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2. Functional analysis of MMR gene VUS from potential Lynch syndrome patients

Author

Mahdouani, Marwa, primary, Zhuri, Drenushe, additional, Sezginer Guler, Hazal, additional, Hmida, Dorra, additional, Sana, Mokni, additional, Azaza, Mohamed, additional, Ben Said, Mariem, additional, Masmoudi, Saber, additional, Hmila, Fahmi, additional, Youssef, Sabri, additional, Ben Sghaier, Rihab, additional, Brieger, Angela, additional, Zeuzem, Stefan, additional, Saad, Ali, additional, Gurkan, Hakan, additional, Yalcintepe, Sinem, additional, Gribaa, Moez, additional, and Plotz, Guido, additional

Published
2024
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3. Erk Inhibition as a Promising Therapeutic Strategy for High IL-8-Secreting and Low SPTAN1-Expressing Colorectal Cancer

Author

Meier, Clara, primary, La Rocca, Gianluca, additional, Nawrot, Virginia, additional, Fißlthaler, Beate, additional, Overby, Sarah J., additional, Hourfar, Kai, additional, Plotz, Guido, additional, Seidl, Christian, additional, Ziegler, Paul, additional, Wild, Peter, additional, Zeuzem, Stefan, additional, Brieger, Jürgen, additional, Jäger, Elke, additional, Battmann, Achim, additional, and Brieger, Angela, additional

Published
2024
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9. Functional characterization of MLH1 missense variants unveils mechanisms of pathogenicity and clarifies role in cancer

Author

Mahdouani, Marwa, primary, Ben Ahmed, Slim, additional, Hmila, Fahmi, additional, Rais, Henda, additional, Ben Sghaier, Rihab, additional, Saad, Hanene, additional, Ben Said, Mariem, additional, Masmoudi, Saber, additional, Hmida, Dorra, additional, Brieger, Angela, additional, Zeuzem, Stefan, additional, Saad, Ali, additional, Gribaa, Moez, additional, and Plotz, Guido, additional

Published
2022
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10. Elucidating the clinical significance of two PMS2 missense variants coexisting in a family fulfilling hereditary cancer criteria

Author

González-Acosta, Maribel, del Valle, Jesús, Navarro, Matilde, Thompson, Bryony A., Iglesias, Sílvia, Sanjuan, Xavier, Paúles, María José, Padilla, Natàlia, Fernández, Anna, Cuesta, Raquel, Teulé, Àlex, Plotz, Guido, Cadiñanos, Juan, de la Cruz, Xavier, Balaguer, Francesc, Lázaro, Conxi, Pineda, Marta, and Capellá, Gabriel

Published
2017
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13. Frequency and phenotypic spectrum of germline mutations in POLE and seven other polymerase genes in 266 patients with colorectal adenomas and carcinomas

Author

Spier, Isabel, Holzapfel, Stefanie, Altmüller, Janine, Zhao, Bixiao, Horpaopan, Sukanya, Vogt, Stefanie, Chen, Sophia, Morak, Monika, Raeder, Susanne, Kayser, Katrin, Stienen, Dietlinde, Adam, Ronja, Nürnberg, Peter, Plotz, Guido, Holinski-Feder, Elke, Lifton, Richard P., Thiele, Holger, Hoffmann, Per, Steinke, Verena, and Aretz, Stefan

Published
2015
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17. Inhibition of the equilibrative nucleoside transporter 1 and activation of A2A adenosine receptors by 8-(4-chlorophenylthio)-modified cAMP analogs and their hydrolytic products

Author

Waidmann, Oliver, Pleli, Thomas, Dvorak, Karel, Bähr, Christina, Mondorf, Ulrich, Plotz, Guido, Biondi, Ricardo M., Zeuzem, Stefan, Piiper, Albrecht, Waidmann, Oliver, Pleli, Thomas, Dvorak, Karel, Bähr, Christina, Mondorf, Ulrich, Plotz, Guido, Biondi, Ricardo M., Zeuzem, Stefan, and Piiper, Albrecht

