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Your search keyword '"Belohradsky, B. H."' showing total 98 results
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98 results on '"Belohradsky, B. H."'

1. The PedPAD study: boys predominate in the hypogammaglobulinaemia registry of the ESID online database

Author

Schatorjé, E. J. H., Gathmann, B., van Hout, R. W. N. M., de Vries, E., Alsina, L, Baumann, U, Belohradsky, B H, Bienemann, K, Boardman, B, Borte, M, Bredius, R G, Brodszki, N, Caracseghi, F, Ciznar, P, de Vries, E, Driessen, G J, Dückers, G, Duppenthaler, A, Farmaki, E, Galal, N, Gennery, A, Gonzalez-Granado, L I, Hlavackova, E, Hoernes, M, Kilic, S S, Krüger, R, Kuijpers, T W, Kütükcüler, N, Llobet, P, Marques, L, van Montfrans, J M, Papadopoulou-Alataki, E, Paschenko, O, Pasic, S, Pietrogrande, M C, Pignata, C, Reda, S M, Reisli, I, Roesler, J, Santos, J L, Schölvinck, E H, Schulze, Ilka, Seidel, M G, Shcherbina, A, Sundin, M, Szaflarska, A, Velbri, S, Warnatz, K, and Warris, A

Published
2014
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2. The German national registry for primary immunodeficiencies (PID)

Author

Gathmann, B., Goldacker, S., Klima, M., Belohradsky, B. H., Notheis, G., Ehl, S., Ritterbusch, H., Baumann, U., Meyer-Bahlburg, A., Witte, T., Schmidt, R., Borte, M., Borte, S., Linde, R., Schubert, R., Bienemann, K., Laws, H.-J., Dueckers, G., Roesler, J., Rothoeft, T., Krüger, R., Scharbatke, E. C., Masjosthusmann, K., Wasmuth, J.-C., Moser, O., Kaiser, P., Gro-Wieltsch, U., Classen, C. F., Horneff, G., Reiser, V., Binder, N., El-Helou, S. M., Klein, C., Grimbacher, B., and Kindle, G.

Published
2013
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4. Clinical spectrum of immunodeficiency, centromeric instability and facial dysmorphism (ICF syndrome)

Author

Hagleitner, M M, Lankester, A, Maraschio, P, Hultén, M, Fryns, J P, Schuetz, C, Gimelli, G, Davies, E G, Gennery, A, Belohradsky, B H, de Groot, R, Gerritsen, E J A, Mattina, T, Howard, P J, Fasth, A, Reisli, I, Furthner, D, Slatter, M A, Cant, A J, Cazzola, G, van Dijken, P J, van Deuren, M, de Greef, J C, van der Maarel, S M, and Weemaes, C M R

Published
2008
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12. Harnwegsinfektionen

Author

Scholz, H, Belohradsky, B H, Bialek, R, Heininger, U, Kreth, H W, Roos, R, Scholz, H ( H ), Belohradsky, B H ( B H ), Bialek, R ( R ), Heininger, U ( U ), Kreth, H W ( H W ), Roos, R ( R ), Nadal, D, Beetz, R, Kuwertz-Bröking, E, Misselwitz, J, Rascher, W, Rösch, W, Schulte-Wissermann, H, Scholz, H, Belohradsky, B H, Bialek, R, Heininger, U, Kreth, H W, Roos, R, Scholz, H ( H ), Belohradsky, B H ( B H ), Bialek, R ( R ), Heininger, U ( U ), Kreth, H W ( H W ), Roos, R ( R ), Nadal, D, Beetz, R, Kuwertz-Bröking, E, Misselwitz, J, Rascher, W, Rösch, W, and Schulte-Wissermann, H

Published
2013

13. A human immunodeficiency syndrome caused by mutations in CARMIL2

Author

Schober, T., primary, Magg, T., additional, Laschinger, M., additional, Rohlfs, M., additional, Linhares, N. D., additional, Puchalka, J., additional, Weisser, T., additional, Fehlner, K., additional, Mautner, J., additional, Walz, C., additional, Hussein, K., additional, Jaeger, G., additional, Kammer, B., additional, Schmid, I., additional, Bahia, M., additional, Pena, S. D., additional, Behrends, U., additional, Belohradsky, B. H., additional, Klein, C., additional, and Hauck, F., additional

Published
2017
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14. Hirnabszess und intrakraniales Epyem

Author

Scholz, H, Belohradsky, B H, Bialek, R, Heininger, U, Kreth, H W, Roos, R, Scholz, H ( H ), Belohradsky, B H ( B H ), Bialek, R ( R ), Heininger, U ( U ), Kreth, H W ( H W ), Roos, R ( R ), Berger, C, Schroten, H, Adam, R, Noack, R, Schaad, U B, Tenenbaum, T, Scholz, H, Belohradsky, B H, Bialek, R, Heininger, U, Kreth, H W, Roos, R, Scholz, H ( H ), Belohradsky, B H ( B H ), Bialek, R ( R ), Heininger, U ( U ), Kreth, H W ( H W ), Roos, R ( R ), Berger, C, Schroten, H, Adam, R, Noack, R, Schaad, U B, and Tenenbaum, T

Published
2009

15. Bartonellosen

Author

Scholz, H, Belohradsky, B H, Bialek, R, Heininger, U, Kreth, H W, Roos, R, Scholz, H ( H ), Belohradsky, B H ( B H ), Bialek, R ( R ), Heininger, U ( U ), Kreth, H W ( H W ), Roos, R ( R ), Nadal, D, Kempf, V, Lutz, E, Oehme, A, Scholz, H, Belohradsky, B H, Bialek, R, Heininger, U, Kreth, H W, Roos, R, Scholz, H ( H ), Belohradsky, B H ( B H ), Bialek, R ( R ), Heininger, U ( U ), Kreth, H W ( H W ), Roos, R ( R ), Nadal, D, Kempf, V, Lutz, E, and Oehme, A

Published
2009

18. X-linked inhibitor of apoptosis (XIAP) deficiency: The spectrum of presenting manifestations beyond hemophagocytic lymphohistiocytosis

Author

Speckmann, C., Lehmberg, K., Albert, M. H., Damgaard, R. B., Fritsch, M., Gyrd-Hansen, M., Rensing-Ehl, A., Vraetz, T., Grimbacher, B., Salzer, U., Fuchs, I., Ufheil, H., Belohradsky, B. H., Hassan, A., Cale, C. M., Elawad, M., Strahm, B., Schibli, S., Lauten, M., Kohl, M., Meerpohl, J. J., Rodeck, B., Kolb, R., Eberl, W., Soerensen, J., von Bernuth, H., Lorenz, M., Schwarz, K., zur Stadt, U., Ehl, S., Speckmann, C., Lehmberg, K., Albert, M. H., Damgaard, R. B., Fritsch, M., Gyrd-Hansen, M., Rensing-Ehl, A., Vraetz, T., Grimbacher, B., Salzer, U., Fuchs, I., Ufheil, H., Belohradsky, B. H., Hassan, A., Cale, C. M., Elawad, M., Strahm, B., Schibli, S., Lauten, M., Kohl, M., Meerpohl, J. J., Rodeck, B., Kolb, R., Eberl, W., Soerensen, J., von Bernuth, H., Lorenz, M., Schwarz, K., zur Stadt, U., and Ehl, S.

