Human immunodeficiency virus type 1 neutralization epitope with conserved architecture elicits early type-specific antibodies in experimentally infected chimpanzees.

机译：具有保守结构的人免疫缺陷病毒1型中和表位在实验感染的黑猩猩中引发早期类型特异性抗体。

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Chimpanzees are susceptible to infection by divergent strains of human immunodeficiency virus type 1 (HIV-1), none of which cause clinical or immunological abnormalities. Chimpanzees were inoculated with one of four strains of HIV-1: human T-lymphotropic virus (HTLV) type IIIB, lymphadenopathy virus (LAV) type 1, HTLV type IIIRF, or an isolate from the brain of a patient with acquired immunodeficiency syndrome. Within 6 months after inoculation with the closely related strains HTLV-IIIB or LAV-1, six chimpanzees developed serum antibodies to the C-terminal half (amino acids 288-467) of the HTLV-IIIB external envelope glycoprotein gp120. Sera from five of those chimpanzees had HTLV-IIIB cell-fusion-inhibiting antibody titers greater than or equal to 20 at that time, indicating that they neutralized the infecting strain of HIV-1 in vitro. No antibodies to the carboxyl terminus of HTLV-IIIB gp120 were observed in sera of chimpanzees inoculated with HTLV-IIIRF or with the brain-tissue strain, and those sera did not neutralize HTLV-IIIB. A rabbit immunized with the C-terminal portion of gp120 acquired neutralizing antibodies that bound to four domains of the HTLV-IIIB external envelope as analyzed by reactivity to 536 overlapping nonapeptides of gp120. One of these domains in the variable region V3, with the amino acid sequence IRIQRGPGRAFVTIG (amino acids 307-321), bound to all chimpanzee sera that neutralized HTLV-IIIB but not to the serum of the HTLV-IIIRF-inoculated chimpanzee that did not neutralize HTLV-IIIB. The HTLV-IIIRF sequence at the same location, ITKGPGRVIYA, was recognized by the serum of the HTLV-IIIRF-inoculated chimpanzee but not by any sera of the HTLV-IIIB-inoculated or LAV-1-inoculated chimpanzees. The HTLV-IIIB residues RIQR and AFV and the HTLV-IIIRF residues lysine and VIYA, flanking a highly conserved beta-turn (GPGR), appear to be critical for antibody binding and subsequent type-specific virus neutralization. This neutralization epitope, putatively consisting of a loop between two cysteine residues (amino acids 296 and 331) connected by a disulfide bond, is immunodominant in HIV-1-infected chimpanzees and induces antibodies restricted to the homologous viral strain.

机译：黑猩猩很容易被人类免疫缺陷病毒1型（HIV-1）的不同菌株感染，但都不会引起临床或免疫学异常。黑猩猩接种了四种HIV-1病毒株之一：人类T型淋巴病毒（HTLV）IIIB型，淋巴结病病毒（LAV）1型，HTLV IIIRF型或患有获得性免疫缺陷综合征的患者的脑中分离株。在用紧密相关的菌株HTLV-IIIB或LAV-1接种后的6个月内，六只黑猩猩产生了针对HTLV-IIIB外膜糖蛋白gp120的C端一半（氨基酸288-467）的血清抗体。这些黑猩猩中有五只的血清当时具有HTLV-IIIB细胞融合抑制抗体效价大于或等于20，表明它们在体外中和了HIV-1感染株。在接种HTLV-IIIRF或脑组织株的黑猩猩血清中未观察到HTLV-IIIB gp120羧基末端的抗体，并且这些血清未中和HTLV-IIIB。用对gp120的536个重叠非肽的反应性分析，用gp120的C端部分免疫的兔子获得了与HTLV-IIIB外膜的四个域结合的中和抗体。可变区V3中的这些结构域之一，具有氨基酸序列IRIQRGPGRAFVTIG（氨基酸307-321），与中和HTLV-IIIB的所有黑猩猩血清结合，但不与未接种HTLV-IIIRF的黑猩猩的血清结合中和HTLV-IIIB。 HTLV-IIIRF接种的黑猩猩的血清可识别同一位置的HTLV-IIIRF序列ITKGPGRVIYA，但HTLV-IIIB接种或LAV-1接种的黑猩猩的任何血清均无法识别。 HTLV-IIIB残基RIQR和AFV以及HTLV-IIIRF残基赖氨酸和VIYA，侧翼为高度保守的β-转角（GPGR），似乎对于抗体结合和随后的类型特异性病毒中和至关重要。该中和表位推测是由两个通过二硫键连接的半胱氨酸残基（氨基酸296和331）之间的环组成，在HIV-1感染的黑猩猩中具有免疫优势，并诱导仅限于同源病毒株的抗体。

