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重组近交系——一种应用于小鼠结肠癌发生发展研究的新型遗传工具。

The recombinant congenic strains--a novel genetic tool applied to the study of colon tumor development in the mouse.

作者信息

Moen C J, van der Valk M A, Snoek M, van Zutphen B F, von Deimling O, Hart A A, Demant P

机构信息

Division of Molecular Genetics, The Netherlands Cancer Institute, Amsterdam.

出版信息

Mamm Genome. 1991;1(4):217-27. doi: 10.1007/BF00352328.

Abstract

The development of tumors in mice is under multigenic control, but, in spite of considerable efforts, the identification of the genes involved has so far been unsuccessful, because of the insufficient resolution power of the available genetic tools. Therefore, a novel genetic tool, the RC (Recombinant Congenic) strains system, was designed. In this system, a series of RC strains is produced from two inbred strains, a "background" strain and a "donor" strain. Each RC strain contains a different small subset of genes from the donor strain and the majority of genes from the background strain. As a consequence, the individual genes of the donor strain which are involved in the genetic control of a multigenic trait, become separated into different RC strains, where they can be identified and studied individually. One of the RC strains series which we produced is made from the parental strains BALB/cHeA (background strain) and STS/A (donor strain). We describe the genetic composition of this BALB/cHeA-C-STS/A (CcS/Dem) series and show, using 45 genetic autosomal markers, that it does not deviate from the theoretical expectation. We studied the usefulness of the CcS/Dem RC strains for analysis of the genetics of colon tumor development. The two parental strains, BALB/cHeA and STS/A, are relatively resistant and highly susceptible, respectively, to the induction of colon tumors by 1,2-dimethylhydrazine (DMH). The individual RC strains differ widely in colon tumor development after DMH treatment; some are highly susceptible, while others are very resistant. This indicates that a limited number of genes with a major effect are responsible for the high susceptibility of the STS strain. Consequently, these genes can be mapped by further analysis of the susceptible RC strains. The differences between the RC strains were not limited to the number of tumors, but the RC strains differed also in size of the tumors and the relative susceptibility of the two sexes. Our data indicate that the number of tumors and the size of tumors are not controlled by the same genes. The genetics of these different aspects of colon tumorigenesis can also be studied by the RC strains. The DMH-treated mice of the parental strains and the RC strains also developed anal tumors and haemangiomas in varying numbers. The strain distribution pattern (SDP) of susceptibility for each of the three types of tumors induced by DMH is different, indicating that development of these tumors is under control of different, largely non-overlapping, sets of genes.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

小鼠肿瘤的发生受多基因控制,然而,尽管付出了巨大努力,但由于现有遗传工具的分辨能力不足,迄今为止,所涉及基因的鉴定仍未成功。因此,设计了一种新型遗传工具——重组近交(RC)系系统。在该系统中,一系列RC系由两个近交系产生,一个是“背景”系,另一个是“供体”系。每个RC系都包含来自供体系的不同小基因子集和来自背景系的大多数基因。因此,供体系中参与多基因性状遗传控制的各个基因,被分离到不同的RC系中,在这些系中它们可以被单独鉴定和研究。我们构建的其中一个RC系系列由亲本系BALB/cHeA(背景系)和STS/A(供体系)培育而成。我们描述了这个BALB/cHeA-C-STS/A(CcS/Dem)系列的遗传组成,并使用45个常染色体遗传标记表明,它并未偏离理论预期。我们研究了CcS/Dem RC系在分析结肠癌发生遗传学方面的实用性。两个亲本系BALB/cHeA和STS/A对1,2 - 二甲基肼(DMH)诱导的结肠癌分别具有相对抗性和高度易感性。经DMH处理后,各个RC系在结肠癌发生方面差异很大;有些系高度易感,而另一些则非常抗性。这表明有限数量的主效基因导致了STS系的高度易感性。因此,通过对易感RC系的进一步分析,可以对这些基因进行定位。RC系之间的差异不仅限于肿瘤数量,而且在肿瘤大小以及两性的相对易感性方面也存在差异。我们的数据表明,肿瘤数量和肿瘤大小并非由相同基因控制。结肠癌发生这些不同方面的遗传学也可以通过RC系进行研究。亲本系和RC系经DMH处理的小鼠还会出现数量不等的肛门肿瘤和血管瘤。DMH诱导的三种肿瘤类型中,每种肿瘤易感性的品系分布模式(SDP)都不同,这表明这些肿瘤的发生受不同的、在很大程度上不重叠的基因集控制。(摘要截选至400字)

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