Publications by authors named "Harsha S Krovi"
Article Synopsis
- The "innate-like" T cell compartment, referred to as T, consists of diverse T cells that bridge innate and adaptive immunity and is analyzed using advanced techniques like single-cell RNA sequencing.
- In human blood, most T cells exhibit an effector program driven by unique transcription factors, contrasting with conventional T cells, while varied developmental stages are observed in thymic T cells.
- Unlike mice, human T cells do not form multiple effector subsets but show a mix of type 1 and type 17 effector potential, revealing key differences in immune regulation between species.
The "innate-like" T cell compartment, known as T, represents a diverse group of T cells that straddle the boundary between innate and adaptive immunity, having the ability to mount rapid responses following activation. In mice, this ability is acquired during thymic development. We explored the transcriptional landscape of T compared to conventional T cells (T) in the human thymus and blood using single cell RNA sequencing and flow cytometry.
View Article and Find Full Text PDFImmortalized T cells such as T cell hybridomas, transfectomas, and transductants are useful tools to study tri-molecular complexes consisting of peptide, MHC, and T cell receptor (TCR) molecules. These cells have been utilized for antigen discovery studies for decades due to simplicity and rapidness of growing cells. However, responsiveness to antigen stimulation is typically less sensitive compared to primary T cells, resulting in occasional false negative outcomes especially for TCRs having low affinity to a peptide-MHC complex (pMHC).
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