Your search keyword '"Martina Schnölzer"' showing total 231 results

1. PFKFB4 interacts with FBXO28 to promote HIF-1α signaling in glioblastoma

Author

Emma Phillips, Jörg Balss, Frederic Bethke, Stefan Pusch, Stefan Christen, Thomas Hielscher, Martina Schnölzer, Michael N. C. Fletcher, Antje Habel, Claudia Tessmer, Lisa-Marie Brenner, Mona Göttmann, David Capper, Christel Herold-Mende, Andreas von Deimling, Sarah-Maria Fendt, and Violaine Goidts

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Glioblastoma is a highly aggressive brain tumor for which there is no cure. The metabolic enzyme 6-Phosphofructo-2-Kinase/Fructose-2,6-Biphosphatase 4 (PFKFB4) is essential for glioblastoma stem-like cell (GSC) survival but its mode of action is unclear. Understanding the role of PFKFB4 in tumor cell survival could allow it to be leveraged in a cancer therapy. Here, we show the importance of PFKFB4 for glioblastoma growth in vivo in an orthotopic patient derived mouse model. In an evaluation of patient tumor samples of different cancer entities, PFKFB4 protein was found to be overexpressed in prostate, lung, colon, mammary and squamous cell carcinoma, with expression level correlating with tumor grade. Gene expression profiling in PFKFB4-silenced GSCs revealed a downregulation of hypoxia related genes and Western blot analysis confirmed a dramatic reduction of HIF (hypoxia inducible factor) protein levels. Through mass spectrometric analysis of immunoprecipitated PFKFB4, we identified the ubiquitin E3 ligase, F-box only protein 28 (FBXO28), as a new interaction partner of PFKFB4. We show that PFKFB4 regulates the ubiquitylation and subsequent proteasomal degradation of HIF-1α, which is mediated by the ubiquitin ligase activity of FBXO28. This newly discovered function of PFKFB4, coupled with its cancer specificity, provides a new strategy for inhibiting HIF-1α in cancer cells.

Published

2022

2. The Wnt-specific astacin proteinase HAS-7 restricts head organizer formation in Hydra

Author

Berenice Ziegler, Irene Yiallouros, Benjamin Trageser, Sumit Kumar, Moritz Mercker, Svenja Kling, Maike Fath, Uwe Warnken, Martina Schnölzer, Thomas W. Holstein, Markus Hartl, Anna Marciniak-Czochra, Jörg Stetefeld, Walter Stöcker, and Suat Özbek

Subjects

Hydra, Wnt signaling, Proteinase, Astacin, Axis formation, Biology (General), QH301-705.5

Abstract

Abstract Background The Hydra head organizer acts as a signaling center that initiates and maintains the primary body axis in steady state polyps and during budding or regeneration. Wnt/beta-Catenin signaling functions as a primary cue controlling this process, but how Wnt ligand activity is locally restricted at the protein level is poorly understood. Here we report a proteomic analysis of Hydra head tissue leading to the identification of an astacin family proteinase as a Wnt processing factor. Results Hydra astacin-7 (HAS-7) is expressed from gland cells as an apical-distal gradient in the body column, peaking close beneath the tentacle zone. HAS-7 siRNA knockdown abrogates HyWnt3 proteolysis in the head tissue and induces a robust double axis phenotype, which is rescued by simultaneous HyWnt3 knockdown. Accordingly, double axes are also observed in conditions of increased Wnt activity as in transgenic actin::HyWnt3 and HyDkk1/2/4 siRNA treated animals. HyWnt3-induced double axes in Xenopus embryos could be rescued by coinjection of HAS-7 mRNA. Mathematical modelling combined with experimental promotor analysis indicate an indirect regulation of HAS-7 by beta-Catenin, expanding the classical Turing-type activator-inhibitor model. Conclusions We show the astacin family protease HAS-7 maintains a single head organizer through proteolysis of HyWnt3. Our data suggest a negative regulatory function of Wnt processing astacin proteinases in the global patterning of the oral-aboral axis in Hydra.

Published

2021

3. TGFBR2-dependent alterations of exosomal cargo and functions in DNA mismatch repair-deficient HCT116 colorectal cancer cells

Author

Fabia Fricke, Jennifer Lee, Malwina Michalak, Uwe Warnken, Ingrid Hausser, Meggy Suarez-Carmona, Niels Halama, Martina Schnölzer, Jürgen Kopitz, and Johannes Gebert

Subjects

Exosomes, Intercellular communication, Proteomics, Transforming Growth Factor Beta Receptor Type 2, DNA mismatch repair deficiency, Microsatellite instability, Medicine, Cytology, QH573-671

Abstract

Abstract Background Colorectal cancers (CRCs) that lack DNA mismatch repair function exhibit the microsatellite unstable (MSI) phenotype and are characterized by the accumulation of frameshift mutations at short repetitive DNA sequences (microsatellites). These tumors recurrently show inactivating frameshift mutations in the tumor suppressor Transforming Growth Factor Beta Receptor Type 2 (TGFBR2) thereby abrogating downstream signaling. How altered TGFBR2 signaling affects exosome-mediated communication between MSI tumor cells and their environment has not been resolved. Here, we report on molecular alterations of exosomes shed by MSI cells and the biological response evoked in recipient cells. Methods Exosomes were isolated and characterized by electron microscopy, nanoparticle tracking, and western blot analysis. TGFBR2-dependent effects on the cargo and functions of exosomes were studied in a MSI CRC model cell line enabling reconstituted and inducible TGFBR2 expression and signaling. Microsatellite frameshift mutations in exosomal and cellular DNA were examined by PCR-based DNA fragment analysis and exosomal protein profiles were identified by mass spectrometry. Uptake of fluorescent-labeled exosomes by hepatoma recipient cells was monitored by confocal microscopy. TGFBR2-dependent exosomal effects on secreted cytokine levels of recipient cells were analyzed by Luminex technology and ELISA. Results Frameshift mutation patterns in microsatellite stretches of TGFBR2 and other MSI target genes were found to be reflected in the cargo of MSI CRC-derived exosomes. At the proteome level, reconstituted TGFBR2 expression and signaling uncovered two protein subsets exclusively occurring in exosomes derived from TGFBR2-deficient (14 proteins) or TGFBR2-proficient (five proteins) MSI donor cells. Uptake of these exosomes by recipient cells caused increased secretion (2–6 fold) of specific cytokines (Interleukin-4, Stem Cell Factor, Platelet-derived Growth Factor-B), depending on the TGFBR2 expression status of the tumor cell. Conclusion Our results indicate that the coding MSI phenotype of DNA mismatch repair-deficient CRC cells is maintained in their exosomal DNA. Moreover, we uncovered that a recurrent MSI tumor driver mutation like TGFBR2 can reprogram the protein content of MSI cell-derived exosomes and in turn modulate the cytokine secretion profile of recipient cells. Apart from its diagnostic potential, these TGFBR2-dependent exosomal molecular and proteomic signatures might help to understand the signaling routes used by MSI tumors. Graphical Abstract Fricke et al. uncovered coding microsatellite instability-associated mutations of colorectal tumor driver genes like TGFBR2 in MSI tumor cellderived exosomes. Depending on the TGFBR2 expression status of their donor cells, shed exosomes show distinct proteomic signatures and promote altered cytokine secretion profiles in recipient cells.

Published

2017

4. Immunoregulatory Effects of Myeloid-Derived Suppressor Cell Exosomes in Mouse Model of Autoimmune Alopecia Areata

Author

Margot Zöller, Kun Zhao, Natalia Kutlu, Nathalie Bauer, Jan Provaznik, Thilo Hackert, and Martina Schnölzer

Subjects

myeloid-derived suppressor cells, exosomes, alopecia areata, therapy, regulatory T cells, Immunologic diseases. Allergy, RC581-607

Abstract

The treatment of autoimmune diseases still poses a major challenge, frequently relying on non-specific immunosuppressive drugs. Current efforts aim at reestablishing self tolerance using immune cells with suppressive activity like the regulatory T cells (Treg) or the myeloid-derived suppressor cells (MDSC). We have demonstrated therapeutic efficacy of MDSC in mouse Alopecia Areata (AA). In the same AA model, we now asked whether MDSC exosomes (MDSC-Exo) can replace MDSC. MDSC-Exo from bone marrow cells (BMC) cultures of healthy donors could substantially facilitate treatment. With knowledge on MDSC-Exo being limited, their suitability needs to be verified in advance. Protein marker profiles suggest comparability of BMC- to ex vivo collected inflammatory MDSC/MDSC-Exo in mice with a chronic contact dermatitis, which is a therapeutic option in AA. Proteome analyses substantiated a large overlap of function-relevant molecules in MDSC and MDSC-Exo. Furthermore, MDSC-Exo are taken up by T cells, macrophages, NK, and most avidly by Treg and MDSC-Exo uptake exceeds binding of MDSC themselves. In AA mice, MDSC-Exo preferentially target skin-draining lymph nodes and cells in the vicinity of remnant hair follicles. MDSC-Exo uptake is accompanied by a strong increase in Treg, reduced T helper proliferation, mitigated cytotoxic activity, and a slight increase in lymphocyte apoptosis. Repeated MDSC-Exo application in florid AA prevented progression and sufficed for partial hair regrowth. Deep sequencing of lymphocyte mRNA from these mice revealed a significant increase in immunoregulatory mRNA, including FoxP3 and arginase 1. Downregulated mRNA was preferentially engaged in prohibiting T cell hyperreactivity. Taken together, proteome analysis provided important insights into potential MDSC-Exo activities, these Exo preferentially homing into AA-affected organs. Most importantly, changes in leukocyte mRNA seen after treatment of AA mice with MDSC-Exo sustainably supports the strong impact on the adaptive and the non-adaptive immune system, with Treg expansion being a dominant feature. Thus, MDSC-Exo could potentially serve as therapeutic agents in treating AA and other autoimmune diseases.

Published

2018

5. Synergistic combination of valproic acid and oncolytic parvovirus H‐1PV as a potential therapy against cervical and pancreatic carcinomas

Author

Junwei Li, Serena Bonifati, Georgi Hristov, Tiina Marttila, Séverine Valmary‐Degano, Sven Stanzel, Martina Schnölzer, Christiane Mougin, Marc Aprahamian, Svitlana P. Grekova, Zahari Raykov, Jean Rommelaere, and Antonio Marchini

Subjects

H‐1PV, pancreatic ductal adenocarcinomas, parvovirus NS1 protein, valproic acid, viral oncotherapy, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract The rat parvovirus H‐1PV has oncolytic and tumour‐suppressive properties potentially exploitable in cancer therapy. This possibility is being explored and results are encouraging, but it is necessary to improve the oncotoxicity of the virus. Here we show that this can be achieved by co‐treating cancer cells with H‐1PV and histone deacetylase inhibitors (HDACIs) such as valproic acid (VPA). We demonstrate that these agents act synergistically to kill a range of human cervical carcinoma and pancreatic carcinoma cell lines by inducing oxidative stress, DNA damage and apoptosis. Strikingly, in rat and mouse xenograft models, H‐1PV/VPA co‐treatment strongly inhibits tumour growth promoting complete tumour remission in all co‐treated animals. At the molecular level, we found acetylation of the parvovirus nonstructural protein NS1 at residues K85 and K257 to modulate NS1‐mediated transcription and cytotoxicity, both of which are enhanced by VPA treatment. These results warrant clinical evaluation of H‐1PV/VPA co‐treatment against cervical and pancreatic ductal carcinomas.

