Your search keyword '"H, Lehnert"' showing total 21 results

1. Phäochromozytom

Author

H. Lehnert

Subjects

business.industry, Medicine, business

Published

2015

2. Autorenverzeichnis

Author

W. Domschke, M. Berger, W. Hohenberger, T. Meinertz, C. Vogelmeier, T. Sauerbruch, H.J. Kramer, S.C. Müller, H. Serve, M.M. Weber, B. Göke, J.R. Kalden, B. Manger, W. Rascher, B. Appenrodt, J. Atta, C. Auernhammer, I.B. Autenrieth, W. Avenhaus, M. Backmund, C. Bausewein, J. Behr, A. Behrens, R. Berner, F. Berr, N. Blank, E. Blind, M. Bockhorn, D. Bokemeyer, M. Böhm, G. Bönner, G.D. Borasio, K. Bork, J. Braun, H.-P. Bruch, T.H. Brümmendorf, U. Brunnberg, M. Brüwer, M.W. Büchler, C. Detter, S. Diederich, C. Diehm, J. Distler, D. Domagk, T. Dörner, H.-G. Dörr, H. Dralle, M. Dreyling, I. Ehlebracht-König, C. Ell, W. Enzensberger, H.-J. Epple, M. Fassnacht, H. Feußner, P. Fiegel, C. Fisang, D. Filipas, W. Fischbach, C.H. Flamme, J. Floege, U.R. Fölsch, C. Fottner, W. Frank, N. Frey, K. Friese, A. Frilling, M. Fröhner, P. Frühmorgen, P.R. Galle, S. Geidel, E. Genth, A. Gingelmaier, F.-D. Goebel, N. Gökbuget, R. Göke, K. Grabitz, M. Grünke, S. Hahner, W. Handrick, C. Hasslacher, E. Heidbreder, W. Heindel, V. Heinemann, J. Heitmann, H.W. Heiß, H. Hof, L. Hering, E. Hiller, A. Hirner, W.-K. Hofmann, E. Holler, A.H. Hölscher, G. Holtmann, J. Hölzen, J. Honegger, S. Hörle, K. Hörmann, R. Hörmann, I. Hornke, R.M. Huber, J. Hübner, R. Hummel, S. Irmscher, T. Jelinek, S. Jonas, E. Jost, H.H. Jung, G.J. Kahaly, M. Karaus, S. Katsoulis, H. Katus, H.P. Kessler, K. Kiehne, W. Kiess, M. Kindermann, Y. von Kodolitsch, H. Köhler, L. Köhler, M. Köhler, E. Kohne, H.-J. Kolb, J. Köninger, K. Koop, R. Köster, I. Kötter, H.J.J. Kramer, B. Kremer, P. Kroll, J.G. Kuipers, F. Lammert, M. Langer, M. Laukötter, H. Lehnert, B. Lembcke, M.M. Lerch, S. Liebe, A. Lieber, R. Loddenkemper, M. Löhr, H.-M. Lorenz, J. Lorenz, T. Löscher, M. Luster, G. Lux, K. Mann, J. Mayerle, U. Merle, H.-J. Meyer, C. Möbius, M. Moehler, H. Mönnikes, J. Mössner, S.A. Müller, T.J. Musholt, J. Nattermann, M. Neubrand, P. Neuhaus, B. Neundörfer, T. Nicolai, J. Nolde, H. Olschewski, J. Ostermeyer, C. Ott, S. Pahernik, U. Pankratius, K.G. Parhofer, B. Passlick, O. Pech, B. Pfaffenbach, T. Pfeiffer, A. Pilatz, T. Pohle, A. Pohl-Koppe, Katharina A. Ponto, H. Prange, A. Pruß, J. Rädle, B. Rauch, F. Raue, C. Reichel, C. Reindl, C. Reißfelder, Dipl.-Phys. J. Rendl, E. Rietschel, E. Rijcken, R. Roos, G. Rudofsky†, W. Samtleben, W. Sandmann, G. Sauter, K.P. Schaal, J.R. Schaefer, U. Schäfer-Graf, W. Schepp, M. Schlemmer, S. Schliep, H. Schmidt, B. Schmied, W. Schmiegel, A. Schießl, A. Schmid, A. Schneider, T. Schneider, J. Schölmerich, H. Scholz, U. Schönermarck, J. Schopohl, H. Schrezenmeier, H. Schulze-Koops, D. Schuppan, V. Schuster, G. Schüßler, O. Schwandner, T.F. Schwarz, R. Secknus, N. Senninger, O. Sezer, B.R. Simmen, U. Spengler, U. Stabenow-Lohbauer, R. Stebler, D. Steven, M. Sticherling, U. Strauch, C. Stremmel, W. Stremmel, B.A. Stuck, H. Stürz, C. Taube, O. Thulesius, K. Thurau, J.W. Thüroff, C. Tomiak, W. Uhl, D. Vallböhmer, T. Vogel, P. von den Driesch, F.M.E. Wagenlehner, A. Wagner, U. Wagner, K. Weber, W. Weidner, T. Weinke, B.T. Weis-Müller, M. Weiß, S. Willems, U. Wintergerst, M. Wirth, G.W. Wolkersdörfer, and M. Zeitz