Abstract

Cyclic AMP analogs containing hydrophobic modification of C(8) at the adenine ring such as 8-(4-chlorophenylthio)-cAMP (8-pCPT-cAMP) and 8-(4-chlorophenylthio)-2'-O-methyl-cAMP (8-pCPT-2'-O-methyl-cAMP) can penetrate membranes due to their high lipophilicity and directly activate intracellular cAMP effectors. Therefore, these cAMP analogs have been used in numerous studies, assuming that their effects reflect the consequences of direct activation of cAMP effectors. The present study provides evidence that 8-pCPT-modified cAMP analogs and their corresponding putative hydrolysis products (8-(4-chlorophenylthio)-adenosine (8-pCPT-ado) and 8-(4-chlorophenylthio)-2'-O-methyl-adenosine (8-pCPT-2'-O-methyl-ado)) inhibit the equilibrative nucleoside transporter 1 (ENT1). In PC12 cells, in which nucleoside transport strongly depended on ENT1, 8-pCPT-ado, 8-pCPT-2'-O-methyl-ado, and, to a smaller extent, 8-pCPT-2'-O-methyl-cAMP caused an increase of protein kinase A substrate motif phosphorylation and anti-apoptotic effect by an A(2A) adenosine receptor (A(2A)R)-dependent mechanism. In contrast, the effects of 8-pCPT-cAMP were mainly A(2A)R-independent. In HEK 293 showing little endogenous ENT1-dependent nucleoside transport, transfection of ENT1 conferred A(2A)R-dependent increase in protein kinase A substrate motif phosphorylation. Together, the data of the present study indicate that inhibition of ENT1 and activation of adenosine receptors have to be considered when interpreting the effects of 8-pCPT-substituted cAMP/adenosine analogs.

Published
2021

22. Alternative AKT2 splicing produces protein lacking the hydrophobic motif regulatory region

Author

Plotz, Guido, Lopez-Garcia, Laura A., Brieger, Angela, Zeuzem, Stefan, Biondi, Ricardo M., Plotz, Guido, Lopez-Garcia, Laura A., Brieger, Angela, Zeuzem, Stefan, and Biondi, Ricardo M.

Abstract

Three AKT serine/threonine kinase isoforms (AKT1/AKT2/AKT3) mediate proliferation, metabolism, differentiation and anti-apoptotic signals. AKT isoforms are activated down- stream of PI3-kinase and also by PI3-kinase independent mechanisms. Mutations in the lipid phosphatase PTEN and PI3-kinase that increase PIP3 levels increase AKT signaling in a large proportion of human cancers. AKT and other AGC kinases possess a regulatory mechanism that relies on a conserved hydrophobic motif (HM) C-terminal to the catalytic core. In AKT, the HM is contiguous to the serine 473 and two other newly discovered (serine 477 and tyrosine 479) regulatory phosphorylation sites. In AKT genes, this regulatory HM region is encoded in the final exon. We identified a splice variant of AKT2 (AKT2-13a), which contains an alternative final exon and lacks the HM regulatory site. We validated the presence of mRNA for this AKT2-13a splice variant in different tissues, and the presence of AKT2-13a protein in extracts from HEK293 cells. When overexpressed in HEK293 cells, AKT2-13a is phosphorylated at the activation loop and at the zipper/turn motif phosphoryla- tion sites but has reduced specific activity. Analysis of the human transcriptome correspond- ing to other AGC kinases revealed that all three AKT isoforms express alternative transcripts lacking the HM regulatory motif, which was not the case for SGK1-3, S6K1-2, and classical, novel and atypical PKC isoforms. The transcripts of splice variants of Akt1-3 excluding the HM regulatory region could lead to expression of deregulated forms of AKT.

Published
2020

30. Additional file 2: of Diagnostic yield and clinical utility of a comprehensive gene panel for hereditary tumor syndromes

Author

Henn, Jonas, Spier, Isabel, Adam, Ronja S., Holzapfel, Stefanie, Uhlhaas, Siegfried, Kayser, Katrin, Plotz, Guido, Peters, Sophia, and Aretz, Stefan

Abstract

Figure S1. Number of genes investigated previously within the context of routine diagnostics and inconspicuous tumor tissue findings in cases of suspected Lynch syndrome in patients with (blue) or without (red) a known germline mutation prior to the present gene panel investigation. Figure S2. Percentage of patients with known mutations (blue) and patients without known mutations (red) carrying 0â 4 additional variants. Figure S3. Percentage of patients with variants in the most frequently mutated 28 genes (â Ľ 3 variants per gene). Figure S4. Top: Sequence logo presentation of protein sequence conservation of POLD1, comprising Leu460 and residues of relevance to its structural role. Highly conserved, hydrophobic residues significantly contributing to the hydrophobic pocket are indicated by yellow shading (mainly Leu469, Tyr472, Leu474, and Tyr396). Bottom: Overview of the structure of POLD1 and its domain architecture (left) (DOCX 527 kb)

Published
2019
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34. Downregulation of SPTAN1 is related to MLH1 deficiency and metastasis in colorectal cancer

