Dexamethasone palmitate ameliorates macrophages-rich graft-versus-host disease by inhibiting macrophage functions

Satoshi Nishiwaki; Takayuki Nakayama; Makoto Murata; Tetsuya Nishida; Seitaro Terakura; Shigeki Saito; Tomonori Kato; Hiroki Mizuno; Nobuhiko Imahashi; Aika Seto; Yukiyasu Ozawa; Koichi Miyamura; Masafumi Ito; Kyosuke Takeshita; Hidefumi Kato; Shinya Toyokuni; Keisuke Nagao; Ryuzo Ueda; Tomoki Naoe

doi:10.1371/journal.pone.0096252

Dexamethasone palmitate ameliorates macrophages-rich graft-versus-host disease by inhibiting macrophage functions

Satoshi Nishiwaki, Takayuki Nakayama, Makoto Murata, Tetsuya Nishida, Seitaro Terakura, Shigeki Saito, Tomonori Kato, Hiroki Mizuno, Nobuhiko Imahashi, Aika Seto, Yukiyasu Ozawa, Koichi Miyamura, Masafumi Ito, Kyosuke Takeshita, Hidefumi Kato, Shinya Toyokuni, Keisuke Nagao, Ryuzo Ueda, Tomoki Naoe

血液内科学

研究成果: Article › 査読

26 被引用数 (Scopus)

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Macrophage infiltration of skin GVHD lesions correlates directly with disease severity, but the mechanisms underlying this relationship remain unclear and GVHD with many macrophages is a therapeutic challenge. Here, we characterize the macrophages involved in GVHD and report that dexamethasone palmitate (DP), a liposteroid, can ameliorate such GVHD by inhibiting macrophage functions. We found that host-derived macrophages could exacerbate GVHD in a mouse model through expression of higher levels of pro-inflammatory TNF-α and IFN-γ, and lower levels of anti-inflammatory IL-10 than resident macrophages in mice without GVHD. DP significantly decreased the viability and migration capacity of primary mouse macrophages compared to conventional dexamethasone in vitro. DP treatment on day 7 and day 14 decreased macrophage number, and attenuated GVHD score and subsequent mortality in a murine model. This is the first study to provide evidence that therapy for GVHD should be changed on the basis of infiltrating cell type.

本文言語	English
論文番号	e96252
ジャーナル	PloS one
巻	9
号	5
DOI	https://doi.org/10.1371/journal.pone.0096252
出版ステータス	Published - 07-05-2014

All Science Journal Classification (ASJC) codes

一般

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10.1371/journal.pone.0096252

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Nishiwaki, S., Nakayama, T., Murata, M., Nishida, T., Terakura, S., Saito, S., Kato, T., Mizuno, H., Imahashi, N., Seto, A., Ozawa, Y., Miyamura, K., Ito, M., Takeshita, K., Kato, H., Toyokuni, S., Nagao, K., Ueda, R., & Naoe, T. (2014). Dexamethasone palmitate ameliorates macrophages-rich graft-versus-host disease by inhibiting macrophage functions. PloS one, 9(5), [e96252]. https://doi.org/10.1371/journal.pone.0096252

Nishiwaki, Satoshi ; Nakayama, Takayuki ; Murata, Makoto ; Nishida, Tetsuya ; Terakura, Seitaro ; Saito, Shigeki ; Kato, Tomonori ; Mizuno, Hiroki ; Imahashi, Nobuhiko ; Seto, Aika ; Ozawa, Yukiyasu ; Miyamura, Koichi ; Ito, Masafumi ; Takeshita, Kyosuke ; Kato, Hidefumi ; Toyokuni, Shinya ; Nagao, Keisuke ; Ueda, Ryuzo ; Naoe, Tomoki. / Dexamethasone palmitate ameliorates macrophages-rich graft-versus-host disease by inhibiting macrophage functions. In: PloS one. 2014 ; Vol. 9, No. 5.

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title = "Dexamethasone palmitate ameliorates macrophages-rich graft-versus-host disease by inhibiting macrophage functions",

abstract = "Macrophage infiltration of skin GVHD lesions correlates directly with disease severity, but the mechanisms underlying this relationship remain unclear and GVHD with many macrophages is a therapeutic challenge. Here, we characterize the macrophages involved in GVHD and report that dexamethasone palmitate (DP), a liposteroid, can ameliorate such GVHD by inhibiting macrophage functions. We found that host-derived macrophages could exacerbate GVHD in a mouse model through expression of higher levels of pro-inflammatory TNF-α and IFN-γ, and lower levels of anti-inflammatory IL-10 than resident macrophages in mice without GVHD. DP significantly decreased the viability and migration capacity of primary mouse macrophages compared to conventional dexamethasone in vitro. DP treatment on day 7 and day 14 decreased macrophage number, and attenuated GVHD score and subsequent mortality in a murine model. This is the first study to provide evidence that therapy for GVHD should be changed on the basis of infiltrating cell type.",

