首页> 外文期刊>The Journal of Experomental Medicine >Stages in development of mink cell focus-inducing (MCF) virus-accelerated leukemia in AKR mice.
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Stages in development of mink cell focus-inducing (MCF) virus-accelerated leukemia in AKR mice.

机译:AKR小鼠中水貂细胞聚焦诱导(MCF)病毒加速白血病的发展阶段。

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Flow cytometric techniques involving correlated dual parameter analysis of fluorescence and light scatter and transplantation bioassays were used to describe a series of cellular changes in thymus of young (1-4 mo old) AKR mice during development of mink cell focus-inducing (MCF) virus-accelerated leukemia. Three stages of leukemogenesis were defined before appearance of frankly leukemic mice. Stage 1, apparent 28-40 d after injection of MCF 69L1 virus, represented steady-state infection of thymocytes by MCF virus without apparent change in light scatter properties of the cells or in expression of alloantigens Thy-1, Lyt-1, Lyt-2, L3T4a, B2A2, or H-2K on the major thymocyte subpopulations. Expression of MCF virus was highest in the population of small cortical thymocytes. Stage II was observed at highest frequency 50-60 d postinjection and represented the emergence of a clonal population of cells with transformed properties which could be resolved from normal thymocytes by light scatter and expression of B2A2, H-2K, and gp70 antigens. Stage III was observed at highest frequency at 70 d postinjection, when considerable enlargement of thymus had occurred, and appeared to represent the outgrowth of fully transformed cells that replaced the normal thymocyte subpopulations. The alloantigen phenotype of blast cells from frankly leukemic mice did not differ qualitatively from that of stage II or stage III cells but displayed considerable heterogeneity with respect to quantitative expression of alloantigens and gp70. At least two populations of leukemic blasts could be resolved in the majority of primary thymomas analyzed. It is unclear whether these populations represent the outgrowth of independent clones of transformed cells or if they are related in some way. Our data are consistent with MCF virus-induced transformation of cells in the lineage to small peanut agglutinin-positive, cortisone-sensitive thymocytes, a subpopulation that predominates in the thymus and which is thought to be destined for cell death in situ.
机译:流式细胞术技术涉及荧光和光散射的相关双参数分析,以及移植生物测定法用于描述水貂细胞聚焦诱导(MCF)病毒发育过程中年轻(1-4个月大)AKR小鼠胸腺的一系列细胞变化-加速白血病。坦白的白血病小鼠出现之前,定义了白血病发生的三个阶段。注射MCF 69L1病毒后28-40 d出现的第1阶段代表MCF病毒对胸腺细胞的稳态感染,而细胞的光散射特性或同种抗原Thy-1,Lyt-1,Lyt-的表达没有明显变化。 2,主要胸腺细胞亚群上的L3T4a,B2A2或H-2K。 MCF病毒的表达在小皮质胸腺细胞群中最高。在注射后50-60 d的最高频率观察到第二阶段,该阶段代表了具有转化特性的克隆细胞的出现,这些克隆特性可以通过光散射和B2A2,H-2K和gp70抗原的表达从正常胸腺细胞中分离出来。注射后70 d最高频率观察到III期,这时胸腺发生了相当大的扩展,似乎代表了完全转化的细胞替代正常胸腺细胞亚群的生长。坦白的白血病小鼠原始细胞的同种异体抗原表型与II期或III期细胞在质上没有差异,但在同种抗原和gp70的定量表达方面显示出相当大的异质性。在分析的大多数原发性胸腺瘤中,至少有两个白血病母细胞群可以解决。目前尚不清楚这些群体是否代表转化细胞独立克隆的产物或它们是否以某种方式相关。我们的数据与MCF病毒诱导的谱系向小花生凝集素阳性,可的松敏感胸腺细胞的转化一致,后者是在胸腺中占主导地位的亚群,被认为是原位死亡的细胞。

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