Your search keyword '"F, Ohl"' showing total 36 results

1. Measurement of the pi^+ meson polarizabilities via the gamma p->gamma pi^+ n reaction

Author

Ahrens, J., Alexeev, V. M., Annand, J. R. M., Arends, H. J., Beck, R., Caselotti, G., Cherepnya, S. N., Drechsel, D., Fil'kov, L. V., F"ohl, K., Giller, I., Grabmayr, P., Hehl, T., Hornidge, D., Kashevarov, V. L., Kotulla, M., Krambrich, D., Krusche, B., Lang, M., McGeorge, J. C., MacGregor, I. J. D., Metag, V., Moinester, M., Novotny, R., Pfeiffer, M., Rost, M., Schadmand, S., Scherer, S., Thomas, A., Unkmeir, C., and Walcher, Th.

Subjects

Nuclear Experiment, High Energy Physics - Experiment, High Energy Physics - Phenomenology, Nuclear Theory

Abstract

An experiment on the radiative pi^+ meson photoproduction from the proton (gamma p->gamma pi^+ n) was carried out at the Mainz Microtron MAMI in the kinematic region 537 MeV

Published

2004

2. SPORT MOTIVES AND PSYCHOACTIVE SUBSTANCE USE OF YOUNG ATHLETES: DOES THE IMPORTANT THING IS REALLY TO TAKE PART?

Author

F Ohl, JC Suris, Vè Perreault-Liard, and Richard E. Bélanger

Subjects

medicine.medical_specialty, biology, Athletes, Pediatrics, Perinatology and Child Health, Psychoactive substance, medicine, Abstracts / Résumés, Psychology, biology.organism_classification, Psychiatry

Abstract

BACKGROUND: As for ergogenic substances, studies show that groups of young athletes are more likely to use psychoactive substances than their peers. The links underlying these two contrasting health habits yet stay elusive.

Published

2017

3. Additional file 1: Table S1. of Consomic mouse strain selection based on effect size measurement, statistical significance testing and integrated behavioral z-scoring: focus on anxiety-related behavior and locomotion

Author

M. Labots, M. Laarakker, F. Ohl, and H. Van Lith

Abstract

Bootstrap P values of comparison of means between C57BL/6J and donor or consomic lines in mHB behavioral dimensions and motivational systems. (DOCX 20 kb)

Published

2016

4. Regulation of the developing hypothalamic–pituitary–adrenal axis in corticotropin releasing hormone receptor 1-deficient mice

Author

M V, Schmidt, M, Schmidt, M S, Oitzl, M B, Müller, F, Ohl, W, Wurst, F, Holsboer, S, Levine, and E R, De Kloet

Subjects

Male, Hypothalamo-Hypophyseal System, medicine.medical_specialty, Genotype, Corticotropin-Releasing Hormone, Pituitary-Adrenal System, Biology, Hippocampus, Receptors, Corticotropin-Releasing Hormone, Corticotropin-releasing hormone receptor 1, Mice, Corticotropin-releasing hormone, chemistry.chemical_compound, Receptors, Glucocorticoid, Glucocorticoid receptor, Mineralocorticoid receptor, Corticosterone, Internal medicine, medicine, Animals, RNA, Messenger, Receptor, In Situ Hybridization, Mice, Knockout, Maternal deprivation, Maternal Deprivation, General Neuroscience, Arginine Vasopressin, Receptors, Mineralocorticoid, Endocrinology, medicine.anatomical_structure, Animals, Newborn, chemistry, Female, Hypothalamic–pituitary–adrenal axis, Paraventricular Hypothalamic Nucleus

Abstract

During postnatal development, mice undergo a so-called stress hyporesponsive period, which is characterized by low basal corticosterone levels and the inability of mild stressors to induce a corticosterone response. The stress hyporesponsiveness is in part regulated by maternal factors. Twenty-four hours of deprivation results in an activation of basal and stress-induced corticosterone and a down-regulation of corticotropin releasing hormone (CRH), mineralocorticoid receptor (MR) and glucocorticoid receptor (GR) expression in the brain. It has been hypothesized that the CRH receptor 1 (CRHr1) may play an important regulatory role during development by mediating the effects of maternal deprivation. Using CRHr1-deficient mice we examined the role of this receptor on the maternal deprivation effects and in regulating the expression of hypothalamic–pituitary–adrenal axis-related genes. We could demonstrate that the CRHr1 is essential for the activation of the corticosterone response following maternal deprivation, most likely due to the lack of the receptor in the pituitary. Furthermore, we could show that the CRHr1 is regulating the expression of CRH and MRs. In contrast, effects of maternal deprivation during postnatal development on GRs are not mediated by this receptor.

Published

2003

5. 195: Caffeinated Products as Ergogenic AIDS Among Sport-Practicing Adolescents: Top of the Chart

Author

F Ohl, E Bernard, JC Suris, and Richard E. Bélanger

Subjects

medicine.medical_specialty, Acquired immunodeficiency syndrome (AIDS), Chart, Family medicine, Pediatrics, Perinatology and Child Health, medicine, medicine.disease, Psychology

