Early immune responses and parasite tissue distribution in mice experimentally infected with oocysts of either archetypal or non-archetypal genotypes of


Journal

Parasitology
ISSN: 1469-8161
Titre abrégé: Parasitology
Pays: England
ID NLM: 0401121

Informations de publication

Date de publication:
04 2021
Historique:
pubmed: 15 12 2020
medline: 28 9 2021
entrez: 14 12 2020
Statut: ppublish

Résumé

In most of the world Toxoplasma gondii is comprised of archetypal types (types I, II and III); however, South America displays several non-archetypal strains. This study used an experimental mouse model to characterize the immune response and parasite kinetics following infection with different parasite genotypes. An oral inoculation of 50 oocysts per mouse from T. gondii M4 type II (archetypal, avirulent), BrI or BrIII (non-archetypal, virulent and intermediate virulent, respectively) for groups (G)2, G3 and G4, respectively was used. The levels of mRNA expression of cytokines, immune compounds, cell surface markers and receptor adapters [interferon gamma (IFNγ), interleukin (IL)-12, CD8, CD4, CD25, CXCR3 and MyD88] were quantified by SYBR green reverse transcription-quantitative polymerase chain reaction. Lesions were characterized by histology and detection by immunohistochemistry established distribution of parasites. Infection in G2 mice was mild and characterized by an early MyD88-dependent pathway. In G3, there were high levels of expression of pro-inflammatory cytokines IFNγ and IL-12 in the mice showing severe clinical symptoms at 8–11 days post infection (dpi), combined with the upregulation of CD25, abundant tachyzoites and tissue lesions in livers, lungs and intestines. Significant longer expression of IFNγ and IL-12 genes, with other Th1-balanced immune responses, such as increased levels of CXCR3 and MyD88 in G4, resulted in survival of mice and chronic toxoplasmosis, with the occurrence of tissue cysts in brain and lungs, at 14 and 21 dpi. Different immune responses and kinetics of gene expression appear to be elicited by the different strains and non-archetypal parasites demonstrated higher virulence.

Identifiants

pubmed: 33315001
doi: 10.1017/S0031182020002346
pii: S0031182020002346
doi:

Substances chimiques

Antigens, CD 0
Cxcr3 protein, mouse 0
Cytokines 0
DNA, Complementary 0
DNA, Protozoan 0
Myeloid Differentiation Factor 88 0
RNA, Protozoan 0
Receptors, CXCR3 0

Types de publication

Journal Article Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

IM

Pagination

464-476

Auteurs

Daniela P Chiebao (DP)

Department of Preventive Veterinary Medicine, Faculty of Veterinary Medicine and Animal Science - FMVZ, University of Sao Paulo, 87 Professor Doutor Orlando Marques de Paiva Avenue, 05508-270São Paulo, Brazil.

Paul M Bartley (PM)

Moredun Research Institute, Pentland Science Park, Bush Loan, EdinburghEH26 0PZ, UK.

Francesca Chianini (F)

Moredun Research Institute, Pentland Science Park, Bush Loan, EdinburghEH26 0PZ, UK.

Lauren E Black (LE)

Moredun Research Institute, Pentland Science Park, Bush Loan, EdinburghEH26 0PZ, UK.

Alison Burrells (A)

Moredun Research Institute, Pentland Science Park, Bush Loan, EdinburghEH26 0PZ, UK.

Hilda F J Pena (HFJ)

Department of Preventive Veterinary Medicine, Faculty of Veterinary Medicine and Animal Science - FMVZ, University of Sao Paulo, 87 Professor Doutor Orlando Marques de Paiva Avenue, 05508-270São Paulo, Brazil.

Rodrigo M Soares (RM)

Department of Preventive Veterinary Medicine, Faculty of Veterinary Medicine and Animal Science - FMVZ, University of Sao Paulo, 87 Professor Doutor Orlando Marques de Paiva Avenue, 05508-270São Paulo, Brazil.

Elisabeth A Innes (EA)

Moredun Research Institute, Pentland Science Park, Bush Loan, EdinburghEH26 0PZ, UK.

Frank Katzer (F)

Moredun Research Institute, Pentland Science Park, Bush Loan, EdinburghEH26 0PZ, UK.

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Classifications MeSH