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1,232 results on '"Brünner, Nils"'

201. Positron emission tomography/computed tomography for optimized colon cancer staging and follow-up.

Author

Engelmann, Bodil E., primary, Loft, Annika, additional, Kjær, Andreas, additional, Nielsen, Hans J., additional, Berthelsen, Anne Kiil, additional, Binderup, Tina, additional, Brinch, Kim, additional, Brünner, Nils, additional, Høyer-Hansen, Gunilla, additional, Gerds, Thomas A., additional, Kristensen, Michael Holmsgaard, additional, Kurt, Engin Y., additional, Latocha, Jan E., additional, Lindblom, Gunnar, additional, Sloth, Carsten, additional, and Højgaard, Liselotte, additional

Published
2014
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202. Positron emission tomography/computed tomography for early treatment response evaluation in metastatic colon cancer.

Author

Engelmann, Bodil E., primary, Loft, Annika, additional, Kjær, Andreas, additional, Nielsen, Hans J., additional, von Benzon, Eric, additional, Brünner, Nils, additional, Christensen, Ib Jarle, additional, Gerds, Thomas A., additional, Hansson, Susanne H., additional, Hollander, Niels Henrik, additional, Kristensen, Michael Holmsgaard, additional, Löfgren, Johan, additional, Markova, Elena, additional, Sloth, Carsten, additional, and Højgaard, Liselotte, additional

Published
2014
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204. An explorative analysis of ERCC1-19q13 copy number aberrations in a chemonaive stage III colorectal cancer cohort

Author

Smith, David Hersi, Christensen, Ib Jarle, Jensen, Niels Frank, Markussen, Bo, Müller, Sven, Nielsen, Hans Jørgen, Brünner, Nils, Nielsen1,7, Kirsten Vang, Smith, David Hersi, Christensen, Ib Jarle, Jensen, Niels Frank, Markussen, Bo, Müller, Sven, Nielsen, Hans Jørgen, Brünner, Nils, and Nielsen1,7, Kirsten Vang

Abstract

Background: Platinum-based chemotherapy has long been used in the treatment of a variety of cancers and functions by inducing DNA damage. ERCC1 and ERCC4 are involved in the removal of this damage and have previously been implicated in resistance to platinum compounds. The aim of the current investigation is to determine the presence, frequency and prognostic impact of ERCC1 or ERCC4 gene copy number alterations in colorectal cancer (CRC). Methods: Fluorescent in situ hybridization probes directed at ERCC1 and ERCC4 with relevant reference probes were constructed. Probes were tested in a CRC cell line panel and in tumor sections from 152 stage III CRC chemonaive patients. Relationships between biomarker status and clinical endpoints (overall survival, time to recurrence, and local recurrence in rectal cancer) were analyzed by survival statistics. Results: ERCC1-19q13 copy number alterations were observed in a single cell line metaphase (HT29). In patient material, ERCC1-19q13 copy number gains (ERCC1-19q13/CEN-2 ≥ 1.5) were detected in 27.0% of specimens, whereas ERCC1-19q13 deletions (ERCC1-19q13/CEN-2 < 0.8) were only detected in 1.3%. ERCC1-19q13 gain was significantly associated with longer survival (multivariate analysis, HR: 0.45, 95% CI: 0.20-1.00, p = 0.049) in patients with colon tumors, but not rectal tumors. No ERCC4 aberrations were detected and scoring was discontinued after 50 patients. Conclusions: ERCC1-19q13 copy number gains occur frequently in stage III CRC and influences survival in patients with colon tumors. Future studies will investigate the effect of ERCC1-19q13 aberrations in a platinum-treated patient population with the aim of developing a predictive biomarker profile for oxaliplatin sensitivity in CRC.

Published
2013

205. Integrative analyses of gene expression and DNA methylation profiles in breast cancer cell line models of tamoxifen-resistance indicate a potential role of cells with stem-like properties

Author

Lin, Xue, Li, Jian, Yin, Guangliang, Zhao, Qian, Elias, Daniel, Lykkesfeldt, Anne, Stenvang, Jan, Brünner, Nils, Wang, Jun, Yang, Huanming, Bolund, Lars, Ditzel, Henrik Jørn, Lin, Xue, Li, Jian, Yin, Guangliang, Zhao, Qian, Elias, Daniel, Lykkesfeldt, Anne, Stenvang, Jan, Brünner, Nils, Wang, Jun, Yang, Huanming, Bolund, Lars, and Ditzel, Henrik Jørn

Abstract

Development of resistance to tamoxifen is an important clinical issue in the treatment of breast cancer. Tamoxifen resistance may be the result of acquisition of epigenetic regulation within breast cancer cells, such as DNA methylation, resulting in changed mRNA expression of genes pivotal for estrogen-dependent growth. Alternatively, tamoxifen resistance may be due to selection of pre-existing resistant cells, or a combination of the two mechanisms.

Published
2013

206. Plasma levels of the MMP-9:TIMP-1 complex as prognostic biomarker in breast cancer:a retrospective study

Author

Thorsen, Stine Buch, Christensen, Sarah Louise T, Würtz, Sidse Ørnbjerg, Lundberg, Martin, Nielsen, Birgitte Egedie Sander, Jensen, Lena Vinther, Knowles, Mick, Gee, Nick, Fredriksson, Simon, Møller, Susanne, Brünner, Nils, Rasmussen, Anne-Sofie Schrohl, Stenvang, Jan, Thorsen, Stine Buch, Christensen, Sarah Louise T, Würtz, Sidse Ørnbjerg, Lundberg, Martin, Nielsen, Birgitte Egedie Sander, Jensen, Lena Vinther, Knowles, Mick, Gee, Nick, Fredriksson, Simon, Møller, Susanne, Brünner, Nils, Rasmussen, Anne-Sofie Schrohl, and Stenvang, Jan

Abstract

Worldwide more than one million women are annually diagnosed with breast cancer. A considerable fraction of these women receive systemic adjuvant therapy; however, some are cured by primary surgery and radiotherapy alone. Prognostic biomarkers guide stratification of patients into different risk groups and hence improve management of breast cancer patients. Plasma levels of Matrix Metalloproteinase-9 (MMP-9) and its natural inhibitor Tissue inhibitor of metalloproteinase-1 (TIMP-1) have previously been associated with poor patient outcome and resistance to certain forms of chemotherapy. To pursue additional prognostic information from MMP-9 and TIMP-1, the level of the MMP-9 and TIMP-1 complex (MMP-9:TIMP-1) was investigated in plasma from breast cancer patients.

Published
2013

207. Biomarker-guided repurposing of chemotherapeutic drugs for cancer therapy:a novel strategy in drug development

Author

Stenvang, Jan, Kümler, Iben, Nygård, Sune Boris, Smith, David Hersi, Nielsen, Dorte, Brünner, Nils, Moreira, José, Stenvang, Jan, Kümler, Iben, Nygård, Sune Boris, Smith, David Hersi, Nielsen, Dorte, Brünner, Nils, and Moreira, José

Abstract

Cancer is a leading cause of mortality worldwide and matters are only set to worsen as its incidence continues to rise. Traditional approaches to combat cancer include improved prevention, early diagnosis, optimized surgery, development of novel drugs, and honing regimens of existing anti-cancer drugs. Although discovery and development of novel and effective anti-cancer drugs is a major research area, it is well known that oncology drug development is a lengthy process, extremely costly and with high attrition rates. Furthermore, those drugs that do make it through the drug development mill are often quite expensive, laden with severe side-effects and unfortunately, to date, have only demonstrated minimal increases in overall survival. Therefore, a strong interest has emerged to identify approved non-cancer drugs that possess anti-cancer activity, thus shortcutting the development process. This research strategy is commonly known as drug repurposing or drug repositioning and provides a faster path to the clinics. We have developed and implemented a modification of the standard drug repurposing strategy that we review here; rather than investigating target-promiscuous non-cancer drugs for possible anti-cancer activity, we focus on the discovery of novel cancer indications for already approved chemotherapeutic anti-cancer drugs. Clinical implementation of this strategy is normally commenced at clinical phase II trials and includes pre-treated patients. As the response rates to any non-standard chemotherapeutic drug will be relatively low in such a patient cohort it is a pre-requisite that such testing is based on predictive biomarkers. This review describes our strategy of biomarker-guided repurposing of chemotherapeutic drugs for cancer therapy, taking the repurposing of topoisomerase I (Top1) inhibitors and Top1 as a potential predictive biomarker as case in point.

Published
2013

208. Is TIMP-1 immunoreactivity alone or in combination with other markers a predictor of benefit from anthracyclines in the BR9601 adjuvant breast cancer chemotherapy trial?

Author

Munro, Alison F., Bartels, Annette, Balslev, Eva, Twelves, Christopher J., Cameron, David A, Brünner, Nils, Bartlett, John Ms, Munro, Alison F., Bartels, Annette, Balslev, Eva, Twelves, Christopher J., Cameron, David A, Brünner, Nils, and Bartlett, John Ms

Abstract

INTRODUCTION: Predictive cancer biomarkers to guide the right treatment to the right patient at the right time are strongly needed. The purpose of the present study was to validate prior results that tissue inhibitor of metalloproteinase 1 (TIMP-1) alone or in combination with either HER2 or TOP2A copy number can be used to predict benefit from epirubicin (E) containing chemotherapy compared with cyclophosphamide, methotrexate and fluorouracil (CMF) treatment. METHODS: For the purpose of this study, formalin fixed paraffin embedded tumor tissue from women recruited into the BR9601 clinical trial, which randomized patients to E-CMF versus CMF, were analyzed for TIMP-1 immunoreactivity. Using previously collected data for HER2 amplification and TOP2A gene aberrations, we defined patients as "anthracycline non-responsive", that is, 2T (TIMP-1 immunoreactive and TOP2A normal) and HT (TIMP-1 immunoreactive and HER2 negative) and anthracycline responsive (all other cases). RESULTS: In total, 288 tumors were available for TIMP-1 analysis with (183/274) 66.8%, and (181/274) 66.0% being classed as 2T and HT responsive, respectively. TIMP-1 was neither associated with patient prognosis (relapse free survival or overall survival) nor with a differential effect of E-CMF and CMF. Also, TIMP-1 did not add to the predictive value of HER2, TOP2A gene aberrations, or to Ki67 immunoreactivity. CONCLUSION: This study could not confirm the predictive value of TIMP-1 immunoreactivity in patients randomized to receive E-CMF versus CMF as adjuvant treatment for primary breast cancer.

