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1.
Zusammenfassung Die Normalentwicklung von Schilddrüse und Hypophyse während der Larvalentwicklung und Metamorphose von Xenopns laevis Daudin und die Veränderungen des Hypophysenvorderlappens (HVL) und der Schilddrüse auf Behandlung mit Dinitrophenol, Natriumthiocyanat, Methylthiouracil, Kaliumperchlorat und Thyroxin im Überschuß wurden untersucht.Die Selbstdifferenzierungsfähigkeit der Schilddrüse und die Wirkung exogenen Thyroxins auf die Schilddrüse wurde an hypophysektomierten Tieren herausgestellt.Schilddrüse und -Zellen des Hypophysenvorderlappens werden mit Beginn des Hinterbeinwachstums funktionsfähig. Zur gleichen Zeit wird das Körpergewebe gegenüber Schilddrüsenhormon empfindlich. Das HVL-Schilddrüsen-Regulationssystem wird ebenfalls zudiesem Zeitpunkt reaktionsbereit.Die Schilddrüse ist bis zu einem gewissen Grad selbstdifferenzierungsfähig; sie wird auch dann morphologisch ausdifferenziert — wenn auch verzögert und nicht in vollem Umfang —, wenn genügend exogenes Thyroxin vorhanden ist, um die Entwicklung weiterzuführen, und beim Fehlen der Hypophyse.Die Sekret-Produktion und -Speicherung in den -Zellen des HVL erfolgt auch dann, wenn genügend exogenes Thyroxin die TSH-Produktion überflüssig macht.Dinitrophenol dämpft die Aktivität der Schilddrüse, ohne daß die -Zellen des HVL hypertrophieren. Eine Hemmung des Rückkopplungsmechanismus ist wahrscheinlich.Natriumthiocyanat, Methylthiouracil und Kaliumperchlorat bewirken Kropfbildung und eine starke Hypertrophie der -Zellen des HVL. Dabei entsprechen die durch diese drei Substanzen verursachten Veränderungen der -Zellen nicht dem jeweiligen Aktivitätsgrad der Schilddrüse. So ist z. B. nach Thiocyanat-Behandlung die Schilddrüsenhemmung am stärksten, die Kernvergrößerung der -Zellen aber am geringsten. Natriumthiocyanat, Methylthiouracil und Kaliumperchlorat hemmen demnach nicht nur die Hormonproduktion der Schilddrüse unterschiedlich, sie greifen außerdem noch störend in das Regulationssystem ein: entweder durch Veränderung des Schilddrüsenhormons selbst oder des Rückkopplungsmechanismus.
Summary The normal development of the thyroid gland and the pituitary during larval development and metamorphosis of the clawed toad Xenopus laevis Daudin and the changes of the anterior pituitary and the thyroid after treatment with dinitrophenol, thiocyanate, thiouracil, perchlorate and exceeding thyroxine were investigated.The capacity of self-differentiation and the effect of exogenous thyroxine on the thyroid were pointed out in hypophysectomized animals.Thyroid and TSH-producing cells (-cells) of the anterior pituitary start functioning at the beginning of the hindlimb-growth. At the same time the body tissue gets sensitive to thyroid-hormone and the anterior pituitary-thyroid-regulating system shows first signs of reactivity.The thyroid is able to selfdifferentiate up to a certain degree. The gland morphologically differentiates — though retarded and not to the full extent —, even if either sufficient exogenous thyroxine is available to proceed the development or the pituitary is lacking.The -cells of the anterior pituitary synthesize and store hormone, even if sufficient exogenous thyroxine makes the TSH-production unnecessary.Dinitrophenol restrains the activity of the thyroid without causing hypertrophy of the -cells of the anterior pituitary. An inhibition of the feed-back mechanism seems to be possible.Thiocyanate, thiouracil and perchlorate cause goitre and a strong hypertrophy of the -cells of the anterior pituitary. Considering the effects of these three substances, the changes of the -cells, caused by the lack of thyroid hormone, do not correspond with the respective activity of the thyroid. The inhibition of the thyroid is strongest after treatment with thiocyanate, but in this case the increase of the nuclear diameter of the -cells is smallest. Therefore thiocyanate, thiouracil and perchlorate do not only inhibit the hormone production of the thyroid. They also interfere with the regulation system in a different manner: they either modify the thyroid hormone itself or interfere with the feed-back mechanism.


