Vera Bergmeier scite author profile

in the nanomolar range. Receptor activity was most efficiently blocked by mianserin, a substance with antidepressant activity in vertebrates. The rank order of inhibitory potency for potential receptor antagonists was very similar on all four honeybee receptors with mianserin >> cyproheptadine > metoclopramide > chlorpromazine > phentolamine. The subroot of octopamine receptors activating adenylyl cyclases is the largest that has so far been characterized in arthropods, and it should now be possible to unravel the contribution of individual receptors to the physiology and behavior of honeybees.

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Identification of a myofibroblast-specific expression signature in skin wounds

Bergmeier

Etich

Pitzler

et al. 2018

Matrix Biology

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Macrophage‐mediated psoriasis can be suppressed by regulatory T lymphocytes

Dantas¹,

Masemann²,

Schied³

et al. 2016

The Journal of Pathology

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We recently described an inducible human TNF transgenic mouse line (ihTNFtg) that develops psoriasis-like arthritis after doxycycline stimulation and analysed the pathogenesis of arthritis in detail. Here, we show that the skin phenotype of these mice is characterized by hyperproliferation and aberrant activation of keratinocytes, induction of pro-inflammatory cytokines, and infiltration with Th1 and Treg lymphocytes, particularly with macrophage infiltration into lesional skin, thus pointing to a psoriasis-like phenotype. To reveal the contribution of T cells and macrophages to the development of TNF-mediated psoriasis, ihTNFtg mice were crossbred into RAG1 mice lacking mature T and B cells. Surprisingly, the psoriatic phenotype in the double mutants was not reduced; rather, it was enhanced. The skin showed significantly increased inflammation and in particular, increased infiltration by macrophages. Consequently, depletion of macrophages in RAG1 or wild-type mice led to decreased disease severity. On the contrary, depletion of Treg cells in wild-type mice increased both psoriasis and the number of infiltrating macrophages, while adoptive transfer of Foxp3-positive cells into RAG1 or wild-type mice decreased both the development of psoriasis and macrophage infiltration. Thus, we conclude that Treg lymphocytes inhibit the pro-inflammatory activity of macrophages, which are the major immune effector cells in hTNF-mediated psoriasis. Copyright © 2016 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.

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miR-126-3p Promotes Matrix-Dependent Perivascular Cell Attachment, Migration and Intercellular Interaction

Pitzler

Auler

Probst

et al. 2016

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microRNAs (miRNAs) can regulate the interplay between perivascular cells (PVC) and endothelial cells (EC) during angiogenesis, but the relevant PVC-specific miRNAs are not yet defined. Here, we identified miR-126-3p and miR-146a to be exclusively upregulated in PVC upon interaction with EC, determined their influence on the PVC phenotype and elucidate their molecular mechanisms of action. Specifically the increase of miR-126-3p strongly promoted the motility of PVC on the basement membrane-like composite and stabilized networks of EC. Subsequent miRNA target analysis showed that miR-126-3p inhibits SPRED1 and PLK2 expression, induces ERK1/2 phosphorylation and stimulates TLR3 expression to modulate cell-cell and cell-matrix contacts of PVC. Gain of expression experiments in vivo demonstrated that miR-126-3p stimulates PVC coverage of newly formed vessels and transform immature into mature, less permeable vessels. In conclusion we showed that miR-126-3p regulates matrix-dependent PVC migration and intercellular interaction to modulate vascular integrity. STEM CELLS 2016;34:1297-1309 SIGNIFICANCE STATEMENTIncreased miR-126-3p levels stimulate matrix-dependent intercellular interaction of perivascular cells to promote PVC coverage of newly formed endothelial vessel and transform immature vessels into mature, less permeable vessels. In contrast, decreased miR-126-3p levels may loosen BM-dependent intercellular connections and support detachment of PVC and EC from preexisting vessels to allow new blood vessel formation. We therefore propose that miR-126-3p is a novel regulator of PVC-mediated vessel stability during neoangiogenesis and in pathological scenarios like tumor angiogenesis.

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Identification of a reference gene for the quantification of mRNA and miRNA expression during skin wound healing

Etich

Bergmeier

Pitzler

et al. 2016

Connective Tissue Research

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Vera Bergmeier

Molecular, pharmacological, and signaling properties of octopamine receptors from honeybee (Apis mellifera) brain

Identification of a myofibroblast-specific expression signature in skin wounds

Macrophage‐mediated psoriasis can be suppressed by regulatory T lymphocytes

miR-126-3p Promotes Matrix-Dependent Perivascular Cell Attachment, Migration and Intercellular Interaction

Identification of a reference gene for the quantification of mRNA and miRNA expression during skin wound healing

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