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抗人α血小板衍生生长因子受体单克隆抗体对血小板衍生生长因子自分泌生长刺激的抑制作用

Inhibition of platelet-derived growth factor autocrine growth stimulation by a monoclonal antibody to the human alpha platelet-derived growth factor receptor.

作者信息

LaRochelle W J, Jensen R A, Heidaran M A, May-Siroff M, Wang L M, Aaronson S A, Pierce J H

机构信息

Laboratory of Cellular and Molecular Biology, National Cancer Institute, Bethesda, Maryland 20892.

出版信息

Cell Growth Differ. 1993 Jul;4(7):547-53.

PMID:7691151
Abstract

A potent neutralizing monoclonal antibody to the human alpha platelet-derived growth factor (PDGF) receptor (alpha PDGFR) was raised by immunizing BALB/c mice with 32D cells expressing the human alpha PDGFR. This monoclonal antibody, designated alpha R1, immunoprecipitated human, monkey, rabbit, pig, dog, and cat, but not hamster, rat, or mouse alpha PDGFRs. Comparison with PR292, a monoclonal antibody previously generated against the alpha PDGFR, showed that both recognized alpha PDGFR extracellular domains, but neither demonstrated reactivity against the beta PDGFR. In vitro binding studies revealed that alpha R1, but not PR292, detection of the alpha PDGFR was blocked by either PDGF AA or PDGF BB. These results strongly suggest that the receptor ligand-binding domain spatially overlapped with the alpha R1 epitope. Monoclonal antibody alpha R1 also inhibited PDGF stimulation of [3H]thymidine uptake by 32D cells expressing the alpha PDGFR (32D alpha R) as well as autocrine growth stimulation of 32D alpha R cells transfected with and expressing PDGF AA or PDGF BB. Therefore, monoclonal antibody alpha R1 may be useful in the detection and growth inhibition of malignancies in which PDGF autocrine stimulation and/or alpha PDGFR overexpression plays an important role(s).

摘要

通过用表达人α血小板衍生生长因子(PDGF)受体(αPDGFR)的32D细胞免疫BALB / c小鼠,制备了一种针对人αPDGF受体的强效中和单克隆抗体。这种单克隆抗体命名为αR1,可免疫沉淀人、猴、兔、猪、狗和猫的αPDGFR,但不能沉淀仓鼠、大鼠或小鼠的αPDGFR。与先前针对αPDGFR产生的单克隆抗体PR292比较表明,二者均识别αPDGFR细胞外结构域,但均未显示出对βPDGFR的反应性。体外结合研究表明,PDGF AA或PDGF BB均可阻断αR1(而非PR292)对αPDGFR的检测。这些结果强烈表明,受体配体结合结构域在空间上与αR1表位重叠。单克隆抗体αR1还抑制了PDGF对表达αPDGFR的32D细胞(32DαR)的[3H]胸苷摄取刺激,以及对转染并表达PDGF AA或PDGF BB的32DαR细胞的自分泌生长刺激。因此,单克隆抗体αR1可能有助于检测和抑制PDGF自分泌刺激和/或αPDGFR过表达起重要作用的恶性肿瘤。

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