Your search keyword '"Jacobsen, Frank"' showing total 15 results

1. Carcinoembryonic Antigen Expression in Human Tumors: A Tissue Microarray Study on 13,725 Tumors.

Author

Jansen, Kristina, Kornfeld, Lara, Lennartz, Maximilian, Dwertmann Rico, Sebastian, Kind, Simon, Reiswich, Viktor, Viehweger, Florian, Bawahab, Ahmed Abdulwahab, Fraune, Christoph, Gorbokon, Natalia, Luebke, Andreas M., Hube-Magg, Claudia, Menz, Anne, Uhlig, Ria, Krech, Till, Hinsch, Andrea, Jacobsen, Frank, Burandt, Eike, Sauter, Guido, and Simon, Ronald

Subjects

TUMOR classification, TISSUE arrays, ADENOCARCINOMA, BLADDER tumors, TISSUES, BREAST tumors, COLORECTAL cancer, IMMUNOHISTOCHEMISTRY, ADENOMA, ESTROGEN receptors, CANCER cells, TUMORS, TUMOR antigens, LUNG cancer, SMALL cell carcinoma, PATHOGENESIS

Abstract

Simple Summary: Carcinoembryonic antigen is a cell-surface glycoprotein and target for anti-cancer drugs. In this study, more than 15,000 samples from 120 different tumor types were analyzed by immunohistochemistry. CEA expression was found at least occasionally in 65 tumor types, most frequently in colorectal cancers and other gastrointestinal tumors, thyroid gland cancers, and pulmonary adenocarcinomas. Reduced CEA expression was linked to colon cancer aggressiveness. In contrast, aggressiveness cancers of the urinary bladder and breast cancers were characterized by CEA overexpression. We present a comprehensive catalog of tumor types that might benefit from anti-CEA therapies. Background/Objectives: Carcinoembryonic antigen (CEA) is a cell-surface glycoprotein serving as a drug target, diagnostic marker, and serum marker for cancer monitoring. However, prevalence data on CEA expression in cancer tissues vary considerably. This study was designed to determine CEA expression in normal and neoplastic tissues. Methods: A tissue microarray containing 13,725 samples from 120 different tumor types, as well as 76 different normal tissue types, was analyzed by immunohistochemistry (IHC). Results: CEA was detectable in 65 (54.2%) of 120 tumor categories, including 49 (40.8%) tumor types with at least one strongly positive case. CEA positivity was most common in colorectal adenomas (100%) and carcinomas (98.7%), other gastrointestinal adenocarcinomas (61.1–80.3%), medullary carcinomas of the thyroid (96.3%), pulmonary adenocarcinoma (73.7%), mucinous carcinomas of the ovary (79.8%) and the breast (43.2%), small-cell carcinomas of the lung (64.3%), and urinary bladder (38.9%). CEA overexpression was linked to high tumor grade and invasive growth (p < 0.0001 each) in urinary bladder cancer, and estrogen and HER2 receptor positivity (p ≤ 0.0158) in invasive breast cancer of no special type. In colorectal adenocarcinomas, reduced CEA expression was associated with mismatch repair deficiency (p < 0.0001). Conclusions: The comprehensive list of CEA-positive human tumor types demonstrates that CEA is expressed in a broad range of epithelial neoplasms, many of which might benefit from CEA serum monitoring and anti-CEA therapies. [ABSTRACT FROM AUTHOR]

Published

2024

2. Epithelial Cell Adhesion Molecule (EpCAM) Expression in Human Tumors: A Comparison with Pan-Cytokeratin and TROP2 in 14,832 Tumors.

Author

Menz, Anne, Lony, Nora, Lennartz, Maximilian, Dwertmann Rico, Sebastian, Schlichter, Ria, Kind, Simon, Reiswich, Viktor, Viehweger, Florian, Dum, David, Luebke, Andreas M., Kluth, Martina, Gorbokon, Natalia, Hube-Magg, Claudia, Bernreuther, Christian, Simon, Ronald, Clauditz, Till S., Sauter, Guido, Hinsch, Andrea, Jacobsen, Frank, and Marx, Andreas H.