Author

Ackermann, Anne, Schrecker, Christopher, Bon, Dimitra, Friedrichs, Nicolaus, Bankov, Katrin, Wild, Peter, Plotz, Guido, Zeuzem, Stefan, Herrmann, Eva, Hansmann, Martin-Leo, Brieger, Angela, Ackermann, Anne, Schrecker, Christopher, Bon, Dimitra, Friedrichs, Nicolaus, Bankov, Katrin, Wild, Peter, Plotz, Guido, Zeuzem, Stefan, Herrmann, Eva, Hansmann, Martin-Leo, and Brieger, Angela

Abstract

Introduction Colorectal cancers (CRCs) deficient in the DNA mismatch repair protein MutL homolog 1 (MLH1) display distinct clinicopathological features and require a different therapeutic approach compared to CRCs with MLH1 proficiency. However, the molecular basis of this fundamental difference remains elusive. Here, we report that MLH1-deficient CRCs exhibit reduced levels of the cytoskeletal scaffolding protein non-erythroid spectrin alpha II (SPTAN1), and that tumor progression and metastasis of CRCs correlate with SPTAN1 levels. Methods and results To investigate the link between MLH1 and SPTAN1 in cancer progression, a cohort of 189 patients with CRC was analyzed by immunohistochemistry. Compared with the surrounding normal mucosa, SPTAN1 expression was reduced in MLH1-deficient CRCs, whereas MLH1-proficient CRCs showed a significant upregulation of SPTAN1. Overall, we identified a strong correlation between MLH1 status and SPTAN1 expression. When comparing TNM classification and SPTAN1 levels, we found higher SPTAN1 levels in stage I CRCs, while stages II to IV showed a gradual reduction of SPTAN1 expression. In addition, SPTAN1 expression was lower in metastatic compared with non-metastatic CRCs. Knockdown of SPTAN1 in CRC cell lines demonstrated decreased cell viability, impaired cellular mobility and reduced cell-cell contact formation, indicating that SPTAN1 plays an important role in cell growth and cell attachment. The observed weakened cell-cell contact of SPTAN1 knockdown cells might indicate that tumor cells expressing low levels of SPTAN1 detach from their primary tumor and metastasize more easily. Conclusion Taken together, we demonstrate that MLH1 deficiency, low SPTAN1 expression, and tumor progression and metastasis are in close relation. We conclude that SPTAN1 is a candidate molecule explaining the tumor progression and metastasis of MLH1-deficient CRCs. The detailed analysis of SPTAN1 is now mandatory to substantiate its relevance and its pot

Published
2019

42. Evaluation of MLH1 variants of unclear significance

Author

Köger, Nicole, primary, Paulsen, Lea, additional, López‐Kostner, Francisco, additional, Della Valle, Adriana, additional, Vaccaro, Carlos Alberto, additional, Palmero, Edenir Inêz, additional, Alvarez, Karin, additional, Sarroca, Carlos, additional, Neffa, Florencia, additional, Kalfayan, Pablo German, additional, Gonzalez, Maria Laura, additional, Rossi, Benedito Mauro, additional, Reis, Rui Manuel, additional, Brieger, Angela, additional, Zeuzem, Stefan, additional, Hinrichsen, Inga, additional, Dominguez‐Valentin, Mev, additional, and Plotz, Guido, additional

Published
2018
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44. Validation of an in VitroMismatch Repair Assay Used in the Functional Characterization of Mismatch Repair Variants

Author

González-Acosta, Maribel, Hinrichsen, Inga, Fernández, Anna, Lázaro, Conxi, Pineda, Marta, Plotz, Guido, and Capellá, Gabriel

Abstract

A significant proportion of DNA-mismatch repair (MMR) variants are classified as of unknown significance, precluding diagnosis. The in vitroMMR assay is used to assess their MMR capability, likely the most important function of an MMR protein. However, the robustness of the assay, crucial for its use in the clinical setting, has been rarely evaluated. The aim of the present work was to validate an in vitroMMR assay approach to the functional characterization of MMR variants, as a first step to meeting quality standards of diagnostic laboratories. The MMR assay was optimized by testing a variety of reagents and experimental conditions. Reference materials and standard operating procedures were established. To determine the intra- and interexperimental variability of the assay and its reproducibility among centers, independent transfections of six previously characterized MLH1variants were performed in two independent laboratories. Reagents and conditions optimal for performing the in vitroMMR assay were determined. The validated assay demonstrated no significant intra- or interexperimental variability and good reproducibility between centers. We set up a robust in vitroMMR assay that can provide relevant in vitrofunctional evidence for MMR variant pathogenicity assessment, eventually improving the molecular diagnosis of hereditary cancer syndromes associated with MMR deficiency.

