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神经生长因子与抗转铁蛋白受体抗体偶联物:对眼内中隔移植中胆碱能神经元存活的短期和长期影响

NGF and anti-transferrin receptor antibody conjugate: short and long-term effects on survival of cholinergic neurons in intraocular septal transplants.

作者信息

Granholm A C, Bäckman C, Bloom F, Ebendal T, Gerhardt G A, Hoffer B, Mackerlova L, Olson L, Söderström S, Walus L R

机构信息

Department of Basic Science, University of Colorado School of Dentistry, Denver.

出版信息

J Pharmacol Exp Ther. 1994 Jan;268(1):448-59.

PMID:8301587
Abstract

We describe a new molecular carrier system that allows for the transport of nerve growth factor (NGF) across the blood-brain barrier (BBB), as assessed by trophic effects on intraocular forebrain transplants that contain central cholinergic neurons. The carrier system involves monoclonal antibodies (OX-26) directed against the transferrin receptor, to which NGF molecules are covalently linked. Transferrin receptors are highly concentrated on brain blood vessels and participate in the transport of iron across the BBB. Host rats with septal transplants were divided into four groups, which received OX-26-NGF, OX-26, NGF or saline intravenously at 2, 4, 6 and 8 weeks after grafting. Half of the animals were killed directly after the final injection, whereas the other half were allowed to survive for an additional 5 months. Control experiments revealed that blood vessels in mature brain grafts in oculo contained large amounts of transferrin receptors. Covalent binding of NGF to the OX-26 antibodies did not impede OX-26 binding to CNS transferrin receptors, nor did conjugation affect the bioactivity of NGF. A time-dependent increase in host brain NGF levels was found after injection of OX-26-NGF into the tail vein. Host serum contained some NGF antibodies in the short-term OX-26-NGF group that had disappeared in the long-term group; host adrenals showed no differences in wet weight or norepinephrine or epinephrine whole tissue levels in any of the groups. As previously reported, the overall growth of intraocular septal transplants was approximately twice as great in the OX-26-NGF group relative to all other groups. This difference in final size persisted unabated for at least 5 months after the last injection. Furthermore, the significantly higher numbers of choline acetyl transferase immunoreactive neurons in transplants of OX-26-NGF-treated hosts also persisted during the 5-month postinjection interval. Taken together, the data suggest that the OX-26 conjugate may be a unique approach to permit passage of neurotrophin peptides into the brain in a biologically active form.

摘要

我们描述了一种新的分子载体系统,该系统能够使神经生长因子(NGF)穿过血脑屏障(BBB),这是通过对含有中枢胆碱能神经元的眼内前脑移植体的营养作用来评估的。该载体系统涉及针对转铁蛋白受体的单克隆抗体(OX-26),NGF分子与之共价连接。转铁蛋白受体高度集中于脑血血管,并参与铁穿过血脑屏障的转运。将接受中隔移植的宿主大鼠分为四组,在移植后2、4、6和8周静脉注射OX-26-NGF、OX-26、NGF或生理盐水。一半动物在最后一次注射后直接处死,另一半再存活5个月。对照实验显示,眼内成熟脑移植体中的血管含有大量转铁蛋白受体。NGF与OX-26抗体的共价结合并不妨碍OX-26与中枢神经系统转铁蛋白受体的结合,结合也不影响NGF的生物活性。将OX-26-NGF注入尾静脉后,宿主脑内NGF水平出现时间依赖性升高。短期OX-26-NGF组的宿主血清中含有一些NGF抗体,而长期组中这些抗体消失;所有组的宿主肾上腺在湿重、去甲肾上腺素或肾上腺素全组织水平上均无差异。如先前报道,相对于所有其他组,OX-26-NGF组眼内中隔移植体的总体生长大约是其两倍。最后一次注射后至少5个月,最终大小的这种差异一直持续且未减弱。此外,在注射后5个月的间隔期内,接受OX-26-NGF治疗的宿主移植体中胆碱乙酰转移酶免疫反应性神经元的数量显著更多也一直持续。综上所述,数据表明OX-26偶联物可能是使神经营养肽以生物活性形式进入脑内的一种独特方法。

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