Subjects

CELL adhesion molecules, SEMINOMA, NEUROENDOCRINE tumors, KIDNEY tumors, EPITHELIAL cells, EPITHELIAL tumors, ADRENAL tumors

Abstract

EpCAM is expressed in many epithelial tumors and is used for the distinction of malignant mesotheliomas from adenocarcinomas and as a surrogate pan-epithelial marker. A tissue microarray containing 14,832 samples from 120 different tumor categories was analyzed by immunohistochemistry. EpCAM staining was compared with TROP2 and CKpan. EpCAM staining was detectable in 99 tumor categories. Among 78 epithelial tumor types, the EpCAM positivity rate was ≥90% in 60 categories—including adenocarcinomas, neuroendocrine neoplasms, and germ cell tumors. EpCAM staining was the lowest in hepatocellular carcinomas, adrenocortical tumors, renal cell neoplasms, and in poorly differentiated carcinomas. A comparison of EpCAM and CKpan staining identified a high concordance but EpCAM was higher in testicular seminomas and neuroendocrine neoplasms and CKpan in hepatocellular carcinomas, mesotheliomas, and poorly differentiated non-neuroendocrine tumors. A comparison of EpCAM and TROP2 revealed a higher rate of TROP2 positivity in squamous cell carcinomas and lower rates in many gastrointestinal adenocarcinomas, testicular germ cell tumors, neuroendocrine neoplasms, and renal cell tumors. These data confirm EpCAM as a surrogate epithelial marker for adenocarcinomas and its diagnostic utility for the distinction of malignant mesotheliomas. In comparison to CKpan and TROP2 antibodies, EpCAM staining is particularly common in seminomas and in neuroendocrine neoplasms. [ABSTRACT FROM AUTHOR]

Published

2024

3. Frequency of Androgen Receptor Positivity in Tumors: A Study Evaluating More Than 18,000 Tumors.

Author

Viehweger, Florian, Hoop, Jennifer, Tinger, Lisa-Marie, Bernreuther, Christian, Büscheck, Franziska, Clauditz, Till S., Hinsch, Andrea, Jacobsen, Frank, Luebke, Andreas M., Steurer, Stefan, Hube-Magg, Claudia, Kluth, Martina, Marx, Andreas H., Krech, Till, Lebok, Patrick, Fraune, Christoph, Burandt, Eike, Sauter, Guido, Simon, Ronald, and Minner, Sarah

Subjects

ANDROGEN receptors, TRANSCRIPTION factors, RENAL cell carcinoma, BLADDER, OPTIMISM, LOBULAR carcinoma, BLADDER cancer

Abstract

Androgen receptor (AR) is a transcription factor expressed in various normal tissues and is a therapeutic target for prostate and possibly other cancers. A TMA containing 18,234 samples from 141 different tumor types/subtypes and 608 samples of 76 different normal tissue types was analyzed by immunohistochemistry. AR positivity was found in 116 tumor types including 66 tumor types (46.8%) with ≥1 strongly positive tumor. Moderate/strong AR positivity was detected in testicular sex cord-stromal tumors (93.3–100%) and neoplasms of the prostate (79.3–98.7%), breast (25.0–75.5%), other gynecological tumors (0.9–100%), kidney (5.0–44.1%), and urinary bladder (5.4–24.2%). Low AR staining was associated with advanced tumor stage (pTa versus pT2-4; p < 0.0001) in urothelial carcinoma; advanced pT (p < 0.0001), high tumor grade (p < 0.0001), nodal metastasis (p < 0.0001), and reduced survival (p = 0.0024) in invasive breast carcinoma; high pT (p < 0.0001) and grade (p < 0.0001) in clear cell renal cell carcinoma (RCC); and high pT (p = 0.0055) as well as high grade (p < 0.05) in papillary RCC. AR staining was unrelated to histopathological/clinical features in 157 endometrial carcinomas and in 221 ovarian carcinomas. Our data suggest a limited role of AR immunohistochemistry for tumor distinction and a prognostic role in breast and clear cell RCC and highlight tumor entities that might benefit from AR-targeted therapy. [ABSTRACT FROM AUTHOR]

Published

2024

4. Novel Filamin C Myofibrillar Myopathy Variants Cause Different Pathomechanisms and Alterations in Protein Quality Systems.

