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免疫缺陷小鼠中的渐进性生长以及多瘤中T抗原转化的小鼠内皮细胞对宿主细胞的募集:对机会性血管肿瘤发病机制的影响

Progressive growth in immunodeficient mice and host cell recruitment by mouse endothelial cells transformed by polyoma middle-sized T antigen: implications for the pathogenesis of opportunistic vascular tumors.

作者信息

Garlanda C, Parravicini C, Sironi M, De Rossi M, Wainstok de Calmanovici R, Carozzi F, Bussolino F, Colotta F, Mantovani A, Vecchi A

机构信息

Istituto Mario Negri, Milan, Italy.

出版信息

Proc Natl Acad Sci U S A. 1994 Jul 19;91(15):7291-5. doi: 10.1073/pnas.91.15.7291.

Abstract

A retroviral construct encoding polyoma middle-sized T antigen was used to generate transformed endothelial cell lines from heart (H5V), brain (B9V), and whole-embryo (E10V) of C57BL/6 mice. When injected into syngeneic recipients, H5V and the less studied B9V and E10V cells caused vascular tumors which, depending on the number of cells inoculated, regressed or progressed, leading to death of the host. When H5V cells were injected into immunodeficient mice, tumors were observed with inocula which did not form lesions in immunocompetent recipients and regression did not occur. Treatment with anti-LFA-1, anti-Thy-1.2, and anti-CD8 antibodies abolished rejection; anti-CD4 was a somewhat less effective inhibitor of resistance. Animals with progressive tumors exhibited secondary lesions in various organs with prominent skin involvement in nude mice. Histologically, the tumors had the appearance of a hemangioma, with areas resembling Kaposi sarcoma. Cells lining vascular lacunae had the morphological features of injected H5V cells. The lesions were characterized by prominent neovascularization and mononuclear cell infiltration. Southern blot hybridization analysis revealed that approximately 5% of the cells in the tumor mass were transplanted H5V cells. Thus, the H5V transformed endothelial line causes vascular lesions that are sustained to a large extent by recruitment of host cells and manifests full malignant behavior only in immunocompromised hosts. The hypothesis of a tumor sustained by a minute proportion of transformed cells, which recruit host elements and express full malignant behavior only in immunodeficient hosts, would account for several features of some vascular neoplasms in man.

摘要

使用一种编码多瘤病毒中T抗原的逆转录病毒构建体,从C57BL/6小鼠的心脏(H5V)、脑(B9V)和全胚胎(E10V)中生成转化的内皮细胞系。当将其注射到同基因受体中时,H5V以及研究较少的B9V和E10V细胞会引发血管肿瘤,这些肿瘤根据接种细胞的数量,会消退或进展,最终导致宿主死亡。当将H5V细胞注射到免疫缺陷小鼠中时,接种了在免疫健全受体中不会形成病变的细胞数量后会观察到肿瘤,且不会发生消退。用抗LFA-1、抗Thy-1.2和抗CD8抗体进行治疗可消除排斥反应;抗CD4抗体是一种效果稍差的抗性抑制剂。患有进展性肿瘤的动物在各个器官出现继发性病变,裸鼠的皮肤受累尤为明显。组织学上,肿瘤呈现血管瘤的外观,有类似卡波西肉瘤的区域。血管腔隙内衬的细胞具有注射的H5V细胞的形态特征。病变的特点是显著的新生血管形成和单核细胞浸润。Southern印迹杂交分析显示,肿瘤块中约5%的细胞是移植的H5V细胞。因此,H5V转化的内皮细胞系会引发血管病变,这种病变在很大程度上是由宿主细胞的募集维持的,并且仅在免疫受损宿主中表现出完全的恶性行为。由一小部分转化细胞维持的肿瘤假说,即这些细胞募集宿主成分并仅在免疫缺陷宿主中表现出完全的恶性行为,这可以解释人类某些血管肿瘤的几个特征。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cc4e/44385/275c318f35f1/pnas01137-0587-a.jpg

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