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期刊名称 Proceedings of the National Academy of Sciences of the United States of America
作者
J Goudsmit; C Debouck; R H Meloen; L Smit; M Bakker; D M Asher; A V Wolff; C J Gibbs Jr; D C Gajdusek;
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年(卷),期 1988(85),12
年度 1988
页码 4478–4482
总页数 5
原文格式 PDF
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1. Immunogenic and antigenic dominance of a nonneutralizing epitope over a highly conserved neutralizing epitope in the gp41 envelope glycoprotein of human immunodeficiency virus type 1: its deletion leads to a strong neutralizing response. [J] . Cleveland SM, Buratti E, Jones TD, Virology . 2000,第1期

机译：在人类免疫缺陷病毒1型的gp41包膜糖蛋白中，高度中和的中和表位上非中和的表位具有免疫原性和抗原性优势：将其删除会导致强烈的中和反应。
2. Lipidated L2 epitope repeats fused with a single-chain antibody fragment targeting human Fc gamma RI elicited cross-neutralizing antibodies against a broad spectrum of human papillomavirus types [J] . Zhang Ting, Liu Hongyang, Chen Xue, Vaccine . 2016,第46期

机译：与靶向人FcγRI的单链抗体片段融合的脂化L2表位重复序列引发针对多种人类乳头瘤病毒类型的交叉中和抗体
3. Potent neutralizing antibodies in humans infected with zoonotic simian foamy viruses target conserved epitopes located in the dimorphic domain of the surface envelope protein [J] . Caroline Lambert, Mathilde Couteaudier, Julie Gouzil, PLoS Pathogens . 2018,第10期

机译：感染人畜共患病猿猴泡沫病毒的人中的中和抗体强力靶向位于表面包膜蛋白双态域中的保守表位
4. Identification of Type-Common and Neutralization Epitopes on Hepatitis E Virus Genotype 4 by Using Monoclonal Antibodies [C] . Hongmei Zhang, Xing Dai, Xiangnian Shan, International Forum on Progress on Post-Genome Technologies(5'IFPT); 20070910-11; Suzhou(CN) . 2007

机译：使用单克隆抗体鉴定戊型肝炎病毒基因型4的常见类型和中和表位
5. Epitope-targeting strategy for a vaccine against human immunodeficiency virus type-1: Peptide ligands for the broadly-neutralizing antibodies b12, 2F5 and 2G12. [D] . Menendez, Alfredo. 2005

机译：针对1型人类免疫缺陷病毒的疫苗的表位靶向策略：广泛中和的抗体b12、2F5和2G12的肽配体。
6. Emergence of viruses resistant to neutralization by V3-specific antibodies in experimental human immunodeficiency virus type 1 IIIB infection of chimpanzees. [O] . P L Nara, L Smit, N Dunlop, 1990

机译：在黑猩猩的实验性人类免疫缺陷病毒1型IIIB型感染中出现了对V3特异性抗体具有抗中和作用的病毒。
7. Human immunodeficiency virus type 1 neutralization epitope with conserved architecture elicits early type-specific antibodies in experimentally infected chimpanzees. [O] . Goudsmit, J, Debouck, C, Meloen, R H, 1988

机译：具有保守结构的人免疫缺陷病毒1型中和表位在实验感染的黑猩猩中引发早期类型特异性抗体。

Human immunodeficiency virus type 1 neutralization epitope with conserved architecture elicits early type-specific antibodies in experimentally infected chimpanzees.

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