Tumor-propagating cells and Yap/Taz activity contribute to lung tumor progression and metastasis

Allison N. Lau; Stephen J. Curtis; Christine M. Fillmore; Samuel P. Rowbotham; Morvarid Mohseni; Darcy E. Wagner; Alexander M. Beede; Daniel T. Montoro; Kerstin W. Sinkevicius; Zandra E. Walton; Juliana Barrios; Daniel J. Weiss; Fernando D. Camargo; Kwok Kin Wong; Carla F. Kim

doi:10.1002/embj.201386082

Tumor-propagating cells and Yap/Taz activity contribute to lung tumor progression and metastasis

Allison N. Lau, Stephen J. Curtis, Christine M. Fillmore, Samuel P. Rowbotham, Morvarid Mohseni, Darcy E. Wagner, Alexander M. Beede, Daniel T. Montoro, Kerstin W. Sinkevicius, Zandra E. Walton, Juliana Barrios, Daniel J. Weiss, Fernando D. Camargo, Kwok Kin Wong, Carla F. Kim

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178 Citas (Scopus)

Resumen

Metastasis is the leading cause of morbidity for lung cancer patients. Here we demonstrate that murine tumor propagating cells (TPCs) with the markers Sca1 and CD24 are enriched for metastatic potential in orthotopic transplantation assays. CD24 knockdown decreased the metastatic potential of lung cancer cell lines resembling TPCs. In lung cancer patient data sets, metastatic spread and patient survival could be stratified with a murine lung TPC gene signature. The TPC signature was enriched for genes in the Hippo signaling pathway. Knockdown of the Hippo mediators Yap1 or Taz decreased in vitro cellular migration and transplantation of metastatic disease. Furthermore, constitutively active Yap was sufficient to drive lung tumor progression in vivo. These results demonstrate functional roles for two different pathways, CD24-dependent and Yap/Taz-dependent pathways, in lung tumor propagation and metastasis. This study demonstrates the utility of TPCs for identifying molecules contributing to metastatic lung cancer, potentially enabling the therapeutic targeting of this devastating disease.

Idioma original	Inglés
Páginas (desde-hasta)	468-481
Número de páginas	14
Publicación	EMBO Journal
Volumen	33
N.º	5
DOI	https://doi.org/10.1002/embj.201386082
Estado	Publicada - 3 mar. 2014
Publicado de forma externa	Sí

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Lau, A. N., Curtis, S. J., Fillmore, C. M., Rowbotham, S. P., Mohseni, M., Wagner, D. E., Beede, A. M., Montoro, D. T., Sinkevicius, K. W., Walton, Z. E., Barrios, J., Weiss, D. J., Camargo, F. D., Wong, K. K., & Kim, C. F. (2014). Tumor-propagating cells and Yap/Taz activity contribute to lung tumor progression and metastasis. EMBO Journal, 33(5), 468-481. https://doi.org/10.1002/embj.201386082

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title = "Tumor-propagating cells and Yap/Taz activity contribute to lung tumor progression and metastasis",

abstract = "Metastasis is the leading cause of morbidity for lung cancer patients. Here we demonstrate that murine tumor propagating cells (TPCs) with the markers Sca1 and CD24 are enriched for metastatic potential in orthotopic transplantation assays. CD24 knockdown decreased the metastatic potential of lung cancer cell lines resembling TPCs. In lung cancer patient data sets, metastatic spread and patient survival could be stratified with a murine lung TPC gene signature. The TPC signature was enriched for genes in the Hippo signaling pathway. Knockdown of the Hippo mediators Yap1 or Taz decreased in vitro cellular migration and transplantation of metastatic disease. Furthermore, constitutively active Yap was sufficient to drive lung tumor progression in vivo. These results demonstrate functional roles for two different pathways, CD24-dependent and Yap/Taz-dependent pathways, in lung tumor propagation and metastasis. This study demonstrates the utility of TPCs for identifying molecules contributing to metastatic lung cancer, potentially enabling the therapeutic targeting of this devastating disease.",