Published

2013

6. Quantification of High-Molecular Weight Protein Platforms by AQUA Mass Spectrometry as Exemplified for the CD95 Death-Inducing Signaling Complex (DISC)

Author

Inna Lavrik, Uwe Warnken, Kolja Schleich, and Martina Schnölzer

Subjects

CD95, DISC, apoptosis, DED, protein quantification, mass spectrometry, AQUA technique, protein platforms, Cytology, QH573-671

Abstract

Contemporary quantitative mass spectrometry provides fascinating opportunities in defining the stoichiometry of high-molecular weight complexes or multiprotein platforms. The composition stoichiometry of multiprotein platforms is a key to understand the regulation of complex signaling pathways and provides a basis for constructing models in systems biology. Here we present an improved AQUA technique workflow that we adapted for the quantitative mass spectrometry analysis of the stoichiometry of the CD95 (Fas/APO-1) death inducing signaling complex (DISC). The DISC is a high-molecular weight platform essential for the initiation of CD95-mediated apoptotic and non-apoptotic responses. For protein quantification, CD95 DISCs were immunoprecipitated and proteins in the immunoprecipitations were separated by one-dimensional gel electrophoresis, followed by protein quantification using the AQUA technique. We will discuss in detail AQUA analysis of the CD95 DISC focusing on the key issues of this methodology, i.e., selection and validation of AQUA peptides. The application of this powerful method allowed getting new insights into mechanisms of procaspase-8 activation at the DISC and apoptosis initiation [1]. Here we discuss the AQUA methodology adapted by us for the analysis of the CD95 DISC in more detail. This approach paves the way for the successful quantification of multiprotein complexes and thereby delineating the intrinsic details of molecular interactions.

Published

2013

7. Transcriptome Analysis in Tardigrade Species Reveals Specific Molecular Pathways for Stress Adaptations

Author

Frank Förster, Daniela Beisser, Markus A. Grohme, Chunguang Liang, Brahim Mali, Alexander Matthias Siegl, Julia C. Engelmann, Alexander V. Shkumatov, Elham Schokraie, Tobias Müller, Martina Schnölzer, Ralph O. Schill, Marcus Frohme, and Thomas Dandekar

Subjects

Biology (General), QH301-705.5

Published

2012

8. Subcellular protein extraction from human pancreatic cancer tissues

Author

Anette Börner, Uwe Warnken, Martina Schnölzer, Jörg von Hagen, Nathalia Giese, Andrea Bauer, and Jörg D. Hoheisel

Subjects

cancer, disease, pancreas, protein extraction, protein fractionation, Biology (General), QH301-705.5

Abstract

Proteins are the major class of effector molecules in cellular systems. For the identification of functional differences between normal and diseased tissues, a reliable analysis of their protein content is essential. Reproducible isolation and fractionation of intact proteins are important in this respect, but their complexity in structure and concentration, their close interaction, and their instability represent major challenges. For protein isolation in tissues, the breakdown of cell-cell and cell-matrix connections within a tissue without affecting protein quality is a critical factor. We compared different processes for a compartmental protein preparation from pancreatic tissue, one of the most challenging tissues for protein isolation because of its high protease content. Success of the different procedures varied greatly. Based on a scheme of tissue-slicing and subsequent cell isolation, we established a reliable workflow for the fractional extraction of cytosolic proteins, membrane and organelle proteins, nuclear proteins, and cytoskeletal filaments. The tissue slices also allow for a representative confirmation of individual samples' cellular status by histochemical processes, and a proper separation or mixing of cellular material from across a tumor if required.

Published

2009

9. Genes and Proteins Differentially Expressed during In Vitro Malignant Transformation of Bovine Pancreatic Duct Cells

Author

R. Jesnowski, Dmitri Zubakov, Ralf Faissner, Jörg Ringel, Jörg D. Hoheisel, Ralf Lösel, Martina Schnölzer, and Matthias Löhr

Subjects

Transcriptomics, proteomics, ki-ras, SV40 large T pancreatic carcinogenesis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Pancreatic carcinoma has an extremely bad prognosis due to lack of early diagnostic markers and lack of effective therapeutic strategies. Recently, we have established an in vitro model recapitulating the first steps in the carcinogenesis of the pancreas. SV40 large T antigen-immortalized bovine pancreatic duct cells formed intrapancreatic adenocarcinoma tumors on k-rasmut transfection after orthotopic injection in the nude mouse pancreas. Here we identified genes and proteins differentially expressed in the course of malignant transformation using reciprocal suppression subtractive hybridization and 2D gel electrophoresis and mass spectrometry, respectively. We identified 34 differentially expressed genes, expressed sequence tags, and 15 unique proteins. Differential expression was verified for some of the genes or proteins in samples from pancreatic carcinoma. Among these genes and proteins, the majority had already been described either to be influenced by a mutated ras or to be differentially expressed in pancreatic adenocarcinoma, thus proving the feasibility of our model. Other genes and proteins (e.g., BBC1, GLTSCR2, and rhoGDlα), up to now, have not been implicated in pancreatic tumor development. Thus, we were able to establish an in vitro model of pancreatic carcinogenesis, which enabled us to identify genes and proteins differentially expressed during the early steps of malignant transformation.

Published

2007

10. Reconstitution of TGFBR2-Mediated Signaling Causes Upregulation of GDF-15 in HCT116 Colorectal Cancer Cells.

Author

Jennifer Lee, Fabia Fricke, Uwe Warnken, Martina Schnölzer, Jürgen Kopitz, and Johannes Gebert

Subjects

Medicine, Science

Abstract

Although inactivating frameshift mutations in the Transforming growth factor beta receptor type 2 (TGFBR2) gene are considered as drivers of microsatellite unstable (MSI) colorectal tumorigenesis, consequential alterations of the downstream target proteome are not resolved completely. Applying a click-it chemistry protein labeling approach combined with mass spectrometry in a MSI colorectal cancer model cell line, we identified 21 de novo synthesized proteins differentially expressed upon reconstituted TGFBR2 expression. One candidate gene, the TGF-ß family member Growth differentiation factor-15 (GDF-15), exhibited TGFBR2-dependent transcriptional upregulation causing increased intracellular and extracellular protein levels. As a new TGFBR2 target gene it may provide a link between the TGF-ß branch and the BMP/GDF branch of SMAD-mediated signaling.

Published

2015

11. A soluble form of the giant cadherin Fat1 is released from pancreatic cancer cells by ADAM10 mediated ectodomain shedding.

Author

Nathalie Wojtalewicz, Elham Sadeqzadeh, Jakob V Weiß, Mahnaz Moradian Tehrani, Susanne Klein-Scory, Stephan Hahn, Wolff Schmiegel, Uwe Warnken, Martina Schnölzer, Charles E de Bock, Rick F Thorne, and Irmgard Schwarte-Waldhoff

Subjects

Medicine, Science

Abstract

In pancreatic cancer, there is a clear unmet need to identify new serum markers for either early diagnosis, therapeutic stratification or patient monitoring. Proteomic analysis of tumor cell secretomes is a promising approach to indicate proteins released from tumor cells in vitro. Ectodomain shedding of transmembrane proteins has previously been shown to contribute significant fractions the tumor cell secretomes and to generate valuable serum biomarkers. Here we introduce a soluble form of the giant cadherin Fat1 as a novel biomarker candidate. Fat1 expression and proteolytic processing was analyzed by mass spectrometry and Western blotting using pancreatic cancer cell lines as compared to human pancreatic ductal epithelial cells. RNA expression in cancer tissues was assessed by in silico analysis of publically available microarray data. Involvement of ADAM10 (A Disintegrin and metalloproteinase domain-containing protein 10) in Fat1 ectodomain shedding was analyzed by chemical inhibition and knockdown experiments. A sandwich ELISA was developed to determine levels of soluble Fat1 in serum samples. In the present report we describe the release of high levels of the ectodomain of Fat1 cadherin into the secretomes of human pancreatic cancer cells in vitro, a process that is mediated by ADAM10. We confirm the full-length and processed heterodimeric form of Fat1 expressed on the plasma membrane and also show the p60 C-terminal transmembrane remnant fragment corresponding to the shed ectodomain. Fat1 and its sheddase ADAM10 are overexpressed in pancreatic adenocarcinomas and ectodomain shedding is also recapitulated in vivo leading to increased Fat1 serum levels in some pancreatic cancer patients. We suggest that soluble Fat1 may find an application as a marker for patient monitoring complementing carbohydrate antigen 19-9 (CA19-9). In addition, detailed analysis of the diverse processed protein isoforms of the candidate tumor suppressor Fat1 can also contribute to our understanding of cell biology and tumor behavior.

Published

2014

12. Serum protein signatures differentiating autoimmune pancreatitis versus pancreatic cancer.

Author

Klaus Felix, Oliver Hauck, Stefan Fritz, Ulf Hinz, Martina Schnölzer, Tore Kempf, Uwe Warnken, Angelika Michel, Michael Pawlita, and Jens Werner

Subjects

Medicine, Science

Abstract

Autoimmune pancreatitis (AIP) is defined by characteristic lymphoplasmacytic infiltrate, ductal strictures and a pancreatic enlargement or mass that can mimic pancreatic cancer (PaCa). The distinction between this benign disease and pancreatic cancer can be challenging. However, an accurate diagnosis may pre-empt the misdiagnosis of cancer, allowing the appropriate medical treatment of AIP and, consequently, decreasing the number of unnecessary pancreatic resections. Mass spectrometry (MS) and two-dimensional differential gel electrophoresis (2D-DIGE) have been applied to analyse serum protein alterations associated with AIP and PaCa, and to identify protein signatures indicative of the diseases. Patients' sera were immunodepleted from the 20 most prominent serum proteins prior to further 2D-DIGE and image analysis. The identity of the most-discriminatory proteins detected, was performed by MS and ELISAs were applied to confirm their expression. Serum profiling data analysis with 2D-DIGE revealed 39 protein peaks able to discriminate between AIP and PaCa. Proteins were purified and further analysed by MALDI-TOF-MS. Peptide mass fingerprinting led to identification of eleven proteins. Among them apolipoprotein A-I, apolipoprotein A-II, transthyretin, and tetranectin were identified and found as 3.0-, 3.5-, 2-, and 1.6-fold decreased in PaCa sera, respectively, whereas haptoglobin and apolipoprotein E were found to be 3.8- and 1.6-fold elevated in PaCa sera. With the exception of haptoglobin the ELISA results of the identified proteins confirmed the 2D-DIGE image analysis characteristics. Integration of the identified serum proteins as AIP markers may have considerable potential to provide additional information for the diagnosis of AIP to choose the appropriate treatment.

