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AKR小鼠中貂细胞融合诱导(MCF)病毒加速白血病的发展阶段。

Stages in development of mink cell focus-inducing (MCF) virus-accelerated leukemia in AKR mice.

作者信息

O'Donnell P V, Woller R, Chu A

出版信息

J Exp Med. 1984 Sep 1;160(3):914-34. doi: 10.1084/jem.160.3.914.

Abstract

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.

摘要

运用涉及荧光与光散射相关双参数分析的流式细胞术以及移植生物测定法,来描述年轻(1 - 4月龄)AKR小鼠在水貂细胞灶诱导(MCF)病毒加速白血病发展过程中胸腺内一系列细胞变化。在明显患白血病的小鼠出现之前,定义了白血病发生的三个阶段。阶段1,在注射MCF 69L1病毒后28 - 40天出现,表现为MCF病毒对胸腺细胞的稳态感染,细胞的光散射特性以及主要胸腺细胞亚群上的同种异体抗原Thy - 1、Lyt - 1、Lyt - 2、L3T4a、B2A2或H - 2K的表达均无明显变化。MCF病毒在小皮质胸腺细胞群体中的表达最高。阶段II在注射后50 - 60天出现频率最高,代表具有转化特性的克隆细胞群体的出现,这些细胞可通过光散射以及B2A2、H - 2K和gp70抗原的表达与正常胸腺细胞区分开来。阶段III在注射后70天出现频率最高,此时胸腺已明显增大,似乎代表完全转化细胞的增殖,这些细胞取代了正常胸腺细胞亚群。明显患白血病小鼠的原始细胞的同种异体抗原表型在质量上与阶段II或阶段III细胞并无差异,但在同种异体抗原和gp70的定量表达方面表现出相当大的异质性。在分析的大多数原发性胸腺瘤中,至少可以区分出两个白血病原始细胞群体。尚不清楚这些群体是代表转化细胞独立克隆的增殖,还是它们在某种程度上相关。我们的数据与MCF病毒诱导向小花生凝集素阳性且对可的松敏感的胸腺细胞谱系中的细胞发生转化一致,该亚群在胸腺中占主导地位,并且被认为注定会在原位发生细胞死亡。

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