Published
2013

209. TIMP1 overexpression mediates resistance of MCF-7 human breast cancer cells to fulvestrant and down-regulates progesterone receptor expression

Author

Bjerre, Christina Annette, Jensen, Lena Vinther, Belling, Kirstine Christensen, Würtz, Sidse Ørnbjerg, Yadav, Rachita, Lademann, Ulrik Axel, Rigina, Olga, Do, Khoa Nguyen, Ditzel, Henrik Jørn, Lykkesfeldt, Anne Elisabeth, Wang, Jun, Nielsen, Henrik Bjørn, Brünner, Nils, Gupta, Ramneek, Rasmussen, Anne-Sofie Schrohl, Stenvang, Jan, Bjerre, Christina Annette, Jensen, Lena Vinther, Belling, Kirstine Christensen, Würtz, Sidse Ørnbjerg, Yadav, Rachita, Lademann, Ulrik Axel, Rigina, Olga, Do, Khoa Nguyen, Ditzel, Henrik Jørn, Lykkesfeldt, Anne Elisabeth, Wang, Jun, Nielsen, Henrik Bjørn, Brünner, Nils, Gupta, Ramneek, Rasmussen, Anne-Sofie Schrohl, and Stenvang, Jan

Abstract

High levels of Tissue Inhibitor of Metalloproteinases-1 (TIMP1) are associated with poor prognosis, reduced response to chemotherapy, and, potentially, also poor response to endocrine therapy in breast cancer patients. Our objective was to further investigate the hypothesis that TIMP1 is associated with endocrine sensitivity. We established a panel of 11 MCF-7 subclones with a wide range of TIMP1 mRNA and protein expression levels. Cells with high expression of TIMP1 versus low TIMP1 displayed significantly reduced sensitivity to the antiestrogen fulvestrant (ICI 182,780, Faslodex®), while TIMP1 levels did not influence the sensitivity to 4-hydroxytamoxifen. An inverse correlation between expression of the progesterone receptor and TIMP1 was found, but TIMP1 levels did not correlate with estrogen receptor levels or growth-promoting effects of estrogen (estradiol, E2). Additionally, the effects of fulvestrant, 4-hydroxytamoxifen, or estrogen on estrogen receptor expression were not associated with TIMP1 levels. Gene expression analyses revealed associations between expression of TIMP1 and genes involved in metabolic pathways, epidermal growth factor receptor 1/cancer signaling pathways, and cell cycle. Gene and protein expression analyses showed no general defects in estrogen receptor signaling except from lack of progesterone receptor expression and estrogen inducibility in clones with high TIMP1. The present study suggests a relation between high expression level of TIMP1 and loss of progesterone receptor expression combined with fulvestrant resistance. Our findings in vitro may have clinical implications as the data suggest that high tumor levels of TIMP1 may be a predictive biomarker for reduced response to fulvestrant.

Published
2013

210. High expression of microRNA-625-3p is associated with poor response to first-line oxaliplatin based treatment of metastatic colorectal cancer

Author

Rasmussen, Mads Heilskov, Jensen, Niels Frank, Tarpgaard, Line Schmidt, Qvortrup, Camilla, Rømer, Maria Unni Koefoed, Stenvang, Jan, Hansen, Tine Plato, Christensen, Lise Lotte, Lindebjerg, Jan, Hansen, Flemming, Jensen, Benny V., Hansen, Torben F., Pfeiffer, Per, Brünner, Nils, Ørntoft, Torben Falck, Andersen, Claus Lindbjerg, Rasmussen, Mads Heilskov, Jensen, Niels Frank, Tarpgaard, Line Schmidt, Qvortrup, Camilla, Rømer, Maria Unni Koefoed, Stenvang, Jan, Hansen, Tine Plato, Christensen, Lise Lotte, Lindebjerg, Jan, Hansen, Flemming, Jensen, Benny V., Hansen, Torben F., Pfeiffer, Per, Brünner, Nils, Ørntoft, Torben Falck, and Andersen, Claus Lindbjerg

Abstract

The backbone of current cytotoxic treatment of metastatic colorectal cancer (mCRC) consists of a fluoropyrimidine together with either oxaliplatin (XELOX/FOLFOX) or irinotecan (XELIRI/FOLFIRI). With an overall objective response rate of approximately 50% for either treatment combination, a major unsolved problem is that no predictors of response to these treatments are available. To address this issue, we profiled 742 microRNAs in laser-capture microdissected cancer cells from responding and non-responding patients receiving XELOX/FOLFOX as first-line treatment for mCRC, and identified, among others, high expression of miR-625-3p, miR-181b and miR-27b to be associated with poor clinical response. In a validation cohort of 94 mCRC patients treated first-line with XELOX, high expression of miR-625-3p was confirmed to be associated with poor response (OR = 6.25, 95%CI [1.8; 21.0]). Independent analyses showed that miR-625-3p was not dysregulated between normal and cancer samples, nor was its expression associated with recurrence of stage II or III disease, indicating that miR-625-3p solely is a response marker. Finally, we also found that these miRNAs were up-regulated in oxaliplatin resistant HCT116/oxPt (miR-625-3p, miR-181b and miR-27b) and LoVo/oxPt (miR-181b) colon cancer cell lines as compared with their isogenic parental cells. Altogether, our results suggest an association between miR-625-3p and response to first-line oxaliplatin based chemotherapy of mCRC.

Published
2013

211. Proximity probing assays for simultaneous visualization of protein complexes in situ

Author

Moreira, José, Thorsen, Stine Buch, Brünner, Nils, Stenvang, Jan, Moreira, José, Thorsen, Stine Buch, Brünner, Nils, and Stenvang, Jan

Abstract

EVALUATION OF: Leuchowius KJ, Clausson CM, Grannas K et al. Parallel visualization of multiple protein complexes in individual cells in tumor tissue. Mol. Cell Proteomics doi:10.1074/mcp.O112.023374 (2013) (Epub ahead of print). Techniques for in situ detection and quantification of proteins in fixed tissue remain an important element of both basic biological analyses and clinical biomarker research. The practical importance of such techniques can be exemplified by the everyday clinical use of immunohistochemical detection of the estrogen receptor and HER2 in tissues from breast cancer patients. Several techniques are currently available for detection of single proteins and post-translational modifications, but very few are suitable for detection of protein complexes. Methods that enable simultaneous detection and quantification of protein complexes provide novel possibilities for understanding the biological role(s) of protein complexes and may open new opportunities to improve clinical biomarker research. Leuchowius et al. describe an improved proximity ligation assay for in situ detection of protein complexes, which is able to detect and quantify several protein complexes simultaneously in the same tissue specimen.

Published
2013

212. Underpinning the repurposing of anthracyclines towards colorectal cancer:assessment of topoisomerase II alpha gene copy number alterations in colorectal cancer

Author

Nygård, Sune Boris, Christensen, Ib Jarle, Smith, David Hersi, Nielsen, Signe Lykke, Jensen, Niels Frank, Nielsen, Hans Jørgen, Vainer, Ben, Brünner, Nils, Nygård, Sune Boris, Christensen, Ib Jarle, Smith, David Hersi, Nielsen, Signe Lykke, Jensen, Niels Frank, Nielsen, Hans Jørgen, Vainer, Ben, and Brünner, Nils

Abstract

Objective. We propose a repurposing strategy where anthracyclines are reintroduced to a subgroup of patients with metastatic colorectal cancer with the highest likelihood of response. In breast cancer, DNA topoisomerase II alpha gene (TOP2A) alterations predict incremental benefit of anthracyclines, but this association has not been investigated in colorectal cancer. Frequency analysis of TOP2A gene alterations in colorectal cancer and the association with prognosis are evaluated and the challenges of using a TOP2A/CEN-17 FISH probe combination are addressed. Material and methods. Formalin-fixed, paraffin-embedded material from 154 stage III colorectal cancer patients included in the RANX05 clinical trial was retrospectively assessed for TOP2A gene alterations using FISH. The TOP2A/CEN-17 ratio as well as the TOP2A gene copy number alone was used to define gene alterations and associations between gene status and outcomes were analyzed. Results. TOP2A gene gain was a frequent finding with 9.8 % having a total of ≥4 TOP2A copies per cell. According to the TOP2A/CEN-17 ratio, 10.5 % had TOP2A gene gain. Polysomy or gain of the centromere region of chromosome-17 was not as frequent as reported in breast cancer. No prognostic characteristic of TOP2A was identified. Conclusion. TOP2A gene gain is present in numbers relevant to identify a subgroup of patients who may benefit from anthracycline therapy. Based on the present findings, we will initiate a prospective clinical trial designed to evaluate this hypothesis in patients with metastatic colorectal cancer who have failed 5-fluorouracil and oxaliplatin chemotherapy.

