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1. First genome-wide association study of esophageal atresia identifies three genetic risk loci at CTNNA3, FOXF1/FOXC2/FOXL1, and HNF1B

Author

Gehlen, Jan, Giel, Ann-Sophie, Koellges, Ricarda, Haas, Stephan L., Zhang, Rong, Trcka, Jiri, Sungur, Ayse O., Renziehausen, Florian, Bornholdt, Dorothea, Jung, Daphne, Hoyer, Paul D., Nordenskjold, Agneta, Tibboel, Dick, Vlot, John, Spaander, Manon C. W., Smigiel, Robert, Patkowski, Dariusz, Roeleveld, Nel, van Rooij, Iris Alm, de Blaauw, Ivo, Hoelscher, Alice, Pauly, Marcus, Leutner, Andreas, Fuchs, Joerg, Niethammer, Joel, Melissari, Maria-Theodora, Jenetzky, Ekkehart, Zwink, Nadine, Thiele, Holger, Hilger, Alina Christine, Hess, Timo, Trautmann, Jessica, Marks, Matthias, Baumgarten, Martin, Blaess, Gaby, Landen, Mikael, Fundin, Bengt, Bulik, Cynthia M., Pennimpede, Tracie, Ludwig, Michael, Ludwig, Kerstin U., Mangold, Elisabeth, Heilmann-Heimbach, Stefanie, Moebus, Susanne, Herrmann, Bernhard G., Alsabeah, Kristina, Burgos, Carmen M., Engstrand Lilja, Helene, Azodi, Sahar, Stenstrom, Pernilla, Arnbjornsson, Einar, Frybova, Barbora, Lebensztejn, Dariusz M., Debek, Wojciech, Kolodziejczyk, Elwira, Kozera, Katarzyna, Kierkus, Jaroslaw, Kalicinski, Piotr, Stefanowicz, Marek, Socha-Banasiak, Anna, Kolejwa, Michal, Piaseczna-Piotrowska, Anna, Czkwianianc, Elzbieta, Noethen, Markus M., Grote, Phillip, Rygl, Michal, Reinshagen, Konrad, Spychalski, Nicole, Ludwikowski, Barbara, Hubertus, Jochen, Heydweiller, Andreas, Ure, Benno, Muensterer, Oliver J., Aubert, Ophelia, Gosemann, Jan-Hendrik, Lacher, Martin, Degenhardt, Petra, Boemers, Thomas M., Mokrowiecka, Anna, Malecka-Panas, Ewa, Woehr, Markus, Knapp, Michael, Seitz, Guido, de Klein, Annelies, Oracz, Grzegorz, Brosens, Erwin, Reutter, Heiko, Schumacher, Johannes, Gehlen, Jan, Giel, Ann-Sophie, Koellges, Ricarda, Haas, Stephan L., Zhang, Rong, Trcka, Jiri, Sungur, Ayse O., Renziehausen, Florian, Bornholdt, Dorothea, Jung, Daphne, Hoyer, Paul D., Nordenskjold, Agneta, Tibboel, Dick, Vlot, John, Spaander, Manon C. W., Smigiel, Robert, Patkowski, Dariusz, Roeleveld, Nel, van Rooij, Iris Alm, de Blaauw, Ivo, Hoelscher, Alice, Pauly, Marcus, Leutner, Andreas, Fuchs, Joerg, Niethammer, Joel, Melissari, Maria-Theodora, Jenetzky, Ekkehart, Zwink, Nadine, Thiele, Holger, Hilger, Alina Christine, Hess, Timo, Trautmann, Jessica, Marks, Matthias, Baumgarten, Martin, Blaess, Gaby, Landen, Mikael, Fundin, Bengt, Bulik, Cynthia M., Pennimpede, Tracie, Ludwig, Michael, Ludwig, Kerstin U., Mangold, Elisabeth, Heilmann-Heimbach, Stefanie, Moebus, Susanne, Herrmann, Bernhard G., Alsabeah, Kristina, Burgos, Carmen M., Engstrand Lilja, Helene, Azodi, Sahar, Stenstrom, Pernilla, Arnbjornsson, Einar, Frybova, Barbora, Lebensztejn, Dariusz M., Debek, Wojciech, Kolodziejczyk, Elwira, Kozera, Katarzyna, Kierkus, Jaroslaw, Kalicinski, Piotr, Stefanowicz, Marek, Socha-Banasiak, Anna, Kolejwa, Michal, Piaseczna-Piotrowska, Anna, Czkwianianc, Elzbieta, Noethen, Markus M., Grote, Phillip, Rygl, Michal, Reinshagen, Konrad, Spychalski, Nicole, Ludwikowski, Barbara, Hubertus, Jochen, Heydweiller, Andreas, Ure, Benno, Muensterer, Oliver J., Aubert, Ophelia, Gosemann, Jan-Hendrik, Lacher, Martin, Degenhardt, Petra, Boemers, Thomas M., Mokrowiecka, Anna, Malecka-Panas, Ewa, Woehr, Markus, Knapp, Michael, Seitz, Guido, de Klein, Annelies, Oracz, Grzegorz, Brosens, Erwin, Reutter, Heiko, and Schumacher, Johannes