Published
2024
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45. Evaluation of <italic>MLH1</italic> variants of unclear significance.

Author

Köger, Nicole, Paulsen, Lea, López‐Kostner, Francisco, Della Valle, Adriana, Vaccaro, Carlos Alberto, Palmero, Edenir Inêz, Alvarez, Karin, Sarroca, Carlos, Neffa, Florencia, Kalfayan, Pablo German, Gonzalez, Maria Laura, Rossi, Benedito Mauro, Reis, Rui Manuel, Brieger, Angela, Zeuzem, Stefan, Hinrichsen, Inga, Dominguez‐Valentin, Mev, and Plotz, Guido

Published
2018
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46. Frequency and phenotypic spectrum of germline mutations inPOLEand seven other polymerase genes in 266 patients with colorectal adenomas and carcinomas

Author

Spier, Isabel, primary, Holzapfel, Stefanie, additional, Altmüller, Janine, additional, Zhao, Bixiao, additional, Horpaopan, Sukanya, additional, Vogt, Stefanie, additional, Chen, Sophia, additional, Morak, Monika, additional, Raeder, Susanne, additional, Kayser, Katrin, additional, Stienen, Dietlinde, additional, Adam, Ronja, additional, Nürnberg, Peter, additional, Plotz, Guido, additional, Holinski-Feder, Elke, additional, Lifton, Richard P., additional, Thiele, Holger, additional, Hoffmann, Per, additional, Steinke, Verena, additional, and Aretz, Stefan, additional

Published
2015
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47. Reduced migration of MLH1 deficient colon cancer cells depends on SPTAN1

Author

Hinrichsen, Inga, Ernst, Benjamin Philipp, Nuber, Franziska, Passmann, Sandra, Schaefer, Dieter, Steinke, Verena, Friedrichs, Nicolaus, Plotz, Guido, Zeuzem, Stefan, Brieger, Angela, Hinrichsen, Inga, Ernst, Benjamin Philipp, Nuber, Franziska, Passmann, Sandra, Schaefer, Dieter, Steinke, Verena, Friedrichs, Nicolaus, Plotz, Guido, Zeuzem, Stefan, and Brieger, Angela

Abstract

Introduction: Defects in the DNA mismatch repair (MMR) protein MLH1 are frequently observed in sporadic and hereditary colorectal cancers (CRC). Affected tumors generate much less metastatic potential than the MLH1 proficient forms. Although MLH1 has been shown to be not only involved in postreplicative MMR but also in several MMR independent processes like cytoskeletal organization, the connection between MLH1 and metastasis remains unclear. We recently identified non-erythroid spectrin all (SPTAN1), a scaffolding protein involved in cell adhesion and motility, to interact with MLH1. In the current study, the interaction of MLH1 and SPTAN1 and its potential consequences for CRC metastasis was evaluated. Methods: Nine cancer cell lines as well as fresh and paraffin embedded colon cancer tissue from 12 patients were used in gene expression studies of SPTAN1 and MLH1. Co-expression of SPTAN1 and MLH1 was analyzed by siRNA knock down of MLH1 in HeLa, HEK293, MLH1 positive HCT116, SW480 and LoVo cells. Effects on cellular motility were determined in MLH1 deficient HCT116 and MLH1 deficient HEK293T compared to their MLH1 proficient sister cells, respectively. Results: MLH1 deficiency is clearly associated with SPTAN1 reduction. Moreover, siRNA knock down of MLH1 decreased the mRNA level of SPTAN1 in HeLa, HEK293 as well as in MLH1 positive HCT116 cells, which indicates a co-expression of SPTAN1 by MLH1. In addition, cellular motility of MLH1 deficient HCT116 and MLH1 deficient HEK293T cells was impaired compared to the MLH1 proficient sister clones. Consequently, overexpression of SPTAN1 increased migration of MLH1 deficient cells while knock down of SPTAN1 decreased cellular mobility of MLH1 proficient cells, indicating SPTAN1-dependent migration ability. Conclusions: These data suggest that SPTAN1 levels decreased in concordance with MLH1 reduction and impaired cellular mobility in MLH1 deficient colon cancer cells. Therefore, aggressiveness of MLH1-positive CRC might

