Exosome-transmitted microRNA-323a-3p participated in the occurrence of Hirschsprung’s disease

Key Points

• This research aims to assess the role of exosomal microRNA-323a-3p in Hirschsprung's disease and its effect on ENCC-derived cell function.
• Identified upregulation of exosomal miR-323a-3p in Hirschsprung's disease samples.
• Evaluated the impact on ENCC-derived cell function.
• Investigated the potential involvement of TET2 pathways.
• Exosomal microRNA-323a-3p is significantly upregulated in Hirschsprung's disease.
• Impaired ENCC-derived cell function is associated with increased levels of miR-323a-3p.
• miR-323a-3p shows promise as a potential diagnostic biomarker for Hirschsprung's disease.