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Dive into the research topics where Alison J. Loughlin is active.

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Featured researches published by Alison J. Loughlin.


Biomaterials | 2013

Engineered neural tissue for peripheral nerve repair.

Melanie Georgiou; Stephen C.J. Bunting; Heather A. Davies; Alison J. Loughlin; Jonathan P. Golding; James B. Phillips

A new combination of tissue engineering techniques provides a simple and effective method for building aligned cellular biomaterials. Self-alignment of Schwann cells within a tethered type-1 collagen matrix, followed by removal of interstitial fluid produces a stable tissue-like biomaterial that recreates the aligned cellular and extracellular matrix architecture associated with nerve grafts. Sheets of this engineered neural tissue supported and directed neuronal growth in a co-culture model, and initial in vivo tests showed that a device containing rods of rolled-up sheets could support neuronal growth during rat sciatic nerve repair (5 mm gap). Further testing of this device for repair of a critical-sized 15 mm gap showed that, at 8 weeks, engineered neural tissue had supported robust neuronal regeneration across the gap. This is, therefore, a useful new approach for generating anisotropic engineered tissues, and it can be used with Schwann cells to fabricate artificial neural tissue for peripheral nerve repair.


Journal of Cellular and Molecular Medicine | 2009

Amyloid-β-induced occludin down-regulation and increased permeability in human brain endothelial cells is mediated by MAPK activation

Leon M. Tai; Karen Holloway; David Male; Alison J. Loughlin; Ignacio A. Romero

Vascular dysfunction is emerging as a key pathological hallmark in Alzheimer’s disease (AD). A leaky blood–brain barrier (BBB) has been described in AD patient tissue and in vivo AD mouse models. Brain endothelial cells (BECs) are linked together by tight junctional (TJ) proteins, which are a key determinant in restricting the permeability of the BBB. The amyloid β (Aβ) peptides of 1–40 and 1–42 amino acids are believed to be pivotal in AD pathogenesis. We therefore decided to investigate the effect of Aβ 1–40, the Aβ variant found at the highest concentration in human plasma, on the permeability of an immortalized human BEC line, hCMEC/D3. Aβ 1–40 induced a marked increase in hCMEC/D3 cell permeability to the paracellular tracer 70 kD FITC‐dextran when compared with cells incubated with the scrambled Aβ 1–40 peptide. Increased permeability was associated with a specific decrease, both at the protein and mRNA level, in the TJ protein occludin, whereas claudin‐5 and ZO‐1 were unaffected. JNK and p38MAPK inhibition prevented both Aβ 1–40‐mediated down‐regulation of occludin and the increase in paracellular permeability in hCMEC/D3 cells. Our findings suggest that the JNK and p38MAPK pathways might represent attractive therapeutic targets for preventing BBB dysfunction in AD.


Biomaterials | 2015

Engineered neural tissue with aligned, differentiated adipose-derived stem cells promotes peripheral nerve regeneration across a critical sized defect in rat sciatic nerve.

Melanie Georgiou; Jon P. Golding; Alison J. Loughlin; Paul J. Kingham; James B. Phillips

Adipose-derived stem cells were isolated from rats and differentiated to a Schwann cell-like phenotype in vitro. The differentiated cells (dADSCs) underwent self-alignment in a tethered type-1 collagen gel, followed by stabilisation to generate engineered neural tissue (EngNT-dADSC). The pro-regenerative phenotype of dADSCs was enhanced by this process, and the columns of aligned dADSCs in the aligned collagen matrix supported and guided neurite extension in vitro. EngNT-dADSC sheets were rolled to form peripheral nerve repair constructs that were implanted within NeuraWrap conduits to bridge a 15 mm gap in rat sciatic nerve. After 8 weeks regeneration was assessed using immunofluorescence imaging and transmission electron microscopy and compared to empty conduit and nerve graft controls. The proportion of axons detected in the distal stump was 3.5 fold greater in constructs containing EngNT-dADSC than empty tube controls. Our novel combination of technologies that can organise autologous therapeutic cells within an artificial tissue construct provides a promising new cellular biomaterial for peripheral nerve repair.


Differentiation | 2007

Culture and differentiation of preadipocytes in two-dimensional and three-dimensional in vitro systems

Sandeep Daya; Alison J. Loughlin; Hilary MacQueen


Archive | 2007

Three Dimensional Cell Culture

Hilary MacQueen; Alison J. Loughlin; Sandeep Daya


Archive | 2013

A multi-well plate model of reactive gliosis for high throughput screening of potential CNS therapies

Caitriona O'Rourke; Alison J. Loughlin; Rosemary Drake; James B. Phillips


Archive | 2012

Astrocytes expressing GFP in 3D collagen gels provide an effective model for screening the glial response to potential CNS cell therapies

N Johns; Emma East; Jon P. Golding; Alison J. Loughlin; James B. Phillips


Archive | 2012

Developing a 3D co-culture model to simulate perinatal hypoxic-ischaemic brain injury in preterm infants

Et Osei; L Evans; James B. Phillips; Alison J. Loughlin


Archive | 2012

Defining glial cell self-alignment parameters for 3D CNS tissue models

Caitriona O'Rourke; Alison J. Loughlin; Rosemary Drake; James B. Phillips


Journal of Tissue Engineering and Regenerative Medicine | 2012

A nerve repair conduit containing differentiated adipose-derived stem cells within engineered neural tissue can support and guide neuronal growth in vitro and in vivo

Melanie Georgiou; Paul J. Kingham; Stephen C.J. Bunting; Jon P. Golding; Alison J. Loughlin; James B. Phillips

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James B. Phillips

UCL Eastman Dental Institute

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