Published
2014

48. Promoter methylation of MLH1, PMS2, MSH2 and p16 is a phenomenon of advanced-stage HCCs

Author

Hinrichsen, Inga, Kemp, Matthias, Peveling-Oberhag, Jan Franz-Josef, Passmann, Sandra, Plotz, Guido, Zeuzem, Stefan, Brieger, Angela, Hinrichsen, Inga, Kemp, Matthias, Peveling-Oberhag, Jan Franz-Josef, Passmann, Sandra, Plotz, Guido, Zeuzem, Stefan, and Brieger, Angela

Abstract

Epigenetic silencing of tumour suppressor genes has been observed in various cancers. Looking at hepatocellular carcinoma (HCC) specific protein silencing was previously demonstrated to be associated with the Hepatitis C virus (HCV). However, the proposed HCV dependent promoter methylation of DNA mismatch repair (MMR) genes and thereby enhanced progression of hepatocarcinogenesis has been the subject of controversial discussion. We investigated promoter methylation pattern of the MMR genes MLH1, MSH2 and PMS2 as well as the cyclin-dependent kinase inhibitor 2A gene (p16) in 61 well characterized patients with HCCs associated with HCV, Hepatitis B virus infection or alcoholic liver disease. DNA was isolated from formalin-fixed, paraffin-embedded tumour and non-tumour adjacent tissue and analysed by methylation-specific PCR. Moreover, microsatellite analysis was performed in tissues showing methylation in MMR gene promoters. Our data demonstrated that promoter methylation of MLH1, MSH2, PMS2 and p16 is present among all considered HCCs. Hereby, promoter silencing was detectable more frequently in advanced-stage HCCs than in low-stage ones. However, there was no significant correlation between aberrant DNA methylation of MMR genes or p16 and HCV infection in related HCC specimens. In summary, we show that promoter methylation of essential MMR genes and p16 is detectable in HCCs most dominantly in pT3 stage tumour cases. Since loss of MMR proteins was previously described to be not only responsible for tumour development but also for chemotherapy resistance, the knowledge of mechanisms jointly responsible for HCC progression might enable significant improvement of individual HCC therapy in the future.

Published
2014

49. N‐terminus of hMLH1 confers interaction of hMutLα and hMutLβ with hMutSα

Author

Plotz, Guido, Raedle, Jochen, Brieger, Angela, Trojan, Jörg, and Zeuzem, Stefan

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, nutritional and metabolic diseases, ddc:610, neoplasms, digestive system diseases
Abstract

Mismatch repair is a highly conserved system that ensures replication fidelity by repairing mispairs after DNA synthesis. In humans, the two protein heterodimers hMutSα (hMSH2‐hMSH6) and hMutLα (hMLH1‐hPMS2) constitute the centre of the repair reaction. After recognising a DNA replication error, hMutSα recruits hMutLα, which then is thought to transduce the repair signal to the excision machinery. We have expressed an ATPase mutant of hMutLα as well as its individual subunits hMLH1 and hPMS2 and fragments of hMLH1, followed by examination of their interaction properties with hMutSα using a novel interaction assay. We show that, although the interaction requires ATP, hMutLα does not need to hydrolyse this nucleotide to join hMutSα on DNA, suggesting that ATP hydrolysis by hMutLα happens downstream of complex formation. The analysis of the individual subunits of hMutLα demonstrated that the hMutSα–hMutLα interaction is predominantly conferred by hMLH1. Further experiments revealed that only the N‐terminus of hMLH1 confers this interaction. In contrast, only the C‐terminus stabilised and co‐immunoprecipitated hPMS2 when both proteins were co‐expressed in 293T cells, indicating that dimerisation and stabilisation are mediated by the C‐terminal part of hMLH1. We also examined another human homologue of bacterial MutL, hMutLβ (hMLH1–hPMS1). We show that hMutLβ interacts as efficiently with hMutSα as hMutLα, and that it predominantly binds to hMutSα via hMLH1 as well.

Published
2006

50. Exome sequencing identifiesMUTYHmutations in a family with colorectal cancer and an atypical phenotype

Author

Seguí, Nuria, primary, Navarro, Matilde, additional, Pineda, Marta, additional, Köger, Nicole, additional, Bellido, Fernando, additional, González, Sara, additional, Campos, Olga, additional, Iglesias, Silvia, additional, Valdés-Mas, Rafael, additional, López-Doriga, Adriana, additional, Gut, Marta, additional, Blanco, Ignacio, additional, Lázaro, Conxi, additional, Capellá, Gabriel, additional, Puente, Xose S, additional, Plotz, Guido, additional, and Valle, Laura, additional

Published
2014
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