A gelatin hydrogel nonwoven fabric improves outcomes of subcutaneous islet transplantation

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作者
Norifumi Kanai
Akiko Inagaki
Yasuhiro Nakamura
Takehiro Imura
Hiroaki Mitsugashira
Ryusuke Saito
Shigehito Miyagi
Kimiko Watanabe
Takashi Kamei
Michiaki Unno
Yasuhiko Tabata
Masafumi Goto
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[1] Tohoku University Graduate School of Medicine,Department of Surgery
[2] Tohoku University Graduate School of Medicine,Division of Transplantation and Regenerative Medicine
[3] Tohoku Medical and Pharmaceutical University,Division of Pathology, Graduate School of Medicine
[4] Kyoto University,Laboratory of Biomaterials, Department of Regeneration Science and Engineering, Institute for Life and Medical Sciences (LiMe)
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Subcutaneous islet transplantation is a promising treatment for severe diabetes; however, poor engraftment hinders its prevalence. We previously reported that a recombinant peptide (RCP) enhances subcutaneous islet engraftment. However, it is impractical for clinical use because RCP must be removed when transplanting islets. We herein investigated whether a novel bioabsorbable gelatin hydrogel nonwoven fabric (GHNF) could improve subcutaneous islet engraftment. A silicon spacer with or without GHNF was implanted into the subcutaneous space of diabetic mice. Syngeneic islets were transplanted into the pretreated space or intraportally (Ipo group). Blood glucose, intraperitoneal glucose tolerance, immunohistochemistry, CT angiography and gene expression were evaluated. The cure rate and glucose tolerance of the GHNF group were significantly better than in the control and Ipo groups (p < 0.01, p < 0.05, respectively). In the GHNF group, a limited increase of vWF-positive vessels was detected in the islet capsule, whereas laminin (p < 0.05), collagen III and IV were considerably enhanced. TaqMan arrays revealed a significant upregulation of 19 target genes (including insulin-like growth factor-2) in the pretreated space. GHNF markedly improved the subcutaneous islet transplantation outcomes, likely due to ECM compensation and protection of islet function by various growth factors, rather than enhanced neovascularization.
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