Your search keyword '"Masjkur, J."' showing total 14 results

1. Plasma Steroid Profiling in Patients With Adrenal Incidentaloma

Author

Berke, Kristina, Constantinescu, Georgiana, Masjkur, J., Kimpel, Otilia, Dischinger, Ulrich, Peitzsch, M., Lenders, J.W.M., Fassnacht, M., Eisenhofer, G., Berke, Kristina, Constantinescu, Georgiana, Masjkur, J., Kimpel, Otilia, Dischinger, Ulrich, Peitzsch, M., Lenders, J.W.M., Fassnacht, M., and Eisenhofer, G.

Abstract

Item does not contain fulltext

Published

2022

2. Optimizing Genetic Workup in Pheochromocytoma and Paraganglioma by Integrating Diagnostic and Research Approaches

Author

Gieldon, L., William, D., Hackmann, K., Jahn, W., Jahn, A., Wagner, J., Rump, A., Bechmann, N., Nolting, S., Knosel, T., Gudziol, V., Constantinescu, G., Masjkur, J., Beuschlein, F., Timmers, H.J.L.M., Canu, L., Pacak, K., Robledo, M., Aust, D., Schrock, E., Eisenhofer, G., Richter, S., Klink, B., Gieldon, L., William, D., Hackmann, K., Jahn, W., Jahn, A., Wagner, J., Rump, A., Bechmann, N., Nolting, S., Knosel, T., Gudziol, V., Constantinescu, G., Masjkur, J., Beuschlein, F., Timmers, H.J.L.M., Canu, L., Pacak, K., Robledo, M., Aust, D., Schrock, E., Eisenhofer, G., Richter, S., and Klink, B.

Abstract

Contains fulltext : 206791.pdf (publisher's version ) (Open Access), Pheochromocytomas and paragangliomas (PPGL) are rare neuroendocrine tumors with a strong hereditary background and a large genetic heterogeneity. Identification of the underlying genetic cause is crucial for the management of patients and their families as it aids differentiation between hereditary and sporadic cases. To improve diagnostics and clinical management we tailored an enrichment based comprehensive multi-gene next generation sequencing panel applicable to both analyses of tumor tissue and blood samples. We applied this panel to tumor samples and compared its performance to our current routine diagnostic approach. Routine diagnostic sequencing of 11 PPGL susceptibility genes was applied to blood samples of 65 unselected PPGL patients at a single center in Dresden, Germany. Predisposing germline mutations were identified in 19 (29.2%) patients. Analyses of 28 PPGL tumor tissues using the dedicated PPGL panel revealed pathogenic or likely pathogenic variants in known PPGL susceptibility genes in 21 (75%) cases, including mutations in IDH2, ATRX and HRAS. These mutations suggest sporadic tumor development. Our results imply a diagnostic benefit from extended molecular tumor testing of PPGLs and consequent improvement of patient management. The approach is promising for determination of prognostic biomarkers that support therapeutic decision-making.

Published

2019

3. Adrenomedullary function, obesity and permissive influences of catecholamines on body mass in patients with chromaffin cell tumours

Author

An, Yaxin, Reimann, M., Masjkur, J., Langton, K., Peitzsch, M., Deutschbein, Timo, Lenders, J., Bornstein, S.R., Eisenhofer, G., An, Yaxin, Reimann, M., Masjkur, J., Langton, K., Peitzsch, M., Deutschbein, Timo, Lenders, J., Bornstein, S.R., and Eisenhofer, G.

Abstract

Item does not contain fulltext

Published

2019

4. Pheochromocytoma and paraganglioma: clinical feature-based disease probability in relation to catecholamine biochemistry and reason for disease suspicion

Author

Geroula, Aikaterini, Deutschbein, Timo, Langton, K., Masjkur, J., Pamporaki, C., Peitzsch, M., Timmers, H.J.L.M., Lenders, J.W.M., Eisenhofe, Graeme, Geroula, Aikaterini, Deutschbein, Timo, Langton, K., Masjkur, J., Pamporaki, C., Peitzsch, M., Timmers, H.J.L.M., Lenders, J.W.M., and Eisenhofe, Graeme

