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1. In vivo CRISPR screens identify a dual function of MEN1 in regulating tumor–microenvironment interactions

Author

Su, Peiran, Liu, Yin, Chen, Tianyi, Xue, Yibo, Zeng, Yong, Zhu, Guanghui, Chen, Sujun, Teng, Mona, Ci, Xinpei, Guo, Mengdi, He, Michael Y., Hao, Jun, Chu, Vivian, Xu, Wenxi, Wang, Shiyan, Mehdipour, Parinaz, Xu, Xin, Marhon, Sajid A., Soares, Fraser, Pham, Nhu-An, Wu, Bell Xi, Her, Peter Hyunwuk, Feng, Shengrui, Alshamlan, Najd, Khalil, Maryam, Krishnan, Rehna, Yu, Fangyou, Chen, Chang, Burrows, Francis, Hakem, Razqallah, Lupien, Mathieu, Harding, Shane, Lok, Benjamin H., O’Brien, Catherine, Berlin, Alejandro, De Carvalho, Daniel D., Brooks, David G., Schramek, Daniel, Tsao, Ming-Sound, and He, Housheng Hansen

Published
2024
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2. Genome-wide CRISPR screens identify novel regulators of wild-type and mutant p53 stability

Author

Lü, YiQing, Cho, Tiffany, Mukherjee, Saptaparna, Suarez, Carmen Florencia, Gonzalez-Foutel, Nicolas S, Malik, Ahmad, Martinez, Sebastien, Dervovic, Dzana, Oh, Robin Hyunseo, Langille, Ellen, Al-Zahrani, Khalid N, Hoeg, Lisa, Lin, Zhen Yuan, Tsai, Ricky, Mbamalu, Geraldine, Rotter, Varda, Ashton-Prolla, Patricia, Moffat, Jason, Chemes, Lucia Beatriz, Gingras, Anne-Claude, Oren, Moshe, Durocher, Daniel, and Schramek, Daniel

Published
2024
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7. In vivo CRISPR screens reveal SCAF1 and USP15 as drivers of pancreatic cancer

Author

Sebastien Martinez, Shifei Wu, Michael Geuenich, Ahmad Malik, Ramona Weber, Tristan Woo, Amy Zhang, Gun Ho Jang, Dzana Dervovic, Khalid N. Al-Zahrani, Ricky Tsai, Nassima Fodil, Philippe Gros, Steven Gallinger, G. Gregory Neely, Faiyaz Notta, Ataman Sendoel, Kieran Campbell, Ulrich Elling, and Daniel Schramek

Subjects
Science
Abstract

Abstract Functionally characterizing the genetic alterations that drive pancreatic cancer is a prerequisite for precision medicine. Here, we perform somatic CRISPR/Cas9 mutagenesis screens to assess the transforming potential of 125 recurrently mutated pancreatic cancer genes, which revealed USP15 and SCAF1 as pancreatic tumor suppressors. Mechanistically, we find that USP15 functions in a haploinsufficient manner and that loss of USP15 or SCAF1 leads to reduced inflammatory TNFα, TGF-β and IL6 responses and increased sensitivity to PARP inhibition and Gemcitabine. Furthermore, we find that loss of SCAF1 leads to the formation of a truncated, inactive USP15 isoform at the expense of full-length USP15, functionally coupling SCAF1 and USP15. Notably, USP15 and SCAF1 alterations are observed in 31% of pancreatic cancer patients. Our results highlight the utility of in vivo CRISPR screens to integrate human cancer genomics and mouse modeling for the discovery of cancer driver genes with potential prognostic and therapeutic implications.

Published
2024
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8. #Winemom culture

Author

Vange Holtz-Schramek

Subjects
#winemom culture, COVID-19, feminist media studies, social media research ethics, Social sciences (General), H1-99
Abstract

Experts trace a congruent trend, pinpointed as originating around the 2010s (Grose, 2020) and only accelerating in the pandemic and its aftermaths: the rise of social media activity relating to parents’ performances of their substance abuse – what this paper defines as “#winemom culture” – with a broader social tendency, a general increase in “rates of high-risk drinking” that lead to such outcomes as “long-term health damage” and “dangers to family” (Macarthur, n.d.). I interrogate the ethics of moralizing against #winemom culture under COVID-19 culture and its aftermaths through exclusively quantitative metrics or surface-level analysis. As with anything coded according to the “momification of the Internet” (Dewey, 2015), such cultures are often disregarded, seen as superficial or in receipt of unchecked judgments. I trace the following question: What can #winemom culture reveal about how parents are processing and communicating within this moment? And begin from the premise that there are as-yet undetermined drivers motivating what appears to be a “zoning out” (Heyes, 2020) in the mediation of #winemom culture production. This project then opens into an analysis of how to actually study digital feminist practices in this current moment, one that is defined by methodological crises surrounding the increasing complexities of enacting justice in social media research. This paper thus serves as a methodological disquisition for feminist researchers attempting to perform ethically just social media research.

Published
2024
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9. In Vivo Screening Unveils Pervasive RNA-Binding Protein Dependencies in Leukemic Stem Cells and Identifies ELAVL1 as a Therapeutic Target.

Author

Vujovic, Ana, de Rooij, Laura, Chahi, Ava, Chen, He, Yee, Brian, Loganathan, Sampath, Liu, Lina, Chan, Derek, Tajik, Amanda, Tsao, Emily, Moreira, Steven, Joshi, Pratik, Xu, Joshua, Wong, Nicholas, Balde, Zaldy, Jahangiri, Soheil, Zandi, Sasan, Dick, John, Minden, Mark, Schramek, Daniel, Yeo, Gene, Hope, Kristin, and Aigner, Stefan

Subjects
Humans, Leukemia, Myeloid, Acute, Cell Differentiation, Hematopoietic Stem Cells, RNA-Binding Proteins, Mitochondrial Precursor Protein Import Complex Proteins, ELAV-Like Protein 1
Abstract

UNLABELLED: Acute myeloid leukemia (AML) is fueled by leukemic stem cells (LSC) whose determinants are challenging to discern from hematopoietic stem cells (HSC) or uncover by approaches focused on general cell properties. We have identified a set of RNA-binding proteins (RBP) selectively enriched in human AML LSCs. Using an in vivo two-step CRISPR-Cas9 screen to assay stem cell functionality, we found 32 RBPs essential for LSCs in MLL-AF9;NrasG12D AML. Loss-of-function approaches targeting key hit RBP ELAVL1 compromised LSC-driven in vivo leukemic reconstitution, and selectively depleted primitive malignant versus healthy cells. Integrative multiomics revealed differentiation, splicing, and mitochondrial metabolism as key features defining the leukemic ELAVL1-mRNA interactome with mitochondrial import protein, TOMM34, being a direct ELAVL1-stabilized target whose repression impairs AML propagation. Altogether, using a stem cell-adapted in vivo CRISPR screen, this work demonstrates pervasive reliance on RBPs as regulators of LSCs and highlights their potential as therapeutic targets in AML. SIGNIFICANCE: LSC-targeted therapies remain a significant unmet need in AML. We developed a stem-cell-adapted in vivo CRISPR screen to identify key LSC drivers. We uncover widespread RNA-binding protein dependencies in LSCs, including ELAVL1, which we identify as a novel therapeutic vulnerability through its regulation of mitochondrial metabolism. This article is highlighted in the In This Issue feature, p. 171.

