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Povezanost polimorfizmov v genih FCGR3A, FCGR2A in IL12B z odzivom na zdravljenje Crohnove bolezni z ustekinumabom
ID Kuk, Jurij (Author), ID Ostanek, Barbara (Mentor) More about this mentor... This link opens in a new window, ID Aguiar Zdovc, Jurij (Comentor)

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Abstract
Crohnova bolezen je kompleksna kronična vnetna bolezen, ki lahko prizadene celoten gastrointestinalni trakt. Gre za avtoimunsko bolezen, v nastanek katere so vpleteni genetski, imunološki in okoljski dejavniki. Diagnosticiramo jo z laboratorijskimi in endoskopskimi metodami, za njeno zdravljenje je na voljo širok nabor različnih skupin zdravil. Eno novejših je tudi ustekinumab, monoklonsko protitelo razreda IgG, ki se specifično veže na podenoto p40 v interlevkinu 12 in interlevkinu 23, ter s tem prepreči kaskado provnetnih procesov v celici. S svojo učinkovitostjo pri indukciji in vzdrževanju remisije predstavlja alternativo zdravljenju z zaviralci dejavnika tumorske nekroze alfa, vendar pri obeh ostajajo bolniki, ki se na terapijo ne odzivajo. Namen magistrske naloge je bil raziskati povezavo med izbranimi polimorfizmi genov IL12B, FCGR2A in FCGR3A in odzivom na zdravljenje Crohnove bolezni z ustekinumabom. Iz polne krvi 57 preiskovancev smo izolirali genomsko DNA in izvedli genotipizacijo z verižno reakcijo s polimerazo v realnem času s pomočjo hidrolizirajočih sond. Podatke o preiskovancih, njihovih genotipih, ter vrednostih biokemijskih in endoskopskih kazalnikov odziva na zdravljenje smo statistično analizirali. Pri IL12B rs3212227 smo glede na koncentracijo fekalnega kalprotektina opazili mejno slabši odziv (p=0,088) na zdravljenje nemutiranih homozigotov (AA) v primerjavi z drugima združenima genotipoma. Pri istem genotipu smo glede na točkovnik SES-CD opazili tudi slabši odziv na zdravljenje (p=0,043) mutiranih homozigotov (CC) v primerjavi z drugima združenima genotipoma. Pri IL12B rs3213094 smo glede na koncenracijo fekalnega kalprotektina opazili slabši odziv (p=0,088) nemutiranih homozigotov (CC) v primerjavi z drugima združenima genotipoma. Pri IL12B rs3213094 smo glede na SES-CD opazili tudi slabši odziv (p=0,043) mutiranih homozigotov (TT) v primerjavi z drugima genotipoma. Pri IL12B rs6887695 smo glede na koncentracijo kalprotektina opazili boljši odziv (p=0,012) heterozigotov (GC) v primerjavi z drugima posameznima genotipoma. Ti bolniki (GC) so dosegali biokemijsko remisijo v višjem deležu (p=0,010) v primerjavi z drugima posameznima genotipoma. Za ta polimorfizem smo glede na koncentracijo kalprotektina opazili tudi slabši odziv (p=0,076) nemutiranih homozigotov (GG), ki so dosegali biokemijsko remisijo v nižjem deležu (p=0,09) v primerjavi z drugima združenima genotipoma. Za FCGR2A rs1801274 nismo opazili povezav z odzivom na zdravljenje. Tudi za FCGR3A rs396991 nismo opazili povezav z odzivom na zdravljenje, smo pa ob začetku zdravljenja opazili nižje koncentracije (p=0,059) fekalnega kalprotektina pri mutiranih homozigotih (CC) v primerjavi z drugima združenima genotipoma. Modeli multivariabilne linearne in logistične regresije so pokazali, da so z odzivom povezane spremenljivke: starost, spol, prisotnost genotipa heterozigotov za FCGR3A, heterozigotov IL12B rs6887695, mutiranih homozigotov IL12B rs3212227 in rs3213094, odsotnost prehodne biološke terapije in prisotnost ulkusa ob začetku zdravljenja. Rezultati naloge kažejo, da so za razjasnitev klinične pomembnosti genetskih polimorfizmov pri zdravljenju z ustekinumabom potrebne nadaljnje raziskave z večjim številom preiskovancev, osredotočene na povezave med IL12B rs3212227, IL12B rs6887695 in odzivom na zdravljenje, ter dodatnim vplivom haplotipa HLA-Cw6.

