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肝脏和脾脏巨噬细胞的器官特异性血清调理素的差异特性。

Differential properties of organ-specific serum opsonins for liver and spleen macrophages.

作者信息

Moghimi S M, Patel H M

机构信息

Department of Biochemistry, Charing Cross and Westminster Medical School, London, U.K.

出版信息

Biochim Biophys Acta. 1989 Sep 18;984(3):379-83. doi: 10.1016/0005-2736(89)90306-4.

Abstract

Earlier we reported that serum contains organ-specific opsonins which selectively enhance recognition of liposomes by macrophages in the specific organs of the reticuloendothelial system (Moghimi, S.M. and Patel, H.M. (1988) FEBS Lett. 233, 143-147). The results presented here describe the properties of these organ-specific opsonins which differentiate between liver-specific and spleen-specific opsonins responsible for the enhancement of phagocytosis of liposomes by Kupffer cells and spleen macrophage, respectively. Liver-specific opsonin is a heat-stable macromolecule which on heating or on freezing and thawing exhibits enhanced opsonic activity. Serum also contains a dialysable factor which inhibits its opsonic activity. On the other hand, the spleen-specific opsonin is a heat-labile macromolecule which is sensitive to freezing and thawing and requires a dialysable serum co-factor for its optimum opsonic activity on spleen macrophages. Removal of this factor from serum brings about an irreversible conformational change in the opsonin. Evidence suggests that the spleen-specific opsonin may be composed of more than one different opsonin molecule. It is suggested that the serum factor(s) that inhibits liver-specific opsonic activity and enhances the spleen-specific activity may not be the same molecule, but in both the cases the factor(s) may mediate its function by modifying the process of the opsonisation of liposomes or by influencing the interaction of the opsonised liposomes with the respective cells. We propose that purification of the organ-specific opsonins may provide an opportunity to target drug carriers selectively to a specific organ of the reticuloendothelial system, and help us to evaluate their role in the altered opsonin states known to exist in certain diseases.

摘要

我们之前报道过,血清中含有器官特异性调理素,可选择性增强网状内皮系统特定器官中巨噬细胞对脂质体的识别(莫吉米,S.M.和帕特尔,H.M.(1988年)《欧洲生物化学学会联合会快报》233,143 - 147)。此处呈现的结果描述了这些器官特异性调理素的特性,它们分别区分了负责增强库普弗细胞和脾巨噬细胞对脂质体吞噬作用的肝脏特异性调理素和脾脏特异性调理素。肝脏特异性调理素是一种热稳定的大分子,加热、冷冻和解冻后其调理活性增强。血清中还含有一种可透析因子,可抑制其调理活性。另一方面,脾脏特异性调理素是一种热不稳定的大分子,对冷冻和解冻敏感,并且在脾脏巨噬细胞上发挥最佳调理活性需要一种可透析的血清辅助因子。从血清中去除该因子会导致调理素发生不可逆的构象变化。有证据表明,脾脏特异性调理素可能由不止一种不同的调理素分子组成。据推测,抑制肝脏特异性调理活性并增强脾脏特异性活性的血清因子可能不是同一分子,但在这两种情况下,该因子可能通过改变脂质体调理过程或影响调理后的脂质体与相应细胞的相互作用来介导其功能。我们提出,纯化器官特异性调理素可能为将药物载体选择性靶向网状内皮系统的特定器官提供机会,并帮助我们评估它们在某些已知疾病中存在的调理素状态改变中的作用。

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