Published

2013

13. Annexin A1 on the surface of early apoptotic cells suppresses CD8+ T cell immunity.

Author

Heiko Weyd, Lucie Abeler-Dörner, Björn Linke, Andrea Mahr, Veronika Jahndel, Sandra Pfrang, Martina Schnölzer, Christine S Falk, and Peter H Krammer

Subjects

Medicine, Science

Abstract

Prevention of an immune response against self-antigens derived from apoptotic cells is essential to preclude autoimmune and chronic inflammatory diseases. Here, we describe apoptosis induced externalization of endogenous cytosolic annexin 1 initiating an anti-inflammatory effector mechanism that suppresses the immune response against antigens of apoptotic cells. Cytosolic annexin 1 rapidly translocated to the apoptotic cell surface and inhibited dendritic cell (DC) activation induced by Toll like receptors (TLR). Annexin 1-inhibited DC showed strongly reduced secretion of pro-inflammatory cytokines (e.g. TNF and IL-12) and costimulatory surface molecules (e.g. CD40 and CD86), while anti-inflammatory mediators like PD-L1 remained unchanged. T cells stimulated by such DC lacked secretion of interferon-γ (IFN-γ) and TNF but retained IL-10 secretion. In mice, annexin 1 prevented the development of inflammatory DC and suppressed the cellular immune response against the model antigen ovalbumin (OVA) expressed in apoptotic cells. Furthermore, annexin 1 on apoptotic cells compromised OVA-specific tumor vaccination and impaired rejection of an OVA-expressing tumor. Thus, our results provide a molecular mechanism for the suppressive activity of apoptotic cells on the immune response towards apoptotic cell-derived self-antigens. This process may play an important role in prevention of autoimmune diseases and of the immune response against cancer.

Published

2013

14. Comparative proteome analysis of Milnesium tardigradum in early embryonic state versus adults in active and anhydrobiotic state.

Author

Elham Schokraie, Uwe Warnken, Agnes Hotz-Wagenblatt, Markus A Grohme, Steffen Hengherr, Frank Förster, Ralph O Schill, Marcus Frohme, Thomas Dandekar, and Martina Schnölzer

Subjects

Medicine, Science

Abstract

Tardigrades have fascinated researchers for more than 300 years because of their extraordinary capability to undergo cryptobiosis and survive extreme environmental conditions. However, the survival mechanisms of tardigrades are still poorly understood mainly due to the absence of detailed knowledge about the proteome and genome of these organisms. Our study was intended to provide a basis for the functional characterization of expressed proteins in different states of tardigrades. High-throughput, high-accuracy proteomics in combination with a newly developed tardigrade specific protein database resulted in the identification of more than 3000 proteins in three different states: early embryonic state and adult animals in active and anhydrobiotic state. This comprehensive proteome resource includes protein families such as chaperones, antioxidants, ribosomal proteins, cytoskeletal proteins, transporters, protein channels, nutrient reservoirs, and developmental proteins. A comparative analysis of protein families in the different states was performed by calculating the exponentially modified protein abundance index which classifies proteins in major and minor components. This is the first step to analyzing the proteins involved in early embryonic development, and furthermore proteins which might play an important role in the transition into the anhydrobiotic state.

Published

2012

15. Quantitative proteomics identify novel miR-155 target proteins.

Author

Christopher Lössner, Jan Meier, Uwe Warnken, Michael A Rogers, Peter Lichter, Armin Pscherer, and Martina Schnölzer

Subjects

Medicine, Science

Abstract

BACKGROUND: MicroRNAs are 22 nucleotides long non-coding RNAs and exert their function either by transcriptional or translational inhibition. Although many microRNA profiles in different tissues and disease states have already been discovered, only little is known about their target proteins. The microRNA miR-155 is deregulated in many diseases, including cancer, where it might function as an oncoMir. METHODOLOGY/PRINCIPAL FINDINGS: We employed a proteomics technique called "stable isotope labelling by amino acids in cell culture" (SILAC) allowing relative quantification to reliably identify target proteins of miR-155. Using SILAC, we identified 46 putative miR-155 target proteins, some of which were previously reported. With luciferase reporter assays, CKAP5 was confirmed as a new target of miR-155. Functional annotation of miR-155 target proteins pointed to a role in cell cycle regulation. CONCLUSIONS/SIGNIFICANCE: To the best of our knowledge we have investigated for the first time miR-155 target proteins in the HEK293T cell line in large scale. In addition, by comparing our results to previously identified miR-155 target proteins in other cell lines, we provided further evidence for the cell line specificity of microRNAs.

Published

2011

16. Proteomic analysis of tardigrades: towards a better understanding of molecular mechanisms by anhydrobiotic organisms.

Author

Elham Schokraie, Agnes Hotz-Wagenblatt, Uwe Warnken, Brahim Mali, Marcus Frohme, Frank Förster, Thomas Dandekar, Steffen Hengherr, Ralph O Schill, and Martina Schnölzer

Subjects

Medicine, Science

Abstract

BackgroundTardigrades are small, multicellular invertebrates which are able to survive times of unfavourable environmental conditions using their well-known capability to undergo cryptobiosis at any stage of their life cycle. Milnesium tardigradum has become a powerful model system for the analysis of cryptobiosis. While some genetic information is already available for Milnesium tardigradum the proteome is still to be discovered.Principal findingsHere we present to the best of our knowledge the first comprehensive study of Milnesium tardigradum on the protein level. To establish a proteome reference map we developed optimized protocols for protein extraction from tardigrades in the active state and for separation of proteins by high resolution two-dimensional gel electrophoresis. Since only limited sequence information of M. tardigradum on the genome and gene expression level is available to date in public databases we initiated in parallel a tardigrade EST sequencing project to allow for protein identification by electrospray ionization tandem mass spectrometry. 271 out of 606 analyzed protein spots could be identified by searching against the publicly available NCBInr database as well as our newly established tardigrade protein database corresponding to 144 unique proteins. Another 150 spots could be identified in the tardigrade clustered EST database corresponding to 36 unique contigs and ESTs. Proteins with annotated function were further categorized in more detail by their molecular function, biological process and cellular component. For the proteins of unknown function more information could be obtained by performing a protein domain annotation analysis. Our results include proteins like protein member of different heat shock protein families and LEA group 3, which might play important roles in surviving extreme conditions.ConclusionsThe proteome reference map of Milnesium tardigradum provides the basis for further studies in order to identify and characterize the biochemical mechanisms of tolerance to extreme desiccation. The optimized proteomics workflow will enable application of sensitive quantification techniques to detect differences in protein expression, which are characteristic of the active and anhydrobiotic states of tardigrades.

Published

2010

17. Suppl. Figure 7 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

Representative multicolor stainings of CFL1, CRKII, NME2, and CNTN1 on acetone-fixed cryosections with markers for common cell types in IDHmut LGGs: anti-GFAP (tumor cells, #Z0334, DAKO), anti-CD68 (microglia/ macrophages, #M0718, DAKO), anti-CD31 (endothelial cells, #223609, BD Pharmingen). Detection was performed by using fluorochrom-conjugated secondary antibodies (anti-mouse AF647 (#A-21463, Invitrogen), anti-rabbit AF555 (#A-21428, Invitrogen), DAPI (#D1306, ThermoFisher), and the Zenon AF488 mouse IgG1 Labeling Kit (#Z25001, ThermoFisher)) according to the manufacturer`s protocol (scale bar: 50 µM, scale bar zoom: 10 µM).

Published

2023

18. Suppl. Figure 5 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

Representative images of immunohistochemical stainings of the isotype controls IgG and IgG1 in normal brain (NB) tissues, astrocytomas (WHO{degree sign}II: n = 10; WHO{degree sign}III: n = 10), and oligodendrogliomas (WHO{degree sign}II: n = 10; WHO{degree sign}III: n = 10). Scale bar: 50 µm.

Published

2023

19. Supplementary Figure 1 from Costimulatory Protein 4IgB7H3 Drives the Malignant Phenotype of Glioblastoma by Mediating Immune Escape and Invasiveness

Author

Wolfgang Wick, Michael Platten, Michael Weller, Ruxandra Tudoran, Martina Schnölzer, Uwe Warnken, Tore Kempf, Ann-Catherine Klein, Felix Sahm, Philipp-Niclas Pfenning, and Dieter Lemke

Abstract

PDF file - 4.7MB

Published

2023

20. Suppl. Figure 9 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

(A) IFN-� ELISpot raw data of all HLA-A*02:01 patients analyzed (n = 7) showing the IFN-� spots / 1x105 T-cells for patient cells against TAAs vs. patient cells against the negative control (human immunodeficiency virus (HIV) gag/pol, 9 amino acids). Grey bars indicate a significantly increased immunogenicity compared to negative control (solid line). (B) Homogenous levels of stimulation while comparing the total immune response by mean of IFN-� spot numbers among astrocytomas (red) and oligodendrogliomas (blue) to a certain reactive epitope. (n.s., not significant, *, p < 0.05; **, p < 0.01)

Published

2023

21. Suppl. Figure 2 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

IFN-� ELISpot raw data to validate antigen immunogenicity in patients of origin. Antigens with a significant increased immunogenicity (grey bars and asterisks) or 1.3-fold increased levels of immune responses (grey bars) were further validated in a bigger study sample of healthy individuals and lower-grade glioma patients. Solid line represents mean background of negative control (IgG1). (*, p < 0.05; **, p < 0.01; ***, p < 0.001)

Published

2023

22. Supplementary Figure Legends 1-4 from Costimulatory Protein 4IgB7H3 Drives the Malignant Phenotype of Glioblastoma by Mediating Immune Escape and Invasiveness

Author

Wolfgang Wick, Michael Platten, Michael Weller, Ruxandra Tudoran, Martina Schnölzer, Uwe Warnken, Tore Kempf, Ann-Catherine Klein, Felix Sahm, Philipp-Niclas Pfenning, and Dieter Lemke

Abstract

PDF file - 64K

Published

2023

23. Supplementary Figure 2 from Costimulatory Protein 4IgB7H3 Drives the Malignant Phenotype of Glioblastoma by Mediating Immune Escape and Invasiveness

Author

Wolfgang Wick, Michael Platten, Michael Weller, Ruxandra Tudoran, Martina Schnölzer, Uwe Warnken, Tore Kempf, Ann-Catherine Klein, Felix Sahm, Philipp-Niclas Pfenning, and Dieter Lemke

Abstract

PDF file - 2.0MB

Published

2023

24. Data from Costimulatory Protein 4IgB7H3 Drives the Malignant Phenotype of Glioblastoma by Mediating Immune Escape and Invasiveness

Author

Wolfgang Wick, Michael Platten, Michael Weller, Ruxandra Tudoran, Martina Schnölzer, Uwe Warnken, Tore Kempf, Ann-Catherine Klein, Felix Sahm, Philipp-Niclas Pfenning, and Dieter Lemke

Abstract

Purpose: Recent work points out a role of B7H3, a member of the B7-family of costimulatory proteins, in conveying immunosuppression and enforced invasiveness in a variety of tumor entities. Glioblastoma is armed with effective immunosuppressive properties resulting in an impaired recognition and ineffective attack of tumor cells by the immune system. In addition, extensive and diffuse invasion of tumor cells into the surrounding brain tissue limits the efficacy of local therapies. Here, 4IgB7H3 is assessed as diagnostic and therapeutic target for glioblastoma.Experimental Design: To characterize B7H3 in glioblastoma, we conduct analyses not only in glioma cell lines and glioma-initiating cells but also in human glioma tissue specimens.Results: B7H3 expression by tumor and endothelial cells correlates with the grade of malignancy in gliomas and with poor survival. Both soluble 4IgB7H3 in the supernatant of glioma cells and cell-bound 4IgB7H3 are functional and suppress natural killer cell–mediated tumor cell lysis. Gene silencing showed that membrane and soluble 4IgB7H3 convey a proinvasive phenotype in glioma cells and glioma-initiating cells in vitro. These proinvasive and immunosuppressive properties were confirmed in vivo by xenografted 4IgB7H3 gene silenced glioma-initiating cells, which invaded significantly less into the surrounding brain tissue in an orthotopic model and by subcutaneously injected LN-229 cells, which were more susceptible to natural killer cell–mediated cytotoxicity than unsilenced control cells.Conclusions: Because of its immunosuppressive and proinvasive function, 4IgB7H3 may serve as a therapeutic target in the treatment of glioblastoma. Clin Cancer Res; 18(1); 105–17. ©2011 AACR.

