Litcius/Paper detail

Organ-specific features of human kidney lymphatics are disrupted in chronic transplant rejection

Daniyal J. Jafree, Benjamin J. Stewart, Karen Price, Maria Kolatsi‐Joannou, C Laroche, Barian Mohidin, Benjamin Davis, Hannah Mitchell, Lauren G. Russell, Lucía Marinas del Rey, Chun Jing Wang, William J. Mason, Byung Il Lee, Lauren Heptinstall, Ayshwarya Subramanian, Gideon Pomeranz, Dale Moulding, Laura Wilson, Tahmina Wickenden, Saif Malik, Natalie Holroyd, Claire Walsh, Jennifer C. Chandler, Kevin Cao, Paul J.D. Winyard, Adrian S. Woolf, Marc Aurel Busche, Simon Walker‐Samuel, Lucy S. K. Walker, Tessa Crompton, Peter Scambler, Reza Motallebzadeh, Menna R. Clatworthy, David A. Long

2025Journal of Clinical Investigation10 citationsDOIOpen Access PDF

Abstract

Lymphatic vessels maintain tissue fluid homeostasis and modulate inflammation, yet their spatial organization and molecular identity in the healthy human kidney, and how these change during chronic transplant rejection, remain poorly defined. Here, we show that lymphatic capillaries initiate adjacent to cortical kidney tubules and lack smooth muscle coverage. These vessels exhibit an organ-specific molecular signature, enriched for CCL14, DNASE1L3, and MDK, with limited expression of canonical immune-trafficking markers found in other organ lymphatics, such as LYVE1 and CXCL8. In allografts with chronic mixed rejection, lymphatics become disorganized and infiltrate the medulla, with their endothelial junctions remodeling from a button-like to a continuous, zipper-like, architecture. Lymphatics in rejecting kidneys localize around and interconnect tertiary lymphoid structures at different maturation stages, with altered intralymphatic and perilymphatic CD4+ T cell distribution. The infiltrating T cells express IFN-γ, which upregulates coinhibitory ligands in lymphatic endothelial cells, including PVR and LGALS9. Simultaneously, lymphatics acquire HLA class II expression and exhibit C4d deposition, consistent with alloantibody binding and complement activation. Together, these findings define the spatial and molecular features of human kidney lymphatics, revealing tolerogenic reprogramming accompanied by structural perturbations during chronic transplant rejection.

Topics & Concepts

Lymphatic systemKidneyKidney transplantationPathologyMedicineOrgan transplantationGraft rejectionTransplant rejectionImmunologyTransplantationBiologyImmune systemInternal medicineGenetic Syndromes and ImprintingLymphatic Disorders and TreatmentsGenetic and Kidney Cyst Diseases