Your search keyword '"Fredrik Pontén"' showing total 376 results

1. Imaging of fibrogenesis in the liver by [18F]TZ-Z09591, an Affibody molecule targeting platelet derived growth factor receptor β

Author

Olivia Wegrzyniak, Bo Zhang, Johanna Rokka, Maria Rosestedt, Bogdan Mitran, Pierre Cheung, Emmi Puuvuori, Sofie Ingvast, Jonas Persson, Helena Nordström, John Löfblom, Fredrik Pontén, Fredrik Y. Frejd, Olle Korsgren, Jonas Eriksson, and Olof Eriksson

Subjects

PET imaging, Platelet derived growth factor receptor, Hepatic stellate cells, Fibrogenesis, Liver fibrosis, Medical physics. Medical radiology. Nuclear medicine, R895-920, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Background Platelet-derived growth factor receptor beta (PDGFRβ) is a receptor overexpressed on activated hepatic stellate cells (aHSCs). Positron emission tomography (PET) imaging of PDGFRβ could potentially allow the quantification of fibrogenesis in fibrotic livers. This study aims to evaluate a fluorine-18 radiolabeled Affibody molecule ([18F]TZ-Z09591) as a PET tracer for imaging liver fibrogenesis. Results In vitro specificity studies demonstrated that the trans-Cyclooctenes (TCO) conjugated Z09591 Affibody molecule had a picomolar affinity for human PDGFRβ. Biodistribution performed on healthy rats showed rapid clearance of [18F]TZ-Z09591 through the kidneys and low liver background uptake. Autoradiography (ARG) studies on fibrotic livers from mice or humans correlated with histopathology results. Ex vivo biodistribution and ARG revealed that [18F]TZ-Z09591 binding in the liver was increased in fibrotic livers (p = 0.02) and corresponded to binding in fibrotic scars. Conclusions Our study highlights [18F]TZ-Z09591 as a specific tracer for fibrogenic cells in the fibrotic liver, thus offering the potential to assess fibrogenesis clearly. Graphical abstract

Published

2023

2. Endothelial cell heterogeneity and microglia regulons revealed by a pig cell landscape at single-cell level

Author

Fei Wang, Peiwen Ding, Xue Liang, Xiangning Ding, Camilla Blunk Brandt, Evelina Sjöstedt, Jiacheng Zhu, Saga Bolund, Lijing Zhang, Laura P. M. H. de Rooij, Lihua Luo, Yanan Wei, Wandong Zhao, Zhiyuan Lv, János Haskó, Runchu Li, Qiuyu Qin, Yi Jia, Wendi Wu, Yuting Yuan, Mingyi Pu, Haoyu Wang, Aiping Wu, Lin Xie, Ping Liu, Fang Chen, Jacqueline Herold, Joanna Kalucka, Max Karlsson, Xiuqing Zhang, Rikke Bek Helmig, Linn Fagerberg, Cecilia Lindskog, Fredrik Pontén, Mathias Uhlen, Lars Bolund, Niels Jessen, Hui Jiang, Xun Xu, Huanming Yang, Peter Carmeliet, Jan Mulder, Dongsheng Chen, Lin Lin, and Yonglun Luo

Subjects

Science

Abstract

Pigs are important large animal models for biomedical research. Here, the authors construct a single-cell landscape of pig tissues, unravelling the phenotypic heterogeneity of blood endothelial cells in adipose tissues and the evolutionally conserved regulons of microglia in brains.

Published

2022

3. Genome-wide annotation of protein-coding genes in pig

Author

Max Karlsson, Evelina Sjöstedt, Per Oksvold, Åsa Sivertsson, Jinrong Huang, María Bueno Álvez, Muhammad Arif, Xiangyu Li, Lin Lin, Jiaying Yu, Tao Ma, Fengping Xu, Peng Han, Hui Jiang, Adil Mardinoglu, Cheng Zhang, Kalle von Feilitzen, Xun Xu, Jian Wang, Huanming Yang, Lars Bolund, Wen Zhong, Linn Fagerberg, Cecilia Lindskog, Fredrik Pontén, Jan Mulder, Yonglun Luo, and Mathias Uhlen

Subjects

Annotation, Protein-coding genes, Genome-wide, Transcriptome, Gene expression, Tissue expression profile, Biology (General), QH301-705.5

Abstract

Abstract Background There is a need for functional genome-wide annotation of the protein-coding genes to get a deeper understanding of mammalian biology. Here, a new annotation strategy is introduced based on dimensionality reduction and density-based clustering of whole-body co-expression patterns. This strategy has been used to explore the gene expression landscape in pig, and we present a whole-body map of all protein-coding genes in all major pig tissues and organs. Results An open-access pig expression map ( www.rnaatlas.org ) is presented based on the expression of 350 samples across 98 well-defined pig tissues divided into 44 tissue groups. A new UMAP-based classification scheme is introduced, in which all protein-coding genes are stratified into tissue expression clusters based on body-wide expression profiles. The distribution and tissue specificity of all 22,342 protein-coding pig genes are presented. Conclusions Here, we present a new genome-wide annotation strategy based on dimensionality reduction and density-based clustering. A genome-wide resource of the transcriptome map across all major tissues and organs in pig is presented, and the data is available as an open-access resource ( www.rnaatlas.org ), including a comparison to the expression of human orthologs.

Published

2022

4. Annotation of pituitary neuroendocrine tumors with genome-wide expression analysis

Author

Abdellah Tebani, Jelena Jotanovic, Neda Hekmati, Åsa Sivertsson, Olafur Gudjonsson, Britt Edén Engström, Johan Wikström, Mathias Uhlèn, Olivera Casar-Borota, and Fredrik Pontén

Subjects

PitNET, Transcriptomics, RNA-seq, Pituitary adenoma, Pathology, Omics, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Pituitary neuroendocrine tumors (PitNETs) are common, generally benign tumors with complex clinical characteristics related to hormone hypersecretion and/or growing sellar tumor mass. PitNETs can be classified based on the expression pattern of anterior pituitary hormones and three main transcriptions factors (TF), SF1, PIT1 and TPIT that regulate differentiation of adenohypophysial cells. Here, we have extended this classification based on the global transcriptomics landscape using tumor tissue from a well-defined cohort comprising 51 PitNETs of different clinical and histological types. The molecular profiles were compared with current classification schemes based on immunohistochemistry. Our results identified three main clusters of PitNETs that were aligned with the main pituitary TFs expression patterns. Our analyses enabled further identification of specific genes and expression patterns, including both known and unknown genes, that could distinguish the three different classes of PitNETs. We conclude that the current classification of PitNETs based on the expression of SF1, PIT1 and TPIT reflects three distinct subtypes of PitNETs with different underlying biology and partly independent from the expression of corresponding hormones. The transcriptomic analysis reveals several potentially targetable tumor-driving genes with previously unknown role in pituitary tumorigenesis.

Published

2021

5. Author Correction: Endothelial cell heterogeneity and microglia regulons revealed by a pig cell landscape at single-cell level

Author

Fei Wang, Peiwen Ding, Xue Liang, Xiangning Ding, Camilla Blunk Brandt, Evelina Sjöstedt, Jiacheng Zhu, Saga Bolund, Lijing Zhang, Laura P. M. H. de Rooij, Lihua Luo, Yanan Wei, Wandong Zhao, Zhiyuan Lv, János Haskó, Runchu Li, Qiuyu Qin, Yi Jia, Wendi Wu, Yuting Yuan, Mingyi Pu, Haoyu Wang, Aiping Wu, Lin Xie, Ping Liu, Fang Chen, Jacqueline Herold, Joanna Kalucka, Max Karlsson, Xiuqing Zhang, Rikke Bek Helmig, Linn Fagerberg, Cecilia Lindskog, Fredrik Pontén, Mathias Uhlen, Lars Bolund, Niels Jessen, Hui Jiang, Xun Xu, Huanming Yang, Peter Carmeliet, Jan Mulder, Dongsheng Chen, Lin Lin, and Yonglun Luo

Subjects

Science

Published

2022

6. Affinity Proteomics Exploration of Melanoma Identifies Proteins in Serum with Associations to T-Stage and Recurrence

Author

Sanna Byström, Claudia Fredolini, Per-Henrik Edqvist, Etienne-Nicholas Nyaiesh, Kimi Drobin, Mathias Uhlén, Michael Bergqvist, Fredrik Pontén, and Jochen M. Schwenk

