Your search keyword '"Ctvt"' showing total 7 results

1. Immunohistochemical, lectin histochemical and ultrastructural studies of canine transmissible venereal tumor in Brazil.

Author

Mascarenhas, Mariana B., Peixoto, Paulo V., Ramadinha, Regina R., Armien, Anibal G., Costa, Samay Z., Miranda, Ileana C., Nogueira, Vivian A., and França, Ticiana N.

Abstract

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Published

2017

2. Could dysregulation of RASSF1 expression be a mechanism of tumorigenesis in CTVT?

Author

Haline B. Fêo, Luis Mauricio M. Flórez, Ricardo S. Yamatogi, Anderson P. Duzanski, João P. Araújo Junior, Rogerio A. Oliveira, and Noeme S. Rocha

Subjects

Dysregulation, tumorigenesis, General Veterinary, canine transmissible venereal tumor, CTVT, RASSF1

Abstract

Canine transmissible venereal tumor (CTVT) is the oldest known somatic cell lineage. It is a transmissible cancer that propagates naturally in dogs and reportedly contains gene mutations. RASSF1 participates in DNA damage repair, and its downregulation, results in tumor progression. Hence, RASSF1 is a tumor suppressor gene. Its expression was quantified in tumors from seventeen animals and three cell cultures derived from tumors. In general, RASSF1 was underexpressed in 65%, and absent in 35% of tumor samples. Cells from tumor tissue cultures showed decreased expression of RASSF1 in 67% and elevated expression in 33% of samples tested. The tumor tissues showed significantly lower levels of RASSF1 expression compared to cultured cells. Previously we reported that both the tumor microenvironment and the host immune system appear to influence the tumorigenesis and stage of CTVT. This is the first article to demonstrate the expression of RASSF1 in CTVT. Decreased RASSF1 possibly helps tumor progression.

Published

2022

3. In vitro Effect of Recombinant Feline Interferon-Ω (rFeIFN-Ω) on the Primary CanineTransmissible Venereal Tumor Culture

Author

Somporn Techangamsuwan, Chanokchon Setthawongsin, Anudep Rungsipipat, and Sirikachorn Tangkawattana

Subjects

in vitro study, 040301 veterinary sciences, medicine.medical_treatment, CTVT, Biology, Canine transmissible venereal tumor, 0403 veterinary science, 03 medical and health sciences, Interferon, In vivo, medicine, Viability assay, 030304 developmental biology, Original Research, 0303 health sciences, primary culture, lcsh:Veterinary medicine, General Veterinary, Tumor-infiltrating lymphocytes, 04 agricultural and veterinary sciences, Immunotherapy, interferon, medicine.disease, In vitro, rFeIFN-Ω, Apoptosis, Cancer research, lcsh:SF600-1100, Veterinary Science, medicine.drug

Abstract

Background: Interferons (IFNs), signaling proteins produced by host cells, are secreted in response to pathogen activity as well as to tumor cells, and display antiviral, antiproliferative, and immunomodulatory effects. Recombinant feline interferon omega (rFeIFN-ω) has in vitro growth inhibition activities on various canine and feline tumor cell lines. Canine transmissible venereal tumor (CTVT) is used as an animal model for immunotherapy due to its specific growth phase. Previous studies have usually focused on the interaction between tumor infiltrating lymphocytes (TILs) and CTVT cells. However, the specific effects of rFeIFN-ω on CTVT cells remains poorly defined. Aims: The aims of this study, therefore, were to evaluate the in vitro effect of rFeIFN-ω on primary CTVT cells and to study the mRNA expression of apoptotic genes and drug resistance genes. Materials and Methods: Purified CTVT cells were treated with various concentrations of rFeIFN-ω and the viability of the cultured cells was ascertained at 24, 48, and 72 h post treatment (hpt) and a dose-response curve plotted. The mRNA expression of apoptotic (BAX and BCL-2) and drug resistance (ABCB1 and ABCG2) genes was performed by reverse transcription quantitative real-time PCR at 72 hpt. Results: rFeIFN-ω displayed an effect against CTVT cell viability, which decreasing viability in a dose-dependent manner within 72 hpt. The relative mRNA expression of BCL-2 was upregulated only at a rFeIFN-ω concentration of 104 IU/100 μl. However, higher concentrations of rFeIFN-ω gave a higher level of relative mRNA expression of ABCB1 transporter gene. Conclusion: This study provided the information of in vitro effect of rFeIFN-ω on CTVT cell viability in a dose dependent manner, as well as, the alteration of BCL-2 and ABCB1 gene expression after treatment. These results encourage future in vivo studies to evaluate the potential efficacy of this treatment in CTVT cases.

