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Group B Streptococcus Capsular Polysaccharide-Cholera Toxin B Subunit Conjugate Vaccines Prepared by Different Methods for Intranasal Immunization

机译:不同方法制备的B组链球菌荚膜多糖-霍乱毒素B亚单位结合疫苗

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Group B Streptococcus (GBS) type III capsular polysaccharide (CPS III) was conjugated to recombinant cholera toxin B subunit (rCTB) using three different methods which employed (i) cystamine and N-succinimidyl-3-(2-pyridyldithio)propionate (SPDP), (ii) carbodiimide with adipic acid dihydrazide (ADH) as a spacer, or (iii) reductive amination (RA). The CPS III-rCTB conjugates were divided into large- and small-molecular-weight (M r) fractions, and the immunogenicities of the different preparations after intranasal (i.n.) immunization were studied in mice. Both large- and small-M rconjugates of CPS III-rCTBRA or CPS III-rCTBADHinduced high, almost comparable levels of CPS-specific immunoglobulin G (IgG) in serum, lungs, and vagina that were generally superior to those obtained with CPS III-rCTBSPDP conjugates or a CPS III and rCTB mixture. However, the smaller-M rconjugates of CPS III-rCTBRA or CPS III-rCTBADHin most cases elicited a lower anti-CPS IgA immune response than the large-M r conjugates, and the highest anti-CPS IgA titers in both tissues and serum were obtained with the large-M r CPS III-rCTBRA conjugate. Serum IgG anti-CPS titers induced by the CPS III-rCTBRAconjugate had high levels of specific IgG1, IgG2a, IgG2b, and IgG3 antibodies. Based on the effectiveness of RA for coupling CPS III to rCTB, RA was also tested for conjugating GBS CPS Ia with rCTB. As for the CPS III-rCTB conjugates, the immunogenicity of CPS Ia was greatly increased by conjugation to rCTB. Intranasal immunization with a combination of CPS Ia-rCTB and CPS III-rCTB conjugates was shown to induce anti-CPS Ia and III immune responses in serum and lungs that were fully comparable with the responses to immunization with the monovalent CPS Ia-rCTB or CPS III-rCTB conjugates. These results suggest that the GBS CPS III-rCTB and CPS Ia-rCTB conjugates prepared by the RA method may be used in bivalent and possibly also in multivalent mucosal GBS conjugate vaccines.
机译:使用三种不同的方法,将B组链球菌(GBS)III型荚膜多糖(CPS III)与重组霍乱毒素B亚基(rCTB)偶联,所述方法采用(i)胱胺和 N M r )组分,鼻内免疫后不同制剂的免疫原性在小鼠中进行了研究。 CPS III-rCTB RA 或CPS III-rCTB ADH 诱导的大和小 M r 共轭物高,几乎可比较的血清,肺和阴道中CPS特异性免疫球蛋白G(IgG)水平,通常优于CPS III-rCTB SPDP 偶联物或CPS III和rCTB混合物获得的水平。但是,大多数情况下,CPS III-rCTB RA 或CPS III-rCTB ADH 的较小 M r 结合物病例引起的抗CPS IgA免疫应答低于大的 M r 结合物,并且在较大的组织和血清中获得的抗CPS IgA滴度最高- M r CPS III-rCTB RA 共轭物。 CPS III-rCTB RA 偶联物诱导的血清IgG抗CPS滴度具有高水平的特异性IgG1,IgG2a,IgG2b和IgG3抗体。基于RA将CPS III与rCTB偶联的有效性,还测试了RA与rCTB偶联GBS CPS Ia。对于CPS III-rCTB缀合物,通过与rCTB的结合大大提高了CPS Ia的免疫原性。已证明结合CPS Ia-rCTB和CPS III-rCTB结合物进行鼻内免疫可诱导血清和肺中抗CPS Ia和III免疫反应,与单价CPS Ia-rCTB或CPS免疫反应完全可比III-rCTB共轭物。这些结果表明,通过RA方法制备的GBS CPS III-rCTB和CPS Ia-rCTB结合物可以用于二价甚至可能用于多价粘膜GBS结合物疫苗。

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