Your search keyword '"sarcomatoid type"' showing total 7 results

1. Advanced Minimally Invasive Approach with Medical Thoracoscopy for Mesothelioma: What Are the Roles in Diagnosis?

Author

Ishii, Satoru, Nakamura, Hiroyuki, Series Editor, Aoshiba, Kazutetsu, Series Editor, Nakano, Takashi, editor, and Kijima, Takashi, editor

Published

2021

2. Possible reversibility between epithelioid and sarcomatoid types of mesothelioma is independent of ERC/mesothelin expression

Author

Masataka Kojima, Kazunori Kajino, Shuji Momose, Nadila Wali, May Thinzar Hlaing, Bo Han, Liang Yue, Masaaki Abe, Tomoaki Fujii, Katsuhisa Ikeda, and Okio Hino

Subjects

Mesothelioma, ERC/mesothelin, Epithelioid type, Sarcomatoid type, Histological reversibility, Diseases of the respiratory system, RC705-779

Abstract

Abstract Background Mesothelioma is histologically divided into three subgroups: epithelioid, sarcomatoid, and biphasic types. The epithelioid or sarcomatoid type is morphologically defined by polygonal or spindle-like forms of cells, respectively. The biphasic type consists of both components. It is not yet understood how histological differentiation of mesothelioma is regulated. ERC/mesothelin is expressed in most cases of the epithelioid type, but not in the sarcomatoid type of mesothelioma. Consequently, its expression is well correlated to the histological subtype. We hypothesized that ERC/mesothelin expression influences the histological differentiation of mesothelioma, and tested this hypothesis. Methods We performed studies using the overexpression or knockdown of ERC/mesothelin in mesothelioma cells to examine its effect on cellular morphology, growth kinetics, or migration/invasion activity, in vitro. We then transplanted ERC/mesothelin-overexpressing and control cells into the intraperitoneal space of mice. We examined the effect of ERC/mesothelin overexpression on mouse survival and tumor phenotype. Results In vitro cell culture manipulations of ERC/mesothelin expression did not affect cellular morphology or proliferation, although its overexpression enhanced cellular adhesion and the migration/invasion activity of mesothelioma cells. The survival rate of mice following intraperitoneal transplantation of ERC/mesothelin-overexpressing mesothelioma cells was significantly lower than that of mice with control cells. The histological evaluation of the tumors, however, did not show any morphological difference between two groups, and our hypothesis was not validated. Unexpectedly, both groups (ERC/mesothelin-overexpressing and control) of mesothelioma cells that were morphologically monophasic and spindle-like in vitro differentiated into a biphasic type consisting of polygonal and spindle-like components in the transplanted tumor, irrespective of ERC/mesothelin expression. Conclusions These results suggested that the histological transition of mesothelioma between epithelioid and sarcomatoid types may be reversible and regulated not by ERC/mesothelin, but by other unknown mechanisms.

Published

2020

3. Possible reversibility between epithelioid and sarcomatoid types of mesothelioma is independent of ERC/mesothelin expression.

Author

Kojima, Masataka, Kajino, Kazunori, Momose, Shuji, Wali, Nadila, Hlaing, May Thinzar, Han, Bo, Yue, Liang, Abe, Masaaki, Fujii, Tomoaki, Ikeda, Katsuhisa, and Hino, Okio

Subjects

MESOTHELIOMA, CELL proliferation, CELL culture, PROTEIN metabolism, CELL differentiation, PROTEINS, ANIMAL experimentation, MACROPHAGES, CELLULAR signal transduction, GLYCOPROTEINS, GENES, CELL lines, SARCOMA, PHENOTYPES, MICE