Published

2015

6. Technical design report for the PANDA (AntiProton Annihilations at Darmstadt) Straw Tube Tracker

Author

Erni, W., Keshelashvili, I., Krusche, B., Steinacher, M., Heng, Y., Liu, Z., Liu, H., Shen, X., Wang, Q., Xu, H., Aab, A., Albrecht, M., Becker, J., Csap´o, A., Feldbauer, F., Fink, M., Friedel, P., Heinsius, F. H., Held, T., Klask, L., Koch, H., Kopf, B., Leiber, S., Leyhe, M., Motzko, C., Peliz¨aus, M., Pychy, J., Roth, B., Schr¨oder, T., Schulze, J., Sowa, C., Steinke, M., Trifterer, T., Wiedner, U., Zhong, J., Beck, R., Bianco, S., Brinkmann, K. T., Hammann, C., Hinterberger, F., Kaiser, D., Kliemt, R., Kube, M., Pitka, A., Quagli, T., Schmidt, C., Schmitz, R., Schnell, R., Thoma, U., Vlasov, P., Walther, D., Wendel, C., W¨urschig, T., Zaunick, H. G., Bianconi, A., Bragadireanu, M., Caprini, M., Pantea, D., Pantelica, D., Pietreanu, D., Serbina, L., Tarta, P. D., Kaplan, D., Fiutowski, T., Idzik, M., Mindur, B., Przyborowski, D., Swientek, K., Czech, B., Kistryn, M., Kliczewski, S., Kozela, A., Kulessa, P., Lebiedowicz, P., Pysz, K., Sch¨afer, W., Siudak, R., Szczurek, A., Jowzaee, S., Kajetanowicz, M., Kamys, B., Kistryn, S., Korcyl, G., Korcyl, K., Krzemien, W., Magiera, A., Moskal, P., Palka, M., Rudy, Z., Salabura, P., Smyrski, J., Wro´nska, A., Augustin, I., Lehmann, I., Nimorus, D., Schepers, G., Al Turany, M., Arora, R., Deppe, H., Flemming, H., Gerhardt, A., G¨otzen, K., Jordi, A. F., Kalicy, G., Karabowicz, R., Lehmann, D., Lewandowski, B., L¨uhning, J., Maas, F., Orth, H., Patsyuk, M., Peters, K., Saito, T., Schmidt, C. J., Schmitt, L., Schwarz, C., Schwiening, J., Traxler, M., Voss, B., Wieczorek, P., Wilms, A., Z¨uhlsdorf, M., Abazov, V. M., Alexeev, G., Arefiev, A., Astakhov, V. I., Barabanov, M. Y., Batyunya, B. V., Davydov, Y. I., Dodokhov, V. K., Efremov, A. A., Fedunov, A. G., Festchenko, A. A., Galoyan, A. S., Grigoryan, S., Karmokov, A., Koshurnikov, E. K., Lobanov, V. I., Lobanov, Y. Y., Makarov, A. F., Malinina, L. V., Malyshev, V. L., Mustafaev, G. A., Olshevskiy, A., Pasyuk, M. A., Perevalova, E. A., Piskun, A. A., Pocheptsov, T. A., Pontecorvo, G., Rodionov, V. K., Rogov, Y. N., Salmin, R. A., Samartsev, A. G., Sapozhnikov, M. G., Shabratova, G. S., Skachkova, A. N., Skachkov, N. B., Strokovsky, E. A., Suleimanov, M. K., Teshev, R. S., Tokmenin, V. V., Uzhinsky, V. V., Vodopyanov, A. S., Zaporozhets, S. A., Zhuravlev, N. I., Zorin, A. G., Branford, D., Glazier, D., Watts, D., Woods, P., Britting, A., Eyrich, W., Lehmann, A., Uhlig, F., Dobbs, S., Metreveli, Z., Seth, K., Tomaradze, A., Xiao, T., Bettoni, D., Carassiti, V., Cotta Ramusino, A., Dalpiaz, P., Drago, A., Fioravanti, E., Garzia, I., Savri`e, M., Stancari, G., Bianchi, N., Gianotti, P., A, Guaraldo, C., Lucherini, V., Orecchini, D., Pace, E., Bersani, A., Bracco, G., Macri, M., Parodi, R. F., Bremer, D., Dormenev, V., Drexler, P., D¨uren, M., Eissner, T., F¨ohl, K., Galuska, M., Gessler, T., Hayrapetyan, A., Hu, J., Koch, P., Kr¨ock, B., K¨uhn, W., Lange, S., Liang, Y., Merle, O., Metag, V., Moritz, M., M¨unchow, D., Nanova, M., Novotny, R., Spruck, B., Stenzel, H., Ullrich, T., Werner, M., Euan, C., Hoek, M., Ireland, D., Keri, T., Montgomery, R., Protopopescu, D., Rosner, G., Seitz, B., Babai, M., Glazenborg Kluttig, A., Kavatsyuk, M., Lemmens, P., Lindemulder, M., L¨ohner, H., Messchendorp, J., Moeini, H., Schakel, P., Schreuder, F., Smit, H., Tambave, G., van der Weele, J. C., Veenstra, R., Sohlbach, H., B¨uscher, M., Deermann, D., Dosdall, R., Esch, S., Gillitzer, A., Goldenbaum, F., Grunwald, D., Henssler, S., Herten, A., Hu, Q., Kemmerling, G., Kleines, H., Kozlov, V., Lehrach, A., Maier, R., Mertens, M., Ohm, H., Orfanitski, S., Prasuhn, D., Randriamalala, T., Ritman, J., R¨oder, M., Schadmand, S., Serdyuk, V., Sterzenbach, G., Stockmanns, T., Wintz, P., W¨ustner, P., Kisiel, J., Li, S., Li, Z., Sun, Z., Rigato, V., Fissum, S., Hansen, K., Isaksson, L., Lundin, M., Schr¨oder, B., Achenbach, P., Bleser, S., Cahit, U., Cardinali, M., Denig, A., Distler, M., Fritsch, M., Jasinski, P., Kangh, D., Karavdina, A., Lauth, W., Merkel, H., Michel, M., Mora Espi, M. C., M¨uller, U., Pochodzalla, J., Sanchez, S., Sanchez Lorente, A., Schlimme, S., Sfienti, C., Thiel, M., Weber, T., Dormenev, V. I., Fedorov, A. A., Korzhik, M. V., Missevitch, O. V., Balanutsa, V., Chernetsky, V., Demekhin, A., Dolgolenko, A., Fedorets, P., Gerasimov, A., Goryachev, V., Varentsov, V., Boukharov, A., Malyshev, O., Marishev, I., Semenov, A., B¨ohmer, F., Dørheim, S., Ketzer, B., Paul, S., Hergem¨oller, A. K., Khoukaz, A., K¨ohler, E., T¨aschner, A., Wessels, J., Varma, R., Chaterjee, A., Jha, V., Kailas, S., Roy, B. J., Yan, Y., Chinorat, K., Khanchai, K., Ayut, L., Pomrad, S., Baldin, E., Kotov, K., Peleganchuk, S., Tikhonov, Y., Boucher, J., Chambert, V., Dbeyssi, A., Gumberidze, M., Hennino, T., Imre, M., Kunne, R., Le Galliard, C., Ma, B., Marchand, D., Maroni, A., Ong, S., Ramstein, B., Rosier, P., Tomasi Gustafsson, E., Van de Wiele, J., Boca, G., Braghieri, A., Costanza, S., Genova, P., Lavezzi, L., Montagna, P., Rotondi, A., Abramov, V., Belikov, N., Davidenko, A., Derevschikov, A., Goncharenko, Y., Grishin, V., Kachanov, V., Konstantinov, D., Kormilitsin, V., Melnik, Y., Levin, A., Minaev, N., Mochalov, V., Morozov, D., Nogach, L., Poslavskiy, S., Ryazantsev, A., Ryzhikov, S., Semenov, P., Shein, I., Uzunian, A., Vasiliev, A., Yakutin, A., B¨ack, T., Cederwall, B., Mak´onyi, K., Tegn´er, P. E., von W¨urtemberg, K. M., Belostotski, S., Gavrilov, G., Itzotov, A., Kashchuk, A., Kisselev, A., Kravchenko, P., Levitskaya, O., Manaenkov, S., Miklukho, O., Naryshkin, Y., Veretennikov, D., Vikhrov, V., Zhadanov, A., Alberto, D., Amoroso, A., Bussa, M. P., Busso, L., De Mori, F., Destefanis, M., Fava, L., Ferrero, L., Greco, M., Maggiora, M., Marcello, S., Sosio, S., Spataro, S., Zotti, L., Calvo, D., Coli, S., De Remigis, P., Filippi, A., Giraudo, G., Lusso, S., Mazza, G., Morra, O., Rivetti, A., Wheadon, R., Iazzi, Felice, Lavagno, Andrea, Younis, MUHAMMAD HANNAN, Birsa, R., Bradamante, F., Bressan, A., Martin, A., Clement, H., Galander, B., Caldeira