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47 results on '"Schulze, Egbert"'

2. Cross-oncopanel study reveals high sensitivity and accuracy with overall analytical performance depending on genomic regions

Author

Gong, Binsheng, Li, Dan, Kusko, Rebecca, Novoradovskaya, Natalia, Zhang, Yifan, Wang, Shangzi, Pabón-Peña, Carlos, Zhang, Zhihong, Lai, Kevin, Cai, Wanshi, LoCoco, Jennifer S., Lader, Eric, Richmond, Todd A., Mittal, Vinay K., Liu, Liang-Chun, Johann, Jr, Donald J., Willey, James C., Bushel, Pierre R., Yu, Ying, Xu, Chang, Chen, Guangchun, Burgess, Daniel, Cawley, Simon, Giorda, Kristina, Haseley, Nathan, Qiu, Fujun, Wilkins, Katherine, Arib, Hanane, Attwooll, Claire, Babson, Kevin, Bao, Longlong, Bao, Wenjun, Lucas, Anne Bergstrom, Best, Hunter, Bhandari, Ambica, Bisgin, Halil, Blackburn, James, Blomquist, Thomas M., Boardman, Lisa, Burgher, Blake, Butler, Daniel J., Chang, Chia-Jung, Chaubey, Alka, Chen, Tao, Chierici, Marco, Chin, Christopher R., Close, Devin, Conroy, Jeffrey, Cooley Coleman, Jessica, Craig, Daniel J., Crawford, Erin, del Pozo, Angela, Deveson, Ira W., Duncan, Daniel, Eterovic, Agda Karina, Fan, Xiaohui, Foox, Jonathan, Furlanello, Cesare, Ghosal, Abhisek, Glenn, Sean, Guan, Meijian, Haag, Christine, Hang, Xinyi, Happe, Scott, Hennigan, Brittany, Hipp, Jennifer, Hong, Huixiao, Horvath, Kyle, Hu, Jianhong, Hung, Li-Yuan, Jarosz, Mirna, Kerkhof, Jennifer, Kipp, Benjamin, Kreil, David Philip, Łabaj, Paweł, Lapunzina, Pablo, Li, Peng, Li, Quan-Zhen, Li, Weihua, Li, Zhiguang, Liang, Yu, Liu, Shaoqing, Liu, Zhichao, Ma, Charles, Marella, Narasimha, Martín-Arenas, Rubén, Megherbi, Dalila B., Meng, Qingchang, Mieczkowski, Piotr A., Morrison, Tom, Muzny, Donna, Ning, Baitang, Parsons, Barbara L., Paweletz, Cloud P., Pirooznia, Mehdi, Qu, Wubin, Raymond, Amelia, Rindler, Paul, Ringler, Rebecca, Sadikovic, Bekim, Scherer, Andreas, Schulze, Egbert, Sebra, Robert, Shaknovich, Rita, Shi, Qiang, Shi, Tieliu, Silla-Castro, Juan Carlos, Smith, Melissa, López, Mario Solís, Song, Ping, Stetson, Daniel, Strahl, Maya, Stuart, Alan, Supplee, Julianna, Szankasi, Philippe, Tan, Haowen, Tang, Lin-ya, Tao, Yonghui, Thakkar, Shraddha, Thierry-Mieg, Danielle, Thierry-Mieg, Jean, Thodima, Venkat J., Thomas, David, Tichý, Boris, Tom, Nikola, Garcia, Elena Vallespin, Verma, Suman, Walker, Kimbley, Wang, Charles, Wang, Junwen, Wang, Yexun, Wen, Zhining, Wirta, Valtteri, Wu, Leihong, Xiao, Chunlin, Xiao, Wenzhong, Xu, Shibei, Yang, Mary, Ying, Jianming, Yip, Shun H., Zhang, Guangliang, Zhang, Sa, Zhao, Meiru, Zheng, Yuanting, Zhou, Xiaoyan, Mason, Christopher E., Mercer, Timothy, Tong, Weida, Shi, Leming, Jones, Wendell, and Xu, Joshua

Published
2021
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13. Typical characteristics of children with congenital adrenal hyperplasia due to 11β-hydroxylase deficiency: a single-centre experience and review of the literature

Author

Breil, Thomas, primary, Yakovenko, Vira, additional, Inta, Ioana, additional, Choukair, Daniela, additional, Klose, Daniela, additional, Mittnacht, Janna, additional, Schulze, Egbert, additional, Alrajab, Abdul, additional, Grulich-Henn, Jürgen, additional, and Bettendorf, Markus, additional