Dissertation der Naturwissenschaftlichen Fakultät der J. W. Goethe-Universität in Frankfurt a. M.Meinem Lehrer, Herrn Prof. Dr.H. Giersberg, danke ich für die Anregung dieser Arbeit, Herrn Prof. Dr. M. Lindauer für die weitere Überlassung des Arbeitsplatzes. Besonderen Dank schulde ich den Herren Prof. Dr. W. Hanke und Dr. F.-W. Pehlemann für jederzeit hilfreichen Rat.  相似文献   
2.
Effect of Long-Lasting Diabetes Mellitus on Rat and Human Brain Monoamines   总被引:3,自引:1,他引:2  
Experimental alloxan- or streptozotocin-produced diabetes in rats was accompanied by an increase in the levels of norepinephrine, dopamine, and serotonin, whereas the contents of metabolites, i.e., 5-hydroxyindoleacetic acid and homovanillic acid, in the whole brain gradually decreased with the duration of diabetes. Among the striatum, thalamus, and hypothalamus of alloxan diabetic rats, monoamine alterations were observed only in the hypothalamus; after 1 week an increase of norepinephrine content and after 13 weeks an increase of norepinephrine and dopamine contents were found. Tissues of 11 brain regions of 10 diabetic and 12 control patients post mortem were investigated for monoamine concentrations. Patients were all male, of similar age and interval between death and autopsy. Diabetic patients had an increase in the content of serotonin in the medial and lateral hypothalamus. The content of dopamine increased in the medial hypothalamus, putamen, and medial and lateral pallidus. In diabetic patients, the content of norepinephrine increased in the lateral pallidus and decreased in the nucleus accumbens and claustrum. Thus, it seems that diabetes mellitus in rats, as well as in humans is associated with regionally specific changes in brain monoamines.  相似文献   
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Capsule Spatial environmental modelling well predicted nesting distribution of the White stork in Southeast Europe and can be used in conservation planning with respect to climate change.

Aims To create spatial models for predicting White Stork presence and densities in the Southeast Europe to identify areas of suitable habitat for White Storks.

Methods We quantified the habitat used by nesting White storks in Southeast Europe. Using spatial modelling, we defined a set of free and available online environmental variables that predict the breeding localities of the species. We employed pseudo-absences and the kriging of the residuals in order to create predictive models of nest presence and density.

Results The presence–absence model was found to be precise in predicting the presence of nests. Both density and presence of breeding pairs were best explained negatively by elevation, slope, minimum temperature during May, and distance to the nearest human settlement and positively by topographic wetness index, total area of human settlement and spring precipitation.

Conclusion Our robust and easily repeatable models offer a conservation tool to reveal suitable but unoccupied localities for breeding White Storks pairs which may inform our understanding of how climate change might affect the species' distribution in the future. For example, protecting White Storks on the Dalmatian coast may become even more significant in the future, because the Dalmatian coast is predicted as the only suitable breeding area in Croatia later this century.  相似文献   
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The distribution of poly(ADP-ribose) polymerase-1 (PARP-1) over different nuclear compartments was studied by nuclear fractionation procedures and Western analysis revealing a prominent role of the nuclear matrix. This structure is operationally defined by the solubility properties of the A- and B-type lamins under defined experimental conditions. We consistently observed that most of the nuclear matrix-associated PARP-1 partitioned, in an active form, with the insoluble, lamin-enriched protein fractions that were prepared by a variety of established biochemical procedures. These PARP-1-protein interactions resisted salt extraction, disulfide reduction, RNase and DNase digestion. An inherent ability of PARP-1 to reassemble with the lamins became evident after a cycle of solubilization/dialysis using either urea or Triton X-100 and disulfide reduction, indicating that these interactions were dominated by hydrophobic forces. Together with in vivo crosslinking and co-immunoprecipitation experiments our results show that the lamins are prominent PARP-1-binding partners which could contribute to the functional sequestration of the enzyme on the nuclear matrix.  相似文献   
9.