author = "Satoshi Nishiwaki and Takayuki Nakayama and Makoto Murata and Tetsuya Nishida and Seitaro Terakura and Shigeki Saito and Tomonori Kato and Hiroki Mizuno and Nobuhiko Imahashi and Aika Seto and Yukiyasu Ozawa and Koichi Miyamura and Masafumi Ito and Kyosuke Takeshita and Hidefumi Kato and Shinya Toyokuni and Keisuke Nagao and Ryuzo Ueda and Tomoki Naoe",

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Nishiwaki, S, Nakayama, T, Murata, M, Nishida, T, Terakura, S, Saito, S, Kato, T, Mizuno, H, Imahashi, N, Seto, A, Ozawa, Y, Miyamura, K, Ito, M, Takeshita, K, Kato, H, Toyokuni, S, Nagao, K, Ueda, R & Naoe, T 2014, 'Dexamethasone palmitate ameliorates macrophages-rich graft-versus-host disease by inhibiting macrophage functions', PloS one, vol. 9, no. 5, e96252. https://doi.org/10.1371/journal.pone.0096252

Dexamethasone palmitate ameliorates macrophages-rich graft-versus-host disease by inhibiting macrophage functions. / Nishiwaki, Satoshi; Nakayama, Takayuki; Murata, Makoto; Nishida, Tetsuya; Terakura, Seitaro; Saito, Shigeki; Kato, Tomonori; Mizuno, Hiroki; Imahashi, Nobuhiko; Seto, Aika; Ozawa, Yukiyasu; Miyamura, Koichi; Ito, Masafumi; Takeshita, Kyosuke; Kato, Hidefumi; Toyokuni, Shinya; Nagao, Keisuke; Ueda, Ryuzo; Naoe, Tomoki.

In: PloS one, Vol. 9, No. 5, e96252, 07.05.2014.

研究成果: Article › 査読

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AU - Nishiwaki, Satoshi

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AU - Terakura, Seitaro

AU - Saito, Shigeki

AU - Kato, Tomonori

AU - Mizuno, Hiroki

AU - Imahashi, Nobuhiko

AU - Seto, Aika

AU - Ozawa, Yukiyasu

AU - Miyamura, Koichi

AU - Ito, Masafumi

AU - Takeshita, Kyosuke

AU - Kato, Hidefumi

AU - Toyokuni, Shinya

AU - Nagao, Keisuke

AU - Ueda, Ryuzo

AU - Naoe, Tomoki

PY - 2014/5/7

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N2 - Macrophage infiltration of skin GVHD lesions correlates directly with disease severity, but the mechanisms underlying this relationship remain unclear and GVHD with many macrophages is a therapeutic challenge. Here, we characterize the macrophages involved in GVHD and report that dexamethasone palmitate (DP), a liposteroid, can ameliorate such GVHD by inhibiting macrophage functions. We found that host-derived macrophages could exacerbate GVHD in a mouse model through expression of higher levels of pro-inflammatory TNF-α and IFN-γ, and lower levels of anti-inflammatory IL-10 than resident macrophages in mice without GVHD. DP significantly decreased the viability and migration capacity of primary mouse macrophages compared to conventional dexamethasone in vitro. DP treatment on day 7 and day 14 decreased macrophage number, and attenuated GVHD score and subsequent mortality in a murine model. This is the first study to provide evidence that therapy for GVHD should be changed on the basis of infiltrating cell type.

AB - Macrophage infiltration of skin GVHD lesions correlates directly with disease severity, but the mechanisms underlying this relationship remain unclear and GVHD with many macrophages is a therapeutic challenge. Here, we characterize the macrophages involved in GVHD and report that dexamethasone palmitate (DP), a liposteroid, can ameliorate such GVHD by inhibiting macrophage functions. We found that host-derived macrophages could exacerbate GVHD in a mouse model through expression of higher levels of pro-inflammatory TNF-α and IFN-γ, and lower levels of anti-inflammatory IL-10 than resident macrophages in mice without GVHD. DP significantly decreased the viability and migration capacity of primary mouse macrophages compared to conventional dexamethasone in vitro. DP treatment on day 7 and day 14 decreased macrophage number, and attenuated GVHD score and subsequent mortality in a murine model. This is the first study to provide evidence that therapy for GVHD should be changed on the basis of infiltrating cell type.

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SN - 1932-6203

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Dexamethasone palmitate ameliorates macrophages-rich graft-versus-host disease by inhibiting macrophage functions

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