Journal
ONCOLOGY RESEARCH
Volume 16, Issue 5, Pages 235-243Publisher
COGNIZANT COMMUNICATION CORP
DOI: 10.3727/000000006783981062
Keywords
MYO18B; orthotopic implantation; malignant mesothelioma; pleural effusion; vascular endothelial growth factor (VEGF)
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Malignant pleural mesothelioma (MPM) is closely related to exposure to asbestos, and a rapid increase in the number of MPM patients is therefore estimated to occur from 2010 to 2040 in Japan. Because MPM is refractory to conventional chemotherapy and radiotherapy, the prognosis of MPM patients is extremely poor. MYO18B, a novel member of the myosin family, is a tumor suppressor gene isolated from a homozygously deleted region at 22q12.1 in a lung cancer cell line. The inactivation of the MYO18B gene plays an important role in several malignant diseases. However, the role of MY018B in the progression of MPM is still unknown. Six different human MTM cell lines were used in this study. Western blot revealed that none of the cell lines expressed a detectable level of MY018B protein. One of the MPM cell lines, EHMES-10, was transfected with the MY018B gene. We found that a restored expression of the MY018B protein in EHMES-10 cells resulted in the inhibition of their anchorage-independent growth and motility in vitro. In addition, it also inhibited their ectopic (subcutaneous space) and orthotopic (thoracic cavity) growth in SCID mice, in association with an increased degree of cell apoptosis. Furthermore, it also suppressed the production of bloody pleural effusion after orthotopic injection. These findings suggest that the restored expression of MY018B may be a useful therapeutic strategy for the treatment of locally advanced MPM in humans.
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