Published
2023

10. Genome-wide CRISPR screens identify novel regulators of wild-type and mutant p53 stability

Author

YiQing Lü, Tiffany Cho, Saptaparna Mukherjee, Carmen Florencia Suarez, Nicolas S Gonzalez-Foutel, Ahmad Malik, Sebastien Martinez, Dzana Dervovic, Robin Hyunseo Oh, Ellen Langille, Khalid N Al-Zahrani, Lisa Hoeg, Zhen Yuan Lin, Ricky Tsai, Geraldine Mbamalu, Varda Rotter, Patricia Ashton-Prolla, Jason Moffat, Lucia Beatriz Chemes, Anne-Claude Gingras, Moshe Oren, Daniel Durocher, and Daniel Schramek

Subjects
Genome-wide CRISPR Screening, Mutant p53, p53 Stability, Breast Cancer, Fluorescence-based Stability Reporter, Biology (General), QH301-705.5, Medicine (General), R5-920
Abstract

Abstract Tumor suppressor p53 (TP53) is frequently mutated in cancer, often resulting not only in loss of its tumor-suppressive function but also acquisition of dominant-negative and even oncogenic gain-of-function traits. While wild-type p53 levels are tightly regulated, mutants are typically stabilized in tumors, which is crucial for their oncogenic properties. Here, we systematically profiled the factors that regulate protein stability of wild-type and mutant p53 using marker-based genome-wide CRISPR screens. Most regulators of wild-type p53 also regulate p53 mutants, except for p53 R337H regulators, which are largely private to this mutant. Mechanistically, FBXO42 emerged as a positive regulator for a subset of p53 mutants, working with CCDC6 to control USP28-mediated mutant p53 stabilization. Additionally, C16orf72/HAPSTR1 negatively regulates both wild-type p53 and all tested mutants. C16orf72/HAPSTR1 is commonly amplified in breast cancer, and its overexpression reduces p53 levels in mouse mammary epithelium leading to accelerated breast cancer. This study offers a network perspective on p53 stability regulation, potentially guiding strategies to reinforce wild-type p53 or target mutant p53 in cancer.

Published
2024
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11. A noncoding single-nucleotide polymorphism at 8q24 drives IDH1-mutant glioma formation

Author

Yanchus, Connor, Drucker, Kristen L, Kollmeyer, Thomas M, Tsai, Ricky, Winick-Ng, Warren, Liang, Minggao, Malik, Ahmad, Pawling, Judy, De Lorenzo, Silvana B, Ali, Asma, Decker, Paul A, Kosel, Matt L, Panda, Arijit, Al-Zahrani, Khalid N, Jiang, Lingyan, Browning, Jared WL, Lowden, Chris, Geuenich, Michael, Hernandez, J Javier, Gosio, Jessica T, Ahmed, Musaddeque, Loganathan, Sampath Kumar, Berman, Jacob, Trcka, Daniel, Michealraj, Kulandaimanuvel Antony, Fortin, Jerome, Carson, Brittany, Hollingsworth, Ethan W, Jacinto, Sandra, Mazrooei, Parisa, Zhou, Lily, Elia, Andrew, Lupien, Mathieu, He, Housheng Hansen, Murphy, Daniel J, Wang, Liguo, Abyzov, Alexej, Dennis, James W, Maass, Philipp G, Campbell, Kieran, Wilson, Michael D, Lachance, Daniel H, Wrensch, Margaret, Wiencke, John, Mak, Tak, Pennacchio, Len A, Dickel, Diane E, Visel, Axel, Wrana, Jeffrey, Taylor, Michael D, Zadeh, Gelareh, Dirks, Peter, Eckel-Passow, Jeanette E, Attisano, Liliana, Pombo, Ana, Ida, Cristiane M, Kvon, Evgeny Z, Jenkins, Robert B, and Schramek, Daniel

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Brain Cancer, Brain Disorders, Human Genome, Neurosciences, Rare Diseases, Genetics, Cancer Genomics, Cancer, 2.1 Biological and endogenous factors, Animals, Brain Neoplasms, Chromosomes, Human, Pair 8, Glioma, Humans, Isocitrate Dehydrogenase, Mice, Mutation, Polymorphism, Single Nucleotide, General Science & Technology
Abstract

Establishing causal links between inherited polymorphisms and cancer risk is challenging. Here, we focus on the single-nucleotide polymorphism rs55705857, which confers a sixfold greater risk of isocitrate dehydrogenase (IDH)-mutant low-grade glioma (LGG). We reveal that rs55705857 itself is the causal variant and is associated with molecular pathways that drive LGG. Mechanistically, we show that rs55705857 resides within a brain-specific enhancer, where the risk allele disrupts OCT2/4 binding, allowing increased interaction with the Myc promoter and increased Myc expression. Mutating the orthologous mouse rs55705857 locus accelerated tumor development in an Idh1R132H-driven LGG mouse model from 472 to 172 days and increased penetrance from 30% to 75%. Our work reveals mechanisms of the heritable predisposition to lethal glioma in ~40% of LGG patients.

Published
2022

12. A designer peptide against the EAG2–Kvβ2 potassium channel targets the interaction of cancer cells and neurons to treat glioblastoma

Author

Dong, Weifan, Fekete, Adam, Chen, Xiaodi, Liu, Hongwei, Beilhartz, Greg L., Chen, Xin, Bahrampour, Shahrzad, Xiong, Yi, Yang, Qi, Zhao, Hongyu, Kong, Tian, Morioka, Malia S., Jung, Geena, Kim, Ji-Eun, Schramek, Daniel, Dirks, Peter B., Song, Yuanquan, Kim, Tae-Hee, He, Ye, Wanggou, Siyi, Li, Xuejun, Melnyk, Roman A., Wang, Lu-Yang, and Huang, Xi

Published
2023
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13. Author Correction: In vivo CRISPR screens reveal Serpinb9 and Adam2 as regulators of immune therapy response in lung cancer

Author

Dervovic, Dzana, Malik, Ahmad A., Chen, Edward L. Y., Narimatsu, Masahiro, Adler, Nina, Afiuni-Zadeh, Somaieh, Krenbek, Dagmar, Martinez, Sebastien, Tsai, Ricky, Boucher, Jonathan, Berman, Jacob M., Teng, Katie, Ayyaz, Arshad, Lü, YiQing, Mbamalu, Geraldine, Loganathan, Sampath K., Lee, Jongbok, Zhang, Li, Guidos, Cynthia, Wrana, Jeffrey, Valipour, Arschang, Roux, Philippe P., Reimand, Jüri, Jackson, Hartland W., and Schramek, Daniel

