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1.
Silver J  Russell WA 《Nature》1979,279(5712):437-439
THE generation of immune responses in mice is influenced by Ir genes located in the I region of the major histocompatibility complex (MHC)(1). In some instances maximum responses require complementation by two genes, one in the I-A or I-B and the other in the I-E or I-C subregion(2,3). The effects of these genes are thought to be mediated by Ia alloantigens, which are cell surface molecules whose expression is controlled by the I region(4). This is based on the observations that anti-Ia sera inhibit in vitro immune responses(5,6), and soluble factors that enhance in vitro immune responses express Ia alloantigenic determinants(7,9). Jones et al.(10), using two-dimensional gel electrophoresis, observed that the expression of I-E subregion antigens is controlled by two genes, one in the I-A subregion, the other in the I-E subregion, and that the polymorphism of these antigens is influenced by an I-A subregion gene. As an explanation, the authors proposed that only one of the two polypeptide chains present in I-E immunoprecipitates is an I-E subregion product, the second being a product of the I-A subregion. Antisera obtained by cross-immunisation of I-E subregion-disparate strains of mice immunoprecipitates a molecular complex consisting of two chains, designated alpha and beta, with molecular weights of 32,000 and 29,000 respectively(11-14). Previous studies suggested that I-E antigens isolated from B10.A(5R) and B10.D2 mice had identical alpha-chains but different (beta)-chains(15). However, as these mice differed at multiple genetic regions, it was not possible to show which I subregion(s) determined the polymorphism of the E(beta) chain. Therefore, we investigated the effects of the I-A subregion on the polymorphism of I-E subregion antigens. We have now shown by peptide mapping that the I-E subregion polymorphism which Jones et al. found to be controlled by the I-A subregion probably reflects structural polymorphism of beta-chains controlled by an I-A subregion gene.  相似文献   

2.
Epidermal Langerhans cells express Ia antigens.   总被引:40,自引:0,他引:40  
L Klareskog  U Tjernlund  U Forsum  P A Peterson 《Nature》1977,268(5617):248-250
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Occurrence of Ia antigens on tissues on non-lymphoid origin.   总被引:7,自引:0,他引:7  
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Human Ia antigens are polymorphic cell-surface sialoglycoproteins which have restricted tissue distribution. They are bimolecular complexes of 34,000 (alpha) and 28,000 (beta) molecular weight and most of the polymorphism is found in the smaller polypeptides. They are involved in the initiation of immune responses and particular Ia antigens are associated with increased susceptibility to certain diseases. They are also the major barrier to human allogeneic tissue transplantation. Whereas serological analysis and mixed lymphocyte typing have defined three polymorphic families of Ia antigens, HLA-DR, -DC and -SB, protein sequencing results and studies with monoclonal antibodies indicate that the complexity is much greater. Thus the HLA-DR and DC specificities as defined by alloantisera, could represent groups of antigens which are controlled by HLA genes in linkage disequilibrium. Here, we have used a monoclonal antibody specific for HLA-DR2 to show that this determinant is carried by molecules which are distinct from those of the DC series and which represent 30% of the Ia antigens expressed on the cell surface of an HLA homozygous line PGF.  相似文献   

7.
E P Reich  R S Sherwin  O Kanagawa  C A Janeway 《Nature》1989,341(6240):326-328
Insulin-dependent diabetes mellitus is widely believed to be an autoimmune disease. Recent onset diabetics show destruction of insulin-secreting pancreatic beta-cells associated with a lymphocytic infiltrate (insulitis), with autoantibodies to beta-cells being found even before the onset of symptoms. Susceptibility to the disease is strongly influenced by major histocompatibility complex (MHC) class II polymorphism in both man and experimental animal models such as the non-obese diabetic (NOD) mouse. As MHC class II molecules are usually associated with dominant immune responsiveness, it was surprising that introduction of a transgenic class II molecule, I-E, protected NOD mice from insulitis and diabetes. This could be explained by a change either in the target tissue or in the T cells presumed to be involved in beta-cell destruction. Recently, several studies have shown that I-E molecules are associated with ontogenetic deletion of T cells bearing antigen/MHC receptors encoded in part by certain T-cell receptor V beta gene segments. To determine the mechanism of the protective effect of I-E, we have produced cloned CD4+ and CD8+ T-cell lines from islets of recently diabetic NOD mice. These cloned lines are islet-specific and pathogenic in both I-E- and I-E+ mice. Both CD4+ and CD8+ cloned T cells bear receptors encoded by a V beta 5 gene segment, known to be deleted during development in I-E expressing mice. Our data provide, therefore, an explanation for the puzzling effect of I-E on susceptibility to diabetes in NOD mice.  相似文献   

