Tolerability and effect of inhibiting microfibrillar-associated protein 4 in small intestinal anastomotic healing

  1. Rasmus Refshauge Andresen
  2. Jesper Brandt Pedersen
  3. Paula Frederikke Hellsegg Grünfeld
  4. Charlotte Skoie Nielsen
  5. Anna Lings Kjelgaard
  6. Anders Frederik Højer Kolind
  7. Nils Grimm
  8. Kasper Emil Rosenbech
  9. Henriette Kirkeby Høiberg
  10. Johanne Kalland
  11. Mie Dilling
  12. Gunvor Iben Madsen
  13. Anders Schlosser
  14. Lasse Bach Steffensen
  15. Hans Christian Beck
  16. Sören Möller
  17. Niels Qvist
  18. Mark Bremholm Ellebaek
  19. Grith Lykke Sorensen
Read the full article See related articles

Listed in

This article is not in any list yet, why not save it to one of your lists.
Log in to save this article

Abstract

Background Crohn’s disease often leads to strictures due to excessive extracellular matrix deposition and smooth muscle cell hyperplasia. Current stricture treatments include surgical and endoscopic interventions, but high recurrence rates remain a challenge. Microfibrillar-associated protein 4 (MFAP4) contributes to fibrosis in various tissues. The anti-MFAP4 antibody was evaluated for its tolerability and anti-fibrotic efficacy on small intestinal anastomotic healing in pig models. Methods Two small intestinal anastomoses were made in 45 pigs. Fibrosis was induced using aethoxysklerol injections. Each anastomosis was locally injected with either anti-MFAP4, positive control anakinra (interleukin-1 receptor antagonist) or negative vehicle control. Tolerability of anti-MFAP4 was observed across three observation durations (5, 10, and 28 days) and assessed by weight gain, anastomotic tissue strength, and histological evaluation. Anti-fibrotic efficacy was tested using semi-quantitative collagen scoring from the 28-days study. Proteome analysis of tissue sections was applied for mechanistic analyses. Results Local anastomotic injections of 16 mg and 32 mg anti-MFAP4 were well tolerated. Anastomotic fibrosis was significantly reduced both by positive control anakinra-treatment and anti-MFAP4-treatment. Anti-MFAP4 reduced fibrosis by 23% relative to the negative control. Gene ontology term analysis showed up-regulation of muscle cell contractile apparatus and down-regulation of transcription and translation in the anti-MFAP4 group. Conclusions The data supported that anti-MFAP4-treatment induced smooth muscle cell switching from the synthetic phenotype involved in fibrosis to the contractile phenotype essential for homeostatic gut motor activity. Anti-MFAP4 has potential as treatment of Crohn’s patients at risk of developing fibrostenosis and as a prophylactic treatment to support post-surgical anastomotic healing.

Article activity feed

  1. Version published to 10.21203/rs.3.rs-7132995/v1 on Research Square