Your search keyword '"mammary carcinoma"' showing total 2,065 results

1. Insights into the role of connexins and specialized intercellular communication pathways in breast cancer: Mechanisms and applications

Author

Rodríguez-Candela Mateos, Marina, Carpintero-Fernández, Paula, Freijanes, Paz Santiago, Mosquera, Joaquin, Nebril, Benigno Acea, and Mayán, María D.

Published

2024

2. Synthesis, Characterization, Molecular Docking, Cytotoxicity, and Antimicrobial Activity of Schiff Base Ligand and Its Metal Complexes.

Author

Tawfiq, K. M., Al Naymi, Hanan Adnan Shaker, Obaid, Shatha M. H., Jarad, Amer J., Al‐Noor, Taghreed H., and Al‐Sarray, Ali J.

Subjects

*LIGANDS (Chemistry), *ESCHERICHIA coli, *METAL complexes, *MOLECULAR docking, *NUCLEAR magnetic resonance spectroscopy, *SCHIFF bases

Abstract

A Schiff base ligand (L) was synthesized via condensation of N‐(1‐naphthyl)ethylenediamine dihydrochloride with phthalaldehyde. The ligand was characterized by FT‐IR, UV–Vis, 1H NMR, mass spectrometry, and elemental analysis (C, H, N). Five metal complexes (Co(II), Ni(II), Cu(II), Zn(II), and Cd(II)) were prepared with the ligand in a 1:1 (M:L) ratio using an aqueous ethanol solution. The complexes were characterized by FT‐IR, UV–Vis, mass spectrometry, and elemental analysis (C, H, N). Additionally, 1H NMR spectroscopy was employed for Cd(II) complex. Antimicrobial activity of the ligand and its metal complexes against pathogenic bacteria (K. pneumoniae, E. coli, S. aureus, and S. epidermidis) and fungus (C. albicans) were evaluated using the agar well diffusion method. All compounds exhibited inhibitory effects with zone diameters ranging from 8 to 16 mm. The ligand and complexes also displayed significant anticancer activity against a mammary carcinoma cell line. Among them, Zn(II) and Cu(II) complexes demonstrated the highest inhibitory effects (70.68% and 70.57%, respectively), followed by the ligand (61.35%) and Co(II), Cd(II), and Ni(II) complexes (60.34%, 58.96%, and 41.63%, respectively). IC50 values followed a similar trend, ranging from 31.69% (Co(II)) to 165.7% (Cd(II)). Molecular docking studies indicated strong binding affinities of the ligand and the Zn(II) complex to the estrogen receptor. [ABSTRACT FROM AUTHOR]

Published

2025

3. Inhibitory effect of PD173074 drug on DMBA-induced mammary carcinoma in female Swiss albino mice.

Author

Alghamdi, Abeer S., Alobaid, Hussah M., Rady, Ahmed M., AL-Qahtani, Badr Abdullah Aldahmash Wejdan S., Alqarni, Aisha H., Almalki, Samiah A., and Elnagar, Doaa M.

Subjects

*IMMUNOHISTOCHEMISTRY, *LABORATORY mice, *DUCTAL carcinoma, *OXIDATIVE stress, *PYRIMIDINE derivatives, *BREAST

Abstract

Purpose: To determine the effect of PD173074 on mammary carcinoma. Methods: Virgin female mice were randomly divided into 4 groups of 10 mice per group. Group 1 (control) received clean water, group 2 received an oral dose of 50 mg/kg PD173074 twice a week, group 3 received a single dose of 50 mg/kg 7,12-Dimethylbenz(a)anthracene (DMBA) in the breast for carcinoma induction, group 4 received DMBA and after that treated with PD173074 one week later for 4 weeks. Hormonal analysis, oxidative stress, levels of cytokines IL6 and TNF-α, and histopathological and immunohistochemical analysis were carried out. Results: Treatment with PD173074 significantly lowered estrogen, progesterone, oxidative stress indices, cytokines IL6, and TNF-α levels (p < 0.05) raised due to carcinoma induction. Pyrido (2,3-d) pyrimidine derivative PD173074 lowered the Nottingham histopathological score and reduced the incidence of invasive ductal carcinoma. Furthermore, immunohistochemical analysis showed that posttreatment with PD173074 significantly decreased K167 expression (p < 0.05). Conclusion: PD173074 significantly reduces estrogen, progesterone, oxidative stress indices, cytokines, TNF-α, Nottingham histopathological score, and KI-67 expression. Additional studies would be required to validate the actual mechanisms of this drug action. [ABSTRACT FROM AUTHOR]

Published

2024

4. Evaluation of Erythrocytes Indices Platelet Indices and Complete Blood Count in Feline Mammary Carcinomas.

Author

KURBAN, İbrahim and GÜNAY UÇMAK, Zeynep

Subjects

ERYTHROCYTES, BLOOD cell count, INFLAMMATION, HEMATOLOGY, RADIOGRAPHY

Abstract

Copyright of Kocatepe Veterinary Journal / Kocatepe Veteriner Dergisi is the property of Afyon Kocatepe University, Faculty of Veterinary Medicine and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2024

5. Exploring Canine Mammary Cancer through Liquid Biopsy: Proteomic Profiling of Small Extracellular Vesicles.

Author

Novais, Adriana Alonso, Tamarindo, Guilherme Henrique, Melo, Luryan Mikaelly Minotti, Balieiro, Beatriz Castilho, Nóbrega, Daniela, dos Santos, Gislaine, Saldanha, Schaienni Fontoura, de Souza, Fabiana Ferreira, Chuffa, Luiz Gustavo de Almeida, Bracha, Shay, and Zuccari, Debora Aparecida Pires de Campos

Subjects

*BREAST cancer prognosis, *BREAST tumor diagnosis, *PROTEIN analysis, *EXTRACELLULAR vesicles, *BIOLOGICAL models, *CANCER relapse, *CENTRIFUGATION, *LIQUID chromatography-mass spectrometry, *RESEARCH funding, *ELECTRON microscopy, *TUMOR markers, *DOGS, *DISEASE remission, *DESCRIPTIVE statistics, *PROTEOMICS, *ANIMAL experimentation, *MASS spectrometry, *GENE expression profiling, *RESEARCH methodology, *EXOSOMES, BODY fluid examination

Abstract

Simple Summary: We studied canine mammary tumors to better understand similar human breast cancer using a technique called liquid biopsy, which analyzes blood samples to detect disease, focusing on the detection of tiny particles called small extracellular vesicles. These structures are very interesting because they can carry proteins that may indicate the presence of cancer. In this study, we collected blood from healthy dogs, dogs with benign and malignant CMTs, and those in remission and also with recurrence. We found no differences in the size or amount of the vesicles among the groups but identified specific proteins that could serve as markers for cancer. These proteins could potentially help in the diagnosis, prognosis and monitoring of mammary cancer. (Background). Canine mammary tumors (CMTs) have emerged as an important model for understanding pathophysiological aspects of human disease. Liquid biopsy (LB), which relies on blood-borne biomarkers and offers minimal invasiveness, holds promise for reflecting the disease status of patients. Small extracellular vesicles (SEVs) and their protein cargo have recently gained attention as potential tools for disease screening and monitoring. (Objectives). This study aimed to isolate SEVs from canine patients and analyze their proteomic profile to assess their diagnostic and prognostic potential. (Methods). Plasma samples were collected from female dogs grouped into CMT (malignant and benign), healthy controls, relapse, and remission groups. SEVs were isolated and characterized using ultracentrifugation (UC), nanoparticle tracking analysis (NTA) and transmission electron microscopy (TEM). Proteomic analysis of circulating SEVs was conducted using liquid chromatography–mass spectrometry (LC–MS). (Results). While no significant differences were observed in the concentration and size of exosomes among the studied groups, proteomic profiling revealed important variations. Mass spectrometry identified exclusive proteins that could serve as potential biomarkers for mammary cancer. These included Inter-alpha-trypsin inhibitor heavy chain (ITIH2 and ITI4), phosphopyruvate hydratase or alpha enolase (ENO1), eukaryotic translation elongation factor 2 (eEF2), actin (ACTB), transthyretin (TTR), beta-2-glycoprotein 1 (APOH) and gelsolin (GSN) found in female dogs with malignant tumors. Additionally, vitamin D-binding protein (VDBP), also known as group-specific component (GC), was identified as a protein present during remission. (Conclusions). The results underscore the potential of proteins found in SEVs as valuable biomarkers in CMTs. Despite the lack of differences in vesicle concentration and size between the groups, the analysis of protein content revealed promising markers with potential applications in CMT diagnosis and monitoring. These findings suggest a novel approach in the development of more precise and effective diagnostic tools for this challenging clinical condition. [ABSTRACT FROM AUTHOR]

Published

2024

6. Immunohistochemical Detection of Indoleamine 2,3-Dioxygenase in Spontaneous Mammary Carcinomas of 96 Pet Rabbits.

Author

Schöniger, Sandra, Degner, Sophie, Schandelmaier, Claudia, Aupperle-Lellbach, Heike, Zhang, Qian, and Schildhaus, Hans-Ulrich

Subjects

*EUROPEAN rabbit, *INDOLEAMINE 2,3-dioxygenase, *RABBITS, *TUMOR-infiltrating immune cells, *BREAST cancer research, RABBIT diseases

Abstract

Simple Summary: Mammary carcinomas have been diagnosed with increasing frequency in pet rabbits. Prognostic biomarkers are limited, and the only available treatment is surgical excision. Additional treatment options are needed, e.g., for animals in which metastases to internal organs preclude complete tumor removal. Human breast cancer may express the immunosuppressive enzyme indoleamine 2,3-dioxygenase 1 (IDO1), that represents a prognostic biomarker and a possible therapeutic target. Since previous studies revealed similarities between human breast cancer and pet rabbit mammary carcinomas, this study investigated IDO1 immunostaining in 96 mammary carcinomas of 96 pet rabbits with an average age of 5.5 years. All rabbits with reported sex were female. Variable percentages of IDO1-positive tumor cells were detected in 90 (94%) carcinomas. Furthermore, IDO1 immunostaining was observed in the secretory epithelial cells of the adjacent non-neoplastic mammary tissue. This study provides further information on the molecular features of mammary carcinomas in rabbits. It also shows similarities in IDO1 expression between rabbit mammary carcinomas and human breast cancer. These findings can have a mutual benefit. They could lead the development of novel treatment options for rabbits with mammary carcinomas. In addition, they further support the value of rabbits with mammary carcinomas for breast cancer research. For mammary carcinomas in pet rabbits, prognostic biomarkers are poorly defined, and treatment is limited to surgical excision. Additional treatment options are needed for rabbit patients for which surgery is not a suitable option. In human breast cancer, the immunosuppressive enzyme indoleamine 2,3-dioxygenase 1 (IDO1) represents a prognostic biomarker and possible therapeutic target. This retrospective immunohistochemical study examined IDO1 in 96 pet rabbit mammary carcinomas with known mitotic count, hormone receptor status, and percentage of stromal tumor infiltrating lymphocytes (TILs). Tumors were obtained from 96 pet rabbits with an average of 5.5 years. All rabbits with reported sex (n = 88) were female or female-spayed. Of the carcinomas, 94% expressed IDO1, and 86% had sparse TILs consistent with cold tumors. Statistically significant correlations existed between a higher percentage of IDO1-positive tumor cells, lower mitotic counts, and increased estrogen receptor expression. The threshold for significance was IDO1 staining in >10% of tumor cells. These results lead to the assumption that IDO1 expression contributes to tumorigenesis and may represent a prognostic biomarker and possible therapeutic target also in pet rabbit mammary carcinomas. They also support the value of rabbits for breast cancer research. [ABSTRACT FROM AUTHOR]

Published

2024

7. Unveiling innovative therapeutic strategies and future trajectories on stimuli-responsive drug delivery systems for targeted treatment of breast carcinoma.