Published

2019

4. Cell-based polymerase chain reaction for canine transmissible venereal tumor (CTVT) diagnosis

Author

Anudep Rungsipipat, Sirikachorn Tangkawattana, Chanokchon Setthawongsin, and Somporn Techangamsuwan

Subjects

0301 basic medicine, Nasal cavity, Male, Pathology, medicine.medical_specialty, 040301 veterinary sciences, diagnosis, Veterinary pathology, Genes, myc, LINE, CTVT, Canine transmissible venereal tumor, Polymerase Chain Reaction, law.invention, 0403 veterinary science, 03 medical and health sciences, Dogs, law, Biopsy, medicine, Neoplasm, Animals, Dog Diseases, Polymerase chain reaction, Venereal Tumors, Veterinary, Gene Rearrangement, General Veterinary, medicine.diagnostic_test, Full Paper, business.industry, 04 agricultural and veterinary sciences, Gene rearrangement, DNA, Neoplasm, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Fine-needle aspiration, PCR, Long Interspersed Nucleotide Elements, FNA, Female, business

Abstract

Canine transmissible venereal tumor (CTVT) is the only naturally contagious tumor that is transmitted during coitus or social behaviors. Based on the tumor's location, the diagnosis of genital TVT (GTVT) is comparably easier than those in the extragenital area (ETVT) that are more easily incorrectly diagnosed. Fortunately, CTVT cells contain a specific long interspersed nuclear elements (LINE), inserted upstream of the myc gene, allowing a diagnostic polymerase chain reaction (PCR) based detection assay. The objectives of this study were aimed to improve the diagnostic accuracy by applying the diagnostic LINE1-c-myc PCR assay and fine needle aspiration (FNA) collection in direct comparison with standard cytological and histopathological analyses. Seventy-four dogs, comprised of 41 and 31 dogs with tumor masses at their external genitalia and extragenital areas (e.g. skin and nasal cavity), respectively, were included in this study. The signalment of these 65 dogs and clinical history of 20 client-owned dogs were collected. Samples were taken by biopsy for both histopathological examination and FNA for cytological examination and diagnostic PCR. The PCR products from 10 apparently CTVT samples were purified and sequenced. Sixty-one CTVT cases were diagnosed by cytological and histological analyses, but 65 were positive by the PCR assay. Overall, the PCR assay improved the accuracy of diagnostic CTVT results, especially for the more difficult ETVT tumors. Moreover, this PCR-based approach can facilitate the decision as to discontinue chemotherapy by discrimination between residual tumor cell masses and fibrotic tissue.

Published

2016

5. Immunohistochemical, lectin histochemical and ultrastructural studies of canine transmissible venereal tumor in Brazil

Author

Paulo Vargas Peixoto, Regina Ruckert Ramadinha, Vivian de Assunção Nogueira, Ileana C. Miranda, Mariana Bezerra Mascarenhas, Ticiana N. França, Aníbal G. Armién, and Samay Zillmann Rocha Costa

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, microscopia eletrônica, cão, 040301 veterinary sciences, medicine.drug_class, CTVT, Biology, Canine transmissible venereal tumor, Monoclonal antibody, 0403 veterinary science, 03 medical and health sciences, lectin histochemistry, Antigen, imuno-histoquímica, ultrastructural, medicine, Tumor venéreo transmissível canino (TVTC), patologia, lectino-histoquímica, lcsh:Veterinary medicine, General Veterinary, Lectin, 04 agricultural and veterinary sciences, medicine.disease, 030104 developmental biology, Polyclonal antibodies, Monoclonal, immunohistochemistry, dog, biology.protein, lcsh:SF600-1100, Immunohistochemistry, pathology, Antibody