Published

2023

25. Data from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

Purpose: Successful immunotherapies for IDHmut gliomas require better knowledge of T-cell target antigens. Here, we elucidated their antigen repertoire recognized by spontaneous T-cell responses using an unbiased proteomic approach.Experimental Design: Protein fractionations of tissue lysates from IDHmut gliomas (n = 4) were performed. Fractions were tested by IFNγ ELISpot assay for recognition through patients' T cells. Proteins of immunogenic fractions were identified by mass spectrometry and validated by in silico-predicted synthetic long peptides in patients of origin, additional IDHmut glioma patients (n = 16), and healthy donors (n = 13). mRNA and protein expression of immunogenic antigens was analyzed in tumor tissues and IDHmut glioma stem-like cells (GSC). HLA-A*02–restricted T-cell epitopes were functionally determined by short peptides and numbers of antigen-specific T cells by HLA-peptide tetramer analysis.Results: A total of 2,897 proteins were identified in immunogenic tumor fractions. Based on a thorough filter process, 79 proteins were selected as potential T-cell antigens. Twenty-six of these were recognized by the patients’ T cells, and five of them (CRKII, CFL1, CNTN1, NME2, and TKT) in up to 56% unrelated IDHmut glioma patients. Most immunogenic tumor-associated antigens (TAA) were expressed in IDHmut gliomas and GSCs, while being almost absent in normal brain tissues. Finally, we identified HLA-A*02–restricted epitopes for CRKII, NME2, and TKT that were recognized by up to 2.82% of antigen-specific peripheral cytotoxic T cells in IDHmut glioma patients.Conclusions: By analyzing the repertoire of T-cell target antigens in IDHmut glioma patients, we identified five novel immunogenic TAAs and confirmed their expression on IDHmut tumors and GSCs. Clin Cancer Res; 24(12); 2951–62. ©2018 AACR.

Published

2023

26. Suppl. Figure 10 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

(A) Applied gating strategy (one representative patient, NCH645) for the expression analysis of tumor-associated antigens in IDHmut lower-grade glioma and secondary glioblastoma GSCs, analyzed by flow cytometry in regard to an adequate isotype control. (B) Fluorescence intensity measurements for the isotype control and the antigen expressing (positive) GSC population, showing counts in percentage [%] over the mean PE-intensity.(C) Gating strategy, including the markers pacific orange (PO), CD3, and CD8, used for quantification of antigen-specific peripheral cytotoxic CD3+CD8+ T-cells by flow cytometry and (D) antigen-loaded pMHC I-tetramers (PE-conjugated) and the respective positive (Influenza M1) as well as negative control HLA-A*02-tetramers. GSCs: glioma stem-like cells, HIV: human immunodeficiency virus, HLA: human leukocyte antigen, MHC: major histocompatibility complex, PE: Phycoerythrin, pos: positive, US: unstained.

Published

2023

27. Supplementary Figure 4 from Costimulatory Protein 4IgB7H3 Drives the Malignant Phenotype of Glioblastoma by Mediating Immune Escape and Invasiveness

Author

Wolfgang Wick, Michael Platten, Michael Weller, Ruxandra Tudoran, Martina Schnölzer, Uwe Warnken, Tore Kempf, Ann-Catherine Klein, Felix Sahm, Philipp-Niclas Pfenning, and Dieter Lemke

Abstract

PDF file - 698K

Published

2023

28. Suppl. Table 2 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

Peptide information of potential T cell target antigens, tested by IFN-γ ELISpot

Published

2023

29. Suppl. Table 1, 3-8 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

Clinical data of IDHmut LGG patients

Published

2023

30. Suppl. Figure 8 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

Usage of RNA Seq TCGA data of IDHmut LGG tumors to compare mRNA expression levels with T-cell infiltration. Significant increased expression of NME2 in the TCGA IDHmut LGG dataset was shown to be positively correlated with the expression of CD3E (encoding CD3-ε as part of the CD3 T-cell receptor complex) (r = 0.2352). Stronger correlation in the histology of astrocytomas (r = 0.3693**) than in oligodendrogliomas (r = 0.1919**). (*, p < 0.05; **, p < 0.01; ***, p < 0.001)

Published

2023

31. Suppl. Figure 6 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

(A) Semi-quantitative evaluation on immunohistochemically stained sections of the frequency of tumor cells expressing the potential T-cell target antigens CRKII, CFL1, NME2, and CNTN1 in astrocytoma (WHO{degree sign}II: n = 10, WHO{degree sign}III: n = 10) and (B) oligodendroglioma (WHO{degree sign}II: n = 10, WHO{degree sign}III: n = 10) tumor tissues.

Published

2023

32. Suppl. Figure 3 from Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Christel Herold-Mende, Philipp Beckhove, Andreas Unterberg, Andreas von Deimling, Markus A. Weigand, Christoph Schramm, Niels Grabe, Volker Eckstein, Uwe Warnken, Christine Jungk, Saskia Roesch, Kolja Pocha, David Reuss, Anchana Rathinasamy, Carmen Rapp, Martina Schnölzer, Rolf Warta, Slava Stamova, and Steffen Dettling

Abstract

(A) Significantly increased immune responses in IDHmut lower-grade glioma patients (P) vs. healthy donors (HD) seen for the potential T-cell target antigens CRKII, CFL1, CNTN1, NME2, and TKT. Homogenous levels of stimulation while comparing IFN-� spot numbers among astrocytomas (red) and oligodendrogliomas (blue) to a certain TAA as well as (B) the total immune response. (C) IFN-� ELISpot raw data showing the spot count / 1x105 T-cells upon stimulation with autologous dendritic cells loaded with antigens (CRKII, CFL1, CNTN1, NME2, or TKT, black bar) vs. negative control (IgG1, grey bar) for each patient (P) (n = 16). Highlighted in green: significant immune responses (p < 0.05) with an > 2-fold increased spot count compared to the negative control (IgG) (*, p < 0.05; **, p < 0.01; ***, p < 0.001)

Published

2023

33. PFKFB4 interacts with FBXO28 to promote HIF-1 alpha signaling in glioblastoma

Author

Emma Phillips, Jörg Balss, Frederic Bethke, Stefan Pusch, Stefan Christen, Thomas Hielscher, Martina Schnölzer, Michael N. C. Fletcher, Antje Habel, Claudia Tessmer, Lisa-Marie Brenner, Mona Göttmann, David Capper, Christel Herold-Mende, Andreas von Deimling, Sarah-Maria Fendt, and Violaine Goidts

Subjects

HYPOXIA INDUCIBLE FACTOR-1-ALPHA, EXPRESSION, Cancer Research, Science & Technology, FRUCTOSE-2,6-BISPHOSPHATE, IDENTIFICATION, CANCER STEM-CELL, DEGRADATION, HIF-2-ALPHA, BREAST, TUMOR ANGIOGENESIS, PATHWAY, Oncology, Molecular Biology, Life Sciences & Biomedicine

Abstract

Glioblastoma is a highly aggressive brain tumor for which there is no cure. The metabolic enzyme 6-Phosphofructo-2-Kinase/Fructose-2,6-Biphosphatase 4 (PFKFB4) is essential for glioblastoma stem-like cell (GSC) survival but its mode of action is unclear. Understanding the role of PFKFB4 in tumor cell survival could allow it to be leveraged in a cancer therapy. Here, we show the importance of PFKFB4 for glioblastoma growth in vivo in an orthotopic patient derived mouse model. In an evaluation of patient tumor samples of different cancer entities, PFKFB4 protein was found to be overexpressed in prostate, lung, colon, mammary and squamous cell carcinoma, with expression level correlating with tumor grade. Gene expression profiling in PFKFB4-silenced GSCs revealed a downregulation of hypoxia related genes and Western blot analysis confirmed a dramatic reduction of HIF (hypoxia inducible factor) protein levels. Through mass spectrometric analysis of immunoprecipitated PFKFB4, we identified the ubiquitin E3 ligase, F-box only protein 28 (FBXO28), as a new interaction partner of PFKFB4. We show that PFKFB4 regulates the ubiquitylation and subsequent proteasomal degradation of HIF-1α, which is mediated by the ubiquitin ligase activity of FBXO28. This newly discovered function of PFKFB4, coupled with its cancer specificity, provides a new strategy for inhibiting HIF-1α in cancer cells. ispartof: ONCOGENESIS vol:11 issue:1 ispartof: location:United States status: published

Published

2022

34. The Wnt-specific astacin proteinase HAS-7 restricts head organizer formation in Hydra

Author

Sumit Kumar, Berenice Ziegler, Markus Hartl, Walter Stöcker, Irene Yiallouros, Jörg Stetefeld, Suat Özbek, Maike Fath, Anna Marciniak-Czochra, Uwe Warnken, Benjamin Trageser, Moritz Mercker, Thomas W. Holstein, Svenja Kling, Martina Schnölzer, and University of Manitoba

Subjects

Proteomics, Physiology, Hydra, QH301-705.5, Xenopus, Plant Science, Proteinase, General Biochemistry, Genetics and Molecular Biology, Structural Biology, Astacin, Axis formation, Animals, RNA, Small Interfering, Biology (General), Wnt Signaling Pathway, Ecology, Evolution, Behavior and Systematics, Actin, beta Catenin, Body Patterning, Gene knockdown, Budding, biology, Regeneration (biology), Wnt signaling pathway, Metalloendopeptidases, Cell Biology, biology.organism_classification, Wnt signaling, Cell biology, Wnt Proteins, Proteolysis, Lernaean Hydra, General Agricultural and Biological Sciences, Head, Developmental Biology, Biotechnology, Research Article

Abstract

Background The Hydra head organizer acts as a signaling center that initiates and maintains the primary body axis in steady state polyps and during budding or regeneration. Wnt/beta-Catenin signaling functions as a primary cue controlling this process, but how Wnt ligand activity is locally restricted at the protein level is poorly understood. Here we report a proteomic analysis of Hydra head tissue leading to the identification of an astacin family proteinase as a Wnt processing factor. Results Hydra astacin-7 (HAS-7) is expressed from gland cells as an apical-distal gradient in the body column, peaking close beneath the tentacle zone. HAS-7 siRNA knockdown abrogates HyWnt3 proteolysis in the head tissue and induces a robust double axis phenotype, which is rescued by simultaneous HyWnt3 knockdown. Accordingly, double axes are also observed in conditions of increased Wnt activity as in transgenic actin::HyWnt3 and HyDkk1/2/4 siRNA treated animals. HyWnt3-induced double axes in Xenopus embryos could be rescued by coinjection of HAS-7 mRNA. Mathematical modelling combined with experimental promotor analysis indicate an indirect regulation of HAS-7 by beta-Catenin, expanding the classical Turing-type activator-inhibitor model. Conclusions We show the astacin family protease HAS-7 maintains a single head organizer through proteolysis of HyWnt3. Our data suggest a negative regulatory function of Wnt processing astacin proteinases in the global patterning of the oral-aboral axis in Hydra.