Author

Naser, Israa Habeeb, Zaid, Muhaned, Ali, Eyhab, Jabar, Hayder Imad, Mustafa, Anfal Nabeel, Alubiady, Mahmood Hasen Shuhata, Ramadan, Montather F., Muzammil, Khursheed, Khalaf, Reem Mohsin, Jalal, Sarah Salah, Alawadi, Ahmed Hussien, and Alsalamy, Ali

Subjects

DRUG delivery systems, CARCINOMA, DRUG resistance, INDIVIDUALIZED medicine, RESEARCH personnel

Abstract

This comprehensive review delineates the latest advancements in stimuli-responsive drug delivery systems engineered for the targeted treatment of breast carcinoma. The manuscript commences by introducing mammary carcinoma and the current therapeutic methodologies, underscoring the urgency for innovative therapeutic strategies. Subsequently, it elucidates the logic behind the employment of stimuli-responsive drug delivery systems, which promise targeted drug administration and the minimization of adverse reactions. The review proffers an in-depth analysis of diverse types of stimuli-responsive systems, including thermoresponsive, pH-responsive, and enzyme-responsive nanocarriers. The paramount importance of material choice, biocompatibility, and drug loading strategies in the design of these systems is accentuated. The review explores characterization methodologies for stimuli-responsive nanocarriers and probes preclinical evaluations of their efficacy, toxicity, pharmacokinetics, and biodistribution in mammary carcinoma models. Clinical applications of stimuli-responsive systems, ongoing clinical trials, the potential of combination therapies, and the utility of multifunctional nanocarriers for the co-delivery of assorted drugs and therapies are also discussed. The manuscript addresses the persistent challenge of drug resistance in mammary carcinoma and the potential of stimuli-responsive systems in surmounting it. Regulatory and safety considerations, including FDA guidelines and biocompatibility assessments, are outlined. The review concludes by spotlighting future trajectories and emergent technologies in stimuli-responsive drug delivery, focusing on pioneering approaches, advancements in nanotechnology, and personalized medicine considerations. This review aims to serve as a valuable compendium for researchers and clinicians interested in the development of efficacious and safe stimuli-responsive drug delivery systems for the treatment of breast carcinoma. [ABSTRACT FROM AUTHOR]

Published

2024

8. Mammary neoplasms in female dogs: Clinical, diagnostic and therapeutic aspects

Author

JR Rueda, CD Porto, RP Franco, IB da Costa, LMC Bueno, RJS Girio, FFR Manhoso, PCS Bueno, and CSF Repetti

Subjects

dogs, mammary tumour, mammary lump, manual, mammary carcinoma, Veterinary medicine, SF600-1100

Abstract

With the increase in the life expectancy of domestic animals and their increasingly affectionate relationship with their owners, it is possible to observe an increase in cases of neoplasms in these animals. Mammary neoplasia mainly affects older females who have not been castrated, due to hormonal dependence for the development of the tumour. The main form of treatment is surgery. This study aims to carry out an updated review on mammary neoplasms in female dogs covering the anatomy, physiology, prevalence, causes, diagnoses, treatments, prevention and prognosis, based on scientific articles by renowned researchers.

Published

2024

9. CELE MAI FRECVENTE TIPURI DE CANCER DIAGNOSTICATE LA PISICI DE PESTE 7 ANI.

Author

Cristea, Otilia Ruxandra and Preda, Cristina Angela

Abstract

Copyright of Romanian Journal of Veterinary Medicine & Pharmacology is the property of Innovation in Health Center and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2024

10. Intranodal Injection of Immune Activator Demonstrates Antitumor Efficacy in an Adjuvant Approach.

Author

Josi, Romano, Ogrina, Anete, Rothen, Dominik, Balke, Ina, Casaramona, Arnau Solé, de Brot, Simone, and Mohsen, Mona O.

Subjects

T-cell exhaustion, SENTINEL lymph nodes, LYMPHADENECTOMY, LYMPH node surgery, HUMORAL immunity, NECK dissection

Abstract

The tumor-draining lymph nodes (tdLN) are the initial site of metastases and are the prime site for generating robust antitumor responses. In this study, we explored the efficacy of a universal immune activator (ImmAct) targeted to the tdLN. This approach can be viewed as an attempt to turn a cold, unresponsive tdLN into a hot, responsive site. The adjuvant antitumor efficacy of our novel intranodal injection was evaluated in an aggressive metastatic mammary carcinoma murine model. The cancer cells were inoculated subcutaneously in the lower quadrant of the mouse to provoke the tdLN (inguinal lymph node). The study encompasses a range of methodologies, including in vivo and in vitro assays and high-dimensional flow cytometry analysis. Our findings demonstrated that intranodal administration of ImmAct following the dissection of the primary tumor led to improved tumor-free survival and minimized weight loss. ImmAct led to both local and systemic alterations in the cellular and humoral immunity. Additionally, after ImmAct treatment, non-responders showed a higher rate of exhausted CD8+ T cells compared to responders. Indeed, our innovative approach surpassed the gold standard surgery of sentinel lymph node excision. Overall, intranodal administration of ImmAct yielded a robust antitumor immune response, offering protection against micrometastases and relapse. [ABSTRACT FROM AUTHOR]

Published

2024

11. Mammary neoplasms in female dogs: Clinical, diagnostic and therapeutic aspects.

Author

REATO RUEDA, JANAINA, DIAS PORTO, CAMILA, PREVEDELLO FRANCO, RODRIGO, BAZZO DA COSTA, ISABELA, CINTRA BUENO, LAIS MELICIO, SILVA GIRIO, RAUL JOSE, RIBEIRO MANHOSO, FABIO FERNANDO, CINCOTTO DOS SANTOS BUENO, PATRICIA, and SAMPAIO FONSECA REPETTI, CLAUDIA

Subjects

FEMALE dogs, DOG anatomy, TUMORS, DOMESTIC animals, LIFE expectancy, RESPITE care

Abstract

With the increase in the life expectancy of domestic animals and their increasingly affectionate relationship with their owners, it is possible to observe an increase in cases of neoplasms in these animals. Mammary neoplasia mainly affects older females who have not been castrated, due to hormonal dependence for the development of the tumour. The main form of treatment is surgery. This study aims to carry out an updated review on mammary neoplasms in female dogs covering the anatomy, physiology, prevalence, causes, diagnoses, treatments, prevention and prognosis, based on scientific articles by renowned researchers. [ABSTRACT FROM AUTHOR]

Published

2024

12. Newcastle disease virus Tabanan-1/ARP/2017 inhibits growth of rat mammary carcinoma models.

Author

Sewoyo, Palagan Senopati, Astawa, I. Nyoman Mantik, Adi, Anak Agung Ayu Mirah, Purwitasari, Made Santi, Tri Hartaputera, I. Nyoman Surya, and Aisyah, Siti

Subjects

NEWCASTLE disease virus, RATS, CARCINOMA, MASTITIS, SPRAGUE Dawley rats, CANCER treatment, VIROTHERAPY

Abstract

The lack of effective therapeutic modalities for mammary cancer is attributed to side effects and therapy resistance, necessitating the exploration of alternative treatment options. Newcastle Disease Virus (NDV) exhibits oncolytic activity, making it a promising candidate for cancer therapy. This study aims to assess the effectiveness of the virulent NDV Tabanan-1/ARP/2017 on the growth of mammary carcinoma. The study involved 15 white female Sprague-Dawley rats induced with mammary carcinoma. After the tumors had developed, the rats were divided into two treatment groups, i.e., treatment 0 (P0) and treatment 1 (P1), which received 500 µL of phosphate-buffered saline and 128 HAU/500 µL of NDV Tabanan-1/ARP/2017, respectively. The rats were euthanized on day 15 post-virotherapy. Rats were necropsied, the tumor was excised to measure its weight, percentage of tumor inhibition, and subsequently routinely processed for histopathological preparations. The tumor weights in each treatment group were 3.70±0.72 and 2.34±0.64 grams, respectively, with a tumor inhibition percentage of 36.62%. The angiogenesis, hemorrhage, and mitotic activity of P1 were lower than those of P0, while inflammatory cell infiltration and areas of necrosis appeared more prominent in the group treated with the NDV. In conclusion, the NDV Tabanan-1/ARP/2017 shows potential as a virotherapy agent for rat mammary carcinoma models. [ABSTRACT FROM AUTHOR]

Published

2024

13. Trattamento dei tumori mammari nella cagna e nella gatta.

Author

Gogny, Anne

Abstract

Copyright of Summa, Animali da Compagnia is the property of Point Veterinaire Italie s.r.l. and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2024

14. Molecular Characterization and Subtyping of Breast Cancer Cell Lines Provide Novel Insights into Cancer Relevant Genes.