Abstract

X-linked inhibitor of apoptosis (XIAP) deficiency caused by mutations in BIRC4 was initially described in patients with X-linked lymphoproliferative syndrome (XLP) who had no mutations in SH2D1A. In the initial reports, EBV-associated hemophagocytic lymphohistiocytosis (HLH) was the predominant clinical phenotype. Among 25 symptomatic patients diagnosed with XIAP deficiency, we identified 17 patients who initially presented with manifestations other than HLH. These included Crohn-like bowel disease (n = 6), severe infectious mononucleosis (n = 4), isolated splenomegaly (n = 3), uveitis (n = 1), periodic fever (n = 1), fistulating skin abscesses (n = 1) and severe Giardia enteritis (n = 1). Subsequent manifestations included celiac-like disease, antibody deficiency, spienomegaly and partial HLH. Screening by flow cytometry identified 14 of 17 patients in our cohort. However, neither genotype nor protein expression nor results from cell death studies were clearly associated with the clinical phenotype. Only mutation analysis can reliably identify affected patients. XIAP deficiency must be considered in a wide range of clinical presentations. (C) 2013 Elsevier Inc. All rights reserved.

Published
2013

19. Clinical and functional characterisation of a novel TNFRSF1A c.605T>A/V173D cleavage site mutation associated with tumour necrosis factor receptor-associated periodic fever syndrome (TRAPS), cardiovascular complications and excellent response to etanercept treatment

Author

Stojanov, S, primary, Dejaco, C, additional, Lohse, P, additional, Huss, K, additional, Duftner, C, additional, Belohradsky, B H, additional, Herold, M, additional, and Schirmer, M, additional

Published
2007
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20. Clinical spectrum of immunodeficiency, centromeric instability and facial dysmorphism (ICF syndrome)

Author

Hagleitner, M M, primary, Lankester, A, additional, Maraschio, P, additional, Hulten, M, additional, Fryns, J P, additional, Schuetz, C, additional, Gimelli, G, additional, Davies, E G, additional, Gennery, A, additional, Belohradsky, B H, additional, de Groot, R, additional, Gerritsen, E J A, additional, Mattina, T, additional, Howard, P J, additional, Fasth, A, additional, Reisli, I, additional, Furthner, D, additional, Slatter, M A, additional, Cant, A J, additional, Cazzola, G, additional, van Dijken, P J, additional, van Deuren, M, additional, de Greef, J C, additional, van der Maarel, S M, additional, and Weemaes, C M R, additional

Published
2007
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25. BTKbase, mutation database for X-linked agammaglobulinemia

Author

Vihinen, M., primary, Belohradsky, B. H., additional, Haire, R. N., additional, Holinski-Feder, E., additional, Kwan, S.- P., additional, Lappalainen, I., additional, Lehvaslaiho, H., additional, Lester, T., additional, Meindl, A., additional, Ochs, H., additional, Ollila, J., additional, Vorechovsky, I., additional, Weiss, M., additional, and Smith, C. I. E., additional

Published
1997
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31. EDITOR'S QUIZ: CI SNAPSHOT: A rare cause of gastrointestinal bleeding in a patient with hyper-IgE syndrome.

Author

Götzberger, M., Schlesinger, A., Dauer, M., Heldwein, W., Jansson, A., Renner, E., and Belohradsky, B. H.

Subjects
MYCOBACTERIAL diseases, IMMUNOSUPPRESSION, ENDOSCOPY, MUCOUS membranes, COLONOSCOPY, IMMUNODEFICIENCY
Abstract

This article discusses about mycobacterial infections. Mycobacterium genavense is a newly recognised non-tuberculous mycobacteria (NTM) that is found mainly in patients with acquired immunodeficiency syndrome and regularly affects the digestive tract. Intestinal infections due to NTM are known to mimic Whipple's disease endoscopically and histologically. Ulcerative lesions affecting the large bowel and causing gastrointestinal bleeding represent a rare endoscopic finding. Mycobacterial infections are uncommon complications in patients with hyper-IgE syndrome and treatment experiences are limited for this NTM species. Treatment was begun with a multidrug regimen of rifabutin, ethambutol, clarithromycin, and ciproflocazin. Three month follow up revealed regression of duodenal defects and normal mucosa on colonoscopy, indicating, to date, an adequate response to therapy.

Published
2004
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33. Initial presenting manifestations in 16,486 patients with inborn errors of immunity include infections and noninfectious manifestations

