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1
Characterization of immunogenic properties of haptenated liposomal model membranes in mice. V. Effect of membrane composition on humoral and cellular immunogenicity.小鼠中半抗原化脂质体模型膜免疫原性特性的表征。V. 膜组成对体液免疫原性和细胞免疫原性的影响。
Immunology. 1981 Nov;44(3):561-8.
2
Characterization of immunogenic properties of haptenated liposomal model membranes in mice.小鼠中半抗原化脂质体模型膜免疫原性特性的表征
Immunology. 1981 Feb;42(2):233-9.
3
Characterization of immunogenic properties of haptenated liposomal model membranes in mice. II. Induction of delayed-type hypersensitivity.小鼠中半抗原化脂质体模型膜免疫原性特性的表征。II. 迟发型超敏反应的诱导。
Immunology. 1981 Jan;42(1):165-73.
4
Characterization of immunogenic properties of haptenated liposomal model membranes in mice. I. Thymus independence of the antigen.小鼠中半抗原化脂质体模型膜免疫原性特性的表征。I. 抗原的胸腺非依赖性
Immunology. 1979 Jun;37(2):505-14.
5
Adjuvant effects of nonionic block polymer surfactants on liposome-induced humoral immune response.非离子嵌段聚合物表面活性剂对脂质体诱导的体液免疫反应的佐剂作用。
J Immunol. 1987 Jan 1;138(1):220-5.
6
Effect of liposomal model membrane composition on immunogenicity.脂质体模型膜组成对免疫原性的影响。
J Immunol. 1978 Apr;120(4):1109-13.
7
Characterization of immunogenic properties of haptenated liposomal model membranes in mice. VI. Response in B-cell-defective CBA/N mice.小鼠中半抗原化脂质体模型膜免疫原性特性的表征。VI. B细胞缺陷型CBA/N小鼠的反应。
Immunology. 1982 Mar;45(3):545-51.
8
Characterization of immunogenic properties of haptenated liposomal model membranes in mice. VII. Synergistic responses to haptenated liposomes and haptenated thymus-dependent antigens in CBA/N mice.小鼠中半抗原化脂质体模型膜免疫原性特性的表征。VII. CBA/N小鼠对半抗原化脂质体和半抗原化胸腺依赖性抗原的协同反应。
Immunology. 1982 Apr;45(4):613-20.
9
Characterization of immunogenic properties of haptenated liposomal model membranes in mice. IV. induction of IgM memory.小鼠中半抗原化脂质体模型膜免疫原性特性的表征。IV. IgM记忆的诱导。
Immunology. 1981 Aug;43(4):627-34.
10
The specificity of antibody formation in mice following immunization with hapten-carrier complexes mixed with the surfactant, dimethyl dioctadecyl ammonium bromide.用与表面活性剂二甲基二辛基溴化铵混合的半抗原-载体复合物免疫小鼠后抗体形成的特异性。
Immunology. 1980 Mar;39(3):361-6.

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Vaccines (Basel). 2023 Mar 15;11(3):661. doi: 10.3390/vaccines11030661.
2
Liposomes as Adjuvants and Vaccine Delivery Systems.脂质体作为佐剂和疫苗递送系统。
Biochem (Mosc) Suppl Ser A Membr Cell Biol. 2022;16(1):1-20. doi: 10.1134/S1990747822020076. Epub 2022 Feb 14.
3
Liposomes used as a vaccine adjuvant-delivery system: From basics to clinical immunization.脂质体作为疫苗佐剂传递系统:从基础到临床免疫。
J Control Release. 2019 Jun 10;303:130-150. doi: 10.1016/j.jconrel.2019.04.025. Epub 2019 May 3.
4
Induction of Plasmodium-Specific Immune Responses Using Liposome-Based Vaccines.利用脂质体疫苗诱导疟原虫特异性免疫应答。
Front Immunol. 2019 Feb 1;10:135. doi: 10.3389/fimmu.2019.00135. eCollection 2019.
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The Multirole of Liposomes in Therapy and Prevention of Infectious Diseases.脂质体在传染病治疗和预防中的多效作用。
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6
Liposomal vaccine formulations as prophylactic agents: design considerations for modern vaccines.脂质体疫苗制剂作为预防性制剂:现代疫苗的设计考虑因素。
J Nanobiotechnology. 2017 Nov 17;15(1):83. doi: 10.1186/s12951-017-0319-9.
7
Design considerations for liposomal vaccines: influence of formulation parameters on antibody and cell-mediated immune responses to liposome associated antigens.脂质体疫苗的设计考虑因素:配方参数对与脂质体相关抗原结合的抗体和细胞介导免疫应答的影响。
Vaccine. 2012 Mar 16;30(13):2256-72. doi: 10.1016/j.vaccine.2012.01.070. Epub 2012 Feb 2.
8
Enhancement of immunogenicity by incorporation of lipid A into liposomal model membranes and its application to membrane-associated antigens.通过将脂多糖A掺入脂质体模型膜来增强免疫原性及其在膜相关抗原中的应用。
Immunology. 1983 Dec;50(4):605-12.
9
The effect of liposomal charge on the neutralizing antibody response against inactivated encephalomyocarditis and Semliki Forest viruses.脂质体电荷对针对灭活脑心肌炎病毒和塞姆利基森林病毒的中和抗体反应的影响。
Clin Exp Immunol. 1984 Jun;56(3):509-14.
10
Enhancement of immunogenicity of tumour virus antigen by liposomes: the effect of lipid composition.脂质体增强肿瘤病毒抗原的免疫原性:脂质组成的影响。
Immunology. 1986 Jul;58(3):507-13.