Author

Sellung, Dominik, Heil, Lorena, Daya, Nassam, Jacobsen, Frank, Mertens-Rill, Janine, Zhuge, Heidi, Döring, Kristina, Piran, Misagh, Milting, Hendrik, Unger, Andreas, Linke, Wolfgang A., Kley, Rudi, Preusse, Corinna, Roos, Andreas, Fürst, Dieter O., Ven, Peter F. M. van der, and Vorgerd, Matthias

Subjects

NEMALINE myopathy, STRUCTURAL failures, MUSCLE weakness, SOIL structure, MUSCLE diseases, CYTOSKELETAL proteins

Abstract

Myofibrillar myopathies (MFM) are a group of chronic muscle diseases pathophysiologically characterized by accumulation of protein aggregates and structural failure of muscle fibers. A subtype of MFM is caused by heterozygous mutations in the filamin C (FLNC) gene, exhibiting progressive muscle weakness, muscle structural alterations and intracellular protein accumulations. Here, we characterize in depth the pathogenicity of two novel truncating FLNc variants (p.Q1662X and p.Y2704X) and assess their distinct effect on FLNc stability and distribution as well as their impact on protein quality system (PQS) pathways. Both variants cause a slowly progressive myopathy with disease onset in adulthood, chronic myopathic alterations in muscle biopsy including the presence of intracellular protein aggregates. Our analyses revealed that p.Q1662X results in FLNc haploinsufficiency and p.Y2704X in a dominant-negative FLNc accumulation. Moreover, both protein-truncating variants cause different PQS alterations: p.Q1662X leads to an increase in expression of several genes involved in the ubiquitin-proteasome system (UPS) and the chaperone-assisted selective autophagy (CASA) system, whereas p.Y2704X results in increased abundance of proteins involved in UPS activation and autophagic buildup. We conclude that truncating FLNC variants might have different pathogenetic consequences and impair PQS function by diverse mechanisms and to varying extents. Further studies on a larger number of patients are necessary to confirm our observations. [ABSTRACT FROM AUTHOR]

Published

2023

5. Mammaglobin-A Expression Is Highly Specific for Tumors Derived from the Breast, the Female Genital Tract, and the Salivary Gland.

Author

Gorbokon, Natalia, Timm, Patrick, Dum, David, Menz, Anne, Büscheck, Franziska, Völkel, Cosima, Hinsch, Andrea, Lennartz, Maximilian, Luebke, Andreas M, Hube-Magg, Claudia, Fraune, Christoph, Krech, Till, Lebok, Patrick, Clauditz, Till S, Jacobsen, Frank, Sauter, Guido, Uhlig, Ria, Steurer, Stefan, Minner, Sarah, and Marx, Andreas H.

Subjects

LOBULAR carcinoma, GENITALIA, SALIVARY glands, MEDULLARY thyroid carcinoma, PROGESTERONE receptors, SQUAMOUS cell carcinoma

Abstract

Human mammaglobin-A (SCGB2A2) is a secretory protein with an unknown function that is used as a diagnostic marker for breast cancer. However, other tumors can also express mammaglobin-A. To comprehensively study patterns of mammaglobin-A expression, a tissue microarray containing 16,328 samples from 128 different tumor types as well as 608 samples of 76 different normal tissue types was analyzed using immunohistochemistry. Mammaglobin-A positivity was found in only a few normal tissues, including luminal cells of the breast as well as endocervical and endometrial glands. In tumor tissues, 37 of 128 tumor categories showed mamma-globin-A staining, 32 of which were derived from one of four organs: breast (6 tumor categories), endometrium (5 tumor categories), ovary (5 tumor categories), and salivary glands (16 tumor categories). Only five additional tumor types showed occasional weak mammaglobin positivity, including medullary thyroid cancer, teratoma of the testis, squamous cell carcinoma of the skin and pharynx, and prostatic adenocarcinoma. Among 1139 evaluable invasive breast carcinomas of no special type, low mammaglobin-A immunostaining was linked to high BRE grade (p = 0.0011), loss of estrogen and progesterone receptor expression (p < 0.0001 each), and triple-negative status (p < 0.0001) but not to patient survival. In endometrial cancer, mammaglobin-A loss was linked to an advanced tumor stage (p = 0.0198). Our data characterize mammaglobin-A as a highly specific marker for tumors derived from either the breast, female genitals, or salivary gland. [ABSTRACT FROM AUTHOR]

Published

2023

6. Seroprevalence of Binding and Neutralizing Antibodies against 39 Human Adenovirus Types in Patients with Neuromuscular Disorders.