Published

2011

3. Autorenverzeichnis

Author

V. Andresen, J. Angenendt, C. Anthoni, B. Appenrodt, M. Arbogast, G. Arco, J. Atta, M. Auer, C. Auernhammer, I.B. Autenrieth, W. Avenhaus, R. Bachem, M. Backmund, D. Bänsch, A. Ballauff, J. Baltzer, J. Barth, A. Batra, M.A. Bazarra-Castro, S. Beck, K. Becker, Karsten Becker, J. Behr, A. Behrens, O. Belyaev, Ch. Bender-Götze, J. Bengel, M. Benz, von Haunerschen, J. Berberich, M. Berger, R. Berner, F. Berr, null S.C., N. Blank, C. Bleh, Eberhard Blind, H.E. Blum, N. Bock, M. Bockhorn, J. Böhler, M. Böhm, D. Bokemeyer, G. Bönner, K. Bork, G. Born, Thomas Brandt, J. Braun, H.-P. Bruch, T.H. Brümmendorf, M. Brüwer, U. Brunnberg, M. Buchfelder, G. Buchkremer, M.W. Büchler, H.-D. Carl, S. Castell, C. Daniels, S. Daum, C. Detter, G. Deuschl, E. Dieckmann, S. Diederich, C. Diehm, T. Diemer, H.C. Diener, H. Diepolder, J. Distler, T. Dörner, null Prof. Dr., D. Domagk, W. Domschke, A. Dragu, H. Dralle, M. Dreyling, P. van, T. Dürk, D. Ebert, I. Ehlebracht-König, C.E. Elger, C. Ell, J. Ellinger, G. Emons, O. Engel, W. Enzensberger, H.-J. Epple, R. Erbel, M. Fassnacht, Hubertus Feußner, M. Fichter, P. Fiegel, D. Filipas, C. Fisang, M. Fisch, W. Fischbach, N. Fischer, M. Fischer, C.H. Flamme, K. Fleckenstein, J. Floege, G. Fluhr, U.R. Fölsch, M. Forsting, C. Fottner, W. Frank, N. Frey, H. Freyberger, K. Friese, A. Frilling, PD. Dr. habil, U. Frommberger, P. Frühmorgen, Johannes Fuss, R. Gätje, P.R. Galle, S. Geidel, H.-Ch. Geiß, Ekkehard Genth, J.M. Gilsbach, A. Gingelmaier, F.-D. Goebel, J. Göhl, N. Gökbuget, R. Gold, M.A. Gonzalez-Carmona, F. Gossé, K. Grabitz, M. Greetfeld, F.A. Gries, I. Grosch-Wörner, N. Grüner, M. Grünke, A. Grüters-Kieslich, V. Gülberg, T. Haak, R. Häfner, M. Härter, T. Hagenacker, S. Hahn, S. Hahner, G. Haidl, M. Hammer, F. Hammersen, W. Handrick, F. Hanisch, M.P. Hansen, Sara Hanke, J. Haschka, C. Hasslacher, Th. Hauer, A. Hauptmann, M. Heckmann, E. Heidbreder, U. Heim, W. Heindel, J. Heitmann, U. Hegenbart, W. Hermann, J.M. Herrmann, B. Herpertz-Dahlmann, B. Heßlinger, D. Heuß, P. Heußner, E. Hiller, A. Hirner, A.H. Hölscher, J. Hölzen, W.H. Hörl†, S. Hörle, H. Hof, W.-K. Hofmann, W. Hohenberger, U. Hohenfellner, E. Holler, G. Holtmann, J. Honegger, H.C. Hopf, R.E. Horch, I. Hornke, T. Hornung, R.M. Huber, A. Hueber, J. Hübner, R. Hummel, S. Irmscher, O.E. Janßen, T. Jelinek, K.A. Jendrissek, S. Jonas, E. Jost, H.H. Jung, G.J. Kahaly, J.R. Kalden, J. Kalff, T. Kapellen, M. Karaus, O. Kastrup, S. Katsoulis, H. Katus, C.P. Kaudel, R. Kaulitz, C. Keck, F. Keller, S. Kellnar, K. Kiehne, W. Kiess, M. Kindermann, A. Kirschbaum, M. Klein, A. Kleindienst, C. Kneitz, Y. von Kodolitsch, D. Köhler, H.P. Kessler, G. Köhler, H. Köhler, L. Köhler, M. Köhler, M. Köhnke, C. Königs, J. Köninger, D. Könsgen-Mustea, R. Köster, I. Kötter, E. Kohne, H.-J. Kolb, S. Koletzko, R. Kollmar, S. Konstantinidis, K. Koop, H.G. Kopp, T. Koschinsky, H.J. Kramer, J. Krauss, M.E. Kreis, B. Kremer, H.K. Kroemer, B. Kröner-Herwig, P. Kroll, A.K. Külz, H. Kuhl, J.G. Kuipers, M. Laaser, U. Lamla, F. Lammert, M. Langer, M. Laß, M. Laukötter, P. Layer, M. Leffler, H. Lehnert, M. Lehrke, B. Lembcke, M.M. Lerch, S. Liebe, A. Lieber, V. Limmroth, H. Lochs, R. Loddenkemper, J.-M. Löhr, T. Löscher, A. Loh, H.-M. Lorenz, J. Lorenz, N. Lügering, M. Luster, G. Lux, O. Luzar, A. Maercker, K. Magdorf, P. Mallmann, T. Marth, K. May, J. Mayerle, T. Meinertz, V. Melichar, U. Merle, H.J. Meyer, Th. Meyer, H. Meyer-Lehnert, A. Meyer-Marcotty, H. Michels, C. Möbius, G. Möddel, M. Möhler, H. Mönnikes, J. Mössner, M.G. Mohaupt, S.C. Müller, S.A. Müller, S. Müller-Lissner, J. Müller-Quernheim, A. Muntau, T.J. Musholt, W. Nacimiento, J. Nattermann, G. Nelles, M. Neubrand, C. Neuhäuser, P. Neuhaus, P.-A. Neumann, B. Neundörfer, T. Nicolai, W.-B. Niebling, T. Niehues, G. Nilius, J. Nolde, J. Noth, H. Olschewski, J. Ostermeyer, C. Ott, S. Pahernik, D. Palmes, U. Pankratius, K. Parhofer, R. Paschke, B. Passlick, O. Pech, F.W. Pelster, E.E. Petersen, E. Petri, B. Pfaffenbach, M. Pfeifer, T. Pfeiffer, H.W. Pfister, null Diplom-Gesundheitswirt, J. Pickel, A. Pilatz, M. Pirlich, E. Polykandriotis, B. Pontz, K. Possinger, A. Pohl-Koppe, T. Pohle, H. Prange, A. Prasse, A. Pruß, J. Rädle, K. Raile, W. Randerath, W. Rascher, B. Rauch, F. Raue, B. Raziorruh, J. Rech, A.C. Regierer, C. Reichel, C. Reindl, D. Reinhardt, C. Reißfelder, J. Rendl, M. Reuss-Borst, P. Rieckmann, C. Riedner, E. Rietschel, E. Rijcken, M. Rister, K. Rödder, S. Rogenhofer, F.C. Roos, R. Roos, D. Rosskopf, S. Rudnik-Schöneborn, G. Rudofsky†, M. Ruhnke, M. Ruß, C.F. Rust, F. Saborowski, M. Sailer, M. Sedigh Salakdeh, Walter Samtleben, W. Sandmann, T. Sauerbruch, K.P. Schaal, G. Schackert, U. Schäfer-Graf, M. Schäfers, A. Schalhorn, W. Schepp, J. Schetelig, M. Schifferdecker, J. Schipper, A. Schießl, U. Schlegel, S. Schliep, A. Schmid, P. Schmid, F. Schmidt, B. Schmied, W. Schmiegel, A. Schneider, T. Schneider, C. Schneider-Gold, H.-G. Schnürch, J. Schölmerich, U. Schönermarck, B. Schönhofer, S. Schönland, H. Scholz, J. Schopohl, G. Schott, J. Schrader, A. Schraml, H. Schrezenmeier, A. Schuchert, G. Schüßler, H. Schulze-Koops, D. Schuppan, V. Schuster, S. Schwab, O. Schwandner, C.H.M. Schwarz, T.F. Schwarz, K.W. Schweppe, R. Secknus, S.E. Segerer, N. Senninger, H. Serve, U. Seybold, O. Sezer, B. Siegmund, W. Siegmund, G. Siemon, B.R. Simmen, G. Simonetti, C. Sommer, U. Spengler, H. Sprott, U. Stabenow-Lohbauer, M. Stahl, G. Stalla, A. Stallmach, T. Stammschulte, R. Stebler, R. Stein, D. Steven, M. Sticherling, M. Stöhr, U. Strauch, A. Strauss, H.-G. Strauß, C. Stremmel, W. Stremmel, M. Strupp, E. Stüber, H. Stürz, U. Sure, B. Swoboda, C. Taube, K. Thiel, C. Thomssen, K. Thurau, J. Thöne, J. Thüroff, C. Tomiak, K.V. Toyka, H. Tröger, R.M. Trüeb, M. Tryba, W. Uhl, H. Ullerich, L. Unger, D. Vallböhmer, D. van Calker, T. Vloet, U. Voderholzer, Thomas M.K. Völkl, T. Vogel, P. Vogt, F.E.M. Wagenlehner, A. Wagner, U. Wagner, V. Wahn, C.W. Wallesch, F. Watzka, K. Weber, L. Weber, M.M. Weber, T. Wehrmann, W. Weidner, T. Weinke, M. Weiß, B.T. Weis-Müller, Michael Weller, F. Wenz, K. Werdan, M. Wettstein, M. Wick, I. Wiegratz, S. Willems, H. Wilke, U. Wintergerst, M. Wirth, G.W. Wolkersdörfer, C. Wüster, F. Zabel, H. Zeidler, M. Zeitz, K. Zerres, G. Ziemer, S. Zierz, T. Zimmermann, and J. Zwerina