Abstract

Background: Mesothelioma is histologically divided into three subgroups: epithelioid, sarcomatoid, and biphasic types. The epithelioid or sarcomatoid type is morphologically defined by polygonal or spindle-like forms of cells, respectively. The biphasic type consists of both components. It is not yet understood how histological differentiation of mesothelioma is regulated. ERC/mesothelin is expressed in most cases of the epithelioid type, but not in the sarcomatoid type of mesothelioma. Consequently, its expression is well correlated to the histological subtype. We hypothesized that ERC/mesothelin expression influences the histological differentiation of mesothelioma, and tested this hypothesis.Methods: We performed studies using the overexpression or knockdown of ERC/mesothelin in mesothelioma cells to examine its effect on cellular morphology, growth kinetics, or migration/invasion activity, in vitro. We then transplanted ERC/mesothelin-overexpressing and control cells into the intraperitoneal space of mice. We examined the effect of ERC/mesothelin overexpression on mouse survival and tumor phenotype.Results: In vitro cell culture manipulations of ERC/mesothelin expression did not affect cellular morphology or proliferation, although its overexpression enhanced cellular adhesion and the migration/invasion activity of mesothelioma cells. The survival rate of mice following intraperitoneal transplantation of ERC/mesothelin-overexpressing mesothelioma cells was significantly lower than that of mice with control cells. The histological evaluation of the tumors, however, did not show any morphological difference between two groups, and our hypothesis was not validated. Unexpectedly, both groups (ERC/mesothelin-overexpressing and control) of mesothelioma cells that were morphologically monophasic and spindle-like in vitro differentiated into a biphasic type consisting of polygonal and spindle-like components in the transplanted tumor, irrespective of ERC/mesothelin expression.Conclusions: These results suggested that the histological transition of mesothelioma between epithelioid and sarcomatoid types may be reversible and regulated not by ERC/mesothelin, but by other unknown mechanisms. [ABSTRACT FROM AUTHOR]

Published

2020

4. Primary malignant pericardial sarcomatoid mesothelioma: An autopsy report.

Author

Muta, Hiroko, Sugita, Yasuo, Ohshima, Koichi, and Otsubo, Hitoshi

Subjects

*HEART failure patients, *OUTPATIENT medical care, *PERICARDIUM disease diagnosis, *IMMUNOSTAINING, *PATHOLOGICAL anatomy

Abstract

Primary malignant pericardial sarcomatoid mesothelioma (PMPSM) is an extremely rare tumor with poor prognosis. We present an autopsy case in an 80-year-old man admitted for heart failure after one month of treatment at an outpatient clinic. He died three months after symptom onset. A complete autopsy revealed localization of the tumor to the pericardium without other lesions. Histologically, mainly spindle-shaped atypical cells with hyperchromatic nuclei and nucleoli were observed. Immunohistochemical markers for mesothelioma were positive for calretinin, cytokeratin AE1/AE3, and cytokeratin CAM5.2. Thus, we diagnosed primary sarcomatoid malignant mesothelioma of the pericardium. To our knowledge, only four PMPSM cases have been reported in the English literature in the past 30 years. Although PMPSM is rare, clinicians and pathologists should recognize it as a possible diagnosis of pericardial tumors. It is necessary to accumulate clinical and pathological diagnostic findings to establish early detection methods for this extremely rare disease. [ABSTRACT FROM AUTHOR]

Published

2017

5. Possible reversibility between epithelioid and sarcomatoid types of mesothelioma is independent of ERC/mesothelin expression

Author

Nadila Wali, Tomoaki Fujii, May Thinzar Hlaing, Shuji Momose, Liang Yue, Masataka Kojima, Kazunori Kajino, Katsuhisa Ikeda, Bo Han, Masaaki Abe, and Okio Hino

Subjects

0301 basic medicine, Mesothelioma, endocrine system diseases, Mice, Nude, Biology, GPI-Linked Proteins, 03 medical and health sciences, ERC/mesothelin, 0302 clinical medicine, Epithelioid type, Cell Line, Tumor, Sarcomatoid type, medicine, Animals, Humans, Mesothelin, Cell adhesion, Histological reversibility, Survival rate, lcsh:RC705-779, Oncogene Proteins, Gene knockdown, Mice, Inbred BALB C, Transition (genetics), Research, Epithelioid Cells, Cell Differentiation, Sarcoma, lcsh:Diseases of the respiratory system, medicine.disease, In vitro, Transplantation, Gene Expression Regulation, Neoplastic, 030104 developmental biology, Phenotype, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Female, Signal Transduction

