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

Meran, L.; Massie, I.; Campinoti, S.; Weston, A. E.; Gaifulina, R.; Tullie, L.; Faull, P.; Orford, M.; Kucharska, A.; Baulies, A.; Novellasdemunt, L.; Angelis, N.; Hirst, E.; König, J.; Tedeschi, A. M.; Pellegata, A. F.; Eli, S.; Snijders, A. P.; Collinson, L.; Thomas, G. M. H.; Eaton, S.; Bonfanti, P.; De Coppi, P.; Li, V. S. W.; Thapar, N.

Please use this identifier to cite or link to this item: https://dora.health.qld.gov.au/qldresearchjspui/handle/1/2841

Title:	Engineering transplantable jejunal mucosal grafts using patient-derived organoids from children with intestinal failure
Authors:	Meran, L. Massie, I. Campinoti, S. Weston, A. E. Gaifulina, R. Tullie, L. Faull, P. Orford, M. Kucharska, A. Baulies, A. Novellasdemunt, L. Angelis, N. Hirst, E. König, J. Tedeschi, A. M. Pellegata, A. F. Eli, S. Snijders, A. P. Collinson, L. Thomas, G. M. H. Eaton, S. Bonfanti, P. De Coppi, P. Li, V. S. W. Thapar, N.
Issue Date:	2020
Source:	26, (10), 2020, p. 1593-1601
Pages:	1593-1601
Journal:	Nature Medicine
Abstract:	Intestinal failure, following extensive anatomical or functional loss of small intestine, has debilitating long-term consequences for children1. The priority of patient care is to increase the length of functional intestine, particularly the jejunum, to promote nutritional independence2. Here we construct autologous jejunal mucosal grafts using biomaterials from pediatric patients and show that patient-derived organoids can be expanded efficiently in vitro. In parallel, we generate decellularized human intestinal matrix with intact nanotopography, which forms biological scaffolds. Proteomic and Raman spectroscopy analyses reveal highly analogous biochemical profiles of human small intestine and colon scaffolds, indicating that they can be used interchangeably as platforms for intestinal engineering. Indeed, seeding of jejunal organoids onto either type of scaffold reliably reconstructs grafts that exhibit several aspects of physiological jejunal function and that survive to form luminal structures after transplantation into the kidney capsule or subcutaneous pockets of mice for up to 2 weeks. Our findings provide proof-of-concept data for engineering patient-specific jejunal grafts for children with intestinal failure, ultimately aiding in the restoration of nutritional autonomy.L20060899302020-09-10
DOI:	10.1038/s41591-020-1024-z
Resources:	https://www.embase.com/search/results?subaction=viewrecord&id=L2006089930&from=exporthttp://dx.doi.org/10.1038/s41591-020-1024-z \|
Keywords:	Young modulus;Wnt signaling;tissue scaffoldalkaline phosphatase;alpha smooth muscle actin;biomaterial;collagen;fibronectin;Kiss1 receptor;laminin;vimentin;article;autotransplantation;biochemical analysis;cell culture;cell infiltration;controlled study;decellularization;down regulation;extracellular matrix;fibroblast;in vitro study;intestinal failure;intestinal organoid;intestinal stem cell;intestine graft;jejunum mucosa;mouse;myofibroblast;nonhuman;pediatric patient;priority journal;protein expression;protein fingerprinting;Raman spectrometry;stroma cell;surface property;tissue engineering;topography;upregulation
Type:	Article
Appears in Sites:	Children's Health Queensland Publications

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