Published

2021

35. AAMP is a binding partner of costimulatory human B7-H3

Author

Sara Ciprut, Anne Berberich, Maximilian Knoll, Stefan Pusch, Dirk Hoffmann, Jennifer Furkel, Aoife Ward Gahlawat, Lena Kahlert-Konzelamnn, Felix Sahm, Uwe Warnken, Martin Winter, Martina Schnölzer, Sonja Pusch, Andreas von Deimling, Amir Abdollahi, Wolfgang Wick, and Dieter Lemke

Subjects

General Medicine

Abstract

Background Targeted immunotherapies are of growing interest in the treatment of various cancers. B7 homolog 3 protein (B7-H3), a member of the co-stimulatory/-inhibitory B7-family, exerts immunosuppressive and pro-tumorigenic functions in various cancer types and is under evaluation in ongoing clinical trials. Unfortunately, interaction partner(s) remain unknown which restricts the druggability. Methods Aiming to identify potential binding partner(s) of B7-H3, a yeast two-hybrid and a mass spectrometry screen were performed. Potential candidates were evaluated by bimolecular fluorescence complementation (BiFC) assay, co-immunoprecipitation (co-IP), and functionally in a 3H-thymidine proliferation assay of Jurkat cells, a T-cell lineage cell line. Prognostic value of angio-associated migratory cell protein (AAMP) and B7-H3 expression was evaluated in isocitrate dehydrogenase 1 wildtype (IDH1wt) glioblastoma (GBM) patients from The Cancer Genome Atlas (TCGA)-GBM cohort. Results Of the screening candidates, CD164, AAMP, PTPRA, and SLAMF7 could be substantiated via BiFC. AAMP binding could be further confirmed via co-IP and on a functional level. AAMP was ubiquitously expressed in glioma cells, immune cells, and glioma tissue, but did not correlate with glioma grade. Finally, an interaction between AAMP and B7-H3 could be observed on expression level, hinting toward a combined synergistic effect. Conclusions AAMP was identified as a novel interaction partner of B7-H3, opening new possibilities to create a targeted therapy against the pro-tumorigenic costimulatory protein B7-H3.

Published

2022

36. TSC22D4 interacts with Akt1 in response to metabolic and stress signals

Author

Sevgican Demir, Gretchen Wolff, Annika Wieder, Adriano Maida, Marco Rahm, Martina Schnölzer, Stefanie Hauck, Julia Szendrödi, Stephan Herzig, and Bilgen Ekim Üstünel

Subjects

embryonic structures

Abstract

Transforming Growth Factor β 1 Stimulated Clone 22 D4 (TSC22D4) is an intrinsically disordered protein that regulates cellular and physiological processes such as cell proliferation, cellular senescence as well as hepatic glucose and lipid metabolism. The molecular mechanism of TSC22D4 action in these cellular and metabolic functions, however, remains largely elusive. Here, we identified TSC22D4 as a novel protein kinase B/Akt1 interacting protein, a critical mediator of insulin/PI3K signaling pathway implicated in diverse set of diseases including type 2 diabetes, obesity and cancer. TSC22D4 interacts with Akt1 not constitutively but rather in a regulatory manner. While glucose and insulin stimulation of cells or refeeding of mice impair the hepatic TSC22D4-Akt1 interaction, inhibition of mitochondria and oxidative stress, promote it; indicating that extra- and intra-cellular cues play a key role in controlling TSC22D4-Akt1 interaction. Our results also demonstrate that together with its dimerization domain, i.e. the TSC box, TSC22D4 requires its intrinsically disordered region (D2 domain) to interact with Akt1. To understand regulation of TSC22D4 function further, we employed tandem mass spectrometry and identified 15 novel phosphorylation sites on TSC22D4. Similar to TSC22D4-Akt1 interaction, TSC22D4 phosphorylation also responds to environmental signals such as starvation, mitochondrial inhibition and oxidative stress. Interestingly, 6 out of the 15 novel phosphorylation sites lie within the TSC22D4 D2 domain, which is required for TSC22D4-Akt1 interaction. Characterization of the regulation and function of these novel phosphorylation sites, in the future, will shed light on our understanding of the role of TSC22D4-Akt1 interaction in both cell biological and physiological functions. Overall, our findings postulate a model whereby TSC22D4 acts as an environmental sensor and interacts with Akt1 to regulate cell proliferation, cellular senescence as well as maintain metabolic homeostasis.

Published

2021

37. Chicken lens development: complete signature of expression of galectins during embryogenesis and evidence for their complex formation with α-, β-, δ-, and τ-crystallins, N-CAM, and N-cadherin obtained by affinity chromatography

Author

Herbert Kaltner, Sebastian Schmidt, Ursula Schlötzer-Schrehardt, Malwina Michalak, Fred Sinowatz, Gabriel García Caballero, Anna-Kristin Ludwig, Joachim C. Manning, Hans-Joachim Gabius, Jürgen Kopitz, and Martina Schnölzer

Subjects

0301 basic medicine, Histology, PAX6 Transcription Factor, Galectins, Blotting, Western, Chick Embryo, Ligands, Real-Time Polymerase Chain Reaction, Chromatography, Affinity, Pathology and Forensic Medicine, Protein–protein interaction, Lens protein, 03 medical and health sciences, 0302 clinical medicine, Crystallin, Lens, Crystalline, Animals, Promoter Regions, Genetic, Transcription factor, Galectin, Cadherin, Chemistry, Stem Cells, Gene Expression Regulation, Developmental, Cell Biology, Crystallins, Glycome, Cell biology, 030104 developmental biology, Microscopy, Fluorescence, Maf Transcription Factors, PAX6, 030217 neurology & neurosurgery, Protein Binding

Abstract

The emerging multifunctionality of galectins by specific protein-glycan/protein interactions explains the interest to determine their expression during embryogenesis. Complete network analysis of all seven chicken galectins (CGs) is presented in the course of differentiation of eye lens that originates from a single type of progenitor cell. It answers the questions on levels of expression and individual patterns of distribution. A qualitative difference occurs in the CG-1A/B paralogue pair, underscoring conspicuous divergence. Considering different cell phenotypes, lens fiber and also epithelial cells can both express the same CG, with developmental upregulation for CG-3 and CG-8. Except for expression of the lens-specific CG (C-GRIFIN), no other CG appeared to be controlled by the transcription factors L-Maf and Pax6. Studying presence and nature of binding partners for CGs, we tested labeled galectins in histochemistry and in ligand blotting. Mass spectrometric (glyco)protein identification after affinity chromatography prominently yielded four types of crystallins, N-CAM, and, in the cases of CG-3 and CG-8, N-cadherin. Should such pairing be functional in situ, it may be involved in tightly packing intracellular lens proteins and forming membrane contact as well as in gaining plasticity and stability of adhesion processes. The expression of CGs throughout embryogenesis is postulated to give meaning to spatiotemporal alterations in the local glycome.

Published

2019

38. Deciphering the galectin-12 protein interactome reveals a major impact of galectin-12 on glutamine anaplerosis in colon cancer cells

Author

Jürgen Kopitz, Martina Schnölzer, Eva-Maria Katzenmaier, Johannes Gebert, Uwe Warnken, and Vera Fuchs

Subjects

Amino Acid Transport System ASC, 0301 basic medicine, Colon, Immunoprecipitation, Colorectal cancer, Galectins, Glutamine, Cellular homeostasis, Apoptosis, Biology, Proteomics, Interactome, Minor Histocompatibility Antigens, 03 medical and health sciences, 0302 clinical medicine, Tumor Cells, Cultured, otorhinolaryngologic diseases, medicine, Humans, Galectin, Glutaminolysis, Cell Differentiation, Cell Biology, medicine.disease, Cell biology, stomatognathic diseases, 030104 developmental biology, 030220 oncology & carcinogenesis, Colonic Neoplasms

Abstract

Galectins are β-galactoside binding proteins which possess a variety of functions including modulation of apoptosis, growth and differentiation. Hence, alterations in the expression profile have been associated with loss of cellular homeostasis contributing to tumor growth and progression. Though galectin-12 is significantly downregulated in several tumor entities, including colon cancer, its impact on cellular homeostasis as well as galectin-12 specific binding partners have not been identified so far. We therefore established an experimental strategy which is based on reversible cross-link immunoprecipitation to capture the galectin-12 protein interactome in colon cancer cells. By applying this approach, we identified 10 novel candidates of galectin-12 interacting proteins including the neutral amino acid exchanger SLC1A5. Remarkably, we uncovered that binding of galectin-12 to SLC1A5 significantly reduced glutamine uptake in our model cell line. Consequently, utilization of glutamine carbon for biomass synthesis was profoundly affected, suggesting galectin-12 as a novel inhibitor of glutamine anaplerosis in colon cancer cells. More detailed analysis revealed that colon cancer cells can counteract galectin-12 mediated glutamine deprivation by induction of compensatory mechanisms which facilitate adaption to low-glutamine conditions and thus survival.

