Difference in response to colony-stimulating factors and involvement of protein kinase C signal transduction system in three subclones from the ME-1 cell line and two sublines

Kohsuke Yanagisawa; Masateru Sato; Takahiko Horiuchi; Hitoshi Hasegawa; Shigeru Fujita

doi:10.1182/blood.v84.1.84.bloodjournal84184

Difference in response to colony-stimulating factors and involvement of protein kinase C signal transduction system in three subclones from the ME-1 cell line and two sublines

Kohsuke Yanagisawa, Masateru Sato, Takahiko Horiuchi, Hitoshi Hasegawa, Shigeru Fujita

研究成果: ジャーナルへの寄稿 › 学術誌 › 査読

2 被引用数 (Scopus)

抄録

We previously established a cell line from a patient with acute myelomonocytic leukemia with eosinophilia (M₄E₀), ME-1. ME-1 cells are responsive to colony-stimulating factors (CSFs) such as interleukin-3 (IL- 3), IL-4, and granulocyte-macrophage CSF (GM-CSF), and exhibit monocyte- macrophage differentiation. We isolated three subclones, ME-F₁ from ME-1, and ME-F₂ and ME-F₃ from two sublines of ME-1. These subclones had different morphologic, cytochemical, phenotypic, and cytogenetic features. They represented different monocytic-lineage differentiation stages and exhibited different responses to IL-3, GM-CSF, and especially IL-4, IL-3, GM- CSF, and IL-4 enhanced proliferation and differentiation to macrophage-like cells in the ME-F₁ subclone. However, they enhanced only proliferation of ME-F₂ cells and only differentiation to macrophage-like cells in the ME-F₃ subclone. To elucidate possible differences in signal transduction mechanisms in ME-F₁, ME-F₂, and ME-F₂ cells following stimulation by CSFs, we studied the effects of IL-3 and IL-4 on protein kinase C (PKC) activity. Both IL-3 and IL-4 induced a rapid, transient decrease of cytosolic PKC in ME-F₁ cells, but did not affect PKC activity in ME-F₂ and ME-F₃ cells. The PKC inhibitors, 1-(5-isoquinolinyl-sulfonyl)-2-methylpiperazine (H-7) and calphostin C inhibited IL-3-induced enhancement of proliferation and differentiation of ME-F₁ cells, but did not inhibit enhancement of proliferation of ME-F₂ cells and differentiation of ME-F₃ cells. Our data suggest that PKC-dependent signal transduction is considerably related to IL- 3-induced proliferation and differentiation of ME-F₁ cells. In addition, it was demonstrated that the two subclones, ME-F₂ and ME-F₃, lost one of the two responses of ME-F₁ cells of CSFs, either proliferation or differentiation, and simultaneously lost PKC-dependent response to CSFs.

本文言語	英語
ページ（範囲）	84-93
ページ数	10
ジャーナル	Blood
巻	84
号	1
DOI	https://doi.org/10.1182/blood.v84.1.84.bloodjournal84184
出版ステータス	出版済み - 7月 1 1994
外部発表	はい

!!!All Science Journal Classification (ASJC) codes

生化学
免疫学
血液学
細胞生物学

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10.1182/blood.v84.1.84.bloodjournal84184

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title = "Difference in response to colony-stimulating factors and involvement of protein kinase C signal transduction system in three subclones from the ME-1 cell line and two sublines",

abstract = "We previously established a cell line from a patient with acute myelomonocytic leukemia with eosinophilia (M4E0), ME-1. ME-1 cells are responsive to colony-stimulating factors (CSFs) such as interleukin-3 (IL- 3), IL-4, and granulocyte-macrophage CSF (GM-CSF), and exhibit monocyte- macrophage differentiation. We isolated three subclones, ME-F1 from ME-1, and ME-F2 and ME-F3 from two sublines of ME-1. These subclones had different morphologic, cytochemical, phenotypic, and cytogenetic features. They represented different monocytic-lineage differentiation stages and exhibited different responses to IL-3, GM-CSF, and especially IL-4, IL-3, GM- CSF, and IL-4 enhanced proliferation and differentiation to macrophage-like cells in the ME-F1 subclone. However, they enhanced only proliferation of ME-F2 cells and only differentiation to macrophage-like cells in the ME-F3 subclone. To elucidate possible differences in signal transduction mechanisms in ME-F1, ME-F2, and ME-F2 cells following stimulation by CSFs, we studied the effects of IL-3 and IL-4 on protein kinase C (PKC) activity. Both IL-3 and IL-4 induced a rapid, transient decrease of cytosolic PKC in ME-F1 cells, but did not affect PKC activity in ME-F2 and ME-F3 cells. The PKC inhibitors, 1-(5-isoquinolinyl-sulfonyl)-2-methylpiperazine (H-7) and calphostin C inhibited IL-3-induced enhancement of proliferation and differentiation of ME-F1 cells, but did not inhibit enhancement of proliferation of ME-F2 cells and differentiation of ME-F3 cells. Our data suggest that PKC-dependent signal transduction is considerably related to IL- 3-induced proliferation and differentiation of ME-F1 cells. In addition, it was demonstrated that the two subclones, ME-F2 and ME-F3, lost one of the two responses of ME-F1 cells of CSFs, either proliferation or differentiation, and simultaneously lost PKC-dependent response to CSFs.",

author = "Kohsuke Yanagisawa and Masateru Sato and Takahiko Horiuchi and Hitoshi Hasegawa and Shigeru Fujita",

year = "1994",

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T1 - Difference in response to colony-stimulating factors and involvement of protein kinase C signal transduction system in three subclones from the ME-1 cell line and two sublines

