Your search keyword '"Bidlingmaier, F."' showing total 10 results

1. Perspectives for personalized therapy for patients with multidrug-resistant tuberculosis.

Author

Lange, C., Alghamdi, W. A., Al‐Shaer, M. H., Brighenti, S., Diacon, A. H., DiNardo, A. R., Grobbel, H. P., Gröschel, M. I., von Groote‐Bidlingmaier, F., Hauptmann, M., Heyckendorf, J., Köhler, N., Kohl, T. A., Merker, M., Niemann, S., Peloquin, C. A., Reimann, M., Schaible, U. E., Schaub, D., and Schleusener, V.

Subjects

INDIVIDUALIZED medicine, MULTIDRUG resistance in bacteria, TUBERCULOSIS, DRUG dosage, MYCOBACTERIUM tuberculosis

Abstract

According to the World Health Organization (WHO), tuberculosis is the leading cause of death attributed to a single microbial pathogen worldwide. In addition to the large number of patients affected by tuberculosis, the emergence of Mycobacterium tuberculosis drug-resistance is complicating tuberculosis control in many high-burden countries. During the past 5 years, the global number of patients identified with multidrug-resistant tuberculosis (MDR-TB), defined as bacillary resistance at least against rifampicin and isoniazid, the two most active drugs in a treatment regimen, has increased by more than 20% annually. Today we experience a historical peak in the number of patients affected by MDR-TB. The management of MDR-TB is characterized by delayed diagnosis, uncertainty of the extent of bacillary drug-resistance, imprecise standardized drug regimens and dosages, very long duration of therapy and high frequency of adverse events which all translate into a poor prognosis for many of the affected patients. Major scientific and technological advances in recent years provide new perspectives through treatment regimens tailor-made to individual needs. Where available, such personalized treatment has major implications on the treatment outcomes of patients with MDR-TB. The challenge now is to bring these adances to those patients that need them most. [ABSTRACT FROM AUTHOR]

Published

2018

2. Direct comparison of liquid-based and smear-based cytology with and without rapid on-site evaluation for fine needle aspirates of thoracic tumors.

Author

Mfokazi, A., Wright, C.A., Louw, M., Von Groote‐Bidlingmaier, F., Schubert, P. T., Koegelenberg, C. F. N., and Diacon, A. H.

Published

2016

3. Differential mRNA Expression of the Two Mineralocorticoid Receptor Splice Variants Within the Human Brain: Structure Analysis of their Different DNA Binding Domains.

Author

Wickert, L., Selbig, J., Watzka, M., Stoffel-Wagner, B., Schramm, J., Bidlingmaier, F., and Ludwig, M.

Subjects

MINERALOCORTICOIDS, MESSENGER RNA, RNA splicing, DNA-protein interactions, BRAIN, CYTOCHEMISTRY

Abstract

Abstract In human brain tissue, cortisol action, at basal concentrations, is mediated by the mineralocorticoid receptor (MR). An in-frame insertion of 12 bp in the MR-DNA-binding domain due to alternative splice site usage between exons 3 and 4 results in an MR mRNA splice variant (MR+4) encoding a receptor protein with four additional amino acids compared to the wild-type MR protein. To elucidate the questions of sex, age, and/or tissue dependent differences of the relative amount of the two mRNA subtypes, we examined 131 fresh human brain tissue samples from temporal and frontal lobe or hippocampus. One hundred and twenty samples were obtained from patients with epilepsy and 11 samples from patients with brain tumours. A small but significant difference of the MR+4 mRNA splice variant proportions in cortex (9.5 ± 0.8%) and subcortical white matter (6.6 ± 0.7%) of the temporal lobe could be detected, indicating differential MR splice variant expression within these brain areas. Moreover, the splice variant ratios in samples of the temporal lobe cortex collected from patients with epilepsy differed from samples of patients with brain tumours. These data point to an altered expression of the MR splice variants in epilepsy, and strengthen the supposition of a tissue specific alternative splicing of the MR mRNA. The frequent occurence of the MR+4 transcript raises the question of its functional significance. For this reason, an MR+4 DNA-binding-domain structure model was generated by computer-based homology modelling based on the known glucocorticoid receptor structure. The data obtained revealed no distorting effect of the inserted four amino acids on the adjacent secondary structures, thereby suggesting that both zinc fingers retain their function. The resulting structure of the MR+4 model leads to the supposition that the receptor retains its function. Moreover, databank analysis with respect to this kind of steroid receptor variation and our own sequence data of the closely related progesterone receptor sustained the hypothesis that only corticosteroid receptors were affected by this alternative splicing event. [ABSTRACT FROM AUTHOR]

