Engineering immunomodulatory biomaterials for type 1 diabetes

Stabler, Cherie L.; Li, Y.; Stewart, Joshua M.; Keselowsky, Benjamin G.

doi:10.1038/s41578-019-0112-5

Cited by 104 publications

(98 citation statements)

References 285 publications

(283 reference statements)

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“…[ 2 ] There are more than 500 000 patients diagnosed with T1DM each year with an annual incidence increment of ≈3% worldwide. [ 3,4 ] Patients with T1DM require lifelong insulin therapy. Currently, insulin administration via subcutaneous insulin injection is the primary mode of treatment.…”

Section: Figurementioning

confidence: 99%

Interpenetrating Network of Alginate–Human Adipose Extracellular Matrix Hydrogel for Islet Cells Encapsulation

Wang

Cheam

Irvine

et al. 2020

Macromol. Rapid Commun.

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Transplantation of microencapsulated islet cells holds great potential for the treatment of type 1 diabetes mellitus. However, its clinical translation is hampered by the peri‐transplantation loss of islet viability and functionality in the microcapsules. In this work, a novel islet cells biomimetic microencapsulant material that is based on the interpenetrating networks of alginate and extracellular matrix (ECM) hydrogel composite (AEC) is presented. The ECM component is derived from human lipoaspirate. In situ encapsulation of pancreatic β islet cells (MIN6 β‐cells) can be achieved via ionotropic gelation of the alginate matrix and thermal‐induced gelation of the pepsin‐solubilized ECM pre‐gel. Due to the enhanced cell–matrix interaction, islets encapsulated within the AEC microcapsules (≈640 µm) display sevenfold increase in cell growth over 1 week of culture and characteristic glucose‐stimulated insulin response in vitro. The results show that the AEC microcapsule is a potent platform to bioaugment the performance of islet cells.

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Section: Figurementioning

confidence: 99%

Interpenetrating Network of Alginate–Human Adipose Extracellular Matrix Hydrogel for Islet Cells Encapsulation

Wang

Cheam

Irvine

et al. 2020

Macromol. Rapid Commun.

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“…To overcome those immunological challenges that are associated with artificial skin grafts derived from autologous cells, allogeneic cells, or xenographic tissues, the patients can receive immunosuppressive treatment (Dixit et al, ). Moreover, immunomodulatory biomaterials (IBMs) can enable localized and targeted immunomodulation to the wound site, promoting specific immune responses, which can prevent the need for immunosuppressive medications, while prolonging the implant's lifetime (Stabler, Li, Stewart, & Keselowsky, ). Common strategies for implementing immunomodulation activity in NFs are the M1/M2 macrophage polarization (Castellano et al, ), glycosaminoglycans (GAGs) (Jiang, Wu, et al, ), and decellularized ECM material (Du et al, ; Gholipourmalekabadi et al, ).…”

Section: D Electrospinning For Skin Tissue Engineeringmentioning

confidence: 99%

2D and 3D electrospinning technologies for the fabrication of nanofibrous scaffolds for skin tissue engineering: A review

Keirouz

Chung

Kwon

et al. 2020

WIREs Nanomed Nanobiotechnol

195

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This review provides insights into the current advancements in the field of electrospinning, focusing on its applications for skin tissue engineering. Furthermore, it reports the evolvement and present challenges of advanced skin substitute product development and explores the recent contributions in 2D and 3D scaffolding, focusing on natural, synthetic, and composite nanomaterials. In the past decades, nanotechnology has arisen as a fascinating discipline that has influenced every aspect of science, engineering, and medicine. Electrospinning is a versatile fabrication method that allows researchers to elicit and explore many of the current challenges faced by tissue engineering and regenerative medicine. In skin tissue engineering, electrospun nanofibers are particularly attractive due to their refined morphology, processing flexibility—that allows for the formation of unique materials and structures, and its extracellular matrix‐like biomimetic architecture. These allow for electrospun nanofibers to promote improved re‐epithelization and neo‐tissue formation of wounds. Advancements in the use of portable electrospinning equipment and the employment of electrospinning for transdermal drug delivery and melanoma treatment are additionally explored. Present trends and issues are critically discussed based on recently published patents, clinical trials, and in vivo studies. This article is categorized under: Implantable Materials and Surgical Technologies > Nanotechnology in Tissue Repair and Replacement Therapeutic Approaches and Drug Discovery > Emerging Technologies Implantable Materials and Surgical Technologies > Nanomaterials and Implants

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“…Subcutaneous administration would avoid bioavailability issues that plague Rapamune including first pass metabolism, elimination by intestinal cytochrome P450 and p-glycoprotein, and variability associated with food content. Importantly, the subcutaneous route of administration provides the advantage of targeting lymphatic drainage 16 . Unlike intravenous administration, the subcutaneous route allows patients to take their medication from their own home.…”

Section: Fig 1 | Subcutaneous Rapamycin Delivery Tomentioning

confidence: 99%

“…But the subcutaneous route does provide access to antigen presenting cells (APCs), including the aforementioned DCs that can elicit potent tolerogenic responses upon modulation by rapamycin. Tolerogenic DCs (tDCs) constitutively generate regulatory T cells (Tregs) as well as express anti-inflammatory cytokines, both of which have been linked to enhanced survival of transplanted islets 16 .…”

Section: Fig 1 | Subcutaneous Rapamycin Delivery Tomentioning

confidence: 99%

Subcutaneous nanotherapy repurposes the immunosuppressive mechanism of rapamycin to enhance allogeneic islet graft viability

Burke¹,

Zhang²,

Bobbala³

et al. 2020

Preprint

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Rapamycin is an orally administered immunosuppressant that is plagued by poor bioavailability and a wide biodistribution. Thus, this pleotropic mTOR inhibitor has a narrow therapeutic window, a wide range of side effects and provides inadequate transplantation protection. Here, we demonstrate that subcutaneous rapamycin delivery via poly(ethylene glycol)-b-poly(propylene sulfide)) (PEG-b-PPS) polymersome (PS) nanocarriers modulates the cellular biodistribution of rapamycin to change its immunosuppressive mechanism of action for enhanced efficacy while minimizing side effects. While oral rapamycin inhibits naive T cell proliferation directly, subcutaneously administered rapamycin-loaded polymersomes (rPS) instead modulated Ly-6Clow monocytes and tolerogenic semi-mature dendritic cells, with immunosuppression mediated by CD8+ Tregs and rare CD4+CD8+ double-positive T cells. As PEG-b-PPS PS are uniquely non-inflammatory, background immunostimulation from the vehicle was avoided, allowing immunomodulation to be primarily attributed to the cellular biodistribution of rapamycin. Repurposing mTOR inhibition significantly improved maintenance of normoglycemia in a clinically relevant, MHC-mismatched, allogeneic, intraportal (liver) islet transplantation model. These results demonstrate the ability of engineered nanocarriers to repurpose drugs for alternate routes of administration by rationally controlling cellular biodistribution.

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Engineering immunomodulatory biomaterials for type 1 diabetes

Cited by 104 publications

References 285 publications

Interpenetrating Network of Alginate–Human Adipose Extracellular Matrix Hydrogel for Islet Cells Encapsulation

Interpenetrating Network of Alginate–Human Adipose Extracellular Matrix Hydrogel for Islet Cells Encapsulation

2D and 3D electrospinning technologies for the fabrication of nanofibrous scaffolds for skin tissue engineering: A review

Subcutaneous nanotherapy repurposes the immunosuppressive mechanism of rapamycin to enhance allogeneic islet graft viability

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