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由正常的、HIV-1阴性供体产生的、对HIV-1包膜糖蛋白gp120具有特异性的人源单克隆抗体。

Human MoAbs produced from normal, HIV-1-negative donors and specific for glycoprotein gp120 of the HIV-1 envelope.

作者信息

Ohlin M, Hinkula J, Broliden P A, Grunow R, Borrebaeck C A, Wahren B

机构信息

Department of Immunotechnology, Lund University, Sweden.

出版信息

Clin Exp Immunol. 1992 Aug;89(2):290-5. doi: 10.1111/j.1365-2249.1992.tb06947.x.

Abstract

Human MoAbs of IgM class were developed against three regions of the HIV-1 envelope. Uninfected donor lymphocytes were immunized in vitro with recombinant protein pB1. Four out of five antibodies were directed to different parts of the V3 region, which contains a major neutralizing site. Two out of these antibodies were directed to more than one amino acid sequence, indicating reactivity to discontinuous sites. Two of the human MoAbs inhibited viral spread between cells in tissue culture, interpreted as reactivities to conserved amino acid sequences exposed during viral maturation. No MoAb neutralized virus, which may be explained by the relatively low avidity of the antibodies. One MoAb was directed to a region containing amino acids participating in CD4 binding. This technique appears to allow formation of antibodies with fine specificities other than those obtained in infected hosts.

摘要

针对HIV-1包膜的三个区域开发了IgM类人单克隆抗体。未感染的供体淋巴细胞在体外用人重组蛋白pB1进行免疫。五分之四的抗体针对V3区域的不同部分,该区域包含一个主要的中和位点。其中两种抗体针对不止一个氨基酸序列,表明对不连续位点有反应性。两种人单克隆抗体抑制了组织培养中病毒在细胞间的传播,这被解释为对病毒成熟过程中暴露的保守氨基酸序列有反应性。没有单克隆抗体中和病毒,这可能是由于抗体的亲和力相对较低。一种单克隆抗体针对一个包含参与CD4结合的氨基酸的区域。这项技术似乎能够形成具有不同于在感染宿主中获得的精细特异性的抗体。

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