Author

Pommerenke, Claudia, Nagel, Stefan, Haake, Josephine, Koelz, Anne Leena, Christgen, Matthias, Steenpass, Laura, and Eberth, Sonja

Subjects

*CELL lines, *TUMOR suppressor genes, *CANCER genes, *BREAST cancer, *GENE regulatory networks, *CANCER cells, *MAMMOGRAMS

Abstract

Continuous cell lines are important and commonly used in vitro models in breast cancer (BC) research. Selection of the appropriate model cell line is crucial and requires consideration of their molecular characteristics. To characterize BC cell line models in depth, we profiled a panel of 29 authenticated and publicly available BC cell lines by mRNA-sequencing, mutation analysis, and immunoblotting. Gene expression profiles separated BC cell lines in two major clusters that represent basal-like (mainly triple-negative BC) and luminal BC subtypes, respectively. HER2-positive cell lines were located within the luminal cluster. Mutation calling highlighted the frequent aberration of TP53 and BRCA2 in BC cell lines, which, therefore, share relevant characteristics with primary BC. Furthermore, we showed that the data can be used to find novel, potential oncogenic fusion transcripts, e.g., FGFR2::CRYBG1 and RTN4IP1::CRYBG1 in cell line MFM-223, and to elucidate the regulatory circuit of IRX genes and KLF15 as novel candidate tumor suppressor genes in BC. Our data indicated that KLF15 was activated by IRX1 and inhibited by IRX3. Moreover, KLF15 inhibited IRX1 in cell line HCC-1599. Each BC cell line carries unique molecular features. Therefore, the molecular characteristics of BC cell lines described here might serve as a valuable resource to improve the selection of appropriate models for BC research. [ABSTRACT FROM AUTHOR]

Published

2024

15. Exosomes from Adipose-Tissue-Derived Stem Cells Induce Proapoptotic Gene Expression in Breast Tumor Cell Line.

Author

Felthaus, Oliver, Vedlin, Simon, Eigenberger, Andreas, Klein, Silvan M., and Prantl, Lukas

Subjects

*STEM cells, *BREAST, *GENE expression, *EXOSOMES, *CELL lines, *BREAST tumors

Abstract

Lipofilling is an option for breast reconstruction after tumor resection to avoid the complications of an implant-based reconstruction. Although some concerns exist regarding the oncological safety of tissue rich in mesenchymal stem cells with their proangiogenic and proliferation-supportive properties, there are also reports that adipose-tissue-derived stem cells can exhibit antitumoral properties. We isolated primary adipose-tissue-derived stem cells. Both conditioned medium and exosomes were harvested from the cell culture and used to treat the breast cancer cell line MCF-7. Cell viability, cytotoxicity, and gene expression of MCF-7 cells in response to the indirect co-culture were evaluated. MCF-7 cells incubated with exosomes from adipose-tissue-derived stem cells show reduced cell viability in comparison to MCF-7 cells incubated with adipose-tissue-derived stem-cell-conditioned medium. Expression of proapoptotic genes was upregulated, and expression of antiapoptotic genes was downregulated. The debate about the oncological safety of autologous fat grafting after tumor resection continues. Here, we show that exosomes from adipose-tissue-derived stem cells exhibit some antitumoral properties on breast cancer cell line MCF-7. [ABSTRACT FROM AUTHOR]

Published

2024

16. Multiple SNPs Downregulate Gene Expression of Matrix Metallopeptidase 2 in MCF7 Breast Cancer Cells.

Author

Suhaimi, Shafinah Ahmad, Chan Soon Choy, Chong Pei Pei, Chau De Ming, Saad, Norazalina, and Rosli, Rozita

Subjects

*GENE expression, *REVERSE transcriptase polymerase chain reaction, *METASTATIC breast cancer, *SINGLE nucleotide polymorphisms, *BREAST cancer

Abstract

Introduction: On a global scale, breast cancer contributes the highest cancer-related deaths in women due to metastasis which renders the treatments ineffective and non-targeted. The members of Matrix Metallopeptidases, particularly Matrix Metallopeptidase 2 (MMP2), are among the key players in breast cancer metastasis. In most cases, MMP2 was markedly upregulated and linked to poor prognosis. In a previous study, in silico analyses revealed that several coding single nucleotide polymorphisms (SNPs) of MMP2 were shown to reduce gene expression and mRNA stability of MMP2 in Malaysian breast cancer patients. Therefore, to validate the in silico predictions, the objective of this study was to determine the effects of multiple coding SNPs of MMP2 on the gene expression and mRNA stability of MMP2 in breast cancer cells. Methods: In the current study, breast adenocarcinoma MCF7 cells were transfected with MMP2 wild type and variant containing the coding SNPs. After confirmation of transfection by DNA sequencing, the gene expression level of MMP2 was evaluated by quantitative reverse transcription polymerase chain reaction (RT-qPCR) whereas mRNA stability of MMP2 was determined following treatment with actinomycin D. Results: MMP2 wild type and variant were successfully transfected in MCF7 cells based on sequencing and PCR analysis. It was found that the presence of coding SNPs lowered the gene expression level of MMP2, but not the stability of MMP2 mRNA. Conclusion: This study supports the in silico effects of MMP2 coding SNPs on its gene expression in an in vitro model. [ABSTRACT FROM AUTHOR]

Published

2024

17. Rs867228 in FPR1 accelerates the manifestation of luminal B breast cancer

Author

Vincent Carbonnier, Julie Le Naour, Thomas Bachelot, Erika Vacchelli, Fabrice André, Suzette Delaloge, and Guido Kroemer

Subjects

Cancer screening, immunodeficiency, immunosurveillance, mammary carcinoma, polygenic risk score, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Formyl peptide receptor-1 (FPR1) is a pathogen recognition receptor involved in the detection of bacteria, in the control of inflammation, as well as in cancer immunosurveillance. A single nucleotide polymorphism in FPR1, rs867228, provokes a loss-of-function phenotype. In a bioinformatic study performed on The Cancer Genome Atlas (TCGA), we observed that homo-or heterozygosity for rs867228 in FPR1 (which affects approximately one-third of the population across continents) accelerates age at diagnosis of specific carcinomas including luminal B breast cancer by 4.9 years. To validate this finding, we genotyped 215 patients with metastatic luminal B mammary carcinomas from the SNPs To Risk of Metastasis (SToRM) cohort. The first diagnosis of luminal B breast cancer occurred at an age of 49.2 years for individuals bearing the dysfunctional TT or TG alleles (n = 73) and 55.5 years for patients the functional GG alleles (n = 141), meaning that rs867228 accelerated the age of diagnosis by 6.3 years (p=0.0077, Mann & Whitney). These results confirm our original observation in an independent validation cohort. We speculate that it may be useful to include the detection of rs867228 in breast cancer screening campaigns for selectively increasing the frequency and stringency of examinations starting at a relatively young age.

Published

2023

18. A Scoping Review on Tyrosine Kinase Inhibitors in Cats: Current Evidence and Future Directions.

Author

Žagar, Žiga and Schmidt, Jarno M.

Subjects

*PROTEIN-tyrosine kinase inhibitors, *MAST cell tumors, *CATS, *SQUAMOUS cell carcinoma, *THERAPEUTICS, *CELL physiology

Abstract

Simple Summary: Oncology is a rapidly advancing field in small-animal medicine, underscoring the importance of innovative therapeutic approaches. Tyrosine kinase inhibitors (TKIs) are drugs that block various important cellular functions and play an important role in treating cancer in people and dogs. However, their role in feline oncology is less established. This comprehensive review surveys the existing literature on tyrosine kinases (TKs) and the use of TKIs in cats, aiming to identify knowledge gaps, speculate on potential indications and lay the groundwork for future investigations. Diverse feline tissues have been examined for various TK expressions. However, although limited evidence exists on the use of TKIs in specific feline tumors, it trails behind progress in human and canine oncology. We believe additional research could identify new uses for these drugs and improve therapeutic options for cats with cancer in the future. Tyrosine kinase inhibitors (TKIs) have become invaluable in the treatment of human and canine malignancies, but their role in feline oncology is less defined. While toceranib phosphate and masitinib mesylate are licensed for use in dogs, no TKI is yet approved for cats. This review systematically maps the research conducted on the expression of tyrosine kinases in neoplastic and non-neoplastic domestic feline tissues, as well as the in vitro/in vivo use of TKIs in domestic cats. We identify and discuss knowledge gaps and speculate on the further research and potential indications for TKI use in cats. A comprehensive search of three electronic databases and relevant paper reference lists identified 139 studies meeting the inclusion criteria. The most commonly identified tumors were mast cell tumors (MCTs), mammary and squamous cell carcinomas and injection-site sarcomas. Based on the current literature, toceranib phosphate appears to be the most efficacious TKI in cats, especially against MCTs. Exploring the clinical use of TKIs in mammary carcinomas holds promise. Despite the progress, currently, the evidence falls short, underscoring the need for further research to discover new indications in feline oncology and to bridge the knowledge gaps between human and feline medicine. [ABSTRACT FROM AUTHOR]

Published

2023

19. Mammary carcinoma: Comparative oncology between small animals and humans—New therapeutic tools.

Author

Frénel, Jean‐Sébastien and Nguyen, Frédérique

Subjects

*ONCOLOGY, *THERAPY dogs, *TUMOR classification, *HORMONE therapy, *COMBINED modality therapy, *DOGS, *CATS

Abstract

The poor outcomes associated with mammary carcinomas (MCs) in dogs and cats in terms of locoregional recurrence, distant metastasis and survival, highlight the need for better management of mammary cancers in small animals. By contrast, the outcomes of women with breast cancer (BC) have dramatically improved during the last 10 years, notably thanks to new therapeutic strategies. The aim of this article was to imagine what could be the future of therapy for dogs and cats with MCs if it became inspired from current practices in human BC. This article focuses on the importance of taking into account cancer stage and cancer subtypes in therapeutic plans, on locoregional treatments (surgery, radiation therapy), new developments in endocrine therapy, chemotherapy, PARP inhibitors and immunotherapy. Ideally, multimodal treatment regimens would be chosen according to cancer stage and cancer subtypes, and according to predictive factors that are still to be defined. [ABSTRACT FROM AUTHOR]

Published

2023

20. Lymphological Liposculpture for Secondary Lymphedema after Breast Cancer and Gynecological Tumors: Long-Term Results after 15 Years

Author

Manuel E. Cornely

Subjects

lymphedema, complex decongestive therapy, mammary carcinoma, cervical carcinoma, liposuction, lipohyperplasia dolorosa, Surgery, RD1-811

Abstract

Background Untreated lymphedema of an extremity leads to an increase in volume. The therapy of this condition can be conservative or surgical. Methods “Lymphological liposculpture” is a two-part procedure consisting of resection and conservative follow-up treatment to achieve curative volume adjustment of the extremities in secondary lymphedema. This treatment significantly reduces the need for complex decongestive therapy (CDT). From 2005 to 2020, 3,184 patients with secondary lymphedema after breast cancer and gynecological tumors were treated in our practice and clinic. “Lymphological liposculpture” was applied to 65 patients, and the data were recorded and evaluated by means of perometry and questionnaires. Results The alignment of the sick to the healthy side was achieved in all patients. In 58.42% (n = 38), the CDT treatment could be completely stopped postoperatively; in another 33.82% (n = 22) of the patients, a permanent reduction of the CDT was achieved. In 7.69% (n = 5) patients, the postoperative CDT could not be reduced. A total of 92.30% (n = 60) of the patients described a lasting significant improvement in their quality of life. Conclusion “Lymphological liposculpture” is a standardized curative sustainable procedure for secondary lymphedema for volume adjustment of the extremities and reduction of postoperative CDT with eminent improvement of the quality of life.

