Lymphatic System and Diseases Open access Peer reviewed

New therapeutic targets in treatment of post-traumatic lymphedema

Felix Reinkemeier, Alexander Wolff, Alexander Fiedler, Christoph Wallner and 8 more

European journal of medical research | Jul 3, 2026

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Integrated human tissue profiling supports the view that chronic post-traumatic lymphedema is a selectively sustained inflammatory–fibrotic state rather than a purely mechanical disorder, suggesting stage-adapted therapeutic avenues that are prospectively testable.

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Abstract Post-traumatic lymphedema is often managed as a mechanical drainage problem. We asked whether the chronic condition reflects a selectively sustained inflammatory–fibrotic state. Skin from patients with manifest post-traumatic lymphedema ( n = 23, typically 1–2 years post-injury) and controls ( n = 10) underwent quantitative immunohistochemistry (% marker-positive cells per standardized dermal ROI) and Luminex multiplex profiling (technical duplicates; two-tailed statistics after Shapiro–Wilk). Lymphedema tissue showed depressed lymphatic endothelial signaling: lower LYVE-1 and podoplanin (each q < 0.001) and reduced VEGFR-3 ( q < 0.001) versus controls; myeloperoxidase was also lower ( q < 0.05), while lipoxygenase was unchanged. Luminex revealed a selective pro-inflammatory core (IL-1β q < 0.05, IL-6 q < 0.01, TNF-α q < 0.01), with no differences in IL-4, IL-10, IL-12p40, IL-13, IL-17A, or RANTES/CCL5. Chemotactic cues were increased (MCP-1 q < 0.01, MIP-1α q < 0.01), aligning with monocyte/macrophage recruitment. Fibrosis-linked growth factors were upregulated (TGF-β1/β2/β3 each q < 0.01; PDGF-AA q < 0.05), while PDGF-BB was unchanged. Together, histology and soluble profiling converge on three axes—innate inflammatory drive, myeloid chemotaxis, and fibrotic remodeling—co-existing with suppressed lymphangiogenic tone. In this cohort, integrated human tissue profiling supports the view that chronic post-traumatic lymphedema is a selectively sustained inflammatory–fibrotic state rather than a purely mechanical disorder, suggesting stage-adapted therapeutic avenues that are prospectively testable.

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Authors

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Felix Reinkemeier

first | BG University Hospital Bergmannsheil Bochum | ORCID 0000-0003-2265-725X

Alexander Wolff

middle | BG University Hospital Bergmannsheil Bochum

Alexander Fiedler

middle | BG University Hospital Bergmannsheil Bochum

Christoph Wallner

middle | BG University Hospital Bergmannsheil Bochum | ORCID 0000-0002-4707-5056

Marius Drysch

middle | BG University Hospital Bergmannsheil Bochum

Sonja Verena Schmidt

middle | BG University Hospital Bergmannsheil Bochum | ORCID 0009-0000-3841-9067

Flemming Puscz

middle | BG University Hospital Bergmannsheil Bochum | ORCID 0000-0002-3599-9243

Maria Füth

middle | BG University Hospital Bergmannsheil Bochum

Carsten Theiß

middle | Ruhr University Bochum | ORCID 0000-0001-7983-0143

Marcus Lehnhardt

middle | BG University Hospital Bergmannsheil Bochum

Björn Behr

middle | Essen University Hospital

Johannes Maximilian Wagner

last | Essen University Hospital | ORCID 0000-0001-6890-4290

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BibTeX

@article{Reinkemeier2026therapeutic,
  title = {New therapeutic targets in treatment of post-traumatic lymphedema},
  author = {Felix Reinkemeier and Alexander Wolff and Alexander Fiedler and Christoph Wallner and Marius Drysch and Sonja Verena Schmidt and Flemming Puscz and Maria Füth and Carsten Theiß and Marcus Lehnhardt and Björn Behr and Johannes Maximilian Wagner},
  journal = {European journal of medical research},
  year = {2026},
  doi = {10.1186/s40001-026-04829-4},
  url = {https://doi.org/10.1186/s40001-026-04829-4}
}

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