Published
2023
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14. In vivo CRISPR screens reveal Serpinb9 and Adam2 as regulators of immune therapy response in lung cancer

Author

Dervovic, Dzana, Malik, Ahmad A., Chen, Edward L. Y., Narimatsu, Masahiro, Adler, Nina, Afiuni-Zadeh, Somaieh, Krenbek, Dagmar, Martinez, Sebastien, Tsai, Ricky, Boucher, Jonathan, Berman, Jacob M., Teng, Katie, Ayyaz, Arshad, Lü, YiQing, Mbamalu, Geraldine, Loganathan, Sampath K., Lee, Jongbok, Zhang, Li, Guidos, Cynthia, Wrana, Jeffrey, Valipour, Arschang, Roux, Philippe P., Reimand, Jüri, Jackson, Hartland W., and Schramek, Daniel

Published
2023
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15. A non-coding single nucleotide polymorphism at 8q24 drives IDH1-mutant glioma formation

Author

Yanchus, Connor, Drucker, Kristen L, Kollmeyer, Thomas M, Tsai, Ricky, Liang, Minggao, Jiang, Lingyan, Pawling, Judy, Ali, Asma, Decker, Paul, Kosel, Matt, Panda, Arijit, Malik, Ahmad, Al-Zahrani, Khalid N, Hernandez, J Javier, Ahmed, Musaddeque, Loganathan, Sampath Kumar, Trcka, Daniel, Michaelraj, Antony, Fortin, Jerome, Mazrooei, Parisa, Zhou, Lily, Elia, Andrew, Lupien, Mathieu, He, Housheng Hansen, Wang, Liguo, Abyzov, Alexej, Dennis, James W, Wilson, Michael D, Wrana, Jeffrey, Lachance, Daniel, Wrensch, Margaret, Wiencke, John, Pennacchio, Len A, Dickel, Diane E, Visel, Axel, Taylor, Michael, Zadeh, Gelareh, Dirks, Peter, Eckel-Passow, Jeanette E, Mak, Tak, Kvon, Evgeny, Jenkins, Robert B, and Schramek, Daniel

Subjects
Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer Genomics, Brain Cancer, Brain Disorders, Rare Diseases, Prevention, Genetics, Human Genome, Cancer, Neurosciences, 2.1 Biological and endogenous factors
Abstract

Establishing causal links between inherited polymorphisms and cancer risk is challenging. Here, we focus on the single nucleotide polymorphism rs55705857 (A>G), which confers a 6-fold increased risk of IDH-mutant low-grade glioma (LGG) and is amongst the highest genetic associations with cancer. By fine-mapping the locus, we reveal that rs55705857 itself is the causal variant and is associated with molecular pathways that drive LGG. Mechanistically, we show that rs55705857 resides within a brain-specific enhancer, where the risk allele disrupts OCT2/4 binding, allowing increased interaction with the Myc promoter and increased Myc expression. To functionally test rs55705857, we generated an IDH1 R132H -driven LGG mouse model and show that mutating the highly conserved, orthologous mouse rs55705857 locus dramatically accelerated tumor development from 463 to 172 days and increased penetrance from 30% to 75%. Overall, our work generates new LGG models and reveals mechanisms of the heritable predisposition to lethal glioma in ∼40% of LGG-patients.

Published
2022

17. In vivo CRISPR screens reveal Serpinb9 and Adam2 as regulators of immune therapy response in lung cancer

Author

Dzana Dervovic, Ahmad A. Malik, Edward L. Y. Chen, Masahiro Narimatsu, Nina Adler, Somaieh Afiuni-Zadeh, Dagmar Krenbek, Sebastien Martinez, Ricky Tsai, Jonathan Boucher, Jacob M. Berman, Katie Teng, Arshad Ayyaz, YiQing Lü, Geraldine Mbamalu, Sampath K. Loganathan, Jongbok Lee, Li Zhang, Cynthia Guidos, Jeffrey Wrana, Arschang Valipour, Philippe P. Roux, Jüri Reimand, Hartland W. Jackson, and Daniel Schramek

Subjects
Science
Abstract

Abstract How the genetic landscape governs a tumor’s response to immunotherapy remains poorly understood. To assess the immune-modulatory capabilities of 573 genes associated with altered cytotoxicity in human cancers, here we perform CRISPR/Cas9 screens directly in mouse lung cancer models. We recover the known immune evasion factors Stat1 and Serpinb9 and identify the cancer testis antigen Adam2 as an immune modulator, whose expression is induced by KrasG12D and further elevated by immunotherapy. Using loss- and gain-of-function experiments, we show that ADAM2 functions as an oncogene by restraining interferon and TNF cytokine signaling causing reduced presentation of tumor-associated antigens. ADAM2 also restricts expression of the immune checkpoint inhibitors PDL1, LAG3, TIGIT and TIM3 in the tumor microenvironment, which might explain why ex vivo expanded and adoptively transferred cytotoxic T-cells show enhanced cytotoxic efficacy in ADAM2 overexpressing tumors. Together, direct in vivo CRISPR/Cas9 screens can uncover genetic alterations that control responses to immunotherapies.

Published
2023
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19. Differential DNA damage repair and PARP inhibitor vulnerability of the mammary epithelial lineages

Author

Hyeyeon Kim, Kazeera Aliar, Pirashaanthy Tharmapalan, Curtis W. McCloskey, Abhijith Kuttanamkuzhi, Barbara T. Grünwald, Luis Palomero, Mathepan J. Mahendralingam, Matthew Waas, Arvind S. Mer, Mitchell J. Elliott, Bowen Zhang, Khalid N. Al-Zahrani, Ellen R. Langille, Michael Parsons, Swami Narala, Stefan Hofer, Paul D. Waterhouse, Razqallah Hakem, Benjamin Haibe-Kains, Thomas Kislinger, Daniel Schramek, David W. Cescon, Miquel A. Pujana, Hal K. Berman, and Rama Khokha

Subjects
Biology (General), QH301-705.5
Published
2023
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20. Towards a Fishing Pressure Prediction System for a Western Pacific EEZ

Author

Cimino, Megan A, Anderson, Mark, Schramek, Travis, Merrifield, Sophia, and Terrill, Eric J

Subjects
Environmental Sciences, International and Comparative Law, Law and Legal Studies, Environmental Management, Life Below Water, Life on Land, Conservation of Natural Resources, Ecosystem, Fisheries, Models, Theoretical, Pacific Ocean
Abstract

Fisheries management faces numerous monitoring and enforcement challenges that are becoming more complex as fish stocks are depleted; and illegal, unregulated, and unreported fishing becomes more sophisticated. For remote island nations, the challenges are compounded by a loosely understood association of pelagic stocks to the ocean environment, and the tyranny of distance in monitoring and surveilling large exclusive economic zones (EEZ). An approach to ocean conservation is establishing protected areas, with the Pacific island nation of Palau as a leader with the recently established National Marine Sanctuary, which closes 80% of their EEZ to commercial fishing in 2020. Here we present an EEZ-wide analysis of Palau commercial fishing over a 6-year period (2011-2016), and develop a system for predicting fishing activity accounting for oceanic variables, climate indices, and vessel flag. Linking pelagic habitat to fishing activity provides high-resolution decision aids for management, highlighting the need for EEZ-specific analyses in addressing fisheries.

