Mechanisms Underlying Asymmetric Rotation and Morphogenesis of the Midgut

Principal Investigator: Natasza Kurpios

Department of Molecular Medicine
Sponsor: NIH-National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Grant Number: 2R01DK092776-11
Title: Mechanisms Underlying Asymmetric Rotation and Morphogenesis of the Midgut
Project Amount: $394,567
Project Period: September 2023 to August 2024

DESCRIPTION (provided by applicant): 

The mechanisms discovered through the study of embryogenesis have been fundamental to understanding disease. We use classic chicken embryology and sophisticated mouse genetics to elucidate how basic cellular processes define the shape and function of organs. We are most fascinated by left-right (LR) organ asymmetry, as errors of organ laterality are linked to life-threatening birth defects. The counterclockwise rotation of the gut is an excellent model to study organ laterality. A critical aspect of this rotation is initiation of a leftward tilt directed by the master regulator of LR asymmetry, Pitx2. Failure to do so leads to gut malrotation and catastrophic volvulus in pediatric patients. Whereas rotation forces had long been assumed intrinsic to the gut tube, we instead discovered that gut rotation is driven by asymmetric deformation of the adjacent dorsalmesentery (DM) that suspends the gut, and whose cellular architecture is downstream of Pitx2. A key property of the DM is its exquisite binary organization, with distinct LR compartments that are readily accessible to genetic manipulation. Cellular and extracellular matrix (ECM) changes in each compartment cause the DM to deform and tilt the attached gut tube leftward. This critical bias determines gut chirality and frames a model to explain how LR gene expression is ultimately responsible for changes in cell behavior that initiate asymmetric organogenesis. Whereas most situs-specific organogenesis depends on Pitx2, mechanistic studies downstream have been hampered by a confounding “double-right” isomerism in Pitx2 mutants. Whereas Pitx2 expression in all vertebrates is activated by Nodal, Nodal disappears before asymmetric morphogenesis, leavingunresolved the question of how Pitx2 directs organogenesis. We discovered that Pitx2 expression in the gut is not an extension of previous induction by Nodal. Instead, we demonstrate that gut rotation requires a “second wave” of Pitx2 that is subject to mechanoregulation by the latent TGFβ, linking LR gene expression to force translation. In aim 1, we determine the mechanism of Pitx2 dose response during gut development and identify two distinct roles for Pitx2 dependent on its repressive threshold on BMP4 signaling. In aim 2, we define the molecular mechanism by which the formin Daam2, a Pitx2 target, directs tilting polarity. In aim 3, we measure tissue physical properties of the chicken DM to elucidate how they contribute to gut rotation. Together, these studies will significantly advance our understanding of the control of asymmetric gut morphogenesis, a critical step toward improved malrotation diagnostics in newborns.