Abstract

Esophageal atresia with or without tracheoesophageal fistula (EA/TEF) is the most common congenital malformation of the upper digestive tract. This study represents the first genome-wide association study (GWAS) to identify risk loci for EA/TEF. We used a European case-control sample comprising 764 EA/TEF patients and 5,778 controls and observed genome-wide significant associations at three loci. On chromosome 10q21 within the gene CTNNA3 (p = 2.11 x 10(-8); odds ratio [OR] = 3.94; 95% confidence interval [CI], 3.10-5.00), on chromosome 16q24 next to the FOX gene cluster (p = 2.25 x 10(-10); OR = 1.47; 95% CI, 1.38-1.55) and on chromosome 17q12 next to the gene HNF1B (p = 3.35 x 10(-16); OR = 1.75; 95% CI, 1.64-1.87). We next carried out an esophageal/tracheal transcriptome profiling in rat embryos at four selected embryonic time points. Based on these data and on already published data, the implicated genes at all three GWAS loci are promising candidates for EA/TEF development. We also analyzed the genetic EA/TEF architecture beyond the single marker level, which revealed an estimated single-nucleotide polymorphism (SNP)-based heritability of around 37% +/- 14% standard deviation. In addition, we examined the polygenicity of EA/TEF and found that EA/TEF is less polygenic than other complex genetic diseases. In conclusion, the results of our study contribute to a better understanding on the underlying genetic architecture of ET/TEF with the identification of three risk loci and candidate genes.

Published
2022
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2. First genome-wide association study of esophageal atresia identifies three genetic risk loci at CTNNA3, FOXF1/FOXC2/FOXL1, and HNF1B

Author

Gehlen, Jan, primary, Giel, Ann-Sophie, additional, Köllges, Ricarda, additional, Haas, Stephan L., additional, Zhang, Rong, additional, Trcka, Jiri, additional, Sungur, Ayse Ö., additional, Renziehausen, Florian, additional, Bornholdt, Dorothea, additional, Jung, Daphne, additional, Hoyer, Paul D., additional, Nordenskjöld, Agneta, additional, Tibboel, Dick, additional, Vlot, John, additional, Spaander, Manon C.W., additional, Smigiel, Robert, additional, Patkowski, Dariusz, additional, Roeleveld, Nel, additional, van Rooij, Iris ALM., additional, de Blaauw, Ivo, additional, Hölscher, Alice, additional, Pauly, Marcus, additional, Leutner, Andreas, additional, Fuchs, Joerg, additional, Niethammer, Joel, additional, Melissari, Maria-Theodora, additional, Jenetzky, Ekkehart, additional, Zwink, Nadine, additional, Thiele, Holger, additional, Hilger, Alina Christine, additional, Hess, Timo, additional, Trautmann, Jessica, additional, Marks, Matthias, additional, Baumgarten, Martin, additional, Bläss, Gaby, additional, Landén, Mikael, additional, Fundin, Bengt, additional, Bulik, Cynthia M., additional, Pennimpede, Tracie, additional, Ludwig, Michael, additional, Ludwig, Kerstin U., additional, Mangold, Elisabeth, additional, Heilmann-Heimbach, Stefanie, additional, Moebus, Susanne, additional, Herrmann, Bernhard G., additional, Alsabeah, Kristina, additional, Burgos, Carmen M., additional, Lilja, Helene E., additional, Azodi, Sahar, additional, Stenström, Pernilla, additional, Arnbjörnsson, Einar, additional, Frybova, Barbora, additional, Lebensztejn, Dariusz M., additional, Debek, Wojciech, additional, Kolodziejczyk, Elwira, additional, Kozera, Katarzyna, additional, Kierkus, Jaroslaw, additional, Kaliciński, Piotr, additional, Stefanowicz, Marek, additional, Socha-Banasiak, Anna, additional, Kolejwa, Michal, additional, Piaseczna-Piotrowska, Anna, additional, Czkwianianc, Elzbieta, additional, Nöthen, Markus M., additional, Grote, Phillip, additional, Rygl, Michal, additional, Reinshagen, Konrad, additional, Spychalski, Nicole, additional, Ludwikowski, Barbara, additional, Hubertus, Jochen, additional, Heydweiller, Andreas, additional, Ure, Benno, additional, Muensterer, Oliver J., additional, Aubert, Ophelia, additional, Gosemann, Jan-Hendrik, additional, Lacher, Martin, additional, Degenhardt, Petra, additional, Boemers, Thomas M., additional, Mokrowiecka, Anna, additional, Małecka-Panas, Ewa, additional, Wöhr, Markus, additional, Knapp, Michael, additional, Seitz, Guido, additional, de Klein, Annelies, additional, Oracz, Grzegorz, additional, Brosens, Erwin, additional, Reutter, Heiko, additional, and Schumacher, Johannes, additional