Balkest˚ahl, L., Cal´en, H., Fransson, K., Johansson, T., Kupsc, A., Marciniewski, P., Thom´e, E., Wolke, M., Zlomanczuk, J., D´ıaz, J., Ortiz, A., Dmowski, K., Duda, P., Korzeniewski, R., Slowinski, B., Chlopik, A., Guzik, Z., Kosinski, K., Melnychuk, D., Wasilewski, A., Wojciechowski, M., Wronka, S., Wysocka, A., Zwieglinski, B., B¨uhler, P., Hartman, O. N., Kienle, P., Marton, J., Suzuki, K., Widmann, E., Zmeskal, J., Erni, W., Keshelashvili, I., Krusche, B., Steinacher, M., Heng, Y., Liu, Z., Liu, H., Shen, X., Wang, Q., Xu, H., Aab, A., Albrecht, M., Becker, J., Csapó, A., Feldbauer, F., Fink, M., Friedel, P., Heinsius, F. H., Held, T., Klask, L., Koch, H., Kopf, B., Leiber, S., Leyhe, M., Motzko, C., Pelizäus, M., Pychy, J., Roth, B., Schröder, T., Schulze, J., Sowa, C., Steinke, M., Trifterer, T., Wiedner, U., Zhong, J., Beck, R., Bianco, S., Brinkmann, K. T., Hammann, C., Hinterberger, F., Kaiser, D., Kliemt, R., Kube, M., Pitka, A., Quagli, T., Schmidt, C., Schmitz, R., Schnell, R., Thoma, U., Vlasov, P., Walther, D., Wendel, C., Würschig, T., Zaunick, H. G., Bianconi, A., Bragadireanu, M., Caprini, M., Pantea, D., Pantelica, D., Pietreanu, D., Serbina, L., Tarta, P. D., Kaplan, D., Fiutowski, T., Idzik, M., Mindur, B., Przyborowski, D., Swientek, K., Czech, B., Kistryn, M., Kliczewski, S., Kozela, A., Kulessa, P., Lebiedowicz, P., Pysz, K., Schäfer, W., Siudak, R., Szczurek, A., Jowzaee, S., Kajetanowicz, M., Kamys, B., Kistryn, S., Korcyl, G., Korcyl, K., Krzemien, W., Magiera, A., Moskal, P., Palka, M., Rudy, Z., Salabura, P., Smyrski, J., Wrońska, A., Augustin, I., Lehmann, I., Nimorus, D., Schepers, G., Al Turany, M., Arora, R., Deppe, H., Flemming, H., Gerhardt, A., Götzen, K., Jordi, A. F., Kalicy, G., Karabowicz, R., Lehmann, D., Lewandowski, B., Lühning, J., Maas, F., Orth, H., Patsyuk, M., Peters, K., Saito, T., Schmidt, C. J., Schmitt, L., Schwarz, C., Schwiening, J., Traxler, M., Voss, B., Wieczorek, P., Wilms, A., Zühlsdorf, M., Abazov, V. M., Alexeev, G., Arefiev, A., Astakhov, V. I., Yu Barabanov, M., Batyunya, B. V., Davydov, Yu I., Kh Dodokhov, V., Efremov, A. A., Fedunov, A. G., Festchenko, A. A., Galoyan, A. S., Grigoryan, S., Karmokov, A., Koshurnikov, E. K., Lobanov, V. I., Lobanov, Yu Yu, Makarov, A. F., Malinina, L. V., Malyshev, V. L., Mustafaev, G. A., Olshevskiy, A., Pasyuk, M. A., Perevalova, E. A., Piskun, A. A., Pocheptsov, T. A., Pontecorvo, G., Rodionov, V. K., Rogov, Yu N., Salmin, R. A., Samartsev, A. G., Sapozhnikov, M. G., Shabratova, G. S., Skachkova, A. N., Skachkov, N. B., Strokovsky, E. A., Suleimanov, M. K., Sh Teshev, R., Tokmenin, V. V., Uzhinsky, V. V., Vodopyanov, A. S., Zaporozhets, S. A., Zhuravlev, N. I., Zorin, A. G., Branford, D., Glazier, D., Watts, D., Woods, P., Britting, A., Eyrich, W., Lehmann, A., Uhlig, F., Dobbs, S., Metreveli, Z., Seth, K., Tomaradze, A., Xiao, T., Bettoni, D., Carassiti, V., Cotta Ramusino, A., Dalpiaz, P., Drago, A., Fioravanti, E., Garzia, I., Savriè, M., Stancari, G., Bianchi, N., Gianotti, P, Guaraldo, C., Lucherini, V., Orecchini, D., Pace, E., Bersani, A., Bracco, G., Macri, M., Parodi, R. F., Bremer, D., Dormenev, V., Drexler, P., Düren, M., Eissner, T., Föhl, K., Galuska, M., Gessler, T., Hayrapetyan, A., Hu, J., Koch, P., Kröck, B., Kühn, W., Lange, S., Liang, Y., Merle, O., Metag, V., Moritz, M., Münchow, D., Nanova, M., Novotny, R., Spruck, B., Stenzel, H., Ullrich, T., Werner, M., Euan, C., Hoek, M., Ireland, D., Keri, T., Montgomery, R., Protopopescu, D., Rosner, G., Seitz, B., Babai, M., Glazenborg Kluttig, A., Kavatsyuk, M., Lemmens, P., Lindemulder, M., Löhner, H., Messchendorp, J., Moeini, H., Schakel, P., Schreuder, F., Smit, H., Tambave, G., van der Weele, J. C., Veenstra, R., Sohlbach, H., Büscher, M., Deermann, D., Dosdall, R., Esch, S., Gillitzer, A., Goldenbaum, F., Grunwald, D., Henssler, S., Herten, A., Hu, Q., Kemmerling, G., Kleines, H., Kozlov, V., Lehrach, A., Maier, R., Mertens, M., Ohm, H., Orfanitski, S., Prasuhn, D., Randriamalala, T., Ritman, J., Röder, M., Schadmand, S., Serdyuk, V., Sterzenbach, G., Stockmanns, T., Wintz, P., Wüstner, P., Kisiel, J., Li, S., Li, Z., Sun, Z., Rigato, V., Fissum, S., Hansen, K., Isaksson, L., Lundin, M., Schröder, B., Achenbach, P., Bleser, S., Cahit, U., Cardinali, M., Denig, A., Distler, M., Fritsch, M., Jasinski, P., Kangh, D., Karavdina, A., Lauth, W., Merkel, H., Michel, M., Mora Espi, M. C., Müller, U., Pochodzalla, J., Sanchez, S., Sanchez Lorente, A., Schlimme, S., Sfienti, C., Thiel, M., Weber, T., Dormenev, V. I., Fedorov, A. A., Korzhik, M. V., Missevitch, O. V., Balanutsa, V., Chernetsky, V., Demekhin, A., Dolgolenko, A., Fedorets, P., Gerasimov, A., Goryachev, V., Varentsov, V., Boukharov, A., Malyshev, O., Marishev, I., Semenov, A., Böhmer, F., Dørheim, S., Ketzer, B., Paul, S., Hergemöller, A. K., Khoukaz, A., Köhler, E., Täschner, A., Wessels, J., Varma, R., Chaterjee, A., Jha, V., Kailas, S., Roy, B. J., Yan, Y., Chinorat, K., Khanchai, K., Ayut, L., Pomrad, S., Baldin, E., Kotov, K., Peleganchuk, S., Tikhonov, Yu, Boucher, J., Chambert, V., Dbeyssi, A., Gumberidze, M., Hennino, T., Imre, M., Kunne, R., Le Galliard, C., Ma, B., Marchand, D., Maroni, A., Ong, S., Ramstein, B., Rosier, P., Tomasi Gustafsson, E., Van de Wiele, J., Boca, G., Braghieri, A., Costanza, S., Genova, P., Lavezzi, L., Montagna, P., Rotondi, A., Abramov, V., Belikov, N., Davidenko, A., Derevschikov, A., Goncharenko, Y., Grishin, V., Kachanov, V., Konstantinov, D., Kormilitsin, V., Melnik, Y., Levin, A., Minaev, N., Mochalov, V., Morozov, D., Nogach, L., Poslavskiy, S., Ryazantsev, A., Ryzhikov, S., Semenov, P., Shein, I., Uzunian, A., Vasiliev, A., Yakutin, A., Bäck, T., Cederwall, B., Makónyi, K., Tegnér, P. E., von Würtemberg, K. M., Belostotski, S., Gavrilov, G., Itzotov, A., Kashchuk, A., Kisselev, A., Kravchenko, P., Levitskaya, O., Manaenkov, S., Miklukho, O., Naryshkin, Y., Veretennikov, D., Vikhrov, V., Zhadanov, A., Alberto, D., Amoroso, A., Bussa, M. P., Busso, L., De Mori, F., Destefanis, M., Fava, L., Ferrero, L., Greco, M., Maggiora, M., Marcello, S., Sosio, S., Spataro, S., Zotti, L., Calvo, D., Coli, S., De Remigis, P., Filippi, A., Giraudo, G., Lusso, S., Mazza, G., Morra, O., Rivetti, A., Wheadon, R., Iazzi, F., Lavagno, A., Younis, H., Birsa, Renato, Bradamante, Franco, Bressan, Andrea, Martin, Anna, Clement, H., Galander, B., Caldeira Balkeståhl, L., Calén, H., Fransson, K., Johansson, T., Kupsc, A., Marciniewski, P., Thomé, E., Wolke, M., Zlomanczuk, J., Díaz, J., Ortiz, A., Dmowski, K., Duda, P., Korzeniewski, R., Slowinski, B., Chlopik, A., Guzik, Z., Kosinski, K., Melnychuk, D., Wasilewski, A., Wojciechowski, M., Wronka, S., Wysocka, A., Zwieglinski, B., Bühler, P., Hartman, O. N., Kienle, P., Marton, J., Suzuki, K., Widmann, E., Zmeskal, J., KVI - Center for Advanced Radiation Technology, and Research unit Nuclear & Hadron Physics

