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Induction of effective cross-reactive immunity by FMDV peptides is critically dependent upon specific MHC-peptide-T cell interactions.

机译:FMDV肽诱导有效的交叉反应性免疫关键取决于特定的MHC-肽-T细胞相互作用。

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摘要

BoCD4+ T-cell clones specific for a peptide derived from foot-and-mouth disease virus envelope protein, VP1 (FMDV15) were generated from two responder cattle. One animal was a high and the other was an intermediate responder in terms of both T-cell and antibody responses. However both animals had identical major histocompatibility complex (MHC) class II DR-like types (DRBF3,6) according to a one-dimensional isoelectric focusing method which distinguishes DR-like alleles. In contrast, mixed lymphocyte reaction (MLR) responses indicated that they shared only one haplotype (DRBF3) and anti-DRBF6 alloclones also differentiated between the animals. This suggested that the animals differed at a non-DR-like locus. Restriction patterns of FMDV-specific clones derived from these animals indicated that FMDV15 was presented by the non-DR-like class II molecules associated with DRBF6. Only one clone, derived from the high responder animal, was restricted to DRBF3. Thus products from the non-DR-like locus (probably DQ-like) are functionally important for presentation of FMDV peptides. Furthermore the allelic differences detected by the alloclones are also critical for peptide binding. The majority of clones from the high responder animal recognized an immunodominant region containing a Rothbard epitope whereas none of the clones from the intermediate responder did so. This suggests that the region recognized by T cells, which is dependent upon MHC type, influences the B-cell response and thus the degree of protection obtained. This has major implications for rational vaccine design involving T- and B-cell epitopes.
机译:对口蹄疫病毒包膜蛋白VP1(FMDV15)衍生的肽具有特异性的BoCD4 + T细胞克隆是从两只有反应的牛身上产生的。就T细胞和抗体反应而言,一只动物是高的,另一只是中等的响应。然而,根据区分DR样等位基因的一维等电聚焦方法,两只动物都具有相同的II型主要组织相容性复合体(MHC)DR样类型(DRBF3,6)。相反,混合淋巴细胞反应(MLR)反应表明它们仅共享一种单倍型(DRBF3),并且抗DRBF6 alloclones也在动物之间分化。这表明动物在非DR样基因座处不同。源自这些动物的FMDV特异性克隆的限制性酶切模式表明FMDV15由与DRBF6相关的非DR类II类分子呈递。仅高反应动物的一个克隆被限制为DRBF3。因此,来自非DR样基因座(可能是DQ样)的产物对于FMDV肽的呈递在功能上很重要。此外,由alloclones检测到的等位基因差异对于肽结合也是关键的。来自高反应性动物的大多数克隆都识别出含有罗斯巴德表位的免疫优势区域,而来自中度响应者的克隆都没有这样做。这表明依赖于MHC类型的T细胞识别的区域会影响B细胞反应,从而影响获得的保护程度。这对涉及T细胞和B细胞表位的合理疫苗设计具有重要意义。

著录项

  • 期刊名称 Immunology
  • 作者

    E J Glass; P Millar;

  • 作者单位
  • 年(卷),期 1994(82),1
  • 年度 1994
  • 页码 1–8
  • 总页数 8
  • 原文格式 PDF
  • 正文语种
  • 中图分类 免疫学;
  • 关键词

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