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Infect Immun. 1984 May;44(2):469-73. doi: 10.1128/iai.44.2.469-473.1984.
2
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本文引用的文献

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Antitoxic immunity to cholera in dogs immunized orally with cholera toxin.用霍乱毒素经口免疫的犬对霍乱的抗毒免疫。
Infect Immun. 1980 Feb;27(2):632-7. doi: 10.1128/iai.27.2.632-637.1980.
2
Mucosal immunology.黏膜免疫学
Immunology. 1980 Oct;41(2):249-70.
3
Oral immunization of dogs with purified cholera toxin, crude cholera toxin, or B subunit: evidence for synergistic protection by antitoxic and antibacterial mechanisms.用纯化霍乱毒素、粗制霍乱毒素或B亚单位对犬进行口服免疫:抗毒素和抗菌机制协同保护的证据。
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Procholeragenoid: a safe and effective antigen for oral immunization against experimental cholera.前霍乱类毒素:一种用于针对实验性霍乱进行口服免疫的安全有效抗原。
Infect Immun. 1983 Jun;40(3):1112-8. doi: 10.1128/iai.40.3.1112-1118.1983.
5
Single bilayer liposomes prepared without sonication.未经过超声处理制备的单层脂质体。
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N,N-dioctadecyl-N',N'-bis(2-hydroxyethyl) propanediamine: antiviral activity and interferon stimulation in mice.N,N-二辛基-N',N'-双(2-羟乙基)丙二胺:小鼠体内的抗病毒活性及干扰素刺激作用
Antimicrob Agents Chemother. 1973 Apr;3(4):498-502. doi: 10.1128/AAC.3.4.498.
7
Antibodies of the IgA type in intestinal plasma cells of germfree mice after oral or parenteral immunization with ferritin.用铁蛋白经口或非肠道免疫无菌小鼠后,其肠道浆细胞中IgA类抗体的情况
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8
Cellular kinetics of the intestinal immune response to cholera toxoid in rats.大鼠对霍乱类毒素肠道免疫反应的细胞动力学
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9
Immunity to experimental cholera. III. Enhanced duration of protection after sequential parenteral-oral administration of toxoid to dogs.实验性霍乱免疫。III. 对犬类先后进行肠胃外-口服类毒素给药后保护期的延长
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10
Preparation of a purified antigenic cholera toxoid.纯化抗原性霍乱类毒素的制备。
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通过霍乱毒素和类霍乱原与脂质胺佐剂(阿弗立定)在脂质体中递送实现增强的粘膜致敏。

Enhanced mucosal priming by cholera toxin and procholeragenoid with a lipoidal amine adjuvant (avridine) delivered in liposomes.

作者信息

Pierce N F, Sacci J B

出版信息

Infect Immun. 1984 May;44(2):469-73. doi: 10.1128/iai.44.2.469-473.1984.

DOI:10.1128/iai.44.2.469-473.1984
PMID:6370867
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC263543/
Abstract

The mucosal adjuvant activity of avridine, a synthetic lipoidal amine [N,N-dioctadecyl-N',N'-(2-hydroxymethyl) propanediamine, previously designated CP-20,961), was studied in rats immunized intraintestinally with cholera toxin or procholeragenoid. Avridine was most efficient as an adjuvant when incorporated into liposomes; liposomes that lacked avridine had no adjuvant effect. Coadministration of avridine-containing liposomes with enteric priming doses of cholera toxin or procholeragenoid enhanced the efficiency of priming for secondary mucosal anti-cholera toxin responses, i.e., the establishment of memory, five- to sevenfold. Avridine-containing liposomes had no significant effect, however, on either the primary mucosal anti-cholera toxin response, when given with the primary dose of antigen, or on the secondary response, when given with the booster dose to previously primed animals. Little or no adjuvant effect occurred when avridine-containing liposomes were given concurrently with antigen, but at a separate mucosal site or parenterally, or at the site of enteric immunization, but 1 day earlier or later. These results support the notion that adjuvants may be developed which enhance the mucosal immunogenicity of locally applied antigens and suggest that liposomes may be effective vehicles for delivery of such adjuvants.

摘要

研究了合成类脂胺阿弗立定(N,N-二十八烷基-N',N'-(2-羟甲基)丙二胺,先前称为CP-20,961)对经肠道用霍乱毒素或类霍乱原免疫的大鼠的黏膜佐剂活性。阿弗立定掺入脂质体时作为佐剂最为有效;不含阿弗立定的脂质体无佐剂作用。含阿弗立定的脂质体与肠道初次免疫剂量的霍乱毒素或类霍乱原共同给药,可使二次黏膜抗霍乱毒素反应(即记忆的建立)的初次免疫效率提高5至7倍。然而,含阿弗立定的脂质体与抗原初次剂量同时给药时,对初次黏膜抗霍乱毒素反应无显著影响;与加强剂量同时给药时,对先前已免疫动物的二次反应也无显著影响。含阿弗立定的脂质体与抗原同时在不同黏膜部位或经胃肠外给药,或在肠道免疫部位但提前或推迟1天给药时,几乎没有或没有佐剂作用。这些结果支持这样一种观点,即可以开发出增强局部应用抗原黏膜免疫原性的佐剂,并表明脂质体可能是递送此类佐剂的有效载体。