Cellular and molecular hemocyte responses of the Pacific oyster, Crassostrea gigas, following bacterial infection with Vibrio aestuarianus strain 01/32
[SDE] Environmental Sciences
0301 basic medicine
570
Hemocytes
Vibrio aestuarianus
Colony Count, Microbial
Cell Count
Pathogenesis
03 medical and health sciences
Phagocytosis
Hemolymph
Animals
bivalve immunity
RNA, Messenger
14. Life underwater
Crassostrea
Vibrio
oyster
Oyster
Reverse Transcriptase Polymerase Chain Reaction
Superoxide Dismutase
pathogenesis
600
Tissue Inhibitor of Metalloproteinases
16. Peace & justice
Gene Expression Regulation
Crassostrea gigas
[SDE]Environmental Sciences
Bivalve immunity
Reactive Oxygen Species
Peptide Hydrolases
DOI:
10.1016/j.micinf.2006.07.020
Publication Date:
2006-08-29T12:23:44Z
AUTHORS (6)
ABSTRACT
The strategies used by bacterial pathogens to circumvent host defense mechanisms remain largely undefined in bivalve molluscs. In this study, we investigated experimentally the interactions between the Pacific oyster (Crassostrea gigas) immune system and Vibrio aestuarianus strain 01/32, a pathogenic bacterium originally isolated from moribund oysters. First, an antibiotic-resistant V. aestuarianus strain was used to demonstrate that only a limited number of bacterial cells was detected in the host circulatory system, suggesting that the bacteria may localize in some organs. Second, we examined the host defense responses to V. aestuarianus at the cellular and molecular levels, using flow-cytometry and real-time PCR techniques. We showed that hemocyte phagocytosis and adhesive capabilities were affected during the course of infection. Our results also uncovered a previously-undescribed mechanism used by a Vibrio in the initial stages of host interaction: deregulation of the hemocyte oxidative metabolism by enhancing the production of reactive oxygen species and down-regulating superoxide dismutase (Cg-EcSOD) gene expression. This deregulation may provide an opportunity to the pathogen by impairing hemocyte functions and survival. These findings provide new insights into the cellular and molecular bases of the host-pathogen interactions in C. gigas oyster.
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