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在感染的早期和晚期时间点鉴定出的丙型肝炎病毒包膜蛋白E1和E2的免疫显性B细胞结构域。

Immunodominant B-cell domains of hepatitis C virus envelope proteins E1 and E2 identified during early and late time points of infection.

作者信息

Zibert A, Kraas W, Ross R S, Meisel H, Lechner S, Jung G, Roggendorf M

机构信息

Institut für Virologie, Universitätsklinikum Essen, Germany.

出版信息

J Hepatol. 1999 Feb;30(2):177-84. doi: 10.1016/s0168-8278(99)80059-2.

Abstract

BACKGROUND/AIMS: We characterized immunoreactive B-cell domains of hepatitis C virus (HCV) envelope proteins E1 and E2 by a peptide ELISA using sera of patients who were infected by the same isolate of HCV (HCV-AD78).

METHODS

Fifty-four overlapping peptides which corresponded to the sequence of E1 and E2 of isolate HCV-AD78 were used to detect specific antibodies. Three groups of HCV-AD78 related sera were analyzed. Two groups were from sera obtained at early time points of infection (months 4-15) from patients who later resolved infection (group A), or who later developed chronic disease (group B). Group C sera were from later time points of chronic disease. As a control, sera of chronic HCV patients who did not have HCV-AD78 infection were also analyzed (group D).

RESULTS

In group A, 25 of the 54 peptides produced OD405 above the cut-off, whereas 17 peptides produced such values in group B. Only 10 and 3 peptides yielded such values in groups C and D, respectively. The overall prevalence of antibodies against peptides was high in the early phase of infection (means of 28.7+/-14.8% and 25.9+/-14.5% in groups A and B, respectively). At later time points of chronic infection (group C), the overall prevalence was lower (mean 18.6+/-15.4%). Group D sera produced the lowest overall prevalence (mean 13.2+/-14.1%). Three peptides, covering aa271-290, aa481-500 and aa551-570, were recognized significantly more frequently (p<0.05) by group A sera than group B sera.

CONCLUSIONS

We conclude that more linear epitopes of the HCV envelope are recognized with a high prevalence of antibodies, as was suggested previously. However, most B-cell domains of the HCV envelope induce a similarly high antibody response in patients who resolve infection or develop chronic disease.

摘要

背景/目的:我们通过肽酶联免疫吸附测定法,利用感染同一株丙型肝炎病毒(HCV-AD78)患者的血清,对丙型肝炎病毒包膜蛋白E1和E2的免疫反应性B细胞结构域进行了特征分析。

方法

使用54个与HCV-AD78分离株E1和E2序列相对应的重叠肽来检测特异性抗体。分析了三组与HCV-AD78相关的血清。两组来自感染早期(4-15个月)患者的血清,这些患者后来感染自行消退(A组),或后来发展为慢性病(B组)。C组血清来自慢性病的后期。作为对照,还分析了未感染HCV-AD78的慢性丙型肝炎患者的血清(D组)。

结果

在A组中,54个肽中有25个产生的OD405高于临界值,而在B组中有17个肽产生这样的值。在C组和D组中,分别只有10个和3个肽产生这样的值。在感染早期,针对肽的抗体总体流行率较高(A组和B组的平均值分别为28.7±14.8%和25.9±14.5%)。在慢性感染的后期(C组),总体流行率较低(平均值为18.6±15.4%)。D组血清产生的总体流行率最低(平均值为13.2±14.1%)。A组血清对覆盖氨基酸271-290、氨基酸481-500和氨基酸551-570的三个肽的识别频率明显高于B组血清(p<0.05)。

结论

我们得出结论,正如之前所表明的,丙型肝炎病毒包膜的更多线性表位被抗体以较高流行率识别。然而,丙型肝炎病毒包膜的大多数B细胞结构域在感染自行消退或发展为慢性病的患者中诱导出类似的高抗体反应。

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