Published

2019

39. Distinct Origin of Claudin7 in Early Tumor Endosomes Affects Exosome Assembly

Author

Jan Provaznik, Nathalie Bauer, Thilo Hackert, Eduard Ryschich, Daisuke Kyuno, Martina Schnölzer, and Margot Zöller

Subjects

cancer-initiating cells, Endosome, gastrointestinal cancer, Cell, tumor exosomes, Biology, Exosomes, Applied Microbiology and Biotechnology, Exosome, 03 medical and health sciences, Cell Line, Tumor, medicine, Animals, Humans, Immunoprecipitation, microvesicle proteome, Molecular Biology, Ecology, Evolution, Behavior and Systematics, 030304 developmental biology, 0303 health sciences, Tight junction, Cell Membrane, Translation (biology), Cell Biology, Microvesicles, Rats, Cell biology, Claudin7, medicine.anatomical_structure, Claudins, Mutation, Proteome, Biogenesis, Research Paper, microvesicle miRNA, Signal Transduction, Developmental Biology

Abstract

Microvesicles are the body's most powerful intercellular communication system and cancer-initiating cell microvesicles (CIC-TEX) reprogram Non-CIC towards fortified malignancy. Claudin7, a CIC-biomarker in gastrointestinal tumors, is recovered in TEX. Recent evidence suggesting individual cells delivering distinct microvesicles became of particular interest for claudin7, which is part of tight junctions (TJ) and glycolipid-enriched membrane domains (GEM), GEM-located claudin7 is palmitoylated. This offered the unique possibility of exploring the contribution of a CIC marker and its origin from distinct membrane domains on CIC-TEX biogenesis and activities. Proteome and miRNA analysis of wild-type, claudin7-knockdown and a rescue with claudin7 harboring a mutated palmitoylation site (mP) of a rat pancreatic and a human colon cancer line uncovered significant, only partly overlapping contributions of palmitoylated and non-palmitoylated claudin7 to TEX composition. Palmitoylated claudin7 facilitates GEM-integrated plasma membrane and associated signaling molecule recruitment; non-palmitoylated claudin7 supports recruitment of trafficking components, proteins engaged in fatty acid metabolism and TJ proteins into TEX. Claudin7mP also assists TEX recovery of selected miRNA. Thus, distinctly located claudin7 affects CIC-TEX composition and TJ-derived cld7 might play a unique role in equipping CIC-TEX with transporters and lipid metabolism-regulating molecules, awareness of distinct TEX populations being crucial facing therapeutic translation.

Published

2019

40. Identification of CRKII, CFL1, CNTN1, NME2, and TKT as Novel and Frequent T-Cell Targets in Human IDH-Mutant Glioma

Author

Volker Eckstein, Steffen Dettling, Andreas von Deimling, Uwe Warnken, Niels Grabe, Andreas Unterberg, Rolf Warta, Philipp Beckhove, Saskia Roesch, Martina Schnölzer, Christine Jungk, Christel Herold-Mende, Markus A. Weigand, Anchana Rathinasamy, Christoph Schramm, Carmen Rapp, Slava Stamova, Kolja Pocha, and David E. Reuss

Subjects

Cofilin 1, Proteomics, 0301 basic medicine, Cancer Research, Proteome, T-Lymphocytes, T cell, Biology, Epitope, 03 medical and health sciences, Antigen, Antigens, Neoplasm, Contactin 1, Tandem Mass Spectrometry, Cell Line, Tumor, Glioma, Biomarkers, Tumor, medicine, Humans, Cytotoxic T cell, ELISPOT, Dendritic Cells, NM23 Nucleoside Diphosphate Kinases, Proto-Oncogene Proteins c-crk, medicine.disease, Immunohistochemistry, Isocitrate Dehydrogenase, 030104 developmental biology, Epitope mapping, medicine.anatomical_structure, Oncology, Mutation, Cancer research, Cytokines, Epitope Mapping, Chromatography, Liquid

Abstract

Purpose: Successful immunotherapies for IDHmut gliomas require better knowledge of T-cell target antigens. Here, we elucidated their antigen repertoire recognized by spontaneous T-cell responses using an unbiased proteomic approach. Experimental Design: Protein fractionations of tissue lysates from IDHmut gliomas (n = 4) were performed. Fractions were tested by IFNγ ELISpot assay for recognition through patients' T cells. Proteins of immunogenic fractions were identified by mass spectrometry and validated by in silico-predicted synthetic long peptides in patients of origin, additional IDHmut glioma patients (n = 16), and healthy donors (n = 13). mRNA and protein expression of immunogenic antigens was analyzed in tumor tissues and IDHmut glioma stem-like cells (GSC). HLA-A*02–restricted T-cell epitopes were functionally determined by short peptides and numbers of antigen-specific T cells by HLA-peptide tetramer analysis. Results: A total of 2,897 proteins were identified in immunogenic tumor fractions. Based on a thorough filter process, 79 proteins were selected as potential T-cell antigens. Twenty-six of these were recognized by the patients’ T cells, and five of them (CRKII, CFL1, CNTN1, NME2, and TKT) in up to 56% unrelated IDHmut glioma patients. Most immunogenic tumor-associated antigens (TAA) were expressed in IDHmut gliomas and GSCs, while being almost absent in normal brain tissues. Finally, we identified HLA-A*02–restricted epitopes for CRKII, NME2, and TKT that were recognized by up to 2.82% of antigen-specific peripheral cytotoxic T cells in IDHmut glioma patients. Conclusions: By analyzing the repertoire of T-cell target antigens in IDHmut glioma patients, we identified five novel immunogenic TAAs and confirmed their expression on IDHmut tumors and GSCs. Clin Cancer Res; 24(12); 2951–62. ©2018 AACR.

Published

2018

41. Widespread expression of perilipin 5 in normal human tissues and in diseases is restricted to distinct lipid droplet subpopulations

Author

Peter Schirmacher, Beate K. Straub, Lena Maria Pawella, Wilfried Roth, Martina Schnölzer, Merita Hashani, Gunhild Mechtersheimer, Hagen Roland Witzel, Judith Lehmann-Koch, and Jens Schumacher

Subjects

0301 basic medicine, Cell type, Histology, Ductal cells, Chemistry, Cell Biology, Mitochondrion, Pathology and Forensic Medicine, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Downregulation and upregulation, Cytoplasm, 030220 oncology & carcinogenesis, Lipid droplet, Hepatocyte, Perilipin, medicine

Abstract

Diseases associated with the accumulation of lipid droplets are increasing in western countries. Lipid droplet biogenesis, structure and degradation are regulated by proteins of the perilipin family. Perilipin 5 has been shown to regulate basal lipolysis in oxidative tissues. We examine perilipin 5 in normal human tissues and in diseases using protein biochemical and microscopic techniques. Perilipin 5 was constitutively located at small lipid droplets in skeletal myocytes, cardiomyocytes and brown adipocytes. In addition, perilipin 5 was detected in the epithelia of the gastrointestinal and urogenital tract, especially in hepatocytes, the mitochondria-rich parietal cells of the stomach, tubular kidney cells and ductal cells of the salivary gland and pancreas. Granular cytoplasmic expression, without a lipid droplet-bound localization was detected elsewhere. In cardiomyopathies, in skeletal muscle diseases and during hepatocyte steatogenesis, perilipin 5 was upregulated and localized to larger and more numerous lipid droplets. In steatotic human hepatocytes, perilipin 5 was moderately increased and colocalized with perilipins 1 and 2 but not with perilipin 3 at lipid droplets. In liver diseases implicated in alterations of mitochondria, such as mitochondriopathies, alcoholic liver disease, Wilson's disease and acute liver injury, perilipin 5 was frequently localized to small lipid droplets and less in the cytoplasm. In tumorigenesis, perilipin 5 was especially upregulated in lipo-, leio- and rhabdomyosarcoma and hepatocellular and renal cell carcinoma. In summary, our study provides evidence that perilipin 5 is not restricted to certain cell types but localizes to distinct lipid droplet subpopulations reflecting a possible function in oxidative energy supply in normal tissues and in diseases.

Published

2018

42. SIRT7-dependent deacetylation of CDK9 activates RNA polymerase II transcription

Author

Sifan Chen, Renate Voit, Fabian Poetz, Maximilian F. Blank, Martina Schnölzer, and Ingrid Grummt

Subjects

Transcriptional Activation, 0301 basic medicine, RNA polymerase II, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Genetics, Humans, RNA, Small Nucleolar, Sirtuins, Positive Transcriptional Elongation Factor B, Molecular Biology, RNA polymerase II holoenzyme, biology, General transcription factor, Ribonucleoproteins, Small Nuclear, Cyclin-Dependent Kinase 9, 030104 developmental biology, Biochemistry, 030220 oncology & carcinogenesis, Transcription preinitiation complex, biology.protein, RNA, Transcription factor II F, RNA Polymerase II, Transcription factor II E, Transcription factor II D, Transcription factor II B

Abstract

SIRT7 is an NAD+-dependent protein deacetylase that regulates cell growth and proliferation. Previous studies have shown that SIRT7 is required for RNA polymerase I (Pol I) transcription and pre-rRNA processing. Here, we took a proteomic approach to identify novel molecular targets and characterize the role of SIRT7 in non-nucleolar processes. We show that SIRT7 interacts with numerous proteins involved in transcriptional regulation and RNA metabolism, the majority of interactions requiring ongoing transcription. In addition to its role in Pol I transcription, we found that SIRT7 also regulates transcription of snoRNAs and mRNAs. Mechanistically, SIRT7 promotes the release of P-TEFb from the inactive 7SK snRNP complex and deacetylates CDK9, a subunit of the elongation factor P-TEFb, which activates transcription by phosphorylating serine 2 within the C-terminal domain (CTD) of Pol II. SIRT7 counteracts GCN5-directed acetylation of lysine 48 within the catalytic domain of CDK9, deacetylation promoting CTD phosphorylation and transcription elongation.

Published

2017

43. The Pancreatic Cancer-Initiating Cell Marker CD44v6 Affects Transcription, Translation, and Signaling: Consequences for Exosome Composition and Delivery

Author

Jan Provaznik, Hanxue Sun, Kun Zhao, Zhe Wang, Martina Schnölzer, Qingjie Lv, Margot Zöller, Sanyukta Rana, and Thilo Hackert

Subjects

Messenger RNA, Gene knockdown, Cell signaling, Article Subject, business.industry, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Exosome, lcsh:RC254-282, Deep sequencing, Cell biology, Transcriptome, Oncology, microRNA, Medicine, business, Transcription factor, Research Article

Abstract

Pancreatic cancer-initiating cells (PaCIC) express CD44v6 and Tspan8. A knockdown (kd) of these markers hinders the metastatic capacity, which can be rescued, if the cells are exposed to CIC-exosomes (TEX). Additional evidence that CD44v6 regulates Tspan8 expression prompted us to explore the impact of these PaCIC markers on nonmetastatic PaCa and PaCIC-TEX. We performed proteome, miRNA, and mRNA deep sequencing analyses on wild-type, CD44v6kd, and Tspan8kd human PaCIC and TEX. Database comparative analyses were controlled by qRT-PCR, Western blot, flow cytometry, and confocal microscopy. Transcriptome analysis of CD44 versus CD44v6 coimmunoprecipitating proteins in cells and TEX revealed that Tspan8, several signal-transducing molecules including RTK, EMT-related transcription factors, and proteins engaged in mRNA processing selectively associate with CD44v6 and that the membrane-attached CD44 intracytoplasmic tail supports Tspan8 and NOTCH transcription. Deep sequencing uncovered a CD44v6 contribution to miRNA processing. Due to the association of CD44v6 with Tspan8 in internalization prone tetraspanin-enriched membrane domains (TEM) and the engagement of Tspan8 in exosome biogenesis, most CD44v6-dependent changes were transferred into TEX such that the input of CD44v6 to TEX activities becomes largely waved in both a CD44v6kd and a Tspan8kd. Few differences between CD44v6kd- and Tspan8kd-TEX rely on CD44v6 being also recovered in non-TEM derived TEX, highlighting distinct TEX delivery from individual cells that jointly account for TEX-promoted target modulation. This leads us to propose a model in which CD44v6 strongly supports tumor progression by cooperating with signaling molecules, altering transcription of key molecules, and through its association with the mRNA processing machinery. The association of CD44v6 with Tspan8, which plays a crucial role in vesicle biogenesis, promotes metastases by transferring CD44v6 activities into TEM and TEM-independently derived TEX. Further investigations of the lead position of CD44v6 in shifting metastasis-promoting activities into CIC-TEX may offer a means of targeting TEX-CD44v6 in therapeutic applications.