Subjects

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

Abstract

BACKGROUND: Blood-based proteomic profiling may aid and expand our understanding of diseases and their different phenotypes. The aim of the presented study was to profile serum samples from patients with malignant melanoma using affinity proteomic assays to describe proteins in the blood stream that are associated to stage or recurrence of melanoma. MATERIAL AND METHODS: Multiplexed protein analysis was conducted using antibody suspension bead arrays. A total of 232 antibodies against 132 proteins were selected from (i) a screening with 4595 antibodies and 32 serum samples from melanoma patients and controls, (ii) antibodies used for immunohistochemistry, (iii) protein targets previously related with melanoma. The analysis was performed with 149 serum samples from patients with malignant melanoma. Antibody selectivity was then assessed by Western blot, immunocapture mass spectrometry, and epitope mapping. Lastly, indicative antibodies were applied for IHC analysis of melanoma tissues. RESULTS: Serum levels of regucalcin (RGN) and syntaxin 7 (STX7) were found to be lower in patients with both recurring tumors and a high Breslow's thickness (T-stage 3/4) compared to low thickness (T-stage 1/2) without disease recurrence. Serum levels of methylenetetrahydrofolate dehydrogenase 1-like (MTHFD1L) were instead elevated in sera of T3/4 patients with recurrence. The analysis of tissue sections with S100A6 and MTHFD1L showed positive staining in a majority of patients with melanoma, and S100A6 was significantly associated to T-stage. CONCLUSIONS: Our findings provide a starting point to further study RGN, STX7, MTHFD1L and S100A6 in serum to elucidate their involvement in melanoma progression and to assess a possible contribution to support clinical indications.

Published

2017

7. Gene‐specific correlation of RNA and protein levels in human cells and tissues

Author

Fredrik Edfors, Frida Danielsson, Björn M Hallström, Lukas Käll, Emma Lundberg, Fredrik Pontén, Björn Forsström, and Mathias Uhlén

Subjects

gene expression, protein quantification, targeted proteomics, transcriptomics, Biology (General), QH301-705.5, Medicine (General), R5-920

Abstract

Abstract An important issue for molecular biology is to establish whether transcript levels of a given gene can be used as proxies for the corresponding protein levels. Here, we have developed a targeted proteomics approach for a set of human non‐secreted proteins based on parallel reaction monitoring to measure, at steady‐state conditions, absolute protein copy numbers across human tissues and cell lines and compared these levels with the corresponding mRNA levels using transcriptomics. The study shows that the transcript and protein levels do not correlate well unless a gene‐specific RNA‐to‐protein (RTP) conversion factor independent of the tissue type is introduced, thus significantly enhancing the predictability of protein copy numbers from RNA levels. The results show that the RTP ratio varies significantly with a few hundred copies per mRNA molecule for some genes to several hundred thousands of protein copies per mRNA molecule for others. In conclusion, our data suggest that transcriptome analysis can be used as a tool to predict the protein copy numbers per cell, thus forming an attractive link between the field of genomics and proteomics.

Published

2016

8. Transcriptomics resources of human tissues and organs

Author

Mathias Uhlén, Björn M Hallström, Cecilia Lindskog, Adil Mardinoglu, Fredrik Pontén, and Jens Nielsen

Subjects

genome‐scale metabolic models, proteomics, transcriptomics, Biology (General), QH301-705.5, Medicine (General), R5-920

Abstract

Abstract Quantifying the differential expression of genes in various human organs, tissues, and cell types is vital to understand human physiology and disease. Recently, several large‐scale transcriptomics studies have analyzed the expression of protein‐coding genes across tissues. These datasets provide a framework for defining the molecular constituents of the human body as well as for generating comprehensive lists of proteins expressed across tissues or in a tissue‐restricted manner. Here, we review publicly available human transcriptome resources and discuss body‐wide data from independent genome‐wide transcriptome analyses of different tissues. Gene expression measurements from these independent datasets, generated using samples from fresh frozen surgical specimens and postmortem tissues, are consistent. Overall, the different genome‐wide analyses support a distribution in which many proteins are found in all tissues and relatively few in a tissue‐restricted manner. Moreover, we discuss the applications of publicly available omics data for building genome‐scale metabolic models, used for analyzing cell and tissue functions both in physiological and in disease contexts.

Published

2016

9. Mast Cell Infiltration in Human Brain Metastases Modulates the Microenvironment and Contributes to the Metastatic Potential

Author

Ananya Roy, Sylwia Libard, Holger Weishaupt, Ida Gustavsson, Lene Uhrbom, Göran Hesselager, Fredrik J. Swartling, Fredrik Pontén, Irina Alafuzoff, and Elena Tchougounova

Subjects

mast cell, brain metastases, IL-8, IL-10, matrix metalloprotease 2, vascular endothelial growth factor, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Metastatic brain tumors continue to be a clinical problem, despite new therapeutic advances in cancer treatment. Brain metastases (BMs) are among the most common mass lesions in the brain that are resistant to chemotherapies, have a very poor prognosis, and currently lack any efficient diagnostic tests. Predictions estimate that about 40% of lung and breast cancer patients will develop BM. Despite this, very little is known about the immunological and genetic aberrations that drive tumorigenesis in BM. In this study, we demonstrate the infiltration of mast cells (MCs) in a large cohort of human BM samples with different tissues of origin for primary cancer. We applied patient-derived BM cell models to the study of BM cell–MC interactions. BM cells when cocultured with MCs demonstrate enhanced growth and self-renewal capacity. Gene set enrichment analyses indicate increased expression of signal transduction and transmembrane proteins related genes in the cocultured BM cells. MCs exert their effect by release of mediators such as IL-8, IL-10, matrix metalloprotease 2, and vascular endothelial growth factor, thereby permitting metastasis. In conclusion, we provide evidence for a role of MCs in BM. Our findings indicate MCs’ capability of modulating gene expression in BM cells and suggest that MCs can serve as a new target for drug development against metastases in the brain.

Published

2017

10. High RBM3 expression is associated with an improved survival and oxaliplatin response in patients with metastatic colorectal cancer.

Author

Christina Siesing, Halfdan Sorbye, Anca Dragomir, Per Pfeiffer, Camilla Qvortrup, Fredrik Pontén, Karin Jirström, Bengt Glimelius, and Jakob Eberhard

Subjects

Medicine, Science

Abstract

High expression of the RNA-binding motif protein 3 (RBM3) has been shown to correlate, with prolonged survival in several malignant diseases and with the benefit of platinum-based chemotherapy in ovarian cancer. The aim of this study was to evaluate RBM3 in metastatic colorectal cancer (mCRC) as a prognostic factor for overall survival and in relation to benefit of first-line chemotherapy.Immunohistochemical staining was conducted and evaluated in tumours from 455 mCRC patients. Kaplan-Meier analysis and Cox regression proportional hazards models were used to access the impact of RBM3 expression on overall survival (OS) and progression-free survival (PFS).High RBM3 expression, both nuclear and cytoplasmic, was an independent prognostic factor for prolonged OS (hazard ratio [HR] 0.67, 95% confidence interval [CI] 0.50-0.90 and HR 0.66, 95% CI 0.48-0.91, respectively). PFS was significantly longer in patients with high RBM3 expression who had received first-line oxaliplatin based treatment, compared to those who had received irinotecan based treatment, both regarding nuclear and cytoplasmic expression (p-value 0.020 and 0.022 respectively).High RBM3 expression is an independent predictor of prolonged survival in mCRC patients, in particular in patients treated with first-line oxaliplatin based chemotherapy.

Published

2017

11. Affinity proteomics within rare diseases: a BIO‐NMD study for blood biomarkers of muscular dystrophies

Author

Burcu Ayoglu, Amina Chaouch, Hanns Lochmüller, Luisa Politano, Enrico Bertini, Pietro Spitali, Monika Hiller, Eric H Niks, Francesca Gualandi, Fredrik Pontén, Kate Bushby, Annemieke Aartsma‐Rus, Elena Schwartz, Yannick Le Priol, Volker Straub, Mathias Uhlén, Sebahattin Cirak, Peter A C ‘t Hoen, Francesco Muntoni, Alessandra Ferlini, Jochen M Schwenk, Peter Nilsson, and Cristina Al‐Khalili Szigyarto

Subjects

antibody‐based proteomics, disease severity biomarkers, Duchenne muscular dystrophy, plasma profilling, protein profiling, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Despite the recent progress in the broad‐scaled analysis of proteins in body fluids, there is still a lack in protein profiling approaches for biomarkers of rare diseases. Scarcity of samples is the main obstacle hindering attempts to apply discovery driven protein profiling in rare diseases. We addressed this challenge by combining samples collected within the BIO‐NMD consortium from four geographically dispersed clinical sites to identify protein markers associated with muscular dystrophy using an antibody bead array platform with 384 antibodies. Based on concordance in statistical significance and confirmatory results obtained from analysis of both serum and plasma, we identified eleven proteins associated with muscular dystrophy, among which four proteins were elevated in blood from muscular dystrophy patients: carbonic anhydrase III (CA3) and myosin light chain 3 (MYL3), both specifically expressed in slow‐twitch muscle fibers and mitochondrial malate dehydrogenase 2 (MDH2) and electron transfer flavoprotein A (ETFA). Using age‐matched sub‐cohorts, 9 protein profiles correlating with disease progression and severity were identified, which hold promise for the development of new clinical tools for management of dystrophinopathies.

