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W4285804571 endingPage "85" @default.
W4285804571 startingPage "62" @default.
W4285804571 abstract "Breast cancer is responsible for cancer-related death among women globally. The known causes of breast cancer include genetic predisposition, dysregulated hormonal signaling due to psychological stress, and aging and lifestyle factors, such as smoking and alcohol consumption. Due to improved treatment strategies, the overall survival is significantly increased; however, it is still significantly associated with death worldwide. Breast cancer's initiation and progression are strongly influenced by genomic instability. Defect in DNA damage response (DDR) pathways, which enable cells to survive, help in the accumulation of mutation, clonal selection, and expansion of cancer cells. Germline mutation in breast cancer susceptibility genes, BRCA1 and BRCA2, TP53, and PTEN, increases the risk of early onset of disease. During the initial and clonal selection of cancer cells, a defect in one DNA repair pathway could potentially be compensated by another pathway. Therefore, cancer cells with defective DNA repair pathways could be easily killed by targeting the compensatory pathways by inducing synthetic lethality. Evidently, cancer cells with defective DDR or decreased DNA repair capacity show synthetic lethality in monotherapy when the backup DNA repair pathway is inhibited. For instance, tumors with defective homologous recombination (HR) can be targeted by inhibitors of double-strand break repair enzymes. Here, we briefly addressed the relevant factors associated with the development of breast cancer and the role of the DDR factor in the development of breast cancer. In addition, recent treatment strategies targeting genomic instability in breast cancer will be summarized as well as how the genomic instability and defective DDR can be targeted for the treatment of breast cancer." @default.
W4285804571 created "2022-07-19" @default.
W4285804571 creator A5069170880 @default.
W4285804571 creator A5075325966 @default.
W4285804571 date "2022-07-14" @default.
W4285804571 modified "2023-09-27" @default.
W4285804571 title "DNA Damage Response: A Therapeutic Landscape For Breast Cancer Treatment" @default.
W4285804571 cites W1523531555 @default.
W4285804571 cites W1538419182 @default.
W4285804571 cites W1592416724 @default.
W4285804571 cites W1752089945 @default.
W4285804571 cites W1765879118 @default.
W4285804571 cites W1775529440 @default.
W4285804571 cites W1830454849 @default.
W4285804571 cites W1836682153 @default.
W4285804571 cites W1965232465 @default.
W4285804571 cites W1965239527 @default.
W4285804571 cites W1970336739 @default.
W4285804571 cites W1975775716 @default.
W4285804571 cites W1976385056 @default.
W4285804571 cites W1977284533 @default.
W4285804571 cites W1980745735 @default.
W4285804571 cites W1983338915 @default.
W4285804571 cites W1985637723 @default.
W4285804571 cites W1993437245 @default.
W4285804571 cites W1996931025 @default.
W4285804571 cites W1999332886 @default.
W4285804571 cites W2004125597 @default.
W4285804571 cites W2010402298 @default.
W4285804571 cites W2010677667 @default.
W4285804571 cites W2010871781 @default.
W4285804571 cites W2012718299 @default.
W4285804571 cites W2013591933 @default.
W4285804571 cites W2015606965 @default.
W4285804571 cites W2016226903 @default.
W4285804571 cites W2025180999 @default.
W4285804571 cites W2029965175 @default.
W4285804571 cites W2037355114 @default.
W4285804571 cites W2040860750 @default.
W4285804571 cites W2048939997 @default.
W4285804571 cites W2049921243 @default.
W4285804571 cites W2054693978 @default.
W4285804571 cites W2061553377 @default.
W4285804571 cites W2065087624 @default.
W4285804571 cites W2074730941 @default.
W4285804571 cites W2078431196 @default.
W4285804571 cites W2080466594 @default.
W4285804571 cites W2083158919 @default.
W4285804571 cites W2083778750 @default.
W4285804571 cites W2086260870 @default.
W4285804571 cites W2087991548 @default.
W4285804571 cites W2092536432 @default.
W4285804571 cites W2097255042 @default.
W4285804571 cites W2101519297 @default.
W4285804571 cites W2105039611 @default.
W4285804571 cites W2107632586 @default.
W4285804571 cites W2109492174 @default.
W4285804571 cites W2109518208 @default.
W4285804571 cites W2109997465 @default.
W4285804571 cites W2110137106 @default.
W4285804571 cites W2111222453 @default.
W4285804571 cites W2112210405 @default.
W4285804571 cites W2114021402 @default.
W4285804571 cites W2114416638 @default.
W4285804571 cites W2116735990 @default.
W4285804571 cites W2117305280 @default.
W4285804571 cites W2117692326 @default.
W4285804571 cites W2118385896 @default.
W4285804571 cites W2120059431 @default.
W4285804571 cites W2122673427 @default.
W4285804571 cites W2125568481 @default.
W4285804571 cites W2131994307 @default.
W4285804571 cites W2132619562 @default.
W4285804571 cites W2132720619 @default.
W4285804571 cites W2135640980 @default.
W4285804571 cites W2139802796 @default.
W4285804571 cites W2139964075 @default.
W4285804571 cites W2148027217 @default.
W4285804571 cites W2148194373 @default.
W4285804571 cites W2152379507 @default.
W4285804571 cites W2155851270 @default.
W4285804571 cites W2160278162 @default.
W4285804571 cites W2162451014 @default.
W4285804571 cites W2165413853 @default.
W4285804571 cites W2165516672 @default.
W4285804571 cites W2170585132 @default.
W4285804571 cites W2170719826 @default.
W4285804571 cites W2173456459 @default.
W4285804571 cites W2209936495 @default.
W4285804571 cites W2221837786 @default.
W4285804571 cites W2265160193 @default.
W4285804571 cites W2327174419 @default.
W4285804571 cites W2494222141 @default.
W4285804571 cites W2502508548 @default.
W4285804571 cites W2527169367 @default.
W4285804571 cites W2548000951 @default.
W4285804571 cites W2562895910 @default.
W4285804571 cites W2572458419 @default.