Published

2019

44. Modeling and multiscale characterization of the quantitative imaging based fibrosis index reveals pathophysiological, transcriptome and proteomic correlates of lung fibrosis induced by fractionated irradiation

Author

Christian Schwager, Bleddyn Jones, Martina Schnölzer, Liji Cao, Mark Kriegsmann, Mahmoud R. Moustafa, Martin Winter, Amir Abdollahi, Cheng Zhou, Tobias Bäuerle, Juergen Debus, Shijun Wang, Wilko Weichert, and Ping-Kun Zhou

Subjects

Proteomics, Cancer Research, Pathology, medicine.medical_specialty, fractionated radiotherapy, Transcriptome, Extracellular matrix, Mice, 03 medical and health sciences, Th2 Cells, 0302 clinical medicine, Fibrosis, Positron Emission Tomography Computed Tomography, Pulmonary fibrosis, Animals, M2 macrophages, Medicine, Longitudinal Studies, Epithelial–mesenchymal transition, Cancer Therapy and Prevention, Th2‐like response, Lung, pulmonary fibrosis, business.industry, Mesenchymal stem cell, medicine.disease, ddc, Mice, Inbred C57BL, Radiation Injuries, Experimental, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, radiation‐induced lung fibrosis, EMT/EndoMT, Immunohistochemistry, Female, Dose Fractionation, Radiation, Blood Gas Analysis, business, Algorithms

Abstract

Pulmonary fibrosis represents a leading cause of morbidity and mortality worldwide. Therapy induced lung fibrosis constitutes a pivotal dose‐limiting side effect of radiotherapy and other anticancer agents. We aimed to develop objective criteria for assessment of fibrosis and discover pathophysiological and molecular correlates of lung fibrosis as a function of fractionated whole thoracic irradiation. Dose–response series of fractionated irradiation was utilized to develop a non‐invasive and quantitative measure for the degree of fibrosis – the fibrosis index (FI). The correlation of FI with histopathology, blood‐gas, transcriptome and proteome responses of the lung tissue was analyzed. Macrophages infiltration and polarization was assessed by immunohistochemistry. Fibrosis development followed a slow kinetic with maximum lung fibrosis levels detected at 24‐week post radiation insult. FI favorably correlated with radiation dose and surrogates of lung fibrosis i.e., enhanced pro‐inflammatory response, tissue remodeling and extracellular matrix deposition. The loss of lung architecture correlated with decreased epithelial marker, loss of microvascular integrity with decreased endothelial and elevated mesenchymal markers. Lung fibrosis was further attributed to a switch of the inflammatory state toward a macrophage/T‐helper cell type 2‐like (M2/Th2) polarized phenotype. Together, the multiscale characterization of FI in radiation‐induced lung fibrosis (RILF) model identified pathophysiological, transcriptional and proteomic correlates of fibrosis. Pathological immune response and endothelial/epithelial to mesenchymal transition were discovered as critical events governing lung tissue remodeling. FI will be instrumental for deciphering the molecular mechanisms governing lung fibrosis and discovery of novel targets for treatment of this devastating disease with an unmet medical need., What's new? The development of fibrosis scar tissue in the lungs is a dose‐limiting effect of radiotherapy for thoracic malignancies. Molecular mechanisms driving radiation‐induced lung fibrosis (RILF), however, remain unclear. In this study, a fibrosis index (FI) was devised to quantitatively detect spatial and temporal kinetics of lung fibrosis development. Multi‐scale characterization of FI uncovered mechanisms governing lung fibrosis, including perturbation of immune balance and microvascular integrity. Radiation dose and FI were correlated with an inflammatory switch toward a macrophage/T‐helper cell type 2‐like polarized phenotype. The findings open the way for further mechanistic study and the discovery of therapeutic targets for RILF.

Published

2019

45. Detection of Proteome Changes in Human Colon Cancer Induced by Cell Surface Binding of Growth-Inhibitory Human Galectin-4 Using Quantitative SILAC-Based Proteomics

Author

Hans-Joachim Gabius, Sabine André, Martina Schnölzer, Malwina Michalak, Uwe Warnken, and Juergen Kopitz

Subjects

Proteomics, 0301 basic medicine, Proteome, Galectin 4, Cell, Endogeny, Biology, Biochemistry, Mass Spectrometry, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Stable isotope labeling by amino acids in cell culture, medicine, Humans, Cell growth, Cell Membrane, General Chemistry, Molecular biology, 3. Good health, Cell biology, Gene Expression Regulation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Colonic Neoplasms, Calretinin, Gelsolin

Abstract

Endogenous lectins have the capacity to translate glycan-encoded information on the cell surface into effects on cell growth. As test cases to examine changes in protein presence associated with tumor growth inhibition, we applied SILAC-based proteomics on human colon carcinoma cells treated with galectin-4 (Gal-4). The five tested lines-LS 180, Vaco 432, Colo 205, CX 1, and HCT 116-responded with differentiation and reduced proliferation to Gal-4 binding. In proteomic analysis (mass spectral data deposited with PRIDE, PXD003489), 2654 proteins were quantified, of which 190 were down-regulated and 115 were up-regulated (2-fold). 1D annotation analysis of the results indicated down-regulation of DNA replication-associated processes, while protein presence for secretory and transport functions appeared increased. The strongest induction was found for CALB2 (calretinin; ∼24-fold), TGM2 (protein-glutamine γ-glutamyltransferase 2; ∼11-fold), S100A3 (∼10-fold), and GSN (gelsolin; 9.5-fold), and the most pronounced decreases were seen for CDKN2A (tumor suppressor ARF; ∼6-fold), EPCAM (epithelial cell adhesion molecule; ∼6-fold), UBE2C (ubiquitin-conjugating enzyme E2 C; ∼5-fold), KIF2C (kinesin-like protein KIF2C; 5-fold), and LMNB1 (lamin-B1; ∼5-fold). The presence of the common proliferation marker Ki-67 was diminished about 4-fold. By tracing significant alterations of protein expression likely relevant for the observed phenotypic effects, the capacity of a galectin to affect the proteome of human colon cancer cells at multiple sites is revealed.

Published

2016

46. CD44v6-competent tumor exosomes promote motility, invasion and cancer-initiating cell marker expression in pancreatic and colorectal cancer cells

Author

Thilo Hackert, Zhe Wang, Margot Zöller, Anja von Au, and Martina Schnölzer

Subjects

cancer stem cells, 0301 basic medicine, Angiogenesis, Motility, exosomes, Metastasis, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Cancer stem cell, Cell Line, Tumor, Biomarkers, Tumor, Cell Adhesion, Animals, Humans, metastasis, Medicine, Neoplasm Invasiveness, adhesion molecules, Cell adhesion, biology, business.industry, CD44, CD44v6, medicine.disease, Microvesicles, Pancreatic Neoplasms, Hyaluronan Receptors, 030104 developmental biology, Oncology, Tumor progression, 030220 oncology & carcinogenesis, Immunology, Neoplastic Stem Cells, biology.protein, Cancer research, Colorectal Neoplasms, business, Research Paper

Abstract

Cancer-initiating cells (CIC) account for metastatic spread, which may rely mostly on CIC exosomes (TEX) that affect host cells and can transfer CIC features into Non-CIC. The CIC marker CD44 variant isoform v6 (CD44v6) being known for metastasis-promotion, we elaborated in cells its contribution to migration and invasion and in TEX the tranfer of migratory and invasive capacity to Non-CIC, using a CD44v6 knockdown (CD44v6kd) as Non-CIC model. A CD44v6kd in human pancreatic and colorectal cancer (PaCa, CoCa) lines led to loss of CIC characteristics including downregulation of additional CIC markers, particularly Tspan8. This aggravated the loss of CD44v6-promoted motility and invasion. Loss of motility relies on the distorted cooperation of CD44v6 and Tspan8 with associated integrins and loss of invasiveness on reduced protease expression. These deficits, transferred into TEX, severely altered the CD44v6kd-TEX composition. As a consequence, unlike the CIC-TEX, CD44v6kd TEX were not taken up by CD44v6kd cells and CIC. The uptake of CIC-TEX was accompanied by partial correction of CIC marker and protease expression in CD44v6kd cells, which regained migratory, invasive and metastatic competence. CIC-TEX also fostered angiogenesis and expansion of myeloid cells, likely due to a direct impact of CIC-TEX on the host, which could be supported by reprogrammed CD44v6kd cells. Taken together, the striking loss of tumor progression by a CD44v6kd relies on the capacity of CD44v6 to cooperate with associating integrins and proteases and its promotion of additional CIC marker expression. The defects by a CD44v6kd are efficiently corrected upon CIC-TEX uptake.