Published

2014

12. CDK‐mediated activation of the SCFFBXO28 ubiquitin ligase promotes MYC‐driven transcription and tumourigenesis and predicts poor survival in breast cancer

Author

Diana Cepeda, Hwee‐Fang Ng, Hamid Reza Sharifi, Salah Mahmoudi, Vanessa Soto Cerrato, Erik Fredlund, Kristina Magnusson, Helén Nilsson, Alena Malyukova, Juha Rantala, Daniel Klevebring, Francesc Viñals, Nimesh Bhaskaran, Siti Mariam Zakaria, Aldwin Suryo Rahmanto, Stefan Grotegut, Michael Lund Nielsen, Cristina Al‐Khalili Szigyarto, Dahui Sun, Mikael Lerner, Sanjay Navani, Martin Widschwendter, Mathias Uhlén, Karin Jirström, Fredrik Pontén, James Wohlschlegel, Dan Grandér, Charles Spruck, Lars‐Gunnar Larsson, and Olle Sangfelt

Subjects

Breast cancer, CDK, F‐box protein, FBXO28, MYC, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract SCF (Skp1/Cul1/F‐box) ubiquitin ligases act as master regulators of cellular homeostasis by targeting key proteins for ubiquitylation. Here, we identified a hitherto uncharacterized F‐box protein, FBXO28 that controls MYC‐dependent transcription by non‐proteolytic ubiquitylation. SCFFBXO28 activity and stability are regulated during the cell cycle by CDK1/2‐mediated phosphorylation of FBXO28, which is required for its efficient ubiquitylation of MYC and downsteam enhancement of the MYC pathway. Depletion of FBXO28 or overexpression of an F‐box mutant unable to support MYC ubiquitylation results in an impairment of MYC‐driven transcription, transformation and tumourigenesis. Finally, in human breast cancer, high FBXO28 expression and phosphorylation are strong and independent predictors of poor outcome. In conclusion, our data suggest that SCFFBXO28 plays an important role in transmitting CDK activity to MYC function during the cell cycle, emphasizing the CDK‐FBXO28‐MYC axis as a potential molecular drug target in MYC‐driven cancers, including breast cancer.

Published

2013

13. A global view of protein expression in human cells, tissues, and organs

Author

Fredrik Pontén, Marcus Gry, Linn Fagerberg, Emma Lundberg, Anna Asplund, Lisa Berglund, Per Oksvold, Erik Björling, Sophia Hober, Caroline Kampf, Sanjay Navani, Peter Nilsson, Jenny Ottosson, Anja Persson, Henrik Wernérus, Kenneth Wester, and Mathias Uhlén

Subjects

antibody‐based analysis, bioimaging, global protein expression, immunofluorescence, immunohistochemistry, Biology (General), QH301-705.5, Medicine (General), R5-920

Abstract

Abstract Defining the protein profiles of tissues and organs is critical to understanding the unique characteristics of the various cell types in the human body. In this study, we report on an anatomically comprehensive analysis of 4842 protein profiles in 48 human tissues and 45 human cell lines. A detailed analysis of over 2 million manually annotated, high‐resolution, immunohistochemistry‐based images showed a high fraction (>65%) of expressed proteins in most cells and tissues, with very few proteins (

Published

2009

14. Defining the Human Brain Proteome Using Transcriptomics and Antibody-Based Profiling with a Focus on the Cerebral Cortex.

Author

Evelina Sjöstedt, Linn Fagerberg, Björn M Hallström, Anna Häggmark, Nicholas Mitsios, Peter Nilsson, Fredrik Pontén, Tomas Hökfelt, Mathias Uhlén, and Jan Mulder

Subjects

Medicine, Science

Abstract

The mammalian brain is a complex organ composed of many specialized cells, harboring sets of both common, widely distributed, as well as specialized and discretely localized proteins. Here we focus on the human brain, utilizing transcriptomics and public available Human Protein Atlas (HPA) data to analyze brain-enriched (frontal cortex) polyadenylated messenger RNA and long non-coding RNA and generate a genome-wide draft of global and cellular expression patterns of the brain. Based on transcriptomics analysis of altogether 27 tissues, we have estimated that approximately 3% (n=571) of all protein coding genes and 13% (n=87) of the long non-coding genes expressed in the human brain are enriched, having at least five times higher expression levels in brain as compared to any of the other analyzed peripheral tissues. Based on gene ontology analysis and detailed annotation using antibody-based tissue micro array analysis of the corresponding proteins, we found the majority of brain-enriched protein coding genes to be expressed in astrocytes, oligodendrocytes or in neurons with molecular properties linked to synaptic transmission and brain development. Detailed analysis of the transcripts and the genetic landscape of brain-enriched coding and non-coding genes revealed brain-enriched splice variants. Several clusters of neighboring brain-enriched genes were also identified, suggesting regulation of gene expression on the chromatin level. This multi-angle approach uncovered the brain-enriched transcriptome and linked genes to cell types and functions, providing novel insights into the molecular foundation of this highly specialized organ.

Published

2015

15. Analysis of the Human Prostate-Specific Proteome Defined by Transcriptomics and Antibody-Based Profiling Identifies TMEM79 and ACOXL as Two Putative, Diagnostic Markers in Prostate Cancer.

Author

Gillian O'Hurley, Christer Busch, Linn Fagerberg, Björn M Hallström, Charlotte Stadler, Anna Tolf, Emma Lundberg, Jochen M Schwenk, Karin Jirström, Anders Bjartell, William M Gallagher, Mathias Uhlén, and Fredrik Pontén

Subjects

Medicine, Science

Abstract

To better understand prostate function and disease, it is important to define and explore the molecular constituents that signify the prostate gland. The aim of this study was to define the prostate specific transcriptome and proteome, in comparison to 26 other human tissues. Deep sequencing of mRNA (RNA-seq) and immunohistochemistry-based protein profiling were combined to identify prostate specific gene expression patterns and to explore tissue biomarkers for potential clinical use in prostate cancer diagnostics. We identified 203 genes with elevated expression in the prostate, 22 of which showed more than five-fold higher expression levels compared to all other tissue types. In addition to previously well-known proteins we identified two poorly characterized proteins, TMEM79 and ACOXL, with potential to differentiate between benign and cancerous prostatic glands in tissue biopsies. In conclusion, we have applied a genome-wide analysis to identify the prostate specific proteome using transcriptomics and antibody-based protein profiling to identify genes with elevated expression in the prostate. Our data provides a starting point for further functional studies to explore the molecular repertoire of normal and diseased prostate including potential prostate cancer markers such as TMEM79 and ACOXL.

Published

2015

16. The Urinary Bladder Transcriptome and Proteome Defined by Transcriptomics and Antibody-Based Profiling.

Author

Masato Habuka, Linn Fagerberg, Björn M Hallström, Fredrik Pontén, Tadashi Yamamoto, and Mathias Uhlen

Subjects

Medicine, Science

Abstract

To understand functions and diseases of urinary bladder, it is important to define its molecular constituents and their roles in urinary bladder biology. Here, we performed genome-wide deep RNA sequencing analysis of human urinary bladder samples and identified genes up-regulated in the urinary bladder by comparing the transcriptome data to those of all other major human tissue types. 90 protein-coding genes were elevated in the urinary bladder, either with enhanced expression uniquely in the urinary bladder or elevated expression together with at least one other tissue (group enriched). We further examined the localization of these proteins by immunohistochemistry and tissue microarrays and 20 of these 90 proteins were localized to the whole urothelium with a majority not yet described in the context of the urinary bladder. Four additional proteins were found specifically in the umbrella cells (Uroplakin 1a, 2, 3a, and 3b), and three in the intermediate/basal cells (KRT17, PCP4L1 and ATP1A4). 61 of the 90 elevated genes have not been previously described in the context of urinary bladder and the corresponding proteins are interesting targets for more in-depth studies. In summary, an integrated omics approach using transcriptomics and antibody-based profiling has been used to define a comprehensive list of proteins elevated in the urinary bladder.