Abstract

Canine transmissible venereal tumor (CTVT) is a naturally occurring contagious round-cell neoplasia, with poorly understood origin and transmission. This study aims to further investigate the tumor nature through immunohistochemistry, lectin histochemistry and transmission electron microscopy (TEM) analysis, and to provide support for diagnostic and differential diagnoses of CTVT. Immunohistochemistry was performed in 10 genital and six exclusively extragenital tumors, which were previously diagnosed by citology and histopathology. CTVT samples were incubated with biotinylated antibodies to specific membrane and cytoplasmic antigens (anti-lysozyme, anti-macrophage, anti-vimentin, anti-CD18, monoclonal anti-CD117, monoclonal anti-CD3, polyclonal anti-CD117, polyclonal CD3 and anti-CD79a), followed by the avidin-biotin-peroxidase complex technique. The lectins Con A, DBA, SBA, PNA, UEA-1, WGA, sWGA, GSL, JSA, PSA, PHA-L, PHA-E and RCA were additionally tested in four genital CTVTs and TEM was performed in eight genital tumors. The anti-vimentin antibody revealed strong immunoreactivity to neoplastic cells in all the assessed samples (16/16). The polyclonal anti-CD3 antibodies showed moderate to strong immunoreactivity in fourteen (14/16) and the polyclonal anti-CD117 in fifteen cases (15/16). There was no immunoreactivity to anti-lysozyme, anti-macrophage, anti-CD18, monoclonal anti-CD117, monoclonal anti-CD3 and anti-CD79a antibodies. At lectin histochemistry, it was observed strong staining of tumor cells to Con-A, PHA-L and RCA. There was no histopathological and immunoreactivity differences between genital and extragenital CTVTs. These findings do not support the hypothesis of histiocytic origin of CTVT. In contrast, the lectin histochemical results were similar to cells from lymphoid/myeloid origin. RESUMO: O Tumor Venéreo Transmissível Canino (CTVT) é uma neoplasia de células células redondas, contagiosa, com origem e transmissão ainda mal compreendidas. Com a finalidade de aprofundar a investigação sobre a natureza (origem) do TVTC, bem como fornecer subsídios para o estabelecimento do diagnóstico e diagnóstico diferencial, realizaram-se avaliações imuno-histoquímica, lectino-histoquímica e ultraestrutural de TVTC(s). A avaliação imuno-histoquímica foi feita em 10 TVTCs genitais e em 6 exclusivamente extragenitais previamente diagnosticados através de citologia e da histopatologia. Os TVTCs foram testados para reagentes específicos de antígenos de membrana e citoplasmáticos (anti-lisozima, anti-macrófago, anti-vimentina, anti-CD18, anti-CD3, anti-CD79, anti-CD117) com utilização da técnica complexo avidina-biotina-peroxidase. Adicionalmente, foram utilizadas as lectinas Con A, DBA, SBA, PNA, UEA-1, WGA, sWGA, GSL, SJA, PSA, PHA-L, PHA-E e RCA em quatro TVTCs genitais. Microscopia eletrônica foi realizada em oito TVTC genitais. Em 100% dos tumores testados (16/16) com anticorpo anti-vimentina (mono e policlonal) houve forte imuno-reatividade. Não houve reatividade para os anticorpos anti-lisozima, anti-macrófago, anti-CD18, anti-CD3, anti-CD79a e anti-CD117 quando empregamos anticorpos monoclonais, entretanto, com a utilização de anticorpos policlonais verificou-se marcação dos tumores com os anticorpos anti-CD3 e anti-CD117. Na avaliação lectino-histoquímica foi verificada forte marcação das células tumorais com Con-A, PHA-L e RCA. Não houve diferença histopatológica e de imuno-reatividade entre os TVTCs genitais e extragenitais. Estes achados não corroboram com a hipótese da origem histiocítica do CTVT (ausência de reatividade dos anticorpos anti-lisozima, anti-macrófago e anti-CD18), entretanto, os resultados da avaliação lectino-histoquímica foram em parte similares aos obtidos quando células de origem linfóide/mielóide (ConA, PHA-L e RCA) foram analisadas (Gimeno et al. 1995).

