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首页> 外文期刊>Journal of Virology >Abelson virus-infected cells can exhibit restricted in vitro growth and low oncogenic potential.
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Abelson virus-infected cells can exhibit restricted in vitro growth and low oncogenic potential.

机译:Abelson病毒感染的细胞可以显示出限制体外生长和低致癌潜力。

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We have designed a method for growing bone marrow cells infected with Abelson murine leukemia virus which permits examination of target cell growth early after infection. This culture system increases the efficiency of target cell growth by favoring rapid growth of a mixed population of adherent cells in the primary culture. The nonadherent Abelson virus-infected cell populations expressed pre-B-cell differentiation markers characteristic of Abelson virus-transformed cells (mu-heavy chains of immunoglobulin M and terminal deoxynucleotidyltransferase). Early after infection, these cell populations exhibited restricted in vitro and in vivo growth properties which differed from those of an established Abelson virus-transformed cell line, 2M3. These included a marked dependency upon the adherent cell layer for growth and viability, a lower efficiency of agar colony formation, and a lower capacity for tumor production in syngeneic animals. Growth of the early populations could be maintained in the absence of the adherent cell layer by using conditioned medium from long-term adherent cell cultures established in the absence of viral infection. After passage of the populations for several weeks, the in vitro growth properties gradually shifted toward that of the 2M3 cell line. Twelve-week-old populations grew independently of the adherent cell layer and showed an increased efficiency of agar colony formation. These data indicate that many lymphoid target cells exhibit an intermediate transformed phenotype when infected with Abelson virus. Growth of these cells in culture is mediated via a synergistic interaction between intracellular expression of the viral transforming gene and an exogenous growth-promoting activity which can be provided by cultures of adherent bone marrow cells.
机译:我们设计了一种生长骨髓细胞的方法,用于患有阿贝森鼠白血病病毒的骨髓细胞,允许在感染后早期检查靶细胞生长。该培养系统通过有利于初级培养物中的粘附细胞混合群的快速生长来提高靶细胞生长的效率。非偏见的阿塞隆病毒感染的细胞群表达了阿比索病毒转化细胞的B-细胞分化标志物特征(免疫球蛋白M和末端脱氧核苷酸转移酶的莫重链。感染早期,这些细胞群在体外含有限制和体内生长性质,其与已建立的阿尔森病毒转化的细胞系2M3不同。这些包括对粘附细胞层的显着依赖性,用于生长和活力,琼脂菌落形成的效率较低,以及在同联的动物中肿瘤产生的较低能力。通过在没有病毒感染的长期粘附细胞培养物中使用条件培养基,可以在没有粘附细胞层的情况下保持早期种群的生长。在群体通过几周后,体外生长性能逐渐朝向2M3细胞系的变化。十二周龄人口独立于粘附细胞层而增长,并显示出琼脂菌落形成的效率提高。这些数据表明,当感染阿米尔逊病毒时,许多淋巴靶细胞表现出中间转化的表型。通过在病毒转化基因的细胞内表达和外源生长促进活性之间的协同相互作用可以通过粘附骨髓细胞的培养物提供这些细胞的生长介导。

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