• 약학회지
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• 제52권5호
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• pp.412-417
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• 2008

BAY11-7082 was initially found to be an anti-inflammatory drug with NF-${\kappa}B$ inhibitory property. In this study, we evaluated modulatory function of BAY11-7082 on U937 cell-cell adhesion induced by CD29 (${\beta}1$-integrins). BAY11-7082 strongly blocked functional activation of CD29 (${\beta}1$-integrins), as assessed by cell-cell adhesion assay. However, this compound did not block a simple activation of CD29, as assessed by cell-fibronectin adhesion assay. In particular, to understand molecular mechanism of BAY11-7082-mediated inhibition, the regulatory roles of CD29-induced actin cytoskeleton rearrangement under cell-cell adhesion and surface level of CD29 were examined using confocal and flow cytometic analysis. Interestingly, this compound strongly suppressed the molecular association of actin cytoskeleton with CD29 at cell-cell adhesion site. Moreover, BAY11-7082 also diminished surface levels of CD29 as well as its-associated adhesion molecule CD147, but not other adhesion molecules such as CD18 and CD43. Therefore, our data suggest that BAY11-7082 may be involved in regulating immune responses managed by CD29-mediated cell-cell adhesion.

• Tuberculosis and Respiratory Diseases
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• 제43권4호
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• pp.579-589
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• 1996

연구배경 : 패혈증에서 백혈구의 활성화는 미생물 및 숙주 독성 물질의 청소에 중요한 역활을 하며 한편으로 활성화된 호중구와 그의 특성 물질은 조직 손상파 장기의 기증 부전을 초래한다. 백혈구의 CD11/18 유착 분자는 감염 및 염증 부위로 호중구 이동의 첫 단계인 호중구-내피 세포 유착을 조절한다. 패혈증 치료 전락으로 호중구 억제 효과의 가능성을 알아보기 위해 rat 에서 Escherichia coli 폐렴을 유발하여 CD11b에 대한 단클론 항체(MAb 1B6)의 효과를 평가하였다. 방법 : 1 mg/kg CD11b에 대한 단클론 항체와 1 mg/kg BSA출 폐렴 유발 6 시간전, 유발시 및 유발 6 시간후 무작위적으로 피하 투여하였다. 폐렴 유발후 무작위적으로 24, 60 및 90%의 산소를 투여하였으며 폐렴 유발후 4시간 및 3일간 하루에 한번씩 100 mg/kg의 ceftriaxone을 투여하였다. 말초 및 폐포 호중구와 폐 손상의 지표인 D(A-a)O2, W/D LW ratio 및 폐포 세척액 단백 농도를 12시간과 96시간까지 생존한 동물에서 측정하였다. 결과 : CD11b에 대한 단클론 항체는 말초 및 폐포 호중구를 감소시켰으며 96시간 보다 12시간에 더욱 감소시켰다. 폐손상 지표는 단클론 항체 투여군과 대조군을 비교시 차이를 보이지 앉았으나 생존 동물 수의 부족으로 통계학적 평가의 의미가 없었다. 조기(6 시간) 사망률은 항체 투여군 51%로 대조군 31%보다 의미(P=0.02) 있게 증가하였으나 후기 사망률(12 시간에서 72 시간)은 항체 투여군 44% 대조군 36%로 의미(P=0.089) 있는 차이가 없었다. 결론 : CD11b/18 유착 분자는 감염 및 염증 부위로 호중구의 이동을 조절하는 것으로 알려져 있다. CD11b에 대한 단클론 항체는 rat의 폐인성 패혈증에서 폐포 호중구를 감소시키고 조기 사망률을 증가시켰다. 따라서 CD11b에 대한 단클론 항체가 rat의 폐인성 패혈증의 초기에 호중구의 폐포내 이동을 억제시켜 숙주의 방어 기전에 장애를 초래하여 조기 사망률을 증가시키는 것으로 사료된다.

• Journal of Acupuncture Research
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• 제18권1호
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• pp.100-112
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• 2001

Objective : The purpose of this study is to investigate the immunological effect of Ramulus Cinnamomum aqua-acupuncture on the cellular immune response in mice with LPS induced arthritis. Methods : All the BALB/C mice used in this study were bred and maintaned in our pathogen-free mouse colony and were 6wk of age at the start of the experiment. The experimental model of arthritis was induced by injeciton of 300${\mu}g$/kg LPS in mice knee joint. Ramulus Cinnamomum aqua-acupuncture was injected into Yangnungchon(Gb34) of mice 2daily for 14days. Immunohistochemical analysis was carried out to assess CD4+, CD8+, CD11b, IL-$1{\beta}$, IL-2R and CD106 expression in common iliac lymph nodes and synovial menbrane after stimulation with Ramulus Cinnamomum. Electron microscopy was carried out to assess change of synovial membrane. Ramulus Cinnamomum aqua-acupuncture stimulation group was compared to control group and non stimutated with aqua-acupuncture. Resutts : At day 14 post arthritis onset, Immunohistological studies using monoclonal antibodies showed that Ramulus Cinnamomum aqua-acupuncture goup had decreased expression of CD4+, CD8+, CD11b, IL-$1{\beta}$, IL-2R and CD106 at common illiac lymph nodes and synovial membrane compared with control group. Conclusions : Ramulus Cinnamomum aqua-acupuncture stimulation inhibited the development of cellular immunity to LPS-induced arthritis in mice. Thus, aqua-acupuncture stimulation may have preventive effects on autoimmune inflammatory joint diseases. The effects of AA on immune function and disease activity in patients with RA warrant further investigation.

• Journal of Periodontal and Implant Science
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• 제29권2호
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• pp.333-350
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• 1999

The modulation of leukocyte cell surface adhesion molecules may influence the development of cellular events that determine the course of the inflammatory process. Direct interaction between activated T cells and monocytes resulted in a large production of $IL-1{\beta}$ by monocytes. In this reactions, adhesion molecules play an important part, yet the role of them in Tmonocytes interaction remain unclear. This study was undertaken in an effort to elucidate, 1) the influence of 1.25(OH)$_2D_3-induced$ differentiation on the monocyte responsiveness to direct contact with T lymphocytes, and 2) the role of adhesion molecules on the T-monocyte direct interaction. Initially, I observed that direct contact of monocyte cell line THP-1 with stimulated fixed T cell line HuT78 markedly induces IL-1${\beta}$ production by THP-1. $IL-1{\beta}$ production was higher when THP-1 had been previously exposed to 1.25(OH)$_2D_3$ as compared to control, with ${\alpha}$- 1.25(OH)$_2D_3$ dose-dependent and exposure time-dependent manner. It was shown that 1.25(OH)$_2D_3$ also increased the expression of ${\beta}_2$ integrin adhesion receptor Mac-1(CD11b/CD18) dose- and timedependently, but did not increase the expression of human leukocyte antigen- D(HLA-D) and intercellular adhesion molecule-1(ICAM-1). The $IL-1{\beta}$ producing activity of THP-1 cells correlated well with the ability to induce the Mac-1 expression on THP-1 surface. Monoclonal antibody raised against relevant cell surface glycoproteins on THP-1 were tested for their ability to block the response of THP-1 to T cells. Antibody to Mac-1 only partially blocked $IL-1{\beta}$ production by THP-1, whereas antibodies to ICAM-1 and HLA-D did not. These data indicate that regulation of Mac-1 expression on THP-1 cells can alter the responsiveness of these cells to contact by activated T cells, however other unknown structures on the THP-1 cells may be involved in this process also.