Published

2017

6. Immunohistochemical, lectin histochemical and ultrastructural studies of canine transmissible venereal tumor in Brazil

Author

Mariana B. Mascarenhas, Paulo V. Peixoto, Regina R. Ramadinha, Anibal G. Armien, Samay Z. Costa, Ileana C. Miranda, Vivian A. Nogueira, and Ticiana N. França

Subjects

Canine transmissible venereal tumor, CTVT, immunohistochemistry, lectin histochemistry, ultrastructural, dog, pathology, Veterinary medicine, SF600-1100

Abstract

ABSTRACT: Canine transmissible venereal tumor (CTVT) is a naturally occurring contagious round-cell neoplasia, with poorly understood origin and transmission. This study aims to further investigate the tumor nature through immunohistochemistry, lectin histochemistry and transmission electron microscopy (TEM) analysis, and to provide support for diagnostic and differential diagnoses of CTVT. Immunohistochemistry was performed in 10 genital and six exclusively extragenital tumors, which were previously diagnosed by citology and histopathology. CTVT samples were incubated with biotinylated antibodies to specific membrane and cytoplasmic antigens (anti-lysozyme, anti-macrophage, anti-vimentin, anti-CD18, monoclonal anti-CD117, monoclonal anti-CD3, polyclonal anti-CD117, polyclonal CD3 and anti-CD79a), followed by the avidin-biotin-peroxidase complex technique. The lectins Con A, DBA, SBA, PNA, UEA-1, WGA, sWGA, GSL, JSA, PSA, PHA-L, PHA-E and RCA were additionally tested in four genital CTVTs and TEM was performed in eight genital tumors. The anti-vimentin antibody revealed strong immunoreactivity to neoplastic cells in all the assessed samples (16/16). The polyclonal anti-CD3 antibodies showed moderate to strong immunoreactivity in fourteen (14/16) and the polyclonal anti-CD117 in fifteen cases (15/16). There was no immunoreactivity to anti-lysozyme, anti-macrophage, anti-CD18, monoclonal anti-CD117, monoclonal anti-CD3 and anti-CD79a antibodies. At lectin histochemistry, it was observed strong staining of tumor cells to Con-A, PHA-L and RCA. There was no histopathological and immunoreactivity differences between genital and extragenital CTVTs. These findings do not support the hypothesis of histiocytic origin of CTVT. In contrast, the lectin histochemical results were similar to cells from lymphoid/myeloid origin.

7. Overexpression of chemokine ligand 7 is associated with the progression of canine transmissible venereal tumor

Author

Rea-Min Chu, Yu-Shan Wang, Chen-Si Lin, Albert Taiching Liao, Chung-Hsi Chou, and Hsin-Chien Chiang

Subjects

TGF-β, Male, Chemokine, DNA, Complementary, CTVT, Canine transmissible venereal tumor, Dogs, medicine, Animals, CXC chemokine receptors, Dog Diseases, RNA, Messenger, Interleukin 6, Cells, Cultured, Venereal Tumors, Veterinary, IL-6, lcsh:Veterinary medicine, CXCR2, General Veterinary, biology, Tumor-infiltrating lymphocytes, Interleukin-6, Interleukin, General Medicine, medicine.disease, veterinary(all), Gene Expression Regulation, Neoplastic, CXCL7, Immunology, biology.protein, Cancer research, lcsh:SF600-1100, Chemokines, CXC, Transforming growth factor, Research Article

Abstract

Background Chemokines play multiple roles in the development and progression in a variety of tumors. Chemokine (C-X-C motif) ligand 7 (CXCL7) has been found associated with pro-inflammatory responses, but its role in cancer growth remains unclear. Our previous study showed that R phase tumor infiltrating lymphocytes (TILs) produced large amounts of interleukin (IL)-6 which antagonized transforming growth factor (TGF)-β derived from CTVT to diminish the immune-suppressive microenvironment. Now we intend to determine the expression pattern of CXCL7 and the role of IL-6/TGF-β in CXCL7 induction during spontaneous progressive (P) and regressive (R) phases in canine transmissible venereal tumor (CTVT). Results We have demonstrated that CXCL7 expressed at high level in P phase and down-regulated in R phase by western blot and real-time PCR. This suggested that CXCL7 expression was negatively correlated with the tumor growth. Co-culturing TILs with CTVT cells was found to reduce CXCL7 expression, while adding IL-6 blocking antibody reversed it. Moreover, in P phase CTVT, while IL-1β and TGF-β had no obvious effect on CXCL7 expression, IL-6 was found significantly to reduce CXCL7 expression in a dose-dependent manner. The mRNA expression results of CXCL7 receptor, CXCR2, further confirmed the effects of IL-6 concentration on the CXCL7 expression. Conclusion CXCL7 overexpression might be associated with the progressive growth of CTVT. The results shown here also suggest the role of CXCL7 in cancer development and the potential as the anti-cancer therapeutic target.

Published

2012