首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Growth of SJL/J-derived transplantable reticulum cell sarcoma as related to its ability to induce T-cell proliferation in the host. I. Dominant negative genetic influences of other parent haplotype in F1 hybrids of SJL/J mice
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Growth of SJL/J-derived transplantable reticulum cell sarcoma as related to its ability to induce T-cell proliferation in the host. I. Dominant negative genetic influences of other parent haplotype in F1 hybrids of SJL/J mice

机译:SJL / J来源的可移植网状细胞肉瘤的生长与其在宿主中诱导T细胞增殖的能力有关。 I. SJL / J小鼠F1杂种中其他亲本单倍型的显性负遗传影响

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摘要

Growth of three transplantable reticulum cell sarcomas (RCS) was studied in a variety of F1 hybrids of SJL/J mice by determination of lymph node (LN) and spleen: body weights ratios 7 and 14 d after intravenous injection of RCS cells. Comparison of BIO.S x SJL and A.SW x SJL with SJL/J showed a negative effect of both the A and the BIO non- H-2 genes, particularly on growth in LN. F1 hybrid resistance was noted with F1 hybrids that carried H-2Dd and was much more evident with F1 hybrids from BIO- than from A-background mice. This resistance was less marked at 14 than at 7 d and was partially overcome by injection of higher tumor doses. Changing the I region in the F1 parent from H-2d to H-2b or H-2f had no effect on growth, but changing to H-2k or H-2d virtually abolished the ability to support tumor growth. This effect appeared partially as a result of the I-E/C and partially of the I-A(B) region and was not overcome by higher tumor dose or longer intervals after injection. There also appeared to be a negative influence on growth of H-2Kk, but this was difficult to differentiate from the I-Ak effect with the available strains. The known proliferative responsiveness that SJL/J Lyt-1 T cells exhibit to Ia determinants on gamma-irradiated RCS cells in vitro was also compared with that of cells from various F1 hybrids. Responsiveness of F1 LN cells was expressed as a percentage of the response in SJL/J LN cells to the same RCS cells, measured as [3H]thymidine incorporation. There was a striking degree of correlation between proliferative responsiveness of F1 LN cells to RCS and the ability of the F1 mice to support tumor growth. This correlation was especially clear with respect to the negative influences of non-H-2 genes, and of H-2 loci in the I region, particularly of I-Ak or -d and of I-E/Ck or -d, but there also appeared to be a (smaller) negative effect of I-Ab or -f. Negative influence of H-2Dd on growth, however, was not reflected in a similarly large effect on the proliferative response. Additional findings showed that LN cells from all F1 hybrids exhibited equivalent syngeneic mixed lymphocyte responses in the presence of polyethylene glycol to mitomycin-treated spleen cells from both the SJL/J and the other parent. The extra high response of F1 cells to RCS cells, as compared with SJL spleen cells, however, was always absent when Ik or -d was contributed by one of the F1 parents. The results suggest a promoting effect of the proliferative response on RCS growth in vivo and, furthermore, an interesting effect of I-A and I-E/C genes, possibly via an interaction product, on the ability of LN cells to be stimulated by Ia determinants on RCS cells.
机译:通过测定RCS细胞静脉注射后的淋巴结(LN)和脾脏,体重比分别为7和14 d,在SJL / J小鼠的各种F1杂种中研究了三种可移植网状细胞肉瘤(RCS)的生长。 BIO.S x SJL和A.SW x SJL与SJL / J的比较显示A和BIO non-H-2基因均具有负面影响,特别是对LN的生长。携带H-2Dd的F1杂种表现出F1杂种抗性,并且BIO-的F1杂种比A背景小鼠的F1杂种更明显。这种抗药性在14时没有7 d时明显,并且通过注射更高剂量的肿瘤可部分克服。将F1亲本中的I区从H-2d更改为H-2b或H-2f对生长没有影响,但更改为H-2k或H-2d实际上消除了支持肿瘤生长的能力。这种作用部分是由于I-E / C引起的,部分是由于I-A(B)区域引起的,而注射后更高的肿瘤剂量或更长的间隔并不能克服这种作用。似乎对H-2Kk的生长也有负面影响,但是很难与可用菌株的I-Ak效应区分开。还比较了SJL / J Lyt-1 T细胞在体外对经γ射线辐照的RCS细胞上的Ia决定簇表现出的增殖反应性,并将其与来自各种F1杂种的细胞的增殖反应性进行了比较。 F1 LN细胞的反应性表示为SJL / J LN细胞对相同RCS细胞反应的百分比,以[3H]胸苷的掺入量来衡量。 F1 LN细胞对RCS的增殖反应性与F1小鼠支持肿瘤生长的能力之间存在显着的相关性。关于非H-2基因和I区H-2基因座,尤其是I-Ak或-d和IE / Ck或-d的负面影响,这种相关性特别明显。似乎是I-Ab或-f的(较小)负面影响。但是,H-2Dd对生长的负面影响并未反映在对增殖反应的类似较大影响中。其他发现表明,在聚乙二醇存在下,来自所有F1杂种的LN细胞对来自SJL / J和另一亲本的丝裂霉素处理的脾细胞均表现出同等的混合淋巴细胞反应。与SJL脾细胞相比,F1细胞对RCS细胞的超高反应在Fk亲代之一促成Ik或-d时总是不存在。结果表明增殖反应对体内RCS生长有促进作用,此外,IA和IE / C基因可能通过相互作用产物对LN细胞受到Ia决定簇刺激RN的能力产生了有趣的作用。细胞。

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