Language:Slovenian
Keywords:Crohnova bolezen, ustekinumab, genotipizacija, verižna reakcija s polimerazo v realnem času, hidrolizirajoče sonde, gen IL12B, gen FCGR2A, gen FCGR3A
Work type:Master's thesis/paper
Organization:FFA - Faculty of Pharmacy
Year:2022
PID:20.500.12556/RUL-137431 This link opens in a new window
Publication date in RUL:17.06.2022
Views:697
Downloads:85
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Secondary language

Language:English
Title:The association between FCGR3A, FCGR2A and IL12B gene polymorphisms and response to ustekinumab in Crohn's disease treatment
Abstract:
Crohn's disease is complex chronic inflammatory bowel disease that can affect the entire digestive tract. As an autoimmune disease, the exact pathogenesis is poorly understood and is a product of several genetic, immunological, and environmental factors. Diagnosis is made with laboratory and endoscopic methods. Treatment includes a wide variety of drug options. Ustekinumab, a novel medication, is a monoclonal antibody that binds to the p40 subunit shared by interleukin 12 and interleukin 23, thus preventing pro-inflammatory processes in the cell. It is effective at inducing and maintaining remission, and so serves as an alternative to anti-tumor necrosis factor drugs. However, some patients do not achieve a satisfactory response to the treatment. The aim of our study was to improve the understanding of the association between gene polymorphisms in IL12B, FCGR2A in FCGR3A and response to ustekinumab treatment in Crohn's disease. First, we isolated DNA from the whole blood of 57 patients and genotyped it using real time polymerase chain reaction and hydrolysis probes. In addition to patients’ genotypes, we collected data of patients’ demographic, biochemical and clinical characteristics, as well as recorded their biochemical and endoscopic markers of response to treatment. Subsequently, we statistically evaluated the association between patients’ characteristics and their response to treatment, For IL12B rs3212227, we observed two relationships: a worse treatment response associated with wild type homozygous genotype (AA) when comparing fecal calprotectin concentration to the other two genotypes combined (p=0,088); and a worse treatment response associated with mutated homozygous genotype (CC) when comparing SES-CD scoring to the other two genotypes combined (p=0,043). For IL12B rs3213094 the same relationships were found: a worse treatment response, associated with wild type homozygous genotype (CC) when comparing fecal calprotectin concentration to the other two genotypes combined (p=0,088); and a worse treatment response associated with mutated homozygous genotype (TT) when comparing SES-CD scoring to the other two genotypes combined (p=0,043). For IL12B rs6887695, we observed the association between heterozygous genotype (GC) and better treatment response compared to both genotypes individually based on the fecal calprotectin concentration (p=0,012) and higher proportion of biochemical response (p=0,010). We also observed a worse response of wild type homozygous genotype (GG) compared to the other two genotypes combined based on the fecal calprotectin concentration (p=0,076) and a lower proportion of biochemical response (p=0,09). For FCGR2A rs1801274 we observed no association with treatment response. Similarly we observed no association for FCGR3A rs396991 with treatment response, however the mutated homozygous genotype (CC) had a nonsignificant trend of a lower fecal calprotectin concentration at baseline compared to the other two genotypes combined (p=0,059). Modeling with multivariable linear and logistic regression showed the association between treatment response and the following variables: age, sex, heterozygous genotype FCGR3A, heterozygous genotype IL12B rs6887695, mutated homozygous genotype IL12B rs3212227 and rs3213094, bio naivety and ulcers at baseline. Our result indicate that more studies with larger sample size are necessary to clarify the clinical relevance of genetic polymorphisms in ustekinumab treatment, and we suggest that further reasearch could be focused especially on IL12B rs3212227 and IL12B rs6887695 polymorphisms while considering the effect of HLA-Cw6 haplotype as well.

Keywords:Crohn's disease, ustekinumab, genotyping, real time polymerase chain reaction, hydrolysis probes, gene IL12B, gene FCGR2A, gene FCGR3A

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