Abstract

Item does not contain fulltext

Published

2019

5. Streptozotocin-induced β-cell damage, high fat diet, and metformin administration regulate Hes3 expression in the adult mouse brain

Author

Nikolakopoulou, P. Chatzigeorgiou, A. Kourtzelis, I. Toutouna, L. Masjkur, J. Arps-Forker, C. Poser, S.W. Rozman, J. Rathkolb, B. Aguilar-Pimentel, J.A. Becker, L. Klopstock, T. Treise, I. Busch, D.H. Beckers, J. Moreth, K. Bekeredjian, R. Garrett, L. Hölter, S.M. Zimprich, A. Wurst, W. Brommage, R. Amarie, O. Graw, J. Calzada-Wack, J. Neff, F. Zimmer, A. Östereicher, M. Steinkamp, R. Lengger, C. Maier, H. Stoeger, C. Leuchtenberger, S. Wolf, E. Klingenspor, M. Ollert, M. Schmidt-Weber, C. Fuchs, H. Gailus-Durner, V. Hrabe de Angelis, M. Tsata, V. Monasor, L.S. Troullinaki, M. Witt, A. Anastasiou, V. Chrousos, G. Yi, C.-X. García-Cáceres, C. Tschöp, M.H. Bornstein, S.R. Androutsellis-Theotokis, A. German Mouse Clinic Consortium

Abstract

Diabetes mellitus is a group of disorders characterized by prolonged high levels of circulating blood glucose. Type 1 diabetes is caused by decreased insulin production in the pancreas whereas type 2 diabetes may develop due to obesity and lack of exercise; it begins with insulin resistance whereby cells fail to respond properly to insulin and it may also progress to decreased insulin levels. The brain is an important target for insulin, and there is great interest in understanding how diabetes affects the brain. In addition to the direct effects of insulin on the brain, diabetes may also impact the brain through modulation of the inflammatory system. Here we investigate how perturbation of circulating insulin levels affects the expression of Hes3, a transcription factor expressed in neural stem and progenitor cells that is involved in tissue regeneration. Our data show that streptozotocin-induced β-cell damage, high fat diet, as well as metformin, a common type 2 diabetes medication, regulate Hes3 levels in the brain. This work suggests that Hes3 is a valuable biomarker helping to monitor the state of endogenous neural stem and progenitor cells in the context of diabetes mellitus. © 2018, The Author(s).

Published

2018

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Author

Nikolakopoulou, P. Chatzigeorgiou, A. Kourtzelis, I. Toutouna, L. Masjkur, J. Arps-Forker, C. Poser, S.W. Rozman, J. Rathkolb, B. Aguilar-Pimentel, J.A. Becker, L. Klopstock, T. Treise, I. Busch, D.H. Beckers, J. Moreth, K. Bekeredjian, R. Garrett, L. Hölter, S.M. Zimprich, A. Wurst, W. Brommage, R. Amarie, O. Graw, J. Calzada-Wack, J. Neff, F. Zimmer, A. Östereicher, M. Steinkamp, R. Lengger, C. Maier, H. Stoeger, C. Leuchtenberger, S. Wolf, E. Klingenspor, M. Ollert, M. Schmidt-Weber, C. Fuchs, H. Gailus-Durner, V. Hrabe de Angelis, M. Tsata, V. Monasor, L.S. Troullinaki, M. Witt, A. Anastasiou, V. Chrousos, G. Yi, C.-X. García-Cáceres, C. Tschöp, M.H. Bornstein, S.R. Androutsellis-Theotokis, A. German Mouse Clinic Consortium and Nikolakopoulou, P. Chatzigeorgiou, A. Kourtzelis, I. Toutouna, L. Masjkur, J. Arps-Forker, C. Poser, S.W. Rozman, J. Rathkolb, B. Aguilar-Pimentel, J.A. Becker, L. Klopstock, T. Treise, I. Busch, D.H. Beckers, J. Moreth, K. Bekeredjian, R. Garrett, L. Hölter, S.M. Zimprich, A. Wurst, W. Brommage, R. Amarie, O. Graw, J. Calzada-Wack, J. Neff, F. Zimmer, A. Östereicher, M. Steinkamp, R. Lengger, C. Maier, H. Stoeger, C. Leuchtenberger, S. Wolf, E. Klingenspor, M. Ollert, M. Schmidt-Weber, C. Fuchs, H. Gailus-Durner, V. Hrabe de Angelis, M. Tsata, V. Monasor, L.S. Troullinaki, M. Witt, A. Anastasiou, V. Chrousos, G. Yi, C.-X. García-Cáceres, C. Tschöp, M.H. Bornstein, S.R. Androutsellis-Theotokis, A. German Mouse Clinic Consortium