Author

Klann, Patrick Julian, Wang, Xiaoyan, Elfert, Anna, Zhang, Wenli, Köhler, Cornelia, Güttsches, Anne-Katrin, Jacobsen, Frank, Weyen, Ute, Roos, Andreas, Ehrke-Schulz, Eric, Ehrhardt, Anja, Vorgerd, Matthias, and Bayer, Wibke

Subjects

NEUROMUSCULAR diseases, GENETIC vectors, IMMUNOGLOBULINS, VIRAL antibodies, ADENOVIRUSES, NEUROMUSCULAR transmission, SEROPREVALENCE

Abstract

High pre-existing antibodies against viral vectors reduce their functionality and may lead to adverse complications. To circumvent this problem in future gene therapy approaches, we tested the seroprevalence of a large range of human adenovirus types in patients with neuromuscular disorders (NMDs) to find appropriate viral vector candidates for gene replacement therapy for NMDs. Binding and neutralizing antibodies against 39 human adenovirus types were tested in the sera of 133 patients with NMDs and 76 healthy controls aged 17–92 years. The influence of age, sex, and NMDs on antibody levels was analyzed. The seroprevalence of different adenoviruses in the cohort varied widely. The highest levels of binding antibodies were detected against HAdV-D27, -C1, -D24, -D70, -B14, -C6, -D13, -B34, and -E4, whereas the lowest reactivity was detected against HAdV-F41, -A31, -B11, -D75, -D8, -D65, -D26, -D80, and -D17. The highest neutralizing reactivity was observed against HAdV-B3, -C2, -E4, -C1, -G52, -C5, and -F41, whereas the lowest neutralizing reactivity was observed against HAdV-D74, -B34, -D73, -B37, -D48, -D13, -D75, -D8, -B35, and -B16. We detected no influence of sex and only minor differences between different age groups. Importantly, there were no significant differences between healthy controls and patients with NMDs. Our data show that patients with NMDs have very similar levels of binding and neutralizing antibodies against HAdV compared to healthy individuals, and we identified HAdV-A31, -B16, -B34, -B35, -D8, -D37, -D48, -D73, -D74, -D75, and -D80 as promising candidates for future vector development due to their low binding and neutralizing antibody prevalence. [ABSTRACT FROM AUTHOR]

Published

2023

7. Analysis of More than 16,000 Human Tumor and Normal Tissues Identifies Uroplakin 3B as a Useful Diagnostic Marker for Mesothelioma and Normal Mesothelial Cells.

Author

Lennartz, Maximilian, Atug, Dennis, Dwertmann Rico, Sebastian, Reiswich, Viktor, Viehweger, Florian, Büscheck, Franziska, Kluth, Martina, Hube-Magg, Claudia, Hinsch, Andrea, Bernreuther, Christian, Sauter, Guido, Burandt, Eike, Marx, Andreas H., Krech, Till, Simon, Ronald, Minner, Sarah, Clauditz, Till S., Jacobsen, Frank, Lebok, Patrick, and Gorbokon, Natalia

Subjects

MESOTHELIOMA, OVARIAN tumors, BLADDER, TISSUES, TRANSITIONAL cell carcinoma, BLADDER cancer