Published

2015

17. The kidney transcriptome and proteome defined by transcriptomics and antibody-based profiling.

Author

Masato Habuka, Linn Fagerberg, Björn M Hallström, Caroline Kampf, Karolina Edlund, Åsa Sivertsson, Tadashi Yamamoto, Fredrik Pontén, Mathias Uhlén, and Jacob Odeberg

Subjects

Medicine, Science

Abstract

To understand renal functions and disease, it is important to define the molecular constituents of the various compartments of the kidney. Here, we used comparative transcriptomic analysis of all major organs and tissues in the human body, in combination with kidney tissue micro array based immunohistochemistry, to generate a comprehensive description of the kidney-specific transcriptome and proteome. A special emphasis was placed on the identification of genes and proteins that were elevated in specific kidney subcompartments. Our analysis identified close to 400 genes that had elevated expression in the kidney, as compared to the other analysed tissues, and these were further subdivided, depending on expression levels, into tissue enriched, group enriched or tissue enhanced. Immunohistochemistry allowed us to identify proteins with distinct localisation to the glomeruli (n = 11), proximal tubules (n = 120), distal tubules (n = 9) or collecting ducts (n = 8). Among the identified kidney elevated transcripts, we found several proteins not previously characterised or identified as elevated in kidney. This description of the kidney specific transcriptome and proteome provides a resource for basic and clinical research to facilitate studies to understand kidney biology and disease.

Published

2014

18. The human pancreas proteome defined by transcriptomics and antibody-based profiling.

Author

Angelika Danielsson, Fredrik Pontén, Linn Fagerberg, Björn M Hallström, Jochen M Schwenk, Mathias Uhlén, Olle Korsgren, and Cecilia Lindskog

Subjects

Medicine, Science

Abstract

The pancreas is composed of both exocrine glands and intermingled endocrine cells to execute its diverse functions, including enzyme production for digestion of nutrients and hormone secretion for regulation of blood glucose levels. To define the molecular constituents with elevated expression in the human pancreas, we employed a genome-wide RNA sequencing analysis of the human transcriptome to identify genes with elevated expression in the human pancreas. This quantitative transcriptomics data was combined with immunohistochemistry-based protein profiling to allow mapping of the corresponding proteins to different compartments and specific cell types within the pancreas down to the single cell level. Analysis of whole pancreas identified 146 genes with elevated expression levels, of which 47 revealed a particular higher expression as compared to the other analyzed tissue types, thus termed pancreas enriched. Extended analysis of in vitro isolated endocrine islets identified an additional set of 42 genes with elevated expression in these specialized cells. Although only 0.7% of all genes showed an elevated expression level in the pancreas, this fraction of transcripts, in most cases encoding secreted proteins, constituted 68% of the total mRNA in pancreas. This demonstrates the extreme specialization of the pancreas for production of secreted proteins. Among the elevated expression profiles, several previously not described proteins were identified, both in endocrine cells (CFC1, FAM159B, RBPJL and RGS9) and exocrine glandular cells (AQP12A, DPEP1, GATM and ERP27). In summary, we provide a global analysis of the pancreas transcriptome and proteome with a comprehensive list of genes and proteins with elevated expression in pancreas. This list represents an important starting point for further studies of the molecular repertoire of pancreatic cells and their relation to disease states or treatment effects.

Published

2014

19. European H16N3 gull influenza virus attaches to the human respiratory tract and eye.

Author

Cecilia Lindskog, Patrik Ellström, Björn Olsen, Fredrik Pontén, Debby van Riel, Vincent J Munster, Daniel González-Acuña, Thijs Kuiken, and Elsa Jourdain

Subjects

Medicine, Science

Abstract

We explored the attachment of an H16N3 influenza virus to human, mallard, and gull tissues using virus histochemistry applied to tissue microarrays and employing human and mallard viruses as references. Of the viruses tested, the H16N3 gull virus most readily attached to the human respiratory tract and eye. These results underscore the need to assess the potential for gull influenza viruses to replicate in human tissues and further investigate the role of gulls in influenza virus ecology.

Published

2013

20. GABA-A channel subunit expression in human glioma correlates with tumor histology and clinical outcome.

Author

Anja Smits, Zhe Jin, Tamador Elsir, Hugo Pedder, Monica Nistér, Irina Alafuzoff, Anna Dimberg, Per-Henrik Edqvist, Fredrik Pontén, Eleonora Aronica, and Bryndis Birnir

Subjects

Medicine, Science

Abstract

GABA (γ-aminobutyric acid) is the main inhibitory neurotransmitter in the CNS and is present in high concentrations in presynaptic terminals of neuronal cells. More recently, GABA has been ascribed a more widespread role in the control of cell proliferation during development where low concentrations of extrasynaptic GABA induce a tonic activation of GABA receptors. The GABA-A receptor consists of a ligand-gated chloride channel, formed by five subunits that are selected from 19 different subunit isoforms. The functional and pharmacological properties of the GABA-A channels are dictated by their subunit composition. Here we used qRT-PCR to compare mRNA levels of all 19 GABA-A channel subunits in samples of human glioma (n = 29) and peri-tumoral tissue (n = 5). All subunits except the ρ1 and ρ3 subunit were consistently detected. Lowest mRNA levels were found in glioblastoma compared to gliomas of lower malignancy, except for the θ subunit. The expression and cellular distribution of the α1, γ1, ρ2 and θ subunit proteins was investigated by immunohistochemistry on tissue microarrays containing 87 gliomas grade II. We found a strong co-expression of ρ2 and θ subunits in both astrocytomas (r = 0.86, p

Published

2012

21. Scalable in situ hybridization on tissue arrays for validation of novel cancer and tissue-specific biomarkers.

Author

Sara Kiflemariam, Sandra Andersson, Anna Asplund, Fredrik Pontén, and Tobias Sjöblom

Subjects

Medicine, Science

Abstract

Tissue localization of gene expression is increasingly important for accurate interpretation of large scale datasets from expression and mutational analyses. To this end, we have (1) developed a robust and scalable procedure for generation of mRNA hybridization probes, providing >95% first-pass success rate in probe generation to any human target gene and (2) adopted an automated staining procedure for analyses of formalin-fixed paraffin-embedded tissues and tissue microarrays. The in situ mRNA and protein expression patterns for genes with known as well as unknown tissue expression patterns were analyzed in normal and malignant tissues to assess procedure specificity and whether in situ hybridization can be used for validating novel antibodies. We demonstrate concordance between in situ transcript and protein expression patterns of the well-known pathology biomarkers KRT17, CHGA, MKI67, PECAM1 and VIL1, and provide independent validation for novel antibodies to the biomarkers BRD1, EZH2, JUP and SATB2. The present study provides a foundation for comprehensive in situ gene set or transcriptome analyses of human normal and tumor tissues.

Published

2012

22. ZBED6, a novel transcription factor derived from a domesticated DNA transposon regulates IGF2 expression and muscle growth.

Author

Ellen Markljung, Lin Jiang, Jacob D Jaffe, Tarjei S Mikkelsen, Ola Wallerman, Martin Larhammar, Xiaolan Zhang, Li Wang, Veronica Saenz-Vash, Andreas Gnirke, Anders M Lindroth, Romain Barrés, Jie Yan, Sara Strömberg, Sachinandan De, Fredrik Pontén, Eric S Lander, Steven A Carr, Juleen R Zierath, Klas Kullander, Claes Wadelius, Kerstin Lindblad-Toh, Göran Andersson, Göran Hjälm, and Leif Andersson

Subjects

Biology (General), QH301-705.5

Abstract

A single nucleotide substitution in intron 3 of IGF2 in pigs abrogates a binding site for a repressor and leads to a 3-fold up-regulation of IGF2 in skeletal muscle. The mutation has major effects on muscle growth, size of the heart, and fat deposition. Here, we have identified the repressor and find that the protein, named ZBED6, is previously unknown, specific for placental mammals, and derived from an exapted DNA transposon. Silencing of Zbed6 in mouse C2C12 myoblasts affected Igf2 expression, cell proliferation, wound healing, and myotube formation. Chromatin immunoprecipitation (ChIP) sequencing using C2C12 cells identified about 2,500 ZBED6 binding sites in the genome, and the deduced consensus motif gave a perfect match with the established binding site in Igf2. Genes associated with ZBED6 binding sites showed a highly significant enrichment for certain Gene Ontology classifications, including development and transcriptional regulation. The phenotypic effects in mutant pigs and ZBED6-silenced C2C12 myoblasts, the extreme sequence conservation, its nucleolar localization, the broad tissue distribution, and the many target genes with essential biological functions suggest that ZBED6 is an important transcription factor in placental mammals, affecting development, cell proliferation, and growth.