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Ia antigens are membrane-bound glycoproteins that play a part in antigen recognition and subsequent cell-cell interactions in the immune response. In the mouse they are coded for by the I region of the major histocompatibility complex H-2 and have been demonstrated on B lymphocytes, monocytes, activated T cells, macrophages and dendritic cells, including Langerhans cells. Ia-like antigens have also been detected on the vascular endothelium in man and on epidermal keratinocytes in rats but expression on the latter cells was induced by a graft-versus-host reaction or by contact hypersensitivity. In the mouse, previous studies have suggested that Ia antigens in skin are restricted to epidermal Langerhans cells and it was thought that these were the targets for Ia-dependent rejection of skin allografts. The results presented here show that Ia antigens in mouse allografts are also present on the vascular endothelium but their expression is variable and dependent on the immunological status of the recipient. These findings suggest that vascular endothelial cells can act as targets in Ia-incompatible skin allograft rejection.  相似文献   

12.
Membrane antigens of murine leukaemia cells   总被引:1,自引:0,他引:1  
J Cerny  M Essex 《Nature》1974,251(5477):742-745
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S Wu  T L Saunders  F H Bach 《Nature》1986,324(6098):676-679
Class II molecules encoded by the human major histocompatibility complex (MHC) are involved in regulating T-cell response to antigens. The mechanisms for generating polymorphism in products of the MHC have been studied extensively for both the murine H-2 and the human HLA complex. Such studies indicate that point mutations plus selection have a major role in the generation of polymorphisms of class I and class II MHC genes. However, a non-reciprocal gene conversion mechanism has been proposed to explain several examples of clustered sequence variation in MHC genes. In all these examples, the proposed gene conversion event is unidirectional; that is, one of the two interacting genes acts as sequence donor and the other as sequence recipient. No examples of potential reciprocal genetic exchange (as occurs in the fungal system), in which the two interacting genes act as both donor and recipient of gene fragments, have been found in the MHC system or in other multigene families of higher organisms. We sequenced two different HLA-DR beta complementary DNAs from each of two different cells all expressing the same serologically defined determinant (DR2) but different T-cell-recognized (Dw) specificities (Dw12 and MN2). Sequence comparisons of these four cDNA clones (and two DR beta amino-acid sequences from the DR2-Dw2 subtype) suggest that new coding sequences for DR beta molecules in the DR2 haplotypes are potentially generated by reciprocal intergenic exchange.  相似文献   

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TC4钛合金在航空航天工业中有着广泛的应用,热塑性加工中的微观组织演变对其使用性能具有重要的影响。该文通过热-力实验分析,得到TC4合金的加工图,并将加工图信息集成在有限元分析中,对板材轧制工艺进行分析。对TC4钛合金进行等温单向压缩实验获得了材料的流动应力,变形温度为800~1 050℃,应变速率为0.01~20s-1。采用动态材料模型(dynamic material model,DMM)绘制出TC4钛合金的加工图,并通过对压缩的微观组织检查分析验证了加工图的有效性。由加工图可知,在1 000~1 050℃应变速率0.01s-1的区域稳定性最好,为超塑性成形区域,在800~900℃应变速率0.1~20s-1的条件不利于塑性加工,应当避免在此区域加工。通过二次开发,将加工图的信息作为有限元程序DEFORM-2D的后处理变量在成形件中显示,从而直观地显示板材轧制变形不同位置的成形性能。在TC4轧制过程中,板坯基本处于功率耗散效率较高的安全区,有利于材料塑性成形。  相似文献   

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利用地形图生成高程数据方法研究   总被引:1,自引:0,他引:1  
张伟  张春华 《长春大学学报》2005,15(2):33-34,79
论述了从地形图中提取等高线、对等高线矢量化以及通过矢量数据生成高程数据的实现方法。在等高线的矢量化过程中,可根据实际需要对采样密度进行控制。实践表明该方法获得了比较满意的效果,在仿真领域中得到了广泛应用。  相似文献   

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地理信息系统是一门介于地理科学与信息科学之间的交叉学科,已被广泛地应用于许多领域,越来越多的信息系统中需要集成地图的一些功能 本文探讨的就是如何利用VB6. 0对MapInfo7. 0进行编程,将MapInfo7. 0地图窗口集成在VB6. 0开发的应用程序中  相似文献   

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