Author

Tim Niehues, Catherine Waruiru, Conleth Feighery, Uwe Schauer, Virginie Courteille, Kai Lehmberg, Ingo Müller, I. Esteves, Henner Morbach, Michael Borte, Patrick Hundsdoerfer, Klaus Schwarz, Ewelina Gowin, Alessandro Aiuti, Andreas Holbro, Federica Barzaghi, João Farela Neves, Dagmar Graf, Hannah Tamary, Veneta Milenova, Benedikt Boetticher, Eleonora Gambineri, Vera Goda, Alia Eldash, Jan-Christian Wasmuth, Fabio Candotti, Svetlana O. Sharapova, Markus Metzler, Juergen Brunner, Anna Hilfanova, Brindusa Ruxandra Capilna, Pere Soler-Palacín, Arnau Antolí, Horst von Bernuth, Vassilios Lougaris, Maria Carrabba, Bernd H. Belohradsky, Julian Thalhammer, Nathalie de Vergnes, Peter Olbrich, Peter Kopač, Leif G. Hanitsch, Alexandra Nieters, Filomeen Haerynck, Juliana Gabzdilova, Sezin Aydemir, Rabab El Hawary, Patrick F.K. Yong, Maria Giovanna Danieli, Alberto Tommasini, Sandra Steinmann, Ulrich Baumann, Figen Dogu, Elisabeth Förster-Waldl, Carolina Marasco, Donato Amodio, Lorenzo Lodi, Xavier Solanich, Caterina Cancrini, Brigita Sitkauskiene, Torsten Witte, Clementina Vanessa, Nima Rezaei, Jean-Christophe Goffard, Kirsten Wittke, Emmanouil Liatsis, Helen Baxendale, Susana L. Silva, Bodo Grimbacher, Henrike Ritterbusch, Evangelia Farmaki, Safa Meshaal, Sujal Ghosh, Larysa Kostyuchenko, David Edgar, Simone Cesaro, R Zeuner, Nerea Salmón Rodríguez, Isabella Quinti, Stephan Ehl, Pauline Brosselin, Joerg C. Henes, Pilar Llobet Agulló, Rosa Maria Dellepiane, Andrea Meinhardt, Marina Kojić, Georgios Sogkas, Stephan Borte, Catharina Schuetz, Suheyla Ocak, Karin Marschall, Lukas M. Gasteiger, Stefan Raffac, Sofia Tantou, Sadia Noorani, Matthaios Speletas, Philippe Randrianomenjanahary, Ursula Holzer, Ayca Kiykim, Johannes G. Liese, Angelo Vacca, Gisela Fecker, Ekrem Unal, Koen J. van Aerde, Alba Parra-Martínez, Kaan Boztug, Sophie Stiehler, Sybille Landwehr-Kenzel, Claudio Pignata, Jennifer Neubert, Janine Reichenbach, Shahnaz Parvin, Sarah Goddard, Andrea Schroll, Dirk Holzinger, Asghar Aghamohammadi, Hassan Abolhassani, Johannes Trück, Estela Paz-Artal, Shereen M. Reda, Anna Shcherbina, Maria Raptaki, Jaroslava Orosova, Beata Wolska-Kuśnierz, Tessa Kerre, Gerrit Ahrenstorf, Ben Zion Garty, Dirk Foell, Benjamin Becker, Ulrike F. Demel, Androniki Kapousouzi, Abraham Rutgers, Klaus Warnatz, Gemma Rocamora Blanch, Stephan Rusch, Luis M. Allende, Dalia Abd Elaziz, Safa Baris, Jorisvan Montfrans, Dominik T. Schneider, Raphael Scheible, Juana Gil-Herrera, Gerhard Kindle, Annarosa Soresina, Giovanna Fabio, Uwe Wintergerst, Emilia Faria, Maria Fasshauer, Silvia Ricci, Aisha Elmarsafy, Barbara Pietrucha, Carsten Speckmann, Nizar Mahlaoui, Ulrich Heininger, Isabelle Meyts, Matthew Buckland, Efimia Papadopoulou-Alataki, Robin Kobbe, A Herwadkar, Sebastian F. N. Bode, Ali Sobh, László Maródi, Baldassarre Martire, Chiara Azzari, Maximilian Heeg, Katja Masjosthusmann, Michael H. Albert, Matteo Chinello, Juan Luis Santos-Pérez, Aarnoud Huissoon, Tanya I. Coulter, Hendrik Schulze-Koops, Norbert Graf, Radwa Alkady, Jolanta Bernatoniene, Seraina Prader, Alenka Gagro, Joachim Roesler, Taco W. Kuijpers, Ewa Więsik-Szewczyk, Maria Elena Maccari, Conrad Ferdinand Lippert, Miriam González-Amores, Johannes Dirks, Daniel E Pleguezuelo, Christof M. Kramm, Anders Fasth, Volker Schuster, Olov Ekwall, Nikolaus Rieber, Javier Carbone, Petra Kaiser-Labusch, Diana Ernst, Lucia Augusta Baselli, Luis Ignacio Gonzalez-Granado, Maria Kanariou, Stefanie S. V. Henriet, Sigune Goldacker, Kerstin Felgentreff, Oana Joean, Fine Roosens, Fabian Hauck, Eva C. Schwaneck, Milos Jesenak, Manfred Hoenig, Lenka Kapustova, Christoph Boesecke, Alain Fischer, Sara Pereira da Silva, Julia Körholz, Ansgar Schulz, Carolynne Schwarze-Zander, Mikko Seppänen, Nermeen Galal, Nora Naumann-Bartsch, Tomaz Garcez, Peter Ciznar, Klara M. Posfay-Barbe, Zelimir Pavle Eric, Reinhold E. Schmidt, Hermann J. Girschick, Sabine Heine, Anika-Kerstin Biegner, Annick A. J. M. van de Ven, Stefan Schreiber, J. Merlijn van den Berg, Nurit Assia Batzir, Alexandra Jablonka, Kim Stol, Gregor Dückers, Antonios G.A. Kolios, Ioannis Kakkas, Christian Klemann, Marina N. Guseva, Sofia Grigoriadou, Elif Karakoc-Aydiner, Antonio Marzollo, Peter D. Arkwright, Urs C. Steiner, Sara Sebnem Kilic, Romina Dieli-Crimi, Gergely Kriván, Monika Sparber-Sauer, Marco Cazzaniga, Fulvio Porta, Paraskevi Maggina, Tomas Milota, Robbert G. M. Bredius, Martine Pergent, Klaus Tenbrock, Jana Pachlopnik Schmid, Florentia Dimitriou, Cathal Laurence Steele, Helen Bourne, Anna Bobcakova, Gerd Horneff, Judith Potjewijd, Marc Schmalzing, Tobias Ankermann, Paul Ryan, Oksana Boyarchuk, Necil Kutukculer, Carl Friedrich Classen, Zita Chovancová, Moira Thomas, Cinzia Milito, Michaela Bitzenhofer-Grüber, Faranaz Atschekzei, Eva Hlaváčková, Viviana Moschese, Julie Smet, Hans-Hartmut Peter, Carla Teixeira, Sabine M El-Helou, Suzanne de Kruijf Bazen, Helmut Wittkowski, Donate Jakoby, Marina Garcia-Prat, Esther de Vries, Richard Herriot, Sven Kracker, Alessandro Plebani, Lisa Göschl, Laura Hora Marques, Anna Sediva, Jiri Litzman, Mark M. Gompels, Renate Krüger, Şefika İlknur Kökçü Karadağ, Nadine Binder, Anna Szaflarska, Peter Jandus, Lisa Ibberson, Johann Greil, Ulf Schulze-Sturm, Mehtap Sirin, Aydan Ikinciogullari, Edyta Heropolitańska-Pliszka, Michael E. Weiss, Alla Skapenko, Lukas Wisgrill, Hana Alachkar, Uta Behrends, Silvia Sánchez-Ramón, Maria N. Hatzistilianou, Otilia Petrovicova, Darko Richter, Zoreh Nademi, Jürgen K. Rockstroh, Sohilla Lotfy, Markus G. Seidel, Timothy Ronan Leahy, Audra Blažienė, Translational Immunology Groningen (TRIGR), Paediatric Infectious Diseases / Rheumatology / Immunology, AII - Inflammatory diseases, ARD - Amsterdam Reproduction and Development, University of Zurich, Ehl, Stephan, Thalhammer, J., Kindle, G., Nieters, A., Rusch, S., Seppanen, M. R. J., Fischer, A., Grimbacher, B., Edgar, D., Buckland, M., Mahlaoui, N., Ehl, S., Boztug, K., Brunner, J., Demel, U. F., Forster-Waldl, E., Gasteiger, L. M., Goschl, L., Kojic, M., Schroll, A., Seidel, M. G., Wintergerst, U., Wisgrill, L., Sharapova, S. O., Goffard, J. -C., Kerre, T., Meyts, I., Roosens, F., Smet, J., Haerynck, F., Eric, Z. P., Milenova, V., Gagro, A., Richter, D., Chovancova, Z., Hlavackova, E., Litzman, J., Milota, T., Sediva, A., Elaziz, D. A., Alkady, R. S., El Sayed El Hawary, R., Eldash, A. S., Galal, N., Lotfy, S., Meshaal, S. S., Reda, S. M., Sobh, A., Elmarsafy, A., Brosselin, P., Courteille, V., De Vergnes, N., Kracker, S., Pergent, M., Randrianomenjanahary, P., Ahrenstorf, G., Albert, M. H., Ankermann, T., Atschekzei, F., Baumann, U., Becker, B. C., Behrends, U., Belohradsky, B. H., Biegner, A. -K., Binder, N., Bode, S. F. N., Boesecke, C., Boetticher, B., Borte, M., Borte, S., Classen, C. F., Dirks, J., Duckers, G., El-Helou, S., Ernst, D., Fasshauer, M., Fecker, G., Felgentreff, K., Foell, D., Ghosh, S., Girschick, H. J., Goldacker, S., Graf, N., Graf, D., Greil, J., Hanitsch, L. G., Hauck, F., Heeg, M., Heine, S. I., Henes, J. C., Hoenig, M., Holzer, U., Holzinger, D., Horneff, G., Hundsdoerfer, P., Jablonka, A., Jakoby, D., Joean, O., Kaiser-Labusch, P., Klemann, C., Kobbe, R., Korholz, J., Kramm, C. M., Kruger, R., Landwehr-Kenzel, S., Lehmberg, K., Liese, J. G., Lippert, C. F., Maccari, M. E., Masjosthusmann, K., Meinhardt, A., Metzler, M., Morbach, H., Muller, I., Naumann-Bartsch, N., Neubert, J., Niehues, T., Peter, H. -H., Rieber, N., Ritterbusch, H., Rockstroh, J. K., Roesler, J., Schauer, U., Scheible, R., Schmalzing, M., Schmidt, R. E., Schneider, D. T., Schreiber, S., Schuetz, C., Schulz, A., Schulze-Koops, H., Schulze-Sturm, U., Schuster, V., Schwaneck, E. C., Schwarz, K., Schwarze-Zander, C., Sirin, M., Skapenko, A., Sogkas, G., Sparber-Sauer, M., Speckmann, C., Steinmann, S., Stiehler, S., Tenbrock, K., von Bernuth, H., Warnatz, K., Wasmuth, J. -C., Weiss, M., Witte, T., Wittke, K., Wittkowski, H., Zeuner, R. A., Farmaki, E., Hatzistilianou, M. N., Kakkas, I., Kanariou, M. G., Kapousouzi, A., Liatsis, E., Maggina, P., Papadopoulou-Alataki, E., Raptaki, M., Speletas, M., Tantou, S., Goda, V., Krivan, G., Marodi, L., Abolhassani, H., Aghamohammadi, A., Rezaei, N., Feighery, C., Leahy, T. R., Ryan, P., Batzir, N. A., Garty, B. Z., Tamary, H., Aiuti, A., Amodio, D., Azzari, C., Barzaghi, F., Baselli, L. A., Cancrini, C., Carrabba, M., Cazzaniga, M., Cesaro, S., Chinello, M., Danieli, M. G., Dellepiane, R. M., Fabio, G., Gambineri, E., Lodi, L., Lougaris, V., Marasco, C., Martire, B., Marzollo, A., Milito, C., Moschese, V., Pignata, C., Plebani, A., Porta, F., Quinti, I., Ricci, S., Soresina, A., Tommasini, A., Vacca, A., Vanessa, C., Blaziene, A., Sitkauskiene, B., Gowin, E., Heropolitanska-Pliszka, E., Pietrucha, B., Szaflarska, A., Wiesik-Szewczyk, E., Wolska-Kusnierz, B., Esteves, I., Faria, E., Marques, L. H., Neves, J. F., Silva, S. L., Teixeira, C., Pereira da Silva, S., Capilna, B. R., Guseva, M. N., Shcherbina, A., Bobcakova, A., Ciznar, P., Gabzdilova, J., Jesenak, M., Kapustova, L., Orosova, J., Petrovicova, O., Raffac, S., Kopac, P., Allende, L. M., Antoli, A., Blanch, G. R., Carbone, J., Dieli-Crimi, R., Garcia-Prat, M., Gil-Herrera, J., Gonzalez-Granado, L. I., Agullo, P. L., Olbrich, P., Parra-Martinez, A., Paz-Artal, E., Pleguezuelo, D. E., Rodriguez, N. S., Sanchez-Ramon, S., Santos-Perez, J. L., Solanich, X., Soler-Palacin, P., Gonzalez-Amores, M., Ekwall, O., Fasth, A., Bitzenhofer-Gruber, M., Candotti, F., Dimitriou, F., Heininger, U., Holbro, A., Jandus, P., Kolios, A. G. A., Marschall, K., Schmid, J. P., Posfay-Barbe, K. M., Prader, S., Reichenbach, J., Steiner, U. C., Truck, J., Bredius, R. G., de Kruijf- Bazen, S., de Vries, E., Henriet, S. S. V., Kuijpers, T. W., Potjewijd, J., Rutgers, A., Stol, K., van Aerde, K. J., Van den Berg, J. M., van de Ven, A. A. J. M., Montfrans, J., Aydemir, S., Baris, S., Dogu, F., Ikinciogullari, A., Karakoc-Aydiner, E., Kilic, S. S., Kiykim, A., Kokcu Karadag, S. I., Kutukculer, N., Ocak, S., Unal, E., Boyarchuk, O., Hilfanova, A., Kostyuchenko, L. V., Alachkar, H., Arkwright, P. D., Baxendale, H. E., Bernatoniene, J., Coulter, T. I., Garcez, T., Goddard, S., Gompels, M. M., Grigoriadou, S., Herriot, R., Herwadkar, A., Huissoon, A., Ibberson, L., Nademi, Z., Noorani, S., Parvin, S., Steele, C. L., Thomas, M., Waruiru, C., Yong, P. F. K., and Bourne, H.