Published
2013

213. Association of tissue inhibitor of metalloproteinases-1 and Ki67 in estrogen receptor positive breast cancer

Author

Bjerre, Christina Annette, Knoop, Ann, Bjerre, Karsten, Larsen, Mathilde S., Henriksen, Katrine L., Lyng, Maria Bibi, Ditzel, Henrik, Rasmussen, Birgitte B, Brünner, Nils, Ejlertsen, Bent, Lænkholm, Anne-Vibeke, Bjerre, Christina Annette, Knoop, Ann, Bjerre, Karsten, Larsen, Mathilde S., Henriksen, Katrine L., Lyng, Maria Bibi, Ditzel, Henrik, Rasmussen, Birgitte B, Brünner, Nils, Ejlertsen, Bent, and Lænkholm, Anne-Vibeke

Abstract

The role of tissue inhibitor of metalloproteinases-1 (TIMP-1) in estrogen receptor (ER) positive breast cancer remains to be fully elucidated. We evaluated TIMP-1 as a prognostic marker in patients treated with adjuvant tamoxifen and investigated TIMP-1s association with Ki67 and ER/progesterone receptor (PR)/human epidermal growth factor receptor 2 (HER2) profiles.

Published
2013

214. Tissue inhibitor of metalloproteinase 1 (TIMP-1) as a biomarker in gastric cancer:a review

Author

Grunnet, Mie, Mau-Sørensen, Morten, Brünner, Nils, Grunnet, Mie, Mau-Sørensen, Morten, and Brünner, Nils

Abstract

The value of Tissue Inhibitor of MetalloProteinase-1 (TIMP-1) as a biomarker in patients with gastric cancer (GC) is widely debated. The aim of this review is to evaluate available literature describing the association between levels of TIMP-1 in tumor tissue and/or blood and the prognosis of patients suffering from GC.

Published
2013

217. TIMP-1 increases expression and phosphorylation of proteins associated with drug resistance in breast cancer cells

Author

Hekmat, Omid, Munk, Stephanie, Fogh, Louise, Yadav, Rachita, Francavilla, Chiara, Horn, Heiko, Würtz, Sidse Ørnbjerg, Schrohl, Anne-Sofie, Damsgaard, Britt, Romer, Maria Unni, Belling, Kirstine, Jensen, Niels Frank, Gromova, Irina, Bekker-Jensen, Dorte B, Moreira, José, Jensen, Lars Juhl, Gupta, Ramneek, Lademann, Ulrik Axel, Brünner, Nils, Olsen, Jesper Velgaard, Stenvang, Jan, Hekmat, Omid, Munk, Stephanie, Fogh, Louise, Yadav, Rachita, Francavilla, Chiara, Horn, Heiko, Würtz, Sidse Ørnbjerg, Schrohl, Anne-Sofie, Damsgaard, Britt, Romer, Maria Unni, Belling, Kirstine, Jensen, Niels Frank, Gromova, Irina, Bekker-Jensen, Dorte B, Moreira, José, Jensen, Lars Juhl, Gupta, Ramneek, Lademann, Ulrik Axel, Brünner, Nils, Olsen, Jesper Velgaard, and Stenvang, Jan

Abstract

Tissue inhibitor of metalloproteinase 1 (TIMP-1) is a protein with a potential biological role in drug resistance. To elucidate the unknown molecular mechanisms underlying the association between high TIMP-1 levels and increased chemotherapy resistance, we employed SILAC-based quantitative mass spectrometry to analyze global proteome and phosphoproteome differences of MCF-7 breast cancer cells expressing high or low levels of TIMP-1. In TIMP-1 high expressing cells, 312 proteins and 452 phosphorylation sites were up-regulated. Among these were the cancer drug targets topoisomerase 1, 2A and 2B, which may explain the resistance phenotype to topoisomerase inhibitors that was observed in cells with high TIMP-1 levels. Pathway analysis showed an enrichment of proteins from functional categories such as apoptosis, cell cycle, DNA repair, transcription factors, drug targets and proteins associated with drug resistance or sensitivity and drug transportation. The NetworKIN algorithm predicted the protein kinases CK2a, CDK1, PLK1 and ATM as likely candidates involved in the hyper-phosphorylation of the topoisomerases. Up-regulation of protein and/or phosphorylation levels of topoisomerases in TIMP-1 high expressing cells may be part of the mechanisms by which TIMP-1 confers resistance to treatment with the widely-used topoisomerase inhibitors in breast- and colorectal cancer.

Published
2013

218. Mechanisms of topoisomerase I (TOP1) gene copy number increase in a stage III colorectal cancer patient cohort

Author

Smith, David Hersi, Christensen, Ib Jarle, Jensen, Niels Frank, Markussen, Bo, Rømer, Maria Unni Koefoed, Nygård, Sune Boris, Müller, Sven, Nielsen, Hans Jørgen, Brünner, Nils, Nielsen, Kirsten Vang, Smith, David Hersi, Christensen, Ib Jarle, Jensen, Niels Frank, Markussen, Bo, Rømer, Maria Unni Koefoed, Nygård, Sune Boris, Müller, Sven, Nielsen, Hans Jørgen, Brünner, Nils, and Nielsen, Kirsten Vang

Abstract

Topoisomerase I (Top1) is the target of Top1 inhibitor chemotherapy. The TOP1 gene, located at 20q12-q13.1, is frequently detected at elevated copy numbers in colorectal cancer (CRC). The present study explores the mechanism, frequency and prognostic impact of TOP1 gene aberrations in stage III CRC and how these can be detected by fluorescent in situ hybridization (FISH).

Published
2013

219. Early detection of recurrence after curative resection for colorectal cancer - obstacles when using soluble biomarkers?

Author

Nielsen, Hans Jørgen, Jess, Per, Aldulaymi, Bahir Hadi, Jørgensen, Lars Nannestad, Laurberg, Søren, Nielsen, Knud Thygesen, Madsen, Mogens Rørbæk, Brünner, Nils, Christensen, Ib Jarle, Nielsen, Hans Jørgen, Jess, Per, Aldulaymi, Bahir Hadi, Jørgensen, Lars Nannestad, Laurberg, Søren, Nielsen, Knud Thygesen, Madsen, Mogens Rørbæk, Brünner, Nils, and Christensen, Ib Jarle

Abstract

Objective. Results from monitoring studies using biomarkers in blood samples aiming at early detection of recurrent colorectal cancer (CRC) are presently evaluated. However, some serological biomarker levels are influenced by the surgical trauma, which may complicate translation of the levels in relation to recurrence. The primary purpose of the present study was to evaluate the frequency of postoperative surgical interventions during a follow-up period of patients who have undergone surgery for primary CRC. Methods. In a prospective multicenter, clinical study, 634 patients resected for primary CRC were followed in the outpatient clinic every third month. Blood samples were drawn at each visit. A subgroup of 165 stage II and III patients, who had been followed for at least 3 years, was selected. Any recent surgical intervention associated with the primary disease and/or other diseases were recorded at each visit to the outpatient clinic. Results. Among the 165 patients, 49 developed recurrence (R+), 107 did not (R-) and 11 developed a new primary cancer, including 2 in the R+ group. Within the 3 years of observation, 78 (47.3%) of the 165 patients underwent 117 (range 1-5) postoperative surgical interventions. Seventy-five operations were related to CRC and 42 to benign diseases, while none were related to a new primary, malignant disease. Conclusion. Patients resected for CRC are frequently undergoing surgical procedures in the postoperative follow-up period. Therefore, postoperative monitoring using soluble biomarker levels, which may be influenced by the surgical trauma, must be adjusted in relation to postoperative surgical interventions.

Published
2013

220. Topoisomerase 1(TOP1) gene copy number in stage III colorectal cancer patients and its relation to prognosis

Author

Rømer, Maria Unni Koefoed, Nygård, Sune Boris, Christensen, Ib Jarle, Nielsen, Signe Lykke, Nielsen, Kirsten Vang, Müller, Sven, Smith, David Hersi, Vainer, Ben, Nielsen, Hans Jørgen, Brünner, Nils, Rømer, Maria Unni Koefoed, Nygård, Sune Boris, Christensen, Ib Jarle, Nielsen, Signe Lykke, Nielsen, Kirsten Vang, Müller, Sven, Smith, David Hersi, Vainer, Ben, Nielsen, Hans Jørgen, and Brünner, Nils

Abstract

A Topoisomerase 1 (Top1) poison is frequently included in the treatment regimens for metastatic colorectal cancer (mCRC). However, no predictive biomarkers for Top1 poisons are available. We here report a study on the TOP1 gene copy number in CRC patients and its association with patient prognosis and tumor cell proliferation.