本文引用的文献

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Effect of the cholesterol content of small unilamellar liposomes on their stability in vivo and in vitro.小单层脂质体胆固醇含量对其体内外稳定性的影响。
Biochem J. 1980 Feb 15;186(2):591-8. doi: 10.1042/bj1860591.
2
Cholesterol content of small unilamellar liposomes controls phospholipid loss to high density lipoproteins in the presence of serum.在有血清存在的情况下,小单层脂质体的胆固醇含量控制着磷脂向高密度脂蛋白的流失。
FEBS Lett. 1980 Mar 10;111(2):324-8. doi: 10.1016/0014-5793(80)80819-2.
3
Characterization of immunogenic properties of haptenated liposomal model membranes in mice.小鼠中半抗原化脂质体模型膜免疫原性特性的表征
Immunology. 1981 Feb;42(2):233-9.
4
Characterization of immunogenic properties of haptenated liposomal model membranes in mice. II. Induction of delayed-type hypersensitivity.小鼠中半抗原化脂质体模型膜免疫原性特性的表征。II. 迟发型超敏反应的诱导。
Immunology. 1981 Jan;42(1):165-73.
5
Thermal analysis of lipids, proteins and biological membranes. A review and summary of some recent studies.脂质、蛋白质及生物膜的热分析:近期一些研究的综述与总结
Chem Phys Lipids. 1969 Dec;3(4):304-56. doi: 10.1016/0009-3084(69)90040-1.
6
Control of the rate of hepatic uptake and catabolism of liposome-entrapped proteins injected into rats. Possible therapeutic applications.大鼠体内脂质体包裹蛋白肝摄取和分解代谢速率的控制。潜在的治疗应用。
Eur J Biochem. 1974 Aug 15;47(1):179-85. doi: 10.1111/j.1432-1033.1974.tb03681.x.
7
The effect of particle size and charge on the clearance rates of liposomes and liposome encapsulated drugs.粒径和电荷对脂质体及脂质体包封药物清除率的影响。
Biochem Biophys Res Commun. 1975 Apr 7;63(3):651-8. doi: 10.1016/s0006-291x(75)80433-5.
8
Phase transitions and fluidity characteristics of lipids and cell membranes.脂质与细胞膜的相变及流动性特征
Q Rev Biophys. 1975 May;8(2):185-235. doi: 10.1017/s0033583500001797.
9
Effect of liposomal model membrane composition on immunogenicity.脂质体模型膜组成对免疫原性的影响。
J Immunol. 1978 Apr;120(4):1109-13.
10
Dimethyl diotadecyl ammonium bromide as adjuvant for delayed hypersensitivity in mice.二甲基二十八烷基溴化铵作为小鼠迟发型超敏反应的佐剂。
Immunology. 1977 Dec;33(6):931-36.

小鼠中半抗原化脂质体模型膜免疫原性特性的表征。V. 膜组成对体液免疫原性和细胞免疫原性的影响。

Characterization of immunogenic properties of haptenated liposomal model membranes in mice. V. Effect of membrane composition on humoral and cellular immunogenicity.

作者信息

van Houte A J, Snippe H, Schmitz M G, Willers J M

出版信息

Immunology. 1981 Nov;44(3):561-8.

PMID:7033115
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1554971/
Abstract

This paper describes the effect of altering liposomal membrane composition on humoral and cellular immunogenicity of haptenated liposomes in mice. Antibody formation was determined by enumeration of direct, plaque-forming cells in the spleen and delayed-type hypersensitivity (DH) was measured with a footpad swelling test. Humoral immunogenicity of haptenated liposomes was strongly influenced by membrane phospholipid, cholesterol and charged amphiphile composition. Haptenated liposomes prepared from phospholipids with a low (dioleoyl- and dilauroyl-phosphatidylcholine) or high (distearoyl phosphatidylcholine) phase-transition temperature were less immunogenic than those prepared from phospholipids with an intermediate phase-transition temperature (dipalmitoyl phosphatidylcholine and sphingomyelin). In general, increasing the amount of liposomal membrane cholesterol induced a higher humoral response. These results are discussed in relation to liposomal membrane fluidity. Induction of an optimal DH with haptenated liposomes did not occur in the absence of the adjuvant dimethyl dioctadecyl ammonium bromide (DDA). When DDA was used, alterations in membrane composition did not influence cellular immunogenicity. From these results it was concluded that 'intermediate' liposomal membrane fluidity is the most important requirement for induction of optimal antibody formation with haptenated liposomes and that a certain physicochemical configuration of the antigen, provided by the adjuvant DDA, is a prerequisite for induction of DH.

摘要

本文描述了改变脂质体膜组成对小鼠中半抗原化脂质体的体液免疫原性和细胞免疫原性的影响。通过计数脾脏中直接的、形成噬斑的细胞来确定抗体形成,并用足垫肿胀试验测量迟发型超敏反应(DH)。半抗原化脂质体的体液免疫原性受膜磷脂、胆固醇和带电荷两亲物组成的强烈影响。由具有低(二油酰基和二月桂酰基磷脂酰胆碱)或高(二硬脂酰磷脂酰胆碱)相变温度的磷脂制备的半抗原化脂质体比由具有中间相变温度(二棕榈酰磷脂酰胆碱和鞘磷脂)的磷脂制备的脂质体免疫原性更低。一般来说,增加脂质体膜胆固醇的量会诱导更高的体液反应。结合脂质体膜流动性对这些结果进行了讨论。在没有佐剂二甲基二十八烷基溴化铵(DDA)的情况下,半抗原化脂质体不会诱导出最佳的DH。当使用DDA时膜组成的改变不会影响细胞免疫原性。从这些结果得出结论,“中等”的脂质体膜流动性是用半抗原化脂质体诱导最佳抗体形成的最重要要求,并且由佐剂DDA提供的抗原的特定物理化学构型是诱导DH的先决条件。