Published

2009

23. Data from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

Purpose: Global gene expression profiling has been widely used in lung cancer research to identify clinically relevant molecular subtypes as well as to predict prognosis and therapy response. So far, the value of these multigene signatures in clinical practice is unclear, and the biologic importance of individual genes is difficult to assess, as the published signatures virtually do not overlap.Experimental Design: Here, we describe a novel single institute cohort, including 196 non–small lung cancers (NSCLC) with clinical information and long-term follow-up. Gene expression array data were used as a training set to screen for single genes with prognostic impact. The top 450 probe sets identified using a univariate Cox regression model (significance level P < 0.01) were tested in a meta-analysis including five publicly available independent lung cancer cohorts (n = 860).Results: The meta-analysis revealed 14 genes that were significantly associated with survival (P < 0.001) with a false discovery rate Conclusions: Using a novel NSCLC cohort together with a meta-analysis validation approach, we have identified a set of single genes with independent prognostic impact. One of these genes, CADM1, was further established as an immunohistochemical marker with a potential application in clinical diagnostics. Clin Cancer Res; 19(1); 194–204. ©2012 AACR.

Published

2023

24. Supplementary Table 1 from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

PDF file - 29K, Characteristics of NSCLC patients from Uppsala for tissue microarray analysis

Published

2023

25. Supplementary Table 4 from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

XLSX file - 24K, Excel file including uni- and multivariate analysis of the top 17 prognostic probe sets

Published

2023

26. Supplementary Discussion from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

PDF file - 117K, Analysis of the 14 gene sinature risk score of Kratz et al., 2012

Published

2023

27. Supplementary Figure 3 from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

PDF file - 41K, Kaplan-Meier plots of recurrence free survival according CADM1 gene expression

Published

2023

28. Supplementary Table 2 from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

PDF file - 25K, Characteristics of NSCLC patients from �rebro for tissue microarray analysis

Published

2023

29. Supplementary Figure 2 from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

PDF file - 312K, Kaplan-Meier suvival plots of the Uppsala cohort for the top prognostic genes according to gene expression

Published

2023

30. Supplementary Figure 4 from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

PDF file - 39K, Kaplan-Meier suvival plot of stage I adenocarcinoma patients according to protein expression

Published

2023

31. Supplementary Figure 1 from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

PDF file - 123K, Survival plot and Kaplan-Meier analysis of clinical parameters in the Uppsala cohort

Published

2023

32. Supplementary Table 5 from Biomarker Discovery in Non–Small Cell Lung Cancer: Integrating Gene Expression Profiling, Meta-analysis, and Tissue Microarray Validation

Author

Patrick Micke, Jan G Hengstler, Jörg Rahnenführer, Christina Karlsson, Gisela Helenius, Mats Karlsson, Oswaldo Fernandes, André König, Fredrik Pontén, Michael Bergqvist, Simon Ekman, Anders Berglund, Mats Lambe, Lars Holmberg, Birte Hellwig, Miriam Lohr, Karolina Edlund, and Johan Botling

Abstract

PDF file - 28K, COX regression analysis for CADM1 protein expression in the Uppsala cohort

Published

2023

33. Supplementary Figure S3 from Elevated Expression of the C-Type Lectin CD93 in the Glioblastoma Vasculature Regulates Cytoskeletal Rearrangements That Enhance Vessel Function and Reduce Host Survival

Author

Anna Dimberg, Anja Smits, Fredrik Pontén, Magnus Essand, George Trendelenburg, Johan Lööf, Wesam Bazzar, Maria Georganaki, Tamador Elsir Abu Elhassan, Hua Huang, Roberta Lugano, Lei Zhang, and Elise Langenkamp

Abstract

Effect of CD93-deficiency in T241 and GL261 necrosis, hypoxia, and apoptosis.

Published

2023

34. Data from Guidance Molecule SEMA3A Restricts Tumor Growth by Differentially Regulating the Proliferation of Tumor-Associated Macrophages

Author

Charlotte Rolny, John Andersson, Arne Östman, Michele De Palma, Angelo De Milito, Jonas Bergh, Johan Hartman, Fredrik Pontén, Mario Leonardo Squadrito, Paola Pellegrini, Pradeepa Pangigadde, Emma Nygren, Nicholas P. Tobin, Artur Mezheyeuski, Jeanette Östling, Margarita Bartish, Tatjana Wallmann, and Majken Wallerius

Abstract

Accumulation of tumor-associated macrophages (TAM) correlates with malignant progression, immune suppression, and poor prognosis. In this study, we defined a critical role for the cell-surface guidance molecule SEMA3A in differential proliferative control of TAMs. Tumor cell–derived SEMA3A restricted the proliferation of protumoral M2 macrophages but increased the proliferation of antitumoral M1, acting through the SEMA3A receptor neuropilin 1. Expansion of M1 macrophages in vivo enhanced the recruitment and activation of natural killer (NK) cells and cytotoxic CD8+ T cells to tumors, inhibiting their growth. In human breast cancer specimens, we found that immunohistochemical levels of SEMA3A correlated with the expression of genes characteristic of M1 macrophages, CD8+ T cells, and NK cells, while inversely correlating with established characters of malignancy. In summary, our results illuminate a mechanism whereby the TAM phenotype is controlled and identify the cell-surface molecule SEMA3A as a candidate for therapeutic targeting. Cancer Res; 76(11); 3166–78. ©2016 AACR.

Published

2023

35. Supplemental Figure Legends from Guidance Molecule SEMA3A Restricts Tumor Growth by Differentially Regulating the Proliferation of Tumor-Associated Macrophages

Author

Charlotte Rolny, John Andersson, Arne Östman, Michele De Palma, Angelo De Milito, Jonas Bergh, Johan Hartman, Fredrik Pontén, Mario Leonardo Squadrito, Paola Pellegrini, Pradeepa Pangigadde, Emma Nygren, Nicholas P. Tobin, Artur Mezheyeuski, Jeanette Östling, Margarita Bartish, Tatjana Wallmann, and Majken Wallerius

Abstract

Legend for Supplemental Figures S1-S6.

Published

2023

36. Supplemental Figure S2 from Guidance Molecule SEMA3A Restricts Tumor Growth by Differentially Regulating the Proliferation of Tumor-Associated Macrophages

Author

Charlotte Rolny, John Andersson, Arne Östman, Michele De Palma, Angelo De Milito, Jonas Bergh, Johan Hartman, Fredrik Pontén, Mario Leonardo Squadrito, Paola Pellegrini, Pradeepa Pangigadde, Emma Nygren, Nicholas P. Tobin, Artur Mezheyeuski, Jeanette Östling, Margarita Bartish, Tatjana Wallmann, and Majken Wallerius

Abstract

SEMA3AS EFFECT ON MONOCYTES AND MACROPHAGES.

Published

2023

37. Supplementary Table S1 from Elevated Expression of the C-Type Lectin CD93 in the Glioblastoma Vasculature Regulates Cytoskeletal Rearrangements That Enhance Vessel Function and Reduce Host Survival

Author

Anna Dimberg, Anja Smits, Fredrik Pontén, Magnus Essand, George Trendelenburg, Johan Lööf, Wesam Bazzar, Maria Georganaki, Tamador Elsir Abu Elhassan, Hua Huang, Roberta Lugano, Lei Zhang, and Elise Langenkamp

Abstract

Semi-quantitative scoring of CD93 expression in 236 human glioma biopsies.

Published

2023

38. Supplemental Table S1 from Guidance Molecule SEMA3A Restricts Tumor Growth by Differentially Regulating the Proliferation of Tumor-Associated Macrophages

Author

Charlotte Rolny, John Andersson, Arne Östman, Michele De Palma, Angelo De Milito, Jonas Bergh, Johan Hartman, Fredrik Pontén, Mario Leonardo Squadrito, Paola Pellegrini, Pradeepa Pangigadde, Emma Nygren, Nicholas P. Tobin, Artur Mezheyeuski, Jeanette Östling, Margarita Bartish, Tatjana Wallmann, and Majken Wallerius

Abstract

TaqMan gene expression assays used for qPCR.