Published
2013

221. Detection of serological biomarkers by proximity extension assay for detection of colorectal neoplasias in symptomatic individuals

Author

Buch Thorsen, Stine, Lundberg, Martin, Villablanca, Andrea, Christensen, Sarah Louise T., Belling, Kirstine C., Sander Nielsen, Birgitte, Knowles, Mick, Gee, Nick, Nielsen, Hans Jørgen, Brünner, Nils, Jarle Christensen, Ib, Fredriksson, Simon, Stenvang, Jan, Assarsson, Erika, Buch Thorsen, Stine, Lundberg, Martin, Villablanca, Andrea, Christensen, Sarah Louise T., Belling, Kirstine C., Sander Nielsen, Birgitte, Knowles, Mick, Gee, Nick, Nielsen, Hans Jørgen, Brünner, Nils, Jarle Christensen, Ib, Fredriksson, Simon, Stenvang, Jan, and Assarsson, Erika

Abstract

Although the potential of biomarkers to aid in early detection of colorectal cancer (CRC) is recognized and numerous biomarker candidates have been reported in the literature, to date only few molecular markers have been approved for daily clinical use. In order to improve the translation of biomarkers from the bench to clinical practice we initiated a biomarker study focusing on a novel technique, the proximity extension assay, with multiplexing capability and the possible additive effect obtained from biomarker panels. We performed a screening of 74 different biomarkers in plasma derived from a case–control sample set consisting of symptomatic individuals representing CRC patients, patients with adenoma, patients with non-neoplastic large bowel diseases and healthy individuals. After statistical evaluation we found 12 significant indicators of CRC and the receiver operating characteristic (ROC) curve of Carcinoembryonic antigen (CEA), Transferrin Receptor-1 (TFRC), Macrophage migration inhibitory factor (MIF), Osteopontin (OPN/SPP1) and cancer antigen 242 (CA242) showed additive effect. This biomarker panel identified CRC patients with a sensitivity of 56% at 90% specificity and thus the performance is sufficiently high to further investigate this combination of five proteins as serological biomarkers for detection of CRC. Furthermore, when applying the indicators to identify early-stage CRC a combination of CEA, TFRC and CA242 resulted in a ROC curve with an area under the curve of 0.861.

Published
2013

222. Data fusion in metabolomic cancer diagnostics

Author

Bro, Rasmus, Nielsen, Hans Jørgen, Savorani, Francesco, Kjeldahl, Karin, Christensen, Ib Jarle, Brünner, Nils, Lawaetz, Anders Juul, Bro, Rasmus, Nielsen, Hans Jørgen, Savorani, Francesco, Kjeldahl, Karin, Christensen, Ib Jarle, Brünner, Nils, and Lawaetz, Anders Juul

Published
2013

223. Expression Patterns of Biomarkers in Primary Tumors and Corresponding Metastases in Breast Cancer

Author

Kümler, Iben, Balslev, Eva, Knop, Ann S., Brünner, Nils, Klausen, Tobias W., Jespersen, Sofie S., Nielsen, Signe L., and Nielsen, Dorte L.

Abstract

Tumor heterogeneity has been shown for several cancers including breast cancer (BC). Despite the fact that expression of tumor markers may change throughout the metastatic process, rebiopsies at the time of recurrence are still not performed routinely at all institutions. The aims of the study were to evaluate changes in biomarker profiles during the metastatic process and to investigate whether previous anthracycline or endocrine therapy given in the adjuvant setting could affect the biomarker profile in metastatic lesions. We investigated the expression pattern of ER, HER2, TOP2a, TOP1, p53, Bcl-2, and Ki-67 in 110 paired samples of primary BC and corresponding asynchronous metastases. We found discordant expressions in primary tumor and metastasis for all biomarkers, although only significant for Ki-67. Changes in the expression profile of the metastatic lesions would have altered treatment decisions in 14% of patients. We found no effect of previous anthracycline or endocrine therapy on the expression profiles. Our data confirm that discordant expressions of biomarkers are common in BC and often carry therapeutic consequences. This emphasizes the need for biopsies from metastatic lesions, even in cases where the localization of the metastatic process is not easily accessible.

Published
2018
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224. Integrative analyses of gene expression and DNA methylation profiles in breast cancer cell line models of tamoxifen-resistance indicate a potential role of cells with stem-like properties

Author

Lin, Xue, primary, Li, Jian, additional, Yin, Guangliang, additional, Zhao, Qian, additional, Elias, Daniel, additional, Lykkesfeldt, Anne E, additional, Stenvang, Jan, additional, Brünner, Nils, additional, Wang, Jun, additional, Yang, Huanming, additional, Bolund, Lars, additional, and Ditzel, Henrik J, additional

Published
2013
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225. Plasma levels of the MMP-9:TIMP-1 complex as prognostic biomarker in breast cancer: a retrospective study

Author

Thorsen, Stine B, primary, Christensen, Sarah LT, additional, Würtz, Sidse Ø, additional, Lundberg, Martin, additional, Nielsen, Birgitte S, additional, Vinther, Lena, additional, Knowles, Mick, additional, Gee, Nick, additional, Fredriksson, Simon, additional, Møller, Susanne, additional, Brünner, Nils, additional, Schrohl, Anne-Sofie, additional, and Stenvang, Jan, additional

Published
2013
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226. Saliva and plasma TIMP-1 in patients with colorectal cancer:a prospective study

Author

Holten-Andersen, Lars, Christensen, Ib Jarle, Jensen, Siri Beier, Reibel, Jesper, Laurberg, Søren, Nauntofte, Birgitte, Brünner, Nils, Nielsen, Hans Jørgen, Holten-Andersen, Lars, Christensen, Ib Jarle, Jensen, Siri Beier, Reibel, Jesper, Laurberg, Søren, Nauntofte, Birgitte, Brünner, Nils, and Nielsen, Hans Jørgen

Abstract

Background and aims. A prospective cross-sectional study was designed to test if total levels of TIMP-1 in saliva and plasma correlated with the diagnosis of colorectal cancer (CRC) in a population with symptoms consistent with this disease. Materials and methods. Stimulated whole saliva and blood samples were collected from 161 individuals referred to colonoscopy with symptoms associated with CRC. The results of the examination, as well as previous and/or current other diseases were recorded. In a blinded study, the authors used an in-house TIMP-1 ELISA previously validated for use in saliva and plasma to determine total levels of TIMP-1. Results. Fifty-six of the patients (35%) were diagnosed with CRC. Plasma TIMP-1 levels were significantly elevated in CRC patients compared with patients with other, non-malignant diseases and individuals without disease. Significant differences in saliva TIMP-1 levels between CRC patients and individuals without CRC could not be demonstrated. In addition, no correlation was found between levels of TIMP-1 in plasma and saliva. Conclusion. Total levels of TIMP-1 in saliva do not reflect the presence of CRC, and TIMP-1 saliva measurements thus cannot substitute plasma TIMP-1 measurements in detection of CRC.

Published
2012

227. TOP1 gene copy numbers in colorectal cancer samples and cell lines and their association to in vitro drug sensitivity

Author

Rømer, Maria Unni, Jensen, Niels Frank, Nielsen, Signe Lykke, Müller, Sven, Nielsen, Kirsten Vang, Nielsen, Hans Jørgen, Brünner, Nils, Rømer, Maria Unni, Jensen, Niels Frank, Nielsen, Signe Lykke, Müller, Sven, Nielsen, Kirsten Vang, Nielsen, Hans Jørgen, and Brünner, Nils

Abstract

Background and aims: A positive relationship between topoisomerase-1 (TOP1) protein and sensitivity towards the TOP1 inhibitor irinotecan has been reported in patients with metastatic colorectal cancer (mCRC). The aim of this study was to analyse TOP1 gene copy number variation in tumor tissue from CRC patients and CRC cell lines with different sensitivities to the TOP1 inhibitor SN-38 and oxaliplatin. Methods: A TOP1 gene probe with a chromosome 20 centromere (CEN-20) reference probe was tested on tumor tissue from 50 stage III CRC patients. Additionally, associations between TOP1/CEN-20 ratio and in vitro sensitivity to SN-38 (the active metabolite of irinotecan) and oxaliplatin were tested for 10 CRC cell lines. Results: The crude TOP1 copy numbers as well as the TOP1/CEN-20 mean ratio +/- 3 STD were determined in non-affected mucosa and in the malignant epithelium of the tumors. In the malignant epithelium 84% of the samples demonstrated an increased TOP1 gene copy number and 66% had an increased TOP1/CEN-20 ratio compared to the non-affected mucosa. Sixteen (32%) of the tumors had a ratio = 1.5 and 9 of these had a ratio of = 2.0. A positive association was observed between the TOP1 gene copy number and the TOP1/CEN-20 ratio and in vitro sensitivity towards SN-38 but not towards oxaliplatin. Conclusion: A large fraction of the samples demonstrated an increased TOP1 gene copy number and an increased TOP1/CEN-20 ratio as compared to the non-affected mucosa. The cell line study suggested an association between TOP1 gene copy number or TOP1/CEN-20 ratio and sensitivity to irinotecan but not oxaliplatin.

Published
2012

228. Multiplexed homogeneous proximity ligation assays for high throughput protein biomarker research in serological material

Author

Lundberg, Martin, Thorsen, Stine Buch, Assarsson, Erika, Villablanca, Andrea, Tran, Bonnie, Gee, Nick, Knowles, Mick, Nielsen, Birgitte Egedie Sander, Couto, Eduardo Golzalez, Martin, Roberto, Nilsson, Olle, Fermer, Christian, Schlingemann, Jorg, Christensen, Ib Jarle, Nielsen, Hans Jørgen, Ekstrom, Bjorn, Andersson, Claes, Gustafsson, Mats, Brünner, Nils, Stenvang, Jan, Fredriksson, Simon, Lundberg, Martin, Thorsen, Stine Buch, Assarsson, Erika, Villablanca, Andrea, Tran, Bonnie, Gee, Nick, Knowles, Mick, Nielsen, Birgitte Egedie Sander, Couto, Eduardo Golzalez, Martin, Roberto, Nilsson, Olle, Fermer, Christian, Schlingemann, Jorg, Christensen, Ib Jarle, Nielsen, Hans Jørgen, Ekstrom, Bjorn, Andersson, Claes, Gustafsson, Mats, Brünner, Nils, Stenvang, Jan, and Fredriksson, Simon

Abstract

Udgivelsesdato: 2011-Jan-17, A high throughput protein biomarker discovery tool has been developed based on multiplexed proximity ligation assays (PLA) in a homogeneous format in the sense of no washing steps. The platform consists of four 24-plex panels profiling 74 putative biomarkers with sub pM sensitivity each consuming only 1 micro Litre of human plasma sample. The system uses either matched monoclonal antibody pairs or the more readily available single batches of affinity purified polyclonal antibodies to generate the target specific reagents by covalently linking with unique nucleic acid sequences. These paired sequences are united by DNA ligation upon simultaneous target binding forming a PCR amplicon. Multiplex PLA thereby converts multiple target analytes into real-time PCR amplicons that are individually quantificatied using microfluidic high capacity qPCR in nano liter volumes. The assay shows excellent specificity, even in multiplex, by its dual recognition feature, its proximity requirement, and most importantly by using unique sequence specific reporter fragments on both antibody-based probes. To illustrate the potential of this protein detection technology, a pilot biomarker research project was performed using biobanked plasma samples for the detection of colorectal cancer (CRC) using a multivariate signature.