Published
2022
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3. Human exome and mouse embryonic expression data implicateZFHX3,TRPS1, andCHD7in human esophageal atresia

Author

Zhang, Rong, Gehlen, Jan, Kawalia, Amit, Melissari, Maria-Theodora, Dakal, Tikam Chand, Menon, Athira M., Hoefele, Julia, Riedhammer, Korbinian, Waffenschmidt, Lea, Fabian, Julia, Breuer, Katinka, Kalanithy, Jeshurun, Hilger, Alina Christine, Sharma, Amit, Hoelscher, Alice, Boemers, Thomas M., Pauly, Markus, Leutner, Andreas, Fuchs, Joerg, Seitz, Guido, Ludwikowski, Barbara M., Gomez, Barbara, Hubertus, Jochen, Heydweiller, Andreas, Kurz, Ralf, Leonhardt, Johannes, Kosch, Ferdinand, Holland-Cunz, Stefan, Muensterer, Oliver, Ure, Beno, Schmiedeke, Eberhard, Neser, Joerg, Degenhardt, Petra, Maerzheuser, Stefanie, Kleine, Katharina, Schaefer, Mattias, Spychalski, Nicole, Deffaa, Oliver J., Gosemann, Jan-Hendrik, Lacher, Martin, Heilmann-Heimbach, Stefanie, Zwink, Nadine, Jenetzky, Ekkehart, Ludwig, Michael, Grote, Phillip, Schumacher, Johannes, Thiele, Holger, Reutter, Heiko, Zhang, Rong, Gehlen, Jan, Kawalia, Amit, Melissari, Maria-Theodora, Dakal, Tikam Chand, Menon, Athira M., Hoefele, Julia, Riedhammer, Korbinian, Waffenschmidt, Lea, Fabian, Julia, Breuer, Katinka, Kalanithy, Jeshurun, Hilger, Alina Christine, Sharma, Amit, Hoelscher, Alice, Boemers, Thomas M., Pauly, Markus, Leutner, Andreas, Fuchs, Joerg, Seitz, Guido, Ludwikowski, Barbara M., Gomez, Barbara, Hubertus, Jochen, Heydweiller, Andreas, Kurz, Ralf, Leonhardt, Johannes, Kosch, Ferdinand, Holland-Cunz, Stefan, Muensterer, Oliver, Ure, Beno, Schmiedeke, Eberhard, Neser, Joerg, Degenhardt, Petra, Maerzheuser, Stefanie, Kleine, Katharina, Schaefer, Mattias, Spychalski, Nicole, Deffaa, Oliver J., Gosemann, Jan-Hendrik, Lacher, Martin, Heilmann-Heimbach, Stefanie, Zwink, Nadine, Jenetzky, Ekkehart, Ludwig, Michael, Grote, Phillip, Schumacher, Johannes, Thiele, Holger, and Reutter, Heiko