Subjects

tubes, Nuclear and High Energy Physics, Gaseous Detectors, Transition Radiation, hep-ex, Physics::Instrumentation and Detectors, Atlas Muon Spectrometer, Cleo-Iii Trigger, Relativistic Rise, Particle Identification, straw tube, Computer Science::Hardware Architecture, Storage-Ring Hesr, Pellet Target, Energy-Loss, Drift Tubes, Nuclear Experiment, physics.ins-det, detectors

Abstract

This document describes the technical layout and the expected performance of the Straw Tube Tracker (STT), the main tracking detector of the P− ANDA target spectrometer. The STT encloses a Micro-Vertex-Detector (MVD) for the inner tracking and is followed in beam direction by a set of GEM stations. The tasks of the STT are the measurement of the particle momentum from the reconstructed trajectory and the measurement of the specific energy loss for a particle identification. Dedicated simulations with full analysis studies of certain proton-antiproton reactions, identified as being benchmark tests for the whole P− ANDA scientific program, have been performed to test the STT layout and performance. The results are presented, and the time lines to construct the STT are described.

Published

2013

7. Technical Design Report for the: PANDA Straw Tube Tracker

Author

Erni, W., Keshelashvili, I., Krusche, B., Steinacher, M., Heng, Y., Liu, Z., Liu, H., Shen, X., Wang, Q., Xu, H., Aab, A., Albrecht, M., Becker, J., Csap´o, A., Feldbauer, F., Fink, M., Friedel, P., Heinsius, F. H., Held, T., Klask, L., Koch, H., Kopf, B., Leiber, S., Leyhe, M., Motzko, C., Peliz¨aus, M., Pychy, J., Roth, B., Schr¨oder, T., Schulze, J., Sowa, C., Steinke, M., Trifterer, T., Wiedner, U., Zhong, J., Beck, R., Bianco, S., Brinkmann, K. T., Hammann, C., Hinterberger, F., Kaiser, D., Kliemt, R., Kube, M., Pitka, A., Quagli, T., Schmidt, C., Schmitz, R., Schnell, R., Thoma, U., Vlasov, P., Walther, D., Wendel, C., W¨urschig, T., Zaunick, H. G., Bianconi, A., Bragadireanu, M., Caprini, M., Pantea, D., Pantelica, D., Pietreanu, D., Serbina, L., Tarta, P. D., Kaplan, D., Fiutowski, T., Idzik, M., Mindur, B., Przyborowski, D., Swientek, K., Czech, B., Kistryn, M., Kliczewski, S., Kozela, A., Kulessa, P., Lebiedowicz, P., Pysz, K., Sch¨afer, W., Siudak, R., Szczurek, A., Jowzaee, S., Kajetanowicz, M., Kamys, B., Kistryn, S., Korcyl, G., Korcyl, K., Krzemien, W., Magiera, A., Moskal, P., Palka, M., Rudy, Z., Salabura, P., Smyrski, J., Wro´nska, A., Augustin, I., Lehmann, I., Nimorus, D., Schepers, G., Al Turany, M., Arora, R., Deppe, H., Flemming, H., Gerhardt, A., G¨otzen, K., Jordi, A. F., Kalicy, G., Karabowicz, R., Lehmann, D., Lewandowski, B., L¨uhning, J., Maas, F., Orth, H., Patsyuk, M., Peters, K., Saito, T., Schmidt, C. J., Schmitt, L., Schwarz, C., Schwiening, J., Traxler, M., Voss, B., Wieczorek, P., Wilms, A., Z¨uhlsdorf, M., Abazov, V. M., Alexeev, G., Arefiev, A., Astakhov, V. I., Barabanov, M. Y. u., Batyunya, B. V., Davydov, Y. u. I., Dodokhov, V. K. h., Efremov, A. A., Fedunov, A. G., Festchenko, A. A., Galoyan, A. S., Grigoryan, S., Karmokov, A., Koshurnikov, E. K., Lobanov, V. I., Lobanov, Y. u. Y. u., Makarov, A. F., Malinina, L. V., Malyshev, V. L., Mustafaev, G. A., Olshevskiy, A., Pasyuk, M. A., Perevalova, E. A., Piskun, A. A., Pocheptsov, T. A., Pontecorvo, G., Rodionov, V. K., Rogov, Y. u. N., Salmin, R. A., Samartsev, A. G., Sapozhnikov, M. G., Shabratova, G. S., Skachkova, A. N., Skachkov, N. B., Strokovsky, E. A., Suleimanov, M. K., Teshev, R. S. h., Tokmenin, V. V., Uzhinsky, V. V., Vodopyanov, A. S., Zaporozhets, S. A., Zhuravlev, N. I., Zorin, A. G., Branford, D., Glazier, D., Watts, D., Woods, P., Britting, A., Eyrich, W., Lehmann, A., Uhlig, F., Dobbs, S., Metreveli, Z., Seth, K., Tomaradze, A., Xiao, T., Bettoni, D., Carassiti, V., Cotta Ramusino, A., Dalpiaz, P., Drago, A., Fioravanti, E., Garzia, I., Savri`e, M., Stancari, G., Bianchi, N., Gianotti, P., A, Guaraldo, C., Lucherini, V., Orecchini, D., Pace, E., Bersani, A., Bracco, G., Macri, M., Parodi, R. F., Bremer, D., Dormenev, V., Drexler, P., D¨uren, M., Eissner, T., F¨ohl, K., Galuska, M., Gessler, T., Hayrapetyan, A., Hu, J., Koch, P., Kr¨ock, B., K¨uhn, W., Lange, S., Liang, Y., Merle, O., Metag, V., Moritz, M., M¨unchow, D., Nanova, M., Novotny, R., Spruck, B., Stenzel, H., Ullrich, T., Werner, M., Euan, C., Hoek, M., Ireland, D., Keri, T., Montgomery, R., Protopopescu, D., Rosner, G., Seitz, B., Babai, M., Glazenborg Kluttig, A., Kavatsyuk, M., Lemmens, P., Lindemulder, M., L¨ohner, H., Messchendorp, J., Moeini, H., Schakel, P., Schreuder, F., Smit, H., Tambave, G., van der Weele, J. C., Veenstra, R., Sohlbach, H., B¨uscher, M., Deermann, D., Dosdall, R., Esch, S., Gillitzer, A., Goldenbaum, F., Grunwald, D., Henssler, S., Herten, A., Hu, Q., Kemmerling, G., Kleines, H., Kozlov, V., Lehrach, A., Maier, R., Mertens, M., Ohm, H., Orfanitski, S., Prasuhn, D., Randriamalala, T., Ritman, J., R¨oder, M., Schadmand, S., Serdyuk, V., Sterzenbach, G., Stockmanns, T., Wintz, P., W¨ustner, P., Kisiel, J., Li, S., Li, Z., Sun, Z., Rigato, V., Fissum, S., Hansen, K., Isaksson, L., Lundin, M., Schr¨oder, B., Achenbach, P., Bleser, S., Cahit, U., Cardinali, M., Denig, A., Distler, M., Fritsch, M., Jasinski, P., Kangh, D., Karavdina, A., Lauth, W., Merkel, H., Michel, M., Mora Espi, M. C., M¨uller, U., Pochodzalla, J., Sanchez, S., Sanchezlorente, A., Schlimme, S., Sfienti, C., Thiel, M., Weber, T., Dormenev, V. I., Fedorov, A. A., Korzhik, M. V., Missevitch, O. V., Balanutsa, V., Chernetsky, V., Demekhin, A., Dolgolenko, A., Fedorets, P., Gerasimov, A., Goryachev, V., Varentsov, V., Boukharov, A., Malyshev, O., Marishev, I., Semenov, A., B¨ohmer, F., Dørheim, a. e. mail: p. a. o. l. a. g. i. a. n. o. t. t. i. @. l. n. f. i. n. f. n. it Page of S., Ketzer, B., Paul, S., Hergem¨oller, A. K., Khoukaz, A., K¨ohler, E., T¨aschner, A., Wessels, J., Varma, R., Chaterjee, A., Jha, V., Kailas, S., Roy, B. J., Yan, Y., Chinorat, K., Khanchai, K., Ayut, L., Pomrad, S., Baldin, E., Kotov, K., Peleganchuk, S., Tikhonov, Y. u., Boucher, J., Chambert, V., Dbeyssi, A., Gumberidze, M., Hennino, T., Imre, M., Kunne, R., Le Galliard, C., Ma, B., Marchand, D., Maroni, A., Ong, S., Ramstein, B., Rosier, P., Tomasi Gustafsson, E., Van de Wiele, J., Boca, G., Braghieri, A., Costanza, S., Genova, P., Lavezzi, L., Montagna, P., Rotondi, A., Abramov, V., Belikov, N., Davidenko, A., Derevschikov, A., Goncharenko, Y., Grishin, V., Kachanov, V., Konstantinov, D., Kormilitsin, V., Melnik, Y., Levin, A., Minaev, N., Mochalov, V., Morozov, D., Nogach, L., Poslavskiy, S., Ryazantsev, A., Ryzhikov, S., Semenov, P., Shein, I., Uzunian, A., Vasiliev, A., Yakutin, A., B¨ack, T., Cederwall, B., Mak´onyi, K., Tegn´er, P. E., von W¨urtemberg, K. M., Belostotski, S., Gavrilov, G., Itzotov, A., Kashchuk, A., Kisselev, A., Kravchenko, P., Levitskaya, O., Manaenkov, S., Miklukho, O., Naryshkin, Y., Veretennikov, D., Vikhrov, V., Zhadanov, A., Alberto, D., Amoroso, Antonio, Bussa, Maria Pia, Busso, Luigi, DE MORI, Francesca, Destefanis, MARCO GIOVANNI, Fava, L., Ferrero, Livio, Greco, Michela, Maggiora, Marco, Marcello, Simonetta, Sosio, Stefano, Spataro, STEFANO GIOVANNI, Zotti, Laura, Calvo, D., Coli, S., De Remigis, P., Filippi, A., Giraudo, G., Lusso, S., Mazza, G., Morra, O., Rivetti, A., Wheadon, R., Iazzi, F., Lavagno, A., Younis, H., Birsa, R., Bradamante, F., Bressan, A., Martin, A., Clement, H., Galander, B., Caldeira Balkest˚ahl, L., Cal´en, H., Fransson, K., Johansson, T., Kupsc, A., Marciniewski, P., Thom´e, E., Wolke, M., Zlomanczuk, J., D´ıaz, J., Ortiz, A., Dmowski, K., Duda, P., Korzeniewski, R., Slowinski, B., Chlopik, A., Guzik, Z., Kosinski, K., Melnychuk, D., Wasilewski, A., Wojciechowski, M., Wronka, S., Wysocka, A., Zwieglinski, B., B¨uhler, P., Hartman, O. N., Kienle, P., Marton, J., Suzuki, K., Widmann, E., Zmeskal, J., Institut de Physique Nucléaire d'Orsay (IPNO), Centre National de la Recherche Scientifique (CNRS)-Institut National de Physique Nucléaire et de Physique des Particules du CNRS (IN2P3)-Université Paris-Sud - Paris 11 (UP11), and PANDA

Subjects

High Energy Physics - Experiment (hep-ex), Computer Science::Hardware Architecture, Physics - Instrumentation and Detectors, hep-ex, Physics::Instrumentation and Detectors, [PHYS.HEXP]Physics [physics]/High Energy Physics - Experiment [hep-ex], FOS: Physical sciences, Instrumentation and Detectors (physics.ins-det), [PHYS.PHYS.PHYS-INS-DET]Physics [physics]/Physics [physics]/Instrumentation and Detectors [physics.ins-det], Detectors and Experimental Techniques, Nuclear Experiment, physics.ins-det, High Energy Physics - Experiment

Abstract

This document describes the technical layout and the expected performance of the Straw Tube Tracker (STT), the main tracking detector of the PANDA target spectrometer. The STT encloses a Micro-Vertex-Detector (MVD) for the inner tracking and is followed in beam direction by a set of GEM-stations. The tasks of the STT are the measurement of the particle momentum from the reconstructed trajectory and the measurement of the specific energy-loss for a particle identification. Dedicated simulations with full analysis studies of certain proton-antiproton reactions, identified as being benchmark tests for the whole PANDA scientific program, have been performed to test the STT layout and performance. The results are presented, and the time lines to construct the STT are described., Comment: accepted for publication on EPJA

Published

2012

8. Van een park voor de Jacht naar jacht voor het Park

Author

L. Hoedemaker, G.J. Spek, F. Ohl, L. Hoedemaker, G.J. Spek, and F. Ohl

Published

2014

9. Practical Guide to Music Notation for Composers, Arrangers and Editors

Author

Carl A. Rosenthal and John F. Ohl

Subjects

Musical notation, Literature, business.industry, Computer science, Library and Information Sciences, business, Music, Visual arts

Published

1968

10. Masterpieces of Music before 1750; An Anthology of Musical Examples from Gregorian Chant to J. S. Bach

Author

Charles Warren Fox, Carl Parrish, and John F. Ohl

Subjects

Literature, medicine.medical_specialty, business.industry, media_common.quotation_subject, Art history, Art, Musical, Library and Information Sciences, Semiology, medicine, Performance art, business, Music, media_common

Published

1951

11. Masterpieces of Music before 1750

Author

Denis Stevens, Carl Parrish, and John F. Ohl

Subjects

Music

Published

1953

12. Editorial: Women's cycling: specificities, situation and perspectives.

Author

Le Douairon Lahaye S and Ohl F

Abstract

Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Published

2024

13. The social grounds of self-tracking in insurance: A mixed-method approach to adoption and use.

Author

Presset B and Ohl F

Abstract

Scholars have explored the role of self-tracking in mediating people's values, perceptions, and practices. But little is known about its institutionalised forms, although it is becoming a routine component of health policies and insurance programs. Furthermore, the role of structural elements such as sociodemographic variables, socialisations, and trajectories has been neglected. Using both quantitative ( n   =  818) and qualitative ( n   =  44) data gathered from users and non-users of an insurance program's self-tracking intervention, and drawing from Bourdieu's theoretical framework, we highlight the impact of users' social background on the adoption and use of the technology. We show that older, poorer, and less educated individual are less likely to adopt the technology, and describe four prototypical categories of users, the meritocrats , the litigants , the scrutinisers and the good-intentioned . Each category displays different reasons and ways to use the technology that are grounded in users' socialisations and life trajectories. Results suggest that too much emphasis may have been put on self-tracking's transformative powers and not enough on its reproductive inertia, with important consequences for both scholars, designers, and public health stakeholders., Competing Interests: The authors declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article., (© The Author(s) 2023.)