Published
2011

229. Cancer therapy trials employing level-of-evidence-1 disease forecast cancer biomarkers uPA and its inhibitor PAI-1

Author

Schmitt, Manfred, Harbeck, Nadia, Brünner, Nils, Jänicke, Fritz, Meisner, Christoph, Mühlenweg, Bernd, Jansen, Heike, Dorn, Julia, Nitz, Ulrike, Kantelhardt, Eva J, Thomssen, Christoph, Schmitt, Manfred, Harbeck, Nadia, Brünner, Nils, Jänicke, Fritz, Meisner, Christoph, Mühlenweg, Bernd, Jansen, Heike, Dorn, Julia, Nitz, Ulrike, Kantelhardt, Eva J, and Thomssen, Christoph

Abstract

Clinical research on cancer biomarkers is essential in understanding recent discoveries in cancer biology and heterogeneity of the cancer disease. However, there are only a few examples of clinically useful studies that have identified cancer biomarkers with clinical benefit. Urokinase-type plasminogen activator (uPA) and its inhibitor plasminogen activator inhibitor type 1 (PAI-1) are two of the few tumor tissue-associated cancer biomarkers that have been evaluated successfully and extensively in many preclinical and clinical studies for their clinical utility. Most of the studies have been conducted in early breast cancer to demonstrate the prognostic and predictive value for this malignancy. As a result of these investigations, uPA and PAI-1 have reached the highest level of clinical evidence, level of evidence 1. This article sheds light on the current status of major clinical Phase II and III breast cancer therapy trials (Chemo-N0, NNBC-3 and Plan B), and introduces ongoing clinical trials targeting uPA in advanced cancers of the breast and pancreas, employing synthetic small-size drugs to counteract uPA activity (WX-UK1, Mesupron(®)). The therapeutic effect of a uPA-derived small-size synthetic peptide (Å6) is tested in advanced ovarian cancer patients.

Published
2011

230. Evaluating TIMP-1, Ki67, and HER2 as markers for non-sentinel node metastases in breast cancer patients with micrometastases to the sentinel node

Author

Tvedskov, Tove Filtenborg, Bartels, Annette, Jensen, Maj-Britt, Paaschburg, Birgitte, Kroman, Niels, Balslev, Eva, Brünner, Nils, Tvedskov, Tove Filtenborg, Bartels, Annette, Jensen, Maj-Britt, Paaschburg, Birgitte, Kroman, Niels, Balslev, Eva, and Brünner, Nils

Abstract

The aim was to investigate whether the biochemical prognostic markers TIMP-1, Ki67, and HER2 could predict metastatic spread to non-sentinel nodes (NSN) in breast cancer patients with micrometastases to sentinel node (SN). We included all breast cancer patients with micrometastases to SN operated between 2001 and 2007 at the Department of Breast Surgery, Herlev Hospital. The study was designed as a matched case-control study with 25 cases with micrometastases to SN and, in addition, metastatic spread to NSN and 50 matched controls with micrometastases to SN, but without NSN metastases. Patient and tumor characteristics were retrieved from the Danish Breast Cancer Cooperative Group database. Immunohistochemical analyses of TIMP-1 and Ki67 and measurements of HER2 on formalin-fixed paraffin-embedded tumor tissue were performed. No significant differences in the immunoreactivity of TIMP-1 and Ki67 were found between patients with and without NSN metastases. Six of seven HER2 positive patients did not have NSN metastases, but the results did not reach statistical significance. Despite being prognostic markers in breast cancer, TIMP-1 and Ki67 could not predict NSN metastases in women with micrometastatic disease to SN. Larger studies are needed to further validate HER2 as a marker for NSN metastases in these patients.

Published
2011

231. Screening for colorectal cancer:possible improvements by risk assessment evaluation?

Author

Nielsen, Hans J., Jakobsen, Karen V., Christensen, Ib J., Brünner, Nils, Nielsen, Hans J., Jakobsen, Karen V., Christensen, Ib J., and Brünner, Nils

Abstract

Emerging results indicate that screening improves survival of patients with colorectal cancer. Therefore, screening programs are already implemented or are being considered for implementation in Asia, Europe and North America. At present, a great variety of screening methods are available including colono- and sigmoidoscopy, CT- and MR-colonography, capsule endoscopy, DNA and occult blood in feces, and so on. The pros and cons of the various tests, including economic issues, are debated. Although a plethora of evaluated and validated tests even with high specificities and reasonable sensitivities are available, an international consensus on screening procedures is still not established. The rather limited compliance in present screening procedures is a significant drawback. Furthermore, some of the procedures are costly and, therefore, selection methods for these procedures are needed. Current research into improvements of screening for colorectal cancer includes blood-based biological markers, such as proteins, DNA and RNA in combination with various demographically and clinically parameters into a "risk assessment evaluation" (RAE) test. It is assumed that such a test may lead to higher acceptance among the screening populations, and thereby improve the compliances. Furthermore, the involvement of the media, including social media, may add even more individuals to the screening programs. Implementation of validated RAE and progressively improved screening methods may reform the cost/benefit of screening procedures for colorectal cancer. Therefore, results of present research, validating RAE tests, are awaited with interest.

Published
2011

232. Human epidermal growth factor receptor 2 (HER2) immunoreactivity:specificity of three pharmacodiagnostic antibodies

Author

Rasmussen, Anne-Sofie Schrohl, Pedersen, Hans Christian, Jensen, Sussie Steen, Nielsen, Signe Lykke, Brünner, Nils, Rasmussen, Anne-Sofie Schrohl, Pedersen, Hans Christian, Jensen, Sussie Steen, Nielsen, Signe Lykke, and Brünner, Nils

Abstract

The availability of specific antibody-based test systems is essential to testing of HER2 protein expression. Here, we mapped epitopes recognized by three pharmacodiagnostic HER2 antibodies and investigated their specificity towards peptides and fusion proteins homologous to the intracellular domains of HER1, HER2, HER3 and HER4. The investigated antibodies were PATHWAY(®) HER2 (clone 4B5; Ventana Medical Systems Inc., Tucson, AZ, USA), HercepTest™ (Dako Denmark A/S, Glostrup, Denmark), and Oracle(®) HER2 (clone CB11; Leica Microsystems GmbH, Wetzlar, Germany).

Published
2011

233. Plasma TIMP-1 and CEA in detection of primary colorectal cancer: a prospective, population based study of 4509 high-risk individuals

Author

Nielsen, Hans J, Brünner, Nils, Jørgensen, Lars Nannestad, Olsen, Jesper, Rahr, Hans B, Thygesen, Knud, Hoyer, Ute, Laurberg, Søren, Stieber, Petra, Blankenstein, Marinus A, Davis, Gerard, Dowell, Barry L, Christensen, Ib J, NN, NN, Olsen, Jesper Arnold, Nielsen, Hans J, Brünner, Nils, Jørgensen, Lars Nannestad, Olsen, Jesper, Rahr, Hans B, Thygesen, Knud, Hoyer, Ute, Laurberg, Søren, Stieber, Petra, Blankenstein, Marinus A, Davis, Gerard, Dowell, Barry L, Christensen, Ib J, NN, NN, and Olsen, Jesper Arnold

Abstract

Udgivelsesdato: 2011-Jan, Objective. The combination of plasma tissue inhibitor of metalloproteinases-1 (TIMP-1) and carcinoembryonic antigen (CEA) may be valuable biomarkers for early detection of colorectal cancer (CRC). A prospective, population based study was performed to validate this hypothesis. Material and methods. Individuals (n = 4509) referred for large bowel endoscopy due to symptoms of CRC were prospectively included. Baseline data and concurrent diseases were recorded. The primary endpoint was detection of CRC and findings at examinations were recorded using International Classification of Diseases-10 codes. Plasma was obtained before endoscopy and TIMP-1 and CEA levels were determined after the inclusion of all individuals. Results. Findings were based on sigmoidoscopy in 1766 and colonoscopy in 2743 individuals. Colon cancer (CC) was detected in 184 and rectal cancer in 110 individuals. Ten individuals with other cancers, 856 with adenomas and 1176 with non-neoplastic findings were also detected. The biomarker levels were increased in a variety of diseases including CRC compared to individuals without any findings at endoscopy. A multivariable analysis demonstrated that both markers were significant and independent detectors of CRC. Combining both biomarkers, independent contributions from each (TIMP-1, odds ratio (OR) = 1.8 (95% confidence interval (CI): 1.4-2.2), p < 0.0001; CEA < 5 ng/ml, OR = 1.6, 1.3-1.9, or =5 ng/ml, OR = 2.3, 95% CI: 1.9-2.7 (p < 0.0001)) were obtained. Subgroup analysis of individuals examined by colonoscopy with CC as the endpoint showed that combining both biomarkers, independent contributions from each (TIMP-1, OR = 2.5, 95% CI: 1.8-3.4, p < 0.0001; CEA < 5 ng/ml, OR = 1.4, 95% CI: 1.1-1.8, and CEA = 5 ng/ml, OR = 2.3, 95% CI: 1.8-3.0 (p < 0.0001)) were obtained. Conclusions. This prospective validation study supports the use of the combination of plasma TIMP-1 and CEA protein measurements as a potential aid in early detection of

