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Glucose-Stimulated Insulin Response of Silicon Nanopore-Immunoprotected Islets under Convective Transport.

Citation
Song, S., et al. “Glucose-Stimulated Insulin Response Of Silicon Nanopore-Immunoprotected Islets Under Convective Transport.”. Acs Biomaterials Science & Engineering, pp. 1051-1061.
Author Shang Song, Raymond Yeung, Jaehyun Park, Andrew M Posselt, Tejal A Desai, Qizhi Tang, Shuvo Roy
Keywords convection, diffusion, glucose-insulin kinetics, immunoisolation, silicon nanopore membranes (SNM)
Abstract

Major clinical challenges associated with islet transplantation for type 1 diabetes include shortage of donor organs, poor engraftment due to ischemia, and need for immunosuppressive medications. Semipermeable membrane capsules can immunoprotect transplanted islets by blocking passage of the host's immune components while providing exchange of glucose, insulin, and other small molecules. However, capsules-based diffusive transport often exacerbates ischemic injury to islets by reducing the rate of oxygen and nutrient transport. We previously reported the efficacy of a newly developed semipermeable ultrafiltration membrane, the silicon nanopore membrane (SNM) under convective-driven transport, in limiting the passage of pro-inflammatory cytokines while overcoming the mass transfer limitations associated with diffusion through nanometer-scale pores. In this study, we report that SNM-encapsulated mouse islets perfused in culture solution under convection outperformed those under diffusive conditions in terms of magnitude (1.49-fold increase in stimulation index and 3.86-fold decrease in shutdown index) and rate of insulin secretion (1.19-fold increase and 6.45-fold decrease during high and low glucose challenges), respectively. Moreover, SNM-encapsulated mouse islets under convection demonstrated rapid glucose-insulin sensing within a physiologically relevant time-scale while retaining healthy islet viability even under cytokine exposure. We conclude that encapsulation of islets with SNM under convection improves islet in vitro functionality. This approach may provide a novel strategy for islet transplantation in the clinical setting.

Year of Publication
2017
Journal
ACS biomaterials science & engineering
Volume
3
Issue
6
Number of Pages
1051-1061
Date Published
06/2017
ISSN Number
2373-9878
DOI
10.1021/acsbiomaterials.6b00814
Alternate Journal
ACS Biomater Sci Eng
PMID
29250596
PMCID
PMC5729757
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