Published

2023

39. Supplementary Materials and Methods from Elevated Expression of the C-Type Lectin CD93 in the Glioblastoma Vasculature Regulates Cytoskeletal Rearrangements That Enhance Vessel Function and Reduce Host Survival

Author

Anna Dimberg, Anja Smits, Fredrik Pontén, Magnus Essand, George Trendelenburg, Johan Lööf, Wesam Bazzar, Maria Georganaki, Tamador Elsir Abu Elhassan, Hua Huang, Roberta Lugano, Lei Zhang, and Elise Langenkamp

Abstract

Description of additional methods and procedures used in the study.

Published

2023

40. Spatial immunophenotyping of the tumour microenvironment in non-small cell lung cancer

Author

Max Backman, Carina Strell, Amanda Lindberg, Johanna S.M. Mattsson, Hedvig Elfving, Hans Brunnström, Aine O'Reilly, Martina Bosic, Miklos Gulyas, Johan Isaksson, Johan Botling, Klas Kärre, Karin Jirström, Kristina Lamberg, Fredrik Pontén, Karin Leandersson, Artur Mezheyeuski, Patrick Micke, Institut Català de la Salut, [Backman M, Lindberg A, Mattsson JSM, Elfving H] Department of Immunology, Genetics and Pathology, Uppsala University, Uppsala, Sweden. [Strell C] Department of Immunology, Genetics and Pathology, Uppsala University, Uppsala, Sweden. Centre for Cancer Biomarkers CCBIO, Department of Clinical Medicine, University of Bergen, Bergen, Norway. [Brunnström H] Division of Pathology, Department of Clinical Sciences Lund, Lund University, Lund, Sweden. [Mezheyeuski A] Department of Immunology, Genetics and Pathology, Uppsala University, Uppsala, Sweden. Molecular Oncology Group, Vall d'Hebron Institute of Oncology (VHIO), Barcelona, Spain, and Vall d'Hebron Barcelona Hospital Campus

Subjects

Diagnosis::Diagnostic Techniques and Procedures::Clinical Laboratory Techniques::Immunologic Tests::Immunophenotyping [ANALYTICAL, DIAGNOSTIC AND THERAPEUTIC TECHNIQUES, AND EQUIPMENT], Cancer Research, Tumour microenvironment, Cancer och onkologi, diagnóstico::técnicas y procedimientos diagnósticos::técnicas de laboratorio clínico::pruebas inmunológicas::inmunofenotipificación [TÉCNICAS Y EQUIPOS ANALÍTICOS, DIAGNÓSTICOS Y TERAPÉUTICOS], Otros calificadores::/diagnóstico [Otros calificadores], Neoplasms::Neoplasms by Site::Thoracic Neoplasms::Respiratory Tract Neoplasms::Lung Neoplasms::Bronchial Neoplasms::Carcinoma, Bronchogenic::Carcinoma, Non-Small-Cell Lung [DISEASES], neoplasias::neoplasias por localización::neoplasias torácicas::neoplasias del tracto respiratorio::neoplasias pulmonares::neoplasias de los bronquios::carcinoma broncogénico::carcinoma de pulmón de células no pequeñas [ENFERMEDADES], Multiplex imaging, Checkpoint therapy, NSCLC, Cèl·lules T, Oncology, Immune cell infiltration, Cancer and Oncology, Pulmons - Càncer - Diagnòstic, Other subheadings::/diagnosis [Other subheadings], Lung cancer

Abstract

Checkpoint therapy; Lung cancer; Tumour microenvironment Terapia de puntos de control; Cáncer de pulmón; Microambiente tumoral Teràpia de punts de control; Càncer de pulmó; Microambient tumoral Introduction: Immune cells in the tumour microenvironment are associated with prognosis and response to therapy. We aimed to comprehensively characterise the spatial immune phenotypes in the mutational and clinicopathological background of non-small cell lung cancer (NSCLC). Methods: We established a multiplexed fluorescence imaging pipeline to spatially quantify 13 immune cell subsets in 359 NSCLC cases: CD4 effector cells (CD4-Eff), CD4 regulatory cells (CD4-Treg), CD8 effector cells (CD8-Eff), CD8 regulatory cells (CD8-Treg), B-cells, natural killer cells, natural killer T-cells, M1 macrophages (M1), CD163+ myeloid cells (CD163), M2 macrophages (M2), immature dendritic cells (iDCs), mature dendritic cells (mDCs) and plasmacytoid dendritic cells (pDCs). Results: CD4-Eff cells, CD8-Eff cells and M1 macrophages were the most abundant immune cells invading the tumour cell compartment and indicated a patient group with a favourable prognosis in the cluster analysis. Likewise, single densities of lymphocytic subsets (CD4-Eff, CD4-Treg, CD8-Treg, B-cells and pDCs) were independently associated with longer survival. However, when these immune cells were located close to CD8-Treg cells, the favourable impact was attenuated. In the multivariable Cox regression model, including cell densities and distances, the densities of M1 and CD163 cells and distances between cells (CD8-Treg-B-cells, CD8-Eff-cancer cells and B-cells-CD4-Treg) demonstrated positive prognostic impact, whereas short M2-M1 distances were prognostically unfavourable. Conclusion: We present a unique spatial profile of the in situ immune cell landscape in NSCLC as a publicly available data set. Cell densities and cell distances contribute independently to prognostic information on clinical outcomes, suggesting that spatial information is crucial for diagnostic use. This study was partly supported by Swedish Cancer Society, The Lions Cancer Foundation Uppsala, Sweden, Selanders Foundation and The Sjöberg Foundation, Sweden.

Published

2023

41. Next generation pan-cancer blood proteome profiling using proximity extension assay

Author

Mathias Uhlen, María Bueno Álvez, Fredrik Edfors, Kalle von Feilitzen, Martin Zwahlen, adil mardinoglu, Per-Henrik Edqvist, Tobias Sjöblom, Emma Lundin, Natallia Rameika, Tomas Axelsson, Mikael Åberg, Jessica Nordlund, Wen Zhong, Max Karlsson, Ulf Gyllensten, Fredrik Pontén, and Linn Fagerberg

Abstract

Cancer is a highly heterogeneous disease in need of accurate and non-invasive diagnostic tools. Here, we describe a novel strategy to explore the proteome signature by comprehensive analysis of protein levels using a pan-cancer approach of patients representing the major cancer types. Plasma profiles of 1,463 proteins from more than 1,400 cancer patients representing altogether 12 common cancer types were measured in minute amounts of blood plasma collected at the time of diagnosis and before treatment. AI-based disease prediction models allowed for the identification of a set of proteins associated with each of the analyzed cancers. By combining the results from all cancer types, a panel of proteins suitable for the identification of all individual cancer types was defined. The results are presented in a new open access Human Disease Blood Atlas. The implication for cancer precision medicine of next generation plasma profiling is discussed.

Published

2022

42. Spatiotemporal dissection of the cell cycle with single-cell proteogenomics

Author

Diana Mahdessian, Fredrik Pontén, Mathias Uhlén, Manuel D. Leonetti, Fredric Johansson, Anna Bäckström, Christian Gnann, Frida Danielsson, Emma Lundberg, Lovisa Stenström, Peter Thul, Adil Mardinoglu, Nathan H. Cho, Cheng Zhang, Rutger Shutten, Devin P. Sullivan, Charlotte Stadler, Oana Carja, Trang Le, Ulrika Axelsson, Cecilia Lindskog, Anthony J. Cesnik, Muhammad Arif, and Burcu Ayoglu

Subjects

Time Factors, Proteome, Cell division, Cell, Mitosis, Cell Cycle Proteins, Cell fate determination, Biology, Proteomics, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Cell Line, Tumor, Human proteome project, medicine, Humans, Cell Lineage, Phosphorylation, Interphase, Cell Proliferation, Proteogenomics, 030304 developmental biology, Oncogene Proteins, 0303 health sciences, Multidisciplinary, Cell growth, Cell Cycle, Cell cycle, Cell biology, medicine.anatomical_structure, Single-Cell Analysis, Protein Kinases, 030217 neurology & neurosurgery

Abstract

The cell cycle, over which cells grow and divide, is a fundamental process of life. Its dysregulation has devastating consequences, including cancer1-3. The cell cycle is driven by precise regulation of proteins in time and space, which creates variability between individual proliferating cells. To our knowledge, no systematic investigations of such cell-to-cell proteomic variability exist. Here we present a comprehensive, spatiotemporal map of human proteomic heterogeneity by integrating proteomics at subcellular resolution with single-cell transcriptomics and precise temporal measurements of individual cells in the cell cycle. We show that around one-fifth of the human proteome displays cell-to-cell variability, identify hundreds of proteins with previously unknown associations with mitosis and the cell cycle, and provide evidence that several of these proteins have oncogenic functions. Our results show that cell cycle progression explains less than half of all cell-to-cell variability, and that most cycling proteins are regulated post-translationally, rather than by transcriptomic cycling. These proteins are disproportionately phosphorylated by kinases that regulate cell fate, whereas non-cycling proteins that vary between cells are more likely to be modified by kinases that regulate metabolism. This spatially resolved proteomic map of the cell cycle is integrated into the Human Protein Atlas and will serve as a resource for accelerating molecular studies of the human cell cycle and cell proliferation.

