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Preureditev gena IGH pri bolnikih s kronično limfatično levkmeijo : magistrska naloga
ID Zorko, Katarina (Avtor), ID Podgornik, Helena (Mentor) Več o mentorju... Povezava se odpre v novem oknu

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Izvleček
Kronična limfatična levkemija (KLL) je najpogostejša vrsta levkemije pri odraslih ljudeh zahodne zemeljske poloble. Je heterogena bolezen z raznolikim kliničnim potekom. Znotraj KLL se pojavlja tudi atipična oblika KLL. Za atipično KLL je značilen agresivnejši potek bolezni in krajše preživetje kot pri bolnikih z značilno KLL. Zaradi morfološke in imunofenotipske heterogenosti je pri določenim deležu bolnikov s KLL negotova že sama postavitev diagnoze. Zahtevna je predvsem diferencialna diagnostika med atipično KLL in limfomom plaščnih celic (LPC). Znani so trije bistveni napovedni kazalci pri KLL: citogenetske preureditve, ki jih določano s fluorescenčno in situ hibridizacijo (FISH), ekspresija specifičnih proteinov v ali na limfomskih celicah (predvsem CD38 in ZAP70) in somatska hipermutacija v variabilnem delu gena za težko verigo imunoglobulina (IGHV). Pri okoli 80% bolnikov s KLL ugotovimo citogenetske preureditve, ki imajo vlogo predvsem pri izbiri zdravljenja in napovedi poteka bolezni, manj pa pri postavitvi diagnoze. Te so delecije področij 13q14, 11q22 (ATM) in 17p13 (TP53) ter trisomija kromosoma 12. Preureditve gena IGH na področju 14q32 so pri KLL redke, zato določanja njihove prisotnosti diagnostične smernice zaenkrat še ne predpisujejo. Ker naj bi imele neugoden vpliv na preživetje bolnikov, smo v magistrski nalogi z metodo FISH določili njihovo pogostost pri slovenskih bolnikih s KLL ob ostalih napovedno pomembnih preureditvah. Nato smo ločeno obravnavali bolnike z značilno KLL, atipično KLL in skupino bolnikov z agresivnim potekom bolezni brez značilnih neugodnih citogenetskih preureditev (del(17p13) in/ali del(11q23)). Ugotovili smo, da je najpogostejša preureditev pri slovenskih bolnikih s KLL delecija področja 13q14, sledijo ji delecija gena ATM, trisomija 12 in delecija gena TP53. Pričakovano je preureditev gena IGH najredkejša. V skupini bolnikov z značilno KLL ni bistvenih odstopanj, medtem ko pri skupini bolnikov z atipično KLL najbolj odstopa pojavnost trisomije kromosoma 12, ki je bila prisotna pri polovici teh bolnikov. Med značilno in atipično skupino KLL je statistično značilna razlika v pojavljanju trisomije kromosoma 12 (p=0,0114). CD38 se pogosteje izraža pri bolnikih z atipično KLL kot pa pri bolnikih z značilno KLL, vendar razlika med skupinami ni statistično značilna (p=0,4440). Pri 46,9% bolnikov, pri katerih je imunofenotip celic ustrezal LPC, s FISH preiskavo nismo potrdili za LPC značilne translokacije t(11;14). Tako smo te bolnike prerazporedili med atipične KLL. Zato je nujno, da je v osnovni nabor DNA-sond vključena DNA-sonda, ki je specifična za translokacijo t(11;14), ki obenem pokaže tudi morebitne druge preureditve gena IGH. Preureditev gena IGH smo določili pri 2/85 (2,3%) bolnikih z značilno KLL, pri 2/24 (8,3%) bolnikih z atipično KLL in pri 2/17 (11,8%) bolnikih z agresivnim potekom bolezni, vendar med omenjenimi skupinami ni statistično značilne razlike. Pri dveh bolnikih s preureditvami gena IGH smo določili translokacijo t(2;14), pri dveh translokacijo t(14;18), pri enem translokacijo t(8;14), pri enem translokacijo t(14;19) in pri enem bolniku bialelno preureditev gena IGH. Pri dveh bolnikih partnerskega kromosoma v preureditvi gena IGH nismo uspeli določiti.