Published
2011

234. Salivary tissue inhibitor of metalloproteinases-1 localization and glycosylation profile analysis

Author

Holten-Andersen, Lars, Thaysen-Andersen, Morten, Jensen, Siri Beier, von Buchwald, Christian, Højrup, Peter, Offenberg, Hanne Kjær, Nielsen, Hans Jørgen, Brünner, Nils, Nauntofte, Birgitte, Reibel, Jesper, Holten-Andersen, Lars, Thaysen-Andersen, Morten, Jensen, Siri Beier, von Buchwald, Christian, Højrup, Peter, Offenberg, Hanne Kjær, Nielsen, Hans Jørgen, Brünner, Nils, Nauntofte, Birgitte, and Reibel, Jesper

Published
2011

235. Preoperative plasma TIMP-1 is an independent prognostic indicator in patients with primary colorectal cancer : a prospective validation study

Author

Birgisson, Helgi, Nielsen, Hans J., Christensen, Ib Jarle, Glimelius, Bengt, Brünner, Nils, Birgisson, Helgi, Nielsen, Hans J., Christensen, Ib Jarle, Glimelius, Bengt, and Brünner, Nils

Abstract

Background: Previous studies have suggested plasma tissue inhibitor of metalloproteinases-1 (TIMP-1) as a stage independent prognostic marker in colorectal cancer (CRC) patients. The aim was to validate plasma TIMP-1 and serum carcino-embryonic antigen (CEA) levels as prognostic indicators in an independent population-based cohort of patients with CRC. Patients and methods: During 2000-2003, plasma and serum were collected preoperatively from 322 patients treated for primary CRC. TIMP-1 and CEA levels were determined by validated ELISA platforms. Results: High TIMP-1 and CEA levels each associated with poor overall survival (OS); TIMP-1 (hazard ratio (HR) 2.1; 95% confidence interval (CI) 1.6-2.7) and CEA (HR 1.2; 95% CI 1.1-1.3), and disease-free survival (DFS); TIMP-1 (HR 2.0; 95% CI: 1.5-2.6) and CEA (HR 1.2; 95% CI: 1.1-1.4) in univariate analyses. In stratified analyses of stages II and III, TIMP-1 levels associated significantly with OS and DFS in stages II and III, associations were not found for CEA. Multivariate analysis for OS, including TIMP-1 and CEA levels and clinico-pathological baseline variables, revealed significant association of TIMP-1 (HR 1.8; 95% CI 1.3-2.4) but not CEA levels. Conclusions: This independent prospective validation study confirms the significant association between preoperative plasma TIMP-1 levels and survival of CRC patients: TIMP-1 provided stronger prognostic information than CEA. Thus, this study brings plasma TIMP-1 to the next level of evidence for its clinical use as a prognostic marker in CRC patients.

Published
2010
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236. Expression of matrix metalloproteinase 9 (MMP-9) and tissue inhibitor of metalloproteinases 1 (TIMP-1) by colorectal cancer cells and adjacent stroma cells--associations with histopathology and patients outcome

Author

Jensen, Søren Astrup, Vainer, Ben, Bartels, Annette, Brünner, Nils, Sørensen, Jens Benn, Jensen, Søren Astrup, Vainer, Ben, Bartels, Annette, Brünner, Nils, and Sørensen, Jens Benn

Abstract

AIM: To elucidate cellular features accountable for colorectal cancers' (CRC) capability to invade normal tissue and to metastasize, we investigated the level of the collagenase matrix metalloproteinase 9 (MMP-9) and its physiological inhibitor tissue inhibitor of metalloproteinases 1 (TIMP-1) in cancer cells and supporting stroma cells of CRC.METHODS: Immunoreactivity of MMP-9 and TIMP-1 by carcinoma cells, lymphocytes and fibroblasts in archival specimens of paraffin-embedded primary tumours were retrospectively associated with outcome in 340 consecutive patients completely resected for CRC stages II-IV and subsequently treated with adjuvant 5-fluorouracil.RESULTS: Expression of MMP-9 by carcinoma cells was demonstrated in 9% of specimens without association to recurrence free survival (RFS) (HR = 1.0; 95% CI: 0.6-1.8; P = 0.9) or overall survival (OS) (HR = 0.9; 95% CI: 0.5-1.6; P = 0.6). TIMP-1 expression by carcinoma cells, which appeared in 64% of the specimens, was inversely related with RFS (HR = 1.3; 95% CI: 0.9-1.8; P = 0.08) and OS (HR = 1.5; 95% CI: 1.1-2.1; P = 0.02). Expression of TIMP-1 by fibroblasts at the invasive border was directly related to RFS (HR = 0.7; 95% CI: 0.6-0.9; P = 0.02) and OS (HR = 0.7; 95% CI: 0.6-1.0; P = 0.05). Expression of MMP-9 by lymphocytes correlated significantly with the degree of peritumoural inflammation (P = 0.02) but not with RFS (HR = .9; 95% CI: 0.7-1.1; P = 0.2) or OS (HR = 0.8; 95% CI: 0.7-1.0; P = 0.07).CONCLUSION: TIMP-1 in cancer cells is associated with poor prognosis independent of its function as inhibitor of MMP-9. MMP-9 and TIMP-1 are important mediators of the host-cancer cell interaction in the tumour microenvironment with significant influence on the histopathology and on prognosis of CRC.

Published
2010

237. HER2, TOP2A, and TIMP-1 and responsiveness to adjuvant anthracycline-containing chemotherapy in high-risk breast cancer patients

Author

Ejlertsen, Bent, Jensen, Maj-Britt, Nielsen, Kirsten, Balslev, Eva, Rasmussen, Birgitte, Willemoe, Gro L, Hertel, Pernille B, Knoop, Ann S, Mouridsen, Henning T, Brünner, Nils Aage, Ejlertsen, Bent, Jensen, Maj-Britt, Nielsen, Kirsten, Balslev, Eva, Rasmussen, Birgitte, Willemoe, Gro L, Hertel, Pernille B, Knoop, Ann S, Mouridsen, Henning T, and Brünner, Nils Aage

Abstract

PURPOSE To evaluate whether the combination of HER2 with TIMP-1 (HT) or TOP2A with TIMP-1 (2T) more accurately identifies patients who benefit from cyclophosphamide, epirubicin, and fluorouracil (CEF) compared with cyclophosphamide, methotrexate, and fluorouracil (CMF) than these markers do when analyzed individually. PATIENTS AND METHODS The Danish Breast Cancer Cooperative Group (DBCG) 89D trial randomly assigned 980 high-risk Danish breast cancer patients to CMF or CEF. Archival tumor tissue was analyzed TIMP-1, and HER2-negative and TIMP-1 immunoreactive tumors were classified as HT nonresponsive and otherwise HT responsive. Similarly, the 2T panel was constructed by combining TOP2A and TIMP-1; tumors with normal TOP2A status and TIMP-1 immunoreactivity were classified as 2T-nonresponsive and otherwise 2T-responsive. Results In total, 623 tumors were available for analysis, of which 154 lacked TIMP-1 immunoreactivity, 188 were HER2 positive, and 139 had a TOP2A aberration. HT status was a statistically significant predictor of benefit from CEF compared with CMF (P(interaction) = .036 for invasive disease-free survival [IDFS] and .047 for overall survival [OS]). The 269 (43%) patients with a 2T-responsive profile had a significant reduction in IDFS events (adjusted hazard ratio, 0.48; 95% CI, 0.34 to 0.69; P <.001) and OS events (adjusted hazard ratio, 0.54; 95% CI, 0.38 to 0.77; P <.001). 2T status was a highly significant predictor of benefit from CEF compared with CMF (P(interaction) <.0001 for IDFS and .004 for OS). CONCLUSION The 2T profile is a more accurate predictor of incremental benefit from anthracycline-containing chemotherapy than HER2, TIMP-1, or TOP2A individually, and compared with these, 2T classifies a larger proportion of patients as sensitive to anthracyclines.

Published
2010

238. High Plasma TIMP-1 and Serum CEA Levels during Combination Chemotherapy for Metastatic Colorectal Cancer Are Significantly Associated with Poor Outcome

Author

Aldulaymi, Bahir, Byström, Per, Berglund, Ake, Christensen, Ib J, Brünner, Nils, Nielsen, Hans Jørgen, Glimelius, Bengt, Aldulaymi, Bahir, Byström, Per, Berglund, Ake, Christensen, Ib J, Brünner, Nils, Nielsen, Hans Jørgen, and Glimelius, Bengt

Abstract

Objective: To evaluate whether combination chemotherapy leads to early changes in plasma TIMP-1 and serum carcinoembryonic antigen (CEA) levels in patients with metastatic colorectal cancer (mCRC), and whether such changes relate to subsequent objective response, time to progression (TTP) and overall survival. Materials and Methods: Eighty-eight patients with mCRC were included. Blood samples were collected before initiation and after 2, 4 and 6 weeks of treatment with an irinotecan-5-fluorouracil combination. Plasma TIMP-1 and serum CEA levels were determined by validated ELISA platforms. The first response evaluation was performed after 8 weeks of chemotherapy. Results: Median plasma TIMP-1 and serum CEA levels did not change significantly during 6 weeks of treatment. High plasma TIMP-1 and high serum CEA levels before treatment and at weeks 2, 4 and 6 were related to poor objective response. Moreover, high levels of plasma TIMP-1 before treatment and at weeks 2 and 4 were significantly associated with short TTP, while high levels of serum CEA at week 4 were significantly associated with short TTP. Finally, high levels of plasma TIMP-1 before and during treatment were significantly associated with poor overall survival; p <0.0001 in all 4 determinations. A similar association between serum CEA and overall survival could only be demonstrated before treatment. Conclusion: Median plasma TIMP-1 or serum CEA levels do not change significantly during the first 6 weeks of chemotherapy for mCRC. The results indicate that plasma TIMP-1 in particular and serum CEA may be valuable biomarkers even in samples collected during treatment with chemotherapy.

