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去铁胺与抗转铁蛋白受体IgG单克隆抗体联合治疗对造血系统肿瘤生长的抑制作用:铁剥夺毒性阈值模型的证据

Inhibition of hematopoietic tumor growth by combined treatment with deferoxamine and an IgG monoclonal antibody against the transferrin receptor: evidence for a threshold model of iron deprivation toxicity.

作者信息

Kemp J D, Thorson J A, Stewart B C, Naumann P W

机构信息

Department of Pathology, University of Iowa College of Medicine, Iowa City 52242.

出版信息

Cancer Res. 1992 Aug 1;52(15):4144-8.

PMID:1638529
Abstract

Recent studies have suggested that iron deprivation may represent a useful new approach in cancer therapy, and several strategies for producing such deprivation are now under investigation. Thus, for example, we recently provided evidence that combined treatment with the iron chelator deferoxamine and an IgG monoclonal antibody against the transferrin receptor (ATRA) produces synergistic inhibition of hematopoietic tumor cell growth in vitro (J. D. Kemp, K. M. Smith, L. J. Kanner, F. Gomez, J. A. Thorson, and P. W. Naumann, Blood, 76: 991-995, 1990). The current study is an attempt to analyze the mechanisms responsible for the synergistic interaction. The data show that a single IgG ATRA can produce up to 75% inhibition of iron uptake while having little effect on DNA synthesis; this suggests that tumor cells either take up or have stored amounts of iron well in excess of that required to support immediate metabolic needs. When deferoxamine and the IgG ATRA are used together, the effects on iron acquisition and receptor down-modulation are either additive or subadditive but are clearly not synergistic. Overall, the findings suggest that the IgG ATRA produces an injury to iron uptake that is just below a critical threshold and that the additional effect provided by the iron chelator is sufficient to exceed that threshold and produce a rapid depletion of iron pools that are vital for short-term DNA synthesis. IgG ATRAS thus seem to be of even greater interest as therapeutic reagents, and further study of their properties and of how they interact with deferoxamine appears to be warranted.

摘要

近期研究表明,铁剥夺可能是癌症治疗中一种有用的新方法,目前正在研究几种产生这种剥夺的策略。例如,我们最近提供的证据表明,铁螯合剂去铁胺与抗转铁蛋白受体的IgG单克隆抗体(ATRA)联合治疗在体外可协同抑制造血肿瘤细胞生长(J.D. Kemp、K.M. Smith、L.J. Kanner、F. Gomez、J.A. Thorson和P.W. Naumann,《血液》,76: 991 - 995,1990)。本研究旨在分析产生协同相互作用的机制。数据显示,单一的IgG ATRA可抑制高达75%的铁摄取,而对DNA合成影响很小;这表明肿瘤细胞摄取或储存的铁量远远超过支持即时代谢需求所需的量。当去铁胺和IgG ATRA一起使用时,对铁摄取和受体下调的影响要么是相加的,要么是次相加的,但显然不是协同的。总体而言,研究结果表明,IgG ATRA对铁摄取造成的损伤略低于临界阈值,而铁螯合剂提供的额外作用足以超过该阈值,并导致对短期DNA合成至关重要的铁池迅速耗竭。因此,IgG ATRAS作为治疗试剂似乎更具吸引力,有必要对其特性以及它们与去铁胺的相互作用方式进行进一步研究。

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引用本文的文献

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Iron and leukemia: new insights for future treatments.铁与白血病:未来治疗的新视角。
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Sensitivity of cells to apoptosis induced by iron deprivation can be reversibly changed by iron availability.细胞对铁缺乏诱导的细胞凋亡的敏感性可因铁的可利用性而发生可逆性改变。
Cell Prolif. 2006 Dec;39(6):551-61. doi: 10.1111/j.1365-2184.2006.00411.x.
3
Identification of the di-pyridyl ketone isonicotinoyl hydrazone (PKIH) analogues as potent iron chelators and anti-tumour agents.
鉴定二吡啶基酮异烟酰腙(PKIH)类似物作为有效的铁螯合剂和抗肿瘤剂。
Br J Pharmacol. 2003 Mar;138(5):819-30. doi: 10.1038/sj.bjp.0705089.
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Differing sensitivity of tumor cells to apoptosis induced by iron deprivation in vitro.
In Vitro Cell Dev Biol Anim. 2001 Jul-Aug;37(7):450-8. doi: 10.1290/1071-2690(2001)037<0450:DSOTCT>2.0.CO;2.
5
Unexpected effects of albumin on apoptosis induction by deferoxamine in vitro.
In Vitro Cell Dev Biol Anim. 2000 Mar;36(3):151-2. doi: 10.1290/1071-2690(2000)036<0151:UEOAOA>2.0.CO;2.
6
Antigen forks: bispecific reagents that inhibit cell growth by binding selected pairs of tumor antigens.抗原叉:通过结合选定的肿瘤抗原对来抑制细胞生长的双特异性试剂。
Cancer Immunol Immunother. 1994 Jul;39(1):41-8. doi: 10.1007/BF01517179.