Background

HIV and Helicobacter pylori are common chronic infections in sub-Saharan Africa. Both conditions can predispose to gastric hypochlorhydria that may be a risk factor for enteric infections and reduced drug absorption. We have investigated to what extent HIV and H. pylori infections are associated with hypochlorhydria in a Malawian cohort of patients undergoing endoscopy.

Methods

104 sequential symptomatic adults referred for gastroscopy at Queen Elizabeth Central Hospital, Blantyre, Malawi, had blood taken for rapid HIV testing and fasting serum gastrin analysis. Gastric fluid was aspirated for pH testing, and gastric biopsies were taken.

Results

After 9/104 HIV-infected patients who were already established on anti-retroviral therapy were excluded, 17/95 (25.0%) were seropositive for untreated HIV, and 68/95 (71.6%) patients were H. pylori positive by histology. Hypochlorhydria (fasting gastric pH>4.0) was present in 55.8% (53/95) of patients. H. pylori infection was significantly associated with hypochlorhydria (OR 2.91, [1.02-7.75], p=0.046). While single infection with HIV was not significantly independently associated with hypochlorhydria. H. pylori and HIV co-infection was more strongly associated with hypochlorhydria (OR 6.25, [1.33-29.43], p=0.020) than either infection alone, suggesting an additive effect of co-infection. HIV infection was associated with higher serum gastrin levels (91.3pM vs. 53.1pM, p=0.040), while H. pylori infection was not (63.1pM vs. 55.1pM, p=0.610). Irrespective of H. pylori and HIV status, most patients (>90%) exhibited pangastritis. Only three patients had histological evidence of gastric atrophy, of which only one was HIV-infected.

Conclusion

H. pylori infection was associated with fasting hypochlorhydria, while HIV was not independently associated. HIV and H. pylori co-infection, however, was more strongly associated with hypochlorhydria than H. pylori infection alone. The mechanism of this apparent additive effect between HIV and H. pylori remains unclear, but appears to be related to chronic pangastritis rather than gastric atrophy, and associated with hypergastrinaemia in HIV-infected individuals.  相似文献   
10.
The intracerebroventricular (icv) application of streptozotocin (STZ) in low dosage was used in 3-month-old rats to explore brain insulin system dysfunction. Three months following STZ icv treatment, the expression of insulin-1 and -2 mRNA was significantly reduced to 11% in hippocampus and to 28% in frontoparietal cerebral cortex, respectively. Insulin receptor (IR) mRNA expression decreased significantly in frontoparietal cerebral cortex and hippocampus (16% and 33% of control). At the protein/activity level, different abnormalities of protein tyrosine kinase activity (increase in hippocampus), total IR beta-subunit (decrease in hypothalamus) and phosphorylated IR tyrosine residues (increase) became apparent. The STZ-induced disturbance in learning and memory capacities was not abolished by icv application of glucose transport inhibitors known to prevent STZ-induced diabetes mellitus. The discrepancy between reduced IR gene expression and increase in both phosphorylated IR tyrosine residues/protein tyrosine kinase activity may indicate imbalance between phosphorylation/dephosphorylation of the IR beta-subunit causing its dysfunction. These abnormalities may point to a complex brain insulin system dysfunction after STZ icv application, which may lead to an increase in hyperphosphorylated tau-protein concentration. Brain insulin system dysfunction is discussed as possible pathological core in the generation of hyperphosphorylated tau protein as a morphological marker of sporadic Alzheimer's disease.  相似文献   
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