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Potek bolezni pri bolnikih s kastracijsko odpornim rakom prostate zdravljenih z avtolognimi imunohibridomi
ID Hawlina, Simon (Author), ID Haque Chowdhury, Helena (Mentor) More about this mentor... This link opens in a new window, ID Smrkolj, Tomaž (Comentor)

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Abstract
Uvod: Rak prostate je v Sloveniji najpogosteje diagnosticirana oblika rakave bolezni in drugi najpogostejši vzrok smrti zaradi raka. Pri približno tretjini kastriranih bolnikov se razvije neozdravljivi, kastracijsko odporni rak prostate (KORP). V zadnjem desetletju so v vzponu nove strategije zdravljenja in obvladovanja bolezni, ki bi upočasnile njeno napredovanje in širjenje ter podaljšale preživetje ob ohranitvi kakovosti življenja. Mednje spada tudi imunoterapija. Namen: Rakave celice v razvoju karcinogeneze razvijejo številne mehanizme, ki jim omogočajo preživetje, proliferacijo in zasevanje. Tako je tudi pri KORP, zato ima imunoterapija velik potencial. Ena od strategij imunske terapije, ki smo jo raziskali, so celična cepiva z dendritičnimi celicami. Uporabili smo napredno avtologno celično cepivo z imunohibridomi (aHyC), ki je bilo razvito v Republiki Sloveniji. Ocenili smo varnost novega terapevtskega pristopa in proučili učinke aHyC na potek bolezni KORP s spremljanjem različnih kliničnih parametrov. Domnevali smo, da bo personalizirana imunoterapija varna, brez resnih neželenih učinkov in ne bo negativno vplivala na preživetje bolnikov s KORP, ki še niso prejeli standardne terapije. Metode: V randomizirani, dvojno slepi, s placebom nadzorovani in navzkrižni klinični raziskavi I./II. faze je bilo vključenih 22 bolnikov s KORP brez simptomov ali le z minimalnimi. Avtologno celično cepivo z imunohibridomi (aHyC) smo pripravili z elektrofuzijo bolnikovih lastnih dendritičnih in tumorskih celic ter subkutano aplicirali nazaj v bolnike. Bolniki so bili naključno porazdeljeni v 2 zaslepljeni skupini; v skupino aHyC (12 bolnikov), ki je prejela aHyC, in skupino placebo (kontrola), ki aHyC v prvi fazi raziskave ni prejela (10 bolnikov). Sedem tednov po zadnjem odmerku je sledilo prekrižanje: bolniki skupine aHyC so prejeli placebo in bolniki skupine placebo so prejeli aHyC v enakem režimu. Vsak je aHyC prejel 4-krat v 3-tedenskih intervalih. Uspešnost zdravljenja smo vrednotili z merjenjem kliničnih, slikovnih, laboratorijskih in imunskih parametrov ter s spremljanjem kakovosti življenja. Opravljena je bila analiza preživetja in opredelitev napovednih dejavnikov. Rezultati: V obeh skupinah bolnikov v raziskavi smo zaznali le nekaj blagih neželenih učinkov; pri 42 % bolnikov v skupini aHyC in pri 38 % bolnikov v skupini placebo (z-test, p = 0,85). Kakovost življenja se z imunoterapijo ni spremenila, kar smo ocenili s seštevkom točk vprašalnika EORTC QLQ-C30, ki je bil pred aplikacijo aHyC 64,0 ± 3,7, po njej pa 65,5 ± 4,5 (p = 0,67). Vpliva na slikovne in na večino laboratorijskih parametrov nismo zaznali. V skupini aHyC smo po zdravljenju ugotovili znatno zmanjšanje vrednosti kostne alkalne fosfataze in osteokalcina (p < 0,05, p < 0,01) v primerjavi z vrednostmi pred zdravljenjem. Mediano celokupno preživetje vseh bolnikov, ki so prejeli aHyC (n = 19) je bilo 58,8 mesecev. Ugotovili smo, da ni statistično značilne povezave med številom živih celic v cepivu in med preživetjem (korelacijski koeficient, r = -0,14, p = 0,56) ter tudi časom do naslednje standardne terapije (r = 0,36, p = 0,13). Zaključek: Izsledki prispevajo k razvoju znanosti na področju uroonkologije in imunologije ter omogočajo boljše razumevanje poteka bolezni KORP. Imunoterapija z aHyC kaže prve varnostne signale in nima vpliva na kakovost življenja.