Published
2019

21. Exosomal mitochondrial tRNAs and miRNAs as potential predictors of inflammation in renal proximal tubular epithelial cells

Author

Glory Ranches, Maximilian Zeidler, Roman Kessler, Martina Hoelzl, Michael W. Hess, Jonathan Vosper, Paul Perco, Herbert Schramek, Kai K. Kummer, Michaela Kress, Anne Krogsdam, Michael Rudnicki, Gert Mayer, and Alexander Huettenhofer

Subjects
MT: Oligonucleotides: Diagnostics and Biosensors, ncRNAs, mtRNAs, miRNAs, exosomes, renal proximal tubular epithelial cells, Therapeutics. Pharmacology, RM1-950
Abstract

Exosomes have emerged as a valuable repository of novel biomarkers for human diseases such as chronic kidney disease (CKD). From a healthy control group, we performed microRNA (miRNA) profiling of urinary exosomes and compared it with a cell culture model of renal proximal tubular epithelial cells (RPTECs). Thereby, a large fraction of abundant urinary exosomal miRNAs could also be detected in exosomes derived from RPTECs, indicating them as a suitable model system for investigation of CKD. We subsequently analyzed exosomes from RPTECs in pro-inflammatory and pro-fibrotic states, mimicking some aspects of CKD. Following cytokine treatment, we observed a significant increase in exosome release and identified 30 dysregulated exosomal miRNAs, predominantly associated with the regulation of pro-inflammatory and pro-fibrotic-related pathways. In addition to miRNAs, we also identified 16 dysregulated exosomal mitochondrial RNAs, highlighting a pivotal role of mitochondria in sensing renal inflammation. Inhibitors of exosome biogenesis and release significantly altered the abundance of selected candidate miRNAs and mitochondrial RNAs, thus suggesting distinct sorting mechanisms of different non-coding RNA (ncRNA) species into exosomes. Hence, these two exosomal ncRNA species might be employed as potential indicators for predicting the pathogenesis of CKD and also might enable effective monitoring of the efficacy of CKD treatment.

Published
2022
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22. Author Correction: In vivo CRISPR screens reveal Serpinb9 and Adam2 as regulators of immune therapy response in lung cancer

Author

Dzana Dervovic, Ahmad A. Malik, Edward L. Y. Chen, Masahiro Narimatsu, Nina Adler, Somaieh Afiuni-Zadeh, Dagmar Krenbek, Sebastien Martinez, Ricky Tsai, Jonathan Boucher, Jacob M. Berman, Katie Teng, Arshad Ayyaz, YiQing Lü, Geraldine Mbamalu, Sampath K. Loganathan, Jongbok Lee, Li Zhang, Cynthia Guidos, Jeffrey Wrana, Arschang Valipour, Philippe P. Roux, Jüri Reimand, Hartland W. Jackson, and Daniel Schramek

Subjects
Science
Published
2023
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23. A CRISPR Path to Finding Vulnerabilities and Solving Drug Resistance: Targeting the Diverse Cancer Landscape and Its Ecosystem

Author

Benjamin McLean, Aji Istadi, Teleri Clack, Mezzalina Vankan, Daniel Schramek, G. Gregory Neely, and Marina Pajic

Subjects
cancer drug resistance, chemotherapy, CRISPR/Cas9, immunotherapy, predictive biomarkers, Genetics, QH426-470
Abstract

Abstract Cancer is the second leading cause of death globally, with therapeutic resistance being a major cause of treatment failure in the clinic. The dynamic signaling that occurs between tumor cells and the diverse cells of the surrounding tumor microenvironment actively promotes disease progression and therapeutic resistance. Improving the understanding of how tumors evolve following therapy and the molecular mechanisms underpinning de novo or acquired resistance is thus critical for the identification of new targets and for the subsequent development of more effective combination regimens. Simultaneously targeting multiple hallmark capabilities of cancer to circumvent adaptive or evasive resistance may lead to significantly improved treatment response in the clinic. Here, the latest applications of functional genomics tools, such as clustered regularly interspaced short palindromic repeats (CRISPR) editing, to characterize the dynamic cancer resistance mechanisms, from improving the understanding of resistance to classical chemotherapeutics, to deciphering unique mechanisms that regulate tumor responses to new targeted agents and immunotherapies, are discussed. Potential avenues of future research in combating therapeutic resistance, the contribution of tumor–stroma signaling in this setting, and how advanced functional genomics tools can help streamline the identification of key molecular determinants of drug response are explored.

Published
2022
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25. A Phase 1/1b Study Evaluating Trametinib Plus Docetaxel or Pemetrexed in Patients With Advanced Non–Small Cell Lung Cancer

Author

Gandara, David R, Leighl, Natasha, Delord, Jean-Pierre, Barlesi, Fabrice, Bennouna, Jaafar, Zalcman, Gerald, Infante, Jeffrey R, Reckamp, Karen L, Kelly, Karen, Shepherd, Frances A, Mazieres, Julien, Janku, Filip, Gardner, Olivia S, Mookerjee, Bijoyesh, Wu, Yuehui, Cox, Donna S, Schramek, Dan, Peddareddigari, Vijay, Liu, Yuan, D'Amelio, Anthony M, and Blumenschein, George

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Lung, Clinical Research, Lung Cancer, Cancer, Clinical Trials and Supportive Activities, Evaluation of treatments and therapeutic interventions, 6.1 Pharmaceuticals, Adenocarcinoma, Adult, Aged, Aged, 80 and over, Antineoplastic Combined Chemotherapy Protocols, Carcinoma, Large Cell, Carcinoma, Non-Small-Cell Lung, Carcinoma, Squamous Cell, Docetaxel, Female, Follow-Up Studies, Humans, Lung Neoplasms, Male, Middle Aged, Neoplasm Staging, Pemetrexed, Prognosis, Pyridones, Pyrimidinones, Survival Rate, Taxoids, Trametinib, MEK inhibitor, NSCLC, KRAS mutations, Cardiorespiratory Medicine and Haematology, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis
Abstract