Published

2023

21. A case report of mammary carcinoma in royal Bengal Tiger

Author

Manasa, B. Baby, Sujani, G., Babu, K. Nagesh, Srinivas, V., Purushotham, Ch., Nandani, S., Ratnakumari, L., and Kumar, R. Amarendhra

Published

2023

22. Intranodal Injection of Immune Activator Demonstrates Antitumor Efficacy in an Adjuvant Approach

Author

Romano Josi, Anete Ogrina, Dominik Rothen, Ina Balke, Arnau Solé Casaramona, Simone de Brot, and Mona O. Mohsen

Subjects

virus-like particles, immune-activator, intranodal, mammary carcinoma, adjuvant therapy, Medicine

Abstract

The tumor-draining lymph nodes (tdLN) are the initial site of metastases and are the prime site for generating robust antitumor responses. In this study, we explored the efficacy of a universal immune activator (ImmAct) targeted to the tdLN. This approach can be viewed as an attempt to turn a cold, unresponsive tdLN into a hot, responsive site. The adjuvant antitumor efficacy of our novel intranodal injection was evaluated in an aggressive metastatic mammary carcinoma murine model. The cancer cells were inoculated subcutaneously in the lower quadrant of the mouse to provoke the tdLN (inguinal lymph node). The study encompasses a range of methodologies, including in vivo and in vitro assays and high-dimensional flow cytometry analysis. Our findings demonstrated that intranodal administration of ImmAct following the dissection of the primary tumor led to improved tumor-free survival and minimized weight loss. ImmAct led to both local and systemic alterations in the cellular and humoral immunity. Additionally, after ImmAct treatment, non-responders showed a higher rate of exhausted CD8+ T cells compared to responders. Indeed, our innovative approach surpassed the gold standard surgery of sentinel lymph node excision. Overall, intranodal administration of ImmAct yielded a robust antitumor immune response, offering protection against micrometastases and relapse.

Published

2024

23. Lymphological Liposculpture for Secondary Lymphedema after Breast Cancer and Gynecological Tumors: Long-Term Results after 15 Years.

Author

Cornely, Manuel E.

Subjects

LYMPHEDEMA, BREAST cancer, TUMORS, CONSERVATIVE treatment

Abstract

Background Untreated lymphedema of an extremity leads to an increase in volume. The therapy of this condition can be conservative or surgical. Methods "Lymphological liposculpture" is a two-part procedure consisting of resection and conservative follow-up treatment to achieve curative volume adjustment of the extremities in secondary lymphedema. This treatment significantly reduces the need for complex decongestive therapy (CDT). From 2005 to 2020, 3,184 patients with secondary lymphedema after breast cancer and gynecological tumors were treated in our practice and clinic. "Lymphological liposculpture" was applied to 65 patients, and the data were recorded and evaluated by means of perometry and questionnaires. Results The alignment of the sick to the healthy side was achieved in all patients. In 58.42% (n = 38), the CDT treatment could be completely stopped postoperatively; in another 33.82% (n = 22) of the patients, a permanent reduction of the CDT was achieved. In 7.69% (n = 5) patients, the postoperative CDT could not be reduced. A total of 92.30% (n = 60) of the patients described a lasting significant improvement in their quality of life. Conclusion "Lymphological liposculpture" is a standardized curative sustainable procedure for secondary lymphedema for volume adjustment of the extremities and reduction of postoperative CDT with eminent improvement of the quality of life. [ABSTRACT FROM AUTHOR]

Published

2023

24. Interleukin-10 overexpression in 4T1 cells: A gateway to suppressing mammary carcinoma growth.

Author

Wang, Xiaoqin, Wang, Xiaoqian, Wang, Dan, Zhou, Can, Lv, Kaige, Ma, Yanfen, Chang, Wenjing, Wang, Baofeng, Hu, Jian, Ji, Yanhong, Dai, Zhijun, and Ma, Yunfeng

Subjects

*MYELOID-derived suppressor cells, *MYELOID cells, *T cells, *CHEMOKINES, *CELL differentiation

Abstract

[Display omitted] • IL-10 overexpression in TNBC suppresses tumor growth by increasing IFN-γ secreting CD8+ T cells and decreasing MDSCs in the tumor microenvironment. • Tumor-derived IL-10 reduces MDSCs infiltration through inhibition of myeloid cell differentiation and CXCL5 downregulation. • CXCL5 expression and MDSC infiltration correlate in human breast cancer, suggesting targeting the IL-10-CXCL5-MDSCs axis for immunotherapy. Interleukin-10 (IL-10) exerts complex effects on tumor growth, exhibiting both pro- and anti-tumor properties. Recent focus on the anti-inflammatory properties of IL-10 has highlighted its potential anti-tumor properties, particularly through the enhancement of CD8+ T cell activity. However, further research is needed to fully elucidate its other anti-tumor mechanisms. Our study investigates novel anti-tumor mechanisms of IL-10 in a murine mammary carcinoma model (4T1). We found that IL-10 overexpression in mouse 4T1 cells suppressed tumor growth in vivo. This suppression was accompanied by an increase in IFN-γ-secreting CD8+ T cells and a decrease in myeloid-derived suppressor cells (MDSCs) in tumor tissue. In vitro experiments showed that IL-10-rich tumor cell-derived supernatants inhibited myeloid cell differentiation into monocytic and granulocytic MDSCs while reducing MDSCs migration. In addition, IL-10 overexpression downregulated CXCL5 expression in 4T1 cells, resulting in decreased CXCR2+ MDSCs infiltration. Using RAG1-deficient mice and CXCL5 knockdown tumor models, we demonstrated that the anti-tumor effects of IL-10 depend on both CD8+ T cells and reduced MDSC infiltration. IL-10 attenuated the immunosuppressive tumor microenvironment by enhancing CD8+ T cell activity and inhibiting MDSCs infiltration. In human breast cancer, we observed a positive correlation between CXCL5 expression and MDSC infiltration. Our findings reveal a dual mechanism of IL-10-mediated tumor suppression: (1) direct enhancement of CD8+ T cell activity and (2) indirect reduction of immunosuppressive MDSCs through CXCL5 downregulation and inhibition of myeloid cell differentiation. This study provides new insights into the role of IL-10 in anti-tumor immunity and suggests potential strategies for breast cancer immunotherapy by modulating the IL-10-CXCL5-MDSCs axis. [ABSTRACT FROM AUTHOR]

Published

2024

25. Rs867228 in FPR1 accelerates the manifestation of luminal B breast cancer.

Author

Carbonnier, Vincent, Le Naour, Julie, Bachelot, Thomas, Vacchelli, Erika, André, Fabrice, Delaloge, Suzette, and Kroemer, Guido

Subjects

BREAST cancer, SINGLE nucleotide polymorphisms, DISEASE risk factors, EARLY detection of cancer, PEPTIDES

Abstract

Formyl peptide receptor-1 (FPR1) is a pathogen recognition receptor involved in the detection of bacteria, in the control of inflammation, as well as in cancer immunosurveillance. A single nucleotide polymorphism in FPR1, rs867228, provokes a loss-of-function phenotype. In a bioinformatic study performed on The Cancer Genome Atlas (TCGA), we observed that homo-or heterozygosity for rs867228 in FPR1 (which affects approximately one-third of the population across continents) accelerates age at diagnosis of specific carcinomas including luminal B breast cancer by 4.9 years. To validate this finding, we genotyped 215 patients with metastatic luminal B mammary carcinomas from the SNPs To Risk of Metastasis (SToRM) cohort. The first diagnosis of luminal B breast cancer occurred at an age of 49.2 years for individuals bearing the dysfunctional TT or TG alleles (n = 73) and 55.5 years for patients the functional GG alleles (n = 141), meaning that rs867228 accelerated the age of diagnosis by 6.3 years (p=0.0077, Mann & Whitney). These results confirm our original observation in an independent validation cohort. We speculate that it may be useful to include the detection of rs867228 in breast cancer screening campaigns for selectively increasing the frequency and stringency of examinations starting at a relatively young age. [ABSTRACT FROM AUTHOR]

Published

2023

26. Statistical Study of Cancer in Diyala Provenance.

Author

Mohammad, Salam Hasoon and Salman, Ruaa A.

Subjects

BENIGN tumors, CELL proliferation, PATHOLOGICAL laboratories, TUMORS

Abstract

Copyright of Diyala Journal of Medicine is the property of Republic of Iraq Ministry of Higher Education & Scientific Research (MOHESR) and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

27. Human breast microbiome correlates with prognostic features and immunological signatures in breast cancer

Author

Alice Tzeng, Naseer Sangwan, Margaret Jia, Chin-Chih Liu, Karen S. Keslar, Erinn Downs-Kelly, Robert L. Fairchild, Zahraa Al-Hilli, Stephen R. Grobmyer, and Charis Eng

Subjects

Host microbial interactions, Biomarkers, Microbiota, Mammary carcinoma, Tumor microenvironment, Medicine, Genetics, QH426-470

Abstract

Abstract Background Currently, over half of breast cancer cases are unrelated to known risk factors, highlighting the importance of discovering other cancer-promoting factors. Since crosstalk between gut microbes and host immunity contributes to many diseases, we hypothesized that similar interactions could occur between the recently described breast microbiome and local immune responses to influence breast cancer pathogenesis. Methods Using 16S rRNA gene sequencing, we characterized the microbiome of human breast tissue in a total of 221 patients with breast cancer, 18 individuals predisposed to breast cancer, and 69 controls. We performed bioinformatic analyses using a DADA2-based pipeline and applied linear models with White’s t or Kruskal–Wallis H-tests with Benjamini–Hochberg multiple testing correction to identify taxonomic groups associated with prognostic clinicopathologic features. We then used network analysis based on Spearman coefficients to correlate specific bacterial taxa with immunological data from NanoString gene expression and 65-plex cytokine assays. Results Multiple bacterial genera exhibited significant differences in relative abundance when stratifying by breast tissue type (tumor, tumor adjacent normal, high-risk, healthy control), cancer stage, grade, histologic subtype, receptor status, lymphovascular invasion, or node-positive status, even after adjusting for confounding variables. Microbiome–immune networks within the breast tended to be bacteria-centric, with sparse structure in tumors and more interconnected structure in benign tissues. Notably, Anaerococcus, Caulobacter, and Streptococcus, which were major bacterial hubs in benign tissue networks, were absent from cancer-associated tissue networks. In addition, Propionibacterium and Staphylococcus, which were depleted in tumors, showed negative associations with oncogenic immune features; Streptococcus and Propionibacterium also correlated positively with T-cell activation-related genes. Conclusions This study, the largest to date comparing healthy versus cancer-associated breast microbiomes using fresh-frozen surgical specimens and immune correlates, provides insight into microbial profiles that correspond with prognostic clinicopathologic features in breast cancer. It additionally presents evidence for local microbial–immune interplay in breast cancer that merits further investigation and has preventative, diagnostic, and therapeutic potential.