Published

2023

14. Editorial: Youth and Winter Sports.

Author

Millet GP and Ohl F

Abstract

Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Published

2021

15. Monosynaptic Hippocampal-Prefrontal Projections Contribute to Spatial Memory Consolidation in Mice.

Author

Binder S, Mölle M, Lippert M, Bruder R, Aksamaz S, Ohl F, Wiegert JS, and Marshall L

Subjects

Animals, Electroencephalography, Male, Mice, Neural Pathways physiology, Neurons physiology, Optogenetics, Sleep physiology, Hippocampus physiology, Maze Learning physiology, Memory Consolidation physiology, Prefrontal Cortex physiology, Spatial Memory physiology

Abstract

Time locking between neocortical sleep slow oscillations, thalamo-cortical spindles, and hippocampal sharp-wave ripples has convincingly been shown to be a key element of systems consolidation. Here we investigate the role of monosynaptic projections from ventral/intermediate hippocampus to medial prefrontal cortex (mPFC) in sleep-dependent memory consolidation in male mice. Following acquisition learning in the Barnes maze, we optogenetically silenced the axonal terminals of hippocampal projections within mPFC during slow-wave sleep. This silencing during SWS selectively impaired recent but not remote memory in the absence of effects on error rate and escape latencies. Furthermore, it prevented the development of the most efficient search strategy and sleep spindle time-locking to slow oscillation. An increase in post-learning sleep sharp-wave ripple (SPWR) density and reduced time locking of learning-associated SPWR activity to sleep spindles may be a less specific response. Our results demonstrate that monosynaptic projections from hippocampus to mPFC contribute to sleep-dependent memory consolidation, potentially by affecting the temporal coupling of sleep-associated electrophysiological events. SIGNIFICANCE STATEMENT Convincing evidence supports the role of slow-wave sleep (SWS), and the relevance of close temporal coupling of neuronal activity between brain regions for systems consolidation. Less attention has been paid so far to the specific neuronal pathways underlying these processes. Here, we optogenetically silenced the direct monosynaptic projection from ventral/intermediate hippocampus (HC) to medial prefrontal cortex (mPFC) during SWS in male mice following repeated learning trials in a weakly aversive spatial task. Our results confirm the concept that the monosynaptic projection between HC and mPFC contributes to memory consolidation and support an important functional role of this pathway in shaping the temporal precision among sleep-associated electrophysiological events., (Copyright © 2019 the authors.)

Published

2019

16. Understanding the Paths to Appearance- and Performance-Enhancing Drug Use in Bodybuilding.

Author

Coquet R, Roussel P, and Ohl F

Abstract

How do gym-goers who are normally not inclined to resort to appearance- and performance-enhancing drugs (APEDs) progressively normalize their use? Based on data collected through a year and a half of participant observation in a gym and 30 semi-directive interviews with practitioners with varying profiles in French-speaking Switzerland, this article examines the evolution of practitioners' relations with APED use by articulating various levels of analysis. Associated with social vulnerabilities, the progressive normalization of APED use is concomitant with the "conversion" to bodybuilding. Our results show the extent to which and under what conditions interactions within the layout of gyms can influence practices. From refusal to normalization, our results suggest that APEDs and the associated beliefs coincide with career stages, which we aim to bring to light here.

Published

2018

17. Consomic mouse strain selection based on effect size measurement, statistical significance testing and integrated behavioral z-scoring: focus on anxiety-related behavior and locomotion.

Author

Labots M, Laarakker MC, Ohl F, and van Lith HA

Subjects

Animals, Anxiety genetics, Female, Male, Mice, Quantitative Trait Loci genetics, Species Specificity, Anxiety physiopathology, Behavior, Animal, Locomotion, Statistics as Topic

Abstract

Background: Selecting chromosome substitution strains (CSSs, also called consomic strains/lines) used in the search for quantitative trait loci (QTLs) consistently requires the identification of the respective phenotypic trait of interest and is simply based on a significant difference between a consomic and host strain. However, statistical significance as represented by P values does not necessarily predicate practical importance. We therefore propose a method that pays attention to both the statistical significance and the actual size of the observed effect. The present paper extends on this approach and describes in more detail the use of effect size measures (Cohen's d, partial eta squared - η p (2) ) together with the P value as statistical selection parameters for the chromosomal assignment of QTLs influencing anxiety-related behavior and locomotion in laboratory mice., Results: The effect size measures were based on integrated behavioral z-scoring and were calculated in three experiments: (A) a complete consomic male mouse panel with A/J as the donor strain and C57BL/6J as the host strain. This panel, including host and donor strains, was analyzed in the modified Hole Board (mHB). The consomic line with chromosome 19 from A/J (CSS-19A) was selected since it showed increased anxiety-related behavior, but similar locomotion compared to its host. (B) Following experiment A, female CSS-19A mice were compared with their C57BL/6J counterparts; however no significant differences and effect sizes close to zero were found. (C) A different consomic mouse strain (CSS-19PWD), with chromosome 19 from PWD/PhJ transferred on the genetic background of C57BL/6J, was compared with its host strain. Here, in contrast with CSS-19A, there was a decreased overall anxiety in CSS-19PWD compared to C57BL/6J males, but not locomotion., Conclusions: This new method shows an improved way to identify CSSs for QTL analysis for anxiety-related behavior using a combination of statistical significance testing and effect sizes. In addition, an intercross between CSS-19A and CSS-19PWD may be of interest for future studies on the genetic background of anxiety-related behavior.

Published

2016

18. Chromosomal assignment of quantitative trait loci influencing baseline circulating total cholesterol level in male laboratory mice: report of a consomic strain survey and comparison with published results.

Author

van Lith HA, Laarakker MC, Lozeman-van't Klooster JG, and Ohl F

Subjects

Age Factors, Animals, Body Weight, Cholesterol, HDL blood, Chromosome Mapping, Crosses, Genetic, Gene-Environment Interaction, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Phenotype, Photoperiod, Seasons, Time Factors, Cholesterol, HDL genetics, Chromosomes chemistry, Quantitative Trait Loci

Abstract

Background: An important risk for atherosclerosis is a low level of HDL cholesterol. Baseline HDL cholesterol is under complex genetic and environmental control. Here we report on results of male mice from a consomic strain survey and the parental inbred strains for baseline circulating total cholesterol concentration, which is almost the same as HDL cholesterol in chow fed mice. The consomic strains have been derived from C57BL/6J (host strain) and A/J (donor strain) inbred lines. The work contributes to the value of the mouse as an animal model for studying the genetic background of differences in baseline circulating total and HDL cholesterol levels., Results: The consomic strain survey suggested that mouse chromosomes 1, 7, 9, 14, 16, 17, 19, X, and Y contained at least one quantitative trait locus that is involved in baseline circulating total cholesterol concentration. All consomic lines, for which there is evidence that the substituted chromosome contains a quantitative trait locus, increase compared to the host strain baseline circulating total cholesterol concentration. Since there is evidence that 'body weight', 'age at blood sampling', 'time of the day blood was collected', and 'season' influence this phenotype, additional statistical analyses (with these variables as covariates) were performed. Now there is only evidence for quantitative trait loci on chromosomes 1, 8, 12, and Y. Taken the present results together with previous consomic strain surveys there is evidence that all mouse chromosomes carry quantitative trait loci that control baseline circulating total cholesterol levels. There was however little agreement between the present consomic strain results and previous sets of data. This might be explained by seasonal effects and differences in methodological variables such as age of the mice, fasting versus non-fasting, percentage of dietary fat, unanesthetized versus anesthetized mice, and the daily light-dark cycle., Conclusions: The present findings, when compared with previous consomic strain surveys, clearly illustrate the complexity of the genetic-environmental architecture for the regulation of baseline circulating total cholesterol levels in mice. Different data can be obtained from different labs and it underscores that animal geneticists should present as accurate a picture as possible of the laboratory mouse's environment.

Published

2015

19. Effects of Transfer from Breeding to Research Facility on the Welfare of Rats.

Author

Arts JW, Oosterhuis NR, Kramer K, and Ohl F

Abstract

Transfer from the breeding facility to a research facility is a stressful event for laboratory animals. Heat stress has been reported to constitute one of the major concerns during transport of animals. This study measured ambient and body temperature, corticosterone and glucose levels, body weight, behavior and water and food intake before, during and after transfer in Wistar rats. Decreased body weight, water and food intake were observed on the day of transfer in rats. Environmental temperature strongly affected body temperature of rats and needs to be controlled. Male rats need to habituate for at least one week, females for two weeks after transfer.

Published

2014

20. Sex Differences in Physiological Acclimatization after Transfer in Wistar Rats.

Author

Arts JW, Kramer K, Arndt SS, and Ohl F

Abstract

Most laboratory animals used in research are vendor-bred and transferred to research facilities. Transfer procedures might have considerable and unintended effects on research results. In the present study we compared physiological and behavioral parameters before and after external and internal transfer, as well as between transferred and non-transferred Wistar rats. The impact of both external and internal transfer on body weight, plasma corticosterone levels, heart rate, blood pressure, and locomotor activity was studied in both male and female Wistar rats, taking into account the sex differences in stress responsivity. External transfer was found to decrease body weight, increase plasma corticosterone, increase activity, increase heart rate in female rats, but decrease heart rate in male rats. Parameters showed differences between the sexes and light phases. This study shows that acclimatization after transfer is sex-specific and researchers should take the sex into consideration when determining the acclimatization period. It is recommended to allow for acclimatization of at least 8 days in males and two weeks in females after external transfer and timely (2 days before starting experiments) transfer the animals internally to the testing room.

