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作为合成免疫原聚合物侧链(聚-L-脯氨酰和聚-DL-丙氨酰)化学性质的函数,不同细胞类型对免疫反应遗传控制的贡献。

Contribution of different cell types to the genetic control of immune responses as a function of the chemical nature of the polymeric side chains (poly-L-prolyl and poly-DL-alanyl) of synthetic immunogens.

作者信息

Shearer G M, Mozes E, Sela M

出版信息

J Exp Med. 1972 May 1;135(5):1009-27. doi: 10.1084/jem.135.5.1009.

Abstract

Genetic regulation of immunological responsiveness was studied at the cellular level by comparing the limiting dilutions of immunocompetent cells from spleen, thymus, and bone marrow of high and low responders as a function of the poly-L-prolyl and poly-DL-alanyl side chains of two synthetic polypeptide immunogens. The spleens of immunized and unimmunized high responder DBA/1 mice were found to contain respectively, 18- and 7-fold more limiting precursor cells specific for (Phe, G)-A--L than the spleens of SJL low responder donors. These results, using a synthetic polypeptide built on multichain poly-DL-alanine, confirm the findings reported for polypeptides built on multichain poly-L-proline (1, 2), that there is a direct correlation between immune response potential and the relative number of immunocompetent precursors stimulated. Cell cooperation between thymocytes and bone marrow cells was demonstrated for both (T, G)-Pro--L and (Phe, G)-A--L. Limiting dilutions of thymus and bone marrow cells in the presence of an excess amount of the complementary cell type indicated an eightfold lower number of detected (T, G)-Pro--L-specific precursors in DBA/1 (low responder) marrow when compared with SJL (high responder) marrow. No differences were observed in the frequency of relevant high and low responder thymocytes for the (T, G)-Pro--L immunogen. These results are similar to those reported for the (Phe, G)-Pro--L (3). In contrast to the cellular studies reported for the Pro--L series of immunogens, the marrow and thymus cell dilution experiments for (Phe, G)-A--L revealed genetically associated differences in both the marrow and thymus populations of immunocytes from high (DBA/1) and low (SJL) responders. In addition to a fivefold difference in limiting marrow cell precursors (similar to that seen in the Pro--L studies), a striking difference was observed between the helper cell activity of high responder DBA/1 and low responder SJL thymocytes. This difference was indicated by the observation that low responder thymocyte dilutions followed the predictions of the Poisson model, whereas dilutions of high responder thymocytes did not conform to Poisson statistics. Transfers of allogeneic thymus and marrow cell mixtures from DBA/1 and SJL donors confirmed the syngeneic dilution studies showing that the genetic defect of immune responsiveness to (Phe, G)-A--L is expressed at both the thymus and marrow immunocompetent cell level. The parameters presently known for genetic control of immune responses specific for (Phe, G) (Ir-1 gene) and for Pro--L (Ir-3 gene) have been compared. The Ir-1 and Ir-3 genes are not only distinct by genetic linkage tests (to H-2) (5, 6, 9), but they are also seen to be different by cellular studies. Furthermore, expression of low responsiveness within a given cell population was shown to depend on the chemical structure of the whole immunogenic macromolecule.

摘要

通过比较高反应者和低反应者脾脏、胸腺和骨髓中免疫活性细胞的极限稀释度,以研究两种合成多肽免疫原的聚-L-脯氨酰和聚-DL-丙氨酰侧链对免疫反应性的遗传调控。发现免疫的和未免疫的高反应性DBA/1小鼠脾脏中,对(苯丙氨酸,甘氨酸)-A-L特异的极限前体细胞分别比SJL低反应性供体的脾脏多18倍和7倍。这些使用基于多链聚-DL-丙氨酸构建的合成多肽的结果,证实了基于多链聚-L-脯氨酸构建的多肽所报道的发现(1,2),即免疫反应潜能与受刺激的免疫活性前体的相对数量之间存在直接相关性。对于(T,甘氨酸)-脯-L和(苯丙氨酸,甘氨酸)-A-L,均证明了胸腺细胞与骨髓细胞之间的细胞协作。在存在过量互补细胞类型的情况下,胸腺细胞和骨髓细胞的极限稀释表明,与SJL(高反应性)骨髓相比,DBA/1(低反应性)骨髓中检测到的(T,甘氨酸)-脯-L特异前体细胞数量低8倍。对于(T,甘氨酸)-脯-L免疫原,高反应性和低反应性胸腺细胞的频率未观察到差异。这些结果与针对(苯丙氨酸,甘氨酸)-脯-L报道的结果相似(3)。与针对脯-L系列免疫原报道的细胞研究相反,(苯丙氨酸,甘氨酸)-A-L的骨髓和胸腺细胞稀释实验揭示了高(DBA/1)反应者和低(SJL)反应者免疫细胞的骨髓和胸腺群体中存在遗传相关差异。除了极限骨髓细胞前体有5倍差异(类似于脯-L研究中所见)外,高反应性DBA/1和低反应性SJL胸腺细胞的辅助细胞活性之间还观察到显著差异。这一差异表现为低反应性胸腺细胞稀释遵循泊松模型的预测,而高反应性胸腺细胞的稀释不符合泊松统计。来自DBA/1和SJL供体的同种异体胸腺和骨髓细胞混合物的转移证实了同基因稀释研究,表明对(苯丙氨酸,甘氨酸)-A-L免疫反应性的遗传缺陷在胸腺和骨髓免疫活性细胞水平均有表达。目前已知的针对(苯丙氨酸,甘氨酸)(Ir-1基因)和脯-L(Ir-3基因)的免疫反应遗传控制参数已进行了比较。Ir-1和Ir-3基因不仅通过遗传连锁试验(与H-2)(5,6,9)不同,而且在细胞研究中也被认为是不同的。此外,给定细胞群体内低反应性的表达显示取决于整个免疫原性大分子的化学结构。

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Thymus-independence of slowly metabolized immunogens.缓慢代谢免疫原的胸腺非依赖性
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The genetic control of antibody specificity.抗体特异性的遗传控制。
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