Published
2019
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15. Heterozygous inactivating CaSR mutations causing neonatal hyperparathyroidism: function, inheritance and phenotype

Author

Glaudo, Markus, primary, Letz, Saskia, additional, Quinkler, Marcus, additional, Bogner, Ulrich, additional, Elbelt, Ulf, additional, Strasburger, Christian J, additional, Schnabel, Dirk, additional, Lankes, Erwin, additional, Scheel, Sandra, additional, Feldkamp, Joachim, additional, Haag, Christine, additional, Schulze, Egbert, additional, Frank-Raue, Karin, additional, Raue, Friedhelm, additional, Mayr, Bernhard, additional, and Schöfl, Christof, additional

Published
2016
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16. Amino Alcohol- (NPS-2143) and Quinazolinone-Derived Calcilytics (ATF936 and AXT914) Differentially Mitigate Excessive Signalling of Calcium-Sensing Receptor Mutants Causing Bartter Syndrome Type 5 and Autosomal Dominant Hypocalcemia

Author

Letz, Saskia, primary, Haag, Christine, additional, Schulze, Egbert, additional, Frank-Raue, Karin, additional, Raue, Friedhelm, additional, Hofner, Benjamin, additional, Mayr, Bernhard, additional, and Schöfl, Christof, additional

Published
2014
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17. Prevalence and Clinical Spectrum of Nonsecretory Medullary Thyroid Carcinoma in a Series of 839 Patients with Sporadic Medullary Thyroid Carcinoma

Author

Frank-Raue, Karin, primary, Machens, Andreas, additional, Leidig-Bruckner, Gudrun, additional, Rondot, Susanne, additional, Haag, Christine, additional, Schulze, Egbert, additional, Lorenz, Angela, additional, Kreissl, Michael C., additional, Dralle, Henning, additional, Raue, Friedhelm, additional, and Schmid, Kurt W., additional

Published
2013
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21. Novel Activating Mutations of the Calcium-Sensing Receptor: The Calcilytic NPS-2143 Mitigates Excessive Signal Transduction of Mutant Receptors

Author

Letz, Saskia, primary, Rus, Ramona, additional, Haag, Christine, additional, Dörr, Helmuth-Günther, additional, Schnabel, Dirk, additional, Möhlig, Matthias, additional, Schulze, Egbert, additional, Frank-Raue, Karin, additional, Raue, Friedhelm, additional, Mayr, Bernhard, additional, and Schöfl, Christof, additional

Published
2010
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22. Alterations in Lipid and Carbohydrate Metabolism in Patients with Classic Congenital Adrenal Hyperplasia due to 21-Hydroxylase Deficiency

Author

Zimmermann, Anca, primary, Grigorescu-Sido, Paula, additional, AlKhzouz, Camelia, additional, Patberg, Karen, additional, Bucerzan, Simona, additional, Schulze, Egbert, additional, Zimmermann, Tim, additional, Rossmann, Heidi, additional, Geiss, Hans-Christian, additional, Lackner, Karl J., additional, and Weber, Matthias M., additional

Published
2010
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26. Machine learning approaches for phenotype–genotype mapping: predicting heterozygous mutations in the CYP21B gene from steroid profiles

Author

Prank, Klaus, primary, Schulze, Egbert, additional, Eckert, Olaf, additional, Nattkemper, Tim W, additional, Bettendorf, Markus, additional, Maser-Gluth, Christiane, additional, Sejnowski, Terrence J, additional, Grote, Arno, additional, Penner, Erika, additional, von zur Mühlen, Alexander, additional, and Brabant, Georg, additional

Published
2005
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39. Site-directed mutagenesis of the dihydrolipoyl transacetylase component (E2p) of the nyruvate dchvdrogenase complex from <em>Azotobacter vinelandii</em>.

Author

Schulze, Egbert, Westphal, Adrie H., Boumans, Hans, and de Kok, Arie

Subjects
*MUTAGENESIS, *ACETYLTRANSFERASES, *AZOTOBACTER, *PROTEOLYTIC enzymes, *ENZYMES, *BIOCHEMISTRY
Abstract

