Reproductive Competition in Colonies of the Ant Leptothorax gredleri

Colonies of the ant, Leptothorax (s. str.) gredleri may contain several inseminated female reproductives of which typically only one is laying eggs. Observations suggest that “functional monogyny” is caused by aggressive interactions among nestmate queens. Only the most dominant queen reproduces. Subordinate queens either leave the colony to found their own nests solitarily or by budding, or stay in the nest without reproducing, but may eventually replace the dominant queen. The interrelations of life history of L. gredleri, population structure and habitat characteristics are examined.     

A new anaerobic,sporing, acetate-oxidizing,sulfate-reducing bacterium,Desulfotomaculum (emend.) acetoxidans

Archives of Microbiology - A new strictly anaerobic, polarly flagellated, sporing, acetate-oxidizing, sulfate-reducing bacterium was isolated from anaerobic fresh or sea water mud samples. The...     

Die Rezeptoren an den ersten Antennen vonLeptestheria dahalacensis Rüppel (Crustacea,Conchostraca)

Zusammenfassung Bei dem ConchostracenLeptestheria dahalacensis kommen auf den ersten Antennen etwa 600 gleich aussehende Sinneshaare vor, die in Gruppen von jeweils 25–30 zusammengefaßt sind. Diese Sinneshaare sind in zwei Teile gegliedert, die durch das lichtmikroskopisch gut sichtbare Basalstück (basal bead) voneinander getrennt sind. Dieses bildet die Basis des Haares, dessen Wand im wesentlichen aus Epicuticula besteht. Apikal wird das Haar durch das Endkügelchen (terminal pellet) abgeschlossen. Das Basalstück wird von der untersten Lage der Epicuticula gebildet. Die 4–10 Receptorcilien, die jeweils einzeln ebensovielen Dendriten aufsitzen, ziehen aus dem inneren Teil des Rezeptors, der von insgesamt 5 Hüllzellen umgeben wird, durch das Basalstück, in dem sie stark eingeengt werden und verzweigen sich dann im äußeren Teil des Rezeptors. Sie ziehen bis zum Endkügelchen, in das sie durch einen Porus, den man als Häutungsporus ansprechen kann, eintreten. In der Häutungsvorbereitung wird der Haarbalg von der Hüllzelle 5, das Basalstück von der Hüllzelle 4, der Haarschaft dagegen von der Hüllzelle 3 gebildet. Dabei spaltet sich die Hüllzelle 3 ringspaltförmig auf, so daß in diesem Spalt der neuangelegte Haarschaft handschuhfingerförmig eingestülpt liegt. Die Hüllzelle 2 formt die Spitze des neuen Haares, während die Dendritenscheide von der Hüllzelle 1 abgegeben wird.

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The receptors on the first antennae ofLeptestheria dahalacensis Rüppel (Crustacea, Conchostraca)

Summary On the antennulae ofLeptestheria dahalacensis (Conchostraca) nearly 600 sensory setae of one type are found. They are gathered in groups of 25–30. The single sensory seta is divided into two parts by the basal bead which is easily visible in the light microscope. The basal bead is the socket of the seta, whose wall is mainly built up by the epicuticle. The terminal pellet closes the tip of the seta. The basal bead is derived from the innermost layer of the epicuticle. 4–10 dendrites each with one receptorcilium innervate the receptor. The receptorcilia stretch through the interior part of the receptor and the basal bead into the exterior part, where they branch. They enter the terminal pellet in a porus, which seems to be a moulting porus. The interior part of the receptor is surrounded by 5 sheath cells. During the premoult it becomes obvious, that the socket of the seta is built by the sheath cell 5, the basal bead by the sheath cell 4 and the shaft by the sheath cell 3. For this the sheath cell 3 is divided into two parts. Between this two parts the newly formed cuticle is invaginated. The sheath cell 2 formes the tip and the sheath cell 1 the cuticular sheath of the new bristle.

     

Surfactant protein D increases phagocytosis and aggregation of pollen-allergen starch granules

Recent studies have shown that surfactant components, in particular the collectins surfactant protein (SP)-A and -D, modulate the phagocytosis of various pathogens by alveolar macrophages. This interaction might be important not only for the elimination of pathogens but also for the elimination of inhaled allergens and might explain anti-inflammatory effects of SP-A and SP-D in allergic airway inflammation. We investigated the effect of surfactant components on the phagocytosis of allergen-containing pollen starch granules (PSG) by alveolar macrophages. PSG were isolated from Dactylis glomerata or Phleum pratense, two common grass pollen allergens, and incubated with either rat or human alveolar macrophages in the presence of recombinant human SP-A, SP-A purified from patients suffering from alveolar proteinosis, a recombinant fragment of human SP-D, dodecameric recombinant rat SP-D, or the commercially available surfactant preparations Curosurf and Alveofact. Dodecameric rat recombinant SP-D enhanced binding and phagocytosis of the PSG by alveolar macrophages, whereas the recombinant fragment of human SP-D, SP-A, or the surfactant lipid preparations had no effect. In addition, recombinant rat SP-D bound to the surface of the PSG and induced aggregation. Binding, aggregation, and enhancement of phagocytosis by recombinant rat SP-D was completely blocked by EDTA and inhibited by d-maltose and to a lesser extent by d-galactose, indicating the involvement of the carbohydrate recognition domain of SP-D in these functions. The modulation of allergen phagocytosis by SP-D might play an important role in allergen clearance from the lung and thereby modulate the allergic inflammation of asthma.     

