Your search keyword '"Ao, Tomoka"' showing total 3 results

1. Thrombomodulin induces anti-inflammatory effects by inhibiting the rolling adhesion of leukocytes in vivo

Author

Nishizawa, Shino, Kikuta, Junichi, Seno, Shigeto, Kajiki, Masahiro, Tsujita, Ryuichi, Mizuno, Hiroki, Sudo, Takao, Ao, Tomoka, Matsuda, Hideo, and Ishii, Masaru

Abstract

Thrombomodulin (TM) is an integral membrane protein expressed on the surface of vascular endothelial cells that suppresses blood coagulation. Recent studies have shown that TM exhibits anti-inflammatory effects by inhibiting leukocyte recruitment. However, the actual modes of action of TM in vivoremain unclear. Here, we describe the pharmacological effects of recombinant human soluble TM (TM alfa) on leukocyte dynamics in living mice using intravital imaging techniques. Under control conditions, neutrophils exhibited three distinct types of adhesion behavior in vessels: 1) “non-adhesion”, in which cells flowed without vessel adhesion; 2) “rolling adhesion”, in which cells transiently interacted with the endothelium; and 3) “tight binding”, in which cells bound strongly to the endothelial cells. Compared to control conditions, local lipopolysaccharide stimulation resulted in an increased frequency of rolling adhesion that was not homogeneously distributed on vessel walls but occurred at specific endothelial sites. Under inflammatory conditions, TM alfa, particularly the D1 domain which is a lectin-like region of TM, significantly decreased the frequency of rolling adhesion, but did not influence the number of tight bindings. This was the first study to demonstrate that TM alfa exerts anti-inflammatory effects by inhibiting rolling adhesion of neutrophils to vascular endothelial cells in living mice.

Published

2020

2. Group 2 innate lymphoid cells support hematopoietic recovery under stress conditions

Author

Sudo, Takao, Motomura, Yasutaka, Okuzaki, Daisuke, Hasegawa, Tetsuo, Yokota, Takafumi, Kikuta, Junichi, Ao, Tomoka, Mizuno, Hiroki, Matsui, Takahiro, Motooka, Daisuke, Yoshizawa, Ryosuke, Nagasawa, Takashi, Kanakura, Yuzuru, Moro, Kazuyo, and Ishii, Masaru

Abstract

The cell-cycle status of hematopoietic stem and progenitor cells (HSPCs) becomes activated following chemotherapy-induced stress, promoting bone marrow (BM) regeneration; however, the underlying molecular mechanism remains elusive. Here we show that BM-resident group 2 innate lymphoid cells (ILC2s) support the recovery of HSPCs from 5-fluorouracil (5-FU)–induced stress by secreting granulocyte-macrophage colony-stimulating factor (GM-CSF). Mechanistically, IL-33 released from chemo-sensitive B cell progenitors activates MyD88-mediated secretion of GM-CSF in ILC2, suggesting the existence of a B cell–ILC2 axis for maintaining hematopoietic homeostasis. GM-CSF knockout mice treated with 5-FU showed severe loss of myeloid lineage cells, causing lethality, which was rescued by transferring BM ILC2s from wild-type mice. Further, the adoptive transfer of ILC2s to 5-FU–treated mice accelerates hematopoietic recovery, while the reduction of ILC2s results in the opposite effect. Thus, ILC2s may function by “sensing” the damaged BM spaces and subsequently support hematopoietic recovery under stress conditions.

Published

2021

3. Two Cases of Gouty Sacroiliitis Evaluated by Dual-energy Computed Tomography

Author

AO, TOMOKA, SHODA, HIROFUMI, and YAMAMOTO, KAZUHIKO

Published

2016