Published

2021

43. Lipogenic signalling modulates prostate cancer cell adhesion and migration via modification of Rho GTPases

Author

Salpie Nowinski, Mario De Piano, Valeria Manuelli, Fredrik Pontén, Giorgia Zadra, Massimo Loda, Jonathan Otte, Mieke Van Hemelrijck, Athanasios Niaouris, Per-Henrik Edqvist, Anita Grigoriadis, and Claire M. Wells

Subjects

Male, rho GTP-Binding Proteins, 0301 basic medicine, Cancer Research, CDC42, GTPase, Article, Metastasis, 03 medical and health sciences, 0302 clinical medicine, Palmitoylation, Cell Movement, Cell Line, Tumor, Genetics, Humans, Cell migration, Protein palmitoylation, Phosphorylation, cdc42 GTP-Binding Protein, Molecular Biology, Paxillin, Cell Proliferation, Cancer och onkologi, biology, Cell growth, Lipogenesis, Prostate, Cell adhesion, Prostatic Neoplasms, Cell biology, Fatty Acid Synthase, Type I, Gene Expression Regulation, Neoplastic, Fatty acid synthase, 030104 developmental biology, Cancer and Oncology, 030220 oncology & carcinogenesis, biology.protein, Signal Transduction

Abstract

Fatty acid synthase (FASN) is commonly overexpressed in prostate cancer and associated with tumour progression. FASN is responsible for de novo synthesis of the fatty acid palmitate; the building block for protein palmitoylation. Recent work has suggested that alongside its established role in promoting cell proliferation FASN may also promote invasion. We now find depletion of FASN expression increases prostate cancer cell adhesiveness, impairs HGF-mediated cell migration and reduces 3D invasion. These changes in motility suggest that FASN can mediate actin cytoskeletal remodelling; a process known to be downstream of Rho family GTPases. Here, we demonstrate that modulation of FASN expression specifically impacts on the palmitoylation of the atypical GTPase RhoU. Impaired RhoU activity in FASN depleted cells leads to reduced adhesion turnover downstream of paxillin serine phosphorylation, which is rescued by addition of exogenous palmitate. Moreover, canonical Cdc42 expression is dependent on the palmitoylation status of RhoU. Thus we uncover a novel relationship between FASN, RhoU and Cdc42 that directly influences cell migration potential. These results provide compelling evidence that FASN activity directly promotes cell migration and supports FASN as a potential therapeutic target in metastatic prostate cancer.

Published

2020

44. Antibody Validation for Estrogen Receptor Beta

Author

Madeleine, Birgersson, Borbala, Katona, Cecilia, Lindskog, Fredrik, Pontén, and Cecilia, Williams

Subjects

Blotting, Western, Estrogen Receptor beta, Humans, Immunoprecipitation, Immunohistochemistry, Antibodies

Abstract

Antibodies can cross-react with proteins other than their intended targets, and antibody-based applications can, if not properly validated, lead to flawed interpretations. When evaluating 13 anti-estrogen receptor beta (ERβ) antibodies in 2017, we concluded that only one of them was specific. Applying this antibody in immunohistochemistry of over 44 different normal human tissues and 20 types of cancers revealed ERβ expression in only a few selected tissues. This aligned with mRNA evidence but contradicted a large set of published literature. ERβ protein expression continues to be reported in tissues without clear support by mRNA expression. In this chapter, we describe how ERβ antibodies can be thoroughly validated and discuss selection of well-characterized positive and negative controls. The validation scheme presented is applicable for immunohistochemistry and Western blotting. The protocol includes evaluation of mRNA evidence, use of public databases, assessment of on- and off-target binding, and an optional step for corroboration with immunoprecipitation and mass spectrometry.

Published

2022

45. Antibody Validation for Estrogen Receptor Beta

Author

Madeleine Birgersson, Borbala Katona, Cecilia Lindskog, Fredrik Pontén, and Cecilia Williams

Published

2022

46. Combined expression of HOXA11 and CD10 identifies endometriosis versus normal tissue and tumors

Author

Jutta Huvila, Matts Olovsson, Sofie Gustafsson, Per-Henrik Edqvist, Julia Bergman-Larsson, Anna Tolf, Fredrik Pontén, and Loren Méar

Subjects

Pathology, medicine.medical_specialty, Endometriosis, Uterus, Reproduktionsmedicin och gynekologi, Cervix Uteri, Endometrium, Differential diagnostics, Pathology and Forensic Medicine, Diagnosis, Differential, Obstetrics, Gynecology and Reproductive Medicine, Biopsy, Medicine, Humans, Fallopian Tubes, Homeodomain Proteins, Tissue microarray, medicine.diagnostic_test, business.industry, Gynecological malignancies, Ovary, General Medicine, Gold standard (test), medicine.disease, Immunohistochemistry, Endometrial Neoplasms, medicine.anatomical_structure, Female, Neprilysin, Stromal Cells, business, Ovarian cancer, Biomarkers

Abstract

The gold standard for diagnosing endometriosis is by laparoscopic visual demonstration of ectopic endometrial lesions outside the uterus, preferably verified by biopsy and microscopical examination. Molecular markers to facilitate the microscopical diagnosis of endometriosis and for distinguishing endometriosis from other benign and malignant lesions are lacking. Our aim was to test and validate an immunohistochemical antibody panel for improved diagnostic accuracy of endometriosis. Both CD10 and HOXA11 have been implicated in regulation of endometrial homeostasis. Here we have analyzed the expression pattern of these two proteins using immunohistochemistry on human tissues in a tissue microarray format. CD10 and HOXA11 expression in endometriosis lesions were compared to expression patterns in a range of normal tissues and in primary- and metastatic lesions of endometrial-, cervical- and ovarian cancer. HOXA11 and CD10 were expressed in 98% and 91% of endometriosis lesions and the combined double-positive expression profile of both HOXA11 and CD10 was highly sensitive for ectopic endometrial tissue (90%). The specificity and sensitivity for this double-positive signature in endometriosis was significantly different from all investigated tissues, cancers and metastases except normal, eutopic endometrial- and cervical mucosa. The combination of HOXA11 and CD10 expression profiles provides a useful tool to identify ectopic endometrial tissue and for distinguishing endometriosis from various types of gynecological malignancies and metastases. De 2 första författarna delar förstaförfattarskapet

Published

2021

47. A human adipose tissue cell-type transcriptome atlas

Author

Marthe Norreen-Thorsen, Eike Christopher Struck, Sofia Öling, Martin Zwahlen, Kalle Von Feilitzen, Jacob Odeberg, Cecilia Lindskog, Fredrik Pontén, Mathias Uhlén, Philip James Dusart, and Lynn Marie Butler

Subjects

Male, Adipose Tissue, Cellbiologi, Cell- och molekylärbiologi, Gene Expression Profiling, Subcutaneous Fat, Humans, Cell Biology, Intra-Abdominal Fat, Transcriptome, Cell and Molecular Biology, General Biochemistry, Genetics and Molecular Biology

Abstract

The importance of defining cell-type-specific genes is well acknowledged. Technological advances facilitate high-resolution sequencing of single cells, but practical challenges remain. Adipose tissue is composed pri-marily of adipocytes, large buoyant cells requiring extensive, artefact-generating processing for separation and analysis. Thus, adipocyte data are frequently absent from single-cell RNA sequencing (scRNA-seq) data -sets, despite being the primary functional cell type. Here, we decipher cell-type-enriched transcriptomes from unfractionated human adipose tissue RNA-seq data. We profile all major constituent cell types, using 527 visceral adipose tissue (VAT) or 646 subcutaneous adipose tissue (SAT) samples, identifying over 2,300 cell-type-enriched transcripts. Sex-subset analysis uncovers a panel of male-only cell-type-enriched genes. By resolving expression profiles of genes differentially expressed between SAT and VAT, we identify mesothelial cells as the primary driver of this variation. This study provides an accessible method to profile cell-type-enriched transcriptomes using bulk RNA-seq, generating a roadmap for adipose tissue biology.

