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首页> 外文期刊>Vaccine >Intravaginal immunization using the recombinant HIV-1 clade-C trimeric envelope glycoprotein CN54gp140 formulated within lyophilized solid dosage forms
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Intravaginal immunization using the recombinant HIV-1 clade-C trimeric envelope glycoprotein CN54gp140 formulated within lyophilized solid dosage forms

机译:使用重组HIV-1的含有重组HIV-1的CN54GP140在冻干固体剂型中配制的含有重组HIV-1 CN54GP140的静脉内免疫。

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Vaccine-mediated prevention of primary HIV-1 infection at the heterosexual mucosal portal of entry may be facilitated by highly optimised formulations or drug delivery devices for intravaginal (i.vag) immunization. Previously we described hydroxyethylcellulose (HEC)-based theologically structured gel vehicles (RSVs) for vaginal immunization of an HIV-1 vaccine candidate, a soluble recombinant trimeric HIV-1 clade-C envelope glycoprotein designated CN54gp140. Here we investigated the efficacy of lyophilized solid dosage formulations (LSDF5) for prolonging antigen stability and as i.vag delivery modalities. LSDFs were designed and developed that upon i.vag administration they would reconstitute with the imbibing of vaginal fluid to mucoadhesive, site-retentive semi-solids. Mice were immunized with lyophilized equivalents of (i) RSVs, (ii) modified versions of the RSVs more suited to lyophilization (sodium carboxymethyl cellulose (NaCMC)-based gels) and (iii) Carbopol (R) gel, all containing CN54gp140. NaCMC-based LSDFs provided significantly enhanced antigen stability compared to aqueous-based RSVs. Rheological analysis indicated the NaCMC-based LSDFs would offer enhanced vaginal retention in woman compared to more conventional vaginal gel formulations. All LSDFs were well tolerated in the mouse model. Following i.vag administration, all LSDFs boosted systemic CN54gp140-specific antibody responses in sub-cutaneously primed mice. Induction of CN54gp140-specific antibody responses in the female genital tract was evident. Of all the LSDFs the fastest releasing which was lyophilized Carbopol (R) gel elicited immune responses comparable to buffer instillation of antigen suggesting that rather than slower sustained release, initial high burst release from the LSDFs may suffice. The boosting of specific immune responses upon i.vag administration indicates that LSDFs are viable mucosal vaccine delivery modalities promoting antigen stability and facilitating intimate exposure of CN54gp140 to the mucosal-associated lymphoid tissue of the female genital tract
机译:通过高度优化的制剂或药物递送装置,可以通过高度优化的制剂(I.VAG)免疫,促进疫苗介导的预防初级HIV-1感染物中的初级HIV-1感染。以前我们描述了基于HIV-1疫苗候选的阴道免疫的基于神经结构化的凝胶载体(RSV)的羟乙基纤维素(RSV),可溶性重组三聚体HIV-1 CLADE-C包络糖蛋白指定CN54GP140。在这里,我们研究了冻干的固体剂量配方(LSDF5)延长抗原稳定性和I.VAG递送方式的疗效。 LSDFS被设计和开发,在I.VAG管理后,他们将重新将阴道液中的吸收到粘膜粘附,位点保持的半固体。用冻干的等当量免疫小鼠(I)RSVS,(II)改性版本的RSV的改性版本,更适合冻干(羧甲基纤维素(NaCMC)的凝胶,(III)Carbopol(R)凝胶,含有CN54GP140。与基于水性的RSV相比,基于NACC的LSDFS提供显着增强的抗原稳定性。流变分析表明,与更常规的阴道凝胶配方相比,基于NACC的LSDFS将提供增强的阴道保留。所有LSDF都在鼠标模型中耐受良好。遵循I.VAG管理,所有LSDFS在亚颧骨底鼠中提升了全身CN54GP140特异性抗体反应。诱导雌性生殖道中CN54GP140特异性抗体反应明显。在所有LSDFS中最快的释放,即冻干的Carbopol(R)凝胶引发免疫应答与抗原的缓冲液滴注表明,来自LSDFS的初始高爆发释放可能足够。对I.VAG施用的特异性免疫应答的提高表明LSDF是可行的粘膜疫苗递送方式,促进抗原稳定性,并促进CN54GP140的亲密暴露于雌性生殖道的粘膜相关淋巴组织

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