Abstract
Immunization is the most effective way to prevent transmission of the hepatitis B virus. However, about one-quarter of hepatitis B vaccinees (HepB vaccinees) aged around 18 years have lost their immune memory. What is responsible for the loss? Five subjects who became asymptomatic HBsAg carriers after anti-HBs seroconversion and ten controls who were negative for both HBsAg and anti-HBs were recruited from individuals born in 1987 and vaccinated at birth. scRNA-seq was performed on peripheral blood mononuclear cells, including library preparation, sequencing, quality control and filtering, normalization, dimensionality reduction, clustering, cell type annotation, differential expression analysis and trajectory analysis. Twelve cell types and nine subpopulations of T cells were identified. No significant differences in the proportions of cell types and subpopulations were found between cases and controls. The expression levels of immune memory-related genes, IL7R in total T cells and BACH2 in naive CD4+ T cells and naive CD8+ T cells, were significantly downregulated in the cases (p = 2.2 × 10(-308), 3.31 × 10(-27) and 9.41 × 10(-100), respectively). IL7R is expressed throughout cellular development, while BACH2 is expressed only in the early stage of cellular development. Downregulation of the IL7R and BACH2 in T cells is associated with immune memory loss, identifying them as candidate genes for future functional studies to explore their potential role in the loss of immune memory. This could inform adjuvant design if a causal mechanism is firmly established.