CD47 prevents the elimination of diseased fibroblasts in scleroderma
Tristan Lerbs, … , Tyler Shibata, Gerlinde Wernig
Tristan Lerbs, … , Tyler Shibata, Gerlinde Wernig
Published August 20, 2020
Citation Information: JCI Insight. 2020;5(16):e140458. https://doi.org/10.1172/jci.insight.140458.
View: Text | PDF
Research Article Dermatology

CD47 prevents the elimination of diseased fibroblasts in scleroderma

Abstract

Scleroderma is a devastating fibrotic autoimmune disease. Current treatments are partly effective in preventing disease progression but do not remove fibrotic tissue. Here, we evaluated whether scleroderma fibroblasts take advantage of the “don’t-eat-me-signal” CD47 and whether blocking CD47 enables the body’s immune system to get rid of diseased fibroblasts. To test this approach, we used a Jun-inducible scleroderma model. We first demonstrated in patient samples that scleroderma upregulated transcription factor JUN and increased promoter accessibilities of both JUN and CD47. Next, we established our scleroderma model, demonstrating that Jun mediated skin fibrosis through the hedgehog-dependent expansion of CD26+Sca1– fibroblasts in mice. In a niche-independent adaptive transfer model, JUN steered graft survival and conferred increased self-renewal to fibroblasts. In vivo, JUN enhanced the expression of CD47, and inhibiting CD47 eliminated an ectopic fibroblast graft and increased in vitro phagocytosis. In the syngeneic mouse, depleting macrophages ameliorated skin fibrosis. Therapeutically, combined CD47 and IL-6 blockade reversed skin fibrosis in mice and led to the rapid elimination of ectopically transplanted scleroderma cells. Altogether, our study demonstrates the efficiency of combining different immunotherapies in treating scleroderma and provides a rationale for combining CD47 and IL-6 inhibition in clinical trials.

Authors

Tristan Lerbs, Lu Cui, Megan E. King, Tim Chai, Claire Muscat, Lorinda Chung, Ryanne Brown, Kerri Rieger, Tyler Shibata, Gerlinde Wernig

×

Figure 7

Combined CD47/IL-6 inhibition reverses skin fibrosis.

Options: View larger image (or click on image) Download as PowerPoint
Combined CD47/IL-6 inhibition reverses skin fibrosis. (A) Schematic outl...
(A) Schematic outline of the therapeutic trial. (B) Representative H&E and trichrome stains of the different groups. Scale bar: 500 μm. n = 4. (C) Hydroxyproline content of the skin. Tukey’s multiple comparison test. *P < 0.05; **P < 0.01. n = 6. Graph bars represent means with standard deviations. (D) Amount of fat tissue. Values indicate μm2/μm skin width. Tukey’s multiple comparison test. *P < 0.05. n = 8. Graph bars represent means with standard deviations. (E) Representative optical images of ectopically transplanted GFP/luciferase-labeled human scleroderma fibroblasts ± CD47/IL-6 inhibition. (F) Optical imaging of explanted kidneys on day 5. (G) Quantification of photon emissions of explanted kidney grafts normalized to the values of the untreated mice. Two-sided t test. *P < 0.05. n = 3–4. Bars represent means with standard deviations. (H) Corresponding caspase-3 staining of kidney grafts. Scale bar: 25 μm. (I) Corresponding percentage of caspase-3+GFP+ fibroblasts. Two-sided t test. **P < 0.01. n = 4–5. Bars represent means with standard deviations.