AI Article Synopsis

  • Bovine tuberculosis is a widespread disease in cattle caused by specific bacteria, despite control efforts.
  • Researchers utilized high-throughput RNA sequencing to analyze the genetic responses in cattle blood samples before and after infection, focusing on various time points.
  • The study identified a 19-gene biosignature that increases in expression from one week to twelve weeks post-infection, which may serve as potential biomarkers for diagnosing the disease.

Article Abstract

Bovine tuberculosis, caused by infection with members of the complex, particularly , is a major endemic disease affecting cattle populations worldwide, despite the implementation of stringent surveillance and control programs in many countries. The development of high-throughput functional genomics technologies, including RNA sequencing, has enabled detailed analysis of the host transcriptome to infection, particularly at the macrophage and peripheral blood level. In the present study, we have analysed the transcriptome of bovine whole peripheral blood samples collected at -1 week pre-infection and +1, +2, +6, +10, and +12 weeks post-infection time points. Differentially expressed genes were catalogued and evaluated at each post-infection time point relative to the -1 week pre-infection time point and used for the identification of putative candidate host transcriptional biomarkers for infection. Differentially expressed gene sets were also used for examination of cellular pathways associated with the host response to infection, construction of gene interaction networks enriched for host differentially expressed genes, and time-series analyses to identify functionally important groups of genes displaying similar patterns of expression across the infection time course. A notable outcome of these analyses was identification of a 19-gene transcriptional biosignature of infection consisting of genes increased in expression across the time course from +1 week to +12 weeks post-infection.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8193354PMC
http://dx.doi.org/10.3389/fvets.2021.662002DOI Listing

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