keywords = "CD24, lung cancer, metastasis, Taz, tumor propagating cells",

author = "Lau, {Allison N.} and Curtis, {Stephen J.} and Fillmore, {Christine M.} and Rowbotham, {Samuel P.} and Morvarid Mohseni and Wagner, {Darcy E.} and Beede, {Alexander M.} and Montoro, {Daniel T.} and Sinkevicius, {Kerstin W.} and Walton, {Zandra E.} and Juliana Barrios and Weiss, {Daniel J.} and Camargo, {Fernando D.} and Wong, {Kwok Kin} and Kim, {Carla F.}",

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Lau, AN, Curtis, SJ, Fillmore, CM, Rowbotham, SP, Mohseni, M, Wagner, DE, Beede, AM, Montoro, DT, Sinkevicius, KW, Walton, ZE, Barrios, J, Weiss, DJ, Camargo, FD, Wong, KK & Kim, CF 2014, 'Tumor-propagating cells and Yap/Taz activity contribute to lung tumor progression and metastasis', EMBO Journal, vol. 33, n.º 5, pp. 468-481. https://doi.org/10.1002/embj.201386082

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AU - Lau, Allison N.

AU - Curtis, Stephen J.

AU - Fillmore, Christine M.

AU - Rowbotham, Samuel P.

AU - Mohseni, Morvarid

AU - Wagner, Darcy E.

AU - Beede, Alexander M.

AU - Montoro, Daniel T.

AU - Sinkevicius, Kerstin W.

AU - Walton, Zandra E.

AU - Barrios, Juliana

AU - Weiss, Daniel J.

AU - Camargo, Fernando D.

AU - Wong, Kwok Kin

AU - Kim, Carla F.

PY - 2014/3/3

Y1 - 2014/3/3

N2 - Metastasis is the leading cause of morbidity for lung cancer patients. Here we demonstrate that murine tumor propagating cells (TPCs) with the markers Sca1 and CD24 are enriched for metastatic potential in orthotopic transplantation assays. CD24 knockdown decreased the metastatic potential of lung cancer cell lines resembling TPCs. In lung cancer patient data sets, metastatic spread and patient survival could be stratified with a murine lung TPC gene signature. The TPC signature was enriched for genes in the Hippo signaling pathway. Knockdown of the Hippo mediators Yap1 or Taz decreased in vitro cellular migration and transplantation of metastatic disease. Furthermore, constitutively active Yap was sufficient to drive lung tumor progression in vivo. These results demonstrate functional roles for two different pathways, CD24-dependent and Yap/Taz-dependent pathways, in lung tumor propagation and metastasis. This study demonstrates the utility of TPCs for identifying molecules contributing to metastatic lung cancer, potentially enabling the therapeutic targeting of this devastating disease.

AB - Metastasis is the leading cause of morbidity for lung cancer patients. Here we demonstrate that murine tumor propagating cells (TPCs) with the markers Sca1 and CD24 are enriched for metastatic potential in orthotopic transplantation assays. CD24 knockdown decreased the metastatic potential of lung cancer cell lines resembling TPCs. In lung cancer patient data sets, metastatic spread and patient survival could be stratified with a murine lung TPC gene signature. The TPC signature was enriched for genes in the Hippo signaling pathway. Knockdown of the Hippo mediators Yap1 or Taz decreased in vitro cellular migration and transplantation of metastatic disease. Furthermore, constitutively active Yap was sufficient to drive lung tumor progression in vivo. These results demonstrate functional roles for two different pathways, CD24-dependent and Yap/Taz-dependent pathways, in lung tumor propagation and metastasis. This study demonstrates the utility of TPCs for identifying molecules contributing to metastatic lung cancer, potentially enabling the therapeutic targeting of this devastating disease.

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KW - Taz

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Tumor-propagating cells and Yap/Taz activity contribute to lung tumor progression and metastasis

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