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造血组织相容性抗原在F1杂交淋巴瘤细胞的H-2缺失变异体上的表达:与转基因调控一致的证据。

Expression of hemopoietic histocompatibility antigens on H-2-loss variants of F1 hybrid lymphoma cells: evidence consistent with trans gene regulation.

作者信息

Rembecki R M, Bennett M, Kumar V, Potter T A

出版信息

J Immunol. 1987 Apr 15;138(8):2734-8.

PMID:3549904
Abstract

H-2 heterozygous marrow stem cells, lymphoid progenitor cells, and leukemia/lymphoma cells do not express hemopoietic or hybrid histocompatibility (Hh) antigens, which are important transplantation antigens recognized during the rejection of normal or neoplastic hemopoietic cells. The Hh-1b determinant of the H-2b haplotype maps to the D region of H-2. We have tested the hypothesis that gene(s) at or near H-2D of the H-2d haplotype down-regulate the expression of Hh-1b in the trans configuration. We used Abelson leukemia virus-transformed pre-B lymphoma cells (ACCb) of BALB/c X BALB.B (H-2d X H-2b) origin, as well as variant lines of ACCb, which were selected for resistance to monoclonal anti-H-2 antibodies plus complement. B6D2F1 (H-2b X H-2d), C3B6F1 (H-2k X H-2b), or B6 (H-2b) mice were infused with inocula of 5 X 10(6) B6 bone marrow cells (BMC). Proliferation of donor-derived marrow cells was judged in terms of DNA synthesis by measuring the splenic incorporation of 5-iodo(125I)-2'-deoxyuridine (IUdR) 5 days after cell transfer. B6 BMC grew much better in B6 than in F1 hybrid host mice, an expression of "hybrid resistance". As observed previously, the injection of EL-4 (H-2b, Hh-1b) tumor cells prior to infusion of B6 (H-2b, Hh-1b) BMC enhanced the growth of B6 BMC in F1 hybrid mice. Therefore, this in vivo "cold target cell competition" type of assay can be used to detect the expression of Hh-1b antigens. Unlike EL-4 (H-2b) cells, hybrid resistance was not affected by prior infusion of (H-2b X H-2d) heterozygous ACCb cells. In contrast, three ACCb variant cell lines, H-2d-, Ld-Dd-, and Dd-, enhanced the growth of B6 BMC in F1 hosts. The ACCb H-2b- cell line did not affect hybrid resistance to B6 BMC. The loss of gene expression on the H-2d chromosome at or very near the H-2Dd locus is correlated with the appearance Hh-1b, as determined by the in vivo cold target competition assay. These results support the hypothesis that heterozygous cells possess trans-acting, dominant, down-regulatory genes mapping near H-2D that control the Hh-1 phenotype of lymphoid tumor cells.

摘要

H-2杂合骨髓干细胞、淋巴样祖细胞和白血病/淋巴瘤细胞不表达造血或杂种组织相容性(Hh)抗原,而这些抗原是在正常或肿瘤性造血细胞排斥过程中被识别的重要移植抗原。H-2b单倍型的Hh-1b决定簇定位于H-2的D区。我们检验了这样一个假说,即H-2d单倍型的H-2D或其附近的基因在反式构型中下调Hh-1b的表达。我们使用了源自BALB/c×BALB.B(H-2d×H-2b)的艾贝尔逊白血病病毒转化的前B淋巴瘤细胞(ACCb),以及ACCb的变异株,这些变异株是通过对单克隆抗H-2抗体加补体的抗性筛选出来的。给B6D2F1(H-2b×H-2d)、C3B6F1(H-2k×H-2b)或B6(H-2b)小鼠输注5×10⁶个B6骨髓细胞(BMC)接种物。在细胞转移5天后,通过测量脾脏对5-碘(¹²⁵I)-2'-脱氧尿苷(IUdR)的摄取来根据DNA合成判断供体来源骨髓细胞的增殖情况。B6 BMC在B6小鼠中比在F1杂种宿主小鼠中生长得好得多,这是“杂种抗性”的一种表现。如先前观察到的,在输注B6(H-2b,Hh-1b)BMC之前注射EL-4(H-2b,Hh-1b)肿瘤细胞可增强B6 BMC在F1杂种小鼠中的生长。因此,这种体内“冷靶细胞竞争”类型的检测可用于检测Hh-1b抗原的表达。与EL-4(H-2b)细胞不同,杂种抗性不受先前输注(H-2b×H-2d)杂合ACCb细胞的影响。相反,三个ACCb变异细胞系,H-2d-、Ld-Dd-和Dd-,增强了B6 BMC在F1宿主中的生长。ACCb H-2b-细胞系不影响对B6 BMC的杂种抗性。通过体内冷靶竞争检测确定,H-2Dd位点或其非常接近的H-2d染色体上基因表达的缺失与Hh-1b的出现相关。这些结果支持这样的假说,即杂合细胞拥有位于H-2D附近的反式作用、显性、下调基因,这些基因控制淋巴样肿瘤细胞的Hh-1表型。

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