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Načrtovanje himernih antigenskih receptorjev z uporabo alternativnih kostimulatornih domen iz signalnih poti celic T
ID Koplan, Eva (Author), ID Fink, Tina (Mentor) More about this mentor... This link opens in a new window

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Abstract
Imunoterapija s celicami T, ki imajo vgrajen himerni antigenski receptor (celice CAR-T) ima poleg številnih pozitivnih učinkov tudi nekaj pomanjkljivosti, kot so prekomeren imunski odziv, neuspešno zdravljenje in ponovitev bolezni. V izogib temu je potrebno načrtovati konstrukte CAR, ki bi imeli nižji aktivacijski prag in tako ob nižji koncentraciji tumorskega antigena prožili močen protitumorski odziv. Receptorji na celicah CAR-T so kompleksne strukture, ki omogočajo številne spremembe in posledično različne odzive na tumorski antigen. V magistrski nalogi smo pripravili različne genske konstrukte, ki so vsebovali spremembe v kostimulatornih domenah ter kombinacije pristopov za ojačanje odziva. Izražanje CAR na površini elektroporiranih celic Jurkat smo preverili z metodo pretočne citometrije, z metodo ELISA pa smo spremljali izločanje hIL-2, ki je bilo povečano ob dodatku povezovalnega člena za aktivacijo celic T (LAT) v kombinaciji s kostimulatorno domeno 4-1BB. Prisotnost variabilnega fragmenta CD20 v strukturi CAR je kazala močnejši protitumorski učinek v primerjavi s CD19 različico. Prav tako je dodatek alternativne domene SLP-76 iz mikrogruče LAT v strukturo CAR pozitivno vplival na izločanje hIL-2 ob prisotnosti kostimulatorne domene 4-1BB. Pokazali smo tudi, da se CAR-T s kostimulatorno domeno iz T-celičnega signaliziranja aktivira tudi ob odsotnosti CD3ζ domene. Uspešno smo testirali tudi nekaj pristopov za znižanje tonične signalizacije, kot so zamenjave različnih tirozinov v LAT, mutacije v genskih regijah, ki kodirajo motive ITAM, in kombinacije teh dveh pristopov.

Language:Slovenian
Keywords:CAR-T, celična terapija, imunoterapija raka, kostimulatorne domene, struktura CAR, LAT
Work type:Master's thesis/paper
Typology:2.09 - Master's Thesis
Organization:BF - Biotechnical Faculty
Year:2024
PID:20.500.12556/RUL-161837 This link opens in a new window
COBISS.SI-ID:207690755 This link opens in a new window
Publication date in RUL:15.09.2024
Views:133
Downloads:582
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Secondary language

Language:English
Title:Design of chimeric antigen receptors using alternative costimulatory domains from T-cell signaling
Abstract:
In addition to many positive effects, immunotherapy with CAR-T cells also has some disadvantages, such as excessive immune response, treatment failure and disease recurrence. To avoid this, it is necessary to design CAR constructs that would have a lower activation threshold and thus trigger a strong antitumor response at a lower concentration of tumor antigen. The receptors on CAR-T cells are complex structures that enable many changes and consequently different responses to the tumor antigen. In this master's thesis, we prepared various genetic constructs that contained changes in costimulatory domains and combinations of response amplification approaches. The expression of CAR on the surface of electroporated Jurkat cells was checked by flow cytometry and the secretion of hIL-2, which was increased by the addition of LAT in combination with the 4-1BB costimulatory domain, was monitored by the ELISA method. The presence of the variable CD20 fragment in the CAR structure showed a stronger antitumor effect compared to the CD19 variant. Also, the addition of the alternative SLP-76 domain from the LAT microcluster to the CAR structure had a positive effect on hIL-2 secretion in the presence of the 4-1BB costimulatory domain. We also showed that CAR-T with a costimulatory domain from T-cell signaling is activated even in the absence of the CD3ζ domain. We have also successfully tested several approaches of reducing tonic signaling, such as mutations of different tyrosine residues in LAT, mutations of ITAM motifs, and combinations of these two approaches.

Keywords:CAR-T, cell therapy, cancer immunotherapy, costimulatory domains, CAR structure, LAT

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