Role of SP-A gene polymorphism in lung transplantation

Lung transplantation is a widely accepted therapeutic option for end stage lung disease. Clinical outcome is yet challenged by primary graft failure responsible for the majority of the early mortality, by chronic allograft dysfunction and chronic rejection accounting for more than 30% of deaths afte...

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Main Author: Aramini, Beatrice <1979>
Other Authors: Mattioli, Sandro
Format: Doctoral Thesis
Language:en
Published: Alma Mater Studiorum - Università di Bologna 2011
Subjects:
Online Access:http://amsdottorato.unibo.it/3634/
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spelling ndltd-unibo.it-oai-amsdottorato.cib.unibo.it-36342014-03-24T16:29:14Z Role of SP-A gene polymorphism in lung transplantation Aramini, Beatrice <1979> MED/21 Chirurgia toracica Lung transplantation is a widely accepted therapeutic option for end stage lung disease. Clinical outcome is yet challenged by primary graft failure responsible for the majority of the early mortality, by chronic allograft dysfunction and chronic rejection accounting for more than 30% of deaths after the third postoperative year. Pulmonary surfactant proteins (SP) A, B, C and D are one of the first host defense mechanisms the lung can mount. SP-A in particular, produced by the type II pneumocytes, is active in the innate and adaptive immune system being an opsonin, but also regulating the macrophage and lymphocyte response. The main hypothesis for this project is that pulmonary surfactant protein A polymorphism may determine the early and long term lung allograft survival. Of note SP-A biologic activity seems to be genetically determined and SP-A polymorphisms have been associated to various lung disease. The two SP-A genes SP-A1 and SP-A2 have several polymorphisms within the coding region, SP-A1 (6A, 6A2-20), and SP-A2(1A, 1A0-13). The SP-A gene expression is regulated by cAMP, TTF-1 and glucocorticoids. In vitro studies have indicated that SP-A1 and SP-A2 gene variants may have a variable response to glucocorticoids. We proposed to determine if SP-A gene polymorphism predicts primary graft dysfunction and/or chronic lung allograft dysfunction and if SP-A may serve as a biomarker of lung allograft dysfunction. We also proposed to study the interaction between immunosuppressive drugs and SP-A expression and determine whether this is dependent on SP-A polymorphisms. This study will generate novel information improving our understanding of lung allograft dysfunction. It is conceivable that the information will stimulate the interest for a multi centre study to investigate if SP-A polymorphism may be integrated in the donor lung selection criteria and/or to implement post transplant tailored immunosuppression. Alma Mater Studiorum - Università di Bologna Mattioli, Sandro 2011-05-02 Doctoral Thesis PeerReviewed application/pdf en http://amsdottorato.unibo.it/3634/ info:eu-repo/semantics/restrictedAccess
collection NDLTD
language en
format Doctoral Thesis
sources NDLTD
topic MED/21 Chirurgia toracica
spellingShingle MED/21 Chirurgia toracica
Aramini, Beatrice <1979>
Role of SP-A gene polymorphism in lung transplantation
description Lung transplantation is a widely accepted therapeutic option for end stage lung disease. Clinical outcome is yet challenged by primary graft failure responsible for the majority of the early mortality, by chronic allograft dysfunction and chronic rejection accounting for more than 30% of deaths after the third postoperative year. Pulmonary surfactant proteins (SP) A, B, C and D are one of the first host defense mechanisms the lung can mount. SP-A in particular, produced by the type II pneumocytes, is active in the innate and adaptive immune system being an opsonin, but also regulating the macrophage and lymphocyte response. The main hypothesis for this project is that pulmonary surfactant protein A polymorphism may determine the early and long term lung allograft survival. Of note SP-A biologic activity seems to be genetically determined and SP-A polymorphisms have been associated to various lung disease. The two SP-A genes SP-A1 and SP-A2 have several polymorphisms within the coding region, SP-A1 (6A, 6A2-20), and SP-A2(1A, 1A0-13). The SP-A gene expression is regulated by cAMP, TTF-1 and glucocorticoids. In vitro studies have indicated that SP-A1 and SP-A2 gene variants may have a variable response to glucocorticoids. We proposed to determine if SP-A gene polymorphism predicts primary graft dysfunction and/or chronic lung allograft dysfunction and if SP-A may serve as a biomarker of lung allograft dysfunction. We also proposed to study the interaction between immunosuppressive drugs and SP-A expression and determine whether this is dependent on SP-A polymorphisms. This study will generate novel information improving our understanding of lung allograft dysfunction. It is conceivable that the information will stimulate the interest for a multi centre study to investigate if SP-A polymorphism may be integrated in the donor lung selection criteria and/or to implement post transplant tailored immunosuppression.
author2 Mattioli, Sandro
author_facet Mattioli, Sandro
Aramini, Beatrice <1979>
author Aramini, Beatrice <1979>
author_sort Aramini, Beatrice <1979>
title Role of SP-A gene polymorphism in lung transplantation
title_short Role of SP-A gene polymorphism in lung transplantation
title_full Role of SP-A gene polymorphism in lung transplantation
title_fullStr Role of SP-A gene polymorphism in lung transplantation
title_full_unstemmed Role of SP-A gene polymorphism in lung transplantation
title_sort role of sp-a gene polymorphism in lung transplantation
publisher Alma Mater Studiorum - Università di Bologna
publishDate 2011
url http://amsdottorato.unibo.it/3634/
work_keys_str_mv AT araminibeatrice1979 roleofspagenepolymorphisminlungtransplantation
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