Abstract

Introduction Esophageal atresia with or without tracheoesophageal fistula (EA/TEF) occurs approximately 1 in 3.500 live births representing the most common malformation of the upper digestive tract. Only half a century ago, EA/TEF was fatal among affected newborns suggesting that the steady birth prevalence might in parts be due to mutationalde novoevents in genes involved in foregut development. Methods To identify mutationalde novoevents in EA/TEF patients, we surveyed the exome of 30 case-parent trios. Identified and confirmedde novovariants were prioritized usingin silicoprediction tools. To investigate the embryonic role of genes harboring prioritizedde novovariants we performed targeted analysis of mouse transcriptome data of esophageal tissue obtained at the embryonic day (E) E8.5, E12.5, and postnatal. Results In total we prioritized 14 novelde novovariants in 14 different genes (APOL2,EEF1D,CHD7,FANCB,GGT6,KIAA0556,NFX1,NPR2,PIGC,SLC5A2,TANC2,TRPS1,UBA3, andZFHX3) and eight rarede novovariants in eight additional genes (CELSR1,CLP1,GPR133,HPS3,MTA3,PLEC,STAB1, andPPIP5K2). Through personal communication during the project, we identified an additional EA/TEF case-parent trio with a rarede novovariant inZFHX3.In silicoprediction analysis of the identified variants and comparative analysis of mouse transcriptome data of esophageal tissue obtained at E8.5, E12.5, and postnatal prioritizedCHD7,TRPS1, andZFHX3as EA/TEF candidate genes. Re-sequencing ofZFHX3in additional 192 EA/TEF patients did not identify further putative EA/TEF-associated variants. Conclusion Our study suggests that rare mutationalde novoevents in genes involved in foregut development contribute to the development of EA/TEF.

Published
2020

4. Human exome and mouse embryonic expression data implicate ZFHX3, TRPS1, and CHD7 in human esophageal atresia

Author

Pastor Santos-Cortez, Regie Lyn, Zhang, Rong, Gehlen, Jan, Kawalia, Amit, Melissari, Maria-Theodora, Dakal, Tikam Chand, Menon, Athira M., Höfele, Julia, Riedhammer, Korbinian, Waffenschmidt, Lea, Fabian, Julia, Breuer, Katinka, Kalanithy, Jeshurun, Hilger, Alina Christine, Sharma, Amit, Hölscher, Alice, Boemers, Thomas M., Pauly, Markus, Leutner, Andreas, Fuchs, Jörg, Seitz, Guido, Ludwikowski, Barbara, Gomez, Barbara, Hubertus, Jochen, Heydweiller, Andreas, Kurz, Ralf, Leonhardt, Johannes, Kosch, Ferdinand, Holland-Cunz, Stefan, Münsterer, Oliver, Ure, Beno, Schmiedeke, Eberhard, Neser, Jörg, Degenhardt, Petra, Märzheuser, Stefanie, Kleine, Katharina, Schäfer, Mattias, Spychalski, Nicole, Deffaa, Oliver J., Gosemann, Jan-Hendrik, Lacher, Martin, Heilmann-Heimbach, Stefanie, Zwink, Nadine, Jenetzky, Ekkehart, Ludwig, Michael, Grote, Phillip, Schumacher, Johannes, Thiele, Holger, Reutter, Heiko, Pastor Santos-Cortez, Regie Lyn, Zhang, Rong, Gehlen, Jan, Kawalia, Amit, Melissari, Maria-Theodora, Dakal, Tikam Chand, Menon, Athira M., Höfele, Julia, Riedhammer, Korbinian, Waffenschmidt, Lea, Fabian, Julia, Breuer, Katinka, Kalanithy, Jeshurun, Hilger, Alina Christine, Sharma, Amit, Hölscher, Alice, Boemers, Thomas M., Pauly, Markus, Leutner, Andreas, Fuchs, Jörg, Seitz, Guido, Ludwikowski, Barbara, Gomez, Barbara, Hubertus, Jochen, Heydweiller, Andreas, Kurz, Ralf, Leonhardt, Johannes, Kosch, Ferdinand, Holland-Cunz, Stefan, Münsterer, Oliver, Ure, Beno, Schmiedeke, Eberhard, Neser, Jörg, Degenhardt, Petra, Märzheuser, Stefanie, Kleine, Katharina, Schäfer, Mattias, Spychalski, Nicole, Deffaa, Oliver J., Gosemann, Jan-Hendrik, Lacher, Martin, Heilmann-Heimbach, Stefanie, Zwink, Nadine, Jenetzky, Ekkehart, Ludwig, Michael, Grote, Phillip, Schumacher, Johannes, Thiele, Holger, and Reutter, Heiko

