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The asymmetric Pitx2 gene regulates gut muscular-lacteal development and protects against fatty liver disease

Shing Hu, Aparna Mahadevan, Isaac F. Elysee, Joseph Choi, Nathan R. Souchet, Gloria H. Bae, Alessandra K. Taboada, Bhargav D. Sanketi, G Duhamel, Carolyn S. Sevier, Ge Tao, Natasza A. Kurpios

2021Cell Reports19 citationsDOIOpen Access PDF

Abstract

Intestinal lacteals are essential lymphatic channels for absorption and transport of dietary lipids and drive the pathogenesis of debilitating metabolic diseases. However, organ-specific mechanisms linking lymphatic dysfunction to disease etiology remain largely unknown. In this study, we uncover an intestinal lymphatic program that is linked to the left-right (LR) asymmetric transcription factor Pitx2. We show that deletion of the asymmetric Pitx2 enhancer ASE alters normal lacteal development through the lacteal-associated contractile smooth muscle lineage. ASE deletion leads to abnormal muscle morphogenesis induced by oxidative stress, resulting in impaired lacteal extension and defective lymphatic system-dependent lipid transport. Surprisingly, activation of lymphatic system-independent trafficking directs dietary lipids from the gut directly to the liver, causing diet-induced fatty liver disease. Our study reveals the molecular mechanism linking gut lymphatic function to the earliest symmetry-breaking Pitx2 and highlights the important relationship between intestinal lymphangiogenesis and the gut-liver axis.

Topics & Concepts

Lymphatic systemPITX2Fatty liverBiologyMorphogenesisEndocrinologyTranscription factorInternal medicineDiseaseImmunologyMedicineGeneGeneticsHomeoboxLymphatic System and DiseasesWnt/β-catenin signaling in development and cancerKruppel-like factors research
The asymmetric Pitx2 gene regulates gut muscular-lacteal development and protects against fatty liver disease | Litcius