Published

2018

7. Biochemical Diagnosis of Chromaffin Cell Tumors in Patients at High and Low Risk of Disease: Plasma versus Urinary Free or Deconjugated O-Methylated Catecholamine Metabolites

Author

Eisenhofer, G., Prejbisz, A., Peitzsch, M., Pamporaki, C., Masjkur, J., Rogowski-Lehmann, Natalie, Timmers, H.J.L.M., Januszewicz, A., Lenders, J.W.M., Eisenhofer, G., Prejbisz, A., Peitzsch, M., Pamporaki, C., Masjkur, J., Rogowski-Lehmann, Natalie, Timmers, H.J.L.M., Januszewicz, A., and Lenders, J.W.M.

Abstract

Item does not contain fulltext

Published

2018

8. Hypertensive crisis in pregnancy due to a metamorphosing pheochromocytoma with postdelivery Cushing's syndrome

Author

Langton, K., Gruber, M., Masjkur, J., Steenblock, C., Peitzsch, M., Meinel, J., Lenders, J., Bornstein, S., Eisenhofer, G., Langton, K., Gruber, M., Masjkur, J., Steenblock, C., Peitzsch, M., Meinel, J., Lenders, J., Bornstein, S., and Eisenhofer, G.

Abstract

Item does not contain fulltext, Pheochromocytomas in pregnancy are rare but potentially lethal. Even rarer is the combination of pheochromocytoma in pregnancy with subsequent development of ectopic Cushing's syndrome. We report a 36-year-old woman, previously diagnosed with essential hypertension, who developed severe hypertension in pregnancy complicated by insulin-dependent gestational diabetes. A cesarean section was performed at 32 weeks following a hypertensive crisis after routine administration of betamethasone. Postnatal persistence of signs and symptoms of catecholamine excess led to the diagnosis of a left adrenal pheochromocytoma. Between diagnosis and planned tumor removal, the patient developed signs and symptoms of Cushing's syndrome (facial edema and hirsutism, myopathy and fatigue). Biochemical testing confirmed hypercortisolism with extremely elevated levels of plasma adrenocorticotropin, urinary cortisol and multiple steroids of a plasma panel that were all normal at previous testing. The previously noradrenergic tumor also started producing epinephrine. Histopathological examination confirmed the pheochromocytoma, which was also immunohistochemically positive for adrenocorticotropin. Full post-surgical recovery was sustained with normal blood pressure and biochemical findings after one year. This report not only underlines the chameleon behavior of pheochromocytoma but also illustrates its potential for a metamorphosing presentation. Corticosteroid administration in pregnancy requires a cautious approach in patients with hypertension.

Published

2018

9. STAT3-Ser/Hes3 Signaling: A New Molecular Component of the Neuroendocrine System?

Author

Nikolakopoulou, P. Poser, S. W. Masjkur, J. de Celis, M. Fernandez Rubin Toutouna, L. Andoniadou, C. L. McKay, R. D. and Chrousos, G. Ehrhart-Bornstein, M. Bornstein, S. R. and Androutsellis-Theotokis, A.