Published

2000

4. Evidence of 11 beta-hydroxylase deficiency in childhood adrenocortical tumors. The plasma corticosterone/11-deoxycorticosterone ratio as a possible marker for malignancy.

Author

Doerr, Helmuth G., Sippell, Wolfgang G., Drop, Stenvert L. S., Bidlingmaier, Frank, Knorr, Dieter, Doerr, H G, Sippell, W G, Drop, S L, Bidlingmaier, F, and Knorr, D

Published

1987

5. EFFECT OF DIFFERENT HUMAN GROWTH HORMONE PREPARATIONS ON NITROGEN RETENTION IN HYPOPITUITARY CHILDREN.

Author

BUTENANDT, O., BIDLINGMAIER, F., and KNORR, D.

Published

1974

6. HLA-A,B,C,DR typing and 17-OHP determination for second trimester prenatal diagnosis of 21-hydroxylase deficient CAH.

Author

Grosse-Wilde, H., Valentine-Thon, E., Vögeler, U., Passarge, E., Lorenzen, F., Sippell, W. G., Bidlingmaier, F., and Knorr, D.

Published

1988

7. Different Gene Defects in the Salt-Wasting (SW), Simple Virilizing (SV), and Nonclassical (NC) Types of Congenital Adrenal Hyperplasia (CAH).

Author

KNORR, D., ALBERT, E. D., BIDLINGMAIER, F., HÖLLER, W., and SCHOLZ, S.

Published

1985

8. A comparison of different methods for diagnosing acromegaly[ Presented].

Author

Stoffel-Wagner, B., Springer, W., Bidlingmaier, F., and Klingmüller, D.

Published

1997

9. How hydrocortisone substitution influences the quality of life and the bone metabolism of patients with secondary hypocortisolism.

Author

Wichers, M., Springer, W., Bidlingmaier, F., and Klingmüller, D.

Subjects

HYDROCORTISONE, BONE metabolism

Abstract

Background Even in the setting of chronic glucocorticoid substitution in hypocortisolaemic patients, severe side-effects will eventually occur when the dosage is inappropriately high. This study evaluates the effect of usual hydrocortisone substitution dosages on the well-being of the patients and on parameters of the bone metabolism to establish an optimum substitution dosage. Design In a double blind study nine patients with secondary hypocortisolism, being divided in three groups of three, received different doages of hydrocortisone (15, 20, 30 mg per day). Well-being was assessed using three different, validated questionnaires. Markers of bone metabolism were measured in blood and urine. Results The patients' quality of life was not impaired even at low dosages of hydrocortisone (15 or 20 mg per day). Of all laboratory parameters only osteocalcin significantly changed, decreasing at higher dosages. Conclusions Our study shows that a risk of bone loss may be avoided with a substitution dosage of 20 mg or even 15 mg hydrocortisone per day, without influencing the well-being of the patient. [ABSTRACT FROM AUTHOR]

Published

2000

10. Nachtrag zur Abhandlung: 'Über den Einfluss der Torsion bei den Ablenkungen eines hängenden Magneten'.

Author

Bidlingmaier, F.

Published

1905