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脂质体免疫刺激DNA序列(ISS-ODN):一种用于流感疫苗和乙肝疫苗的高效肠胃外及黏膜佐剂。

Liposomal immunostimulatory DNA sequence (ISS-ODN): an efficient parenteral and mucosal adjuvant for influenza and hepatitis B vaccines.

作者信息

Joseph Aviva, Louria-Hayon Igal, Plis-Finarov Alla, Zeira Evelyne, Zakay-Rones Zichria, Raz Eyal, Hayashi Tomoko, Takabayashi Kenji, Barenholz Yechezkel, Kedar Eli

机构信息

The Lautenberg Center for General and Tumor Immunology, Hebrew University-Hadassah Medical School, P.O. Box 12272, Jerusalem 91120, Israel.

出版信息

Vaccine. 2002 Sep 10;20(27-28):3342-54. doi: 10.1016/s0264-410x(02)00295-5.

Abstract

Synthetic oligodeoxynucleotides (ODNs) containing immunostimulatory sequences (ISS-ODN, also known as CpG-ODNs) have been shown to display in experimental models potent Th1-biassed immunoadjuvant activity upon parenteral or mucosal co-administration with a variety of antigens. In an attempt to potentiate adjuvant activity, and to reduce dose and number of administrations, ISS-ODN was entrapped (up to 90% efficiency) in large (1.5 microm) multilamellar liposomes using a simple and fast (5 min) procedure. Mice were vaccinated once or twice intramuscularly (i.m.) or intranasally (i.n.) with subunit influenza vaccines (consisting of the viral hemagglutinin and neuraminidase, HN) or with hepatitis B surface antigen particles (HBsAg), either non-encapsulated or liposome-encapsulated, together with free or liposomal ISS-ODN (5-25 microg per dose). At 3-12 weeks post-vaccination, the humoral (systemic, mucosal) and cellular responses and protective immunity were assessed. Vaccine formulations containing liposomal ISS-ODN co-administered with either soluble antigen or liposomal antigen (in the same vesicles or in separate vesicles) were up to 30 times more effective than formulations containing un-encapsulated ISS-ODN in inducing: (a) antigen-specific serum and mucosal IgG2a and IgA antibodies; (b) splenocyte proliferative response, cytotoxic activity and IFNgamma production; (c) a DTH response; and (d) protection against virus challenge. The response was Th1-dominant in the influenza model and a mixed Th1+Th2 response in the hepatitis B model. No adverse reactions were noted. Thus, liposomal encapsulation of ISS-ODN further enhances its inherent adjuvant activity.

摘要

含有免疫刺激序列的合成寡脱氧核苷酸(ODN,也称为CpG - ODN)已在实验模型中显示,在与多种抗原进行肠胃外或粘膜共同给药时,具有强大的偏向Th1的免疫佐剂活性。为了增强佐剂活性,并减少给药剂量和次数,采用简单快速(5分钟)的程序,将ISS - ODN包裹(包封效率高达90%)在大的(1.5微米)多层脂质体中。用亚单位流感疫苗(由病毒血凝素和神经氨酸酶组成,即HN)或乙肝表面抗原颗粒(HBsAg)对小鼠进行一次或两次肌肉注射(i.m.)或鼻内注射(i.n.),疫苗可以是未包封的或脂质体包封的,同时伴有游离的或脂质体包裹的ISS - ODN(每剂量5 - 25微克)。在接种疫苗后3 - 12周,评估体液(全身和粘膜)和细胞反应以及保护性免疫。含有脂质体包裹的ISS - ODN与可溶性抗原或脂质体抗原共同给药(在同一囊泡或不同囊泡中)的疫苗制剂,在诱导以下方面的效果比含有未包封的ISS - ODN的制剂高30倍:(a)抗原特异性血清和粘膜IgG2a及IgA抗体;(b)脾细胞增殖反应、细胞毒性活性和IFNγ产生;(c)迟发型超敏反应(DTH);(d)针对病毒攻击的保护作用。在流感模型中,反应以Th1为主,而在乙肝模型中则是Thl + Th2混合反应。未观察到不良反应。因此,脂质体包裹ISS - ODN进一步增强了其固有的佐剂活性。

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