izpis_h1_title_alt

Molekulsko profiliranje majhnih zunajceličnih veziklov in njihovih izvornih celic pri antifosfolipidnem sindromu
ID Štok, Ula (Author), ID Žigon, Polona (Mentor) More about this mentor... This link opens in a new window, ID Čučnik, Saša (Comentor)

.pdfPDF - Presentation file, Download (44,10 MB)
MD5: FFAD55D0D6D10CBB867175AAA2D23CE8

Abstract
Antifosfolipidni sindrom (APS) je sistemska avtoimunska bolezen, ki se klinično izraža s trombozami v venah, arterijah ali mikrožilju in/ali z zapleti v nosečnosti, laboratorijsko pa s prisotnostjo antifosfolipidnih protiteles (aPL). Vezava aPL na površino celic sproži njihovo aktivacijo, ki vodi v sproščanje zunajceličnih veziklov (EVs po angleškem izrazu »extracellular vesicles«). Tako v plazmi bolnikov z APS kot in vitro so najpogosteje preučevani srednji/veliki vezikli endotelijskega izvora. Ostali podtipi veziklov ter skupina majhnih zunajceličnih veziklov (sEVs) so pri APS slabše raziskani. Namen doktorskega dela je ugotoviti pomen izločanja sEVs in njihovega molekulskega profila pri razlagi patogeneze in heterogenosti APS. V plazmi bolnikov s trombotičnim APS smo pokazali zvišane vrednosti celokupnih in endotelijskih sEVs ter nekaterih podtipov, ki nakazuje na aktivacijo endotelija in trombocitov tudi v odsotnosti akutnega trombotičnega dogodka. Čeprav pri APS nismo zaznali zvišane pojavnosti monocitnih sEVs, je analiza njihovih izvornih celic pokazala na aktivacijo monocitov v polni krvi bolnikov z APS. Zvišano izražanje integrina VLA4 na monocitih je lahko vpleteno v intenzivnejšo interakcijo med monociti in endotelijem. Blokada tega integrina bi lahko v prihodnosti predstavljala alternativo za zdravljenje težjih in na zdravljenje neodzivnih bolnikov z APS. Rezultati raziskav v okviru doktorske naloge kažejo na to, da je profil sEVs, ki jih izločajo različne celice pri bolnikih s trombotičnim APS, spremenjen ter da nakazuje na izvor sEVs in aktivacijski status njihovih izvornih celic. S tem smo pokazali, da sEVs pri APS zagotovo igrajo pomembno vlogo, vendar so potrebne nadaljnje raziskave, ki bodo natančneje opredelile učinke sEVs na endotelijske celice, monocite in trombocite, ter rezultate naših raziskav natančneje umestile v patogenezo APS.

Language:Slovenian
Keywords:Antifosfolipidni sindrom, antifosfolipidna protitelesa, zunajcelični vezikli, endotelijske celice, monociti
Work type:Doctoral dissertation
Organization:FFA - Faculty of Pharmacy
Year:2023
PID:20.500.12556/RUL-143854 This link opens in a new window
Publication date in RUL:15.01.2023
Views:896
Downloads:104
Metadata:XML DC-XML DC-RDF
:
Copy citation
Share:Bookmark and Share

Secondary language

Language:English
Title:Molecular profiling of small extracellular vesicles and their originating cells in antiphospholipid syndome
Abstract:
Antiphospholipid syndrome (APS) is a systemic autoimmune disorder characterized by thromboembolism, obstetric complications, and the presence of antiphospholipid antibodies (aPL). Binding of aPL to the cell surface triggers their activation, leading to the release of extracellular vesicles (EVs). Medium/large vesicles of endothelial origin are most commonly studied in vitro as well as in plasma of APS patients. Other subtypes of vesicles and the group of small extracellular vesicles (sEVs) are less well understood in APS. The aim of this dissertation is to determine the importance of sEVs and their molecular profile in explaining the pathogenesis and heterogeneity of APS. In the plasma of thrombotic APS patients, we found increased levels of total sEVs, endothelial sEVs, and some sEV subtypes, indicating endothelial and platelet activation even in the absence of an acute thrombotic event. Although we did not detect increased levels of monocyte sEVs in APS, analysis of their cells of origin suggests monocyte activation. The increased surface expression of the integrin VLA4 on monocytes could be involved in the enhanced interaction between monocytes and the endothelium. Blocking this integrin could provide an alternative treatment option for more severe and difficult-to-treat APS patients in the future. Taken together, our results suggest that the profile of secreted sEVs is altered in patients with thrombotic APS, indicating their origin and the activation status of the cells of origin. Thus, we have shown that sEVs play an important role in APS, but further research is needed to more precisely define the effects of sEVs on endothelial cells, monocytes, and platelets and to better situate our findings in the pathogenesis of APS.

Keywords:Antiphospholipid syndrome, antiphospholipid antibodies, extracellular vesicles, endothelial cells, monocytes

Similar documents

Similar works from RUL:
Similar works from other Slovenian collections:

Back