Mutacije u genima koji doprinose riziku za oboljevanje od karcinoma dojke i/ili jajnika kod BRCA1 i BRCA2 negativnih visokorizičnih porodica u Srbiji
Mutations in breast cancer susceptibility genes in BRCA1 and BRCA2 negative hereditary breast and ovarian cancer families in Serbia
Author
Krivokuća, Ana M.Mentor
Stamenković-Radak, Marina
Committee members
Branković-Magić, Mirjana
Radulović, Siniša
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Uvod: Nasledni karcinom čini 5-10% od svih slučajeva karcinoma dojke i prvenstveno je
povezan sa štetnim mutacijama u visoko penetrabilnim genima BRCA1 i BRCA2. I pored
intenzivnog istraživanja ostatka nasledne komponente, treći visoko penetrabilni gen u
karcinomu dojke (BRCA3) još uvek nije pronadjen. Pod okriljem poligenog modela
otkrivene su tri grupe alela koji doprinose riziku za karcinom dojke: visoko penetrabilni,
koji povećavaju rizik na 40-85% (BRCA1, BRCA2, TP53), srednje penetrabilni (povećavaju
rizik na 20-40%) kao što su CHEK2, RAD51, RAD51C i XRCC1, i učestale genske
varijante koje su nisko penetrabilne. Pored štetnih mutacija u ovim genima, odredjene
polimorfne varijante mogu uticati na efikasnost popravke grešaka u DNK i na nastanak
karcinoma.
Cilj: Obzirom da prisustvo mutacija u BRCA1/2 genima ne može da opiše celu genetičku
osnovu naslednog karcinoma dojke, cilj ovog rada je istraživanje prisustva populaciono
specifičnih mutacija u drugim genima (TP53, CHEK2, NBS1, R...
Background: 5-10% of all breast cancer cases are hereditary, and are often caused by
deleterious mutations in high penetrance BRCA1 and BRCA2 genes. Despite significant
efforts in unraveling the rest of the familial component, BRCA3 could not be identified.
Under the polygenic model of inheritance, three groups of genetic predisposition alleles
have been identified so far: high-risk genes, conferring 40–85% lifetime risk (BRCA1,
BRCA2, TP53), moderate-risk genes (20–40% lifetime risk) including CHEK2, RAD51,
RAD51C and XRCC1, and low-risk common alleles. Besides the deleterious mutations in
these genes, certain polymorphic variants have functional significance in DNA repair
pathways, and may be responsible for cancer development.
Aim: Considering the fact that mutations in BRCA1/2 can’t explain the whole range of
hereditary predisposition to breast cancer, we aimed to investigate the presence and
frequency of population-specific mutations in other susceptibility genes (TP53, CHEK2,
NBS...