Tannic Acid, as a Structural Moiety Coupled to a Protein Antigen, Exhibiting a Molecular-structure Adjuvant Activity for Antibody Specificity Enhancement

Author:

Castillo-Maldonado Irais1ORCID,Pedroza-Escobar David1ORCID,Molina-Ramírez Brenda1ORCID,Cabral-Hipólito Nidia1ORCID,Delgadillo-Guzmán Dealmy2ORCID,Meza-Velázquez Rocío3ORCID,Ramírez-Moreno Agustina4ORCID,Flores-Loyola Erika4ORCID,Ruíz-Flores Pablo5ORCID,Cruz Jorge Haro-Santa5ORCID,Espino-Silva Perla-Karina5ORCID,Avalos-Soto Joaquín6ORCID,Téllez-López Miguel-Ángel6ORCID,Vertti Rubén Daniel Arellano Pérez7ORCID,Rosales-González Manuel-Gerardo8ORCID

Affiliation:

1. Department of Biochemistry, Biomedical Research Centre, Faculty of Medicine, Universidad Autonoma de Coahuila, Unidad Torreon, Torreon, Mexico

2. Department of Pharmacology, Faculty of Medicine, Universidad Autonoma de Coahuila, Unidad Torreon, Torreon, Mexico

3. Department of Research, FACSA, Universidad Juarez del Estado de Durango, Gomez Palacio, Palacio, Mexico

4. Faculty of Biological Sciences, Universidad Autonoma de Coahuila Unidad Torreon, Torreon, Mexico

5. Department of Genetics, Biomedical Research Centre, Faculty of Medicine, Universidad Autonoma de Coahuila, Unidad Torreon, Torreon, Mexico

6. Cuerpo Academico Farmacia y Productos Naturales, Facultad de Ciencias Quimicas, Universidad Juarez del Estado de Durango, Gomez Palacio, Palacio, Mexico

7. Facultad de Medicina Torreon, Universidad Autonoma de Coahuila, Coahuila, Mexico

8. Facultad de Ciencias de la Salud, Universidad Juarez del Estado de Durango, Gomez Palacio, Palacio, Mexico

Abstract

Background: An antigen is a small foreign substance, such as a microorganism structural protein, that may trigger an immune response once inside the body. Antigens are preferentially used rather than completely attenuated microorganisms to develop safe vaccines. Unfortunately, not all antigens are able to induce an immune response. Thus, new adjuvants to enhance the antigen’s ability to stimulate immunity must be developed. Objectives: Therefore, this work aimed to evaluate the molecular-structure adjuvant activity of tannic acid (TA) coupled to a protein antigen in Balb/c mice. Method: Bovine serum albumin (BSA) was used as an antigen. The coupling of BSA and TA was mediated by carbodiimide crosslinking, and verified by SDS-PAGE. Forty-two Balb/c mice were divided into seven groups, including two controls without antigen, an antigen control, an adjuvant control, and two treatment groups. An additional group was used for macrophages isolation. A 30-day scheme was used to immunize the mice. The analysis of humoral immunity included immunoglobulin quantification, isotyping and antigen-antibody precipitation. The analysis of cell-mediated immunity included the quantification of nitric oxide from peritoneal macrophages and splenocytes’ proliferation assay after treatment stimulation. Results: No differences were found in the antibodies’ concentration or isotypes induced with the conjugate or the pure BSA. However, an immunogenicity improvement (p < 0.05) was observed through the specific anti-BSA antibody titers in mice immunized with the conjugate. Besides, macrophage activation (p < 0.05) was detected when stimulated with the treatments containing TA. Conclusion: Tannic acid exhibited macrophages’ activation properties. Moreover, when TA was incorporated into the structure of a protein antigen, such as BSA, an antibody specificity enhancement was observed. This was a consequence of antigen processing by activated antigen-presenting cells. These results showed the use of tannic acid as a novel candidate for vaccine molecular-structure adjuvant.

Publisher

Bentham Science Publishers Ltd.

Subject

Biochemistry,General Medicine,Structural Biology

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