Published

2014

21. Differential effects of diazepam and MPEP on habituation and neuro-behavioural processes in inbred mice.

Author

Salomons AR, Pinzon NE, Boleij H, Kirchhoff S, Arndt SS, Nordquist RE, Lindemann L, Jaeschke G, Spooren W, and Ohl F

Subjects

Animals, Male, Mice, Mice, 129 Strain, Mice, Inbred BALB C, Mice, Inbred Strains, Random Allocation, Avoidance Learning drug effects, Avoidance Learning physiology, Diazepam pharmacology, Habituation, Psychophysiologic drug effects, Habituation, Psychophysiologic genetics, Pyridines pharmacology

Abstract

Background: Previous studies have demonstrated a profound lack of habituation in 129P3 mice compared to the habituating, but initially more anxious, BALB/c mice. The present study investigated whether this non-adaptive phenotype of 129P3 mice is primarily based on anxiety-related characteristics., Methods: To test this hypothesis and extend our knowledge on the behavioural profile of 129P3 mice, the effects of the anxiolyticdiazepam (1, 3 and 5 mg/kg) and the putative anxiolytic metabotropic glutamate receptor 5 (mGlu5R) antagonist 2-methyl-6-(phenylethynyl)pyridine (MPEP, 3, 10 and 30 mg/kg) treatment on within-trial (intrasession) habituation, object recognition (diazepam: 1 mg/kg; MPEP 10 mg/kg) and on the central-nervous expression of the immediate early gene c-Fos (diazepam: 1 mg/kg; MPEP 10 mg/kg) were investigated., Results: Behavioural findings validated the initially high, but habituating phenotype of BALB/c mice, while 129P3 mice were characterized by impaired intrasession habituation. Diazepam had an anxiolytic effect in BALB/c mice, while in higher doses caused behavioural inactivity in 129P3 mice. MPEP revealed almost no anxiolytic effects on behaviour in both strains, but reduced stress-induced corticosterone responses only in 129P3 mice. These results were complemented by reduced expression of c-Fos after MPEP treatment in brain areas related to emotional processes, and increased c-Fos expression in higher integrating brain areas such as the prelimbic cortex compared to vehicle-treated 129P3 mice., Conclusions: These results suggest that the strain differences observed in (non)adaptive anxiety behaviour are at least in part mediated by differences in gamma-aminobutyric acid- A and mGluR5 mediated transmission.

Published

2012

22. Social contexts of sports-practicing youths' hazardous drinking.

Author

Bélanger RE, Ohl F, Berchtold A, Akre C, and Suris JC

Subjects

Adolescent, Age Factors, Female, Humans, Male, Sex Factors, Social Class, Switzerland, Young Adult, Alcohol Drinking psychology, Alcoholic Intoxication psychology, Athletes psychology, Peer Group, Social Environment

Abstract

Sports-practicing youths are at an elevated risk for alcohol use and misuse. Although much attention has recently been given to depicting subgroups facing the greatest threats, little evidence exists on the contexts in which their drinking takes place. Using data from a cross-sectional study on youth sports participation and substance use in the French-speaking part of Switzerland, this study focused on the social contexts associated with hazardous drinking of 894 sports-practicing adolescents aged 16 to 20. Divided between those who had been drunk in the last month (hazardous drinkers, n = 315) and those who had not (n = 579), sports-practicing adolescents were compared on reported gatherings (sports-related, sports-unrelated, mixed) likely linked to their drinking behaviour. Mixed social contexts, followed by sports-unrelated ones, were reported as the most common context by both male and female youths who practiced sports. After controlling for several possible confounders, male hazardous drinkers were more than 3 times more likely to report sports-unrelated social contexts as the most common, compared to sport-related ones, while females were more than 7 times more likely to do so. Our findings seem to indicate that, rather than focusing only on sports-related factors, prevention of alcohol misuse among sports-practicing youths should also pay attention to the social contextualisation of their hazardous drinking.

Published

2012

23. The impact of transportation on physiological and behavioral parameters in Wistar rats: implications for acclimatization periods.

Author

Arts JW, Kramer K, Arndt SS, and Ohl F

Subjects

Animal Welfare, Animals, Male, Random Allocation, Rats, Rats, Wistar, Stress, Physiological physiology, Acclimatization physiology, Behavior, Animal physiology, Transportation

Abstract

Transportation of laboratory rodents unavoidably causes stress. Nevertheless, very little is known about the effects of transportation and how long it takes for the animal to recuperate. In the present study, we investigated physiological and behavioral parameters before and after transportation in both transported and nontransported animals. We took blood samples to analyze plasma corticosterone and creatine kinase, and performed physiological measurements by means of telemetry, measuring heart rate, blood pressure, and activity. Behavior was measured by means of home cage observations. This study revealed that plasma corticosterone levels increased at least up to 16 days after transportation, blood pressure and heart rate showed a lasting decrease after transportation, grooming increased, and social interactions and locomotor activity decreased after transportation. With these data we demonstrate that there is a long-lasting effect of transportation on physiological and behavioral parameters. Our results show that the stressful impact of transportation embraces all parts of the procedure, including for example the packing of the animals. Researchers must be aware of this impact and provide a sufficient acclimatization period to allow for the (re-)stabilization of parameters. Insufficient acclimatization periods endanger not only the reliability of research results but also the welfare of the animal used.

Published

2012

24. Not all mice are equal: welfare implications of behavioural habituation profiles in four 129 mouse substrains.

Author

Boleij H, Salomons AR, van Sprundel M, Arndt SS, and Ohl F

Subjects

Animals, Arousal physiology, Avoidance Learning physiology, Corticosterone blood, Crosses, Genetic, Exploratory Behavior physiology, Feeding Behavior physiology, Female, Latency Period, Psychological, Locomotion physiology, Male, Mice, Mice, 129 Strain, Risk Assessment, Animal Welfare, Behavior, Animal physiology, Habituation, Psychophysiologic

Abstract

Safeguarding the welfare of animals is an important aim when defining housing and management standards in animal based, experimental research. While such standards are usually defined per animal species, it is known that considerable differences between laboratory mouse strains exist, for example with regard to their emotional traits. Following earlier experiments, in which we found that 129P3 mice show a lack of habituation of anxiety related behaviour after repeated exposure to an initially novel environment (non-adaptive profile), we here investigated four other 129 inbred mouse substrains (129S2/SvPas, 129S2/SvHsd (exp 1); 129P2 and 129X1 (exp 2)) on habituation of anxiety related behaviour. Male mice of each strain were repeatedly placed in the modified hole board test, measuring anxiety-related behaviour, exploratory and locomotor behaviour. The results reveal that all four substrains show a lack of habituation behaviour throughout the period of testing. Although not in all of the substrains a possible confounding effect of general activity can be excluded, our findings suggest that the genetic background of the 129 substrains may increase their vulnerability to cope with environmental challenges, such as exposure to novelty. This vulnerability might negatively affect the welfare of these mice under standard laboratory conditions when compared with other strains. Based on our findings we suggest to consider (sub)strain-specific guidelines and protocols, taking the (subs)train-specific adaptive capabilities into account.

Published

2012

25. Critical evaluation of the use of dogs in biomedical research and testing in Europe.

Author

Hasiwa N, Bailey J, Clausing P, Daneshian M, Eileraas M, Farkas S, Gyertyán I, Hubrecht R, Kobel W, Krummenacher G, Leist M, Lohi H, Miklósi A, Ohl F, Olejniczak K, Schmitt G, Sinnett-Smith P, Smith D, Wagner K, Yager JD, Zurlo J, and Hartung T

Subjects

Animal Rights, Animals, Animals, Laboratory, Biomedical Research ethics, Disease Models, Animal, Dog Diseases chemically induced, Dog Diseases therapy, Drug-Related Side Effects and Adverse Reactions, Europe, Pesticides adverse effects, Pets, Veterinary Medicine methods, Animal Use Alternatives methods, Biomedical Research methods, Dogs physiology

Abstract

Dogs are sometimes referred to as "man's best friend" and with the increase in urbanization and lifestyle changes, dogs are seen by their owners as family members. Society expresses specific concerns about the experimental use of dogs, as they are sometimes perceived to have a special status for humans. This may appear somewhat conflicting with the idea that the intrinsic value of all animals is the same, and that also several other animal species are used in biomedical research and toxicology. This aspect and many others are discussed in an introductory chapter dealing with ethical considerations on the use of dogs as laboratory animals. The report gives an overview on the use of dogs in biomedical research, safety assessment and the drug developmental process and reflects the discussion on the use of dogs as second (non-rodent)species in toxicity testing. Approximately 20,000 dogs are used in scientific procedures in Europe every year, and their distinct genetic, physiological and behavioral characteristics may support their use as models for e.g. behavioral analysis and genetic research. Advances in the 3Rs (Replacement, Reduction and Refinement of experiments using dogs) are described, potential opportunities are discussed and recommendations for further progress in this area are made.

Published

2011

26. A framework program for the teaching of alternative methods (replacement, reduction, refinement) to animal experimentation.

