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Synthetic peptides as antigens and competitors in recognition by H-2-restricted cytolytic T cells specific for HLA.合成肽作为被H-2限制的、针对HLA的溶细胞性T细胞识别中的抗原和竞争者。
J Exp Med. 1988 Apr 1;167(4):1391-405. doi: 10.1084/jem.167.4.1391.
2
H2-restricted recognition of cloned HLA class I gene products expressed in mouse cells.对在小鼠细胞中表达的克隆化HLA I类基因产物的H2限制性识别。
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3
Mapping of HLA epitopes recognized by H-2-restricted cytotoxic T lymphocytes specific for HLA using recombinant genes and synthetic peptides.利用重组基因和合成肽对由H-2限制的、针对HLA的细胞毒性T淋巴细胞所识别的HLA表位进行定位。
J Immunol. 1988 Feb 1;140(3):871-7.
4
Two epitopes and one agretope map to a single HLA-A2 peptide recognized by H-2-restricted T cells.两个表位和一个辅佐位映射到一个由H-2限制性T细胞识别的单一HLA - A2肽段上。
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H-2-restricted cytolytic T lymphocytes specific for HLA display T cell receptors of limited diversity.对HLA具有特异性的H - 2限制性细胞溶解T淋巴细胞表现出有限多样性的T细胞受体。
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Cross-recognition of a mouse H-2-peptide complex by human HLA-restricted cytotoxic T cells.人HLA限制的细胞毒性T细胞对小鼠H-2-肽复合物的交叉识别。
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Specific lysis of murine cells expressing HLA molecules by allospecific human and murine H-2-restricted anti-HLA T killer lymphocytes.同种特异性人和鼠的H-2限制性抗HLA T杀伤淋巴细胞对表达HLA分子的鼠细胞的特异性裂解作用。
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Induction of CTL in vivo by major histocompatibility complex class I-peptide complexes covalently associated on the cell surface.通过与细胞表面共价结合的主要组织相容性复合体I类-肽复合物在体内诱导细胞毒性T淋巴细胞。
Eur J Immunol. 1995 Jun;25(6):1535-40. doi: 10.1002/eji.1830250610.

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Induction in transgenic mice of HLA-A2.1-restricted cytotoxic T cells specific for a peptide sequence from a mutated p21ras protein.在转基因小鼠中诱导产生针对突变型p21ras蛋白肽序列的HLA - A2.1限制性细胞毒性T细胞。
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An anti-CD19 antibody coupled to a tetanus toxin peptide induces efficient Fas ligand (FasL)-mediated cytotoxicity of a transformed human B cell line by specific CD4+ T cells.一种与破伤风毒素肽偶联的抗CD19抗体可诱导特异性CD4 + T细胞对转化的人B细胞系产生高效的Fas配体(FasL)介导的细胞毒性。
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T cell receptor selection by and recognition of two class I major histocompatibility complex-restricted antigenic peptides that differ at a single position.T细胞受体对两个在单个位置上不同的I类主要组织相容性复合体限制抗原肽的选择与识别。
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Peptide-major histocompatibility complex class II complexes with mixed agonist/antagonist properties provide evidence for ligand-related differences in T cell receptor-dependent intracellular signaling.具有混合激动剂/拮抗剂特性的肽-主要组织相容性复合体II类复合物为T细胞受体依赖性细胞内信号传导中配体相关差异提供了证据。
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T cells sensitized to synthetic HLA-DR3 peptide give evidence of continuous presentation of denatured HLA-DR3 molecules by HLA-DP.对合成的HLA - DR3肽致敏的T细胞显示出HLA - DP持续呈递变性HLA - DR3分子的证据。
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Mouse cytotoxic T cells can recognize HLA-B27 antigen without H-2 restriction.小鼠细胞毒性T细胞可识别HLA - B27抗原,且不受H - 2限制。
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7
Structural requirements for class I MHC molecule-mediated antigen presentation and cytotoxic T cell recognition of an immunodominant determinant of the human immunodeficiency virus envelope protein.I类主要组织相容性复合体(MHC)分子介导的抗原呈递及细胞毒性T细胞对人类免疫缺陷病毒包膜蛋白免疫显性决定簇识别的结构要求
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8
Identification of residues necessary for clonally specific recognition of a cytotoxic T cell determinant.鉴定细胞毒性T细胞决定簇克隆特异性识别所必需的残基。
EMBO J. 1989 Aug;8(8):2321-8. doi: 10.1002/j.1460-2075.1989.tb08359.x.
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Influenza-specific cytotoxic T-cell recognition is inhibited by peptides unrelated in both sequence and MHC restriction.流感特异性细胞毒性T细胞识别受到序列和MHC限制均不相关的肽的抑制。
Immunology. 1989 Feb;66(2):163-9.
10
Recognition of oligonucleotide-encoded T cell epitopes introduced into a gene unrelated to the original antigen.对引入与原始抗原无关基因中的寡核苷酸编码T细胞表位的识别。
J Exp Med. 1989 Jan 1;169(1):297-302. doi: 10.1084/jem.169.1.297.