Subjects
0301 basic medicine, Male, Pediatrics, syndromic, Sex Factor, Disease, registry, medicine.disease_cause, Cohort Studies, 0302 clinical medicine, Primary Immunodeficiency Disease, inborn error of immunity, Immunology and Allergy, warning signs, Age Factor, Registries, Family history, presenting symptom, Child, Primary immunodeficiency, Granuloma, autoimmune, immune dysregulation, inflammatory, Adult, Autoimmune Diseases, Female, Humans, Infections, Lymphoproliferative Disorders, Middle Aged, Primary Immunodeficiency Diseases, Sex Factors, Age Factors, 10177 Dermatology Clinic, Infections/epidemiology, 3. Good health, Settore MED/02, Warning signs, Lymphoproliferative Disorder, 2723 Immunology and Allergy, Infection, Human, medicine.medical_specialty, Immunology, 610 Medicine & health, Malignancy, primary immunodeficiency, Autoimmune Disease, 03 medical and health sciences, Immunity, Autoimmune Diseases/epidemiology, medicine, 2403 Immunology, business.industry, warning sign, Common variable immunodeficiency, Granuloma/epidemiology, Immune dysregulation, medicine.disease, Primary Immunodeficiency Diseases/epidemiology, 030104 developmental biology, Lymphoproliferative Disorders/epidemiology, Cohort Studie, business, 030215 immunology
Abstract

BACKGROUND: Inborn errors of immunity (IEI) are rare diseases, which makes diagnosis a challenge. A better description of the initial presenting manifestations should improve awareness and avoid diagnostic delay. Although increased infection susceptibility is a well-known initial IEI manifestation, less is known about the frequency of other presenting manifestations.OBJECTIVE: We sought to analyze age-related initial presenting manifestations of IEI including different IEI disease cohorts.METHODS: We analyzed data on 16,486 patients of the European Society for Immunodeficiencies Registry. Patients with autoinflammatory diseases were excluded because of the limited number registered.RESULTS: Overall, 68% of patients initially presented with infections only, 9% with immune dysregulation only, and 9% with a combination of both. Syndromic features were the presenting feature in 12%, 4% had laboratory abnormalities only, 1.5% were diagnosed because of family history only, and 0.8% presented with malignancy. Two-third of patients with IEI presented before the age of 6 years, but a quarter of patients developed initial symptoms only as adults. Immune dysregulation was most frequently recognized as an initial IEI manifestation between age 6 and 25 years, with male predominance until age 10 years, shifting to female predominance after age 40 years. Infections were most prevalent as a first manifestation in patients presenting after age 30 years.CONCLUSIONS: An exclusive focus on infection-centered warning signs would have missed around 25% of patients with IEI who initially present with other manifestations.

Published
2021

34. Clinical and molecular analysis of patients with defects in μ heavy chain gene

Author

Eduardo Lopez Granados, Andrea S. Porpiglia, Mary Beth Hogan, Nuria Matamoros, Silvia Krasovec, Claudio Pignata, C.I.E. Smith, Lennart Hammarstrom, Janne Bjorkander, Bernd H. Belohradsky, G. Fontan Casariego, M.C. Garcia Rodriguez, Mary Ellen Conley, LOPEZ GRANADOS, E., Porpiglia, A. S., Hogan, M. B., Matamoros, N., Krasovec, S., Pignata, Claudio, Smith, C. I., Hammarstrom, L., Bjorkander, J., Belohradsky, B. H., and Casariego, G. F. GARCIA RODRIGUEZ M. C. CONLEY M. E.