Published

2016

47. Palmitoylated claudin7 captured in glycolipid-enriched membrane microdomains promotes metastasis via associated transmembrane and cytosolic molecules

Author

Florian Thuma, Martina Schnölzer, Margot Zöller, and Sarah Heiler

Subjects

0301 basic medicine, claudin7 palmitoylation, Lipoylation, Adenocarcinoma, Exosomes, 03 medical and health sciences, Phosphatidylinositol 3-Kinases, 0302 clinical medicine, Ezrin, Cytosol, Membrane Microdomains, Palmitoylation, Cell Movement, Cell Line, Tumor, PTEN, metastasis, Animals, Neoplasm Metastasis, PI3K/AKT/mTOR pathway, biology, Kinase, glycolipid-enriched membrane microdomains, Membrane Proteins, Transmembrane protein, Microvesicles, Cell biology, Rats, Vesicular transport protein, Pancreatic Neoplasms, 030104 developmental biology, Oncology, complex-dependent bioactivity, 030220 oncology & carcinogenesis, Gene Knockdown Techniques, Claudins, biology.protein, Glycolipids, Proto-Oncogene Proteins c-akt, Research Paper, Signal Transduction, Transcription Factors

Abstract

// Florian Thuma 1, * , Sarah Heiler 1, * , Martina Schnolzer 2 , Margot Zoller 1 1 Department of Tumor Cell Biology, University Hospital of Surgery, Heidelberg, Germany 2 Department of Functional Proteome Analysis, German Cancer Research Center, Heidelberg, Germany * These authors contributed equally to this work Correspondence to: Margot Zoller, email: m.zoeller@uni-hd.de Keywords: claudin7 palmitoylation, metastasis, glycolipid-enriched membrane microdomains, complex-dependent bioactivity Received: November 26, 2015 Accepted: March 31, 2016 Published: April 22, 2016 ABSTRACT In epithelial cells claudin7 (cld7) is a major component of tight junctions, but is also recovered from glycolipid-enriched membrane microdomains (GEM). In tumor cells, too, cld7 exists in two stages. Only GEM-located cld7, which is palmitoylated, promotes metastasis. Searching for the underlying mechanism(s) revealed the following. The metastatic capacity of the rat pancreatic adenocarcinoma cell line ASML is lost by a knockdown (kd) of cld7 and is not regained by rescuing cld7 with a mutated palmitoylation site (cld7 mPalm ). ASML-cld7 kd and ASML-cld7 mPalm cells show reduced motility and invasiveness. This is due to cld7, but not cld7 mPalm associating with α6β4, ezrin, uPAR and MMP14, which jointly support motility and invasion. Palmitoylated cld7 also is engaged in drug resistance by repressing Pten, allowing activation of the antiapoptotic PI3K/Akt pathway. An association of cld7 mPalm with the major Pten phosphorylating kinases does not restore apoptosis resistance as phosphorylated Pten is not guided towards GEM to compete with non-phosphorylated Pten. The pathway whereby palmitoylated cld7 supports expression of several EMT genes and nuclear translocation of EMT transcription factors remains to be unraveled. An association with Notch, reduced in ASML-cld7 mPalm cells, might be the starting point. Finally, GEM-located, palmitoylated cld7 associates with several components of vesicle transport machineries engaged in exosome biogenesis. Taken together, prerequisites for cld7 acting as a cancer-initiating cell marker are GEM location and palmitoylation, which support a multitude of associations and integration into exosomes. The latter suggests palmitoylated cld7 contributing to message transfer via exosomes.

Published

2016

48. Characterization of a Threonine-Rich Cluster in Hepatitis C Virus Nonstructural Protein 5A and Its Contribution to Hyperphosphorylation

Author

Volker Lohmann, Christian Harak, Max Meyrath, Christian Schenk, Uwe Warnken, Martina Schnölzer, and Walter Mier

Subjects

0301 basic medicine, Proteomics, Threonine, 030106 microbiology, Immunology, Population, Hyperphosphorylation, Hepacivirus, Biology, Viral Nonstructural Proteins, Virus Replication, Microbiology, Mass Spectrometry, Cell Line, 03 medical and health sciences, Virology, Humans, Phosphorylation, education, NS5A, education.field_of_study, Phosphopeptide, Virus Assembly, Cell biology, Genome Replication and Regulation of Viral Gene Expression, 030104 developmental biology, Insect Science, Phosphoprotein, Mutation, Casein kinase 1, PI4KA

Abstract

Hepatitis C virus (HCV) nonstructural protein 5A (NS5A) is a phosphoprotein with key functions in regulating viral RNA replication and assembly. Two phosphoisoforms are discriminated by their different apparent molecular weights: a basally phosphorylated (p56) and a hyperphosphorylated (p58) variant. The precise mechanisms governing p58 synthesis and specific functions of the isoforms are poorly understood. Our study aimed at a deeper understanding of determinants involved in p58 synthesis. We analyzed two variants of p56 and p58 of isolate JFH-1 separately by mass spectrometry using an expression model and thereby identified a threonine-rich phosphopeptide exclusively found in the hyperphosphorylated variant. Individual exchange of possible phosphoacceptor sites to phosphoablatant or -mimetic residues had little impact on HCV replication or assembly in cell culture. A phosphospecific antibody recognizing pT242 revealed that this position was indeed phosphorylated only in p58 and depended on casein kinase Iα. Importantly, phosphoablative mutations at positions T244 and S247 abrogated pT242 detection without substantial effects on global p58 levels, whereas mutations in the preceding serine-rich cluster dramatically reduced total p58 levels but had minor impact on pT242 levels, suggesting the existence of distinct subspecies of hyperphosphorylated NS5A. Mass spectrometry analyses of different genotypes showed variable phosphorylation patterns across NS5A and suggested that the threonine-rich region is also phosphorylated at T242 in gt4a and at S249 in gt1a, gt1b, and gt4a. Our data therefore indicate that p58 is not a single homogenously phosphorylated protein species but rather a population of various phosphoisoforms, with high variability between genotypes. IMPORTANCE Hepatitis C virus infections affect 71 million people worldwide and cause severe chronic liver disease. Recently, efficient antiviral therapies have been established, with inhibitors of nonstructural protein NS5A as a cornerstone. NS5A is a central regulator of HCV replication and assembly but is still enigmatic in its molecular functions. It exists in two phosphoisoforms, p56 and p58. We identified a phosphopeptide exclusively found in p58 and analyzed the determinants involved in phosphorylation of this region. We found evidence for very different phosphorylation patterns resulting in p58. These results challenge the concept of p58 being a homogenous species of NS5A molecules phosphorylated at the same positions and argues for at least two independently phosphorylated variants showing the same electrophoretic mobility, likely serving different functions.

Published

2018

49. Detection of malignancy-associated phosphoproteome changes in human colorectal cancer induced by cell surface binding of growth-inhibitory galectin-4

Author

Jürgen Kopitz, Hans-Joachim Gabius, Malwina Michalak, Uwe Warnken, and Martina Schnölzer

Subjects

0301 basic medicine, Amino Acid Transport System ASC, Cofilin 1, Proteome, Chromosomal Proteins, Non-Histone, Glutamine, Clinical Biochemistry, Cell, Galectin 4, Antineoplastic Agents, Biochemistry, Minor Histocompatibility Antigens, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Stable isotope labeling by amino acids in cell culture, Cell Line, Tumor, Genetics, medicine, Humans, Qc-SNARE Proteins, Phosphorylation, Molecular Biology, Centromere Protein F, Carbon Isotopes, biology, Nitrogen Isotopes, Chemistry, Microfilament Proteins, CENPF, Phosphoproteomics, Biological Transport, Cell Biology, HCT116 Cells, Phosphoproteins, Recombinant Proteins, Cell biology, Neoplasm Proteins, 030104 developmental biology, medicine.anatomical_structure, Cell culture, 030220 oncology & carcinogenesis, Isotope Labeling, biology.protein, Growth inhibition, Protein Processing, Post-Translational

Abstract

Emerging evidence on efficient tumor growth regulation by endogenous lectins directs interest to determine on a proof-of-principle level the range of information on alterations provided by full-scale analysis using phosphoproteomics. In our pilot study, we tested galectin-4 (gal-4) that is a growth inhibitor for colon cancer cells (CRC), here working with the LS 180 line. In order to cover monitoring of short- and long-term effects stable isotope labeling by amino acids in cell culture-based quantitative phosphoproteomic analyses were conducted on LS 180 cell preparations collected 1 and 72 h after adding gal-4 to the culture medium. After short-term treatment, 981 phosphosites, all of them S/T based, were detected by phosphoproteomics. Changes higher than 1.5-fold were seen for eight sites in seven proteins. Most affected were the BET1 homolog (BET1), whose level of phosphorylation at S50 was about threefold reduced, and centromere protein F (CENPF), extent of phosphorylation at S3119 doubling in gal-4-treated cells. Phosphoproteome analysis after 72 h of treatment revealed marked changes at 33 S/T-based phosphosites from 29 proteins. Prominent increase of phosphorylation was observed for cofilin-1 at position S3. Extent of phosphorylation of the glutamine transporter SLC1A5 at position S503 was decreased by a factor of 3. Altered phosphorylation of BET1, CENPF, and cofilin-1 as well as a significant effect of gal-4 treatment on glutamine uptake by cells were substantiated by independent methods in the Vaco 432, Colo 205, CX 1, and HCT 116 cell lines. With the example of gal-4 which functions as a tumor suppressor in CRC cells, we were able to prove that cell surface binding of the lectin not only markedly influences the cell proteome, but also has a bearing on malignancy-associated intracellular protein phosphorylation. These results underscore the potential of this approach to give further work on elucidating the details of signaling underlying galectin-triggered growth inhibition a clear direction. © 2018 IUBMB Life, 71(3):364-375, 2019.

Published

2018

50. Claudin7-dependent exosome-promoted reprogramming of nonmetastasizing tumor cells

Author

Thilo Hackert, Daisuke Kyuno, Kun Zhao, Martina Schnölzer, Jan Provaznik, and Margot Zöller

Subjects

Cancer Research, Epithelial-Mesenchymal Transition, Angiogenesis, Cell, Integrin, Mice, Nude, Apoptosis, Exosomes, Exosome, Tight Junctions, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Pancreatic cancer, Cell Line, Tumor, medicine, Animals, Humans, Cell Proliferation, biology, Chemistry, medicine.disease, Xenograft Model Antitumor Assays, Microvesicles, Rats, Pancreatic Neoplasms, medicine.anatomical_structure, Oncology, Tumor progression, 030220 oncology & carcinogenesis, Claudins, Colonic Neoplasms, biology.protein, Cancer research, Disease Progression, Neoplastic Stem Cells, RNA Interference, Signal transduction

Abstract

Claudin7 (cld7) is a cancer-initiating cell (CIC) marker in gastrointestinal tumors, a cld7-knockdown (kd) being accompanied by loss of tumor progression. Tumor exosomes (TEX) restoring CIC activities, we explored the contribution of cld7. This became particularly interesting, as tight junction (TJ)- and glycolipid-enriched membrane domain (GEM)-derived cld7 is recruited into distinct TEX. TEXs were derived from CIC or cld7kd cells of a rat pancreatic and a human colon cancer line. TEX derived from pancreatic cancer cld7kd cells rescued with palmitoylation site-deficient cld7 (cld7mP) allowed selectively evaluating the contribution of GEM-derived TEX, only palmitoylated cld7 being integrated into GEM. Cld7 CIC-TEX promoted tumor cell dissemination and metastatic growth without a major impact on proliferation, apoptosis resistance and epithelial-mesenchymal transition. Instead, migration, invasion and (lymph)angiogenesis were strongly supported, only migration being selectively fostered by GEM-derived cld7 TEX. CIC-TEX coculture of cld7kd cells uncovered significant changes in the cld7kd cell protein and miRNA profiles. However, changes did not correspond to the CIC-TEX profile, CIC-TEX rather initiating integrin, protease and RTK, particularly lymphangiogenic receptor activation. CIC-TEX preferentially rescuing cld7kd-associated defects in signal transduction was backed up by an RTK inhibitor neutralizing the impact of CIC-TEX on tumor progression. In conclusion, cld7 contributes to selective steps of the metastatic cascade. Defects of cld7kd and cld7mP cells in migration, invasion and (lymph)angiogenesis are effaced by CIC-TEX that act by signaling cascade activation. Accordingly, RTK inhibitors are an efficient therapeutic defeating CIC-TEX.

Published

2018