Das Sediment des Kummerower Sees. Untersuchungen des Chemismus und der Diatomeenflora

The Sediment of Lake Kummerow. Investigations on the Chemism and the Diatom Flora The paper deals with the distribution of chemical parameters and of diatoms in the deposits of the eutrophic Lake Kummerow (GDR), produced during about the last 3500 years. The sediment consists of a calcareous gyttja with a very low content of sand and clay. The results indicate a relatively constant trophic state of the lake in former times and an increased production within the last five centuries. Stephanodiscus astraea and its variety minutula is by far the most constant diatom species; in the uppermost parts of the sediment small sized planctonic taxa are increasing, in the main Stephanodiscus hantzschii var. pusillus, Melosira granulata var. angustissima, Asterionella formosa and Synedra acus var. angustissima and var. radians.     

Subcellular localization of EGFR in esophageal carcinoma cell lines

Background: The EGF receptor is a therapeutic target in cancer cells, whereby mutations of EGFR and/or signalling members act as predictive markers. EGFR however also exhibits dynamic changes of subcellular localization, leading to STAT5 complex formation, nuclear translocation and induction of Aurora-A expression in squamous cancer cells. We previously described high EGFR and Aurora-A expression in esophageal cancer cells. Here, we investigated subcellular localization of EGFR and STAT5 in esophageal cancer cells. Results: Quantitative immunofluorescence analyses of four esophageal cancer cell lines reflecting esophageal squamous cell carcinomas (ESCC) and esophageal adenocarcinomas (EAC) revealed that the subcellular localization of EGFR was shifted from a membranous to cytoplasmic localization upon EGF-stimulation in OE21 (ESCC) cells. Thereby, EGFR in part co-localized with E-Cadherin. In parallel, phosphorylated STAT5-Tyr694 appeared to increase in the nucleus and to decrease at the cell membrane. In three additional cell lines, EGFR was only marginally (Kyse-410/ESCC; OE19/EAC) and weakly (OE33, EAC) detectable at the cell membrane. Partial co-localization of EGFR and E-Cadherin occurred in OE33 cells. Post EGF-stimulation, EGFR was detected in the cytoplasm, resembling endosomal compartments. Furthermore, OE19 and OE33 exhibited nuclear STAT5-Tyr694 phosphorylation upon EGF-stimulation. None of the four cell lines showed nuclear EGFR expression and localization. Conclusion: In contrast to other (squamous) cancer cells, activation of EGFR in esophageal squamous cancer cells does not result in nuclear translocation of EGFR. Still, the subcellular localization of EGFR may influence STAT5-associated signaling pathways in esophageal cancer cells and hence possibly also the responses to ErbB, respective EGFR-targeted therapies.     

Cyclic AMP-induced reversible decrease in cAMP-binding to cell surface receptors of Dictyostelium discoideum

Abstract Adaptation may be the result of a change in affinity and/or number of cAMP-binding sites at the cell surface. To test this possibility we used agip 53, a mutant that does not synthesize cAMP in response to cAMP stimulation. cAMP induced a fast decrease in cAMP-binding to aggregation-competent cells, which reached a maximum at 10–20 s and was reversible with a t _0.5 of about 70 s. The decrease in cAMP-binding involved 46000 sites per cell and was mainly due to a reduction in the apparent affinity for cAMP-binding and to a smaller extent to slowly dissociating cAMP. Our results suggest that under these conditions only a fraction of the cAMP-binding sites at the cell surface are involved in transmembrane signalling, which is indeed observed for many of the physiological responses in Dictyostelium discoideum .     

Seminal prostaglandins in men with subnormal sperm motility and therapeutic treatment

The contents of prostaglandins in seminal plasma from a total of 73 men were evaluated. The subjects were grouped as follows: normospermic men, patients with impaired motility, patients with small untreated varicocelle and patients with impaired motility and Kallikrein therapy. Sperm density, morphology and motility were examined. High performance reversed phase liquid chromatography (HPLC) in combination with specific radioimmunoassays were used for the determination of PGE₂, PGI₂ and PGF_2α. There was a significant difference (p < 0, 025; F-test) between the PGI₂ concentrations in patients with impaired motility (5,6 ± 1,4 pg/mg protein) and normal men (8,8 ± 3,7 pg/mg protein). PGE₂ and PGF_2α were significantly different in patients with varicocele (p < 0,025, F-test). Wide ranges of prostaglandins occured in the Kallikrein-group with no significant differences. We conclude that: a) PGI₁ is an additional prostaglandin compound in seminal plasma. b)its measurement may not be useful as diagnostic parameter in subfertile men and c) Kallikrein has no influence on the prostaglandin content in seminal plasma and other seminal parameters as motility, motility index and sperm counts.     

Effects of two chitin synthesis inhibitors on Thalassiosira fluviatilis and Cyclotella cryptica

Abstract The effects of two commercial chitin synthesis inhibitors, dimilin and polyoxin D, on chitin fiber formation and cell sedimentation for the diatoms Thalassiosira fluviatilis and Cyclotella cryptica (Bacillariophyceae) were investigated. Dimilin treatments for both diatom species were indistinguishable from controls in terms of chitin fiber productions, cell density and sedimentation. Polyoxin D-treated cells of both diatom species completely lacked the characteristic chitin fibers. Polyoxin D cultures were also characterized by a significant decrease in population density, increased sedimentation rates and a strong tendency to clump in comparison with control and dimilin treatments. It was concluded that (1) dimilin does not directly inhibit chitin synthesis in diatoms; (2) polyoxin-D inhibits β-chitin fibril formation, and (3) chitin fibers play an important role in cell separation and cell buoyancy.