Published

2007

4. Familial hypercholesterolemia in primary care in Germany. Diabetes and cardiovascular risk evaluation: Targets and Essential Data for Commitment of Treatment (DETECT) study.

Author

Schmidt N, Schmidt B, Dressel A, Gergei I, Klotsche J, Pieper L, Scharnagl H, Kleber ME, März W, Lehnert H, Pittrow D, Stalla G, Wittchen HU, and Grammer TB

Subjects

Adult, Analysis of Variance, Biomarkers blood, Cardiovascular Diseases diagnosis, Cardiovascular Diseases prevention & control, Chi-Square Distribution, Diabetes Mellitus diagnosis, Diabetes Mellitus prevention & control, Female, Germany epidemiology, Humans, Hyperlipoproteinemia Type II blood, Hyperlipoproteinemia Type II diagnosis, Hyperlipoproteinemia Type II therapy, Lipids blood, Male, Middle Aged, Predictive Value of Tests, Prevalence, Prognosis, Reproducibility of Results, Risk Assessment, Risk Factors, Cardiovascular Diseases epidemiology, Diabetes Mellitus epidemiology, Hyperlipoproteinemia Type II epidemiology, Primary Health Care

Abstract

Background and Aims: Familial hypercholesterolemia (FH) is an inherited disorder of lipoprotein metabolism characterised by impaired removal of low-density lipoproteins (LDL) from the circulation, which leads to an increased risk of cardiovascular disease (CVD). This risk can be significantly lowered by early diagnosis and treatment. In Germany, reliable estimates of the prevalence of FH are lacking. We therefore examined the prevalence rate of FH in Germany in a primary care based cohort., Method: We utilized records of 4722 participants in the DETECT study, in whom complete data on blood lipids and medical history were available. Prevalence rates were assessed using the Dutch Lipid Clinics Network (DLCN) and the US-MEDPED criteria. We stratified for gender and age. Group differences were analyzed using Chi 2 and ANOVA tests., Results: Using the DLCN (probable or definite FH) and the US.MEDPED criteria yielded prevalence rates of 1:278 and 1:295, respectively. The established diagnostic scores used in this analysis identify different patients. In women below 50 years of age, the LDL-C concentration is lower than in men, leading to the possibility of under-diagnosing FH in this group because women under the age of 50 are less likely to reach a higher DLCN-Score., Conclusions: FH has a higher than expected prevalence in Germany. Clinical diagnostic algorithms may not be concordant., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

5. Tip Design of Hemodialysis Catheters Influences Thrombotic Events and Replacement Rate.

Author

Petridis C, Nitschke M, Lehne W, Smith E, Goltz JP, Lehnert H, and Meier M

Subjects

Aged, Aged, 80 and over, Blood Flow Velocity, Catheterization, Central Venous adverse effects, Equipment Design, Female, Fibrinolytic Agents administration & dosage, Humans, Kaplan-Meier Estimate, Kidney Failure, Chronic diagnosis, Male, Middle Aged, Prospective Studies, Regional Blood Flow, Risk Factors, Surveys and Questionnaires, Thrombolytic Therapy, Thrombosis diagnosis, Thrombosis physiopathology, Thrombosis therapy, Time Factors, Tissue Plasminogen Activator administration & dosage, Treatment Outcome, Catheter Obstruction etiology, Catheterization, Central Venous instrumentation, Catheters, Indwelling, Central Venous Catheters, Device Removal, Kidney Failure, Chronic therapy, Renal Dialysis, Thrombosis etiology

