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使用一组大鼠单克隆抗体对人小细胞肺癌分化抗原进行分析。

Analysis of human small cell lung cancer differentiation antigens using a panel of rat monoclonal antibodies.

作者信息

Rosen S T, Mulshine J L, Cuttitta F, Fedorko J, Carney D N, Gazdar A F, Minna J D

出版信息

Cancer Res. 1984 May;44(5):2052-61.

PMID:6713399
Abstract

The antigen expression of human small cell lung cancer (SCLC) was studied using a panel of 21 independent rat monoclonal antibodies. The panel was selected by isolating hybridomas producing antibodies reactive with two SCLC lines but not with autologous B-lymphoblastoid lines. The antibodies were then tested in radiobinding assays against a panel of 17 SCLC lines, 13 non-small cell lung cancer lines, 6 SCLC necropsy specimens, 13 neuroectodermal lines (melanomas, neuroblastomas, glioblastomas), 15 other human lines, the glycolipid extracts of SCLC, human meconium, and human red blood cells. Using immunohistochemical assays, 14 of the antibodies were tested against normal lung, liver, and kidney, and lung cancer biopsies and xenografts. These analyses revealed the following: (a) SCLC elicited predominantly immunoglobulin M antibodies despite hyperimmunization; (b) the 21 antibodies displayed distinct binding and immunohistochemical phenotypes, indicating that they recognized many different epitopes; (c) 14 of the 21 antibodies reacted with glycolipid determinants; (d) the 21 determinants were expressed on over 80% of SCLC cell lines, necropsy samples, and xenografts; (e) the determinants were also expressed on normal adult bronchial epithelium, proximal tubules of adult kidney, and in a few instances on other normal cell types; (f) the antigens were expressed less frequently on nonsmall cell lung cancer samples but did not clearly distinguish SCLC from non-small cell lung cancer; (g) biochemical and morphological variants of SCLC exhibiting more malignant and undifferentiated behavior and containing greatly amplified c-myconcogenes failed to express several determinants or expressed them at lower levels; (h) and finally, while many human cell lines failed to express the antigens including human melanoma and glioblastoma lines, human neuroblastoma lines frequently did express the SCLC antigens. These detailed studies utilizing a panel of distinct monoclonal antibodies define a series of antigens on the surface of the majority of SCLC undescribed previously.

摘要

使用一组21种独立的大鼠单克隆抗体研究了人类小细胞肺癌(SCLC)的抗原表达。该组抗体是通过分离产生与两种SCLC细胞系反应但不与自体B淋巴细胞系反应的抗体的杂交瘤而选择的。然后,在放射结合试验中针对一组17种SCLC细胞系、13种非小细胞肺癌细胞系、6份SCLC尸检标本、13种神经外胚层细胞系(黑色素瘤、神经母细胞瘤、胶质母细胞瘤)、15种其他人类细胞系、SCLC的糖脂提取物、人类胎粪和人类红细胞对这些抗体进行了测试。使用免疫组织化学分析,针对正常肺、肝和肾以及肺癌活检和异种移植物对其中14种抗体进行了测试。这些分析揭示了以下几点:(a)尽管进行了超免疫,SCLC主要引发免疫球蛋白M抗体;(b)这21种抗体表现出不同的结合和免疫组织化学表型,表明它们识别许多不同的表位;(c)21种抗体中的14种与糖脂决定簇反应;(d)这21种决定簇在超过80%的SCLC细胞系、尸检样本和异种移植物中表达;(e)这些决定簇也在正常成人支气管上皮、成人肾近端小管中表达,并且在少数情况下在其他正常细胞类型中表达;(f)这些抗原在非小细胞肺癌样本中表达频率较低,但不能明确区分SCLC和非小细胞肺癌;(g)表现出更恶性和未分化行为且含有大量扩增的c-myc原癌基因的SCLC生化和形态学变体未能表达几种决定簇或表达水平较低;(h)最后,虽然许多人类细胞系未能表达这些抗原,包括人类黑色素瘤和胶质母细胞瘤细胞系,但人类神经母细胞瘤细胞系经常表达SCLC抗原。这些利用一组不同单克隆抗体进行的详细研究定义了大多数SCLC表面上一系列以前未描述的抗原。

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