following drugs: atropine; LY163443, a selective LTD4/E4 antagonist; indomethacin; propranolol; and pyrilamine. The guinea pigs were exposed for 8 minutes to the A23187 aerosol, and ELGV measurements were then made. Atropine or pyrilamine prevented the A23187-induced gas trapping. Indomethacin or propranolol tended to potentiate the response and when combined, they potentiated the gas trapping by 80%. LY163443 had no effect alone, but when combined with indomethacin, propranolol, and pyrilamine, inhibited A23187-induced gas trapping by 67%. We conclude that cholinergic and histaminergic mechanisms play major roles in the ionophore-induced pulmonary gas trapping of the guinea pig. With appropriate pretreatment, sulfidopeptide leukotrienes may produce a substantial effect. 相似文献
5.
Eberhard Stengel 《Plant biology (Stuttgart, Germany)》1970,83(11):589-606
- 1 . Es werden Anlagentypen für die autotrophe, mixotrophe oder heterotrophe Saubere Kultur von Mikroalgen sowie Verfahren der Algenkultur auf Abwasserbasis beschrieben. Zur Erstellung von Freilandanlagen erscheinen Beckenkonstruktionen besonders geeignet, die auf die Verwendung industrieller Fertigteile abgestellt sind. Bei der autotrophen Kultur von Mikroalgen im Freiland besteht das Hauptproblem darin, einen effizienten CO2-Eintrag zu erzielen
- 2 . Massenkulturen mariner und limnischer Mikroalgen haben vor allem in Japan als Komponenten komplexer Aquakultursysteme wirtschaftliche Bedeutung erlangt
- 3 . Besonderes Interesse verdienen Verfahren zur Massenkultur von Mikroalgen in Abwässern. Mit ihrer Hilfe gelingt es, auf verhältnismäßig engem Raum hohe Abbauleistungen der organischen Fracht zu erzielen und gleichzeitig proteinreiche Substanz für die Tierernährung zu produzieren
6.
Lung degassing: an evaluation of two methods 总被引:1,自引:0,他引:1
7.
E. Stengel 《BMJ (Clinical research ed.)》1965,1(5451):1667-1668
8.
9.
10.
Andreas Stengel Tobias Hofmann Miriam Goebel-Stengel Vanessa Lembke Anne Ahnis Ulf Elbelt Nils W. G. Lambrecht Jürgen Ordemann Burghard F. Klapp Peter Kobelt 《Histochemistry and cell biology》2013,139(6):909-918
The orexigenic peptide ghrelin and the anorexigenic peptide nesfatin-1 are expressed by the same endocrine cell of the rat stomach, the X/A-like cell. However, data in humans are lacking, especially under conditions of obesity. We collected gastric tissue of obese patients undergoing sleeve gastrectomy and investigated the expression of nesfatin-1 and ghrelin in the gastric oxyntic mucosa by immunofluorescence. Nesfatin-1 immunoreactivity was detected in the human oxyntic mucosa in cells with an endocrine phenotype. A major portion of nesfatin-1 immunoreactive cells (78 %) co-localized with ghrelin indicating the occurrence in human X/A-like cells. In patients with very high body mass index (BMI 55–65 kg/m2), the number of nesfatin-1 immunoreactive cells/low-power field was significantly higher than in obese patients with lower BMI (40–50 kg/m2, 118 ± 10 vs. 82 ± 11, p < 0.05). On the other hand, the number of ghrelin immunoreactive cells was significantly reduced in obese patients with higher compared to lower BMI (96 ± 12 vs. 204 ± 21, p < 0.01). Also the ghrelin-acylating enzyme ghrelin-O-acyltransferase decreased with increasing BMI. In conclusion, nesfatin-1 immunoreactivity is also co-localized with ghrelin in human gastric X/A-like cells giving rise to a dual role of this cell type with differential effects on stimulation and inhibition of appetite dependent on the peptide released. The expression of these two peptides is differentially regulated under obese conditions with an increase of nesfatin-1 and a decrease of ghrelin immunoreactivity with rising BMI pointing towards an adaptive change of expression that may counteract further body weight increase. 相似文献