Conclusions

  • We identified a number of mRNA-microRNA pairs that were differentially expressed in patients with IPF in the lowest versus the highest tertile of FVC % predicted.
  • This supports the idea that microRNA regulation may be related to the progression of IPF.
  • Ongoing studies will assess whether circulating microRNAs and their related mRNAs are associated with a greater risk of disease progression in patients with IPF.
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