Site-directed mutagenesis was performed in the protease-sensitive region, between the lipoyl and catalytic domains and in the catalytic domain, of the dihydrolipoyl transacetylase component (E2p) of the pyruvate dehydrogenase complex from Azotobacter vinelandii. The interaction of the mutated enzymes with the peripheral components pyruvate dehydrogenase (E1p) and lipoamide dehydrogenase (E3) was studied by gel filtration experiments, analytical ultracentrifugation and reconstitution of the pyruvate dehydrogenase complex. Upon binding of peripheral components, the 24-subunit core of A. vinelandii wild-type E2p dissociates into tetramers. Four E1p or E3 dimers can bind to a tetramer. Binding is mutually exclusive, resulting in an active complex containing one E3 and three E1p dimers. Large deletions of the protease-sensitive region of E2p resulted in a total loss of the E1p and E3 binding. A small deletion (Δ P361–R362) or the point mutation K367Q in the protease-sensitive region did not influence E3 binding, but affected E1p binding strongly, although with excess E1p almost complete reconstitution was reached. For E2p with the point mutation R416D in the N-terminal region of the catalytic domain only 16% overall activity could be measured in reconstituted complexes. This is due to a very weak E1p/E2p interaction, whereas the E3 binding was not affected. The point mutation R416D did not influence the catalytic activity of E2p, although a function for this residue in the formation of the active site was predicted from amino acid similarities with chloramphenicol acetyltransferase type III from Escherichia coli. Deletion of the complete Ala + Pro-rich sequence between the protease-sensitive region and the catalytic domain did not affect the enzymological properties of E2p, nor the affinity for E1p or E3. A further deletion of 20 N-terminal residues from the catalytic domain destroyed the E2p activity. From gel filtration experiments it was concluded that the quaternary structure was unaffected, as was E3 binding. E1p binding was lost and, in contrast to the wild-type enzyme, no dissociation of the core upon addition of E3 was observed. This mutant enzyme possesses, like E. coli E2p, six E3 binding sites and clearly shows that interaction of E3 or E1p with the E1p sites and dissociation are linked processes. It is concluded that the binding site for E3 is located on the N-terminal part of the protease-sensitive region. In contrast, the binding site for E1p consists of two regions, one located on the protease-sensitive region and one of the catalytic domain. These regions are separated by a flexible sequence of about 20 amino acids. [ABSTRACT FROM AUTHOR]

Published
1991
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40. The catalytic domain of the dihydrolipoyl transacetylase component of the pyruvate dehydrogenase complex from <em>Azotobacter vinelandii</em> and <em>Escherichia coli</em>.

Author

Schulze, Egbert, Westphal, Adrie H., Obmolova, Galya, Mattevi, Andrea, Hol, Wim G. J., and De Kok, Arie

Subjects
*PYRUVATES, *KETONIC acids, *PYRUVATE kinase, *PHOSPHOTRANSFERASES, *AZOTOBACTER, *AZOTOBACTERACEAE, *ESCHERICHIA coli, *ESCHERICHIA
Abstract

Partial sequences of the dihydrolipoyl transacetytase component (E2p) of the pyruvate dehydrogenase complex from Azotobacter vinelandii and Escherichia coli, containing the catalytic domain, were cloned in pUC plasmids and over-expressed in E. coli TG2. A high expression of a homogeneous protein was only detectable for E2p mutants consisting of the catalytic domain and the alanine-proline-rich sequence between a putative binding region for the peripheral components and the catalytic domain(apa-4). Most of the catalytic domain from A. vinelandii without the apa-4 sequence was degraded intracellularly, probably due to incorrect folding. Fusion proteins of six amino acids from β-galactosidase, the apa-4 region and the catalytic domains of ,4, vinelandii or E. coli E2p could be highly purified. Both catalytic domains were assembled in 24-subtmit structures with a molecular mass of approximately 670 kDa. The expression of catalytic domain from A. vinelandii E2p is more than twice as high as found for wild-type E2p. This can be explained by intracellular degradation of overexpressed wild-type E2p, whereas the catalytic domains are stable against proteolysis/n vivo and in vitro. The interaction of the peripheral components pyruvate dehydrogenase (E1p) and dihydrolipoamide dehydrogenase (E3) with the catalytic domains was studied, using gel filtration on Superose-6 and sedimentation velocity experiments. No binding of either E1p or E3 to the catalytic domain of either organism was detectable. Crystals of the catalytic domain of A. vinelandii E2p could ix: grown to a maximum size of 0.6 × 0.6 times; 0.4 mm. They diffract up to a resolution of 0.28 nm. [ABSTRACT FROM AUTHOR]

Published
1991
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41. Interaction of lipoamide dehydrogenase with the dihydrolipoyl transacetylase component of the pyruvate dehydrogenase complex from <em>Azotobacter vinelandii</em>.