Subjects
Adult, Male, Polymorphism, Genetic, X Chromosome, Adolescent, Genetic Linkage, Immunoglobulin mu-Chains, Infant, General Medicine, Middle Aged, Article, Agammaglobulinemia, Mutation, Humans, Female, Child, Polymorphism, Single-Stranded Conformational
Abstract

Autosomal recessive disorders of B cell development are rare and heterogeneous. To determine the proportion of affected patients who have defects in the micro heavy chain (IGHM) gene, we used single-stranded conformational polymorphism analysis to screen genomic DNA from 40 unrelated patients with early onset infections, profound hypogammaglobulinemia, and absent B cells. All of the patients were genotypically normal in BTK, the gene that underlies X-linked agammaglobulinemia. Eight different mutations in the micro heavy chain were identified in 19 members of 12 unrelated families. Four of the mutations were large deletions that removed more than 40 kb of DNA in the IGHM locus. In six of the 12 families, the affected patients had an identical single base pair substitution, a G-->A, at the -1 position of the alternative splice site. Immunoglobulin haplotype analysis showed that this mutation occurred on at least three different haplotypes, indicating that this is a hot spot for mutations. Compared with patients with mutations in Btk, patients with defects in the micro heavy chain had an earlier onset of disease and more complications. Our study indicates that at least 20-30% of patients with autosomal recessive defects in B cell development have mutations in the micro heavy chain.

Published
2002

35. Treatment of relapsing Mycobacterium avium infection with interferon-gamma and interleukin-2 in an HIV-negative patient with low CD4 syndrome.

Author

Sternfeld T, Nigg A, Belohradsky BH, and Bogner JR

Subjects
Adjuvants, Immunologic therapeutic use, CD4 Lymphocyte Count, HIV Seronegativity, Humans, Lymphopenia immunology, Male, Middle Aged, Mycobacterium avium-intracellulare Infection etiology, Recombinant Proteins, Recurrence, Syndrome, Interferon-gamma therapeutic use, Interleukin-2 therapeutic use, Lymphopenia complications, Mycobacterium avium-intracellulare Infection drug therapy
Abstract

A patient with idiopathic CD4 T-lymphopenia was diagnosed with a recurrent disseminated Mycobacterium avium infection. Because of progressive disease, treatment with interferon-gamma (IFN-γ) and interleukin-2 (IL-2) was started. The patient was successfully treated with IFN-γ-1b and IL-2 in addition to anti-mycobacterial combination therapy. To our knowledge, this is the first report of successful combination therapy with IFN-γ-1b and IL-2 in a patient with idiopathic CD4 T-lymphopenia. Short-term IFN-γ-1b and IL-2 might be considered as therapeutic options in refractory mycobacterial infections in patients with idiopathic CD4 lymphopenia., (Copyright © 2009 International Society for Infectious Diseases. Published by Elsevier Ltd. All rights reserved.)

Published
2010
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36. Home-based subcutaneous immunoglobulin G replacement therapy under real-life conditions in children and adults with antibody deficiency.

Author

Hoffmann F, Grimbacher B, Thiel J, Peter HH, and Belohradsky BH

Subjects
Adolescent, Adult, Aged, Child, Child, Preschool, Female, Health Status, Humans, Immunoglobulins blood, Immunologic Deficiency Syndromes immunology, Immunologic Deficiency Syndromes physiopathology, Immunotherapy methods, Infant, Injections, Subcutaneous, Male, Middle Aged, Product Surveillance, Postmarketing, Prospective Studies, Quality of Life, Severity of Illness Index, Young Adult, Immunoglobulins administration & dosage, Immunologic Deficiency Syndromes therapy
Abstract

Background: Subcutaneous immunoglobulin (SCIG) therapy is an alternative to intravenous immunoglobulin (IVIG) therapy., Methods: We evaluated the efficacy and safety of the SCIG Vivaglobin(formerly known as Beriglobin SC) under real-life conditions in a post-marketing observational study in 82 patients with primary or secondary antibody deficiencies. Health-related quality of life (HRQoL) was evaluated in a subset of 30 patients previously treated with IVIG (including 11 children <14 years) using the Short Form 36 (SF-36) for patients > or = 14 years of age (adults) and the Child Health Questionnaire - Parental Form 50 (CHQ-PF50) for children <14 years of age. Treatment preferences were assessed in adults., Results: The mean serum immunoglobulin G (IgG) trough level during SCIG treatment (7.5 g/L) was higher than during previous IVIG treatment (6.6 g/L; p<0.01). The investigators assessed the efficacy of SCIG therapy as "excellent" in 89% of patients. No systemic adverse drug reactions were observed. Improvements by > or = 5 points were observed in 5 of 8 SF-36 subscales and in 6 of 12 CHQ-PF50 subscales. Statistically significant improvements (p< or =0.05) were observed for the SF-36 subscales of bodily pain, general health perceptions, and vitality (adults), and for the CHQ-PF50 subscales of general health perceptions, parental impact - time, parental impact - emotional, and family activities (children). Patients preferred SCIG over IVIG therapy (92%) and home therapy over therapy at the clinic/physician (83%)., Conclusion: This study confirms that therapy with Vivaglobin at home is effective, safe, well tolerated, and improves quality of life in patients with antibody deficiency.

Published
2010
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37. Therapy of focal viral encephalitis in children with aciclovir and recombinant beta-interferon - results of a placebo-controlled multicenter study.

Author

Wintergerst U, Kugler K, Harms F, Belohradsky BH, and Pfluger T

Subjects
Adolescent, Child, Child, Preschool, Double-Blind Method, Drug Therapy, Combination, Encephalitis, Viral pathology, Encephalitis, Viral physiopathology, Female, Focal Infection pathology, Herpes Simplex pathology, Humans, Infant, Male, Nervous System pathology, Nervous System physiopathology, Recombinant Proteins therapeutic use, Recovery of Function drug effects, Treatment Outcome, Acyclovir therapeutic use, Antiviral Agents therapeutic use, Encephalitis, Viral drug therapy, Focal Infection drug therapy, Herpes Simplex drug therapy, Interferon-beta therapeutic use
Abstract

Focal viral encephalitis in childhood is a rare but life-threatening disease. Animal experiments and case reports suggest a positive effect of an additional therapy with interferon-beta on the course of the disease. Therefore, we initiated a prospective, double-blind placebo-controlled study to investigate the benefit of a combination therapy of Aciclovir (ACV) and recombinant interferon-beta (rIFN-beta) in juvenile focal viral encephalitis. - Initial inclusion criterium was suspicion of focal viral encephalitis. Diagnosis was proven by demonstration of characteristic focal lesions in cerebral imaging or virological evidence of HSV in cerebrospinal fluid. Patients were treated with ACV plus rIFN-beta or ACV plus placebo. Neurological outcome was determined 21 days and 3 months after onset of the disease. - Initially 59 patients were enrolled in the study. Encephalitis was proven in 14 patients (7 ACV + rIFN-beta, 7 ACV + placebo). The study groups were balanced in terms of important prognostic criteria. 10 patients (5 ACV + rIFN-beta, 5 ACV + placebo) were cured or had slight defects, 4 patients (2 ACV + rIFN-beta, 2 ACV + placebo) showed moderate to severe defects. There was no significant difference in favour of the additive therapy with rIFN-beta.

Published
2005

38. Effect of antiretroviral triple combinations including the protease inhibitor nelfinavir in heavily pretreated children with HIV-1 infection.