Abstract

The endocrine system involves communication among different tissues in distinct organs, including the pancreas and components of the Hypothalamic-Pituitary-Adrenal Axis. The molecular mechanisms underlying these complex interactions are a subject of intense study as they may hold clues for the progression and treatment of a variety of metabolic and degenerative diseases. A plethora of signaling pathways, activated by hormones and other endocrine factors have been implicated in this communication. Recent advances in the stem cell field introduce a new level of complexity: adult progenitor cells appear to utilize distinct signaling pathways than the more mature cells in the tissue they co-reside. It is therefore important to elucidate the signal transduction requirements of adult progenitor cells in addition to those of mature cells. Recent evidence suggests that a common non-canonical signaling pathway regulates adult progenitors in several different tissues, rendering it as a potentially valuable starting point to explore their biology. The STAT3-Ser/Hes3 Signaling Axis was first identified as a major regulator of neural stem cells and, subsequently, cancer stem cells. In the endocrine/neuroendocrine system, this pathway operates on several levels, regulating other types of plastic cells: (a) it regulates pancreatic islet cell function and insulin release; (b) insulin in turn activates the pathway in broadly distributed neural progenitors and possibly also hypothalamic tanycytes, cells with important roles in the control of the adrenal gland; (c) adrenal progenitors themselves operate this pathway. The STAT3-Ser/Hes3 Signaling Axis therefore deserves additional research in the context of endocrinology.

Published

2016

10. Reference intervals for plasma concentrations of adrenal steroids measured by LC-MS/MS: Impact of gender, age, oral contraceptives, body mass index and blood pressure status

Author

Eisenhofer, G., Peitzsch, M., Kaden, D., Langton, K., Pamporaki, C., Masjkur, J., Tsatsaronis, G., Mangelis, A., Williams, T.A., Reincke, M., Lenders, J.W.M., Bornstein, S.R., Eisenhofer, G., Peitzsch, M., Kaden, D., Langton, K., Pamporaki, C., Masjkur, J., Tsatsaronis, G., Mangelis, A., Williams, T.A., Reincke, M., Lenders, J.W.M., and Bornstein, S.R.

Abstract

Contains fulltext : 174653.pdf (Publisher’s version ) (Open Access), BACKGROUND: Mass spectrometric-based measurements of the steroid metabolome have been introduced to diagnose disorders featuring abnormal steroidogenesis. Defined reference intervals are important for interpreting such data. METHODS: Liquid chromatography-tandem mass spectrometry was used to establish reference intervals for 16 steroids (pregnenolone, progesterone, 11-deoxycorticosterone, corticosterone, aldosterone, 18-oxocortisol, 18-hydroxycortisol, 17-hydroxyprogesterone, 21-deoxycortisol, 11-deoxycortisol, cortisol, cortisone, dehydroepiandrosterone, dehydroepiandrosterone-sulfate, androstenedione, testosterone) measured in plasma from 525 volunteers with (n=227) and without (n=298) hypertension, including 68 women on oral contraceptives. RESULTS: Women showed variable plasma concentrations of several steroids associated with menstrual cycle phase, menopause and oral contraceptive use. Progesterone was higher in females than males, but most other steroids were higher in males than females and almost all declined with advancing age. Using models that corrected for age and gender, body mass index showed weak negative relationships with corticosterone, 21-deoxycortisol, cortisol, cortisone, testosterone, progesterone, 17-hydroxyprogesterone and 11-deoxycorticosterone, but a positive relationship with 18-hydroxycortisol. Hypertensives and normotensives showed negligible differences in plasma concentrations of steroids. CONCLUSION: Age and gender are the most important variables for plasma steroid reference intervals, which have been established here according to those variables for a panel of 16 steroids primarily useful for diagnosis and subtyping of patients with endocrine hypertension.

Published

2017

11. STAT3-Ser/Hes3 signaling: a new molecular component of the neuroendocrine system?

Author

Nikolakopoulou, P., Poser, S.W., Masjkur, J., Fernandez Rubin de Celis, M., Toutouna, L., Andoniadou, C.L., McKay, R.D., Chrousos, G., Ehrhart-Bornstein, M., Bornstein, S.R., Androutsellis-Theotokis, A., Nikolakopoulou, P., Poser, S.W., Masjkur, J., Fernandez Rubin de Celis, M., Toutouna, L., Andoniadou, C.L., McKay, R.D., Chrousos, G., Ehrhart-Bornstein, M., Bornstein, S.R., and Androutsellis-Theotokis, A.