Abstract

Uroplakin 3B (Upk3b) is involved in stabilizing and strengthening the urothelial cell layer of the bladder. Based on RNA expression studies, Upk3b is expressed in a limited number of normal and tumor tissues. The potential use of Upk3b as a diagnostic or prognostic marker in tumor diagnosis has not yet been extensively investigated. A tissue microarray containing 17,693 samples from 151 different tumor types/subtypes and 608 samples of 76 different normal tissue types was analyzed by immunohistochemistry. In normal tissues, Upk3b expression was largely limited to mesothelial cells, urothelial umbrella cells, and amnion cells. In tumor tissues, Upk3b was detectable in only 17 of 151 (11.3%) of tumor types. Upk3b expression was most frequent in mesotheliomas (82.1% of epithelioid and 30.8% of biphasic) and in urothelial tumors of the urinary bladder, where the positivity rate decreased from 61.9% in pTaG2 (low grade) to 58.0% in pTaG3 (high grade) and 14.6% in pT2-4 cancers. Among pT2-4 urothelial carcinomas, Upk3b staining was unrelated to tumor stage, lymph node status, and patient prognosis. Less commonly, Upk3b expression was also seen in Brenner tumors of the ovary (10.8%), as well as in four other subtypes of ovarian cancer (0.9–10.6%). Four additional tumor entities showed a weak to moderate Upk3b positivity in less than 5% of cases. In summary, Upk3b immunohistochemistry is a useful diagnostic tool for the distinction of mesotheliomas from other thoracic tumors and the visualization of normal mesothelial and umbrella cells. [ABSTRACT FROM AUTHOR]

Published

2022

8. Inhibin Alpha Expression in Human Tumors: A Tissue Microarray Study on 12,212 Tumors.

Author

Weidemann, Sören, Noori, Nessar Ahmad, Lennartz, Maximilian, Reiswich, Viktor, Dum, David, Menz, Anne, Chirico, Viktoria, Hube-Magg, Claudia, Fraune, Christoph, Bawahab, Ahmed Abdulwahab, Bernreuther, Christian, Simon, Ronald, Clauditz, Till S., Sauter, Guido, Hinsch, Andrea, Kind, Simon, Jacobsen, Frank, Steurer, Stefan, Minner, Sarah, and Burandt, Eike

Subjects

GRANULOSA cell tumors, INHIBIN, PANCREATIC acinar cells, TESTIS tumors, CELL tumors, ADRENAL cortex

Abstract

As a result of its expression in corresponding normal cell types, inhibin alpha (INHA) is used as an immunohistochemical marker for adrenocortical neoplasms and testicular or ovarian sex cord stromal tumors. However, other tumors can also express INHA. To comprehensively determine INHA expression in cancer, a tissue microarray containing 15,012 samples from 134 different tumor types and subtypes was analyzed by immunohistochemistry. INHA positivity was found in 72 of 134 tumor categories, including 26 categories with ≥1 strongly positive case. A moderate to strong INHA positivity was found in 100% of 37 granulosa cell tumors of the ovary, 100% of 43 other sex cord stromal tumors of the ovary/testis, 100% of 31 granular cell tumors, 78.5% of 28 adenomas, 44% of 25 carcinomas of the adrenal cortex, and 46.7% of 15 pancreatic acinar cell carcinomas. At least a weak INHA positivity was seen in <33% of cases of 46 additional tumor entities. In summary, these data support the use of INHA antibodies for detecting sex cord stromal tumors, granular cell tumors, and adrenocortical neoplasms. Since INHA can also be found in other tumor entities, INHA immunohistochemistry should only be considered as a part of any panel for the distinction of tumor entities. [ABSTRACT FROM AUTHOR]

Published

2022

9. High-Level γ-Glutamyl-Hydrolase (GGH) Expression is Linked to Poor Prognosis in ERG Negative Prostate Cancer.

Author

Melling, Nathaniel, Rashed, Masoud, Schroeder, Cornelia, Hube-Magg, Claudia, Kluth, Martina, Lang, Dagmar, Simon, Ronald, Möller-Koop, Christina, Steurer, Stefan, Sauter, Guido, Jacobsen, Frank, Büscheck, Franziska, Wittmer, Corinna, Clauditz, Till, Krech, Till, Tsourlakis, Maria Christina, Minner, Sarah, Huland, Hartwig, Graefen, Markus, and Budäus, Lars

Subjects

PROSTATE cancer prognosis, HYDROLASE genetics, HYDROLASES regulation, FOLIC acid, CELL proliferation, IMMUNOHISTOCHEMISTRY, PHYSIOLOGY