Author

Hoffmann F, Funk M, Linde R, Notheis G, Petropoulou T, Eberle J, Gürtler L, Belohradsky BH, and Wintergerst U

Subjects
Adolescent, Anti-HIV Agents adverse effects, CD4 Lymphocyte Count, Child, Child, Preschool, Disease Progression, Drug Resistance, Viral, Drug Therapy, Combination, Female, HIV Infections genetics, HIV Infections immunology, HIV Infections virology, HIV Protease Inhibitors adverse effects, HIV-1 genetics, HIV-1 isolation & purification, Humans, Infant, Male, Nelfinavir adverse effects, RNA, Viral blood, Retrospective Studies, Time Factors, Treatment Refusal, Viral Load, Viremia drug therapy, Viremia immunology, Viremia virology, Anti-HIV Agents administration & dosage, Anti-HIV Agents therapeutic use, HIV Infections drug therapy, HIV Protease Inhibitors administration & dosage, HIV Protease Inhibitors therapeutic use, Nelfinavir administration & dosage, Nelfinavir therapeutic use
Abstract

Background: In this retrospective study the effect of antiretroviral triple therapy including the protease-inhibitor nelfinavir (NFV) on CD4-cells and viral load (VL) in heavily pretreated HIV-infected children was evaluated., Patients and Methods: 20 children (<18 years) were included. Median duration of antiretroviral pretreatment was 27 months (range, 7 65), median initial VL was 4.7 log subset 10 (3.2 6.1) and median relative CD4-cells was 17.5% (3 33). Patients were put on combinations with NFV because of treatment failure (increasing VL), intolerance to prior therapy with PIs or adherence problems with prior indinavir. Viral load (RT-PCR, detection limit 50 copies/ml) and CD4-cells were measured every 4-8 weeks., Results: Median viral load decreased 1.2 log(10) (-1.3 2.5), 0.9 log(10) (-0.8 - 2.5) and 0.4 log(10) (-0.5 - 3.0) after 12, 24 and 36 weeks. The VL of 2 patients was below the detection limit (50 copies/ml) after 24 weeks. The relative CD4-cell count increased from a median of 17.5% to 22%, 23% and 25% after 12, 24 and 36 weeks, respectively. Side effects of NFV were usually mild. WHO grade 1 or 2 diarrhea occurred in 70% and moderate elevations of triglycerides in 40% of the patients. At 48 weeks 18/20 patients had to be switched to other combinations due to virological failure., Conclusions: In children with intensive prior antiretroviral therapy combination therapy including NFV lead to a modest short-term reduction of the VL and increase in CD4-cells. However, the long-term antiretroviral effect was poor.

Published
2002

39. Effect of antiretroviral combination therapies including efavirenz in heavily pretreated HIV-infected children.

Author

Engelhorn C, Hoffmann F, Notheis G, Funk M, Eberle J, Belohradsky BH, and Wintergerst U

Subjects
Adolescent, Alkynes, Antiretroviral Therapy, Highly Active, Benzoxazines, CD4 Lymphocyte Count, Child, Child, Preschool, Cyclopropanes, Female, HIV Infections immunology, HIV Infections virology, HIV Protease Inhibitors administration & dosage, Humans, Male, Nelfinavir administration & dosage, RNA, Viral blood, Viremia drug therapy, Viremia immunology, Viremia virology, Anti-HIV Agents administration & dosage, HIV Infections drug therapy, Oxazines administration & dosage, Reverse Transcriptase Inhibitors administration & dosage
Abstract

Background: In this retrospective study the effect of antiretroviral combination regimens including the non nucleoside reverse transcriptase inhibitor (NNRTI) efavirenz (EFV) on viral load (VL) and CD4-cell count in heavily pretreated HIV-infected children was investigated., Design: The data of 15 children (< 16 years) were evaluated during a treatment period of at least 52 weeks. Patients received a median of 4 prior antiretroviral regimens and were changed to combinations with EFV because of renewed increasing VL., Methods: Viral load (Amplicor, detection limit 50 copies/ml) and CD4-cells were measured every 4-8 weeks., Results: The median reduction of the viral load for the total study population was 1.9 log10 (0.8 - 4.7), 2.3 log(10) (0.5 - 4.7) and 2.6 log(10) (0-4.7) after 12, 24 and 52 weeks, respectively. After 24 weeks 7/15 children and after 52 weeks 9/15 patients had reductions of the VL below the detection limit. The median increase of CD4-cells in the study population during the treatment period were 104 cells/microl (189-969), 220 cells/microl (170-831) and 321 cells/ml (162-574) after 12, 24 and 52 weeks, respectively., Conclusions: In children with intensive prior antiretroviral therapy and multiple therapeutic failures with PI-containing regimens, combination therapy including EFV resulted in an excellent antiretroviral efficacy. After 52 weeks 9/15 patients had persistent reductions of the VL below 50 copies/ml, although none of these children reached this level of viral suppression during their multiple prior protease inhibitor-containing regimens.

Published
2002

40. Discontinuation of primary Pneumocystis carinii prophylaxis after reconstitution of CD4 cell counts in HIV-infected children.

Author

Urschel S, Schuster T, Dunsch D, Wintergerst U, Hofstetter R, and Belohradsky BH

Subjects
Anti-HIV Agents therapeutic use, CD4 Lymphocyte Count, Child, Child, Preschool, Female, HIV Infections drug therapy, Humans, Male, AIDS-Related Opportunistic Infections prevention & control, Antifungal Agents administration & dosage, HIV Infections immunology, Pneumonia, Pneumocystis prevention & control
Published
2001
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41. Bromelain is an accelerator of phagocytosis, respiratory burst and Killing of Candida albicans by human granulocytes and monocytes.

Author

Brakebusch M, Wintergerst U, Petropoulou T, Notheis G, Husfeld L, Belohradsky BH, and Adam D

Subjects
Adolescent, Adult, Agammaglobulinemia immunology, Bromelains immunology, Child, Child, Preschool, Common Variable Immunodeficiency immunology, Granulocytes metabolism, Humans, Monocytes metabolism, Phagocytosis physiology, Respiratory Burst physiology, Trypsin pharmacology, Adjuvants, Immunologic pharmacology, Bromelains pharmacology, Candida albicans immunology, Granulocytes immunology, Monocytes immunology, Phagocytosis drug effects, Respiratory Burst drug effects
Abstract

Objective: The aim of this study was to examine the influence of immuno modulating agents like bromelain and trypsin (e.g. Wobenzym on granulocyte and monocyte functions in healthy volunteers and patients with disorders of the humoral immuno system X-linked agammaglobulinaemia (XLA) and common variable immuno deficiency (CVID) and to find out whether the unspecific immunity could be improved by these enzymes., Methods: In a whole-blood assay kinetics of phagocytosis, respiratory burst and killing (PBK) were measured in blood samples incubated with and without bromelain and trypsin (B/T) using Candida albicans as target organism. The time-reaction curves were analysed determining their gradient (T1) and their onset (T2) as well as the half effect time (HET)., Results: Phagocytes from patients with XLA showed a significantly accelerated basal phagocytosis (reduction of HET by 24% p < 0.001) compared to healthy controls. After incubation with B/T (10 microg/ml each) speed of phagocytosis was nearly doubled (phagocyte activity p < 0.0001, Candida uptake p < 0.003), T2 of respiratory burst was reduced by 65 % (p < 0.0001) and killing was accelerated by 27% (p < 0.046). However, the maximal activities of all kinetics were not altered. Incubation of phagocytes from healthy controls with B/T accelerated phagocytosis to a level comparable to that of untreated phagocytes from patients with XLA and also accelerated reactive oxygen species (ROS) production (reduction of HET by 28%, p < 0.012). In contrast to phagocytes from patients with XLA, phagocytes of patients with CVID showed a similar stimulation by B/T like healthy controls. Further experiments with the single substances showed that bromelain was the active compound., Conclusion: Our data suggest, that bromelain possesses immuno stimulatory properties. Phagocytes of XLA patients appear to be particularly susceptible to this stimulation.

