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人肺癌低分子量物质对单核细胞补体受体增强作用的抑制

Inhibition of monocyte complement receptor enhancement by low molecular weight material from human lung cancers.

作者信息

Glass E J, Abell C A, Kay A B

出版信息

Clin Exp Immunol. 1981 Mar;43(3):540-8.

Abstract

We have studied the effect of dialysates from lung cancer homogenates to alter both the expression of complement (C3b) receptors per se and also to inhibit leucoattractant-induced enhancement of complement rosettes on monocytes from healthy individuals. Enhancement and enhancement-inhibition by tumour extracts were compared with material derived from normal lung excised from distance from the tumour. There was no significant difference between tumour homogenate (TH) and normal lung homogenate (NLH) in terms of enhancement of complement rosettes per se. In contrast, TH produced a dose- and time-dependent inhibition of leucoattractant-induced enhancement of C3b rosettes which was significantly different from that obtained with NLH. This enhancement-inhibition was observed with four undifferentiated, four squamous and three adenocarcinomas of lung. The degree of enhancement-inhibition was not related to the type of tumour or varying accompanying histological features such as necrosis and the degree of infiltration with inflammatory cells. Following gel filtration on Sephadex G-50 each type of cancer gave a major peak of inhibitory activity which eluted with molecules having an apparent molecular size of approximately 3,000 daltons. A second larger peak (8,000-10,000 daltons) was also detected with extracts from the undifferentiated and adenocarcinomas. These results support previous findings, mainly from experimental animals, indicating that 'anti-macrophage/monocyte principles' are elaborated from certain tumour types.

摘要

我们研究了肺癌匀浆透析液对健康个体单核细胞上补体(C3b)受体表达本身的影响,以及对趋化因子诱导的补体花环增强作用的抑制作用。将肿瘤提取物的增强和增强抑制作用与距肿瘤一定距离处切除的正常肺组织提取物进行了比较。就补体花环本身的增强而言,肿瘤匀浆(TH)和正常肺匀浆(NLH)之间没有显著差异。相反,TH对趋化因子诱导的C3b花环增强产生了剂量和时间依赖性的抑制作用,这与NLH显著不同。在4例未分化型、4例鳞状和3例肺腺癌中均观察到这种增强抑制作用。增强抑制程度与肿瘤类型或不同的伴随组织学特征如坏死和炎症细胞浸润程度无关。在Sephadex G - 50上进行凝胶过滤后,每种癌症类型都给出了一个主要的抑制活性峰,其洗脱的分子表观分子量约为3000道尔顿。在未分化癌和腺癌提取物中还检测到第二个较大的峰(8000 - 10000道尔顿)。这些结果支持了之前主要来自实验动物的研究结果,表明某些肿瘤类型会产生“抗巨噬细胞/单核细胞因子”。

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