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Spatiotemporal dynamics and heterogeneity of renal lymphatics in mammalian development and cystic kidney disease.

Daniyal J JafreeDale MouldingMaria Kolatsi-JoannouNuria Perretta TejedorKaren L PriceNatalie J MilmoeClaire L WalshRosa Maria CorreraPaul Jd WinyardPeter C HarrisChristiana RuhrbergSimon Walker-SamuelPaul R RileyAdrian S WoolfPeter J ScamblerDavid A Long
Published in: eLife (2019)
Heterogeneity of lymphatic vessels during embryogenesis is critical for organ-specific lymphatic function. Little is known about lymphatics in the developing kidney, despite their established roles in pathology of the mature organ. We performed three-dimensional imaging to characterize lymphatic vessel formation in the mammalian embryonic kidney at single-cell resolution. In mouse, we visually and quantitatively assessed the development of kidney lymphatic vessels, remodeling from a ring-like anastomosis under the nascent renal pelvis; a site of VEGF-C expression, to form a patent vascular plexus. We identified a heterogenous population of lymphatic endothelial cell clusters in mouse and human embryonic kidneys. Exogenous VEGF-C expanded the lymphatic population in explanted mouse embryonic kidneys. Finally, we characterized complex kidney lymphatic abnormalities in a genetic mouse model of polycystic kidney disease. Our study provides novel insights into the development of kidney lymphatic vasculature; a system which likely has fundamental roles in renal development, physiology and disease.
Keyphrases
  • lymph node
  • endothelial cells
  • single cell
  • mouse model
  • poor prognosis
  • high resolution
  • gene expression
  • genome wide
  • photodynamic therapy
  • binding protein