Published

2021

48. ELTD1 deletion reduces vascular abnormality and improves T-cell recruitment after PD-1 blockade in glioma

Author

Anna Dimberg, Bàrbara Laviña, Maria Georganaki, Lei Liu Conze, Hua Huang, Luuk van Hooren, Kalyani Vemuri, Tiarne van de Walle, Liqun He, Lei Zhang, Roberta Lugano, Mohanraj Ramachandran, Peetra U. Magnusson, Fredrik Pontén, Christer Betsholtz, Michael Bergqvist, Elisabetta Dejana, and Anja Smits

Subjects

Cancer Research, Cell- och molekylärbiologi, medicine.medical_treatment, T cell, T-Lymphocytes, Programmed Cell Death 1 Receptor, ELTD1, Receptors, G-Protein-Coupled, Mice, Downregulation and upregulation, glioma, Glioma, Cell Line, Tumor, Medicine, Animals, Humans, Receptor, ADGRL4, vascular normalization, Mice, Knockout, Tissue microarray, business.industry, Brain Neoplasms, Endothelial Cells, Immunotherapy, medicine.disease, Phenotype, medicine.anatomical_structure, Oncology, Basic and Translational Investigations, Cancer research, Increased inflammatory response, immunotherapy, Neurology (clinical), business, Cell and Molecular Biology, Gene Deletion

Abstract

Background Tumor vessels in glioma are molecularly and functionally abnormal, contributing to treatment resistance. Proteins differentially expressed in glioma vessels can change vessel phenotype and be targeted for therapy. ELTD1 (Adgrl4) is an orphan member of the adhesion G-protein-coupled receptor family upregulated in glioma vessels and has been suggested as a potential therapeutic target. However, the role of ELTD1 in regulating vessel function in glioblastoma is poorly understood. Methods ELTD1 expression in human gliomas and its association with patient survival was determined using tissue microarrays and public databases. The role of ELTD1 in regulating tumor vessel phenotype was analyzed using orthotopic glioma models and ELTD1−/− mice. Endothelial cells isolated from murine gliomas were transcriptionally profiled to determine differentially expressed genes and pathways. The consequence of ELTD1 deletion on glioma immunity was determined by treating tumor-bearing mice with PD-1-blocking antibodies. Results ELTD1 levels were upregulated in human glioma vessels, increased with tumor malignancy, and were associated with poor patient survival. Progression of orthotopic gliomas was not affected by ELTD1 deletion, however, tumor vascular function was improved in ELTD1−/− mice. Bioinformatic analysis of differentially expressed genes indicated increased inflammatory response and decreased proliferation in tumor endothelium in ELTD1−/− mice. Consistent with an enhanced inflammatory response, ELTD1 deletion improved T-cell infiltration in GL261-bearing mice after PD-1 checkpoint blockade. Conclusion Our data demonstrate that ELTD1 participates in inducing vascular dysfunction in glioma, and suggest that targeting of ELTD1 may normalize the vessels and improve the response to immunotherapy.

Published

2021

49. Infiltration of NK and plasma cells is associated with a distinct immune subset in non-small cell lung cancer

Author

Johan Botling, Johan Isaksson, Linnea La Fleur, Dijana Djureinovic, Fredrik Pontén, Klas Kärre, Amanda Lindberg, Hans Brunnström, Victor Pontén, Cecilia Lindskog, Artur Mezheyeuski, Karin Leandersson, Carina Strell, Mohamed Eltahir, Patrick Micke, Karin Jirström, Max Backman, Miklos Gulyas, Sara M. Mangsbo, Johanna Sofia Margareta Mattsson, Pinja Kurppa, and Hedvig Elfving

Subjects

PD-L1, p53, Adult, Male, Lung Neoplasms, medicine.medical_treatment, animal diseases, Plasma Cells, chemical and pharmacologic phenomena, Stem cell marker, NSCLC, Pathology and Forensic Medicine, Immune system, Lymphocytes, Tumor-Infiltrating, Carcinoma, Non-Small-Cell Lung, medicine, Tumor Microenvironment, tumor microenvironment, Humans, Aged, Tumor microenvironment, Cancer och onkologi, Innate immune system, biology, Clinical Laboratory Medicine, immune cell infiltration, FOXP3, Immunotherapy, biochemical phenomena, metabolism, and nutrition, Middle Aged, Killer Cells, Natural, lung cancer, Klinisk laboratoriemedicin, checkpoint therapy, Cancer and Oncology, biology.protein, Cancer research, bacteria, Female, CD8

Abstract

Immune cells of the tumor microenvironment are central but erratic targets for immunotherapy. The aim of this study was to characterize novel patterns of immune cell infiltration in non-small cell lung cancer (NSCLC) in relation to its molecular and clinicopathologic characteristics. Lymphocytes (CD3+, CD4+, CD8+, CD20+, FOXP3+, CD45RO+), macrophages (CD163+), plasma cells (CD138+), NK cells (NKp46+), PD1+, and PD-L1+ were annotated on a tissue microarray including 357 NSCLC cases. Somatic mutations were analyzed by targeted sequencing for 82 genes and a tumor mutational load score was estimated. Transcriptomic immune patterns were established in 197 patients based on RNA sequencing data. The immune cell infiltration was variable and showed only poor association with specific mutations. The previously defined immune phenotypic patterns, desert, inflamed, and immune excluded, comprised 30, 13, and 57% of cases, respectively. Notably, mRNA immune activation and high estimated tumor mutational load were unique only for the inflamed pattern. However, in the unsupervised cluster analysis, including all immune cell markers, these conceptual patterns were only weakly reproduced. Instead, four immune classes were identified: (1) high immune cell infiltration, (2) high immune cell infiltration with abundance of CD20+ B cells, (3) low immune cell infiltration, and (4) a phenotype with an imprint of plasma cells and NK cells. This latter class was linked to better survival despite exhibiting low expression of immune response-related genes (e.g. CXCL9, GZMB, INFG, CTLA4). This compartment-specific immune cell analysis in the context of the molecular and clinical background of NSCLC reveals two previously unrecognized immune classes. A refined immune classification, including traits of the humoral and innate immune response, is important to define the immunogenic potency of NSCLC in the era of immunotherapy. © 2021 The Authors. The Journal of Pathology published by John Wiley & Sons, Ltd. on behalf of The Pathological Society of Great Britain and Ireland.

Published

2021

50. Stroma-normalised vessel density predicts benefit from adjuvant fluorouracil-based chemotherapy in patients with stage II/III colon cancer

Author

Bengt Glimelius, Eric Osterman, Mia Karlberg, Anna Portyanko, Peter Ragnhammar, Arne Östman, Ina Hrynchyk, Fredrik Pontén, Tobias Sjöblom, Mercedes Herrera, David Edler, and Artur Mezheyeuski

Subjects

Oncology, Cancer Research, medicine.medical_specialty, Colorectal cancer, medicine.medical_treatment, Population, Predictive markers, Article, 03 medical and health sciences, 0302 clinical medicine, Stroma, Internal medicine, Statistical significance, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Neoplasm Invasiveness, education, Neoplasm Staging, Chemotherapy, education.field_of_study, business.industry, medicine.disease, Colon cancer, Fluorouracil, 030220 oncology & carcinogenesis, Colonic Neoplasms, Cohort, business, Adjuvant, medicine.drug

Abstract

Background Identification of biomarkers associated with benefit of adjuvant chemotherapy in stage II/III colon cancer is an important task. Methods Vessel density (VD) and tumour stroma were analysed in a randomised-trial-derived discovery cohort (n = 312) and in a stage II/III group of a population-based validation cohort (n = 85). VD was scored separately in the tumour centre, invasive margin and peritumoral stroma compartments and quantitated as VD/total analysed tissue area or VD/stroma area. Results High stroma-normalised VD in the invasive margin was associated with significantly longer time to recurrence and overall survival (OS) (p = 0.002 and p = 0.006, respectively) in adjuvant-treated patients of the discovery cohort, but not in surgery-only patients. Stroma-normalised VD in the invasive margin and treatment effect were significantly associated according to a formal interaction test (p = 0.009). Similarly, in the validation cohort, high stroma-normalised VD was associated with OS in adjuvant-treated patients, although statistical significance was not reached (p = 0.051). Conclusion Through the use of novel digitally scored vessel-density-related metrics, this exploratory study identifies stroma-normalised VD in the invasive margin as a candidate marker for benefit of adjuvant 5-FU-based chemotherapy in stage II/III colon cancer. The findings, indicating particular importance of vessels in the invasive margin, also suggest biological mechanisms for further exploration.

Published

2019