Published

2021

28. Mouse Mammary Tumor Virus (MMTV) and MMTV-like Viruses: An In-depth Look at a Controversial Issue.

Author

Parisi, Francesca, Freer, Giulia, Mazzanti, Chiara Maria, Pistello, Mauro, and Poli, Alessandro

Subjects

*MOUSE mammary tumor virus, *EPITHELIAL cells

Abstract

Since its discovery as a milk factor, mouse mammary tumor virus (MMTV) has been shown to cause mammary carcinoma and lymphoma in mice. MMTV infection depends upon a viral superantigen (sag)-induced immune response and exploits the immune system to establish infection in mammary epithelial cells when they actively divide. Simultaneously, it avoids immune responses, causing tumors through insertional mutagenesis and clonal expansion. Early studies identified antigens and sequences belonging to a virus homologous to MMTV in human samples. Several pieces of evidence fulfill a criterion for a possible causal role for the MMTV-like virus in human breast cancer (BC), though the controversy about whether this virus was linked to BC has raged for over 40 years in the literature. In this review, the most important issues related to MMTV, from its discovery to the present days, are retraced to fully explore such a controversial issue. Furthermore, the hypothesis of an MMTV-like virus raised the question of a potential zoonotic mouse–man transmission. Several studies investigate the role of an MMTV-like virus in companion animals, suggesting their possible role as mediators. Finally, the possibility of an MMTV-like virus as a cause of human BC opens a new era for prevention and therapy. [ABSTRACT FROM AUTHOR]

Published

2022

29. A Plasmonic Supramolecular Nanohybrid as a Contrast Agent for Site‐Selective Computed Tomography Imaging of Tumor.

Author

Bindra, Anivind Kaur, Sreejith, Sivaramapanicker, Prasad, Rajendra, Gorain, Mahadeo, Thomas, Rijil, Jana, Deblin, Nai, Mui Hoon, Wang, Dongdong, Tharayil, Abhimanyu, Kundu, Gopal C., Srivastava, Rohit, Thomas, Sabu, Lim, Chwee Teck, and Zhao, Yanli

Subjects

*CONTRAST media, *COMPUTED tomography, *PLASMONICS, *GOLD nanoparticles, *PYRENE derivatives

Abstract

Design of organic–inorganic hybrids by anchoring of plasmonic materials such as gold nanoparticles (AuNPs) on self‐assembled organic substrates is useful but challenging. Herein, in situ anchoring of plasmonic nanoparticles on the surface of a designed spherical assembly via AuS bond formation is presented. First, a thiol tailed pyrene derivative (2) undergoes solvent dependent self‐assembly, transforming into an organic spherical aggregate (2agg). The thiol (‐SH) rich surface of the organic assembly allows cumulative anchoring of AuNPs on the surface to form an organic–inorganic hybrid (Au@2agg). Further coating of biocompatible polyethylene glycol (PEG) leads to the construction of the final multicomponent system (PEG‐Au@2agg) exhibiting morphological and spectroscopic features. The potential of PEG‐Au@2agg as a bioprobe and a contrast agent is investigated by X‐ray computed tomography (CT) experiments in vivo. High X‐ray attenuation of directly anchored AuNP clusters on the surface of this supramolecular nanohybrids enhances the X‐ray CT contrast and allows tracing of site‐selective accumulation in mouse 4T1 breast tumor. Thus, this approach of designing organic–inorganic nanohybrids paves the way for developing future intelligent multifunctional nanosystems capable of cancer detection and imaging. [ABSTRACT FROM AUTHOR]

Published

2022

30. Circulating microRNA as biomarkers of canine mammary carcinoma in dogs

Author

Eric J. Fish, Esther Gisela Martinez‐Romero, Patricia DeInnocentes, Jey W. Koehler, Nripesh Prasad, Annette N. Smith, and Richard Curt Bird

Subjects

canine, microRNA, serum biomarkers, mammary carcinoma, Veterinary medicine, SF600-1100

Abstract

Abstract Background Differentiating benign from canine malignant mammary tumors requires invasive surgical biopsy. Circulating microRNAs (miRNA) may represent promising minimally invasive cancer biomarkers in people and animals. Objectives To evaluate the serum mRNA profile between dogs with and without mammary carcinoma, and to determine if any of these markers have prognostic significance. Animals Ten healthy client‐owned female dogs (5 intact, 5 spayed) and 10 dogs with histologically confirmed mammary carcinoma were included; 9 were client‐owned, whereas 1 was a research colony dog. Methods Retrospective study. Serum miRNA was evaluated by RNA deep‐sequencing (RNAseq) and digital droplet PCR (dPCR).Expression of candidate biomarkers miR‐18a, miR‐19b, miR‐29b, miR‐34c, miR‐122, miR‐125a, and miR‐181a was compared with clinical characteristics, including grade, metastasis, and survival. Results 452 unique serum miRNAs were detected by RNAseq. Sixty‐five individual miRNAs were differentially expressed (>±1.5‐fold) and statistically significant between groups. Serum miR‐19b (P = .003) and miR‐125a (P

Published

2020

31. Effect of perioperative desmopressin in cats with mammary carcinoma treated with bilateral mastectomy.

Author

Wood, Christopher J., Chu, Margaret L., Selmic, Laura E., Mayhew, Philipp D., Holt, David E., Martano, Marina, Séguin, Bernard, Singh, Ameet, Boston, Sarah E., Lux, Cassie, and Liptak, Julius M.

Subjects

*DESMOPRESSIN, *MASTECTOMY, *CANCER relapse, *CARCINOMA, *SURGICAL complications, *SURVIVAL rate, *BEAGLE (Dog breed)

Abstract

Perioperative administration of desmopressin has shown to significantly decrease rates of local recurrence and metastasis, and increase survival times in dogs with grade II and III mammary carcinomas. The objective of this study was to compare the oncologic outcome of cats with mammary carcinoma treated with bilateral mastectomy with or without perioperative administration of desmopressin. Medical records from nine veterinary institutions were searched to identify cats diagnosed with mammary carcinoma treated with bilateral mastectomy. Sixty cats treated with single-session or staged bilateral mastectomy were included. There were no significant differences in oncologic outcomes found between cats treated and not treated with desmopressin. No adverse effects were seen in any of the cats treated with perioperative desmopressin. Postoperative complications occurred in 18 cats (38.3%) treated with single-session bilateral mastectomy and in three cats (23.1%) treated with staged bilateral mastectomy (P = .48). Histologic grade and a modification of a proposed five-stage histologic staging system were both prognostic for disease-free interval. Incomplete histologic excision was associated with significantly increased rates of metastasis and tumour progression, and a shorter median survival time (MST). Cats that developed local recurrence also had a significantly shorter MST. The results of this study do not support the use of perioperative desmopressin to improve outcome when performing bilateral mastectomy for the treatment of mammary carcinoma in cats. [ABSTRACT FROM AUTHOR]

Published

2021

32. Assessing the viability of carbamoylethyl pullulan-g-stearic acid based smart polymeric micelles for tumor targeting of raloxifene.

Author

Sethi, Sheshank, Bhatia, Sachin, Kamboj, Sunil, Singh, Ram Sarup, and Rana, Vikas

Subjects

MICELLES, STEARIC acid, RALOXIFENE, ANTINEOPLASTIC agents, GLUCOPYRANOSE, ACRYLAMIDE, MOIETIES (Chemistry), ACIDS

Abstract

The present investigation entails the synthesis of smart pullulan polymeric micelles for evaluating its tumor targeting potential. For this purpose, two step polymerization synthesis reactions were conducted. In the first step, carbamoylethylation occurs by reaction of the free alcoholic moieties at 6th position of glucopyranose unit of pullulan with acrylamide in presence of alkali to obtain carbamoylethyl pullulan (CmP). In the second step, CmP undergoes graft polymerization with stearic acid (SA) to obtain CmP-g-stearic acid diblock co-polymer (CmP-g-SA) as evident from FTIR and NMR analysis. The XpRD spectra showed crystalline nature that was further confirmed by SEM indicating rough and poly-porous morphology. The QbD based optimized formulations of raloxifene HCl (RLX) loaded polymeric micelles (RLX PMs) exhibited pH-dependent release profile with added advantage of 1.2 times reduction in percentage hemolysis giving substantial compatibility with erythrocytes. In vivo pharmacokinetic performance of RLX PMs suggested enhanced mean residence time and volume of distribution. Besides, the biodistribution study of RLX PMs manifested enhanced entry of RLX in mammary carcinoma tissues as compared to normal tissues suggested that CmP-g-SA based micelles enhanced the anti-tumor activity of RLX. Overall, the findings pointed toward the biocompatibility of CmP-g-SA as a potential carrier system for the delivery of RLX. [ABSTRACT FROM AUTHOR]

Published

2021

33. Neoplasia and Tumor-Like Lesions in Pet Rabbits (Oryctolagus cuniculus): A Retrospective Analysis of Cases Between 1995 and 2019.

Author

Bertram, Christof A., Bertram, Beate, Bartel, Alexander, Ewringmann, Anja, Fragoso-Garcia, Marco A., Erickson, Nancy A., Müller, Kerstin, and Klopfleisch, Robert

Subjects

EUROPEAN rabbit, RABBITS, TUMORS, LABORATORY rabbits, UTERINE tumors, MECKEL diverticulum

Abstract

Prevalence and age distribution of tumors is largely unknown in pet rabbits. Currently available studies focused on specific organ systems or specific tumor types and never covered a comparative examination of all tumor types. Previous studies on laboratory rabbits suggested a low tumor prevalence but were mostly limited to young adult animals. In the present study, all tumor types and several tumor-like lesions of all organ systems were analyzed retrospectively in archived pet rabbit samples of all ages. Cases included necropsy cases (n = 2,014) or postmortem tissue samples (n = 102) as well as surgical biopsies (n = 854). All lesions suspicious of neoplasia were reevaluated by histopathology and, when indicated, by immunohistochemistry. Necropsy cases had a tumor prevalence of 14.4% in both sexes or 19.8% in female intact rabbits of all age groups, and up to 47.2% or 66.7%, respectively, in rabbits older than 6 years. Overall, the most common tumor types were uterine adenocarcinoma (prevalence in female intact animals: 13.1%), lymphoma (prevalence: 2.8%), and thymoma (prevalence: 2.1%). Lymphoma, the most common tumor of rabbits ≤24 months of age, were of B-cell immunophenotype in 96% of cases and most commonly located in the lymph nodes (57%), gastrointestinal tract (54%), kidneys (48%), spleen (42%), and liver (41%). Tumors accounted for 81.1% of surgical biopsies and mostly comprised cutaneous, mammary, and uterine tumors. In conclusion, tumor types and prevalence varied significantly with respect to age, revealing some differences from previous studies on laboratory rabbits. [ABSTRACT FROM AUTHOR]

Published

2021

34. Functional Analysis of Matrix Metallopeptidase-3 (MMP3) Coding Single Nucleotide Polymorphisms in MCF7 Breast Cancer Cells.