Abstract

Objective/background: Central venous tunnelled hemodialysis catheters (CVTC) are used for initial vascular access in patients with renal failure. Tip design of the CVTC may play an important role in catheter function and complication rates, influencing adequate hemodialysis treatment of these patients., Methods: This prospective, observational cohort study compared the function and complication rates of two CVTCs in patients with end stage renal disease (ESRD) within a follow-up period of 24 months. The study included patients with ESRD who received either a CVTC with a split tip (ST) or a shotgun tip (SG). All patients underwent dialysis within 24 h of intervention. Blood flow was documented initially (Qb 0 ) and was followed up after 6 (Qb 6 ), 12 (Qb 12 ), and 24 (Qb 24 ) months. Analysis of blood flow and complication rates within the follow-up period was performed by questionnaires., Results: In total, 185 patients were included, of whom 93 received a ST CVTC and 92 a SG CVTC. Baseline parameters did not differ significantly between groups. CVTC blood flow was not significantly different between the two devices. Thrombolytic therapy with Alteplase was used significantly more often in the ST group (29%) than in the SG group (16%) (p < 0.05). The CVTC replacement rate was significantly higher in the ST group (19.3%) compared with the SG group (8.7%) (p < 0.05)., Conclusions: The tip design of CVTC (split or shotgun) appears to be irrelevant for long-term blood flow during dialysis treatment. However, patients may benefit from SG catheters over ST catheters where replacement rates and thrombolytic treatment are concerned., (Copyright © 2016 European Society for Vascular Surgery. Published by Elsevier Ltd. All rights reserved.)

Published

2017

6. Hypoxia-Inducible Factor 2α Mutation-Related Paragangliomas Classify as Discrete Pseudohypoxic Subcluster.

Author

Fliedner SM, Shankavaram U, Marzouca G, Elkahloun A, Jochmanova I, Daerr R, Linehan WM, Timmers H, Tischler AS, Papaspyrou K, Brieger J, de Krijger R, Breza J, Eisenhofer G, Zhuang Z, Lehnert H, and Pacak K

Subjects

Adolescent, Adult, Aged, Basic Helix-Loop-Helix Transcription Factors metabolism, Child, Cluster Analysis, Female, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Humans, Hypoxia genetics, Hypoxia metabolism, Male, Middle Aged, Oxidative Phosphorylation, Paraganglioma metabolism, Protein Binding, Transcriptome, Young Adult, Basic Helix-Loop-Helix Transcription Factors genetics, Mutation, Paraganglioma genetics

Abstract

Recently, activating mutations of the hypoxia-inducible factor 2α gene (HIF2A/EPAS1) have been recognized to predispose to multiple paragangliomas (PGLs) and duodenal somatostatinomas associated with polycythemia, and ocular abnormalities. Previously, mutations in the SDHA/B/C/D, SDHAF2, VHL, FH, PHD1, and PHD2 genes have been associated with HIF activation and the development of pseudohypoxic (cluster-1) PGLs. These tumors overlap in terms of tumor location, syndromic presentation, and noradrenergic phenotype to a certain extent. However, they also differ especially by clinical outcome and by presence of other tumors or abnormalities. In the present study, we aimed to establish additional molecular differences between HIF2A and non-HIF2A pseudohypoxic PGLs. RNA expression patterns of HIF2A PGLs (n=6) from 2 patients were compared with normal adrenal medullas (n=8) and other hereditary pseudohypoxic PGLs (VHL: n=13, SDHB: n=15, and SDHD: n=14). Unsupervised hierarchical clustering showed that HIF2A PGLs made up a separate cluster from other pseudohypoxic PGLs. Significance analysis of microarray yielded 875 differentially expressed genes between HIF2A and other pseudohypoxic PGLs after normalization to adrenal medulla (false discovery rate 0.01). Prediction analysis of microarray allowed correct classification of all HIF2A samples based on as little as three genes (TRHDE, LRRC63, IGSF10; error rate: 0.02). Genes with the highest expression difference between normal medulla and HIF2A PGLs were selected for confirmatory quantitative reverse transcriptase polymerase chain reaction. In conclusion, HIF2A PGLs show a characteristic expression signature that separates them from non-HIF2A pseudohypoxic PGLs. Unexpectedly, the most significantly differentially expressed genes have not been previously described as HIF target genes., (Copyright © 2016 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2016

7. Genotype and tumor locus determine expression profile of pseudohypoxic pheochromocytomas and paragangliomas.

Author

Shankavaram U, Fliedner SM, Elkahloun AG, Barb JJ, Munson PJ, Huynh TT, Matro JC, Turkova H, Linehan WM, Timmers HJ, Tischler AS, Powers JF, de Krijger R, Baysal BE, Takacova M, Pastorekova S, Gius D, Lehnert H, Camphausen K, and Pacak K

Subjects

Adolescent, Adrenal Gland Neoplasms metabolism, Adult, Aged, Cell Hypoxia, Child, Child, Preschool, Cluster Analysis, Female, Genotype, Humans, Liver Cirrhosis genetics, Male, Middle Aged, Mutation, Oligonucleotide Array Sequence Analysis, Oxidative Phosphorylation, Paraganglioma genetics, Paraganglioma metabolism, Pheochromocytoma metabolism, Principal Component Analysis, Succinate Dehydrogenase genetics, Succinate Dehydrogenase metabolism, Von Hippel-Lindau Tumor Suppressor Protein genetics, Von Hippel-Lindau Tumor Suppressor Protein metabolism, Young Adult, Adrenal Gland Neoplasms genetics, Pheochromocytoma genetics, Transcriptome

Abstract

Pheochromocytomas (PHEOs) and paragangliomas (PGLs) related to mutations in the mitochondrial succinate dehydrogenase (SDH) subunits A, B, C, and D, SDH complex assembly factor 2, and the von Hippel-Lindau (VHL) genes share a pseudohypoxic expression profile. However, genotype-specific differences in expression have been emerging. Development of effective new therapies for distinctive manifestations, e.g., a high rate of malignancy in SDHB- or predisposition to multifocal PGLs in SDHD patients, mandates improved stratification. To identify mutation/location-related characteristics among pseudohypoxic PHEOs/PGLs, we used comprehensive microarray profiling (SDHB: n = 18, SDHD-abdominal/thoracic (AT): n = 6, SDHD-head/neck (HN): n = 8, VHL: n = 13). To avoid location-specific bias, typical adrenal medulla genes were derived from matched normal medullas and cortices (n = 8) for data normalization. Unsupervised analysis identified two dominant clusters, separating SDHB and SDHD-AT PHEOs/PGLs (cluster A) from VHL PHEOs and SDHD-HN PGLs (cluster B). Supervised analysis yielded 6937 highly predictive genes (misclassification error rate of 0.175). Enrichment analysis revealed that energy metabolism and inflammation/fibrosis-related genes were most pronouncedly changed in clusters A and B, respectively. A minimum subset of 40 classifiers was validated by quantitative real-time polymerase chain reaction (quantitative real-time polymerase chain reaction vs. microarray: r = 0.87). Expression of several individual classifiers was identified as characteristic for VHL and SDHD-HN PHEOs and PGLs. In the present study, we show for the first time that SDHD-HN PGLs share more features with VHL PHEOs than with SDHD-AT PGLs. The presented data suggest novel subclassification of pseudohypoxic PHEOs/PGLs and implies cluster-specific pathogenic mechanisms and treatment strategies.

