A Perspective on the Clinical Translation of Scaffolds for Tissue Engineering

Webber, Matthew J.; Khan, Omar F.; Sydlik, Stefanie A.; Tang, Benjamin C.; Langer, Robert

doi:10.1007/s10439-014-1104-7

Cited by 187 publications

(149 citation statements)

References 116 publications

(118 reference statements)

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“…The cohort expressing both growth factors simultaneously was found to be better in terms of the formation and deposition of newly formed bone compared to the cohorts expressing only one of the two growth factors in rabbit orbital defect model [72]. The delivery of VEGF in combination with the osteogenic BMP-2 induces neo-vascularization of the newly formed bone tissue thus enabling superior supply of nutrients [73].…”

Section: Gene Delivery By Cells Ex Vivo Transfected With Bmp-2 Encodimentioning

confidence: 97%

How to use BMP-2 for clinical applications? A review on pros and cons of existing delivery strategies

Mumcuoglu¹,

Siverino²,

Tabisz³

et al. 2017

J Transl Sci

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Section: Gene Delivery By Cells Ex Vivo Transfected With Bmp-2 Encodimentioning

confidence: 97%

How to use BMP-2 for clinical applications? A review on pros and cons of existing delivery strategies

Mumcuoglu¹,

Siverino²,

Tabisz³

et al. 2017

J Transl Sci

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“…The efficacy of manual decellularisation has been demonstrated successfully by numerous groups, and manually prepared xenogenic-derived tissue substitutes have been used in clinical practice for many years; however, little attention has been directed towards their 'upscaled' production [Badylak, 1989;Price et al, 2014;G et al, 2015;Webber et al, 2015]. In this current ex vivo study, a comparative analysis of the repeatable nature of ADP, which was previously described for the preparation of ovine aortaderived ECMs, was investigated using Triton X-100 as the main active decellularisation reagent [Mooney et al, 2015].…”

Section: Discussionmentioning

confidence: 99%

“…As decellularised extracellular matrices (ECMs) become more relevant in delivering these advanced tissue therapies, automation of the decellularisation process will ultimately be required to provide for the increasing number of patients and also at an affordable sustainable price for world health care providers [G et al, 2015]. Various authors such as G et al [2015] and Webber et al [2015] have suggested that one of the principal reasons that so little clinical translation has occurred to date is due to the extremely high costs of delivering such treatments and also the lack of availability of quality-assured consistent ECMderived scaffolds for implantation and research purposes Price et al, 2014;G et al, 2015;Webber et al, 2015]. They have suggested that 'up-scaled' production is one key area that needs greater investigation, to ensure cost-effectively decellularised ECM scaffolds which can safely be used to treat a much larger cohort of patients [WHO, 2013;G et al, 2015;Webber et al, 2015].…”

mentioning

confidence: 99%

“…Various authors such as G et al [2015] and Webber et al [2015] have suggested that one of the principal reasons that so little clinical translation has occurred to date is due to the extremely high costs of delivering such treatments and also the lack of availability of quality-assured consistent ECMderived scaffolds for implantation and research purposes Price et al, 2014;G et al, 2015;Webber et al, 2015]. They have suggested that 'up-scaled' production is one key area that needs greater investigation, to ensure cost-effectively decellularised ECM scaffolds which can safely be used to treat a much larger cohort of patients [WHO, 2013;G et al, 2015;Webber et al, 2015]. Limitations associated with xenogenic ECMs include the absence of gold standard preparation techniques for a repeatable decellularisation process, compounded by the fact that decellularisation is performed manually, lacking standardisation and is extremely time consuming [Naso et al, 2014;Price et al, 2014].…”

mentioning

confidence: 99%

“…A large research effort has been applied to the development of newer alternatives to current gold standard treatments for tissue and organ failure, using these tissue engineering approaches [Pellegata et al, 2012;WHO, 2013;Price et al, 2014;G et al, 2015;Webber et al, 2015]. Although decellularised xenogenic scaffolds promise to deliver more effective outcomes than the current gold standard treatments, very little of the current research effort has been translated into clinical practice, although major milestones have been achieved, such as the world's first decellularised trachea replacement by Macchiarini et al [2008].…”

mentioning

confidence: 99%

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On the Automatic Decellularisation of Porcine Aortae: A Repeatability Study Using a Non-Enzymatic Approach

Mooney

Davis

Hoey

et al. 2016

Cells Tissues Organs

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Objective: To investigate the repeatability of automatic decellularisation of porcine aortae using a non-enzymatic approach, addressing current limitations associated with other automatic decellularisation processes. Materials and Methods: Individual porcine aortae (n = 3) were resected and every third segment (n = 4) was allocated to one of three different groups: a control or a manually or automatically decellularised group. Manual and automatic decellularisation was performed using Triton X-100 (2% v/v) and sodium deoxycholate. Protein preservation and the elimination of a galactosyl-α(1,3)galactose (GAL) epitope were measured using immunohistochemistry and protein binding assays. The presence of residual DNA was determined with gel electrophoresis and spectrophotometry. Scaffold integrity was characterised with scanning electron microscopy and uni-axial tensile testing. Manual and automatic results were compared to one another, to control groups and to current gold standards. Results: The results were comparable to those of current gold standard decellularisation techniques. Successful repeatability was achieved, both manually and automatically, with little effect on mechanical characteristics. Complete acellularity was not confirmed in either decellularisation group. Protein preservation was consistent in both the manually and automatically decellularised groups and between each individual aorta. Elimination of GAL was not achieved. Conclusion: Repeatable automatic decellularisation of porcine aortae is feasible using a Triton X-100-sodium deoxycholate protocol. Protein preservation was satisfactory; however, gold standard thresholds for permissible residual DNA levels were not achieved. Future research will focus on addressing this issue by optimisation of the existing protocol for thick tissues.

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