Author

Suhaimi, Shafinah Ahmad, Soon Choy Chan, Saad, Norazalina, De Ming Chau, Pei Pei Chong, and Rosli, Rozita

Subjects

*SINGLE nucleotide polymorphisms, *MATRIX metalloproteinases, *METASTATIC breast cancer, *BREAST cancer, *FUNCTIONAL analysis

Abstract

Introduction: Due to its role in cancer metastasis, matrix metallopeptidase 3 (MMP3) has been targeted for improvement of current treatment and diagnosis of breast cancer, particularly as biomarker of cancer metastasis. Previously, in silico analysis in Malaysian breast cancer patients revealed that several coding single nucleotide polymorphisms (SNPs) of MMP3 were predicted to reduce its mRNA stability and expression, and hence contribute to a lower risk of developing breast cancer metastasis. However, functional predictions made with in silico analyses do not often reflect actual biological effects of SNPs due to unforeseen biological intricacies. Therefore, in vitro corroboration of biological effects by the genetic variants following in silico predictions is extremely crucial. The current study aimed to confirm the effects of MMP3 coding SNPs at mRNA and protein levels as well as on cancer invasiveness in vitro. Methods: In this study, plasmids containing wild-type (MMP3-WT) and coding SNPs of MMP3 (MMP3-Var) were stably transfected into breast carcinoma MCF7 cell line. Then, comparisons of mRNA stability, gene and protein expression levels, and enzymatic activity between MMP3-WT and MMP3-Var were made via quantitative real time polymerase chain reaction (RT-qPCR), Western blotting and MMP3 activity assay, respectively. Finally, the effect of MMP3-Var on cell invasiveness in MCF7 cells was evaluated by Transwell invasion assay. Results: Although there was no difference in gene expression level of MMP3-WT and MMP3-Var, the mRNA stability of MMP3-Var was significantly lower than MMP3-WT. Moreover, protein expression and enzymatic activity of MMP3-Var were also significantly lower than MMP3-WT. Similarly, cell invasion of MCF7 cells transfected with MMP3-Var was significantly reduced. Conclusion: In conclusion, the effect of MMP3 coding SNPs towards breast cancer invasiveness was determined in vitro. This finding may provide a better understanding between the association of MMP3 coding SNPs with breast cancer metastasis. [ABSTRACT FROM AUTHOR]

Published

2024

35. Amelioration of Doxorubicin-Induced Cognitive Impairment by Quercetin in a Rat Model of Breast Cancer

Author

Ramalingayya, Grandhi Venkata, John, Jeena, Gourishetti, Karthik, Nayak, Pawan Ganesh, Rao, C. Mallikarjuna, Kishore, Anoop, Alnasser, Sulaiman M., Hussain, Shalam M., and Krishnadas, Nandakumar

Published

2023

36. A novel epigenetic signature for overall survival prediction in patients with breast cancer

Author

Xuanwen Bao, Natasa Anastasov, Yanfang Wang, and Michael Rosemann

Subjects

Breast cancer, Mammary carcinoma, Epigenetics, Molecular marker, Response, Prognosis, Medicine

Abstract

Abstract Background Breast cancer is the most common malignancy in female patients worldwide. Because of its heterogeneity in terms of prognosis and therapeutic response, biomarkers with the potential to predict survival or assist in making treatment decisions in breast cancer patients are essential for an individualised therapy. Epigenetic alterations in the genome of the cancer cells, such as changes in DNA methylation pattern, could be a novel marker with an important role in the initiation and progression of breast cancer. Method DNA methylation and RNA-seq datasets from The Cancer Genome Atlas (TCGA) were analysed using the Least Absolute Shrinkage and Selection Operator (LASSO) Cox model. Applying gene ontology (GO) and single sample gene set enrichment analysis (ssGSEA) an epigenetic signature associated with the survival of breast cancer patients was constructed that yields the best discrimination between tumour and normal breast tissue. A predictive nomogram was built for the optimal strategy to distinguish between high- and low-risk cases. Results The combination of mRNA-expression and of DNA methylation datasets yielded a 13-gene epigenetic signature that identified subset of breast cancer patients with low overall survival. This high-risk group of tumor cases was marked by upregulation of known cancer-related pathways (e.g. mTOR signalling). Subgroup analysis indicated that this epigenetic signature could distinguish high and low-risk patients also in different molecular or histological tumour subtypes (by Her2-, EGFR- or ER expression or different tumour grades). Using Gene Expression Omnibus (GEO) the 13-gene signature was confirmed in four external breast cancer cohorts. Conclusion An epigenetic signature was discovered that effectively stratifies breast cancer patients into low and high-risk groups. Since its efficiency appears independent of other known classifiers (such as staging, histology, metastasis status, receptor status), it has a high potential to further improve likely individualised therapy in breast cancer.

Published

2019

37. Metformin potentiates the chemotherapeutic effects of doxorubicin on 2‐amino‐1‐methyl‐6‐phenylimidazo[4,5b] pyridine‐induced Mammary Carcinoma in rats.

Author

Salim, Elsayed, El‐Sisi, Alaa El‐Din, Sokar, Samia, EL‐Sayad, Magda, and Moussa, Ethar

Subjects

*METFORMIN, *RATS, *DOXORUBICIN, *CANCER chemotherapy, *CELL proliferation, *CARCINOMA, *DRINKING water

Abstract

This study was carried out to evaluate the antitumor activity of Metformin (Met) and its impending utility to potentiate the chemotherapeutic action of doxorubicin on 2‐amino‐1‐methyl‐6‐phenylimidazo[4,5b]pyridine (PhIP)‐induced rat mammary carcinogenesis. Female Sprague –Dawley (SD) rats were divided into seven groups (n = 15 each). Mammary carcinogenesis was induced by the administration of PhIP at a dose of 75 mg/kg by gavage. Met treatment was 2 mg/ml in drinking water for 26 weeks started after the last PhIP dose. Doxorubicin (Dox) treatment started after one month of the last PhIP dose with a dose of 4 mg/kg, i.v. once per week for 4 weeks. Compared to the PhIP group, the latency period of tumors in the PhIP+Dox, PhIP+Met, and PhIP+Dox+Met groups were significantly increased and tumors' incidences and multiplicities were significantly reduced. By immunohistochemistry, carcinomas from the combination treatment groups showed a significant decrease in the labeling indexes (LI%) of cellular proliferation and CD44 compared to the PhIP group while LI% for ERα was significantly decreased in all combination treatment groups compared to the PhIP‐administered group. Moreover, the quantitative mRNA expression of ERα was significantly decreased in mammary tumors from PhIP + Dox+Met combined group more than the PhIP + Dox group. However, mRNA expression of EGF was found significantly lower in all combination treatment groups compared to the PhIP group. These findings suggest that Metformin potentiate the antitumor efficacy of doxorubicin and had beneficial effects on PhIP‐induced mammary carcinogenesis through the prevention of cellular proliferation and mRNA expression of ERα and EGF. [ABSTRACT FROM AUTHOR]

Published

2021

38. Unilateral right mammary gland enlargement in a multiparous, pregnant 14-year-old American Quarter Horse mare.

Author

Castillo, Juan, Hilburger, Lindsay, Rosenberg, Lacey, Soon Hon Cheong, Duhamel, Gerald E., and Diel de Amorim, Mariana

Subjects

*MASTITIS, *MAMMARY glands, *MARES, *HORSES, *MEDICAL sciences

Abstract

The article focuses on comparing the proximal diffusion of modified abaxial sesamoid nerve block (MASB) with traditional low plantar nerve block (TLPB) in equine hind limbs. MASB exhibits enhanced diffusion compared to basisesamoid block (BSB) and lower diffusion than TLPB. Topics include injection techniques, diffusion patterns, and potential clinical implications.

Published

2023

39. Matrix Metalloproteinase-2 Expression as a Prognostic Marker in Breast Carcinomas

Author

B Jayashre, Priyathersini Nagarajan, and Thanka Johnson

Subjects

immunohistochemistry, mammary carcinoma, molecular subtyping, Medicine

Abstract

Introduction: Matrix Metalloproteinase-2 (MMP-2) is over expressed in a variety of malignant tumours and their expression and activity are often associated with tumour aggressiveness and a poor prognosis. It serves as a prognostic marker in breast carcinoma regardless of patient age, disease stage, malignancy grade, or hormone receptor status and modulation of MMP-2 expression and activation provides a new mechanism for breast cancer treatment. Aim: To evaluate the expression of MMP-2 in breast carcinoma tumour cells and peritumoural stroma and also to analyse the findings with the existing other prognostic markers of mammary carcinoma. Materials and Methods: The present study was a retrospective study conducted on paraffin blocks of 90 cases of invasive breast carcinoma specimens received in the Department of Pathology, Sri Raamachandra Institute of Higher Education and Research a tertiary care centre in Chennai, Tamil Nadu, India, from January 2012 to June 2017. Immunohistochemical staining for MMP-2, Oestrogen Receptor (ER), Progesterone Receptor (PR) and Human Epidermal Growth Factor Receptor 2 (HER2) was done. Statistical analysis was done on the data collected by using the software GNU-PSPP version 0.10.1. Pearson Chi-square test was used to determine significant clinicopathological differences between MMP-2 expression in positive and negative tumours. Differences were considered statistically significant when p-value was

Published

2021

40. Primary 4T1 tumor resection provides critical “window of opportunity” for immunotherapy

Author

Ghochikyan, Anahit, Davtyan, Arpine, Hovakimyan, Armine, Davtyan, Hayk, Poghosyan, Anna, Bagaev, Alexander, Ataullakhanov, Ravshan I, Nelson, Edward L, and Agadjanyan, Michael G

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Immunotherapy, Women's Health, Cancer, Breast Cancer, 2.1 Biological and endogenous factors, Animals, CD4-Positive T-Lymphocytes, CD8-Positive T-Lymphocytes, Mammary Neoplasms, Experimental, Mice, Mammary carcinoma, Animal model of cancer, Immunosuppression, Clonogenic tumor cells, Window of opportunity for immunotherapy, Clinical Sciences, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis

Abstract

It is believed that primary tumor resection modulates host-tumor immune interaction, but this has not been characterized in a stringent breast cancer tumor model. This report, using the 4T1 murine mammary tumor model, characterizes for the first time the dynamic longitudinal changes in immunosuppressive and effector components of the immune system after resection of an established orthotopic primary tumor with a defined natural history of developing lung metastases. More specifically, we analyzed changes of absolute numbers and frequencies of MDSC, regulatory T cells (Treg), as well as activated CD4 and CD8 positive T cells in spleens and, in some studies, lungs of 4T1 tumor-bearing mice and mice after primary tumor resection. Importantly, using mathematical analyses we established that primary resection of an orthotopic tumor had created a "window of opportunity" with decreased tumor-associated immune suppression that existed for approximately 10 days. Although tumor resection did slightly prolong survival, it did not affect the ultimate development of metastatic disease since animals with resected tumors or intact primary tumors eventually died by day 47 and 43, respectively. This window of opportunity likely occurs in humans providing a rationale and parameters for integration and testing of immunotherapeutic strategies in this critical "window of opportunity" to combat the development of metastatic disease.