Abstract

Introduction: Esophageal atresia with or without tracheoesophageal fistula (EA/TEF) occurs approximately 1 in 3.500 live births representing the most common malformation of the upper digestive tract. Only half a century ago, EA/TEF was fatal among affected newborns suggesting that the steady birth prevalence might in parts be due to mutational de novo events in genes involved in foregut development. Methods: To identify mutational de novo events in EA/TEF patients, we surveyed the exome of 30 case-parent trios. Identified and confirmed de novo variants were prioritized using in silico prediction tools. To investigate the embryonic role of genes harboring prioritized de novo variants we performed targeted analysis of mouse transcriptome data of esophageal tissue obtained at the embryonic day (E) E8.5, E12.5, and postnatal. Results: In total we prioritized 14 novel de novo variants in 14 different genes (APOL2, EEF1D, CHD7, FANCB, GGT6, KIAA0556, NFX1, NPR2, PIGC, SLC5A2, TANC2, TRPS1, UBA3, and ZFHX3) and eight rare de novo variants in eight additional genes (CELSR1, CLP1, GPR133, HPS3, MTA3, PLEC, STAB1, and PPIP5K2). Through personal communication during the project, we identified an additional EA/TEF case-parent trio with a rare de novo variant in ZFHX3. In silico prediction analysis of the identified variants and comparative analysis of mouse transcriptome data of esophageal tissue obtained at E8.5, E12.5, and postnatal prioritized CHD7, TRPS1, and ZFHX3 as EA/TEF candidate genes. Re-sequencing of ZFHX3 in additional 192 EA/TEF patients did not identify further putative EA/TEF-associated variants. Conclusion: Our study suggests that rare mutational de novo events in genes involved in foregut development contribute to the development of EA/TEF.

Published
2020

8. Human exome and mouse embryonic expression data implicate ZFHX3, TRPS1, and CHD7 in human esophageal atresia

Author

Zhang, Rong, primary, Gehlen, Jan, additional, Kawalia, Amit, additional, Melissari, Maria-Theodora, additional, Dakal, Tikam Chand, additional, Menon, Athira M., additional, Höfele, Julia, additional, Riedhammer, Korbinian, additional, Waffenschmidt, Lea, additional, Fabian, Julia, additional, Breuer, Katinka, additional, Kalanithy, Jeshurun, additional, Hilger, Alina Christine, additional, Sharma, Amit, additional, Hölscher, Alice, additional, Boemers, Thomas M., additional, Pauly, Markus, additional, Leutner, Andreas, additional, Fuchs, Jörg, additional, Seitz, Guido, additional, Ludwikowski, Barbara M., additional, Gomez, Barbara, additional, Hubertus, Jochen, additional, Heydweiller, Andreas, additional, Kurz, Ralf, additional, Leonhardt, Johannes, additional, Kosch, Ferdinand, additional, Holland-Cunz, Stefan, additional, Münsterer, Oliver, additional, Ure, Beno, additional, Schmiedeke, Eberhard, additional, Neser, Jörg, additional, Degenhardt, Petra, additional, Märzheuser, Stefanie, additional, Kleine, Katharina, additional, Schäfer, Mattias, additional, Spychalski, Nicole, additional, Deffaa, Oliver J., additional, Gosemann, Jan-Hendrik, additional, Lacher, Martin, additional, Heilmann-Heimbach, Stefanie, additional, Zwink, Nadine, additional, Jenetzky, Ekkehart, additional, Ludwig, Michael, additional, Grote, Phillip, additional, Schumacher, Johannes, additional, Thiele, Holger, additional, and Reutter, Heiko, additional

