Your search keyword '"Emmendörffer A"' showing total 11 results

1. Diagnosis of chronic granulomatous disease and of its mode of inheritance by dihydrorhodamine 123 and flow microcytofluorometry.

Author

Roesler, J., Hecht, M., Freihorst, J., Lohmann-Matthes, M., Emmendörffer, A., Lohmann-Matthes, M L, and Emmendörffer, A

Abstract

Dihydrorhodamine 123 (DHR) attached to membranes of granulocytes (PMN) and monocytes is caused to fluoresce by reactive oxygen intermediates (ROI) indicating the ability of phagocytes to produce these microbicide metabolites in a flow microcytofluorimeter. Whole blood samples from five boys with known chronic granulomatous disease (CGD) and from their mothers (and from one father and one grandmother), were examined following erythrocyte lysis in order to test this new method. An incubation period of 10 min with phorbol-myristate-acetate, followed by another 15 min incubation period with DHR before flow microcytofluorimetric analysis of 5 or 10 x 10(3) phagocytes, was sufficient to obtain the following results. PMN and monocytes from four patients with CGD could clearly not produce any ROI whereas cells from one patient displayed decreased activity in ROI production as compared to cells from a healthy donor. The X-linked mode of inheritance was detected in six carriers by the presence of two different cell populations (one normal ROI-producing and one negative or less active population). All the phagocytes from one mother produced ROI in normal amounts suggesting an autosomal mode of inheritance. All in all, the method presented provides a fast and most simple tool to diagnose CGD, to determine a decrease or total lack of ROI production and to establish the mode of inheritance of the disease. [ABSTRACT FROM AUTHOR]

Published

1991

2. Orodispersible Films: A Delivery Platform for Solid Lipid Nanoparticles?

Author

Steiner, Denise, Emmendörffer, Jakob F., and Bunjes, Heike

Subjects

SOLID dosage forms, METHYLCELLULOSE, NANOPARTICLES

Abstract

To overcome the poor bioavailability observed for many newly developed active pharmaceutical ingredients (APIs), an appropriate formulation strategy is necessary. One approach is the formulation of these substances in solid lipid nanoparticles and their further processing into solid dosage forms. A promising and innovative oral delivery platform could be orodispersible films (ODFs). ODFs were already investigated more closely, e.g., for the administration of API nanoparticles, and proved their suitability for this formulation approach. The current study was aimed at investigating if the HPMC (hydroxypropyl methyl cellulose) film matrix is also suitable to serve as an appropriate delivery platform for solid lipid nanoparticles. Dependent on the type of triglyceride nanoparticles embedded in the film matrix and the formulation of the lipid particles, lipid contents of up to 54 wt.% could be realized in the film matrix without the loss of the nanoparticulate state. Good mechanical properties were confirmed for these films by determining the tensile strength as well as the elongation before breakage. Interestingly, processing of a lipid suspension into this solid dosage form led to a significantly reduced transformation of the lipid particles from the metastable α- into the stable β-polymorph. This could prove very beneficial when the lipid particles are loaded with APIs. [ABSTRACT FROM AUTHOR]

Published

2021

3. Local Activation of Nonspecific Defense against a Respiratory Model Infection by Application of Interferon-γ.

Author

Steinmüller, Christiane, Franke-Ullmann, Gabriela, Lohmann-Matthes, Marie-Luise, and Emmendörffer, Andreas

Published

2000

4. Expansion and high proliferate potential of the macrophage system throughout life time of lupus-prone NZB/W and MRL lpr/lpr mice. Lack of down-regulation of extramedullar macrophage proliferation in the postnatal period.

Author

Müller, Meike, Emmendörffer, Andreas, and Lohmann-Matthes, Marie-Luise

Published

1991

5. Production of oxygen radicals by fibroblasts and neutrophils from a patient with x-linked chronic granulomatous disease.

Author

Emmendörffer, Andreas, Roesler, Joachim, Eisner, Jörn, Raeder, Evilyn, Lohmann-Matthes, Marie-Luise, and Meier, Beate

Published

1993

6. Altered function and surface marker expression of neutrophils induced by rhG-CSF treatment in severe congenital neutropenia.