Published

2014

41. Human breast microbiome correlates with prognostic features and immunological signatures in breast cancer.

Author

Tzeng, Alice, Sangwan, Naseer, Jia, Margaret, Liu, Chin-Chih, Keslar, Karen S., Downs-Kelly, Erinn, Fairchild, Robert L., Al-Hilli, Zahraa, Grobmyer, Stephen R., and Eng, Charis

Subjects

HUMAN microbiota, BREAST cancer, GUT microbiome, BREAST, RANK correlation (Statistics), GENES, CARCINOGENESIS

Abstract

Background: Currently, over half of breast cancer cases are unrelated to known risk factors, highlighting the importance of discovering other cancer-promoting factors. Since crosstalk between gut microbes and host immunity contributes to many diseases, we hypothesized that similar interactions could occur between the recently described breast microbiome and local immune responses to influence breast cancer pathogenesis. Methods: Using 16S rRNA gene sequencing, we characterized the microbiome of human breast tissue in a total of 221 patients with breast cancer, 18 individuals predisposed to breast cancer, and 69 controls. We performed bioinformatic analyses using a DADA2-based pipeline and applied linear models with White's t or Kruskal–Wallis H-tests with Benjamini–Hochberg multiple testing correction to identify taxonomic groups associated with prognostic clinicopathologic features. We then used network analysis based on Spearman coefficients to correlate specific bacterial taxa with immunological data from NanoString gene expression and 65-plex cytokine assays. Results: Multiple bacterial genera exhibited significant differences in relative abundance when stratifying by breast tissue type (tumor, tumor adjacent normal, high-risk, healthy control), cancer stage, grade, histologic subtype, receptor status, lymphovascular invasion, or node-positive status, even after adjusting for confounding variables. Microbiome–immune networks within the breast tended to be bacteria-centric, with sparse structure in tumors and more interconnected structure in benign tissues. Notably, Anaerococcus, Caulobacter, and Streptococcus, which were major bacterial hubs in benign tissue networks, were absent from cancer-associated tissue networks. In addition, Propionibacterium and Staphylococcus, which were depleted in tumors, showed negative associations with oncogenic immune features; Streptococcus and Propionibacterium also correlated positively with T-cell activation-related genes. Conclusions: This study, the largest to date comparing healthy versus cancer-associated breast microbiomes using fresh-frozen surgical specimens and immune correlates, provides insight into microbial profiles that correspond with prognostic clinicopathologic features in breast cancer. It additionally presents evidence for local microbial–immune interplay in breast cancer that merits further investigation and has preventative, diagnostic, and therapeutic potential. [ABSTRACT FROM AUTHOR]

Published

2021

42. Matrix Metalloproteinase-2 Expression as a Prognostic Marker in Breast Carcinomas.

Author

JAYASHREE, B., NAGARAJAN, PRIYATHERSINI, and JOHNSON, THANKA

Subjects

HORMONE receptor positive breast cancer, EPIDERMAL growth factor receptors, PROGESTERONE receptors, HIGHER education research, HORMONE receptors, CARCINOMA

Abstract

Introduction: Matrix Metalloproteinase-2 (MMP-2) is over expressed in a variety of malignant tumours and their expression and activity are often associated with tumour aggressiveness and a poor prognosis. It serves as a prognostic marker in breast carcinoma regardless of patient age, disease stage, malignancy grade, or hormone receptor status and modulation of MMP-2 expression and activation provides a new mechanism for breast cancer treatment. Aim: To evaluate the expression of MMP-2 in breast carcinoma tumour cells and peritumoural stroma and also to analyse the findings with the existing other prognostic markers of mammary carcinoma. Materials and Methods: The present study was a retrospective study conducted on paraffin blocks of 90 cases of invasive breast carcinoma specimens received in the Department of Pathology, Sri Raamachandra Institute of Higher Education and Research a tertiary care centre in Chennai, Tamil Nadu, India, from January 2012 to June 2017. Immunohistochemical staining for MMP-2, Oestrogen Receptor (ER), Progesterone Receptor (PR) and Human Epidermal Growth Factor Receptor 2 (HER2) was done. Statistical analysis was done on the data collected by using the software GNU-PSPP version 0.10.1. Pearson Chi-square test was used to determine significant clinicopathological differences between MMP-2 expression in positive and negative tumours. Differences were considered statistically significant when p-value was <0.05. Results: The study included 90 cases of histological proven invasive breast carcinoma. The study parameters include age, clinical staging, histopathological grade, lymphnode status, molecular subtype and MMP-2 expression in invasive breast carcinoma. Out of 90 cases, 62 cases were positive for MMP-2 and 18 cases were positive for peritumoural stroma, 30 cases were negative for MMP-2 in tumoural cells and 72 cases were negative surrounding the peritumoural stroma. Conclusion: Present study showed high MMP-2 immunohistochemical expression in breast carcinomas. There was a statistically significant association of increased MMP-2 expression with tumour stage. There was also a statistically significant association of MMP-2 in the tumour and stroma with High Grade Ductal Carcinoma In Situ (HGDCIS). There was an increased expression of MMP-2 in Luminal A subtype. Low expression was seen in the other molecular subtypes. In view of these findings and association with other studies in the literature, the present study demonstrates that the expression of MMP-2 in tumour and stromal cells could serve as a parameter of poor prognosis in breast cancer. [ABSTRACT FROM AUTHOR]

Published

2021

43. ErbB2 copy number gain is associated with adverse outcome in canine mammary carcinoma.

Author

Kosei SAKAI, CHAMBERS, James Ken, Kazuyuki UCHIDA, Takayuki NAKAGAWA, Ryohei NISHIMURA, Tomohiro YONEZAWA, and Shingo MAEDA

Subjects

PROGNOSIS, CARCINOMA, MAMMARY glands, COMPRESSED natural gas

Abstract

Copy number gain (CNG) and/or protein overexpression of ErbB2 have been observed in human breast cancer patients and are associated with poor prognosis. Similarly, ErbB2 overexpression has also been observed in canine mammary carcinoma; however, data on ErbB2 copy number is limited. The purposes of this study were to evaluate ErbB2 copy number in dogs with mammary carcinoma and to investigate associations of ErbB2 CNG with ErbB2 expression, histological and clinical characteristics, and survival. DNA samples were isolated from 59 formalinfixed paraffin-embedded canine mammary gland tissues (34 carcinoma, 14 adenoma, and 11 normal). Using a digital PCR assay, the ErbB2 copy number in these samples was determined as compared to a reference gene on canine chromosome 8. ErbB2 CNG was detected in 14/34 (41%) carcinomas and 2/14 (14%) adenomas. ErbB2 overexpression was observed in 3/34 (9%) carcinomas but not in adenomas. Neither ErbB2 CNG nor ErbB2 overexpression were detected in the normal controls. There was no significant association of the ErbB2 CNG with histological and clinical characteristics such as age, neutered status, histological grade, tumor size, lymph node involvement, distant metastasis, and clinical stage in the dogs with mammary carcinoma. The presence of ErbB2 CNG, but not ErbB2 overexpression, was significantly related to the shorter overall survival. These findings suggest that ErbB2 CNG is a prognostic factor in dogs with mammary carcinoma. [ABSTRACT FROM AUTHOR]

Published

2021

44. The Impact of miRNAs on the Efficacy of Tamoxifen in Breast Cancer Treatment: A Systematic Review.

Author

Kavishahi NN, Rezaee A, and Jalalian S

Subjects

Humans, Female, Gene Expression Regulation, Neoplastic drug effects, Tamoxifen therapeutic use, Breast Neoplasms drug therapy, Breast Neoplasms genetics, Breast Neoplasms pathology, MicroRNAs genetics, Antineoplastic Agents, Hormonal therapeutic use, Antineoplastic Agents, Hormonal pharmacology, Drug Resistance, Neoplasm genetics

Abstract

Seventy percent of breast cancer patients have an active estrogen receptor. Tamoxifen interferes with estrogen's ability to bind to cancer cells. The most challenging aspect of tamoxifen, however, is that breast cancer cells become resistant to its effects. Some studies have shown that alterations in miRNA expression contribute significantly to drug resistance in breast cancer. Therefore, the present systematic review aims to investigate miRNAs that significantly influence the response to tamoxifen treatment. The present study follows the PRISMA instructions. The Web of Science, PubMed, and Scopus databases were searched to retrieve English articles. The searches were conducted up to September 11, 2022. The search strategy included the terms "Tamoxifen", "Breast Neoplasm", and "MicroRNA". The inclusion criteria of this study are English, original, and experimental studies investigating miRNAs that are effective in the treatment efficacy of tamoxifen. A total of 565 articles were retrieved. After screening, 75 studies met our inclusion criteria. This systematic review study examined 105 miRNAs, of which 44 have a positive effect, and 47 miRNAs inhibit tamoxifen function. Fourteen miRNAs have a controversial effect, ie, some studies show positive and negative effects. The study of miRNAs affecting tamoxifen function in breast cancer patients may facilitate the identification of individuals at higher risk of disease recurrence. Conversely, it can potentially utilize appropriate interventions to defeat drug resistance effectively., Competing Interests: Disclosure The authors have no conflict of interest to declare., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

45. Detection of Epithelial Cell Adhesion Molecule in Feline Normal and Tumor Cell Lines and Tissues With Selected Commercial Anti-human EpCAM Antibodies

