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T细胞杂交瘤在小鼠肝细胞和成纤维细胞单层中的侵袭性及转移潜能。

Invasiveness in hepatocyte and fibroblast monolayers and metastatic potential of T-cell hybridomas in mice.

作者信息

la Rivière G, Schipper C A, Collard J G, Roos E

机构信息

Division of Cell Biology, The Netherlands Cancer Institute, Amsterdam.

出版信息

Cancer Res. 1988 Jun 15;48(12):3405-10.

PMID:3285995
Abstract

Fusion of noninvasive, nonmetastatic BW5147 T-lymphoma cells with normal T-lymphocytes usually resulted in highly invasive and metastatic T-cell hybridomas, apparently due to properties derived from the normal T-cell. Occasionally hybrids arose that were non- or low invasive, probably by loss of relevant genes upon chromosome segregation, since these cells contained much less DNA than highly invasive hybrids. The metastatic potential of 20 representative T-cell hybridomas was tested by tail vein injection in syngeneic mice and cells were found to be either nonmetastatic (NM), low metastatic (LM), or high metastatic (HM). NM hybrids were tumorigenic but did not form metastases and HM hybridomas caused wide-spread metastasis. LM cells formed metastases in a limited number of mice and predominantly in lymphoid tissues. In hepatocyte cultures, NM cell lines were found to be the least invasive, HM cells the most, whereas LM hybrids exhibited intermediate levels. Invasiveness was not only measured in rat hepatocyte cultures but also in rat embryo fibroblast monolayers, and the relative invasive capacity in both model systems correlated well. Pertussis toxin inhibited invasion in both systems to 20-30% of control values. This suggests that the mechanisms of invasion into hepatocyte and fibroblast cultures are at least partially similar and that the fibroblast invasion assay is a relevant model to study aspects of lymphoma metastasis. We conclude that invasive potential is a prerequisite for T-cell hybridomas to colonize tissues from the bloodstream and that a minimum level of invasiveness is necessary for extensive and wide-spread metastasis formation.

摘要

非侵袭性、非转移性的BW5147 T淋巴瘤细胞与正常T淋巴细胞融合通常会产生高度侵袭性和转移性的T细胞杂交瘤,这显然是由于源自正常T细胞的特性所致。偶尔会出现非侵袭性或低侵袭性的杂交瘤,可能是由于染色体分离时相关基因的丢失,因为这些细胞所含的DNA比高侵袭性杂交瘤少得多。通过在同基因小鼠尾静脉注射来测试20种代表性T细胞杂交瘤的转移潜力,发现这些细胞要么是非转移性的(NM)、低转移性的(LM),要么是高转移性的(HM)。NM杂交瘤具有致瘤性但不形成转移灶,而HM杂交瘤会导致广泛转移。LM细胞在少数小鼠中形成转移灶,且主要在淋巴组织中。在肝细胞培养中,发现NM细胞系侵袭性最低,HM细胞最高,而LM杂交瘤表现出中等水平。侵袭性不仅在大鼠肝细胞培养中进行测量,也在大鼠胚胎成纤维细胞单层中进行测量,并且在这两种模型系统中的相对侵袭能力具有良好的相关性。百日咳毒素在两种系统中均将侵袭抑制至对照值的20% - 30%。这表明侵入肝细胞和成纤维细胞培养物的机制至少部分相似,并且成纤维细胞侵袭试验是研究淋巴瘤转移方面的一个相关模型。我们得出结论,侵袭潜力是T细胞杂交瘤从血液中定植到组织的先决条件,并且对于广泛和扩散性转移灶的形成,最低水平 的侵袭性是必要的。

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