Published
2020
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12. Fremdkörper im Kniegelenk nach Bagatellverletzung

Author

Wirmer, Johannes, Degenhardt, Petra, Rothe, Karin, and Jung, Tobias

Subjects
ddc: 610, 610 Medical sciences, Medicine
Abstract

Einleitung: Oberflächliche Verletzungen an den Extremitäten, auch im Bereich des Knies sind häufig Grund der Vorstellung in der kinderchirurgischen Rettungsstelle. Intraartikuläre Fremdkörper im Kniegelenk, als Folge dieser Verletzungen, sind dagegen selten. In der Literatur[for full text, please go to the a.m. URL], 131. Kongress der Deutschen Gesellschaft für Chirurgie

Published
2014

13. Klinisches und radiologisches Outcome nach arthroskopischem Ersatz des vorderen Kreuzbandes bei Patienten mit offenen Wachstumsfugen

Author

Gwinner, Clemens, Kopf, Sebastian, Lackner, Theresa, Degenhardt, Petra, Haas, Norbert, and Jung, Tobias

Subjects
ddc: 610, 610 Medical sciences, Medicine
Abstract

Einleitung: Die konservative Therapie nach VKB Ruptur im Wachstumsalter ist mit unbefriedigenden klinischen Ergebnissen und einer hohen Rate an Sekundärschäden verbunden. Der hohe Aktivitätsanspruch, die häufig fehlende Compliance sowie die spezielle Anatomie des Kniegelenks im Kindesalter[for full text, please go to the a.m. URL], 131. Kongress der Deutschen Gesellschaft für Chirurgie

Published
2014
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14. Reduced Microvascular Density in Omental Biopsies of Children with Chronic Kidney Disease

Author

Burkhardt, Dorothea, primary, Bartosova, Maria, additional, Schaefer, Betti, additional, Grabe, Niels, additional, Lahrmann, Bernd, additional, Nasser, Hamoud, additional, Freise, Christian, additional, Schneider, Axel, additional, Lingnau, Anja, additional, Degenhardt, Petra, additional, Ranchin, Bruno, additional, Sallay, Peter, additional, Cerkauskiene, Rimante, additional, Malina, Michal, additional, Ariceta, Gema, additional, Schmitt, Claus Peter, additional, and Querfeld, Uwe, additional

Published
2016
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15. Interdisziplinäres Management am Beispiel der CPAM

Author

Rothe, Karin, Kalache, Karim, Degenhardt, Petra, and Proquitte, Hans

Subjects
ddc: 610, 610 Medical sciences, Medicine
Abstract

Einleitung: Durch die verbesserte pränatale Diagnostik der letzten Jahre wurde zum einen die Variabilität angeborener zystischer Lungenerkrankungen und zum anderen die individuelle Biologie der Entitäten deutlich. Aus der Vielzahl untersuchter Prognoseparameter sind bilaterale Erkrankungen[for full text, please go to the a.m. URL], 129. Kongress der Deutschen Gesellschaft für Chirurgie

Published
2012

16. Erfahrungen mit der sonographiegestützen Einlage zentraler Venenverweilkatheter in Seldingertechnik bei Säuglingen im interdisziplinären Setting

Author

Märzheuser, Stefanie, Von Dem Busche, Katja, Knipprath, Ulrike, and Degenhardt, Petra

Subjects
ddc: 610, 610 Medical sciences, Medicine
Abstract

Einleitung: Die Einlage zentraler Venenverweilkatheter mit perkutaner Ausleitung per punctionem und Seldingertechnik wenden wir auch im Säuglingsalter gefäßschonend sonographiegestützt an. In einer retrospektiven Analyse wurden Patienten untersucht, bei denen vor dem vollendeten [for full text, please go to the a.m. URL], 128. Kongress der Deutschen Gesellschaft für Chirurgie

Published
2011

25. First genome-wide association study of esophageal atresia identifies three genetic risk loci at CTNNA3 , FOXF1 / FOXC2 / FOXL1 , and HNF1B .