Abstract

γ-glutamyl-hydrolase (GGH) is a ubiquitously-expressed enzyme that regulates intracellular folate metabolism for cell proliferation, DNA synthesis, and repair. Employing GGH immunohistochemistry on a tissue microarray with 12,427 prostate cancers, we found that GGH expression was negative to low in normal prostate epithelium, whereas 88.3% of our 10,562 interpretable cancers showed GGH expression. GGH staining was considered as low intensity in 49.6% and as high intensity in 38.6% of cancers. High GGH expression was linked to the TMPRSS2:ERG-fusion positive subset of cancers (p < 0.0001), advanced pathological tumor stage, and high Gleason grade (p < 0.0001 each). Further analysis revealed that these associations were merely driven by the subset of ERG-negative cancers, High GGH expression was weakly linked to early biochemical recurrence in ERG negative cancers (p < 0.0001) and independent from established histo-pathological parameters. Moreover, GGH expression was linked to features of genetic instability, including presence of recurrent deletions at 3p, 5q, 6q, and 10q (PTEN, p ≥ 0.01 each), as well as to accelerated cell proliferation as measured by Ki67 immunohistochemistry (p < 0.0001). In conclusion, the results of our study identify GGH as an ERG subtype specific molecular marker with modest prognostic relevance, which may have clinical relevance if analyzed in combination with other molecular markers. [ABSTRACT FROM AUTHOR]

Published

2017

10. Oncolytic Activities of Host Defense Peptides.

Author

Al-Benna, Sammy, Shai, Yechiel, Jacobsen, Frank, and Steinstraesser, Lars

Subjects

ONCOLOGY, TUMORS, DRUG therapy, CANCER treatment, CELL membranes, PHARMACOLOGY, PEPTIDES, MANAGEMENT

Abstract

Cancer continues to be a leading source of morbidity and mortality worldwide in spite of progress in oncolytic therapies. In addition, the incidence of cancers affecting the breast, kidney, prostate and skin among others continue to rise. Chemotherapeutic drugs are widely used in cancer treatment but have the serious drawback of nonspecific toxicity because these agents target any rapidly dividing cell without discriminating between healthy and malignant cells. In addition, many neoplasms eventually become resistant to conventional chemotherapy due to selection for multidrug-resistant variants. The limitations associated with existing chemotherapeutic drugs have stimulated the search for new oncolytic therapies. Host defense peptides (HDPs) may represent a novel family of oncolytic agents that can avoid the shortcomings of conventional chemotherapy because they exhibit selective cytotoxicity against a broad spectrum of malignant human cells, including multi-drug-resistant neoplastic cells. Oncolytic activity by HDPs is usually via necrosis due to cell membrane lysis, but some HDPs can trigger apoptosis in cancer cells via mitochondrial membrane disruption. In addition, certain HDPs are anti-angiogenic which may inhibit cancer progression. This paper reviews oncolytic HDP studies in order to address the suitability of selected HDPs as oncolytic therapies. [ABSTRACT FROM AUTHOR]

Published

2011

11. Host Defense Peptides as Effector Molecules of the Innate Immune Response: A Sledgehammer for Drug Resistance?

Author

Steinstraesser, Lars, Kraneburg, Ursula M., Hirsch, Tobias, Kesting, Marco, Steinau, Hans-Ulrich, Jacobsen, Frank, and Al-Benna, Sammy

Subjects

PEPTIDES, DRUG resistance, IMMUNITY, ANTI-infective agents, SEPSIS, INFLAMMATION, NATURAL immunity, ANTIBIOTICS, VACCINES

Abstract

Host defense peptides can modulate the innate immune response and boost infection-resolving immunity, while dampening potentially harmful pro-inflammatory (septic) responses. Both antimicrobial and/or immunomodulatory activities are an integral part of the process of innate immunity, which itself has many of the hallmarks of successful anti-infective therapies, namely rapid action and broad-spectrum antimicrobial activities. This gives these peptides the potential to become an entirely new therapeutic approach against bacterial infections. This review details the role and activities of these peptides, and examines their applicability as development candidates for use against bacterial infections. [ABSTRACT FROM AUTHOR]

Published

2009

12. Large-Scale Tissue Microarray Evaluation Corroborates High Specificity of High-Level Arginase-1 Immunostaining for Hepatocellular Carcinoma.

