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Modeling mesothelioma utilizing human mesothelial cells reveals involvement of phospholipase-C beta 4 in YAP-active mesothelioma cell proliferation.
Kakiuchi, Tatsuo; Takahara, Taishi; Kasugai, Yumiko; Arita, Kotaro; Yoshida, Noriaki; Karube, Kennosuke; Suguro, Miyuki; Matsuo, Keitaro; Nakanishi, Hayao; Kiyono, Tohru; Nakamura, Shigeo; Osada, Hirotaka; Sekido, Yoshitaka; Seto, Masao; Tsuzuki, Shinobu.
Afiliação
  • Kakiuchi T; Division of Molecular Medicine, Aichi Cancer Center Research Institute , Nagoya 464-8681 , Japan.
  • Takahara T; Department of Pathology and Clinical Laboratories, Nagoya University Hospital , Nagoya 466-0065 , Japan.
  • Kasugai Y; Division of Molecular Medicine, Aichi Cancer Center Research Institute , Nagoya 464-8681 , Japan.
  • Arita K; Department of Pathology and Clinical Laboratories, Nagoya University Hospital , Nagoya 466-0065 , Japan.
  • Yoshida N; Division of Molecular Medicine, Aichi Cancer Center Research Institute , Nagoya 464-8681 , Japan.
  • Karube K; Third Department of Internal Medicine, Graduate School of Medicine and Pharmaceutical Sciences, University of Toyama , Toyama 930-0194 , Japan.
  • Suguro M; Department of Pathology, Kurume University School of Medicine , Kurume 830-0011 , Japan.
  • Matsuo K; Present address: Department of Medical Oncology, Dana-Farber Cancer Institute, Harvard Medical School, Boston, MA 02115, USA.
  • Nakanishi H; Laboratory of Cytopathology, Faculty of Medicine, University of the Ryukyus , Okinawa 903-0215 , Japan.
  • Kiyono T; Division of Molecular Medicine, Aichi Cancer Center Research Institute , Nagoya 464-8681 , Japan.
  • Nakamura S; Division of Molecular Medicine, Aichi Cancer Center Research Institute , Nagoya 464-8681 , Japan.
  • Osada H; Laboratory of Pathology and Clinical Research, Aichi Cancer Center , Aichi Hospital, Okazaki 444-0011 , Japan.
  • Sekido Y; Division of Carcinogenesis and Cancer Prevention, National Cancer Center Research Institute , Tokyo 104-0045 , Japan.
  • Seto M; Department of Pathology and Clinical Laboratories, Nagoya University Hospital , Nagoya 466-0065 , Japan.
  • Tsuzuki S; Division of Molecular Oncology, Aichi Cancer Center Research Institute , Nagoya 464-8681 , Japan.
Carcinogenesis ; 37(11): 1098-1109, 2016 Nov 01.
Article em En | MEDLINE | ID: mdl-27559111
Mesotheliomas are frequently characterized by disruption of Hippo pathway due to deletion and/or mutation in genes, such as neurofibromin 2 ( NF2 ). Hippo disruption attenuates yes-associated protein (YAP) phosphorylation allowing YAP to translocate to the nucleus and regulate gene expression. The role of disrupted Hippo pathway in maintenance of established mesotheliomas has been extensively investigated using cell lines; however, its involvement in development of human mesothelioma has not been explored much. Here, we employed immortalized human mesothelial cells to disrupt Hippo pathway. YAP phosphorylation was reduced on NF2 knockdown and the cells exhibited altered growth in vitro , developing tumors when transplanted into nude mice. Similar results were obtained from enforced expression of wild-type or constitutively active (S127A) YAP, indicating the crucial role of activated YAP in the transformation of mesothelial cells. Gene expression analysis comparing control- and YAP-transduced immortalized human mesothelial cells revealed phospholipase-C beta 4 ( PLCB4 ) to be among the genes highly upregulated by YAP. PLCB4 was upregulated by YAP in immortalized human mesothelial cells and downregulated on YAP knockdown in Hippo-disrupted mesothelioma cell lines. PLCB4 knockdown attenuated the growth of YAP-transduced immortalized mesothelial cells and YAP-active, but not YAP-nonactive, mesothelioma cell lines. Our model system thus provides a versatile tool to investigate the mechanisms underlying mesothelioma development. We suggest that PLCB4 may be an attractive drug target for the treatment of mesothelioma.

Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2016 Tipo de documento: Article

Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2016 Tipo de documento: Article