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العنوان
Genetic profiling of cell free circulating tumor DNA in breast cancer patients /
الناشر
Mai Mohamed Elsayed Lotfy ,
المؤلف
Mai Mohamed Elsayed Lotfy
هيئة الاعداد
باحث / Mai Mohamed Elsayed Lotfy
مشرف / Abdelrahman Nabawy Zekri
مشرف / Amany Abdelhhameed Aboubakr
مشرف / Zeinab Korany M. Hassan
تاريخ النشر
2021
عدد الصفحات
138 P. :
اللغة
الإنجليزية
الدرجة
الدكتوراه
التخصص
الطب
تاريخ الإجازة
13/9/2020
مكان الإجازة
جامعة القاهرة - معهد الأورام القومى - Cancer Biology
الفهرس
Only 14 pages are availabe for public view

from 150

from 150

Abstract

detected pathogenic variants (PVs) and likely pathogenic variants (LPVs). These genes were found to be involved in DNA repair mechanisms and WNT/Ý-catenin signalling pathways that will ultimately lead to cancer development. Also, it was revealed that 27.2% of the tissue-derived PVs/LPVs could be detected in ctDNAs, and 35.7% of ctDNA-derived PVs/LPVs could be found in paired tissues. The overall concordance rates for all of the identified somatic variants, PVs/LPVs only and genes carrying PVs/LPVs between both assays across all patients are 85.48%, 82.46% and 76.10%, respectively. According to their Cohen{u2019}s Kappa values, they have a statistically significant slight to fair agreement in both biopsies. While, the positive concordance rates for all of the identified somatic variants, PVs/LPVs only and the genes carrying PVs/LPVs in both assays across all patients are 28.77%, 7.79% and 11.56%, respectively. The level of agreement between the 2 assays -confined to the presence of concordant variants only- was represented by the negative values of Cohen{u2019}s Kappa which implies a statistically significant disagreement between the two platforms