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Original Article

First successful xenotransplantation of microencapsulated human parathyroid tissue in experimental hypopara-thyroidism: Long-term function without immunosuppression

, , , , , & show all
Pages 617-626 | Received 17 Sep 1996, Accepted 14 Dec 1996, Published online: 26 Jun 2009
 

Abstract

Owing to the complexity of the parathyroid hormone's metabolic interactionsclinical hypoparathyroidism is one of the most difficult of all endocrine disorders to treat. Thereforecausative treatment of this disorder by transplantation of parathyroid glands is highly desirable., We have recently documented the long-term in vivo function of iso- and allotransplanted rat parathyroid tissue without systemic immunosuppression in an animal model., In view of the potential clinical use of this methodhuman parathyroid tissue has been microencapsulated and transplanted over the highest immunological barrier., In a controlledlong-term animal study in the parathyroidectomized ratthe effect of microencapsulation on xenotransplanted human parathyoid tissue was evaluated over 30 weeks (native and microencapsulated parathyroid tissue = 40 rats respectively)., Functionallyhuman parathyroid tissue was able to replace that of the rat., All animals that had received microencapsulated parathyroid tissue were normocalcemic for 16 weeks; 27/40 at the end of the study., In contrastserum calcium concentrations dropped to post-parathyroidectomy levels within 4 weeks in those animals that had received native tissue only., Histologic evaluation of the explantedfunctionally successful xenografts showed vital parathyroid tissue inside intact microcapsules surrounded by a small rim of fibroblasts., Avital fibrotic remnants were demonstrated in animals with non-encapsulated parathyroid tissue., Thuswe have established the feasibility of microencapsulation of human parathyroid tissuepreserving its viability over long periods in vivo even if xenotransplanted., In combination with an improved tissue culture methodtransplantation of human parathyroid tissue and maintenance of its physiological function is reproducibly achieved without postoperative systemic immunosuppression over the highest transplantation barrier., This may be a crucial step towards the first clinical application of this method.

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