ObjectivesThis two-part study evaluated trametinib, a MEK1/2 inhibitor, in combination with anticancer agents. Inhibition of MEK, a downstream effector of KRAS, demonstrated preclinical synergy with chemotherapy in KRAS-mutant NSCLC cell lines. Part 1 of this study identified recommended phase 2 doses of trametinib combinations. Part 2, reported herein, evaluated the safety, tolerability, pharmacokinetics, and efficacy of trametinib combinations in patients with NSCLC with and without KRAS mutations.MethodsPhase 1b evaluated trametinib plus docetaxel with growth factor support (trametinib, 2.0 mg once daily, and docetaxel, 75 mg/m2 every 3 weeks) or pemetrexed (trametinib, 1.5 mg once daily, and pemetrexed, 500 mg/m2 every 3 weeks). Eligibility criteria for the expansion cohorts included metastatic NSCLC with measurable disease, known KRAS mutation status, Eastern Cooperative Oncology Group performance status of 1 or lower, and no more than two prior regimens.ResultsThe primary end point of overall response rate (ORR) was met for both combinations. A confirmed partial response (PR) was observed in 10 of the 47 patients with NSCLC who received trametinib plus docetaxel (21%). The ORR was 18% (four PRs in 22 patients) in those with KRAS wild-type NSCLC versus 24% (six PRs in 25 patients) in those with KRAS-mutant NSCLC. Of the 42 patients with NSCLC treated with trametinib plus pemetrexed, six (14%) had a PR; the ORR was 17% (four of 23) in patients with KRAS-mutated NSCLC versus 11% (two of 19) in KRAS wild-type NSCLC. Adverse events-most commonly diarrhea, nausea, and fatigue-were manageable.ConclusionsTrametinib-plus-chemotherapy combinations were tolerable. Clinical activity exceeding the ORRs previously reported with docetaxel or pemetrexed alone in KRAS-mutated NSCLC and meeting prespecified criteria was observed.

Published
2017

27. RANKL/RANK control Brca1 mutation-driven mammary tumors

Author

Sigl, Verena, Owusu-Boaitey, Kwadwo, Joshi, Purna A, Kavirayani, Anoop, Wirnsberger, Gerald, Novatchkova, Maria, Kozieradzki, Ivona, Schramek, Daniel, Edokobi, Nnamdi, Hersl, Jerome, Sampson, Aishia, Odai-Afotey, Ashley, Lazaro, Conxi, Gonzalez-Suarez, Eva, Pujana, Miguel A, CIMBA, for, Heyn, Holger, Vidal, Enrique, Cruickshank, Jennifer, Berman, Hal, Sarao, Renu, Ticevic, Melita, Uribesalgo, Iris, Tortola, Luigi, Rao, Shuan, Tan, Yen, Pfeiler, Georg, Lee, Eva YHP, Bago-Horvath, Zsuzsanna, Kenner, Lukas, Popper, Helmuth, Singer, Christian, Khokha, Rama, Jones, Laundette P, and Penninger, Josef M

Subjects
Biochemistry and Cell Biology, Biological Sciences, Stem Cell Research, Cancer, Aging, Genetic Testing, Genetics, Prevention, Breast Cancer, Aetiology, 2.1 Biological and endogenous factors, Animals, BRCA1 Protein, BRCA2 Protein, Breast Neoplasms, Cell Proliferation, Cells, Cultured, DNA Damage, Epithelial Cells, Estrogen Receptor alpha, Female, Genotype, Humans, Mice, Mice, Inbred C57BL, Mice, Transgenic, RANK Ligand, Receptor Activator of Nuclear Factor-kappa B, Receptors, Progesterone, Recombinant Fusion Proteins, Stem Cells, Tumor Suppressor Protein p53, BRCA1, RANK, RANKL, inherited breast cancer, mammary progenitor cells, Clinical Sciences, Developmental Biology, Biochemistry and cell biology
Abstract

Breast cancer is the most common female cancer, affecting approximately one in eight women during their life-time. Besides environmental triggers and hormones, inherited mutations in the breast cancer 1 (BRCA1) or BRCA2 genes markedly increase the risk for the development of breast cancer. Here, using two different mouse models, we show that genetic inactivation of the key osteoclast differentiation factor RANK in the mammary epithelium markedly delayed onset, reduced incidence, and attenuated progression of Brca1;p53 mutation-driven mammary cancer. Long-term pharmacological inhibition of the RANK ligand RANKL in mice abolished the occurrence of Brca1 mutation-driven pre-neoplastic lesions. Mechanistically, genetic inactivation of Rank or RANKL/RANK blockade impaired proliferation and expansion of both murine Brca1;p53 mutant mammary stem cells and mammary progenitors from human BRCA1 mutation carriers. In addition, genome variations within the RANK locus were significantly associated with risk of developing breast cancer in women with BRCA1 mutations. Thus, RANKL/RANK control progenitor cell expansion and tumorigenesis in inherited breast cancer. These results present a viable strategy for the possible prevention of breast cancer in BRCA1 mutant patients.

Published
2016

28. Copper bioavailability is a KRAS-specific vulnerability in colorectal cancer

Author

Léo Aubert, Neethi Nandagopal, Zachary Steinhart, Geneviève Lavoie, Sami Nourreddine, Jacob Berman, Marc K. Saba-El-Leil, David Papadopoli, Sichun Lin, Traver Hart, Graham Macleod, Ivan Topisirovic, Louis Gaboury, Christoph J. Fahrni, Daniel Schramek, Sylvain Meloche, Stephane Angers, and Philippe P. Roux

Subjects
Science
Abstract

The oncogene KRAS is frequently mutated in cancer, including colorectal cancer. Here, using a cell-surface proteomics approach, KRAS-mutated colorectal cancer cells are shown to express high levels of the copper transporter ATP7A, which has an essential roles in cancer cell survival and proliferation.

Published
2020
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29. Differential Expression of Dickkopf 1 and Periostin in Mouse Strains with High and Low Bone Mass

Author

Katharina Kerschan-Schindl, Victoria Schramek, Maria Butylina, Ursula Föger-Samwald, and Peter Pietschmann

Subjects
C57BL/6J mice, C3H/J mice, sclerostin, dickkopf 1, periostin, Biology (General), QH301-705.5
Abstract

By expressing different genes and proteins that regulate osteoclast as well as osteoblast formation, osteocytes orchestrate bone metabolism. The aim of this project was the evaluation of the differences in the osteocytes’ secretory activity in the low bone mass mouse strain C57BL/6J and the high bone mass strain C3H/J. The femura of eight- and sixteen-week-old male C57BL/6J and C3H/J mice—six animals per group—were analyzed. Using immunohistochemistry, osteocytes expressing dickkopf 1, sclerostin, periostin, fibroblast growth factor 23 (FGF23), and osteoprotegerin were detected. By means of the OsteoMeasure-System, 92.173 osteocytes were counted. At the age of eight weeks, approximately twice as many cortical and trabecular osteocytes from the C57BL/6J mice compared to the C3H/J mice expressed dickkopf 1 (p < 0.005). The number of cortical osteocytes expressing sclerostin was also higher in the C57BL/6J mice (p < 0.05). In contrast, the cortical and trabecular osteocytes expressing periostin were twice as high in the C3H/J mice (p < 0.005). The dickkopf 1 expressing osteocytes of the C57BL/6J mice decreased with age and showed a strain-specific difference only in cortical bone by 16 weeks of age (p < 0.05). In the C3H/J mice, the amount of osteocytes expressing periostin tended to increase with age. Thus, strain-related differences were maintained in 16-week-old rodents (p < 0.005). No strain-specific differences in the expression of FGF23 or osteoprotegerin in the cortical compartment could be detected. This experimental study showed that the osteocytes’ protein expression reflects differences in bone characteristics and strain-related differences during skeletal maturation. Besides the osteocytes’ expression of sclerostin, their expression of dickkopf 1 and periostin seems to be important for bone properties as well.

