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绵羊地高辛特异性IgG和Fab片段在兔和狒狒体内的免疫原性、分布动力学及消除情况

Immunogenicity and kinetics of distribution and elimination of sheep digoxin-specific IgG and Fab fragments in the rabbit and baboon.

作者信息

Smith T W, Lloyd B L, Spicer N, Haber E

出版信息

Clin Exp Immunol. 1979 Jun;36(3):384-96.

Abstract

To evaluate the relative merits of purified IgG and Fab preparations of defined specificity for potential clinical use, immunogenicity studies were carried out in baboon and rabbit experimental models. Distribution and elimination kinetics of purified sheep digoxin-specific IgG and Fab fragments were also studied following intravenous administration to baboons. Serial plasma and urine Fab concentrations were determined from trichloroacetic acid-precipitable 125I counts from pre-labelled preparations and also by measurement of the antibody's functional 3H-digoxin binding capacity. Results were compared with data obtained from IgG by 3H-digoxin binding. Kinetic data analysed by computer-fitted functions demonstrated that plasma Fab disappearance was best described by a tri-exponential function, whereas a bi-exponential function best described the IgG data. Initial distribution half-life (t 1/2) of Fab (0.28-0.32 hr) was considerably shorter than that of IgG (4.0 hr) and contributed a greater proportion of the total fall in plasma level over 24 hr. Fab elimination t 1/2 (9-13 hr) was also shorter than IgG (61 hr), but appreciably longer than earlier estimates in rabbits, guinea-pigs, rats and mice. The total volume of distribution of Fab was 8.7 times greater than that of IgG measured by the same method. Over the first 24 hr after administration 30-45% of administered Fab was recoverable in active form in urine, while 93% of total administered 125I counts from 125I-Fab preparations (bound and free) could be recovered. Less than 1% of administered IgG binding activity was recovered in urine during the initial 24 hr. The relative immunogenicities of sheep digoxin-specific IgG and Fab fragments were studied in six baboons. Both IgG and Fab elicited prompt immune responses when injected intramuscularly with Freund's complete adjuvant. Intravenous injection of soluble sheep IgG resulted in a prompt immune response in one baboon while repeated injections caused only a late, weak response in a second animal. Soluble sheep Fab fragments elicited only delayed and weak responses in the two baboons thus challenged. Further immunogenicity studies in ninteen rabbits showed significantly earlier and greater antibody responses to intravenously administered sheep IgG antigen than to Fab fragments derived from the same IgG population. These studies demonstrate that digoxin-specific Fab fragments undergo more rapid and extensive distribution to the extra vascular compartment and also more rapid renal excretion than IgG. Furthermore, Fab fragments are significantly less immunogenic than the parent IgG population. These data indicate potentially important therapeutic advantages for digoxin-specific Fab compared with IgG when administered for the reversal of life-threatening digitlis toxicity.

摘要

为评估具有特定特异性的纯化IgG和Fab制剂在临床应用中的相对优势,在狒狒和兔子实验模型中开展了免疫原性研究。在给狒狒静脉注射后,还研究了纯化的羊地高辛特异性IgG和Fab片段的分布及消除动力学。通过对预标记制剂经三氯乙酸沉淀后的125I计数,以及通过测量抗体的功能性3H-地高辛结合能力,来测定系列血浆和尿液中的Fab浓度。将结果与通过3H-地高辛结合从IgG获得的数据进行比较。通过计算机拟合函数分析的动力学数据表明,血浆中Fab的消失情况最好用三指数函数描述,而双指数函数最能描述IgG的数据。Fab的初始分布半衰期(t1/2)(0.28 - 0.32小时)明显短于IgG的(4.0小时),并且在24小时内血浆水平的总下降中占比更大。Fab的消除t1/2(9 - 13小时)也短于IgG的(61小时),但明显长于之前在兔子、豚鼠、大鼠和小鼠中的估计值。用相同方法测得的Fab的分布总体积比IgG的大8.7倍。给药后的头24小时内,30 - 45%给予的Fab以活性形式可在尿液中回收,而来自125I - Fab制剂(结合和游离)的总给予125I计数的93%可被回收。在最初的24小时内,尿液中回收的给予的IgG结合活性不到1%。在六只狒狒中研究了羊地高辛特异性IgG和Fab片段的相对免疫原性。当与弗氏完全佐剂一起肌肉注射时,IgG和Fab均引发了迅速的免疫反应。静脉注射可溶性羊IgG在一只狒狒中引发了迅速的免疫反应,而重复注射在另一只动物中仅引起了迟发、微弱的反应。可溶性羊Fab片段在接受挑战的两只狒狒中仅引发了延迟且微弱的反应。在19只兔子中进行的进一步免疫原性研究表明,与源自相同IgG群体的Fab片段相比,静脉注射羊IgG抗原引发的抗体反应明显更早且更强。这些研究表明,地高辛特异性Fab片段比IgG更快且更广泛地分布到血管外腔室,并且肾脏排泄也更快。此外,Fab片段的免疫原性明显低于亲本IgG群体。这些数据表明,在用于逆转危及生命的洋地黄毒性时,与IgG相比,地高辛特异性Fab具有潜在的重要治疗优势。

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