Abstract
Cell-mediated immune responses to Mycobacterium avium subsp. paratuberculosis (MAP) are regulated by various types of T lymphocytes. The aim of this study was to quantitate T cell subsets in the mid-ileum of cows naturally infected with MAP to identify differences during different stages of infection, and to determine whether these subsets could be used as predictors of disease state. Immunofluorescent labeling of T cell subsets and macrophages was performed on frozen mid-ileal tissue sections archived from naturally infected dairy cows in either subclinical or clinical disease status, and noninfected control cows. Comprehensive IF staining for CD4, CD8α, TcR1-N24 (gamma delta), FoxP3, CXCR3 and CCR9 served to define T cell subsets and was correlated with macrophages present. Clinically affected cows demonstrated significantly higher numbers of CXCR3+ (Th1-type) and CCR9+ (total small intestinal lymphocytes) cells at the site of infection compared to the subclinical cows and noninfected controls. Further, predictive modeling indicated a significant interaction between CXCR3+ and AM3K+ (macrophages) cells, suggesting that progression to clinical disease state aligns with increased numbers of these cell types at the site of infection. The ability to predict disease state with this model was improved from previous modeling using immunofluorescent macrophage data. Predictive modelling indicated an interaction between CXCR3+ and AM3K+ cells, which could more sensitively detect subclinical cows compared to clinical cows. It may be possible to use this knowledge to improve and develop an assay to detect subclinically infected animals with more confidence during the early stages of the disease.
Highlights
Johne’s disease (JD) is a chronic gastroenteritis of ruminants caused by Mycobacterium avium subspecies paratuberculosis (MAP)
Upon infection with MAP, infected animals enter into an often-protracted subclinical stage of infection, which eventually may shift into clinical disease
The mechanism(s) that direct the switch from subclinical to clinical disease is not yet well understood, research to gain a better understanding of host immunity to MAP infection is an important step towards effective control
Summary
Johne’s disease (JD) is a chronic gastroenteritis of ruminants caused by Mycobacterium avium subspecies paratuberculosis (MAP). The initial host response to infection involves a strong cell-mediated immune response, which helps to sustain animals in a state of subclinical disease. Populations of CD4+CD8+FoxP3+ Tregs have been shown to develop in response to low level antigenic stimulation with MAP [4], and the number of F oxP3+ cells increase with increased severity of intestinal lesions [5]. Despite these previous studies, there is little information on how the dynamics of T cell subsets at the site of infection in JD influences disease state. The identification of T cells that strongly influence disease state may be a useful tool to focus research towards improving the diagnosis of Johne’s disease
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