Inhibition of IL-6, TNF-alpha, and cyclooxygenase-2 protein expression by prostaglandin E2-induced IL-10 in bone marrow-derived dendritic cells

Several endogenously produced mediators, including cytokines such as IL-6, IL-10, and TNF-alpha and prostanoids such as prostaglandin E(2) (PGE(2)), regulate dendritic cell (DC) function and contribute to immune homeostasis. In this study, we report that exogenous PGE(2) enhances the production of IL-10 from bone marrow-derived DC (BM-DC). IL-6, but not TNF-alpha, release is enhanced by PGE(2) in the presence of anti-IL-10, suggesting that endogenous IL-10 masks PGE(2)-induced IL-6. Furthermore, both exogenous IL-10 and PGE(2) inhibit LPS-induced IL-6 and TNF-alpha, whereas selective inhibition of cyclooxygenase-2 (COX-2) or addition of anti-IL-10 causes the reverse effects. Exogenous IL-10, but not IL-6, dose-dependently suppresses COX-2 protein expression and PGE(2) production, and TNF-alpha does not reverse this effect. In contrast, anti-IL-10 up-regulates prostanoid production by LPS-stimulated BM-DC. Taken together, our results show that in response to PGE(2), BM-DC produce IL-10, which in turn down-regulates their own production of IL-6-, TNF-alpha-, and COX-2-derived prostanoids, and plays crucial roles in determining the BM-DC pro-inflammatory phenotype.     

EpCAM: Structure and function in health and disease

Injection of tumor cells in mice more than 30 years ago resulted in the discovery of an epithelial antigen, later defined as a cell adhesion molecule (EpCAM). Although EpCAM has since evoked significant interest as a target in cancer therapy, mechanistic insights on the functions of this glycoprotein have been emerging only very recently. This may have been caused by the multitude of functions attributed to the glycoprotein, its localization at different subcellular sites and complex posttranslational modifications. Here, we review how EpCAM modifies cell–cell contact adhesion strength and tissue plasticity, and how it regulates cell proliferation and differentiation. Major knowledge derived from human diseases will be highlighted: Mutant EpCAM that is absent from the cell surface leads to fatal intestinal abnormalities (congenital tufting enteropathy). EpCAM-mediated cell proliferation in cancer may result from signaling (i) via regulated intramembrane proteolysis and/or (ii) the localization and association with binding partners in specialized membrane microdomains. New insight in EpCAM signaling will help to develop optimized cancer therapies and open new avenues in the field of regenerative medicine.     

Lymphocytic Choriomeningitis Virus Infection in FVB Mouse Produces Hemorrhagic Disease

The viral family Arenaviridae includes a number of viruses that can cause hemorrhagic fever in humans. Arenavirus infection often involves multiple organs and can lead to capillary instability, impaired hemostasis, and death. Preclinical testing for development of antiviral or therapeutics is in part hampered due to a lack of an immunologically well-defined rodent model that exhibits similar acute hemorrhagic illness or sequelae compared to the human disease. We have identified the FVB mouse strain, which succumbs to a hemorrhagic fever-like illness when infected with lymphocytic choriomeningitis virus (LCMV). FVB mice infected with LCMV demonstrate high mortality associated with thrombocytopenia, hepatocellular and splenic necrosis, and cutaneous hemorrhage. Investigation of inflammatory mediators revealed increased IFN-γ, IL-6 and IL-17, along with increased chemokine production, at early times after LCMV infection, which suggests that a viral-induced host immune response is the cause of the pathology. Depletion of T cells at time of infection prevented mortality in all treated animals. Antisense-targeted reduction of IL-17 cytokine responsiveness provided significant protection from hemorrhagic pathology. F1 mice derived from FVB×C57BL/6 mating exhibit disease signs and mortality concomitant with the FVB challenged mice, extending this model to more widely available immunological tools. This report offers a novel animal model for arenavirus research and pre-clinical therapeutic testing.     

Isosteric ramatroban analogs: selective and potent CRTH-2 antagonists

The chemoattractant receptor-homologous molecule expressed on T(H)2 cells (CRTH-2), also found on eosinophils and basophils, is a prostaglandin D2 receptor involved in the recruitment of these cell types during an inflammatory response. In this report, we describe the synthesis and optimization of a ramatroban isostere that is a selective and potent antagonist of CRTH-2 which may be useful in the treatment of certain diseases.