Author

Elsner, Jörn, Roesler, Joachim, Emmendörffer, Andreas, Zeidler, Cornelia, Lohmann-Matthes, Marie-Luise, and Welte, Karl

Published

1992

7. In vitro functions of neutrophils induced by treatment with rhG-CSF in severe congenital neutropenia.

Author

Roesler, J., Emmendörffer, A., Eisner, J., Zeidler, C., Lohmann-Matthes, M., and Welte, K.

Published

1991

8. Effect of chemotherapy on T-lymphocyte subsets in B-cell proliferative disorders.

Author

Emmendörffer, C. and Pichler, W.

Abstract

The T-cell subset distribution and the activity markers of 41 patients with multiple Myeloma, Waldenström's macroglobulinaemia and benign monoclonal gammopathy were repeatedly analysed using monoclonal antibodies (T3, T4, T8, anti-TAC, anti DR) and rosetting techniques. In myeloma and macroglobulinaemia the relative and absolute numbers of T4 cells were diminished while the absolute number of T8 cells was not decreased. No significant difference between stage I and III of the myeloma disease was seen. The diminished number of T4 cells in myeloma was partly due to the effect of chemotherapy. Chemotherapy-induced lymphopenia resulted in a drop of circulating T4 cells and an inverted T4/T8 cell ratio. Untreated patients with myeloma were not significantly different from patients with benign gammopathy. Patients with macroglobulinaemia differed from patients with myeloma as they had an increased absolute T8 cell count and a significantly elevated percentage of TAC (= IL 2 receptor expressing) cells. In macroglobulinaemia chemotherapy affected also the T8 cell subset. Thus, patients with macroglobulinaemia, but not with myeloma appear to have activated T8 cells in their circulation. [ABSTRACT FROM AUTHOR]

Published

1985

9. Complex effects of long-term 50 Hz magnetic field exposure in vivo on immune functions in female Sprague-Dawley rats depend on duration of exposure.

Author

Mevissen, Meike, Häussler, Monika, Szamel, Marta, Emmendörffer, Andreas, Thun-Battersby, Susanne, and Löscher, Wolfgang

Published

1998

10. Flow cytometry reveals different lag times in rapid cytoplasmic calcium elevations in human neutrophils in response to N-formyl peptide.

Author

Elsner, Jörn, Norgauer, Johannes, Dobos, Gustav J., Emmendörffer, Andreas, Schöpf, Erwin, Kapp, Alexander, and Roesler, Joachim

Published

1993

11. Human melanocytes can be isolated, propagated and expanded from plucked anagen hair follicles.

Author

Dieckmann, Christina, Milkova, Linda, Hunziker, Thomas, Emmendörffer, Andreas, and Simon, Jan C.

Subjects

MELANOCYTES, HAIR follicles, OXYGEN, IMMUNOHISTOCHEMISTRY, ANTIGENS, PHENOL oxidase

Abstract

Please cite this paper as: Human melanocytes can be isolated, propagated and expanded from plucked anagen hair follicles. Experimental Dermatology 2010; 19: 543–545. Herein, we report a technically simple method for isolation and culture of human follicular melanocytes based on explant cultures of epilated hair follicles. This technique does not require any surgical intervention and allows the isolation and cultivation of follicular melanocytes from a comparatively small amount of raw material. Generally, 30–60 human anagen hair follicles have been plucked from the scalp of healthy donors and cultivated under low oxygen pressure (5%). After a short period of time cells of various types were growing out from the outer root sheath (ORS) of the hair follicles. Under the selected culture conditions, most of the cells other than melanocytes have been eliminated and a nearly 100% pure population of melanocytes has been achieved, as confirmed by immunohistochemical analyses for melanocyte-specific markers, for example, Tyrosinase-1, S-100 and premelanosomal antigens. These melanocytes derived from the ORS were proliferating for up to 2 months. [ABSTRACT FROM AUTHOR]

Published

2010