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利妥昔单抗(嵌合抗CD20抗体)的同型二聚体而非单体可诱导人B淋巴瘤细胞凋亡,并与化疗药物和免疫毒素协同作用。

Homodimers but not monomers of Rituxan (chimeric anti-CD20) induce apoptosis in human B-lymphoma cells and synergize with a chemotherapeutic agent and an immunotoxin.

作者信息

Ghetie M A, Bright H, Vitetta E S

机构信息

Cancer Immunobiology Center, University of Texas Southwestern Medical Center at Dallas, TX 75390-8576, USA.

出版信息

Blood. 2001 Mar 1;97(5):1392-8. doi: 10.1182/blood.v97.5.1392.

Abstract

In 1997, a chimeric anti-CD20 monoclonal antibody (mAb) (Rituxan) was approved for the treatment of low-grade/follicular B-cell lymphoma. Rituxan has a long half-life and low immunogenicity, and it mediates effector function. Rituxan induces apoptosis in some tumor cell lines in vitro. Previous studies with mAbs that react with neoplastic B cells have demonstrated that homodimers of immunoglobulin G (IgG) often inhibit cell growth more effectively than their monomeric (IgG)(1) counterparts. In this study, the ability of IgG or F(ab')(2) homodimers vs monomers of Rituxan were compared for their ability to inhibit the growth of several different B-lymphoma cell lines in vitro. It was found that homodimers of Rituxan had superior antigrowth activity in vitro and that F(ab')(2) homodimers were the most active. Homodimers, but not monomers, of Rituxan induced both apoptosis and necrosis of several B-cell lymphoma lines in vitro; the inhibition of cell growth was not dependent upon the presence of Fc receptors or upon 10-fold or greater differences in the density of CD20 on the target cells. Rituxan homodimers, compared with monomers, also rendered drug-resistant CD20(+) B-lymphoma cells more sensitive to chemotherapeutic agents and synergized with an anti-CD22 immunotoxin in vitro.

摘要

1997年,一种嵌合抗CD20单克隆抗体(mAb)(利妥昔单抗)被批准用于治疗低度/滤泡性B细胞淋巴瘤。利妥昔单抗半衰期长且免疫原性低,并介导效应功能。利妥昔单抗在体外可诱导某些肿瘤细胞系发生凋亡。先前针对与肿瘤性B细胞反应的单克隆抗体的研究表明,免疫球蛋白G(IgG)的同二聚体通常比其单体(IgG)(1)对应物更有效地抑制细胞生长。在本研究中,比较了利妥昔单抗的IgG或F(ab')(2)同二聚体与单体在体外抑制几种不同B淋巴瘤细胞系生长的能力。结果发现,利妥昔单抗的同二聚体在体外具有更强的抗生长活性,且F(ab')(2)同二聚体活性最强。利妥昔单抗的同二聚体而非单体在体外可诱导几种B细胞淋巴瘤系发生凋亡和坏死;细胞生长的抑制不依赖于Fc受体的存在,也不依赖于靶细胞上CD20密度10倍或更大的差异。与单体相比,利妥昔单抗同二聚体还使耐药的CD20(+) B淋巴瘤细胞对化疗药物更敏感,并在体外与抗CD22免疫毒素协同作用。

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