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Prominin-1 (CD133) modulates the architecture and dynamics of microvilli.

Kristina ThammDeimantė ŠimaitėJana KarbanováVicente BermúdezDoreen ReichertAnne MorgensternMartin BornhäuserWieland B HuttnerMichaela Wilsch-BräuningerDenis Corbeil
Published in: Traffic (Copenhagen, Denmark) (2018)
Prominin-1 is a cell surface biomarker that allows the identification of stem and cancer stem cells from different organs. It is also expressed in several differentiated epithelial and non-epithelial cells. Irrespective of the cell type, prominin-1 is associated with plasma membrane protrusions. Here, we investigate its impact on the architecture of membrane protrusions using microvilli of Madin-Darby canine kidney cells as the main model. Our high-resolution analysis revealed that upon the overexpression of prominin-1 the number of microvilli and clusters of them increased. Microvilli with branched and/or knob-like morphologies were observed and stimulated by mutations in the ganglioside-binding site of prominin-1. The altered phenotypes were caused by the interaction of prominin-1 with phosphoinositide 3-kinase and Arp2/3 complex. Mutation of tyrosine 828 of prominin-1 impaired its phosphorylation and thereby inhibited the aforementioned interactions abolishing altered microvilli. This suggests that the interplay of prominin-1-ganglioside membrane complexes, phosphoinositide 3-kinase and cytoskeleton components regulates microvillar architecture. Lastly, the expression of prominin-1 and its mutants modified the structure of filopodia emerging from fibroblast-like cells and silencing human prominin-1 in primary hematopoietic stem cells resulted in the loss of uropod-associated microvilli. Altogether, these findings strengthen the role of prominin-1 as an organizer of cellular protrusions.
Keyphrases
  • stem cells
  • high resolution
  • cancer stem cells
  • protein kinase
  • cell surface
  • transcription factor
  • mass spectrometry
  • tyrosine kinase
  • cell proliferation
  • induced pluripotent stem cells
  • high speed
  • wild type