本文引用的文献

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Antigen recognition by H-2-restricted T cells. II. A tryptic ovalbumin peptide that substitutes for processed antigen.H-2 限制性 T 细胞的抗原识别。II. 一种替代加工抗原的胰蛋白酶消化卵清蛋白肽。
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The influenza A virus nucleoprotein gene controls the induction of both subtype specific and cross-reactive cytotoxic T cells.甲型流感病毒核蛋白基因控制亚型特异性和交叉反应性细胞毒性T细胞的诱导。
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Fine specificity of genetic regulation of guinea pig T lymphocyte responses to angiotensin II and related peptides.豚鼠T淋巴细胞对血管紧张素II及相关肽反应的遗传调控的精细特异性
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Generation of cytotoxic T lymphocytes in vitro. I. Response of normal and immune mouse spleen cells in mixed leukocyte cultures.体外细胞毒性T淋巴细胞的产生。I. 混合白细胞培养中正常和免疫小鼠脾细胞的反应。
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10
H-2-restricted cytolytic T cells specific for HLA can recognize a synthetic HLA peptide.对HLA具有特异性的H-2限制性细胞溶解T细胞能够识别一种合成的HLA肽。
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合成肽作为被H-2限制的、针对HLA的溶细胞性T细胞识别中的抗原和竞争者。

Synthetic peptides as antigens and competitors in recognition by H-2-restricted cytolytic T cells specific for HLA.

作者信息

Maryanski J L, Pala P, Cerottini J C, Corradin G

机构信息

Ludwig Institute for Cancer Research, Lausanne Branch, Switzerland.

出版信息

J Exp Med. 1988 Apr 1;167(4):1391-405. doi: 10.1084/jem.167.4.1391.

DOI:10.1084/jem.167.4.1391
PMID:3128632
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2188917/
Abstract

The specificity of peptide recognition by a number of Kd-restricted CTL clones specific for HLA-CW3 or HLA-A24 was investigated. The CTL clones were derived from DBA/2 (H-2d) mice immunized with syngeneic P815 mouse cells transfected with genes encoding HLA-CW3 or HLA-A24 class I molecules. We had previously shown that CTL clones that lysed P815-CW3 transfectant target cells could lyse P815 (HLA-) target cells incubated with synthetic CW3 peptides corresponding to the COOH-terminal end of the alpha 2 domain. In the present study, we found that Kd-restricted CTL clones that lysed P815-A24 transfectant target cells recognized a synthetic peptide from the same region (residues 170-182) of the A24 molecule. CW3 and A24 differ by only one amino acid within this region. Recognition of CW3 or A24 peptides corresponded exactly with lysis of P815-HLA transfectants both for clones that mutually exclusively lysed CW3 or A24 transfectant target cells and for CW3/A24 crossreactive CTL clones. The latter CTL clones that lysed both CW3 and A24 transfectant target cells showed a clear preference for the peptide corresponding to the immunizing HLA allele. The homologous CW3 and A24 peptides could compete with each other for recognition, in contrast to a peptide from the same region of HLA-B7. Peptides from the corresponding region of the endogenous Kd and Dd/Ld molecules could also inhibit recognition of CW3 and A24 peptides. Competition with peptides apparently occurred at the level of the target cell. These results are consistent with a model whereby MHC class I molecules position protein fragments or peptides for specific recognition by T cells.

摘要

我们研究了多个对HLA - CW3或HLA - A24具有Kd限制的CTL克隆对肽的识别特异性。这些CTL克隆源自用编码HLA - CW3或HLA - A24 I类分子的基因转染的同基因P815小鼠细胞免疫的DBA/2(H - 2d)小鼠。我们之前已经表明,能够裂解P815 - CW3转染靶细胞的CTL克隆可以裂解与α2结构域COOH末端对应的合成CW3肽孵育的P815(HLA - )靶细胞。在本研究中,我们发现能够裂解P815 - A24转染靶细胞的Kd限制的CTL克隆识别来自A24分子相同区域(第170 - 182位氨基酸)的合成肽。CW3和A24在该区域仅相差一个氨基酸。对于相互排斥地裂解CW3或A24转染靶细胞的克隆以及CW3/A24交叉反应性CTL克隆,对CW3或A24肽的识别与P815 - HLA转染细胞的裂解完全对应。后者能够裂解CW3和A24转染靶细胞的CTL克隆对与免疫的HLA等位基因对应的肽表现出明显的偏好。与来自HLA - B7相同区域的肽相反,同源的CW3和A24肽可以相互竞争识别。来自内源性Kd和Dd/Ld分子相应区域的肽也可以抑制对CW3和A24肽的识别。与肽的竞争显然发生在靶细胞水平。这些结果与一种模型一致,即MHC I类分子将蛋白质片段或肽定位以供T细胞特异性识别。