Published
2022
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31. Pan-cancer analysis of non-coding transcripts reveals the prognostic onco-lncRNA HOXA10-AS in gliomas

Author

Keren Isaev, Lingyan Jiang, Shuai Wu, Christian A. Lee, Valérie Watters, Victoire Fort, Ricky Tsai, Fiona J. Coutinho, Samer M.I. Hussein, Jie Zhang, Jinsong Wu, Peter B. Dirks, Daniel Schramek, and Jüri Reimand

Subjects
long non-coding RNAs, lncRNAs, cancer, prognostic biomarkers, machine learning, glioma, Biology (General), QH301-705.5
Abstract

Summary: Long non-coding RNAs (lncRNAs) are increasingly recognized as functional units in cancer and powerful biomarkers; however, most remain uncharacterized. Here, we analyze 5,592 prognostic lncRNAs in 9,446 cancers of 30 types using machine learning. We identify 166 lncRNAs whose expression correlates with survival and improves the accuracy of common clinical variables, molecular features, and cancer subtypes. Prognostic lncRNAs are often characterized by switch-like expression patterns. In low-grade gliomas, HOXA10-AS activation is a robust marker of poor prognosis that complements IDH1/2 mutations, as validated in another retrospective cohort, and correlates with developmental pathways in tumor transcriptomes. Loss- and gain-of-function studies in patient-derived glioma cells, organoids, and xenograft models identify HOXA10-AS as a potent onco-lncRNA that regulates cell proliferation, contact inhibition, invasion, Hippo signaling, and mitotic and neuro-developmental pathways. Our study underscores the pan-cancer potential of the non-coding transcriptome for identifying biomarkers and regulators of cancer progression.

Published
2021
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32. CRISPR-Switch regulates sgRNA activity by Cre recombination for sequential editing of two loci

Author

Krzysztof Chylinski, Maria Hubmann, Ruth E. Hanna, Connor Yanchus, Georg Michlits, Esther C. H. Uijttewaal, John Doench, Daniel Schramek, and Ulrich Elling

Subjects
Science
Abstract

Inducible genome editing systems often suffer from leakiness or reduced activity. Here the authors develop CRISPR-Switch, a Cre recombinase ON/OFF-controlled sgRNA cassette that allows consecutive editing of two loci.

Published
2019
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33. Opulent Servitude: Shoplifting in a Culture of Material Excess and Systemic Racism

Author

Evangeline Holtz Schramek and Carolyn L. Kane

Subjects
shoplifting, shopping, consumer culture, deviance, resistance, race, gender, Visual arts, N1-9211
Abstract

Why did the latter part of the nineteenth century witness a sudden growth of white, middle class female shoplifters? Psychology tells us that shoplifting is a mental deficiency manifested in women as “kleptomania” (Abelson 4). Given the subsequent international growth of shoplifting, we argue instead that shoplifting is in many ways condoned in contemporary culture: used as a form of social and political control in a late capitalist society. This article first turns to female consumers as shoplifters in the late nineteenth century, alongside the growth of mass production, large-scale department stores, and visually spectacular forms of display. In line with feminist critiques of Marx’s Capital, we uphold the conditions prescribed to women under capitalism and extend this argument to newer forms of systemic racism in the consumer sphere, which ensure that women of colour and of lower economic standing face even greater obstacles to success. Using a broad historical view, we analyze the act of shoplifting in two forms of cultural media, both set in Paris. The first is Émile Zola’s novel The Ladies’ Paradise (1883), based on Paris’s first department store, Le Bon Marché. Due to Zola’s commitment to verisimilitude, we argue, his work offers the strongest corroboration of the ways in which new forms of visual display and a new class of psychologically-entitled females worked together to generate astounding accounts of theft. Our analysis then turns to a work of cinema produced nearly a century and a half later, Céline Sciamma’s 2014 Girlhood. Sciamma portrays a group of young French African girls who navigate their paths into adulthood from the vantage of Bagnolet, a lower income immigrant suburb over four kilometers from Paris’s city centre. The girls experience racial profiling and demonstrate varying forms of resistance, one of them shoplifting. While shoplifting then appears to be an enduring weapon of the weak and strategy of resistance by the dispossessed, leading to, not surprisingly, tacitly permissibility for white middle class women and harsher consequences for women of colour, we conclude that the activity is leveraged to perpetuate pre-existent forms of gendered social control and cultural stereotyping.

Published
2019
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34. Apelin inhibition prevents resistance and metastasis associated with anti‐angiogenic therapy

Author

Iris Uribesalgo, David Hoffmann, Yin Zhang, Anoop Kavirayani, Jelena Lazovic, Judit Berta, Maria Novatchkova, Tsung‐Pin Pai, Reiner A Wimmer, Viktória László, Daniel Schramek, Rezaul Karim, Luigi Tortola, Sumit Deswal, Lisa Haas, Johannes Zuber, Miklós Szűcs, Keiji Kuba, Balazs Dome, Yihai Cao, Bernhard J Haubner, and Josef M Penninger

Subjects
anti‐angiogenic therapy, Apelin–Apelin receptor, therapy‐induced resistance, tumor angiogenesis, VEGF‐VEGFR, Medicine (General), R5-920, Genetics, QH426-470
Abstract

Abstract Angiogenesis is a hallmark of cancer, promoting growth and metastasis. Anti‐angiogenic treatment has limited efficacy due to therapy‐induced blood vessel alterations, often followed by local hypoxia, tumor adaptation, progression, and metastasis. It is therefore paramount to overcome therapy‐induced resistance. We show that Apelin inhibition potently remodels the tumor microenvironment, reducing angiogenesis, and effectively blunting tumor growth. Functionally, targeting Apelin improves vessel function and reduces polymorphonuclear myeloid‐derived suppressor cell infiltration. Importantly, in mammary and lung cancer, Apelin prevents resistance to anti‐angiogenic receptor tyrosine kinase (RTK) inhibitor therapy, reducing growth and angiogenesis in lung and breast cancer models without increased hypoxia in the tumor microenvironment. Apelin blockage also prevents RTK inhibitor‐induced metastases, and high Apelin levels correlate with poor prognosis of anti‐angiogenic therapy patients. These data identify a druggable anti‐angiogenic drug target that reduces tumor blood vessel densities and normalizes the tumor vasculature to decrease metastases.