Published

2013

8. Brain insulin and leptin signaling in metabolic control: from animal research to clinical application.

Author

Scherer T, Lehnert H, and Hallschmid M

Subjects

Animals, Energy Metabolism, Humans, Obesity metabolism, Signal Transduction, Brain metabolism, Insulin metabolism, Leptin metabolism

Abstract

Besides the well-characterized effects of brain insulin and leptin in regulating food intake, insulin and leptin signaling to the central nervous system modulates a variety of metabolic processes, such as glucose and lipid homeostasis, as well as energy expenditure. This review summarizes the current literature on the contribution of central nervous insulin and leptin action to metabolic control in animals and humans. Potential therapeutic options based on the direct delivery of these peptides to the brain by, for example, intranasal administration, are discussed., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

9. A hypertensive patient presenting with paraneoplastic perimyocarditis and myositis due to pheochromocytoma.

Author

Harbeck B, Joost A, Lehne W, Böhm A, Süfke S, Werth S, Lehnert H, and Haas CS

Subjects

Aged, Female, Humans, Adrenal Gland Neoplasms complications, Hypertension complications, Myocarditis etiology, Myositis etiology, Paraneoplastic Syndromes etiology, Pericardium, Pheochromocytoma complications

Published

2012

10. Improved prediction of all-cause mortality by a combination of serum total testosterone and insulin-like growth factor I in adult men.

Author

Friedrich N, Schneider HJ, Haring R, Nauck M, Völzke H, Kroemer HK, Dörr M, Klotsche J, Jung-Sievers C, Pittrow D, Lehnert H, März W, Pieper L, Wittchen HU, Wallaschofski H, and Stalla GK

Subjects

Adult, Aged, Follow-Up Studies, Germany epidemiology, Humans, Incidence, Insulin-Like Growth Factor I deficiency, Male, Middle Aged, Predictive Value of Tests, Proportional Hazards Models, Prospective Studies, Risk Factors, Survival Analysis, Testosterone deficiency, Aging blood, Insulin-Like Growth Factor I analysis, Mortality ethnology, Testosterone blood

Abstract

Objective: Lower levels of anabolic hormones in older age are well documented. Several studies suggested that low insulin-like growth factor I (IGF-I) or testosterone levels were related to increased mortality. The aim of the present study was to investigate the combined influence of low IGF-I and low testosterone on all-cause mortality in men., Methods and Results: From two German prospective cohort studies, the DETECT study and SHIP, 3942 men were available for analyses. During 21,838 person-years of follow-up, 8.4% (n=330) of men died. Cox model analyses with age as timescale and adjusted for potential confounders revealed that men with levels below the 10th percentile of at least one hormone [hazard ratio (HR) 1.38 (95% confidence-interval (CI) 1.06-1.78), p=0.02] and two hormones [HR 2.88 (95% CI 1.32-6.29), p<0.01] showed a higher risk of all-cause mortality compared to men with non-low hormones. The associations became non-significant by using the 20th percentile as cut-off showing that the specificity increased with lower cut-offs for decreased hormone levels. The inclusion of both IGF-I and total testosterone in a mortality prediction model with common risk factors resulted in a significant integrated discrimination improvement of 0.5% (95% CI 0.3-0.7%, p=0.03)., Conclusions: Our results prove that multiple anabolic deficiencies have a higher impact on mortality than a single anabolic deficiency and suggest that assessment of more than one anabolic hormone as a biomarker improve the prediction of all-cause mortality., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2012

11. The anti-atherogenic aspect of metformin treatment in insulin resistant women with the polycystic ovary syndrome: role of the newly established pro-inflammatory adipokine Acute-phase Serum Amyloid A; evidence of an adipose tissue-monocyte axis.

Author

Tan BK, Adya R, Shan X, Aghilla M, Lehnert H, Keay SD, and Randeva HS

Subjects

Adipokines metabolism, Adipose Tissue metabolism, Adult, Animals, Atherosclerosis blood, Case-Control Studies, Female, Humans, Inflammation blood, Macrophages metabolism, Monocytes metabolism, Serum Amyloid A Protein biosynthesis, Insulin Resistance, Metformin metabolism, Polycystic Ovary Syndrome blood, Polycystic Ovary Syndrome drug therapy

Abstract

Objective: Acute-phase Serum Amyloid A (ASAA) is a novel pro-inflammatory adipokine, increased in obese, insulin resistant subjects. Polycystic ovary syndrome (PCOS) is associated with inflammation and atherosclerosis. We assessed sera, adipose tissue (AT) mRNA and protein levels of ASAA of PCOS women and matched controls. Ex vivo regulation of AT ASAA by d-glucose, effects of metformin treatment on circulating ASAA in PCOS subjects and effects of sera from normal and PCOS subjects (before and after metformin) on ASAA production (THP-1 macrophages) were also studied., Methods and Results: Circulating ASAA (ELISA), subcutaneous and omental AT ASAA mRNA (RT-PCR) and protein (western blotting) were significantly higher in PCOS women (P<0.05). In AT explants, glucose significantly increased ASAA production and secretion (P<0.05, P<0.01). Furthermore, ASAA production (THP-1 macrophages) was significantly greater by sera from PCOS women compared to controls (P<0.01). ASAA protein production was significantly decreased by sera from PCOS women following 6 months of metformin treatment (P<0.05). After 6 months of metformin treatment, there was a significant decrease in circulating ASAA (P<0.05). Importantly, changes in intima media thickness were predictive of changes in circulating ASAA (P=0.034)., Conclusion: Serum and AT ASAA are increased in PCOS women and are elevated by glucose. Metformin treatment decreases serum ASAA in these women. An adipose tissue-monocyte axis may be pivotal in the pathogenesis of inflammation and atherosclerosis. ASAA may be a valuable diagnostic marker in the management of dysmetabolic states including PCOS., (Copyright © 2010 Elsevier Ireland Ltd. All rights reserved.)

