Human Recombinant Antithrombin (ATryn®) Administration Improves Survival and Prevents Intravascular Coagulation after Intraportal Islet Transplantation in a Piglet Model

Author:

Gmyr Valery123,Bonner Caroline12,Moerman Ericka123,Tournoys Antoine4,Delalleau Nathalie123,Quenon Audrey12,Thevenet Julien123,Chetboun Mikael124,Kerr-Conte Julie123,Pattou François1234,Hubert Thomas1234,Jourdain Merce1234

Affiliation:

1. European Genomic Institute for Diabetes, Lille, France

2. Inserm UMR 1190, Translational Research for Diabetes, Lille, France

3. University of Lille 2, Lille, France

4. Lille University Hospital, Lille, France

Abstract

Human islet transplantation is a viable treatment option for type 1 diabetes mellitus (T1DM). However, pancreatic islet inflammation after transplantation induced by innate immune responses is likely to hinder graft function. This is mediated by incompatibility between islets and the blood interface, known as instant blood-mediated inflammatory reaction (IBMIR). Herein we hypothesized that portal venous administration of islet cells with human recombinant antithrombin (ATryn®), a serine protease inhibitor (serpin), which plays a central role in the physiological regulation of coagulation and exerts indirect anti-inflammatory activities, may offset coagulation abnormalities such as disseminated intravascular coagulation (DIC) and IBMIR. The current prospective, randomized experiment was conducted using an established preclinical pig model. Three groups were constituted for digested pancreatic tissue transplantation (0.15 ml/kg): control, NaCl 0.9% ( n = 7); gold standard, heparin (25 UI/kg) ( n = 7); and human recombinant ATryn® (500 UI/kg) ( n = 7). Blood samples were collected over time (T0 to 24 h), and biochemical, coagulation, and inflammatory parameters were evaluated. In both the control and heparin groups, one animal died after a portal thrombosis, while no deaths occurred in the ATryn®-treated group. As expected, islet transplantation was associated with an increase in plasma IL-6 or TNF-α levels in all three groups. However, DIC was only observed in the control group, an effect that was suppressed after ATryn® administration. ATryn® administration increased antithrombin activity by 800%, which remained at 200% for the remaining period of the study, without any hemorrhagic complications. These studies suggest that coadministration of ATryn® and pancreatic islets via intraportal transplantation may be a valuable therapeutic approach for DIC without risk for islets and subjects.

Publisher

SAGE Publications

Subject

Transplantation,Cell Biology,Biomedical Engineering

Cited by 6 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. Production of biopharmaceuticals from transgenic animals;Pharmaceutical Biotechnology in Drug Development;2023

2. Modulating the foreign body response of implants for diabetes treatment;Advanced Drug Delivery Reviews;2021-07

3. Characterizing and overcoming innate immunity in beta-cell replacement therapy;Journal of Immunology and Regenerative Medicine;2020-12

4. Polymeric Approaches to Reduce Tissue Responses Against Devices Applied for Islet-Cell Encapsulation;Frontiers in Bioengineering and Biotechnology;2019-06-04

5. Physical Protection of Pancreatic Islets for Transplantation;Biomaterials - Physics and Chemistry - New Edition;2018-05-02

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