Litcius/Paper detail

Prostaglandins regulate invasive, collective border cell migration

Emily F. Fox, Maureen C. Lamb, Samuel Q. Mellentine, Tina L. Tootle

2020Molecular Biology of the Cell16 citationsDOI

Abstract

cyclooxygenase-like enzyme responsible for PG synthesis. Loss of Pxt results in both delayed border cell migration and elongated clusters, whereas somatic Pxt knockdown causes delayed migration and compacted clusters. These findings suggest PGs act in both the border cells and nurse cells, the substrate on which the border cells migrate. As PGs regulate the actin bundler Fascin, and Fascin is required for on-time migration, we assessed whether PGs regulate Fascin to promote border cell migration. Coreduction of Pxt and Fascin results in delayed migration and elongated clusters. The latter may be due to altered cell adhesion, as loss of Pxt or Fascin, or coreduction of both, decreases integrin levels on the border cell membranes. Conversely, integrin localization is unaffected by somatic knockdown of Pxt. Together these data lead to the model that PG signaling controls Fascin in the border cells to promote migration and in the nurse cells to maintain cluster cohesion.

Topics & Concepts

FascinCell migrationBiologyCell biologyBorder cellsGene knockdownIntegrinLamellipodiumActinCellCell cultureBiochemistryGeneticsCell Adhesion Molecules ResearchCellular Mechanics and InteractionsNeurobiology and Insect Physiology Research