Abstract

The endocrine system involves communication among different tissues in distinct organs, including the pancreas and components of the Hypothalamic- Pituitary-Adrenal Axis. The molecular mechanisms underlying these complex interactions are a subject of intense study as they may hold clues for the progression and treatment of a variety of metabolic and degenerative diseases. A plethora of signaling pathways, activated by hormones and other endocrine factors have been implicated in this communication. Recent advances in the stem cell field introduce a new level of complexity: adult progenitor cells appear to utilize distinct signaling pathways than the more mature cells in the tissue they co-reside. It is therefore important to elucidate the signal transduction requirements of adult progenitor cells in addition to those of mature cells. Recent evidence suggests that a common non-canonical signaling pathway regulates adult progenitors in several different tissues, rendering it as a potentially valuable starting point to explore their biology. The STAT3- Ser/Hes3 Signaling Axis was first identified as a major regulator of neural stem cells and, subsequently, cancer stem cells. In the endocrine/neuroendocrine system, this pathway operates on several levels, regulating other types of plastic cells: (a) it regulates pancreatic islet cell function and insulin release; (b) insulin in turn activates the pathway in broadly distributed neural progenitors and possibly also hypothalamic tanycytes, cells with important roles in the control of the adrenal gland; (c) adrenal progenitors themselves operate this pathway. The STAT3-Ser/Hes3 Signaling Axis therefore deserves additional research in the context of endocrinology.

12. Plasma Steroid Profiles in Subclinical Compared With Overt Adrenal Cushing Syndrome

Author

Felix Beuschlein, Katharina Langton, Guido Di Dalmazi, Matthias Gruber, Stefan R. Bornstein, Graeme Eisenhofer, Julia Fazel, Stephanie Zopp, Martin Reincke, Denise Kaden, Mirko Peitzsch, Martin Bidlingmaier, Jimmy Masjkur, Masjkur J., Gruber M., Peitzsch M., Kaden D., Di Dalmazi G., Bidlingmaier M., Zopp S., Langton K., Fazel J., Beuschlein F., Bornstein S.R., Reincke M., and Eisenhofer G.

Subjects

Cortisol secretion, Male, medicine.medical_specialty, Hypothalamo-Hypophyseal System, Endocrinology, Diabetes and Metabolism, Clinical Biochemistry, Dehydroepiandrosterone, 030209 endocrinology & metabolism, Context (language use), Biochemistry, Sensitivity and Specificity, Severity of Illness Index, Statistics, Nonparametric, Hospitals, University, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, Adrenocorticotropic Hormone, Reference Values, Tandem Mass Spectrometry, Internal medicine, Germany, Severity of illness, medicine, Humans, Subclinical Hypercortisolism, steroidomics, Cushing Syndrome, Dexamethasone, 030304 developmental biology, Subclinical infection, Retrospective Studies, 0303 health sciences, business.industry, Biochemistry (medical), Retrospective cohort study, 3. Good health, Cross-Sectional Studies, ROC Curve, Multivariate Analysis, Pregnenolone, Female, Steroids, business, Switzerland, medicine.drug, Chromatography, Liquid

Abstract

Context Diagnosis of subclinical adrenal hypercortisolism is based on several tests of the hypothalamic-pituitary-adrenal axis to establish mild alterations of cortisol secretion and dysregulated cortisol physiology. Objective We assessed whether plasma steroid profiles might assist diagnosis of subclinical Cushing syndrome (SC). Design Retrospective cross-sectional study. Setting Two tertiary medical centers. Patients Of 208 patients tested for hypercortisolism, disease was excluded in 152 and confirmed in 21 with overt adrenal Cushing syndrome (AC) compared to 35 with SC. Another 277 age- and sex-matched hypertensive and normotensive volunteers were included for reference. Main Outcome Measures A panel of 15 plasma steroids was measured by mass spectrometry, with classification by discriminant analysis. Results Patients with SC had lower plasma concentrations of dehydroepiandrosterone and dehydroepiandrosterone-sulfate than subjects without SC (P < 0.05). The largest increases (P < 0.001) in plasma steroids among patients with SC were observed for 11-deoxycortisol and 11-deoxycorticosterone. Nevertheless, concentrations of 11-deoxycorticosterone, 11-deoxycortisol, and pregnenolone in patients with AC were higher (P < 0.05) than in those with SC. Patients with SC or AC could be distinguished from subjects without disease using this combination of steroids as precisely as with use of measurements of serum cortisol after administration of dexamethasone. The steroid combination provided superior diagnostic performance compared with each of the other routine biochemical tests. Conclusion Distinct plasma steroid profiles in patients with SC may provide a simple and reliable screening method for establishing the diagnosis.