Author

Christa Y. Heyward, Lynn Dong, Hayk Shakhzadyan, Christopher Wan, and Tracy Stokol

Subjects

cat, cancer, immunohistochemistry, flow cytometry, circulating tumor cells, mammary carcinoma, Veterinary medicine, SF600-1100

Abstract

Epithelial cell adhesion molecule (EpCAM) is a transmembrane protein expressed at intercellular junctions in epithelial cells. As an epithelial biomarker, it used for immunologic-based capture of epithelial-derived circulating tumor cells (CTCs) in human patients with different carcinomas. EpCAM expression has not been described in normal or neoplastic epithelial tissues in cats. Our goal was to find a commercial antibody that recognizes surface EpCAM expression for CTC detection. We tested two anti-human EpCAM antibodies, designated for use with flow cytometry, for detection of surface EpCAM expression on feline cell lines derived from normal mammary and renal epithelia and mammary and oropharyngeal squamous cell carcinomas in cats. Only one of the antibodies, a goat polyclonal antibody, labeled normal and neoplastic feline mammary epithelial cells and oropharyngeal squamous cell carcinoma cells; no labeling was observed for normal feline kidney epithelial cells. At low dilution, this antibody immunohistochemically stained the intercellular junctions of normal pancreatic, intestinal and mammary epithelium, as well as neoplastic mammary epithelium in feline tissues; however, oral mucosa, skin, and an oropharyngeal squamous cell carcinoma showed no positive immunostaining. The antibody only weakly bound feline squamous cell carcinoma cell lines under static adhesion. Our results indicate that EpCAM is expressed in specific epithelia in cats but is variably expressed in feline mammary tumors and oropharyngeal squamous cell carcinoma. A higher avidity cross-reactive or feline-specific antibody will be required to further investigate EpCAM expression in normal and neoplastic feline tissue or for detecting CTCs in the blood of tumor-bearing cats.

Published

2021

46. Unfavorable Prognostic Effects of the Stem Cell Pluripotency Factor Sox2 in Feline Invasive Mammary Carcinomas

Author

Yohan Truchot, Elie Dagher, Jérôme Abadie, and Frédérique Nguyen

Subjects

androgen receptor, cat, mammary carcinoma, prognosis, regulatory T cells, SOX2, Veterinary medicine, SF600-1100

Abstract

Background: Sex-determining Region Y (SRY)-box transcription factor-2 (Sox2) belongs to the “Yamanaka's factors,” necessary and sufficient to convert somatic cells into pluripotent stem cells. In breast cancers, Sox2 expression has been associated with poor prognosis, and resistance to therapy. The aims of this study were to determine the frequency of Sox2 positivity in feline invasive mammary carcinomas (FMCs), its relationships with other clinical-pathologic variables, and with patient outcomes.Materials and Methods: This study relies on a previously described retrospective cohort of 180 FMCs, diagnosed in female cats treated by mastectomy alone, with 2-year follow-up. Sox2 (clone SP76), Estrogen Receptor alpha (ER), Progesterone Receptor (PR), Ki-67, Human Epidermal growth factor Receptor 2 (HER2), Androgen Receptor (AR), Bcl-2, Forkhead box protein A1 (FOXA1), basal markers and FoxP3-positive regulatory T cells (Tregs) were detected by automated immunohistochemistry. Sox2 expression was quantitated as an index (percentage of neoplastic cells demonstrating a positive nuclear signal). The FMCs were considered Sox2-positive at threshold >42%.Results: Sox2 was not expressed in the normal mammary gland or in mammary hyperplasia without atypia, but was occasionally detected in atypical hyperplasia. In FMCs, the mean Sox2 index was 38 ± 30%, and 79/180 FMCs (44%) were Sox2-positive. Sox2 expression was associated with older age at diagnosis, lymphovascular invasion, high Ki-67 proliferation indexes, low PR and FOXA1 expression, and increased numbers of tumor-associated Tregs, but was not significantly associated with the clinical stage, histological types, and histological grade. By multivariate survival analysis, Sox2 was associated with poor cancer-specific survival (Hazard Ratio = 1.48, 95% confidence interval 1.04–2.11, p = 0.0292), independently of the pathologic tumor size, pathologic nodal stage, distant metastasis, and AR expression. A rare subgroup of FMCs characterized by an AR+Sox2–phenotype (19/180 cases, 11%) was associated with very favorable outcomes.Conclusion: Sox2 expression was associated with poor cancer-specific survival of female cats with invasive mammary carcinomas, as previously reported in human breast cancer, but was more commonly expressed in cats than reported in breast cancers. Sox2 showed complementarity with AR in FMC prognostication.

Published

2021

47. Iron Supplementation Interferes With Immune Therapy of Murine Mammary Carcinoma by Inhibiting Anti-Tumor T Cell Function

Author

Piotr Tymoszuk, Manfred Nairz, Natascha Brigo, Verena Petzer, Simon Heeke, Brigitte Kircher, Natascha Hermann-Kleiter, Victoria Klepsch, Igor Theurl, Günter Weiss, and Christa Pfeifhofer-Obermair

Subjects

T cell, immunotherapy, cancer prognosis, iron, immune checkpoint, mammary carcinoma, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Iron is both, an essential compound for many metabolic processes, and iron deficiency can impact on the proliferation of cells including lymphocytes but also tumor cells. On the other hand, excess iron-catalyzed radical formation can induce cellular toxicity which has been previously demonstrated for T cells in hereditary iron overload. Despite these interconnections, little is known on the effects of clinically approved intravenous iron supplements for curing cancer-related anemia, on T cell differentiation, tumor proliferation, anti-tumor T cell responses and, of clinical importance, on efficacy of cancer immunotherapies. Herein, we analyzed the effects of intravenous iron supplementation on T cell function and on the effectiveness of anti-cancer chemotherapy with IL-2/doxorubicin or immunotherapy with checkpoint-inhibitor anti-PD-L1 in C57Bl/6N female mice with implanted E0771 mammary carcinomas. We found that iron application resulted to an increased availability of iron in the tumor microenvironment and stimulation of tumor growth. In parallel, iron application inhibited the activation, expansion and survival of cytotoxic CD8+ T cells and of CD4+ T helper cells type 1 and significantly reduced the efficacy of the investigated anti-cancer treatments. Our results indicate that iron administration has a tumor growth promoting effect and impairs anti-cancer responses of tumor infiltrating T lymphocytes along with a reduced efficacy of anti-cancer therapies. Iron supplementation in cancer patients, especially in those treated with immunotherapies in a curative setting, may be thus used cautiously and prospective studies have to clarify the impact of such intervention on the outcome of patients.

Published

2020

48. Comparing Human Breast Cancer with Canine Mammary Cancer

Author

Hadzijusufovic, Emir, Willmann, Michael, and Jensen-Jarolim, Erika, editor

Published

2017

49. Iron Supplementation Interferes With Immune Therapy of Murine Mammary Carcinoma by Inhibiting Anti-Tumor T Cell Function.

Author

Tymoszuk, Piotr, Nairz, Manfred, Brigo, Natascha, Petzer, Verena, Heeke, Simon, Kircher, Brigitte, Hermann-Kleiter, Natascha, Klepsch, Victoria, Theurl, Igor, Weiss, Günter, and Pfeifhofer-Obermair, Christa

Subjects

IRON supplements, T cells, CELL physiology, T helper cells, CYTOTOXIC T cells, T cell differentiation

Abstract

Iron is both, an essential compound for many metabolic processes, and iron deficiency can impact on the proliferation of cells including lymphocytes but also tumor cells. On the other hand, excess iron-catalyzed radical formation can induce cellular toxicity which has been previously demonstrated for T cells in hereditary iron overload. Despite these interconnections, little is known on the effects of clinically approved intravenous iron supplements for curing cancer-related anemia, on T cell differentiation, tumor proliferation, anti-tumor T cell responses and, of clinical importance, on efficacy of cancer immunotherapies. Herein, we analyzed the effects of intravenous iron supplementation on T cell function and on the effectiveness of anti-cancer chemotherapy with IL-2/doxorubicin or immunotherapy with checkpoint-inhibitor anti-PD-L1 in C57Bl/6N female mice with implanted E0771 mammary carcinomas. We found that iron application resulted to an increased availability of iron in the tumor microenvironment and stimulation of tumor growth. In parallel, iron application inhibited the activation, expansion and survival of cytotoxic CD8+ T cells and of CD4+ T helper cells type 1 and significantly reduced the efficacy of the investigated anti-cancer treatments. Our results indicate that iron administration has a tumor growth promoting effect and impairs anti-cancer responses of tumor infiltrating T lymphocytes along with a reduced efficacy of anti-cancer therapies. Iron supplementation in cancer patients, especially in those treated with immunotherapies in a curative setting, may be thus used cautiously and prospective studies have to clarify the impact of such intervention on the outcome of patients. [ABSTRACT FROM AUTHOR]

Published

2020

50. A prospective randomized trial of desmopressin in canine mammary carcinoma.

Author

Sorenmo, Karin, Durham, Amy C., Evans, Brolin, Scavello, Heather, and Stefanovski, Darko

Subjects

*PROGNOSIS, *DESMOPRESSIN, *BREAST cancer, *VASOPRESSIN, *CARCINOMA

Abstract

Metastatic disease represents a serious and often fatal development in patients with solid tumours, including women with breast cancer and dogs with mammary tumours. Therefore, preventing and treating metastatic disease has remained a priority in cancer research. Desmopressin, a synthetic derivative of vasopressin, traditionally used to treat patients with bleeding disorders, has been proposed as a potential anti‐metastatic agent due to its effect on haemostasis as well as multiple other anti‐proliferative and anti‐angiogenic mechanisms. The purpose of this study was to retest desmopressin in dogs with mammary carcinomas. A prospective randomized study was performed. Twenty‐four dogs with mammary carcinomas were enrolled; 12 dogs received perioperative desmopressin and 12 received placebo. All dogs underwent standard pre‐surgical staging followed by complete resection of all tumours. Intact dogs were spayed. All tumours were graded and classified according to the published guidelines. Follow‐up was performed every 4 months the first year and every 6 months thereafter. Necropsies were requested on all dogs. There was no difference in time to primary metastasis or survival between desmopressin treated dogs and the placebo arm (P =.43 and.73, respectively). The distribution of negative prognostic factors, including tumour grade, stage, and high vs low bioscore (refined flexible bioscoring) category between arms was not statistically different, even though more dogs in the placebo arm had grade 3 tumours and high bioscores. Based on the results of this study, perioperative desmopressin does not prevent metastasis in dogs with mammary carcinomas. [ABSTRACT FROM AUTHOR]

Published

2020