Language:Slovenian
Keywords:Kastracijsko odporen rak prostate, Cepiva z dendritičnimi celicami, avtologno celično cepivo z imunohibridomi, Imunoterapija
Work type:Doctoral dissertation
Organization:MF - Faculty of Medicine
Year:2022
PID:20.500.12556/RUL-137845 This link opens in a new window
COBISS.SI-ID:115301635 This link opens in a new window
Publication date in RUL:03.07.2022
Views:1361
Downloads:106
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Secondary language

Language:English
Title:The course of disease in patients with castration resistant prostate cancer treated with autologous immunohybridoma cell
Abstract:
Introduction: Prostate cancer is the most commonly diagnosed cancer in Slovenia and the second most common cause of death due to cancer. About one-third of castrated patients develop incurable, castration-resistant prostate cancer (CRPC). In the last decade, new strategies for treating and controlling the disease have been on the rise, slowing its progression and spread and prolonging survival while maintaining the quality of life. These include immunotherapy. Aim: In the development of carcinogenesis, cancer cells develop a number of mechanisms that allow cancer cells to survive, proliferate and metastasize. This is also the case with CRPC, so immunotherapy has great potential. One of the immunotherapy strategies we investigated is dendritic cell-based vaccines. We used an advanced autologous cell vaccine with immunohybridomas (aHyC), which was developed in the Republic of Slovenia. We evaluated the safety of a new therapeutic approach and examined the effects of aHyC on the course of CRPC disease by monitoring various clinical parameters. We hypothesized that personalized immunotherapy would be safe, free of serious adverse events, and would not adversely affect the survival of patients with CRPC who had not yet received standard therapy. Methods: A randomized, double-blind, placebo-controlled, cross-over, phase I/II clinical trial included 22 asymptomatic/minimally symptomatic patients with CRPC. An autologous immunohybridoma cell-based vaccine (aHyC) was prepared by electrofusion of the patient's own dendritic and tumor cells and applied back to the patients, subcutaneously. Patients were randomly divided into 2 blinded groups; the aHyC group (12 patients) who received aHyC and the placebo group (control) who did not receive aHyC (10 patients). Seven weeks after the last dose, a crossover occurred: aHyC group received placebo and placebo group received aHyC in the same regimen. Patients received aHyC four times at three-week intervals. The success of the treatment was evaluated by measuring clinical, imaging, laboratory and immune parameters and by monitoring the quality of life. Survival analysis and identification of prognostic factors were performed. Results: Only a few mild adverse events were detected in both groups of patients in the study; in 42 % of patients in the aHyC group and in 38 % of patients in the placebo group (z-test, p = 0.85). The quality of life did not change with immunotherapy, as assessed by the sum of the EORTC QLQ-C30 questionnaire scores, which was 64.0 ± 3.7 before aHyC administration and 65.5 ± 4.5 after (p = 0.67). No effects on imaging and on most laboratory parameters were detected. In the aHyC group, a significant decrease in bone alkaline phosphatase and osteocalcin was observed after treatment (p <0.05, p <0.01) compared to pre-treatment values. The median overall survival of all patients receiving aHyC (n = 19) was 58.8 months. We found that there was no statistically significant association between the number of living cells in the vaccine and survival (correlation coefficient, r = -0.14, p = 0.56) as well as the time to the next standard therapy (r = 0.36, p = 0.13). Conclusion: The results contribute to the development of science in the field of uro-oncology and immunology and provide a better understanding of the course of CRPC disease. Immunotherapy with aHyC shows the first safety signals and has no effect on quality of life.

Keywords:Castration-resistant prostate cancer, Dendritic-tumor hybridoma vaccine, Autologous cell therapy, Immunotherapy

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