Published

2011

12. All-cause mortality and serum insulin-like growth factor I in primary care patients.

Author

Friedrich N, Schneider H, Dörr M, Nauck M, Völzke H, Klotsche J, Sievers C, Pittrow D, Böhler S, Lehnert H, Pieper L, Wittchen HU, Wallaschofski H, and Stalla GK

Subjects

Adult, Cardiovascular Diseases mortality, Female, Humans, Insulin-Like Growth Factor Binding Protein 3 blood, Male, Middle Aged, Prospective Studies, Risk, Survival Analysis, Insulin-Like Growth Factor I metabolism, Mortality, Primary Health Care

Abstract

Objective: Previous population-based studies provided conflicting results regarding the association of total serum insulin-like growth factor I (IGF-I) and mortality. The aim of the present study was to assess the relation of IGF-I levels with all-cause mortality in a prospective study., Design: DETECT (Diabetes Cardiovascular Risk-Evaluation: Targets and Essential Data for Commitment of Treatment) is a large, multistage, and nationally representative study of primary care patients in Germany. The study population included 2463 men and 3603 women. Death rates were recorded by the respective primary care physician. Serum total IGF-I levels were determined by chemiluminescence immunoassays and categorized into three groups (low, moderate, and high) according to the sex- and age-specific 10th and 90th percentiles., Results: Adjusted analyses revealed that men with low [hazard ratio (HR) 1.70 (95% confidence interval [CI] 1.05-2.73), p=0.03] and high [HR 1.76 (95% CI 1.09-2.85), p=0.02] IGF-I levels had higher risk of all-cause mortality compared to men with moderate IGF-I levels. The specificity of low IGF-I and high IGF-I levels increased with lower and higher cut-offs, respectively. No such association became apparent in women., Conclusions: The present study revealed a U-shaped relation between IGF-I and all-cause mortality in male primary care patients., (Copyright © 2011 Growth Hormone Research Society. Published by Elsevier Ltd. All rights reserved.)

Published

2011

13. High glucose disrupts oligosaccharide recognition function via competitive inhibition: a potential mechanism for immune dysregulation in diabetes mellitus.

Author

Ilyas R, Wallis R, Soilleux EJ, Townsend P, Zehnder D, Tan BK, Sim RB, Lehnert H, Randeva HS, and Mitchell DA

Subjects

Adipose Tissue pathology, Bacterial Infections, Binding, Competitive immunology, Cell Adhesion Molecules genetics, Complement Pathway, Mannose-Binding Lectin, Dendritic Cells immunology, Dendritic Cells pathology, Diabetes Complications, Glucose chemistry, Host-Pathogen Interactions, Humans, Immunity, Innate, Immunohistochemistry, Immunomodulation, Lectins, C-Type genetics, Mannose-Binding Lectin genetics, Mannose-Binding Lectin immunology, Oligosaccharides, Branched-Chain chemistry, Oligosaccharides, Branched-Chain immunology, Receptors, Cell Surface genetics, Stereoisomerism, Surface Plasmon Resonance, Cell Adhesion Molecules metabolism, Dendritic Cells metabolism, Glucose metabolism, Lectins, C-Type metabolism, Mannose-Binding Lectin metabolism, Oligosaccharides, Branched-Chain metabolism, Receptors, Cell Surface metabolism

Abstract

Diabetic complications include infection and cardiovascular disease. Within the immune system, host-pathogen and regulatory host-host interactions operate through binding of oligosaccharides by C-type lectin. A number of C-type lectins recognise oligosaccharides rich in mannose and fucose - sugars with similar structures to glucose. This raises the possibility that high glucose conditions in diabetes affect protein-oligosaccharide interactions via competitive inhibition. Mannose-binding lectin, soluble DC-SIGN and DC-SIGNR, and surfactant protein D, were tested for carbohydrate binding in the presence of glucose concentrations typical of diabetes, via surface plasmon resonance and affinity chromatography. Complement activation assays were performed in high glucose. DC-SIGN and DC-SIGNR expression in adipose tissues was examined via immunohistochemistry. High glucose inhibited C-type lectin binding to high-mannose glycoprotein and binding of DC-SIGN to fucosylated ligand (blood group B) was abrogated in high glucose. Complement activation via the lectin pathway was inhibited in high glucose and also in high trehalose - a nonreducing sugar with glucoside stereochemistry. DC-SIGN staining was seen on cells with DC morphology within omental and subcutaneous adipose tissues. We conclude that high glucose disrupts C-type lectin function, potentially illuminating new perspectives on susceptibility to infectious and inflammatory disease in diabetes. Mechanisms involve competitive inhibition of carbohydrate binding within sets of defined proteins, in contrast to broadly indiscriminate, irreversible glycation of proteins., (Copyright © 2010 Elsevier GmbH. All rights reserved.)

Published

2011

14. The CD40-CD40L pathway contributes to the proinflammatory function of intestinal epithelial cells in inflammatory bowel disease.

Author

Borcherding F, Nitschke M, Hundorfean G, Rupp J, von Smolinski D, Bieber K, van Kooten C, Lehnert H, Fellermann K, and Büning J

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Animals, Biopsy, Female, Fibroblasts metabolism, Humans, Interferon-gamma metabolism, Interleukin-8 metabolism, Male, Mice, Middle Aged, Remission Induction, CD40 Antigens biosynthesis, CD40 Ligand biosynthesis, Epithelial Cells metabolism, Gene Expression Regulation, Inflammatory Bowel Diseases metabolism, Intestinal Mucosa metabolism