Author

Daneshian M, Akbarsha MA, Blaauboer B, Caloni F, Cosson P, Curren R, Goldberg A, Gruber F, Ohl F, Pfaller W, van der Valk J, Vinardell P, Zurlo J, Hartung T, and Leist M

Subjects

Animals, Curriculum, Drug and Narcotic Control legislation & jurisprudence, Education, Ethics, Research, Public Opinion, Reproducibility of Results, Animal Testing Alternatives methods, Hazardous Substances toxicity, Research Design

Abstract

Development of improved communication and education strategies is important to make alternatives to the use of animals, and the broad range of applications of the 3Rs concept better known and understood by different audiences. For this purpose, the Center for Alternatives to Animal Testing in Europe (CAAT-Europe) together with the Transatlantic Think Tank for Toxicology (t(4)) hosted a three-day workshop on "Teaching Alternative Methods to Animal Experimentation". A compilation of the recommendations by a group of international specialists in the field is summarized in this report. Initially, the workshop participants identified the different audience groups to be addressed and also the communication media that may be used. The main outcome of the workshop was a framework for a comprehensive educational program. The modular structure of the teaching program presented here allows adaptation to different audiences with their specific needs; different time schedules can be easily accommodated on this basis. The topics cover the 3Rs principle, basic research, toxicological applications, method development and validation, regulatory aspects, case studies and ethical aspects of 3Rs approaches. This expert consortium agreed to generating teaching materials covering all modules and providing them in an open access online repository.

Published

2011

27. Identification methods in newborn C57BL/6 mice: a developmental and behavioural evaluation.

Author

Castelhano-Carlos MJ, Sousa N, Ohl F, and Baumans V

Subjects

Animals, Animals, Newborn, Mice, Reflex physiology, Animal Identification Systems methods, Animals, Laboratory growth & development, Mice, Inbred C57BL growth & development

Abstract

The use of group-housed rodents in many fields of biomedical research imposes a need to identify individuals in a cage. Few studies have been designed to assess possible negative effects of identification methods of newborn mice on their development and wellbeing. In the present study, three different identification methods were applied to newborn C57BL/6J mice on postnatal day (pnd) 5 (toe clipping, toe tattoo ink puncture and subcutaneous implantation of a small transponder). All identification methods used proved to be effective for long-term marking of individual animals. Newborn mice showed the least reaction to toe clipping followed by toe tattoo ink puncture and transponder implantation was the most distressful individual identification procedure in newborn mice. Importantly, clipped toe tissue proved to be enough for genotyping purposes. No overall consistent differences in somatic and neurological reflex development during the postnatal period were shown as a result of the newborn individual identification procedures used. Further, none of the methods interfered significantly with the adult animals' general normal behaviour (e.g. ability to move, grasp, climb) and sensory-motor functions as assessed with a simplified SHIRPA battery of tests, as well as Rotarod and Elevated Plus Maze tests. Postmortem thymus and adrenal gland weights gave no indication of chronic stress as a consequence of the identification method. We conclude that toe clipping might even be advisable in newborn mice at a very young age, when genotyping is needed. Toe tattoo ink puncture is also a good identification method for newborn mice and transponder implantation should only be used in older newborns or applied at weaning.

Published

2010

28. Identifying emotional adaptation: behavioural habituation to novelty and immediate early gene expression in two inbred mouse strains.

Author

Salomons AR, van Luijk JA, Reinders NR, Kirchhoff S, Arndt SS, and Ohl F

Subjects

Animals, Anxiety Disorders, Cognition, Color, Corticosterone blood, Disease Models, Animal, Habituation, Psychophysiologic physiology, Immunohistochemistry, Lighting, Male, Mice, Mice, Inbred BALB C, Motor Activity, Pattern Recognition, Visual, Proto-Oncogene Proteins c-fos metabolism, Stress, Psychological etiology, Adaptation, Psychological, Anxiety psychology, Exploratory Behavior, Gene Expression, Genes, Immediate-Early, Habituation, Psychophysiologic genetics, Mice, Inbred Strains

Abstract

Normal anxiety is an adaptive emotional response. However, when anxiety appears to lack adaptive value, it might be defined as pathological. Adaptation in animals can be assessed for example by changes in behavioural responses over time, i.e. habituation. We hypothesize that non-adaptive anxiety might be reflected by impaired habituation. To test our hypothesis, we repeatedly exposed male mice from two inbred strains to a novel environment, the modified hole board. BALB/cJ mice were found to be initially highly anxious, but subsequently habituated to the test environment. In contrast, 129P3/J mice initially showed less anxiety-related behaviour compared with the BALB/cJ mice but no habituation in anxiety-related behaviour was observed. Notably, anxiety-related behaviour even increased during the experimental period. Complementary, 129P3/J mice did not show habituation in other parameters such as locomotor and exploratory activity, whereas significant changes appeared in these behaviours in BALB/c mice. Finally, the expression of the immediate early gene c-fos differed between the two strains in distinct brain areas, known to regulate the integration of emotional and cognitive processes. These results suggest that 129P3/J mice might be a promising (neuro)-behavioural animal model for non-adaptive, i.e. pathological anxiety.

Published

2010

29. Chromosomal assignment of quantitative trait loci influencing modified hole board behavior in laboratory mice using consomic strains, with special reference to anxiety-related behavior and mouse chromosome 19.

Author

Laarakker MC, Ohl F, and van Lith HA

Subjects

Animals, Arousal, Crosses, Genetic, Exploratory Behavior, Memory, Mice, Motivation, Motor Activity, Risk Assessment, Anxiety genetics, Chromosome Mapping, Mice, Inbred C57BL genetics, Quantitative Trait Loci

Abstract

Male mice from a panel of chromosome substitution strains (CSS, also called consomic strains or lines)--in which a single full-length chromosome from the A/J inbred strain has been transferred onto the genetic background of the C57BL/6J inbred strain--and the parental strains were examined in the modified hole board test. This behavioral test allows to assess for a variety of different motivational systems in parallel (i.e. anxiety, risk assessment, exploration, memory, locomotion, and arousal). Such an approach is essential for behavioral characterization since the motivational system of interest is strongly influenced by other behavioral systems. Both univariate and bivariate analyses, as well as a factor analysis, were performed. The C57BL/6J and A/J mouse parental inbred strains differed in all motivational systems. The chromosome substitution strain survey indicated that nearly all mouse chromosomes (with the exception of chromosome 2) each contain at least one quantitative trait locus (QTL) that is involved in modified hole board behavior. The results agreed well with previous reports of QTLs for anxiety-related behavior using the A/J and C57BL/6J as parental strains. The present study confirmed that mouse chromosomes 5, 8, 10, 15, 18 and 19 likely contain at least one anxiety QTL. There was also evidence for a novel anxiety QTL on the Y chromosome. With respect to anxiety-related avoidance behavior towards an unprotected area, we have special interest for mouse chromosome 19. CSS-19 (C57BL/6J-Chr19(A)/NaJ) differed in avoidance behavior from the C57BL/6J, but not in locomotion. Thus pleiotropic contribution of locomotion could be excluded.

Published

2008

30. Effects of light or dark phase testing on behavioural and cognitive performance in DBA mice.

Author

Roedel A, Storch C, Holsboer F, and Ohl F

Subjects

Animals, Male, Mice, Mice, Inbred DBA, Behavior, Animal physiology, Behavior, Animal radiation effects, Circadian Rhythm physiology, Cognition physiology, Cognition radiation effects, Darkness, Light

Abstract

Behavioural experiments in mice are often carried out during the resting phase of these nocturnal animals. Ignoring the fact that mice are more active during the dark period, results from resting-phase testing has also been used to characterize these animals. Since the influence of the light/dark cycle on testing is likely to be a relevant factor for the analysis of behavioural results, the aim of this study was to evaluate the effects of the relative time of the day as well as light conditions during testing on behavioural and cognitive performance in inbred mice. Naïve DBA/2N (DBA) mice were tested in the modified hole board (mHB) either during the dark phase under red light or during the light phase under white light. Different behavioural dimensions and cognitive functions were evaluated in parallel. Depending on the testing conditions, the results showed significant differences in behavioural activity, with DBA mice being less inhibited during dark phase. The same experimental group made fewer memory errors in a visuo-spatial task and showed a faster habituation compared with the group tested during the dark phase. From the results we conclude that testing during the light phase induces a pronounced behavioural inhibition as well as a cognitive disruption in DBA mice, which should be taken into account when cognitively testing these animals.

Published

2006

31. Gene expression studies in prostate cancer tissue: which reference gene should be selected for normalization?

Author

Ohl F, Jung M, Xu C, Stephan C, Rabien A, Burkhardt M, Nitsche A, Kristiansen G, Loening SA, Radonić A, and Jung K

Subjects

Aged, Carcinoma genetics, Carcinoma metabolism, Carcinoma pathology, Gene Expression Profiling methods, Humans, Male, Middle Aged, Prostatic Neoplasms metabolism, Prostatic Neoplasms pathology, RNA, Messenger genetics, Reference Standards, Reverse Transcriptase Polymerase Chain Reaction, Gene Expression Profiling standards, Gene Expression Regulation, Neoplastic, Genes, Prostatic Neoplasms genetics, RNA, Messenger metabolism

Abstract

Using quantitative reverse transcription-polymerase chain reaction (RT-PCR), reference genes are utilized as endogenous controls for relative quantification of target genes in gene profiling studies. The suitability of housekeeping genes for that purpose in prostate cancer tissue has not been sufficiently investigated so far. The objective of this study was to select from a panel of 16 potential candidate reference genes the most stable genes for gene normalization. Expression of mRNA encoding ACTB, ALAS1, ALB, B2M, G6PD, GAPD, HMBS, HPRT1, K-ALPHA-1, POLR2A, PPIA, RPL13A, SDHA, TBP, UBC, and YWHAZ was examined in matched, microdissected malignant and nonmalignant tissue specimens obtained from 17 nontreated prostate carcinomas after radical prostatectomy by real-time RT-PCR. The genes studied displayed a wide expression range with cycle threshold values between 16 and 37. The expression was not different between samples from pT2 and pT3 tumors or between samples with Gleason scores <7 and >or=7 (P>0.05). ACTB, RPL13A, and HMBS showed significant differences (P<0.02 at least) in expressions between malignant and nonmalignant pairs. All other genes did not differ between the matched pairs, and the software programs geNorm and NormFinder were used to ascertain the most suitable reference genes from these candidates. HPRT1, ALAS1, and K-ALPHA-1 were calculated by both programs to be the most stable genes covering a broad range of expression. The expression of the target gene RECK normalized with HRPT1 alone and with the normalization factors generated by the combination of these three reference genes as well as with the unstable genes ACTB or RPL13A is given. That example shows the significance of using suitable reference genes to avoid erroneous normalizations in gene profiling studies for prostate cancer. The use of HPRT1 alone as a reference gene shown in our study was sufficient, but the normalization factors generated from two (HRPT1, ALAS1) or all three genes (HRPT1, ALAS1, K-ALPHA-1) should be considered for an improved reliability of normalization in gene profiling studies of prostate cancer.