Author

Gehlen J, Giel AS, Köllges R, Haas SL, Zhang R, Trcka J, Sungur AÖ, Renziehausen F, Bornholdt D, Jung D, Hoyer PD, Nordenskjöld A, Tibboel D, Vlot J, Spaander MCW, Smigiel R, Patkowski D, Roeleveld N, van Rooij IA, de Blaauw I, Hölscher A, Pauly M, Leutner A, Fuchs J, Niethammer J, Melissari MT, Jenetzky E, Zwink N, Thiele H, Hilger AC, Hess T, Trautmann J, Marks M, Baumgarten M, Bläss G, Landén M, Fundin B, Bulik CM, Pennimpede T, Ludwig M, Ludwig KU, Mangold E, Heilmann-Heimbach S, Moebus S, Herrmann BG, Alsabeah K, Burgos CM, Lilja HE, Azodi S, Stenström P, Arnbjörnsson E, Frybova B, Lebensztejn DM, Debek W, Kolodziejczyk E, Kozera K, Kierkus J, Kaliciński P, Stefanowicz M, Socha-Banasiak A, Kolejwa M, Piaseczna-Piotrowska A, Czkwianianc E, Nöthen MM, Grote P, Rygl M, Reinshagen K, Spychalski N, Ludwikowski B, Hubertus J, Heydweiller A, Ure B, Muensterer OJ, Aubert O, Gosemann JH, Lacher M, Degenhardt P, Boemers TM, Mokrowiecka A, Małecka-Panas E, Wöhr M, Knapp M, Seitz G, de Klein A, Oracz G, Brosens E, Reutter H, and Schumacher J

Abstract

Esophageal atresia with or without tracheoesophageal fistula (EA/TEF) is the most common congenital malformation of the upper digestive tract. This study represents the first genome-wide association study (GWAS) to identify risk loci for EA/TEF. We used a European case-control sample comprising 764 EA/TEF patients and 5,778 controls and observed genome-wide significant associations at three loci. On chromosome 10q21 within the gene CTNNA3 (p = 2.11 × 10 -8 ; odds ratio [OR] = 3.94; 95% confidence interval [CI], 3.10-5.00), on chromosome 16q24 next to the FOX gene cluster (p = 2.25 × 10 -10 ; OR = 1.47; 95% CI, 1.38-1.55) and on chromosome 17q12 next to the gene HNF1B (p = 3.35 × 10 -16 ; OR = 1.75; 95% CI, 1.64-1.87). We next carried out an esophageal/tracheal transcriptome profiling in rat embryos at four selected embryonic time points. Based on these data and on already published data, the implicated genes at all three GWAS loci are promising candidates for EA/TEF development. We also analyzed the genetic EA/TEF architecture beyond the single marker level, which revealed an estimated single-nucleotide polymorphism (SNP)-based heritability of around 37% ± 14% standard deviation. In addition, we examined the polygenicity of EA/TEF and found that EA/TEF is less polygenic than other complex genetic diseases. In conclusion, the results of our study contribute to a better understanding on the underlying genetic architecture of ET/TEF with the identification of three risk loci and candidate genes., Competing Interests: The co-author C.M.B. declares the following interests: Shire (grant recipient, Scientific Advisory Board member), Idorsia (consultant), Lundbeckfonden (grant recipient), Pearson (author, royalty recipient), and Equip Health Inc. (Clinical Advisory Board). All other co-authors declare no competing interests., (© 2022 The Authors.)

Published
2022
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26. [Emergencies in pediatric traumatology--fractures in the growing age and pediatric polytrauma].

Author

Degenhardt P, Kleber C, and Bail HJ

Subjects
Child, Germany, Humans, Multiple Trauma diagnosis, Emergency Medical Services methods, Fractures, Bone diagnosis, Fractures, Bone therapy, Multiple Trauma therapy, Pediatrics methods, Traumatology methods
Abstract

Deep knowledge of characteristic features of the growing skeleton is necessary for effective treatment of fractures in the pediatric population. The first part of emergency treatment of pediatric fractures involves immobilisation and appropriate pain management. In addition reduction of the fracture, either open or closed, with or without internal or external fixation are further treatment options used by the experienced pediatric surgeon. Generally, the principles of therapy of pediatric polytrauma are similar to the management of trauma in adults (ATLS). Nonetheless, attention must be paid to anatomical and physiological differences especially between young children and adults.

Published
2009
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