Abstract

In inflammatory bowel diseases (IBD), intestinal epithelial cells (IECs) are involved in the outbalanced immune responses toward luminal antigens. However, the signals responsible for this proinflammatory capacity of IECs in IBD remain unclear. The CD40/CD40L interaction activates various pathways in immune and nonimmune cells related to inflammation and was shown to be critical for the development of IBD. Here we demonstrate CD40 expression within IECs during active IBD. Endoscopically obtained biopsies taken from Crohn's disease (n = 112) and ulcerative colitis patients (n = 67) consistently showed immunofluorescence staining for CD40 in IECs of inflamed ileal or colonic mucosa. In noninvolved mucosa during active disease, tissue obtained during Crohn's disease or ulcerative colitis in remission and biopsies from healthy controls (n = 38) IECs almost entirely lacked CD40 staining. Flow cytometry and RT-PCR analysis using different intestinal epithelial cell lines (HT29, SW480, and T84) showed IFN-gamma to effectively induce CD40 in IECs. Cells were virtually unresponsive to LPS or whole E. coli regarding CD40 expression. In addition, a moderate induction of CD40 was found in response to TNF-alpha, which exerted synergistical effects with IFN-gamma. CD40 ligation by CD40L-transfected murine fibroblasts or soluble CD40L increased the secretion of IL-8 in IFN-gamma pretreated HT29 cells. Our findings provide evidence for the epithelial expression and modulation of CD40 in IBD-affected mucosa and indicate its involvement in the proinflammatory function of IECs.

Published

2010

15. Short-term sleep loss decreases physical activity under free-living conditions but does not increase food intake under time-deprived laboratory conditions in healthy men.

Author

Schmid SM, Hallschmid M, Jauch-Chara K, Wilms B, Benedict C, Lehnert H, Born J, and Schultes B

Subjects

Adult, Appetite, Cross-Over Studies, Ghrelin blood, Humans, Hunger, Leptin blood, Male, Satiety Response, Eating, Motor Activity, Sleep

Abstract

Background: Short sleep duration is correlated with an increased risk of developing obesity and cardiovascular disease, but the mechanisms behind this relation are largely unknown., Objective: We aimed to test the hypothesis that acute sleep loss decreases physical activity while increasing food intake, thereby shifting 2 crucial behavioral components of energy homeostasis toward weight gain., Design: In 15 healthy, normal-weight men, spontaneous physical activity was registered by accelerometry during the entire experiment, and food intake as well as relevant hormones were assessed during a 15-h daytime period after 2 nights of regular sleep (bed time: 2245-0700) and after 2 nights of restricted sleep (bed time: 0245-0700). Experiments were performed in a crossover design., Results: Sleep restriction significantly decreased physical activity during the daytime spent under free-living conditions after the first night of sleep manipulation (P = 0.008). Also, intensities of physical activity were shifted toward lower levels, with less time spent with intense activities (P = 0.046). Total energy intake, feelings of hunger, and appetite as well as ghrelin and leptin concentrations during day 2 remained unaffected by acute sleep restriction., Conclusions: In contrast to our expectation, short-term sleep loss neither increased food intake nor affected concentrations of the hunger-regulating hormones leptin and ghrelin. However, the observed decrease in daytime physical activity may point to another potentially important behavioral mechanism for the health-impairing influence of sleep loss.

Published

2009

16. Unmet needs in the diagnosis and treatment of dyslipidemia in the primary care setting in Germany.

Author

Böhler S, Scharnagl H, Freisinger F, Stojakovic T, Glaesmer H, Klotsche J, Pieper L, Pittrow D, Kirch W, Schneider H, Stalla GK, Lehnert H, Zeiher AM, Silber S, Koch U, Ruf G, März W, and Wittchen HU

Subjects

Blood Chemical Analysis, Blood Pressure, Coronary Disease diagnosis, Coronary Disease epidemiology, Coronary Disease therapy, Cross-Sectional Studies, Diabetic Angiopathies diagnosis, Diabetic Angiopathies epidemiology, Diabetic Angiopathies therapy, Dyslipidemias epidemiology, Dyslipidemias therapy, Germany epidemiology, Humans, Dyslipidemias diagnosis, Primary Health Care standards

Abstract

Objectives and Methods: DETECT is a cross-sectional study of 55,518 unselected consecutive patients in 3188 representative primary care offices in Germany. In a random subset of 7519 patients, an extensive standardized laboratory program was undertaken. The study investigated the prevalence of cardiovascular disease, known risk factors (such as diabetes, hypertension and dyslipidemia and their co-morbid manifestation), as well as treatment patterns. The present analysis of the DETECT laboratory dataset focused on the prevalence and treatment of dyslipidemia in primary medical care in Germany. Coronary artery disease (CAD), risk categories and LDL-C target achievement rates were determined in the subset of 6815 patients according to the National Cholesterol Education Program (NCEP) ATP III Guidelines., Results: Of all patients, 54.3% had dyslipidemia. Only 54.4% of the NCEP-classified dyslipidemic patients were diagnosed as 'dyslipidemic' by their physicians. Only 27% of all dyslipidemic patients (and 40.7% of the recognized dyslipidemic patients) were treated with lipid-lowering medications, and 11.1% of all dyslipidemic patients (41.4% of the patients treated with lipid-lowering drugs) achieved their LDL-C treatment goals. In conclusion, 80.3% of patients in the sample with dyslipidemia went undiagnosed, un-treated or under-treated.

Published

2007

17. Obesity: sometimes more than adipose tissue.

Author

Reschke K, Klose S, Ridwelski K, and Lehnert H

Subjects

Adult, Angiography, Digital Subtraction, Cystadenoma surgery, Diagnosis, Differential, Female, Humans, Ovarian Neoplasms surgery, Tomography, X-Ray Computed, Cystadenoma diagnosis, Obesity, Morbid diagnosis, Ovarian Neoplasms diagnosis

Published

2000

18. Rapid and sensitive determination of catecholamines and the metabolite 3-methoxy-4-hydroxyphen-ethyleneglycol using HPLC following novel extraction procedures.