Published

2005

32. Reduction of hypothalamic vasopressinergic hyperdrive contributes to clinically relevant behavioral and neuroendocrine effects of chronic paroxetine treatment in a psychopathological rat model.

Author

Keck ME, Welt T, Müller MB, Uhr M, Ohl F, Wigger A, Toschi N, Holsboer F, and Landgraf R

Subjects

Animals, Anxiety Disorders drug therapy, Hypothalamus metabolism, Male, Neurosecretory Systems metabolism, RNA, Messenger biosynthesis, Rats, Species Specificity, Vasopressins antagonists & inhibitors, Anxiety Disorders metabolism, Disease Models, Animal, Hypothalamus drug effects, Neurosecretory Systems drug effects, Paroxetine administration & dosage, Vasopressins biosynthesis

Abstract

The neuroendocrine and behavioral effects of chronic paroxetine treatment were investigated in two rat lines selectively bred for high anxiety-related behavior (HAB) or low anxiety-related behavior (LAB) emotionality. In addition to a characteristic behavioral phenotype with markedly passive stress-coping strategies, HAB rats show a hypothalamic vasopressinergic hyperdrive that is causally related to hypothalamic-pituitary-adrenocortical dysregulation as demonstrated in the combined dexamethasone (DEX)/corticotropin-releasing hormone (CRH) test. A total of 8 weeks of chronic paroxetine treatment induced a more active coping strategy in the forced swim test in HAB rats only. In contrast, paroxetine-treated LAB rats did not change their swimming behavior. To investigate the neuroendocrine alterations linked to these behavioral changes, a combined DEX/CRH test was performed. In HAB rats, the paroxetine-induced behavioral changes towards more active coping strategies were accompanied by a normalization of the CRH-stimulated increase in corticotropin (ACTH) and corticosterone secretion. Concomitantly, the hypothalamic vasopressinergic hyperdrive was found to be reduced in HAB but not LAB rats, as indicated by a decrease in vasopressin mRNA expression, whereas vasopressin 1a receptor binding was unaffected. These findings provide the first evidence that the vasopressinergic system is likely to be critically involved in the behavioral and neuroendocrine effects of antidepressant drugs. This novel mechanism of action of paroxetine on vasopressin gene regulation renders vasopressinergic neuronal circuits a promising target for the development of more causal antidepressant treatment strategies.

Published

2003

33. Memory consolidation for the discrimination of frequency-modulated tones in mongolian gerbils is sensitive to protein-synthesis inhibitors applied to the auditory cortex.

Author

Kraus M, Schicknick H, Wetzel W, Ohl F, Staak S, and Tischmeyer W

Subjects

Acoustic Stimulation, Animals, Auditory Cortex drug effects, Auditory Perception drug effects, Auditory Perception physiology, Discrimination Learning physiology, Emetine pharmacology, Gerbillinae, Male, Memory physiology, Microinjections, Anisomycin pharmacology, Auditory Cortex physiology, Discrimination Learning drug effects, Memory drug effects, Protein Synthesis Inhibitors pharmacology

Abstract

Differential conditioning of Mongolian gerbils to linearly frequency-modulated tones (FM) has recently received experimental attention. In the study of the role of cerebral protein synthesis for FM discrimination memory, gerbils received post-training bilateral injections of anisomycin into the auditory cortex under light halothane anesthesia. Compared with saline-treated controls, anisomycin-treated gerbils showed a discrimination decrement during the subsequent three days of training. They markedly improved their performance within training sessions, but started each session at low levels. When repeatedly trained gerbils received post-session injections of anisomycin, discrimination performance during subsequent sessions was similar to the pre-injection performance, indicating that retention, retrieval, reconsolidation, and expression of the established reaction were not affected. However, the improvement of a partially established discrimination reaction was impaired after this treatment. Intracortical injections of emetine confirmed this finding. Neither drug affected FM discrimination learning when given several days before the initial training. Our results suggest that protein-synthesis inhibitors applied to the auditory cortex of gerbils during the post-acquisition phase interfered with learning and memory-related aspects of FM processing. The resulting deficit was evident for a number of post-injection training days. This effect was probably due to impaired consolidation, i.e., processes required for long-term stabilization or retrieval of the memory trace while leaving short-term memory intact.

Published

2002

34. Mechanisms underlying the protective potential of alpha-tocopherol (vitamin E) against haloperidol-associated neurotoxicity.

Author

Post A, Rücker M, Ohl F, Uhr M, Holsboer F, Almeida OF, and Michaelidis TM

Subjects

Animals, Antioxidants therapeutic use, Antipsychotic Agents toxicity, Apoptosis drug effects, Apoptosis physiology, Cell Line, Haloperidol toxicity, Hippocampus metabolism, Hippocampus pathology, Male, Mice, Motor Activity drug effects, Motor Activity physiology, NF-kappa B biosynthesis, Neurotoxins pharmacology, Oxidative Stress drug effects, Oxidative Stress physiology, Protective Agents pharmacology, Protective Agents therapeutic use, Rats, Rats, Wistar, alpha-Tocopherol therapeutic use, Antioxidants pharmacology, Antipsychotic Agents pharmacology, Haloperidol pharmacology, Hippocampus drug effects, alpha-Tocopherol pharmacology

Abstract

The undesired side-effects of haloperidol treatment include a number of extrapyramidal side-effects which have been proposed to result from drug-induced damage to the basal ganglia. The drug also causes irregular movements and locomotor patterns in experimental animals. Here we show that haloperidol treatment in rats is associated with increases in the expression of p53 and the ratio of pro-apoptotic (Bax) to anti-apoptotic (Bcl-2/Bcl-x(L)) proteins in the hippocampus and caudate putamen (CPu). In addition, haloperidol induces the DNA binding activity of the redox-sensitive nuclear factor-kappa B (NF-kappaB) and concomitantly upregulates the levels of the phosphorylated form of IkappaBalpha protein in vivo. Similar responses are observed when a mouse hippocampal cell line (HT-22) is treated with haloperidol and/or vitamin E. Interestingly, all of these biochemical effects of haloperidol are significantly attenuated when animals or cultured cells are pretreated with alpha-tocopherol (vitamin E). Consistent with this, vitamin E is demonstrated to substantially reduce the haloperidol-induced impairment of locomotor activity in rats. Collectively, the data indicate the usefulness of vitamin E as an adjunct to haloperidol treatment and provide initial clues about the underlying molecular mechanisms involved in these effects.

Published

2002

35. The modified hole board as a differential screen for behavior in rodents.

Author

Ohl F, Holsboer F, and Landgraf R

Subjects

Analysis of Variance, Animals, Male, Rats, Rats, Wistar, Social Isolation, Statistics, Nonparametric, Behavior, Animal, Behavioral Sciences instrumentation

Abstract

We describe a modified hole board (mHB) paradigm as a test for unconditioned behavior in rodents that is aimed at analyzing a variety of behavioral dimensions. We demonstrate that the mHB enables the investigation of different behavioral dimensions in rodents in only one test by reproducing the behavioral characteristics previously collected from multiple behavioral tests in rats bred for either high or low anxiety-related behavior. In addition, the test design, which allows the experimental animal to maintain social contact with its group mates during the test, was shown to minimize stress for experimental animals and, moreover, to enable the investigator to assess social affinity among group mates. In summary, the mHB test enables animal models to be comprehensively phenotyped, while simultaneously reducing the number of animals and the amount of time required. Therefore, the mHB represents an alternative to the common practice of using a series of more specific tests.

Published

2001

36. Evaluation of hypothalamo-pituitary-adrenal activity in the tree shrew (Tupaia belangeri) via salivary cortisol measurement.

Author

Ohl F, Kirschbaum C, and Fuchs E

Subjects

Animals, Learning physiology, Male, Specimen Handling methods, Specimen Handling veterinary, Stress, Psychological, Adrenal Glands physiology, Hydrocortisone analysis, Hypothalamus physiology, Pituitary Gland physiology, Saliva chemistry, Tupaiidae physiology

Abstract

Saliva sampling is frequently used in humans for adrenal glucocorticoid hormone analysis because of advantages such as non-invasiveness, the ease of collection, and storing of the samples. To transfer this advantageous method to laboratory mammals, potentially confounding factors such as stressful handling procedures have to be excluded. In the present study we established a method for collecting saliva for cortisol measurement in freely moving adult male tree shrews (Tupaia belangeri). The practicability of the procedure was demonstrated (i) by stress-induced changes in cortisol levels revealing a significant increase during the stress phase (control = 0.91 nmol/l vs stress = 1.71 nmol/l), and (ii) by reporting no significant differences in salivary cortisol levels before and after performance of a learning task. The present study emphasizes the use of salivary cortisol analysis especially for monitoring acute changes in the hypothalamo-pituitary-adrenal axis activity in male tree shrews.

Published

1999