AU - Yanagisawa, Kohsuke

AU - Sato, Masateru

AU - Horiuchi, Takahiko

AU - Hasegawa, Hitoshi

AU - Fujita, Shigeru

PY - 1994/7/1

Y1 - 1994/7/1

N2 - We previously established a cell line from a patient with acute myelomonocytic leukemia with eosinophilia (M4E0), ME-1. ME-1 cells are responsive to colony-stimulating factors (CSFs) such as interleukin-3 (IL- 3), IL-4, and granulocyte-macrophage CSF (GM-CSF), and exhibit monocyte- macrophage differentiation. We isolated three subclones, ME-F1 from ME-1, and ME-F2 and ME-F3 from two sublines of ME-1. These subclones had different morphologic, cytochemical, phenotypic, and cytogenetic features. They represented different monocytic-lineage differentiation stages and exhibited different responses to IL-3, GM-CSF, and especially IL-4, IL-3, GM- CSF, and IL-4 enhanced proliferation and differentiation to macrophage-like cells in the ME-F1 subclone. However, they enhanced only proliferation of ME-F2 cells and only differentiation to macrophage-like cells in the ME-F3 subclone. To elucidate possible differences in signal transduction mechanisms in ME-F1, ME-F2, and ME-F2 cells following stimulation by CSFs, we studied the effects of IL-3 and IL-4 on protein kinase C (PKC) activity. Both IL-3 and IL-4 induced a rapid, transient decrease of cytosolic PKC in ME-F1 cells, but did not affect PKC activity in ME-F2 and ME-F3 cells. The PKC inhibitors, 1-(5-isoquinolinyl-sulfonyl)-2-methylpiperazine (H-7) and calphostin C inhibited IL-3-induced enhancement of proliferation and differentiation of ME-F1 cells, but did not inhibit enhancement of proliferation of ME-F2 cells and differentiation of ME-F3 cells. Our data suggest that PKC-dependent signal transduction is considerably related to IL- 3-induced proliferation and differentiation of ME-F1 cells. In addition, it was demonstrated that the two subclones, ME-F2 and ME-F3, lost one of the two responses of ME-F1 cells of CSFs, either proliferation or differentiation, and simultaneously lost PKC-dependent response to CSFs.

AB - We previously established a cell line from a patient with acute myelomonocytic leukemia with eosinophilia (M4E0), ME-1. ME-1 cells are responsive to colony-stimulating factors (CSFs) such as interleukin-3 (IL- 3), IL-4, and granulocyte-macrophage CSF (GM-CSF), and exhibit monocyte- macrophage differentiation. We isolated three subclones, ME-F1 from ME-1, and ME-F2 and ME-F3 from two sublines of ME-1. These subclones had different morphologic, cytochemical, phenotypic, and cytogenetic features. They represented different monocytic-lineage differentiation stages and exhibited different responses to IL-3, GM-CSF, and especially IL-4, IL-3, GM- CSF, and IL-4 enhanced proliferation and differentiation to macrophage-like cells in the ME-F1 subclone. However, they enhanced only proliferation of ME-F2 cells and only differentiation to macrophage-like cells in the ME-F3 subclone. To elucidate possible differences in signal transduction mechanisms in ME-F1, ME-F2, and ME-F2 cells following stimulation by CSFs, we studied the effects of IL-3 and IL-4 on protein kinase C (PKC) activity. Both IL-3 and IL-4 induced a rapid, transient decrease of cytosolic PKC in ME-F1 cells, but did not affect PKC activity in ME-F2 and ME-F3 cells. The PKC inhibitors, 1-(5-isoquinolinyl-sulfonyl)-2-methylpiperazine (H-7) and calphostin C inhibited IL-3-induced enhancement of proliferation and differentiation of ME-F1 cells, but did not inhibit enhancement of proliferation of ME-F2 cells and differentiation of ME-F3 cells. Our data suggest that PKC-dependent signal transduction is considerably related to IL- 3-induced proliferation and differentiation of ME-F1 cells. In addition, it was demonstrated that the two subclones, ME-F2 and ME-F3, lost one of the two responses of ME-F1 cells of CSFs, either proliferation or differentiation, and simultaneously lost PKC-dependent response to CSFs.

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