Published
2019
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35. Federalism and Recent Political Dynamics in Austria

Author

Peter Bussjäger, Christoph Schramek, and Mirella M. Johler

Subjects
federalism, Austria, distribution of competences, education, government program, Political institutions and public administration (General), JF20-2112, Social Sciences
Abstract

From a comparative perspective, the Austrian Federal Constitution appears rather centralized, given that the majority of legislative competences are allocated at the federal level. However, a closer look indicates that the Länder (the federal units) gain considerable political weight by serving as the administrative centre of gravity; namely, the Länder execute their own laws and most of the laws based on the federation’s subject-matters. Hence, one might speak of “administrative federalism”. History shows that Austrian politics resemble a tug-of-war over the federal division of (legislative) competences. The newly elected coalition government’s program joins the ranks of long-winded discussions on how to make Austrian federalism more efficient. Even if pro-federal by rhetoric, the actual content of the government program is either conceptually ambivalent or substantially in favour of increased (legislative) centralization, especially in the realm of social and educational policy.

Published
2018
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36. Prevalence of the Brazilian TP53 Founder c.1010G>A (p.Arg337His) in Lung Adenocarcinoma: Is Genotyping Warranted in All Brazilian Patients?

Author

Igor Araujo Vieira, Tiago Finger Andreis, Bruna Vieira Fernandes, Maria Isabel Achatz, Gabriel S. Macedo, Daniel Schramek, and Patricia Ashton-Prolla

Subjects
TP53 gene, p53 protein, lung adenocarcinoma, founder variant, TP53 (p.Arg337His), R337H, Genetics, QH426-470
Abstract

In Southern and Southeastern Brazil, there is a germline pathogenic variant with incomplete penetrance located in the oligomerization domain of TP53, c.1010G>A (p.Arg337His). Due to a founder effect, the variant is present in 0.3% of the general population of the region. Recently, this variant was identified in 4.4 and 8.9% of two apparently unselected, single center case series of Brazilian lung adenocarcinoma (LUAD) patients from the Southeastern and Central regions of the country, respectively. In the present study, our aim was to examine TP53 c.1010G>A allele and genotype frequencies in LUAD samples obtained from patients diagnosed in Southern Brazil. A total of 586 LUAD samples (tumor DNA) recruited from multiple centers in the region were tested, and the mutant allele was identified using TaqMan® assays in seven cases (7/586, 1.2%) which were submitted to next generation sequencing analyses for confirmation. Somatic EGFR mutations were more frequent in TP53 c.1010G>A carriers than in non-carriers (57.1 vs. 17.6%, respectively). Further studies are needed to confirm if TP53 c.1010G>A is a driver in LUAD carcinogenesis and to verify if there is a combined effect of EGFR and germline TP53 c.1010G>A. Although variant frequency was higher than observed in the general population, it is less than previously reported in LUAD patients from other Brazilian regions. Additional data, producing regional allele frequency information in larger series of patients and including cost-effectiveness analyses, are necessary to determine if TP53 c.1010G>A screening in all Brazilian LUAD patients is justified.

Published
2021
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37. AIF-regulated oxidative phosphorylation supports lung cancer development

Author

Rao, Shuan, Mondragón, Laura, Pranjic, Blanka, Hanada, Toshikatsu, Stoll, Gautier, Köcher, Thomas, Zhang, Peng, Jais, Alexander, Lercher, Alexander, Bergthaler, Andreas, Schramek, Daniel, Haigh, Katharina, Sica, Valentina, Leduc, Marion, Modjtahedi, Nazanine, Pai, Tsung-Pin, Onji, Masahiro, Uribesalgo, Iris, Hanada, Reiko, Kozieradzki, Ivona, Koglgruber, Rubina, Cronin, Shane J., She, Zhigang, Quehenberger, Franz, Popper, Helmut, Kenner, Lukas, Haigh, Jody J., Kepp, Oliver, Rak, Malgorzata, Cai, Kaican, Kroemer, Guido, and Penninger, Josef M.

Published
2019
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38. Germline HAVCR2 mutations altering TIM-3 characterize subcutaneous panniculitis-like T cell lymphomas with hemophagocytic lymphohistiocytic syndrome

Author

Gayden, Tenzin, Sepulveda, Fernando E., Khuong-Quang, Dong-Anh, Pratt, Jonathan, Valera, Elvis T., Garrigue, Alexandrine, Kelso, Susan, Sicheri, Frank, Mikael, Leonie G., Hamel, Nancy, Bajic, Andrea, Dali, Rola, Deshmukh, Shriya, Dervovic, Dzana, Schramek, Daniel, Guerin, Frédéric, Taipale, Mikko, Nikbakht, Hamid, Majewski, Jacek, Moshous, Despina, Charlebois, Janie, Abish, Sharon, Bole-Feysot, Christine, Nitschke, Patrick, Bader-Meunier, Brigitte, Mitchell, David, Thieblemont, Catherine, Battistella, Maxime, Gravel, Simon, Nguyen, Van-Hung, Conyers, Rachel, Diana, Jean-Sebastien, McCormack, Chris, Prince, H. Miles, Besnard, Marianne, Blanche, Stephane, Ekert, Paul G., Fraitag, Sylvie, Foulkes, William D., Fischer, Alain, Neven, Bénédicte, Michonneau, David, de Saint Basile, Geneviève, and Jabado, Nada

Published
2018
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40. In vivo CRISPR screens reveal potent driver mutations in head and neck cancers

Author

Sampath Kumar Loganathan and Daniel Schramek

Subjects
hnscc, notch, mouse models of cancer, long-tail genes, in vivo crispr, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

We have recently tested the transforming potential of 484 ‘long-tail’ genes, which are recurrently albeit infrequently mutated in head and neck cancers (HNSCC). We identified 15 novel tumor suppressors and our top hits converge on regulating the NOTCH signaling pathway. Therapeutic approaches activating NOTCH signaling could be a promising strategy to treat two-thirds of human HNSCC patients.

Published
2020
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41. In Vitro Selection of Cell-Internalizing DNA Aptamers in a Model System of Inflammatory Kidney Disease

Author

Glory Ranches, Melanie Lukasser, Herbert Schramek, Andreas Ploner, Taras Stasyk, Gert Mayer, Günter Mayer, and Alexander Hüttenhofer

Subjects
Therapeutics. Pharmacology, RM1-950
Abstract

Chronic kidney disease (CKD) is a progressive pathological condition marked by a gradual loss of kidney function. Treatment of CKD is most effective when diagnosed at an early stage and patients are still asymptomatic. However, current diagnostic biomarkers (e.g., serum creatinine and urine albumin) are insufficient for prediction of the pathogenesis of the disease. To address this need, we applied a cell-SELEX (systematic evolution of ligands by exponential enrichment) approach and identified a series of DNA aptamers, which exhibit high affinity and selectivity for cytokine-stimulated cells, resembling some aspects of a CKD phenotype. The cell-SELEX approach was driven toward the enrichment of aptamers that internalize via the endosomal pathway by isolating the endosomal fractions in each selection cycle. Indeed, we demonstrated co-localization of selected aptamers with lysosomal-associated membrane protein 1 (LAMP-1), a late endosomal and lysosomal marker protein, by fluorescence in situ hybridization. These findings are consistent with binding and subsequent internalization of the aptamers into cytokine-stimulated cells. Thus, our study sets the stage for applying selected DNA aptamers as theragnostic reagents for the development of targeted therapies to combat CKD. Keywords: cell-SELEX, DNA aptamers, chronic kidney disease, inflammatory kidney disease, cytokines