Author

Schulze, Egbert, Benen, Jacques A. E., Westphal, Adrie H., and De Kok, Arie

Subjects
*DEHYDROGENASES, *PYRUVATES, *PSEUDOMONAS fluorescens, *AZOTOBACTER, *GLUTATHIONE, *AMINO acids
Abstract

The interaction between lipoamide dehydrogenase (E3) and dihydrolipoyl transacetylase (E2p) from the pyruvate dehydrogenase complex was studied during the reconstitution of monomeric E3 apoenzymes from Azotobacter vinelandii and Pseudomonas fluorescens. The dimeric form of E3 is not only essential for catalysis but also for binding to the E2p core, because the apoenzymes as well as a monomeric holoenzyme from P. fluorescens, which can be stabilized as an intermediate at 0°C, do not bind to E2p. Lipoamide dehydrogenase from A. vinelandii contains a C-terminal extension of 15 amino acids with respect to glutathione reductase which is, in contrast to E3, presumably not part of a multienzyme complex. Furthermore, the last 10 amino acid residues of E3 are not visible in the electron density map of the crystal structure and are probably disordered. Therefore, the C-terminal tail of E3 might be an attractive candidate for a binding region. To probe this hypothesis, a set of deletions of this part was prepared by site-directed mutagenesis. Deletion of the last five amino acid residues did not result in significant changes. A further deletion of four amino acid residues resulted in a decrease of lipoamide activity to 5% of wild type, but the binding to E2p was unaffected. Therefore it is concluded that the C-terminus is not directly involved in binding to the E2p core. Deletion of the last 14 amino acids produced an enzyme with a high tendency to dissociate (Kd approximately 2.5 μM). This mutant binds only weakly to E2p. The diaphorase activity was still high. This indicates, together with the decreased Km for NADH, that the structure of the monomer is not appreciably changed by the mutation. Rather the orientation of the monomers with respect to each other is changed. It can be concluded that the binding region of E3 for E2p is constituted from structural parts of both monomers and binding occurs only when dimerization is complete. [ABSTRACT FROM AUTHOR]

Published
1991
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42. The 2-oxoglutarate dehydrogenase complex from <em>Azotobacter vinelandii</em> 1. Molecular cloning and sequence analysis of the gene encoding the 2-oxoglutarate dehydrogenase component.

Author

Schulze, Egbert, Westphal, Adrie H., Hanemaaijer, Roeland, and de Kok, Arie

Subjects
*DEHYDROGENASES, *ENZYMES, *ESCHERICHIA coli, *NUCLEIC acid analysis, *ENTEROBACTERIACEAE, *GENES, *MESSENGER RNA, *PYRUVATES
Abstract

The nucleotide sequence of the gene encoding the 2-oxoglutarate dehydrogenase component (Elo) of the 2- oxoglutarate dehydrogenase complex from Azotobacter vinelandii has been determined. The protein-coding se- quence consists of 2832 bp (944 codons, including the AUG start codon and the UAA stop codon). The predicted molecular mass (105687 Da) is in good agreement with that published for the isolated enzyme. The Elo gene is separated from the gene encoding the E2o component by a 42-bp intergenic region. No Escherichia-coli-like promoter sequences are found in the sequenced 97 bp upstream from the Elo gene. A putative ribosome-binding site is located 10–16 bp upstream from the start codon of the Elo gene. No terminator sequences could be detected downstream from the stop codon. Together with the identical situation for the E2o gene and the presence of terminating sequences downstream of the E3 gene, it can be assumed that all three genes of the 2-oxoglutarate dehydrogenase multienzyme complex are transcribed as a single mRNA transcript under the control of a promoter, located more than 100 bp upstream of the Elo gene, analogous to the pyruvate dehydrogenase complex in E. coli. The similarity with the sucA gene of E. coli is high with 59% identity. [ABSTRACT FROM AUTHOR]

Published
1990
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44. A Homozygous L299P Mutation in the CYP11B1Gene Leads to Complete Virilization in 46,XX Individuals with 11-Beta-Hydroxylase Deficiency

Author

Riedl, Stefan, Nguyen, Huy-Hoang, Clausmeyer, Susanne, Schulze, Egbert, Waldhauser, Franz, and Bernhardt, Rita