Jezik:Slovenski jezik
Ključne besede:kronična limfatična levkemija kromosomske translokacije gojenje celic maligni limfomi
Vrsta gradiva:Magistrsko delo/naloga
Tipologija:2.09 - Magistrsko delo
Organizacija:FFA - Fakulteta za farmacijo
Kraj izida:Ljubljana
Založnik:[K. Zorko]
Leto izida:2015
Št. strani:X, 69 f.
PID:20.500.12556/RUL-121066 Povezava se odpre v novem oknu
UDK:616.155.392+616-07(043.3)
COBISS.SI-ID:3866737 Povezava se odpre v novem oknu
Datum objave v RUL:29.09.2020
Število ogledov:1536
Število prenosov:152
Metapodatki:XML DC-XML DC-RDF
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Sekundarni jezik

Jezik:Angleški jezik
Naslov:IGH rearrangements in patients with chronic lymphocytic leukemia
Izvleček:
Chronic lymphocytic leukemia (CLL) is the most common leukemia of adults of Western world. It is a heterogeneous disease with a diverse clinical course. Within CLL occurs also atypical form of CLL. Atypical CLL is characterized by a more aggressive course of the disease and a shorter survival of patients than in typical CLL. Due to the morphological and immunophenotypical heterogeneity of the disease diagnosis is uncertain in small proportion of patients with CLL. A particularly challenging is a differential diagnosis between atypical CLL and mantle cell lymphoma (MCL). Three main prognostic factors in CLL are: cytogenetic aberrations, which are determined by fluorescence in situ hybridization (FISH), the expression of specific proteins (primarily CD38 and ZAP70) and IGHV mutation status of CLL clone. Cytogenetic rearrangements are detected in up to 80% of CLL patients. They are crucial for treatment descision and as prognostic factor, rather than in establishment of diagnosis. These are trisomy of chromosome 12 and deletions of chromosomal regions 13q14, 11q22 (ATM) and 17p13 (TP53). Chromosome 14q32 translocations involving immunoglobulin heavy chain gene (IGH) are rare in CLL, and their determination is not yet prescribed by diagnostic guidelines. Since it is assumed that they have unfavorable prognostic significance, we determine their frequency in Slovenian CLL patients with others aberrations that have a prognostic impact. Separately, we treated a group of patients with typical CLL, atypical CLL and a group of patients with an unfavorable course of the disease without any of significant adverse cytogenetic rearrangements (del(17p13) or del(11q23)). The most common rearrangement in Slovenian patients with CLL is a deletion of chromosomal region 13q14, followed by a deletion of the gene ATM, trisomy 12, deletion of the gene TP53 and as expected, IGH gene translocations is the rarest. In the group of patients with atypical CLL departed incidence of trisomy 12, which was observed in half of the patients. Between typical and atypical CLL the difference in the frequency of trisomy 12 is statistically significant (p=0.0114). CD38 was more often expressed in patients with atypical CLL than in patients with typical CLL, but the difference between groups was not statistically significant (p=0.4440). In 46,9% of patients with atypical CLL immunophenotyp that corresponded to MCL was determined, but with the FISH analysis for MCL characteristic translocation t(11;14) was not confirmed. Because of that, we have reallocated them into a group of patients with atypical CLL. Therefore, it is necessary that the basic panel of DNA probes includes a DNA probe that is specific for the translocation t(11;14), which at the same time also determines other IGH gene rearrangements. We have found IGH rearrangements in 2/85 (2.3%) patients with typically CLL, in 2/24 (8.3%) patients with atypical CLL and in 2/17 (11.8%) patients with aggressive course of the disease, but the difference between these groups was not statistically significant. In two patients with the IGH gene rearrangement translocation t(2;14) was detected, in two translocation t(14;18), in one translocation t(8;14), in one translocation t(14;19), and in one patient a biallelic rearrangement of IGH gene. In two patients we were not able to determine the partner chromosome involved in IGH gene rearrangement.


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