Lucy Collinson scite author profile

Data availability The RNA sequencing datasets (GSE117930) and the single cell RNA sequencing datasets (GSE131508) are deposited in the Gene Expression Omnibus (GEO, NCBI) repository. The proteomic datasets are deposited in PRoteomics IDEntifications (PRIDE) repository (PXD010597). Author Contribution L.O. designed and performed most of the experiments, analysed and interpreted the data and contributed to the manuscript preparation. E.N. assisted with data collection, performed all the 3D-scaffold co-culture experiments, the in vivo Wisp1 experiments, the scRNA sequencing, interpreted and analysed the data and contributed to the manuscript preparation. I.K. performed the qPCR analysis, some of the tissue IF staining and analysed the data. A.M. and J.H.L. performed some of the tissue IF staining, all the lung organoid experiments, interpreted and analysed the data. V.B. performed some of the tissue IF staining. P.C. and S. H. performed bioinformatics analysis. I.H., J.K. and A.O. performed the proteomic and analysed the data. E.G.G. helped with the collection of Ly6G + cells for proteomics. G.M. performed the 3D-scaffold co-culture to analyse CD104 + cells. A.W. and L.C. performed the electron microscopy experiments. E.H. and V.S. provided human samples. L.O., E.N., I.K., V.B. and J.H.L., critically reviewed the manuscript. J.H.L., supervised the lung organoid experiments. I.M. designed and supervised the study, interpreted the data and wrote the manuscript.

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Functional redundancy of Rab27 proteins and the pathogenesis of Griscelli syndrome

Barral¹,

Ramalho²,

Anders³

et al. 2002

J. Clin. Invest.

137

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Griscelli syndrome (GS) patients and the corresponding mouse model ashen exhibit defects mainly in two types of lysosome-related organelles, melanosomes in melanocytes and lytic granules in CTLs. This disease is caused by loss-of-function mutations in RAB27A, which encodes 1 of the 60 known Rab GTPases, critical regulators of vesicular transport. Here we present evidence that Rab27a function can be compensated by a closely related protein, Rab27b. Rab27b is expressed in platelets and other tissues but not in melanocytes or CTLs. Morphological and functional tests in platelets derived from ashen mice are all within normal limits. Both Rab27a and Rab27b are found associated with the limiting membrane of platelet-dense granules and to a lesser degree with α-granules. Ubiquitous transgenic expression of Rab27a or Rab27b rescues ashen coat color, and melanocytes derived from transgenic mice exhibit widespread peripheral distribution of melanosomes instead of the perinuclear clumping observed in ashen melanocytes. Finally, transient expression in ashen melanocytes of Rab27a or Rab27b, but not other Rab's, restores peripheral distribution of melanosomes. Our data suggest that Rab27b is functionally redundant with Rab27a and that the pathogenesis of GS is determined by the relative expression of Rab27a and Rab27b in specialized cell types.

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Subcellular antibiotic visualization reveals a dynamic drug reservoir in infected macrophages

Santos

Huang

et al. 2019

Science

132

134

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Tuberculosis, caused by the intracellular pathogen Mycobacterium tuberculosis, remains the world's deadliest infectious disease. Sterilising chemotherapy requires at least six months of multidrug therapy. Difficulty visualising the subcellular localisation of antibiotics in infected host cells means that it is unclear whether antibiotics penetrate into all mycobacteria-containing compartments in the cell. Here, we combine correlated light, electron and ion microscopy to image the distribution of Bedaquiline in infected human macrophages at sub-micrometre resolution. Bedaquiline accumulated primarily in host cell lipid droplets, but heterogeneously in mycobacteria within a variety of intracellular compartments. Furthermore, lipid droplets did not sequester antibiotic but constituted a transferable reservoir that enhanced antibacterial efficacy. Thus, strong lipid binding facilitated drug trafficking by host organelles to an intracellular target during antimicrobial treatment.Mycobacterium tuberculosis (Mtb) can persist in multiple intracellular niches within human * Correspondence to: max.

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The receptor DNGR-1 signals for phagosomal rupture to promote cross-presentation of dead-cell-associated antigens

et al. 2020

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Engineering transplantable jejunal mucosal grafts using patient-derived organoids from children with intestinal failure

Meran

Massie

Campinoti

et al. 2020

Nat Med

113

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Lucy Collinson

Metastatic-niche labelling reveals parenchymal cells with stem features

Functional redundancy of Rab27 proteins and the pathogenesis of Griscelli syndrome

Subcellular antibiotic visualization reveals a dynamic drug reservoir in infected macrophages

The receptor DNGR-1 signals for phagosomal rupture to promote cross-presentation of dead-cell-associated antigens

Engineering transplantable jejunal mucosal grafts using patient-derived organoids from children with intestinal failure

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