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白细胞在体内与小鼠提睾肌微循环的相互作用,以响应肿瘤条件培养基。

Leucocyte interactions with the mouse cremaster muscle microcirculation in vivo in response to tumour-conditioned medium.

作者信息

Brown N J, Reed M W

机构信息

Department of Surgical and Anaesthetic Sciences, Royal Hallamshire Hospital, Sheffield, UK.

出版信息

Br J Cancer. 1997;75(7):993-9. doi: 10.1038/bjc.1997.171.

Abstract

Leucocyte interactions with the cremaster muscle microcirculation in vivo were investigated in response to culture medium conditioned with different cell types in 25 adult male Swiss mice. Animals were divided into five groups. Three groups received ex vivo fluorescently labelled lymphokine activated killer (LAK) cells systemically and had either tumour (murine melanoma K1735)-conditioned medium (TCM), fibroblast (murine 3T3)-conditioned medium (FCM) or fresh culture medium administered topically to the cremaster muscle. In the two remaining groups, the host leucocytes were labelled fluorescently by systemic administration of acridine red, and either TCM or FCM was applied topically to the cremaster muscle. There was an immediate but transient increase in the frequency of rolling and adherent LAK cells, and a subsequent (90-120 min later) increase in rolling and adherent host leucocytes, demonstrating temporal differences in the response to topical administration of TCM. These increases in contact with the vascular endothelium occurred in all vessel types, venules, arterioles and capillaries, with the greatest response observed in the venules. The FCM and normal culture medium did not affect the distribution and localization of either LAK cells or host leucocytes. These data suggest that there are one or more soluble tumour-specific chemoattractants for leucocytes present in the conditioned medium. The mouse cremaster muscle microcirculation is therefore a useful model to investigate the mechanism of leucocyte-endothelium interactions in tumour biology.

摘要

在25只成年雄性瑞士小鼠体内,研究了白细胞与提睾肌微循环的相互作用,以响应不同细胞类型条件培养基的作用。动物被分为五组。三组全身接受体外荧光标记的淋巴因子激活杀伤细胞(LAK),并分别将肿瘤(鼠黑色素瘤K1735)条件培养基(TCM)、成纤维细胞(鼠3T3)条件培养基(FCM)或新鲜培养基局部应用于提睾肌。在其余两组中,通过全身给予吖啶红对宿主白细胞进行荧光标记,并将TCM或FCM局部应用于提睾肌。滚动和黏附的LAK细胞频率立即但短暂增加,随后(90 - 120分钟后)滚动和黏附的宿主白细胞增加,这表明对TCM局部给药的反应存在时间差异。与血管内皮细胞的这些接触增加发生在所有血管类型中,即小静脉、小动脉和毛细血管,其中小静脉中的反应最为明显。FCM和正常培养基对LAK细胞或宿主白细胞的分布和定位没有影响。这些数据表明,条件培养基中存在一种或多种针对白细胞的可溶性肿瘤特异性趋化因子。因此,小鼠提睾肌微循环是研究肿瘤生物学中白细胞 - 内皮细胞相互作用机制的有用模型。

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