Abstract

AbstractBackground/Aim:11-β-hydroxylase deficiency (11βOHD) is caused by CYP11B1gene defects and leads to congenital adrenal hyperplasia associated with hypertension. Recently, a novel L299P mutation has been described in a compound heterozygous male individual. We observed two 46,XX siblings with a homozygous L299P mutation and investigated the functional properties of this CYP11B1variant. Patients:The index patient from a consanguineous Turkish family showed complete external virilization and was diagnosed incidentally at the age of 19 months during hospital admission for severe combined bacterial (urosepsis) and viral (CMV and EBV) infection. The younger sibling was diagnosed at the age of 5 months. Their genital phenotype was identical and both demonstrated borderline elevated blood pressure. Results:Biochemical findings revealed 11βOHD. A homozygous L299P mutation of the CYP11B1gene was detected. In vitro expression studies performed in HCT116 cells showed a markedly decreased CYP11B1 activity in the L299P mutant (1.6 ± 0.8) for the conversion of 11-deoxycortisol to cortisol. Conclusions:Our study provides clear data on the functional properties and clinical phenotype in 46,XX individuals homozygous for this point mutation. Adrenal insufficiency might have contributed to the severe infectious disease that was present in the index patient at diagnosis.Copyright © 2008 S. Karger AG, Basel

Published
2008
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45. Time-resolved fluorescence studies on mutants of the dihydrolipoyl transacetylase (E2) component of the pyruvate dehydrogenase complex from Azotobacter vinelandii

Author

Schulze, Egbert, Westphal, Adrie H., Berg, Axel, and de Kok, Arie

Abstract

Fluorescence anisotropy decays were measured for the wild-type dihydrolipoyl transacetylase (E2) component of pyruvate dehydrogenase complex from Azotobacter vinelandiiand E. coliand for E2-mutants from A. vinelandiiin which the alanine-proline-rich sequence between the binding domain and the catalytic domain is partially or completely deleted. In both E2-mutants the rotational mobility of the lipoyl domain and the overall activity after reconstitution of the complex are significantly decreased indicating the important role of the deleted sequence for the movement of the lipoyl domain and the transfer of substrates between the different active sites within the complex.

Published
1990
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46. Clinical utility gene card for: multiple endocrine neoplasia type 2.

Author

Raue, Friedhelm, Rondot, Susanne, Schulze, Egbert, Szpak-Ulczok, Sylwia, Jarzab, Barbara, and Frank-Raue, Karin

Subjects
MUCOSAL neuroma syndrome, SIPPLE syndrome, TEXTILE fibers, GENEALOGY, PLANT fibers, DIAGNOSIS
Abstract

The article offers information on the disease multiple endocrine neoplasia type 2. It mentions that RET-mutation screening is a test available for familial MTC. It also mentions that the clinical specificity of the disease dependents on variable factors such as family history or age. Further it mentions that multiple endocrine neoplasia type 2 is also known as multiple endocrine neoplasia 2A, multiple endocrine neoplasia 2B (MEN 2B), and familial medullary thyroid carcinoma (FMTC).

Published
2012
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47. Change in the spectrum of RET mutations diagnosed between 1994 and 2006.

Author

Frank-Raue K, Rondot S, Schulze E, and Raue F

Subjects
DNA Mutational Analysis, DNA Primers, Humans, Proto-Oncogene Mas, Carcinoma, Medullary genetics, Multiple Endocrine Neoplasia Type 2a genetics, Multiple Endocrine Neoplasia Type 2b genetics, Mutation genetics, Proto-Oncogene Proteins c-ret genetics, Thyroid Neoplasms genetics
Abstract

Medullary thyroid carcinoma (MTC) is a rare calcitonin producing tumor. About 70-75% of patients with MTC have sporadic disease while the others suffer from hereditary MTC. Hereditary MTC is divided into three clinical subtypes: multiple endocrine neoplasia (MEN) type 2A is characterized by MTC, pheochromocytoma and primary hyperparathyroidism. MEN 2B is characterized by aggressive MTC, pheochromocytoma, marfanoid habitus and the presence of distinctive mucosal neuromas on the tongue, lips and subconjunctival areas as well as ganglioneuromatosis of the gastrointestinal tract. The third clinical subtype of inherited MTC, familial MTC, is defined as the presence of MTC in families without evidence of adrenal or parathyroid gland involvement. Hereditary MTC is caused by autosomal dominant gain-of-function mutations in the RET proto-oncogene. The first RET germline mutations were identified in 1993 in patients with MEN 2A and FMTC. Initially a codon 634 (exon 11) mutation was found in approximately 85% of patients with MEN 2A, and germline mutations in FMTC kindreds were more equally distributed throughout the RET proto-onocogene. In about 5% of families in these earlier series, mutations did not reside in exons 10 and 11. We now report a change in the spectrum of mutations detected in the RET proto-oncogene in patients with hereditary MTC from the 'classical' mutation at codon 634 in exon 11 (level 2) to more cases with mutations in the exons 13-15 (level 1) and less aggressive disease. In our series 38.9% of mutations were level 1 mutations, 54.4% level 2, and 5.6% level 3 mutations.

Published
2007

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