Author

Hollenbach E, Schulz C, and Lehnert H

Subjects

Adolescent, Adult, Aged, Catecholamines blood, Catecholamines urine, Female, Humans, Male, Methoxyhydroxyphenylglycol blood, Methoxyhydroxyphenylglycol urine, Middle Aged, Reference Values, Reproducibility of Results, Statistics as Topic, Catecholamines analysis, Chromatography, High Pressure Liquid methods, Methoxyhydroxyphenylglycol analysis

Abstract

In the present study assays were improved for the determination of free catecholamines and 3-methoxy-4-hydroxyphenethyleneglycol (MHPG), the major metabolite of peripheral and central noradrenaline. The compounds were extracted by a fluid phase extraction: a diphenyl boric acid method for the purification of catecholamines and an ethyl acetate extraction for MHPG were used, respectively. High-performance liquid chromatography with electrochemical detection was employed for quantitative analysis. In previous studies, significant differences between plasma concentrations of these substances in normal volunteers and hospital patients were demonstrated. Therefore, we established valid reference values for a hospital population. Blood and urine samples of 59 patients without disorders and medication affecting catecholamine synthesis and metabolism or the activity of the sympatho-adrenal system were collected and analyzed for free and total (free plus conjugated) MHPG, noradrenaline (NA), adrenaline (A) and dopamine (DA); total MHPG was assayed after enzymatic hydrolysis of conjugates. Our data clearly demonstrate that these methods are sensitive, specific, rapid, and can easily be standardized. The intra- and inter-assay precision were high (CV 2.6-5.3% and 4.3-6.9% for plasma, CV 3.8-4.9% and 5.1-8.2% for urine, respectively). For plasma, the mean concentrations +/- SD were determined to be 20.82+/-4.70 pmol/ml for free MHPG, 68.43+/-16.21 pmol/ml for total MHPG, 2.11+/-0.24 pmol/ml for NA and 0.31+/-0.08 pmol/ml for A. For 24h-urine the mean concentrations +/-SD were determined to be 0.44+/-0.13 mmol/24h for free MHPG, 8.79+/-2.13 mmol/24h for total MHPG, 169.8+/-58.25 nmol/24h for NA, 62.19+/-21.79 nmol/24h for A and 757.2+/-382.6 nmol/24h for DA. In summary, these novel and rapid methods can clearly be employed in a routine clinical setting.

Published

1998

19. Corticotropin-releasing hormone (CRH) is a respiratory stimulant in humans: a comparative study of human and ovine CRH.

Author

Nink M, Salomon E, Coutinho M, Treese N, Bernhard G, Krause U, Beyer J, and Lehnert H

Subjects

Adrenocorticotropic Hormone blood, Adult, Animals, Heart Rate drug effects, Humans, Hydrocortisone blood, Male, Sheep, Corticotropin-Releasing Hormone pharmacology, Respiration drug effects

Abstract

Previous experimental and clinical studies clearly demonstrated that exogenously administered CRH possesses respiratory properties. Until now, these effects were investigated using human (h) CRH in both healthy volunteers and patients under long-term respiration. We now compared the effects of hCRH with those of ovine (o) CRH in ten healthy young males. In particular it should be evaluated whether oCRH with its longer plasma half-life induces a more profound respiratory stimulation. On two separate days within two weeks, ventilation and cardiac performance were measured during steady state conditions by using a computerized cardio-pulmonary exercise testing system. In this placebo controlled double-blind-crossover study h- and oCRH (100 ug i.v. each) both augmented minute volume significantly during the observation period. Heart rate also increased after both analogues. All effects were comparable without a significant difference between both substances. There were no major side effects observable. Our data thus demonstrate that both analogues might be suitable for both diagnostic (i.e., testing of respiratory and autonomic responses) and therapeutic purposes.

Published

1994

20. Tyrosine prevents behavioral and neurochemical correlates of an acute stress in rats.

Author

Reinstein DK, Lehnert H, Scott NA, and Wurtman RJ

Subjects

Animals, Male, Methoxyhydroxyphenylglycol analogs & derivatives, Methoxyhydroxyphenylglycol analysis, Motor Activity drug effects, Norepinephrine analysis, Rats, Rats, Inbred Strains, Stress, Physiological psychology, Behavior, Animal drug effects, Brain Chemistry drug effects, Stress, Physiological metabolism, Tyrosine pharmacology

Abstract

Exposure of rats to an acute, uncontrollable stressor can increase brain norepinephrine (NE) turnover and decrease locomotor and exploratory behavior. We examined the ability of exogenous tyrosine, NE's amino acid precursor, to protect rats from developing these neurochemical and behavioral changes when stressed. Animals pretreated with saline or tyrosine (200 mg/kg, i.p.) were subjected to tail shock (15 v, 2 mA, 5 sec/30 sec) or to no shock during a 60-min period. Exposure to shock depleted NE and increased its turnover [as indicated by altered NE and 3-methoxy-4-hydroxy-phenylene-glycol sulfate levels (MHPG-SO4)] within the locus coeruleus, the hippocampus and the hypothalamus. Behavioral deficits were observed using measures of locomotion, standing on hind legs, and hole-poking in an open-field apparatus. Animals given tyrosine before shock displayed neither shock-induced NE depletion nor the deficits in locomotion and hole-poking; brain MHPG-SO4 levels tended to be greater than after shock alone. These observations suggest that the stress caused NE to be released from some neurons more rapidly than it could be restored by synthesis or reuptake, thereby impairing noradrenergic transmission and NE-dependent exploratory behaviors. Tyrosine administration presumably enhanced the transmitter's synthesis in stressed animals, thereby preventing both the neurochemical and the behavioral deficits.

Published

1984

21. Dietary tyrosine suppresses the rise in plasma corticosterone following acute stress in rats.

Author

Reinstein DK, Lehnert H, and Wurtman RJ

Subjects

Animals, Behavior, Animal drug effects, Diet, Hypothalamus drug effects, Hypothalamus metabolism, Norepinephrine metabolism, Rats, Stress, Physiological metabolism, Tyrosine administration & dosage, Tyrosine metabolism, Corticosterone blood, Stress, Physiological blood, Tyrosine pharmacology

Abstract

Acute, uncontrollable stress increases norepinephrine (NE) turnover in the rat's brain (depleting NE) and diminishes the animal's subsequent tendency to explore a novel environment. Pre-treatment with tyrosine can reverse these adverse effects of stress, presumably by preventing the depletion of NE in the hypothalamus. Numerous studies suggest that NE inhibits the release of adrenocorticotropic hormone (ACTH) by suppressing corticotropic releasing factor (CRF) secretion in the hypothalamus. In the present study, we found that pre-treatment with supplemental tyrosine not only prevented the behavioral depression and hypothalamic NE depletion observed after an acute stress, but also suppressed the rise in plasma corticosterone. These results support a role for brain NE in stress-induced corticosterone secretion and demonstrate that supplemental tyrosine can protect against several adverse consequences of such stress.

Published

1985