Published
2010

239. Changes in soluble CEA and TIMP-1 levels during adjuvant chemotherapy for stage III colon cancer

Author

Aldulaymi, Bahir, Christensen, Ib Jarle, Sölétormos, György, Jess, Per, Nielsen, Svend Erik, Brünner, Nils, Nielsen, Hans J., Aldulaymi, Bahir, Christensen, Ib Jarle, Sölétormos, György, Jess, Per, Nielsen, Svend Erik, Brünner, Nils, and Nielsen, Hans J.

Abstract

Tissue inhibitor of metalloproteinases-1 (TIMP-1) has been suggested to be a valuable marker in colorectal cancer (CRC), but the effects of chemotherapy on TIMP-1 levels are unknown. The present study evaluated the effect of chemotherapy on TIMP-1 levels in comparison with carcinoembryonic antigen (CEA) levels in patients with stage III colon cancer.

Published
2010

240. Association between tumor tissue TIMP-1 levels and objective response to first-line chemotherapy in metastatic breast cancer

Author

Klintman, Marie, Würtz, Sidse Ørnbjerg, Christensen, Ib Jarle, Hertel, Pernille Bræmer, Fernö, Mårten, Malmberg, Martin, Mouridsen, Henning, Cold, Frederik, Schrohl, Anne-Sofie, Foekens, John A., Malmström, Per, Brünner, Nils, Klintman, Marie, Würtz, Sidse Ørnbjerg, Christensen, Ib Jarle, Hertel, Pernille Bræmer, Fernö, Mårten, Malmberg, Martin, Mouridsen, Henning, Cold, Frederik, Schrohl, Anne-Sofie, Foekens, John A., Malmström, Per, and Brünner, Nils

Abstract

In a previous study from our laboratory, high tumor levels of tissue inhibitor of metalloproteinases-1 (TIMP-1) have been associated with an adverse response to chemotherapy in metastatic breast cancer suggesting that TIMP-1, which is known to inhibit apoptosis, may be a new predictive marker in this disease. The purpose of this study was to investigate the association between TIMP-1 and objective response to chemotherapy in an independent patient population consisting of patients with metastatic breast cancer from Sweden and Denmark. TIMP-1 was measured using ELISA in 162 primary tumor extracts from patients who later developed metastatic breast cancer and these levels were related to the objective response to first-line chemotherapy. Increasing levels of TIMP-1 were associated with a decreasing probability of response to treatment, reaching borderline significance (OR = 1.59, 95% CI: 0.97-2.62, P = 0.07). This OR is very similar to the result from our previous study. Increasing levels of TIMP-1 were also associated with a shorter disease-free survival and overall survival, however, not statistically significant. The results from the present study support previous data that TIMP-1 is associated with objective response to chemotherapy for metastatic breast cancer.

Published
2010

241. Changes in plasma TIMP-1 levels after resection for primary colorectal cancer

Author

Frederiksen, C., Lomholt, A.F., Davis, G.J., Dowell, B.L., Blankenstein, M.A., Christensen, I.J., Brünner, Nils, Nielsen, H.J., Frederiksen, C., Lomholt, A.F., Davis, G.J., Dowell, B.L., Blankenstein, M.A., Christensen, I.J., Brünner, Nils, and Nielsen, H.J.

Abstract

BACKGROUND: Increased plasma levels of tissue inhibitor of metalloproteinases (TIMP-1) are associated with poor outcome in colorectal cancer (CRC), however postoperative changes in plasma TIMP-1 levels after resections for CRC have not been thoroughly evaluated. MATERIALS AND METHODS: Plasma samples were collected from 45 patients with primary CRC, preoperatively, 2 hours after surgery, and at days 1, 2, 7, 28, 45, 60, 75 and 90 after surgery. TIMP-1 and CEA levels were determined using the ARCHITECT Immunoanalyzer. RESULTS: Postoperatively, the mean (geometric) TIMP-1 level increased and had a maximum level at day 1 (p < 0.0001). The mean TIMP-1 level then declined to a level at day 90 similar to the mean preoperative level. CONCLUSION: A mean decline in plasma TIMP-1 levels was not observed within 90 days. However, individual significant reductions of plasma TIMP-1 levels did occur within 28-60 days postoperatively.

Published
2009

243. PPARa and PPAR¿ coactivation rapidly induces Egr-1 in the nuclei of the dorsal and ventral urinary bladder and kidney pelvis urothelium of rats

Author

Egerod, Frederikke Lihme, Svendsen, Jette Eldrup, Hinley, Jennifer, Southgate, Jennifer, Bartels, Annette, Brünner, Nils, Oleksiewicz, Martin B, Egerod, Frederikke Lihme, Svendsen, Jette Eldrup, Hinley, Jennifer, Southgate, Jennifer, Bartels, Annette, Brünner, Nils, and Oleksiewicz, Martin B

Abstract

To facilitate studies of the rat bladder carcinogenicity of dual-acting PPAR alpha+gamma agonists, we previously identified the Egr-1 transcription factor as a candidate carcinogenicity biomarker and developed rat models based on coadministration of commercially available specific PPAR alpha and PPAR gamma agonists. Immunohistochemistry for Egr-1 with a rabbit monoclonal antibody demonstrated that male vehicle-treated rats exhibited minimal urothelial expression and specifically, no nuclear signal. In contrast, Egr-1 was induced in the nuclei of bladder, as well as kidney pelvis, urothelia within one day (2 doses) of oral dosing of rats with a combination of 8 mg/kg rosiglitazone and 200 mg/kg fenofibrate (specific PPAR gamma and PPAR alpha agonists, respectively). These findings were confirmed by Western blotting using a different Egr-1 antibody. Egr-1 was induced to similar levels in the dorsal and ventral bladder urothelium, arguing against involvement of urinary solids. Egr-1 induction sometimes occurred in a localized fashion, indicating physiological microheterogeneity in the urothelium. The rapid kinetics supported that Egr-1 induction occurred as a result of pharmacological activation of PPAR alpha and PPAR gamma, which are coexpressed at high levels in the rat urothelium. Finally, our demonstration of a nuclear localization supports that the Egr-1 induced by PPAR alpha and PPAR gamma coactivation in the rat urothelium may be biologically active.

Published
2009

245. Plasma tissue inhibitor of metalloproteinases-1 (TIMP-1): A novel biological marker in the detection of primary colorectal cancer. Protocol outlines of the Danish-Australian endoscopy study group on colorectal cancer detection

Author

Nielsen, Hans Jørgen, Brünner, Nils, Frederiksen, Camilla, Lomholt, Anne Fog, King, Denis, Jørgensen, Lars Nannestad, Olsen, Jesper, Rahr, Hans B, Thygesen, Knud, Hoyer, Ute, Laurberg, Søren, Christensen, Ib Jarle, Nielsen, Hans Jørgen, Brünner, Nils, Frederiksen, Camilla, Lomholt, Anne Fog, King, Denis, Jørgensen, Lars Nannestad, Olsen, Jesper, Rahr, Hans B, Thygesen, Knud, Hoyer, Ute, Laurberg, Søren, and Christensen, Ib Jarle

Abstract

Udgivelsesdato: februar

Published
2008

246. TIMP-1 as a Prognostic Marker in Colorectal Cancer

Author

Edwards, Dylan, Høyer-Hansen, Gunilla, Blasi, Francesco, Sloane, Bonnie F., Frederiksen, Camilla, Lomholt, Anne Fog, Nielsen, Hans Jørgen, Brünner, Nils, Edwards, Dylan, Høyer-Hansen, Gunilla, Blasi, Francesco, Sloane, Bonnie F., Frederiksen, Camilla, Lomholt, Anne Fog, Nielsen, Hans Jørgen, and Brünner, Nils

Published
2008

247. National Academy of Clinical Biochemistry laboratory medicine practice guidelines for use of tumor markers in testicular, prostate, colorectal, breast, and ovarian cancers

Author

Sturgeon, Catharine M., Duffy, Michael J., Stenman, Ulf-Håkan, Lilja, Hans, Brünner, Nils, Chan, Daniel W., Babaian, Richard, Bast, Robert C., Dowell, Barry, Esteva, Francisco J., Haglund, Caj, Harbeck, Nadia, Hayes, Daniel F., Holten-Andersen, Mads Nikolaj, Klee, George G, Lamerz, Rolf, Looijenga, Leendert H, Molina, Rafael, Nielsen, Hans Jørgen, Rittenhouse, Harry, Semjonow, Axel, Shih, Ie-Ming, Sibley, Paul, Sölétormos, György, Stephan, Carsten, Sokoll, Lori, Hoffman, Barry R., Diamandis, Eleftherios P., Sturgeon, Catharine M, Duffy, Michael J, Chan, Daniel W, Bast, Robert C, Esteva, Francisco J, Hayes, Daniel F, Holten-Andersen, Mads, Hoffman, Barry R, Diamandis, Eleftherios P, NN, NN, Sturgeon, Catharine M., Duffy, Michael J., Stenman, Ulf-Håkan, Lilja, Hans, Brünner, Nils, Chan, Daniel W., Babaian, Richard, Bast, Robert C., Dowell, Barry, Esteva, Francisco J., Haglund, Caj, Harbeck, Nadia, Hayes, Daniel F., Holten-Andersen, Mads Nikolaj, Klee, George G, Lamerz, Rolf, Looijenga, Leendert H, Molina, Rafael, Nielsen, Hans Jørgen, Rittenhouse, Harry, Semjonow, Axel, Shih, Ie-Ming, Sibley, Paul, Sölétormos, György, Stephan, Carsten, Sokoll, Lori, Hoffman, Barry R., Diamandis, Eleftherios P., Sturgeon, Catharine M, Duffy, Michael J, Chan, Daniel W, Bast, Robert C, Esteva, Francisco J, Hayes, Daniel F, Holten-Andersen, Mads, Hoffman, Barry R, Diamandis, Eleftherios P, and NN, NN