Published
2017
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45. Apelin inhibition prevents resistance and metastasis associated with anti‐angiogenic therapy

Author

Uribesalgo, Iris, Hoffmann, David, Zhang, Yin, Kavirayani, Anoop, Lazovic, Jelena, Berta, Judit, Novatchkova, Maria, Pai, Tsung‐Pin, Wimmer, Reiner A, László, Viktória, Schramek, Daniel, Karim, Rezaul, Tortola, Luigi, Deswal, Sumit, Haas, Lisa, Zuber, Johannes, Szűcs, Miklós, Kuba, Keiji, Dome, Balazs, Cao, Yihai, Haubner, Bernhard J, and Penninger, Josef M

Published
2019
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47. Is there evidence for a close connection between side of intravesical tumor location and ipsilateral lymphatic spread in lymph node-positive bladder cancer patients at radical cystectomy? Results of the PROMETRICS 2011 database

Author

May, M., Protzel, C., Vetterlein, M. W., Gierth, M., Noldus, J., Karl, A., Grimm, T., Wullich, B., Grimm, M. O., Nuhn, P., Bastian, P. J., Roigas, J., Hadaschik, B., Gilfrich, C., Burger, M., Fisch, M., Brookman-May, S., Aziz, A., Hakenberg, O. W., Bartsch, G., Bolenz, C., Buchner, A., Chun, F. K., Durschnabel, M., Ellinger, J., Fritsche, H. M., Froehner, M., Georgieva, G., Gilfrich, C., Gördük, M., Haferkamp, A., Hartmann, F., Herrmann, E., Hohenfellner, M., Janetschek, G., Keck, B., Kraischits, N., Krausse, A., Lusuardi, L., Martini, T., Mayr, R., Moritz, R., Müller, S. C., Novotny, V., Pahernik, S., Palisaar, R. J., Ponholzer, A., Pycha, A., Rink, M., Roghmann, F., Schmid, M., Schramek, P., Seitz, C., Shariat, S. F., Sikic, D., Stief, C. G., Syring, I., Vallo, S., Wagenlehner, F. M., Wirth, M. P., and the PROMETRICS 2011 Research Group

Published
2017
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48. Impact of photodynamic diagnosis-assisted transurethral resection of bladder tumors on the prognostic outcome after radical cystectomy: results from PROMETRICS 2011

Author

May, Matthias, Fritsche, Hans-Martin, Vetterlein, Malte W., Bastian, Patrick J., Gierth, Michael, Nuhn, Philipp, Aziz, Atiqullah, Fisch, Margit, Stief, Christian G., Hohenfellner, Markus, Wirth, Manfred P., Novotny, Vladimir, Hakenberg, Oliver W., Noldus, Joachim, Gilfrich, Christian, Bolenz, Christian, Burger, Maximilian, Brookman-May, Sabine D., Bartsch, G, Bolenz, C, Buchner, A, Chun, FK, Dahlem, R, Durschnabel, M, Ellinger, J, Froehner, M, Georgieva, G, Gördük, M, Grimm, MO, Grimm, T, Hadaschik, B, Haferkamp, A, Hartmann, F, Herrmann, E, Janetschek, G, Karl, A, Keck, B, Kraischits, N, Krausse, A, Lusuardi, L, Martini, T, Mayr, R, Michel, MS, Moritz, R, Müller, SC, Nuhn, P, Pahernik, S, Palisaar, RJ, Ponholzer, A, Protzel, C, Pycha, A, Rink, M, Roghmann, F, Roigas, J, Schmid, M, Schramek, P, Seitz, C, Shariat, SF, Sikic, D, Syring, I, Vallo, S, Wagenlehner, FM, Wullich, B, and PROMETRICS 2011 Research Group

Published
2017
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49. Ocean-Island Interactions in the Western Pacific

Author

Schramek, Travis Allen

Subjects
Physical oceanography, fore reefs, islands, nearshore processess, oceanography, physical oceanography
Abstract

Coastal processes around islands encompass dynamics on a range of scales with physics that can differ from typical continental shelves due to steeper bathymetry, potentially allowing the surrounding basin waters to ‘communicate’ quickly to the shoreline. This thesis work advances our understanding about these interactions, using a unique set of nearshore oceanographic observations from around the island group encompassed by the Republic of Palau in the tropical western Pacific.The influence of large scale and climatic variability on nearshore island environments can be seen through an empirical model of fore reef temperature structure based on SST and sea level anomaly (SLA) made from nearly two decades of temperature observations (2-90m depth) from three stations around Palau. SLA complements SST by providing a proxy for vertical isotherm displacements driven by local and remote winds on intraseasonal to interannual time scales. Thermal stress on coral ecosystems can now be forecast into the mesophotic zone using this means of predicting subsurface temperatures which are easily accessible for the tropical Pacific. Baroclinic variability around islands has multiple drivers on a range of time scales. Observations of temperature and currents from around the main island group of Palau exhibit a persistent presence of baroclinic coastally trapped waves and internal tides. The largest amplitude signals of coastally trapped waves in fore reef temperature were concurrent with the passage of Typhoon Haiyan, which crossed the northern most Palauan islands in November of 2013. The sub-inertial signals present after Typhoon Haiyan were tracked propagating around the island group for upwards of a week after the typhoon passed. Internal tides were also deemed to be present, but with varying amplitude and phase modulating in and out of phase with the local surface tide. Surface currents impinging upon Palau have a direct impact on the local sea level field around the island group. An array of nearshore pressure gauges, in depths of 20-28 m, encircling the island group and a high resolution (1/120° x 1/120°) regional circulation model are used to examine the space-time characteristics of the flow in a channel in the southern extent of Palau in comparison to the large-scale currents near the island group. A balance between the along-channel pressure difference and bottom friction in the channel was inferred based on the current and pressure observations and the high-resolution model simulations. A drag coefficient for the channel, computed using in situ observations, is O(10-3-10-4). Variations in large-scale zonal currents correlate with the pressure difference across the channel as well as the along-channel flow. The model simulations indicate that as the large-scale flow impinges on the island group, topographic blocking results in a pressure difference on either side of the island which causes a pressure gradient along the channel. The fore reef waters of Palau are shown to be influenced by a range of dynamics across all spatial and temporal scales of our observations. There is an apparent omnipresence of both internal tides and coastally trapped waves throughout the observational window which provide a regular cycling of temperature at depth. These waves have their largest effects at the thermocline, the depth of which can be estimated in this region using only surface variables, as described above. Together, our assessments of these dynamics provide an enhanced perspective on the potential for thermal conditioning of benthic communities living on the outer reef slopes and an advanced perspective of how the large-scale oceanographic field translates to the fore reef environment.

Published
2018

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