Published

2018

13. PTBP1 is required for embryonic development before gastrulation.

Author

Suckale J, Wendling O, Masjkur J, Jäger M, Münster C, Anastassiadis K, Stewart AF, and Solimena M

Subjects

Animals, Blastocyst metabolism, Blastocyst physiology, Cell Differentiation genetics, Cell Division genetics, Embryo, Mammalian, Female, Gastrulation physiology, Gene Expression Regulation, Developmental, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Models, Biological, Polypyrimidine Tract-Binding Protein genetics, Pregnancy, Time Factors, Embryonic Development genetics, Gastrulation genetics, Polypyrimidine Tract-Binding Protein physiology

Abstract

Polypyrimidine-tract binding protein 1 (PTBP1) is an important cellular regulator of messenger RNAs influencing the alternative splicing profile of a cell as well as its mRNA stability, location and translation. In addition, it is diverted by some viruses to facilitate their replication. Here, we used a novel PTBP1 knockout mouse to analyse the tissue expression pattern of PTBP1 as well as the effect of its complete removal during development. We found evidence of strong PTBP1 expression in embryonic stem cells and throughout embryonic development, especially in the developing brain and spinal cord, the olfactory and auditory systems, the heart, the liver, the kidney, the brown fat and cartilage primordia. This widespread distribution points towards a role of PTBP1 during embryonic development. Homozygous offspring, identified by PCR and immunofluorescence, were able to implant but were arrested or retarded in growth. At day 7.5 of embryonic development (E7.5) the null mutants were about 5x smaller than the control littermates and the gap in body size widened with time. At mid-gestation, all homozygous embryos were resorbed/degraded. No homozygous mice were genotyped at E12 and the age of weaning. Embryos lacking PTBP1 did not display differentiation into the 3 germ layers and cavitation of the epiblast, which are hallmarks of gastrulation. In addition, homozygous mutants displayed malformed ectoplacental cones and yolk sacs, both early supportive structure of the embryo proper. We conclude that PTBP1 is not required for the earliest isovolumetric divisions and differentiation steps of the zygote up to the formation of the blastocyst. However, further post-implantation development requires PTBP1 and stalls in homozygous null animals with a phenotype of dramatically reduced size and aberration in embryonic and extra-embryonic structures.

Published

2011

14. Tamoxifen-independent recombination in the RIP-CreER mouse.

Author

Liu Y, Suckale J, Masjkur J, Magro MG, Steffen A, Anastassiadis K, and Solimena M

Subjects

Animals, Mice, Integrases genetics, Recombination, Genetic, Tamoxifen pharmacology

Abstract

Background: The inducible Cre-lox system is a valuable tool to study gene function in a spatial and time restricted fashion in mouse models. This strategy relies on the limited background activity of the modified Cre recombinase (CreER) in the absence of its inducer, the competitive estrogen receptor ligand, tamoxifen. The RIP-CreER mouse (Tg (Ins2-cre/Esr1) 1Dam) is among the few available β-cell specific CreER mouse lines and thus it has been often used to manipulate gene expression in the insulin-producing cells of the endocrine pancreas., Principal Findings: Here, we report the detection of tamoxifen-independent Cre activity as early as 2 months of age in RIP-CreER mice crossed with three distinct reporter strains., Significance: Evidence of Cre-mediated recombination of floxed alleles even in the absence of tamoxifen administration should warrant cautious use of this mouse for the study of pancreatic β-cells.

Published

2010