Published
2001

42. CD95 (APO-1/Fas) expression on naive CD4(+) T cells increases with disease progression in HIV-infected children and adolescents: effect of highly active antiretroviral therapy (HAART).

Author

Böhler T, Wintergerst U, Linde R, Belohradsky BH, and Debatin KM

Subjects
Adolescent, Child, Child, Preschool, Disease Progression, HIV Infections drug therapy, HIV-1 isolation & purification, Humans, Infant, Infant, Newborn, Interferon-gamma blood, Viral Load, Antiretroviral Therapy, Highly Active, CD4-Positive T-Lymphocytes immunology, HIV Infections immunology, fas Receptor immunology
Abstract

We studied the expression of the CD95 receptor (APO-1/Fas) on peripheral blood T cell subpopulations in 37 HIV-1-infected children and adolescents stratified according to disease stage or antiretroviral treatment regimen and compared the results to values obtained in 12 healthy age-matched control subjects. CD95 expression on CD45RA(+) CD45RO(-)/CD62L(+) (resting/naive) and CD45RO(+) CD45RA(-) (primed/memory) CD4(+) and CD8(+) T cells was assessed quantitatively by four-color and three-color flow cytometry. CD4(+) T cells contained a population of predominantly CD95(-) resting/naive cells and a population of CD95(high) primed/memory cells, whereas CD8(+) T cells had a more uniform pattern of CD95 expression. The percentage of CD95(+) CD4(+) T cells increased with disease progression because of both an augmented median fluorescence intensity on resting/naïve cells and an increased percentage of CD95(high) cells. Patients with highly active antiretroviral combination therapy who maintained stable CD4 counts in the presence of elevated plasma viral load had nearly normal numbers of CD95(-) resting/naive CD4(+) T cells, whereas CD95 expression in the CD8(+) T cell subset was still elevated compared with control subjects. Low CD95 expression on resting/naive CD4(+) T cells may therefore indicate a low risk for disease progression in antiretrovirally treated and untreated patients.

Published
2001
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43. Pharmacokinetic interaction of amprenavir in combination with efavirenz or delavirdine in HIV-infected children.

Author

Wintergerst U, Engelhorn C, Kurowski M, Hoffmann F, Notheis G, and Belohradsky BH

Subjects
Adolescent, Alkynes, Anti-HIV Agents administration & dosage, Benzoxazines, Carbamates, Child, Child, Preschool, Cyclopropanes, Delavirdine administration & dosage, Drug Interactions, Drug Therapy, Combination, Furans, Humans, Oxazines administration & dosage, Reverse Transcriptase Inhibitors administration & dosage, Sulfonamides administration & dosage, Time Factors, Anti-HIV Agents pharmacokinetics, Delavirdine pharmacokinetics, HIV Infections drug therapy, Oxazines pharmacokinetics, Reverse Transcriptase Inhibitors pharmacokinetics, Sulfonamides pharmacokinetics
Published
2000
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44. Mitochondrial and peroxisomal dysfunction following perinatal exposure to antiretroviral drugs.

Author

Stojanov S, Wintergerst U, Belohradsky BH, and Rolinski B

Subjects
Anti-HIV Agents therapeutic use, Female, HIV Infections drug therapy, HIV Protease Inhibitors therapeutic use, Humans, Infant, Lamivudine therapeutic use, Male, Mitochondria physiology, Peroxisomes physiology, Pregnancy, Pregnancy Complications, Infectious drug therapy, Prenatal Exposure Delayed Effects, Reverse Transcriptase Inhibitors therapeutic use, Ritonavir therapeutic use, Saquinavir therapeutic use, Zidovudine therapeutic use, Anti-HIV Agents adverse effects, HIV Infections prevention & control, Lamivudine adverse effects, Mitochondria drug effects, Perinatal Care, Peroxisomes drug effects, Reverse Transcriptase Inhibitors adverse effects, Zidovudine adverse effects
Published
2000
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45. Genetic linkage of hyper-IgE syndrome to chromosome 4.

Author

Grimbacher B, Schäffer AA, Holland SM, Davis J, Gallin JI, Malech HL, Atkinson TP, Belohradsky BH, Buckley RH, Cossu F, Español T, Garty BZ, Matamoros N, Myers LA, Nelson RP, Ochs HD, Renner ED, Wellinghausen N, and Puck JM

Subjects
Chromosome Deletion, Female, Genes, Recessive genetics, Genetic Markers, Genotype, Humans, Lod Score, Male, Pedigree, Penetrance, Polymorphism, Genetic, Quantitative Trait, Heritable, Chromosome Mapping, Chromosomes, Human, Pair 4 genetics, Job Syndrome genetics
Abstract

The hyper-IgE syndrome (HIES) is a rare primary immunodeficiency characterized by recurrent skin abscesses, pneumonia, and highly elevated levels of serum IgE. HIES is now recognized as a multisystem disorder, with nonimmunologic abnormalities of the dentition, bones, and connective tissue. HIES can be transmitted as an autosomal dominant trait with variable expressivity. Nineteen kindreds with multiple cases of HIES were scored for clinical and laboratory findings and were genotyped with polymorphic markers in a candidate region on human chromosome 4. Linkage analysis showed a maximum two-point LOD score of 3.61 at recombination fraction of 0 with marker D4S428. Multipoint analysis and simulation testing confirmed that the proximal 4q region contains a disease locus for HIES.

Published
1999
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46. Long-term antiretroviral combination therapy including lamivudine in HIV-1 infected women during pregnancy.

Author

Grubert TA, Wintergerst U, Lutz-Friedrich R, Belohradsky BH, and Rolinski B

Subjects
Adult, Drug Therapy, Combination, Female, HIV Infections virology, HIV Protease Inhibitors therapeutic use, Humans, Infant, Newborn, Infectious Disease Transmission, Vertical prevention & control, Lamivudine blood, Pregnancy, Pregnancy Complications, Infectious virology, Reverse Transcriptase Inhibitors blood, Anti-HIV Agents therapeutic use, HIV Infections drug therapy, HIV-1 physiology, Lamivudine therapeutic use, Pregnancy Complications, Infectious drug therapy, Reverse Transcriptase Inhibitors therapeutic use
Published
1999
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47. Fine localization of the Nijmegen breakage syndrome gene to 8q21: evidence for a common founder haplotype.

