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RECOMBINANT RETROVIRUSES AND LEUKEMOGENESIS IN AKR STRAIN MICE.

机译:AKR应变小鼠的重组逆转录病毒和白血病的发生。

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摘要

A complex pattern of murine leukemia virus (MuLV) expression is associated with the 'spontaneous' development of thymic leukemias in six to nine-month-old AKR strain mice. The AKR mouse genome contains endogenous MuLV proviruses of two major host range preferences, defined by the viral envelope gene products, gp70 and p15E: ecotropic MuLV, which replicate in murine cells, and xenotropic MuLV, which are restricted to heterologous species. Life-long expression of the ecotropic AKV MuLV begins in embryonic AKR mice and ecotropic-nonecotropic envelope gene recombinant MCF MuLV appear in the preleukemic and leukemic AKR thymus. This thesis describes the arrangement and structure of these MuLV proviruses in the AKR germ-line and thymus.; Multiple discrete ecotropic and nonecotropic MuLV specific hybridization probes, which map within and adjacent to the recombinant regions of two MCF viruses, discriminate between endogenous germ-line MuLV populations and show that MCF viruses arise by recombination during ontogeny (Chapter 2). The nucleotide sequence of the AKV envelope gene and surrounding regions (Chapter 3) defines the genetic map of the 3' half of AKV and suggests that the thymotropic host range of oncogenic MCF viruses may be a consequence of the juxtaposition of a nonecotropic gp70 receptor binding activity with an ecotropic p15E virus-cell membrane-fusion activity. Highly inbred AKR strain mice from the Jackson Laboratory (Bar Harbor, Maine) colony had differing numbers of germ-line ecotropic proviruses suggesting germ-line AKV reintegrations had occurred (Chapter 4, Nature 269, 865-868 {lcub}1982{rcub}).; Many recombinant MuLV proviruses, structurally analogous to oncogenic MCF viruses, appear unintegrated in the preleukemic thymus and integrated in the leukemic thymus (Chapters 5 and 6). The proviral ecotropic-nonecotropic recombination patterns are highly variable but in individual thymuses both the free and integrated proviral forms exhibit structural homogeneity. This suggests that the recombination events which create oncogenic MCF viruses are infrequent and may be a rate-limiting step in AKR leukemogenesis. The leukemic-cell population is of clonal cell origin, yet may exhibit multiple rearrangements of the immunoglobulin heavy-chain J segment exons (Chapter 7), suggesting that such rearrangements, which have been observed in T-cell lines, occur after viral transformation.
机译:鼠白血病病毒(MuLV)表达的复杂模式与六至九个月大的AKR株小鼠的胸腺白血病的“自发”发展有关。 AKR小鼠基因组包含两个主要宿主范围偏好的内源性MuLV前病毒,它们由病毒包膜基因产物gp70和p15E定义:在鼠类细胞中复制的嗜生性MuLV和异源性MuLV(仅限于异源物种)。嗜生性AKV MuLV的终生表达始于胚胎AKR小鼠,嗜生性-非嗜性包膜基因重组MCF MuLV出现在白血病前和白血病的AKR胸腺中。本文描述了这些MuLV原病毒在AKR种系和胸腺中的排列和结构。定位在两种MCF病毒的重组区域之内和附近的多个离散的亲热和非嗜性MuLV特异性杂交探针可区分内源种系MuLV群体,并显示MCF病毒是在个体发育过程中通过重组产生的(第2章)。 AKV包膜基因和周围区域的核苷酸序列(第3章)定义了AKV 3'一半的遗传图谱,并表明致癌MCF病毒的促变宿主范围可能是非促同性gp70受体结合的结果嗜酸性p15E病毒细胞膜融合活性。来自杰克逊实验室(缅因州巴港)的高度近交AKR品系小鼠的生殖系亲生态原病毒数量不同,表明发生了生殖系AKV重整合(第4章,自然269,865-868 {lcub} 1982 {rcub} )。在结构上类似于致癌MCF病毒的许多重组MuLV原病毒看起来未整合在白血病前胸腺中,而整合在白血病胸腺中(第5章和第6章)。前病毒的生态亲和非重组形式是高度可变的,但在单个胸腺中,游离和整合的前病毒形式均表现出结构同质性。这表明产生致癌MCF病毒的重组事件是罕见的,并且可能是AKR白血病发生中的限速步骤。白血病细胞群是克隆细胞起源的,但是可能表现出免疫球蛋白重链J节外显子的多重重排(第7章),这表明在病毒转化后发生了这种在T细胞系中观察到的重排。

著录项

  • 作者

    HERR, WINSHIP RICHARD.;

  • 作者单位

    Harvard University.;

  • 授予单位 Harvard University.;
  • 学科 Biology General.
  • 学位 Ph.D.
  • 年度 1982
  • 页码 277 p.
  • 总页数 277
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 普通生物学;
  • 关键词

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