Your search keyword '"Rinnenthal, Jan L."' showing total 2 results

1. Th2- M2 immunity in lesions of muscular sarcoidosis and macrophagic myofasciitis.

Author

Preusse, Corinna, Goebel, Hans‐H., Pehl, Debora, Rinnenthal, Jan L., Kley, Rudolf A., Allenbach, Yves, Heppner, Frank L., Vorgerd, Matthias, Authier, François Jerôme, Gherardi, Romain, and Stenzel, Werner

Subjects

*PSEUDOTUBERCULOSIS, *SARCOIDOSIS, *NEUROLOGICAL disorders, *NEUROLOGY, *NEUROBIOLOGY

Abstract

Objective To analyse the paradox of a lack of giant cell formation and fibrosis in chronic lesions of macrophagic myofasciitis ( MMF) in comparison with muscular sarcoidosis ( MuS). Methods Inflammatory lesions and contiguous muscle regions from biopsy samples of 10 patients with MuS and 10 patients with MMF were cut out by laser microdissection. Mediators of the T helper cell ( Th)1 inducing classical macrophage activation (e.g. STAT1, IFNγ and CXCR3), and Th2 inducing alternative activation of macrophages (e.g. CD206/ MRC1, STAT6, SOCS1), molecules involved in development of fibrosis (e.g. TGFβ) and giant cells (e.g. TYROBP), were assessed by immunohistochemistry and real-time polymerase chain reaction ( PCR). Results STAT6-induced Th2 immunity was associated with up-regulated gene expression of MRC 1, SOCS 1 and TGFB in inflammatory foci, in comparison with adjacent tissue. TYROBP and TREM 2, genes regulating giant cell formation, were more strongly expressed in lesions of MuS patients than in those of MMF. TGFβ co-localized with CD206+ macrophages in MuS but not in MMF. Conversely, Th1 immunity was illustrated by STAT1 staining both in macrophages and myofibres in MuS, but not in MMF. Also, STAT1-induced IFNG and CXCR 3 expression in lesions and the surrounding tissue was elevated compared with normal controls, but without statistically significant differences. Conclusion Giant cell and typical granuloma formations, including fibrogenesis, is dependent on two main mechanisms, both involving specific macrophage activation: a strong Th2- M2 polarization and a significant expression of TYROBP and TGFβ in macrophages. The low-grade alternative activation of macrophages in MMF lesions and poor TYROBP and TGFβco-expression are obviously insufficient to produce giant cells. [ABSTRACT FROM AUTHOR]

Published

2015

2. Functional Impairment of Microglia Coincides with Beta-Amyloid Deposition in Mice with Alzheimer-Like Pathology.

Author

Krabbe, Grietje, Halle, Annett, Matyash, Vitali, Rinnenthal, Jan L., Eom, Gina D., Bernhardt, Ulrike, Miller, Kelly R., Prokop, Stefan, Kettenmann, Helmut, and Heppner, Frank L.

Subjects

*MICROGLIA, *AMYLOID beta-protein, *LABORATORY mice, *ALZHEIMER'S disease, *IMMUNOLOGY, *NEUROSCIENCES, *DEMENTIA

Abstract

Microglial cells closely interact with senile plaques in Alzheimer’s disease and acquire the morphological appearance of an activated phenotype. The significance of this microglial phenotype and the impact of microglia for disease progression have remained controversial. To uncover and characterize putative changes in the functionality of microglia during Alzheimer’s disease, we directly assessed microglial behavior in two mouse models of Alzheimer’s disease. Using in vivo two-photon microscopy and acute brain slice preparations, we found that important microglial functions - directed process motility and phagocytic activity - were strongly impaired in mice with Alzheimer’s disease-like pathology compared to age-matched non-transgenic animals. Notably, impairment of microglial function temporally and spatially correlated with Aβ plaque deposition, and phagocytic capacity of microglia could be restored by interventionally decreasing amyloid burden by Aβ vaccination. These data suggest that major microglial functions progressively decline in Alzheimer’s disease with the appearance of Aβ plaques, and that this functional impairment is reversible by lowering Aβ burden, e.g. by means of Aβ vaccination. [ABSTRACT FROM AUTHOR]

Published

2013