Experimental cell research

How making rabbit joint cells immortal changes their production of enzymes that break down tissue

Updated

Abstract

In HIG-82 cells, the induction of stromelysin and collagenase mRNAs occurred faster compared to primary synovial fibroblasts.

  • Both autocrine factors and phorbol myristate acetate (PMA) led to quicker mRNA induction for collagenase and stromelysin in HIG-82 cells than in primary cells.
  • HIG-82 cells showed partial resistance to inhibition by cycloheximide, unlike primary cells.
  • Increased levels of c-fos and c-jun mRNAs were observed in both cell types, but the increase in c-jun was significantly greater and sustained in HIG-82 cells.
  • AP-1 binding activity was enhanced by both inducers in both cell types, with primary cells showing sensitivity to cycloheximide while HIG-82 cells demonstrated only partial sensitivity.
  • Antisense oligonucleotides targeting c-fos and c-jun inhibited stromelysin mRNA induction in primary cells but had limited effectiveness in HIG-82 cells, suggesting alternative pathways may be involved.

Simplified

Full Text

Full text is available at the source.

what lands in your inbox each week:

  • 📚7 fresh studies
  • 📝plain-language summaries
  • direct links to original studies
  • 🏅top journal indicators
  • 📅weekly delivery
  • 🧘‍♂️always free