4.7 Article

Mycophenolate Mofetil Treatment of Systemic Sclerosis Reduces Myeloid Cell Numbers and Attenuates the Inflammatory Gene Signature in Skin

Journal

JOURNAL OF INVESTIGATIVE DERMATOLOGY
Volume 138, Issue 6, Pages 1301-1310

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.jid.2018.01.006

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Funding

  1. National Institutes of Health Eunice Kennedy Shriver National Institute of Child Health and Human Development [K12 HD055884]
  2. NIAMS [K23 AR059763, R21 AR068035, P30 AR061920, R56 AR063985, R44 AR061920, T32 GM008704]
  3. Cancer Center Support Grant [NCI CA060553]
  4. Scleroderma Research Foundation
  5. Scleroderma Foundation
  6. Dartmouth Graduate Studies
  7. John Osborn Polak Endowment
  8. Northwestern University Mouse Histology and Phenotyping Laboratory

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Fewer than half of patients with systemic sclerosis demonstrate modified Rodnan skin score improvement during mycophenolate mofetil (MMF) treatment. To understand the molecular basis for this observation, we extended our prior studies and characterized molecular and cellular changes in skin biopsies from subjects with systemic sclerosis treated with MMF. Eleven subjects completed >= 24 months of MMF therapy. Two distinct skin gene expression trajectories were observed across six of these subjects. Three of the six subjects showed attenuation of the inflammatory signature by 24 months, paralleling reductions in CCL2 mRNA expression in skin and reduced numbers of macrophages and myeloid dendritic cells in skin biopsies. MMF cessation at 24 months resulted in an increased inflammatory score, increased CCL2 mRNA and protein levels, modified Rodnan skin score rebound, and increased numbers of skin myeloid cells in these subjects. In contrast, three other subjects remained on MMF >24 months and showed a persistent decrease in inflammatory score, decreasing or stable modified Rodnan skin score, CCL2 mRNA reductions, sera CCL2 protein levels trending downward, reduction in monocyte migration, and no increase in skin myeloid cell numbers. These data summarize molecular changes during MMF therapy that suggest reduction of innate immune cell numbers, possibly by attenuating expression of chemokines, including CCL2.

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