Meningococcus Hijacks a β2-Adrenoceptor/β-Arrestin Pathway to Cross Brain Microvasculature Endothelium

Coureuil, Mathieu; Lécuyer, Hervé; Scott, Mark G. H.; Boularan, Cédric; Enslen, Hervé; Soyer, Magali; Mikaty, Guillain; Bourdoulous, Sandrine; Nassif, Xavier; Marullo, Stéfano

doi:10.1016/j.cell.2010.11.035

Cited by 165 publications

(228 citation statements)

References 42 publications

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“…E. coli BL21(DE3) was used for protein expression and purification experiments. Derivatives of the pMAL-p2X expression vector (New England Biolabs) encoding fusions between MBP and the soluble portions of ComP, PilE, PilV, and PilX (ComP , PilE , PilV , and PilX 39-162 ) have been described previously (19,34). All of the fusion proteins are directed to the periplasm, which is important for disulfide bond formation, and the MBP can be cleaved off by factor Xa, giving soluble proteins with four vector-derived N-terminal residues (ISEF).…”

Section: Methodsmentioning

confidence: 99%

Specific DNA recognition mediated by a type IV pilin

Cehovin

Simpson

McDowell

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

145

169

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Natural transformation is a dominant force in bacterial evolution by promoting horizontal gene transfer. This process may have devastating consequences, such as the spread of antibiotic resistance or the emergence of highly virulent clones. However, uptake and recombination of foreign DNA are most often deleterious to competent species. Therefore, model naturally transformable Gramnegative bacteria, including the human pathogen Neisseria meningitidis, have evolved means to preferentially take up homotypic DNA containing short and genus-specific sequence motifs. Despite decades of intense investigations, the DNA uptake sequence receptor in Neisseria species has remained elusive. We show here, using a multidisciplinary approach combining biochemistry, molecular genetics, and structural biology, that meningococcal type IV pili bind DNA through the minor pilin ComP via an electropositive stripe that is predicted to be exposed on the filaments surface and that ComP displays an exquisite binding preference for DNA uptake sequence. Our findings illuminate the earliest step in natural transformation, reveal an unconventional mechanism for DNA binding, and suggest that selective DNA uptake is more widespread than previously thought.DNA receptor | genetic competence

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Section: Methodsmentioning

confidence: 99%

Specific DNA recognition mediated by a type IV pilin

Cehovin

Simpson

McDowell

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

145

169

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“…1C) was sufficient to allow some binding of Notch to Itch. To demonstrate this, we knocked down the endogenous b-arrestin 1 and barrestin 2 as described previously (Coureuil et al, 2010). The efficiency of siRNA targeting b-arrestins (sib-arr) was confirmed by western blot (Fig.…”

Section: B-arrestins Are Necessary For Itch-notch Interactionmentioning

confidence: 99%

α-arrestin 1 (ARRDC1) and β-arrestins cooperate to mediate Notch degradation in mammals

Puca

Chastagner

Meas-Yedid

et al. 2013

Journal of Cell Science

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SummaryNotch signaling is a conserved signaling pathway implicated in embryogenesis and adult tissue maintenance. Notch signaling strength is strictly regulated, notably by maintaining a controlled pool of functional receptor at the cell surface. Mammalian non-activated Notch receptor is internalized, ubiquitylated by the Itch E3 ubiquitin ligase and degraded in the lysosomes. Here, we show that b-arrestins are necessary for Itch-Notch interaction and for Itch-driven ubiquitylation and degradation of Notch. Interestingly, b-arrestins do not directly bind Itch but heterodimerize with a member of another subfamily of arrestins called ARRDC1 or a-arrestin 1, which harbors PPxY motifs that allow direct interaction with Itch. Cells transfected with ARRDC1 mutated in PPxY motifs show reduced Itchmediated Notch ubiquitylation and impaired lysosomal degradation of Notch, as observed in b-arrestin 2/2 or Itch 2/2 cells. Our data show for the first time that ARRDC1 and b-arrestins heterodimerize and cooperate in the same complex to promote non-activated Notch receptor degradation, thus acting as negative regulators of Notch signaling.

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“…E. coli K1 OmpA initiates a signaling process that leads to the dissociation of b-catenins from cadherins which further results in disruption of barrier integrity . The type-IV pili of N. meningitides, on the other hand, stimulates the b2-adrenoceptor/b-arrestin signaling pathway in endothelial cells, leading to recruitment of the Par3/Par6/PKCz polarity complex and delocalization of junctional proteins which result in anatomical gaps that are used by the bacteria to penetrate into the CNS (Coureuil et al 2009(Coureuil et al , 2010. Human immunodeficiency virus (HIV) envelope glycoprotein gp120 has also been shown to increase BBB permeability by interacting with endothelial trans-membrane coreceptor CCR5 and CXCR4 (Kanmogne et al 2007).…”

Section: Paracytosismentioning

confidence: 99%