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脂质体介导的细胞因子递送:包裹于常规脂质体和长循环脂质体中的白细胞介素-2的造血及免疫调节活性

Delivery of cytokines by liposomes: hematopoietic and immunomodulatory activity of interleukin-2 encapsulated in conventional liposomes and in long-circulating liposomes.

作者信息

Kedar E, Gur H, Babai I, Samira S, Even-Chen S, Barenholz Y

机构信息

The Lautenberg Center for General and Tumor Immunology, Hebrew University-Hadassah Medical School, Jerusalem, Israel.

出版信息

J Immunother. 2000 Jan;23(1):131-45. doi: 10.1097/00002371-200001000-00016.

Abstract

Although liposomal delivery of interleukin-2 (IL-2) and other cytokines improves their pharmacokinetics and biologic activity in vivo, there are no comparative functional studies of various liposomal formulations as cytokine carriers. In the present investigation, recombinant human IL-2 was encapsulated in two formulations of large (mean diameter 0.75-1.5 microns) multilamellar vesicles (MLV, referred to as conventional liposomes) or in small (mean diameter, 60 nm), unilamellar, long-circulating liposomes (referred to as sterically stabilized liposomes, SSL). The biologic activity of the liposomal formulations and of free IL-2 was tested in parallel in vitro and in mice. The main observations were as follows: (a) All the liposomal IL-2 (Lip-IL-2) formulations were more efficient than soluble IL-2 in stimulating spleen cell proliferation and lymphokine-activated killer (LAK) cell activation in vitro, particularly at low cytokine doses (1-100 CU/mL). (b) After i.v. injection, the circulation time of MLV-IL-2 and SSL-IL-2 was 7 and 17 times greater, respectively, than that of soluble IL-2. (c) In comparison with IL-2, all Lip-IL-2 formulations caused a marked increase in the leukocyte levels in blood, spleen, and peritoneal exudate, especially in those of myeloid origin (neutrophils, eosinophils, immature granulocytes, and macrophages). (d) Although SSL-IL-2 exhibited the longest circulation time, MLV-IL-2 was more potent in elevating leukocyte levels and in triggering LAK cell activity in vivo. (e) The route of Lip-IL-2 administration greatly affected the immunomodulatory activity in the various compartments. (f) MLV-IL-2 proved to be a much more efficient immunoadjuvant than free IL-2 for influenza subunit vaccines as well as for tumor cell vaccines. These findings lend support to our previous studies in which we demonstrated the superior immunomodulatory activity of liposomal IL-2, and suggest that cytokine pharmacokinetics, biodistribution, and pharmacodynamics are markedly influence both by liposomal formulation and route of administration.

摘要

尽管白细胞介素-2(IL-2)和其他细胞因子的脂质体递送改善了它们在体内的药代动力学和生物学活性,但对于作为细胞因子载体的各种脂质体制剂,尚无比较性的功能研究。在本研究中,重组人IL-2被包裹在两种大的(平均直径0.75 - 1.5微米)多层囊泡(MLV,称为传统脂质体)或小的(平均直径60纳米)单层长效循环脂质体(称为空间稳定脂质体,SSL)制剂中。脂质体制剂和游离IL-2的生物学活性在体外和小鼠体内进行了平行测试。主要观察结果如下:(a)所有脂质体IL-2(Lip-IL-2)制剂在体外刺激脾细胞增殖和淋巴因子激活的杀伤(LAK)细胞活化方面比可溶性IL-2更有效,特别是在低细胞因子剂量(1 - 100 CU/mL)时。(b)静脉注射后,MLV-IL-2和SSL-IL-2的循环时间分别比可溶性IL-2长7倍和17倍。(c)与IL-2相比,所有Lip-IL-2制剂均导致血液、脾脏和腹腔渗出液中的白细胞水平显著增加,尤其是髓系来源的白细胞(中性粒细胞、嗜酸性粒细胞、未成熟粒细胞和巨噬细胞)。(d)尽管SSL-IL-2的循环时间最长,但MLV-IL-2在提高白细胞水平和触发体内LAK细胞活性方面更有效力。(e)Lip-IL-2的给药途径极大地影响了各个部位的免疫调节活性。(f)对于流感亚单位疫苗以及肿瘤细胞疫苗,MLV-IL-2被证明是比游离IL-2更有效的免疫佐剂。这些发现支持了我们之前的研究,即我们证明了脂质体IL-2具有卓越的免疫调节活性,并表明细胞因子的药代动力学、生物分布和药效学均受到脂质体制剂和给药途径的显著影响。

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