Cholera toxin B subunit modulation of mucosal vaccines for infectious and autoimmune diseases.

William Langridge, Béla Dénes, István Fodor
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Abstract

Parenteral vaccination is generally considered to be the most effective form of therapy for protection against infectious diseases. In recent years, vaccination at mucosal surfaces and combinatorial vaccination strategies that link immunostimulatory molecules to antigens have been developed to enhance vaccine efficacy. Prominent among immunological enhancement strategies are the bacterial A and B toxins, which include the cholera toxin (CT)A and CTB subunits. In contrast to the toxic CTA subunit, the non-toxic CTB subunit displays both carrier and immunostimulatory properties. When linked to pathogen antigens, CTB can impart immunostimulatory properties that are characteristic of the linked antigen. Vaccination strategies have also been broadened to include 'self' proteins applied for the immunological suppression of autoimmunity. When CTB is linked to an autoantigen, the outcome might be considered paradoxical. In type 1 diabetes, self proteins become strongly immunosuppressive, while cancer CTB-autoantigen fusion proteins may exert a strong inflammatory response. This review discusses the immunostimulatory and immunosuppressive roles played by the CTB subunit in vaccine protection and therapy against infectious and autoimmune diseases.

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霍乱毒素B亚基对传染性和自身免疫性疾病粘膜疫苗的调节作用。
一般认为,注射疫苗是预防传染病最有效的治疗方式。近年来,在粘膜表面接种疫苗和将免疫刺激分子与抗原联系起来的组合接种策略已经被开发出来,以提高疫苗的效力。在免疫增强策略中突出的是细菌A和B毒素,其中包括霍乱毒素(CT)A和CTB亚基。与有毒的CTA亚基相反,无毒的CTB亚基同时具有载体和免疫刺激特性。当与病原体抗原连接时,CTB可以赋予免疫刺激特性,这是连接抗原的特征。疫苗接种策略也已扩大到包括用于免疫抑制自身免疫的“自身”蛋白质。当CTB与自身抗原连接时,结果可能被认为是矛盾的。在1型糖尿病中,自身蛋白具有强烈的免疫抑制作用,而癌症ctb -自身抗原融合蛋白可能会产生强烈的炎症反应。本文综述了CTB亚基在疫苗保护和治疗感染性和自身免疫性疾病中的免疫刺激和免疫抑制作用。
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