Lymphatic deletion of calcitonin receptor–like receptor exacerbates intestinal inflammation
Reema B. Davis, Daniel O. Kechele, Elizabeth S. Blakeney, John B. Pawlak, Kathleen M. Caron
Reema B. Davis, Daniel O. Kechele, Elizabeth S. Blakeney, John B. Pawlak, Kathleen M. Caron
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Research Article Gastroenterology

Lymphatic deletion of calcitonin receptor–like receptor exacerbates intestinal inflammation

Abstract

Lymphatics play a critical role in maintaining gastrointestinal homeostasis and in the absorption of dietary lipids, yet their roles in intestinal inflammation remain elusive. Given the increasing prevalence of inflammatory bowel disease, we investigated whether lymphatic vessels contribute to, or may be causative of, disease progression. We generated a mouse model with temporal and spatial deletion of the key lymphangiogenic receptor for the adrenomedullin peptide, calcitonin receptor–like receptor (Calcrl), and found that the loss of lymphatic Calcrl was sufficient to induce intestinal lymphangiectasia, characterized by dilated lacteals and protein-losing enteropathy. Upon indomethacin challenge, Calcrlfl/fl/Prox1-CreERT2 mice demonstrated persistent inflammation and failure to recover and thrive. The epithelium and crypts of Calcrlfl/fl/Prox1-CreERT2 mice exhibited exacerbated hallmarks of disease progression, and the lacteals demonstrated an inability to absorb lipids. Furthermore, we identified Calcrl/adrenomedullin signaling as an essential upstream regulator of the Notch pathway, previously shown to be critical for intestinal lacteal maintenance and junctional integrity. In conclusion, lymphatic insufficiency and lymphangiectasia caused by loss of lymphatic Calcrl exacerbates intestinal recovery following mucosal injury and underscores the importance of lymphatic function in promoting recovery from intestinal inflammation.

Authors

Reema B. Davis, Daniel O. Kechele, Elizabeth S. Blakeney, John B. Pawlak, Kathleen M. Caron

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Figure 4

Increased proliferation in the crypts but diminished proliferation in lacteals lacking Calcrl.

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Increased proliferation in the crypts but diminished proliferation in la...
Representative images of proliferation marker phospho-histone H3–stained (A) and apoptosis marker cleaved caspase-3–stained ilea (B) of tamoxifen-treated (TAM-treated) Calcrlfl/fl and Calcrlfl/fl/Prox1-CreERT2 mice after TAM treatment and 7 days after indomethacin (INDO) challenge. (C) Representative images of proliferation marker Ki67- and lymphatic vessel endothelial hyaluronan receptor 1–stained (LYVE1-stained) ilea of TAM-treated Calcrlfl/fl and Calcrlfl/fl/Prox1-CreERT2 mice 7 days after INDO challenge. Arrows point to the Ki67-positive area within the villi lacteal. Arrowhead indicates Ki67 staining in crypt. n = 7–8 animals in each group. Scale bar: 50 μm.