Abstract

Udgivelsesdato: 2008-Dec, BACKGROUND: Updated National Academy of Clinical Biochemistry (NACB) Laboratory Medicine Practice Guidelines for the use of tumor markers in the clinic have been developed. METHODS: Published reports relevant to use of tumor markers for 5 cancer sites--testicular, prostate, colorectal, breast, and ovarian--were critically reviewed. RESULTS: For testicular cancer, alpha-fetoprotein, human chorionic gonadotropin, and lactate dehydrogenase are recommended for diagnosis/case finding, staging, prognosis determination, recurrence detection, and therapy monitoring. alpha-Fetoprotein is also recommended for differential diagnosis of nonseminomatous and seminomatous germ cell tumors. Prostate-specific antigen (PSA) is not recommended for prostate cancer screening, but may be used for detecting disease recurrence and monitoring therapy. Free PSA measurement data are useful for distinguishing malignant from benign prostatic disease when total PSA is <10 microg/L. In colorectal cancer, carcinoembryonic antigen is recommended (with some caveats) for prognosis determination, postoperative surveillance, and therapy monitoring in advanced disease. Fecal occult blood testing may be used for screening asymptomatic adults 50 years or older. For breast cancer, estrogen and progesterone receptors are mandatory for predicting response to hormone therapy, human epidermal growth factor receptor-2 measurement is mandatory for predicting response to trastuzumab, and urokinase plasminogen activator/plasminogen activator inhibitor 1 may be used for determining prognosis in lymph node-negative patients. CA15-3/BR27-29 or carcinoembryonic antigen may be used for therapy monitoring in advanced disease. CA125 is recommended (with transvaginal ultrasound) for early detection of ovarian cancer in women at high risk for this disease. CA125 is also recommended for differential diagnosis of suspicious pelvic masses in postmenopausal women, as well as for detection of recurrence, monitoring of therap

Published
2008

248. Tumor tissue levels of Tissue Inhibitor of Metalloproteinases-1 (TIMP-1) and survival following adjuvant chemotherapy in pre-menopausal lymph node-positive breast cancer patients (N=525)

Author

Rasmussen, Anne-Sofie Schrohl, Look, Maxime P., Meijer-van Gelder, Marion E., Foekens, John A., Brünner, Nils, Rasmussen, Anne-Sofie Schrohl, Look, Maxime P., Meijer-van Gelder, Marion E., Foekens, John A., and Brünner, Nils

Abstract

Predictive markers are needed to guide planning of adjuvant therapy for patients with breast cancer. We have recently shown that high tumor tissue levels of TIMP-1 are associated with decreased response to chemotherapy in metastatic breast cancer patients (Schrohl et al, Clin Cancer Res, 2006) suggesting that TIMP-1 may be a predictive marker in breast cancer patients. Purpose: This study investigates the association of tumor tissue TIMP-1 levels with response to adjuvant chemotherapy with CMF (cyclophosphamide/methotrexate/5-fluorouracil) or an anthracycline-containing regimen.Patients and Methods: 525 pre-menopausal lymph node-positive patients were included; 324 patients received adjuvant CMF, 99 received an adjuvant anthracycline-containing regimen and 102 had no adjuvant chemotherapy. Total TIMP-1 levels were measured by use of ELISA in cytosolic extracts of frozen primary tumors. Using the untreated patient group as a reference group, we analyzed the benefit of adjuvant CMF and anthracyclines in TIMP-1 high and low patients, respectively. The median TIMP-1 concentration was used to dichotomize patients into high and low TIMP-1 groups. End points were disease-free and overall survival (DFS, OS).Results: The median TIMP-1 level in the total patient group was 12,54 ng/mg of total protein (range, 0 - 112,9 ng/mg). TIMP-1 levels in subgroups according to adjuvant therapy were not significantly different (P=0,20). In a multivariate model including basic clinico-pathological parameters, TIMP-1 low and high patients benefited differentially from adjuvant CMF and anthracyclines when compared to untreated patients. In particular, patients with high tumor levels of TIMP-1 had little benefit from adjuvant anthracyclines. Hazard ratios (HR) and 95% confidence intervals (CI) are given in the table below for the analysis of DFS. A similar pattern was seen in the analyses of OS. In the group treated with CMF, both TIMP-1 low and high patients had significant

Published
2008

249. Investigating the biomarker potential of glycoproteins using comparative glycoprofiling - application to tissue inhibitor of metalloproteinases-1.

Author

Thaysen-Andersen, Morten, Thøgersen, Ida, Lademann, Ulrik Axel, Offenberg, Hanne Kjær, Giessing, Anders, Enghild, Jan J., Nielsen, Hans Jørgen, Brunner, Nils, Højrup, Peter, Thøgersen, Ida B, Lademann, Ulrik, Offenberg, Hanne, Giessing, Anders M B, Enghild, Jan J, Brünner, Nils, Thaysen-Andersen, Morten, Thøgersen, Ida, Lademann, Ulrik Axel, Offenberg, Hanne Kjær, Giessing, Anders, Enghild, Jan J., Nielsen, Hans Jørgen, Brunner, Nils, Højrup, Peter, Thøgersen, Ida B, Lademann, Ulrik, Offenberg, Hanne, Giessing, Anders M B, Enghild, Jan J, and Brünner, Nils

Abstract

Udgivelsesdato: 2008-Mar, Cancer-induced alterations of protein glycosylations are well-known phenomena. Hence, the glycoprofile of certain glycoproteins can potentially be used as biomarkers for early diagnosis. However, there are a substantial number of candidates and the techniques for measuring their biomarker potential are limited, calling for new methods. Here, we have investigated the cancer marker potential of the glycoprofile of tissue inhibitor of metalloproteinase-1 (TIMP-1) using a method for comparative glycoprofiling. Glycoprofiles were obtained from plasma TIMP-1 of five healthy donors and five colorectal cancer (CRC) patients showing increased amounts of TIMP-1. Furthermore, the TIMP-1 glycoprofiles of media from two colon cancer cell lines (CCC) and a prostate cancer cell line were determined as disease references. TIMP-1 was purified from IgG-depleted samples using immuno affinity and gel electrophoresis and the glycoprofiling was performed using glycopeptide enrichment and mass spectrometry. The heterogeneous glycoprofiles of TIMP-1 were found to be highly conserved among the healthy donors, proving an ideal candidate marker and showed high reproducibility of the method. Numerous CCC-specific TIMP-1 glycans were observed illustrating cancer-induced changes. Unexpectedly, quantitation revealed that the glycoprofiles of healthy donors and CRC patients varied minimally. Considering the increased CRC TIMP-1 levels and the observed CCC-specific glycans, the lack of variation indicates that the increased amount of CRC TIMP-1 is not a direct product of the cancer cells. Hence, the TIMP-1 glycoprofile holds no biomarker potential for CRC when using plasma as the sample origin. This study clearly illustrates that the technique is capable of performing individualised site-specific glycan analysis and representing a new tool for biomarker investigation of low-abundant glycoproteins.

Published
2008

250. Biology and potential clinical implications of tissue inhibitor of metalloproteinases-1 in colorectal cancer treatment

Author

Sørensen, Nanna Møller, Sørensen, irene Vejgaard, Würtz, Sidse Ørnbjerg, Schrohl, Anne-Sofie, Dowell, Barry, Davis, Gerard, Christensen, Ib Jarle, Nielsen, Hans Jørgen, Brünner, Nils, Sørensen, Nanna Møller, Sørensen, irene Vejgaard, Würtz, Sidse Ørnbjerg, Schrohl, Anne-Sofie, Dowell, Barry, Davis, Gerard, Christensen, Ib Jarle, Nielsen, Hans Jørgen, and Brünner, Nils

Abstract

Colorectal cancer (CRC) is the second leading cause of cancer-related death in the industrialized world. About half of "curatively" resected patients develop recurrent disease within the next 3-5 years despite the lack of clinical, histological and biochemical evidence of remaining overt disease after resection of the primary tumour. Availability of validated biological markers for early detection, selection for adjuvant therapy, prediction of treatment efficacy and monitoring of treatment efficacy would most probably increase survival. Tissue inhibitor of metalloproteinases-1 (TIMP-1) may be such a marker. TIMP-1 inhibits the proteolytic activity of metalloproteinases, which are centrally involved in tumour invasion and metastases. However, in clinical investigations high tumour tissue or plasma levels of TIMP-1 have shown a strong and independent association with a shorter survival time in CRC patients, suggesting that TIMP-1 could have a tumour-promoting function. Furthermore, measurement of plasma TIMP-1 has been shown to be useful for disease detection, with a high sensitivity and high specificity for early-stage colon cancer. This review describes some basic information on the current knowledge of the biology of TIMP-1 as well as the potential use of TIMP-1 as a biological marker in the management of CRC patients.

Published
2008

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