Author

Lennartz, Maximilian, Gehrig, Eva, Weidemann, Sören, Gorbokon, Natalia, Menz, Anne, Büscheck, Franziska, Hube-Magg, Claudia, Hinsch, Andrea, Reiswich, Viktor, Höflmayer, Doris, Fraune, Christoph, Jacobsen, Frank, Bernreuther, Christian, Lebok, Patrick, Sauter, Guido, Wilczak, Waldemar, Steurer, Stefan, Burandt, Eike, Marx, Andreas H., and Simon, Ronald

Subjects

HEPATOCELLULAR carcinoma, IMMUNOSTAINING, SQUAMOUS cell carcinoma, TISSUES, TRANSITIONAL cell carcinoma, ARGINASE

Abstract

Arginase-1 catalyzes the conversion of arginine to ornithine and urea. Because of its predominant expression in hepatocytes, it serves as a marker for hepatocellular carcinoma, although other tumor entities can also express arginase-1. To comprehensively determine arginase-1 expression in normal and neoplastic tissues, tissue microarrays containing 14,912 samples from 117 different tumor types and 608 samples of 76 different normal tissue types were analyzed by immunohistochemistry. In normal tissues, arginase-1 was expressed in the liver, the granular layer of the epidermis, and in granulocytes. Among tumors, a nuclear and cytoplasmic arginase-1 immunostaining was predominantly observed in hepatocellular carcinoma, where 96% of 49 cancers were at least moderately positive. Although 22 additional tumor categories showed occasional arginase immunostaining, strong staining was exceedingly rare in these entities. Staining of a few tumor cells was observed in squamous cell carcinomas of various sites. Staining typically involved maturing cells with the beginning of keratinization in these tumors and was significantly associated with a low grade in 635 squamous cell carcinomas of various sites (p = 0.003). Teratoma, urothelial carcinoma and pleomorphic adenomas sometimes also showed arginase expression in areas with squamous differentiation. In summary, arginase-1 immunohistochemistry is highly sensitive and specific for hepatocellular carcinoma if weak and focal staining is disregarded. [ABSTRACT FROM AUTHOR]

Published

2021

13. Angiotensin-Converting Enzyme 2 Protein Is Overexpressed in a Wide Range of Human Tumour Types: A Systematic Tissue Microarray Study on >15,000 Tumours.

Author

Meiners, Jan, Jansen, Kristina, Gorbokon, Natalia, Büscheck, Franziska, Luebke, Andreas M., Kluth, Martina, Hube-Magg, Claudia, Höflmayer, Doris, Weidemann, Sören, Fraune, Christoph, Möller, Katharina, Bernreuther, Christian, Lebok, Patrick, Menz, Anne, Jacobsen, Frank, Clauditz, Till, Sauter, Guido, Uhlig, Ria, Wilczak, Waldemar, and Izbicki, Jakob

Subjects

ANGIOTENSIN converting enzyme, RENAL cell carcinoma, RENIN-angiotensin system, CORPUS luteum, TUMORS

Abstract

Angiotensin-converting enzyme 2 (ACE2) is a regulator in the renin-angiotensin system. ACE2 expression was analysed immunohistochemically in 15,306 samples from 119 tumour types and in 608 samples of 76 normal tissue types. In normal tissue, ACE2 was most abundant in testis and corpus luteum, kidney, small intestine and capillaries of selected organs. At least an occasional weak ACE2 positivity of tumour cells was seen in 83 of 119 (70%) tumour types. ACE2 tumour cell positivity was particularly frequent in papillary (94%) and clear cell (86%) renal cell carcinoma, colorectal adenocarcinoma (81%), mucinous ovarian cancer (61%), cholangiocarcinoma (58%), hepatocellular carcinoma (56%), and in adenocarcinomas of the stomach (47%), pancreas (42%), and the lung (35%). ACE2-positive capillaries were found in 409/12,644 (3%) of analysable tumours, most frequently in tumours with endocrine/neuroendocrine activity. Presence of ACE2-positive capillaries was linked to low stage in papillary thyroid cancer and low grade in neuroendocrine neoplasms. In conclusion, ACE2 expression can occur both in tumour cells and tumour-associated capillaries in a broad variety of different tumour types at highly variable frequencies. [ABSTRACT FROM AUTHOR]

