Using an Aluminum Hydroxide-Chitosan Matrix Increased the Vaccine Potential and Immune Response of Mice against Multi-Drug-Resistant <i>Acinetobacter baumannii</i>.

Deusdará, Túllio T; Félix, Mellanie K C; de S Brito, Helio; Cangussu, Edson W S; de S Moura, Wellington; Albuquerque, Benedito; Silva, Marcos G; Dos Santos, Gil R; de Morais, Paula B; da Silva, Elizangela F; Chaves, Yury O; Mariúba, Luis Andre M; Nogueira, Paulo A; Astolfi-Filho, Spartaco; Assunção, Enedina N; Epiphanio, Sabrina; Marinho, Claudio R F; Brandi, Igor V; Viana, Kelvinson F; Oliveira, Eugenio E; Cangussu, Alex Sander R

Using an Aluminum Hydroxide-Chitosan Matrix Increased the Vaccine Potential and Immune Response of Mice against Multi-Drug-Resistant Acinetobacter baumannii.

Deusdará, Túllio T; Félix, Mellanie K C; de S Brito, Helio; Cangussu, Edson W S; de S Moura, Wellington; Albuquerque, Benedito; Silva, Marcos G; Dos Santos, Gil R; de Morais, Paula B; da Silva, Elizangela F; Chaves, Yury O; Mariúba, Luis Andre M; Nogueira, Paulo A; Astolfi-Filho, Spartaco; Assunção, Enedina N; Epiphanio, Sabrina; Marinho, Claudio R F; Brandi, Igor V; Viana, Kelvinson F; Oliveira, Eugenio E; Cangussu, Alex Sander R.

Afiliação

Deusdará TT; Graduate Program for Biodiversity and Biotechnology of Legal Amazon, Federal University of Tocantins, Palmas 77001-090, TO, Brazil.
Félix MKC; Graduate Program for Biodiversity and Biotechnology of Legal Amazon, Federal University of Tocantins, Palmas 77001-090, TO, Brazil.
de S Brito H; Graduate Program for Biodiversity and Biotechnology of Legal Amazon, Federal University of Tocantins, Palmas 77001-090, TO, Brazil.
Cangussu EWS; Graduate Program in Biotechnology, Federal University of Tocantins, Gurupi 77425-000, TO, Brazil.
de S Moura W; Graduate Program for Biodiversity and Biotechnology of Legal Amazon, Federal University of Tocantins, Palmas 77001-090, TO, Brazil.
Albuquerque B; Graduate Program in Biotechnology, Federal University of Tocantins, Gurupi 77425-000, TO, Brazil.
Silva MG; Graduate Program in Biotechnology, Federal University of Tocantins, Gurupi 77425-000, TO, Brazil.
Dos Santos GR; Graduate Program for Biodiversity and Biotechnology of Legal Amazon, Federal University of Tocantins, Palmas 77001-090, TO, Brazil.
de Morais PB; Graduate Program in Biotechnology, Federal University of Tocantins, Gurupi 77425-000, TO, Brazil.
da Silva EF; Graduate Program for Biodiversity and Biotechnology of Legal Amazon, Federal University of Tocantins, Palmas 77001-090, TO, Brazil.
Chaves YO; Instituto Leônidas e Maria Deane, Oswaldo Cruz Foundation-Fiocruz Amazônia, Manaus 69057-070, AM, Brazil.
Mariúba LAM; Instituto Leônidas e Maria Deane, Oswaldo Cruz Foundation-Fiocruz Amazônia, Manaus 69057-070, AM, Brazil.
Nogueira PA; Instituto Leônidas e Maria Deane, Oswaldo Cruz Foundation-Fiocruz Amazônia, Manaus 69057-070, AM, Brazil.
Astolfi-Filho S; Instituto Leônidas e Maria Deane, Oswaldo Cruz Foundation-Fiocruz Amazônia, Manaus 69057-070, AM, Brazil.
Assunção EN; Laboratory of DNA Technology, Biotechnology Department, Multidisciplinary Support Center, Federal University of Amazonas, Manaus 69080-900, AM, Brazil.
Epiphanio S; Laboratory of DNA Technology, Biotechnology Department, Multidisciplinary Support Center, Federal University of Amazonas, Manaus 69080-900, AM, Brazil.
Marinho CRF; Department of Immunology, Biomedical Science Institute, University of São Paulo (USP), São Paulo 05508-060, SP, Brazil.
Brandi IV; Department of Immunology, Biomedical Science Institute, University of São Paulo (USP), São Paulo 05508-060, SP, Brazil.
Viana KF; Institute of Agricultural Sciences, Federal University of Minas Gerais, Montes Claros 39400-310, MG, Brazil.
Oliveira EE; Department of Biotchnology, State University of Montes Claros, Montes Claros 39401-089, MG, Brazil.
Cangussu ASR; Interdisciplinary Center for Life Sciences and Nature, Federal University of Latin American Integration (UNILA), Foz do Iguaçu 85866-000, PR, Brazil.

Vaccines (Basel) ; 11(3)2023 Mar 16.

Article em En | MEDLINE | ID: mdl-36992253

ABSTRACT

ABSTRACT

Acinetobacter baumannii is a Gram-negative, immobile, aerobic nosocomial opportunistic coccobacillus that causes pneumonia, septicemia, and urinary tract infections in immunosuppressed patients. There are no commercially available alternative antimicrobials, and multi-drug resistance is an urgent concern that requires emergency measures and new therapeutic strategies. This study evaluated a multi-drug-resistant A. baumannii whole-cell vaccine, inactivated and adsorbed on an aluminum hydroxide-chitosan (mAhC) matrix, in an A. baumannii sepsis model in immunosuppressed mice by cyclophosphamide (CY). CY-treated mice were divided into immunized, non-immunized, and adjuvant-inoculated groups. Three vaccine doses were given at 0D, 14D, and 28D, followed by a lethal dose of 4.0 × 108 CFU/mL of A. baumannii. Immunized CY-treated mice underwent a significant humoral response, with the highest IgG levels and a higher survival rate (85%); this differed from the non-immunized CY-treated mice, none of whom survived (p < 0.001), and from the adjuvant group, with 45% survival (p < 0.05). Histological data revealed the evident expansion of white spleen pulp from immunized CY-treated mice, whereas, in non-immunized and adjuvanted CY-treated mice, there was more significant organ tissue damage. Our results confirmed the proof-of-concept of the immune response and vaccine protection in a sepsis model in CY-treated mice, contributing to the advancement of new alternatives for protection against A. baumannii infections.

Palavras-chave

Acinetobacter baumannii; immunosuppression model; inactivated whole-cell vaccine; multi-drug-resistant

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Texto completo: 1 Base de dados: MEDLINE Idioma: En Ano de publicação: 2023 Tipo de documento: Article

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