Author

Cerosaletti KM, Lange E, Stringham HM, Weemaes CM, Smeets D, Sölder B, Belohradsky BH, Taylor AM, Karnes P, Elliott A, Komatsu K, Gatti RA, Boehnke M, and Concannon P

Subjects
Chromosome Mapping, Female, Founder Effect, Genes, Recessive genetics, Genetic Linkage genetics, Genotype, Haplotypes, Humans, Linkage Disequilibrium genetics, Lod Score, Male, Microsatellite Repeats genetics, Pedigree, Recombination, Genetic genetics, Chromosome Breakage genetics, Chromosomes, Human, Pair 8 genetics
Abstract

Nijmegen breakage syndrome (NBS) is a rare autosomal recessive disorder characterized by microcephaly, a birdlike face, growth retardation, immunodeficiency, lack of secondary sex characteristics in females, and increased incidence of lymphoid cancers. NBS cells display a phenotype similar to that of cells from ataxia-telangiectasia patients, including chromosomal instability, radiation sensitivity, and aberrant cell-cycle-checkpoint control following exposure to ionizing radiation. A recent study reported genetic linkage of NBS to human chromosome 8q21, with strong linkage disequilibrium detected at marker D8S1811 in eastern European NBS families. We collected a geographically diverse group of NBS families and tested them for linkage, using an expanded panel of markers at 8q21. In this article, we report linkage of NBS to 8q21 in 6/7 of these families, with a maximum LOD score of 3.58. Significant linkage disequilibrium was detected for 8/13 markers tested in the 8q21 region, including D8S1811. In order to further localize the gene for NBS, we generated a radiation-hybrid map of markers at 8q21 and constructed haplotypes based on this map. Examination of disease haplotypes segregating in 11 NBS pedigrees revealed recombination events that place the NBS gene between D8S1757 and D8S270. A common founder haplotype was present on 15/18 disease chromosomes from 9/11 NBS families. Inferred (ancestral) recombination events involving this common haplotype suggest that NBS can be localized further, to an interval flanked by markers D8S273 and D8S88.

Published
1998
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48. Vaccine tolerance in steroid substituted patients with congenital adrenal hyperplasia.

Author

Weiss M, Dörr HG, Brandmaier R, Schwarz HP, and Belohradsky BH

Subjects
Adolescent, Adrenal Hyperplasia, Congenital drug therapy, Adult, Child, Child, Preschool, Female, Humans, Male, Retrospective Studies, Surveys and Questionnaires, Adrenal Cortex Hormones therapeutic use, Adrenal Hyperplasia, Congenital immunology, Immune Tolerance, Vaccination adverse effects, Vaccines
Abstract

The tolerance and side effects of vaccinations were determined in patients with congenital adrenal hyperplasia (CAH) who receive physiological corticosteroid substitution. In a retrospective approach, questionnaires about the frequencies of vaccinations and observed side effects were sent to CAH patients, and medical records were reviewed. We received 82 questionnaires from 63 patients with CAH and salt-losing and 19 patients without salt-losing. Patients age ranged from 2-40 years. No statistical differences were found for vaccination frequencies between patients with or without salt-losing. CAH patients had received complete vaccinations against diphtheria, tetanus and poliomyelitis in 79%, 85% and 78%, respectively, whereas pertussis vaccination was complete in only 23%. Live vaccination against measles, mumps and rubella was performed in 63%, 50% and 38%. Side effects of vaccination were indicated in 5 out of 82 questionnaires who all belonged to CAH patients with salt-losing. Transient side effects were an anaphylactic reaction, probably to tetanus immunoglobulin, in 1 case, and fever and convulsions after diphtheria, pertussis and tetanus (DPT) vaccine in 2 cases. In 2 further patients putative complications were noted. Encephalitis with permanent disabilities was observed after the third DPT vaccination, but a causative relation could not be established. In another boy, encephalopathy noticed after measles vaccination was induced by previous toxicosis. Although encephalopathy was described in 2 patients after vaccinations, no vaccination damage could be proven in our retrospective study. As expected, an increased vaccination risk in CAH patients was not demonstrated.

Published
1997

49. Improvement of superoxide production in monocytes from patients with chronic granulomatous disease by recombinant cytokines.

Author

Jendrossek V, Peters AM, Buth S, Liese J, Wintergerst U, Belohradsky BH, and Gahr M

Subjects
Cells, Cultured, Female, Granulocyte-Macrophage Colony-Stimulating Factor pharmacology, Humans, Interferon-gamma pharmacology, Interleukin-1 pharmacology, Interleukin-3 pharmacology, Male, N-Formylmethionine Leucyl-Phenylalanine pharmacology, Neutrophils metabolism, Recombinant Proteins pharmacology, Tetradecanoylphorbol Acetate pharmacology, Tumor Necrosis Factor-alpha pharmacology, Cytokines pharmacology, Granulomatous Disease, Chronic blood, Monocytes metabolism, Superoxides blood
Abstract

Cytokines have been shown to modulate the respiratory burst of polymorphonuclear leukocytes and monocytes from normal controls. We have examined whether monocytes from children with chronic granulomatous disease (CGD) can be primed by cytokines other than interferon-gamma (IFN gamma), which has been demonstrated to improve the production of reactive oxygen species in vivo and in vitro. Monocytes isolated from peripheral blood were cultured without and with IFN gamma (500 U/mL), tumor necrosis factor-alpha (500 U/mL), interleukin-1 beta (IL-1 beta) (100 U/mL), and IL-3 (100 U/mL). After 3 days of culture, the phorbolmyristate acetate (2 ng/mL) and the formyl-methionyl-leucyl-phenylalanine (0.1 mumol/L)-stimulated superoxide-production was determined in a microtiter system. In nearly all of the 14 patients examined (5 autosomal, 5 X-chromosomal, and 4 of unknown inheritance), an improvement of superoxide production could be demonstrated. The most impressive effect with the cytokines newly tested was seen with monocytes from autosomal CGD patients treated with IL-3 and stimulated by phorbolmyristate acetate. In single patients cultivation of monocytes with IL-6 and granulocyte-macrophage colony-stimulating factor resulted in only slight improvement of superoxide production. Our findings indicate that cytokines other than IFN gamma can positively modulate the defective respiratory burst in CGD and that each patient reacts with an individual pattern to different cytokines.

Published
1993

50. Chronic granulomatous disease with partial deficiency of cytochrome b558 and incomplete respiratory burst: variants of the X-linked, cytochrome b558-negative form of the disease.

Author

Roos D, de Boer M, Borregard N, Bjerrum OW, Valerius NH, Seger RA, Mühlebach T, Belohradsky BH, and Weening RS

Subjects
Blood Bactericidal Activity, Blotting, Western, Gene Expression, Genetic Complementation Test, Granulomatous Disease, Chronic genetics, Humans, Male, NADPH Oxidases, RNA, Messenger genetics, X Chromosome, Cytochrome b Group deficiency, Granulomatous Disease, Chronic physiopathology, NADH, NADPH Oxidoreductases deficiency, Respiratory Burst
Abstract

Five male patients from four different families presented with a clinical record of chronic granulomatous disease (CGD): recurrent infections of the skin and/or respiratory tract with catalase-positive microorganisms, sometimes in combination with granulomata and/or abscesses in various organs. These patients differed from "classical" forms of the disease in that their neutrophils, although deficient in killing in vitro of Staphylococcus aureus, contained a decreased but measurable amount of cytochrome b558 (10-60% of normal on a heme basis), causing weak staining in the nitroblue tetrazolium dye test and a depressed respiratory burst after contact of the cells with fluid or particulate activators of the NADPH:O2 oxidoreductase. In the cell-free activation system, the defect in the patients' cells was localized in the membrane fraction. In each of the four families, the cellular abnormalities showed an X-linked inheritance. Fusion experiments performed with the monocytes from these patients and those from patients with classical X-linked, cytochrome b558-negative (Xb(0)) or autosomal, cytochrome b558-positive (Ab+) CGD showed complementation of NADPH:O2 oxidoreductase activity in the latter but not in the former combination. Thus, the unusual CGD patients represent variant forms of Xb(0) CGD, with mutations in the gene coding for the beta subunit of cytochrome b558 that do not cause complete loss of this protein.

Published
1992
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