Abstract

Background Mesothelioma is histologically divided into three subgroups: epithelioid, sarcomatoid, and biphasic types. The epithelioid or sarcomatoid type is morphologically defined by polygonal or spindle-like forms of cells, respectively. The biphasic type consists of both components. It is not yet understood how histological differentiation of mesothelioma is regulated. ERC/mesothelin is expressed in most cases of the epithelioid type, but not in the sarcomatoid type of mesothelioma. Consequently, its expression is well correlated to the histological subtype. We hypothesized that ERC/mesothelin expression influences the histological differentiation of mesothelioma, and tested this hypothesis. Methods We performed studies using the overexpression or knockdown of ERC/mesothelin in mesothelioma cells to examine its effect on cellular morphology, growth kinetics, or migration/invasion activity, in vitro. We then transplanted ERC/mesothelin-overexpressing and control cells into the intraperitoneal space of mice. We examined the effect of ERC/mesothelin overexpression on mouse survival and tumor phenotype. Results In vitro cell culture manipulations of ERC/mesothelin expression did not affect cellular morphology or proliferation, although its overexpression enhanced cellular adhesion and the migration/invasion activity of mesothelioma cells. The survival rate of mice following intraperitoneal transplantation of ERC/mesothelin-overexpressing mesothelioma cells was significantly lower than that of mice with control cells. The histological evaluation of the tumors, however, did not show any morphological difference between two groups, and our hypothesis was not validated. Unexpectedly, both groups (ERC/mesothelin-overexpressing and control) of mesothelioma cells that were morphologically monophasic and spindle-like in vitro differentiated into a biphasic type consisting of polygonal and spindle-like components in the transplanted tumor, irrespective of ERC/mesothelin expression. Conclusions These results suggested that the histological transition of mesothelioma between epithelioid and sarcomatoid types may be reversible and regulated not by ERC/mesothelin, but by other unknown mechanisms.

Published

2020

6. The recurrence of malignant pleural mesothelioma 14 years after extrapleural pneumonectomy: Possible histological transformation.

Author

Kinoshita, Tomonari, Ishii, Genichiro, Matsumura, Yuki, Shiozawa, Toshihiro, Aokage, Keiju, Hishida, Tomoyuki, Yoshida, Junji, and Nagai, Kanji

Subjects

*MESOTHELIOMA, *PNEUMONECTOMY, *PLEURAL tumors, *CANCER relapse, *HISTOLOGY, *SARCOMA

Abstract

A 56-year-old man underwent extrapleural pneumonectomy for malignant pleural mesothelioma (MPM). The histological diagnosis was epithelioid mesothelioma with T2N0M0, and no sarcomatoid component was observed. Subsequently, 14 years after complete resection, screening computed tomography detected a rapidly growing right thoracic mass, which was diagnosed as a recurrence of MPM on resection. However, it was composed of both epithelioid (50%) and sarcomatoid (50%) components, suggesting possible histological transformation. Although there have been some previous reports on the recurrence of MPM, to the best of our knowledge, this is the first clinical case which indicated that histological transformation of MPM might occur. [ABSTRACT FROM AUTHOR]

Published

2012

7. A Case of Sarcomatoid Peritoneal Mesothelioma with Death due to Rapid Aggravation of Ascites

Subjects

ascites, sarcomatoid type, 腹膜原発悪性中皮腫, peritoneal mesothelioma, hyaluronic acid, 肉腫型, asbestos, アスベスト, ヒアルロン酸

Abstract

A 70-year-old man with a history of doing wiring work for 30 years was admitted to our hospital because of lower abdominal pain and ascites. Four months before admission he underwent cholecystectomy due to cholelithiasis and cholecystitis.At that time there were no macroscopic abnormal findings in the peritoneum, surface of the gall bladder,liver,stomach or intestine.We suspected peritonitis carcinomatosa,but ascetic fluid was light yellow and clear, and cytology showed no malignant cells. Computed tomography (CT)showed no malignant findings in visceral organs including the liver, pancreas, spleen, kidney and lung, but prominent ascites and thickening of the peritoneum and omentum were observed.After admission the ascites increased significantly and pleural effusion appeared. The patient died due to respiratory insufficiency two weeks from the onset of disease. Autopsy findings revealed sarcomatoid mesothelioma of the peritoneum, omentum and mesentery.Asbestos bodies were found in the lung,and the concentration of hyaluronic acid in ascites was very high. In conclusion, in cases with rapidly progressive and refractory ascites, asbestos-induced mesothelioma should be included in the differential diagnosis., Article, 信州医学雑誌. 58(2): 69-74 (2010)

Published

2010