Published

2021

14. Mesothelin Expression in Human Tumors: A Tissue Microarray Study on 12,679 Tumors.

Author

Weidemann, Sören, Gagelmann, Pauline, Gorbokon, Natalia, Lennartz, Maximilian, Menz, Anne, Luebke, Andreas M., Kluth, Martina, Hube-Magg, Claudia, Blessin, Niclas C., Fraune, Christoph, Möller, Katharina, Bernreuther, Christian, Lebok, Patrick, Clauditz, Till S., Jacobsen, Frank, Izbicki, Jakob R., Jansen, Kristina, Sauter, Guido, Uhlig, Ria, and Wilczak, Waldemar

Subjects

BLADDER cancer, MUCINOUS adenocarcinoma, ENDOMETRIAL cancer, TUMORS, THYROID gland, TISSUES, TISSUE arrays

Abstract

Mesothelin (MSLN) represents an attractive molecule for targeted cancer therapies. To identify tumors that might benefit from such therapies, tissue microarrays including 15,050 tumors from 122 different tumor types and 76 healthy organs were analyzed for MSLN expression by immunohistochemistry. Sixty-six (54%) tumor types showed at least occasional weak staining, including 50 (41%) tumor types with at least one strongly positive sample. Highest prevalence of MSLN positivity had ovarian carcinomas (serous 97%, clear cell 83%, endometrioid 77%, mucinous 71%, carcinosarcoma 65%), pancreatic adenocarcinoma (ductal 75%, ampullary 81%), endometrial carcinomas (clear cell 71%, serous 57%, carcinosarcoma 50%, endometrioid 45%), malignant mesothelioma (69%), and adenocarcinoma of the lung (55%). MSLN was rare in cancers of the breast (7% of 1138), kidney (7% of 807), thyroid gland (1% of 638), soft tissues (0.3% of 931), and prostate (0 of 481). High expression was linked to advanced pathological tumor (pT) stage (p < 0.0001) and metastasis (p < 0.0001) in 1619 colorectal adenocarcinomas, but unrelated to parameters of malignancy in 1072 breast-, 386 ovarian-, 174 lung-, 757 kidney-, 171 endometrial-, 373 gastric-, and 925 bladder carcinomas. In summary, numerous important cancer types with high-level MSLN expression might benefit from future anti-MSLN therapies, but MSLN's prognostic relevance appears to be limited. [ABSTRACT FROM AUTHOR]

Published

2021

15. Stimulator of Interferon Genes Protein (STING) Expression in Cancer Cells: A Tissue Microarray Study Evaluating More than 18,000 Tumors from 139 Different Tumor Entities.

Author

Menz A, Zerneke J, Viehweger F, Büyücek S, Dum D, Schlichter R, Hinsch A, Bawahab AA, Fraune C, Bernreuther C, Kluth M, Hube-Magg C, Möller K, Lutz F, Reiswich V, Luebke AM, Lebok P, Weidemann SA, Sauter G, Lennartz M, Jacobsen F, Clauditz TS, Marx AH, Simon R, Steurer S, Burandt E, Gorbokon N, Minner S, and Krech T

Abstract

Stimulator of interferon genes protein (STING) activates the immune response in inflammatory cells. STING expression in cancer cells is less well characterized, but STING agonists are currently being evaluated as anticancer drugs. A tissue microarray containing 18,001 samples from 139 different tumor types was analyzed for STING by immunohistochemistry. STING-positive tumor cells were found in 130 (93.5%) of 139 tumor entities. The highest STING positivity rates occurred in squamous cell carcinomas (up to 96%); malignant mesothelioma (88.5%-95.7%); adenocarcinoma of the pancreas (94.9%), lung (90.3%), cervix (90.0%), colorectum (75.2%), and gallbladder (68.8%); and serous high-grade ovarian cancer (86.0%). High STING expression was linked to adverse phenotypes in breast cancer, clear cell renal cell carcinoma, colorectal adenocarcinoma, hepatocellular carcinoma, and papillary carcinoma of the thyroid ( p < 0.05). In pTa urothelial carcinomas, STING expression was associated with low-grade carcinoma ( p = 0.0002). Across all tumors, STING expression paralleled PD-L1 positivity of tumor and inflammatory cells ( p < 0.0001 each) but was unrelated to the density of CD8+ lymphocytes. STING expression is variable across tumor types and may be related to aggressive tumor phenotype and PD-L1 positivity. The lack of relationship with tumor-infiltrating CD8+ lymphocytes argues against a significant IFN production by STING positive tumor cells.

Published

2024