Fusion Tyrosine Kinases Induce Drug Resistance by Stimulation of Homology-Dependent Recombination Repair, Prolongation of G<sub>2</sub>/M Phase, and Protection from Apoptosis

Słupianek, Artur; Hoser, Grazyna; Majsterek, Ireneusz; Bronisz, Agnieszka; Małecki, Maciej T.; Błasiak, Janusz; Fishel, Richard; Skórski, Tomasz

doi:10.1128/mcb.22.12.4189-4201.2002

Cited by 193 publications

(194 citation statements)

References 86 publications

(99 reference statements)

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“…FTKs display common and unique characteristics of activation of these pathways; for example, PI-3k is stimulated by all FTKs listed above, whereas STAT5 and PLCg seem to be activated by the BCR/ABL-related FTKs, with exception to TEL/TRKC (Liu et al, 2000;Nieborowska-Skorska et al, 2001;Slupianek et al, 2002;Baumann et al, 2003). In addition, leukemogenic properties of TEL/ABL seem to be distinct from those of BCR/ABL (Million et al, 2002).…”

Section: Consequences Of Ftks Expressionmentioning

confidence: 99%

“…Drug resistance BCR/ABL and related FTKs such as TEL/ABL TEL/ PDGFbR, TEL/JAK2 and NPM/ALK demonstrate an enhanced ability to survive genotoxic stress probably owing to enhanced DNA repair, prolonged S and G 2 /M checkpoints for extended repair and inhibition of proapoptotic pathways (Bedi et al, 1995;AmaranteMendes et al, 1998;Skorski, 2002;Slupianek et al, 2002Slupianek et al, , 2006Canitrot et al, 2003;Lauren et al, 2003;Nieborowska-Skorska et al, 2006) (Figure 3). These three factors may work in concert to provide the necessary protection from DNA damage-induced apoptosis.…”

Section: Consequences Of Ftks Expressionmentioning

confidence: 99%

“…The former mechanism involves RAD51-driven invasion and pairing of a single-stranded DNA to the homologous template. Elevated levels of RAD51 have been observed in various tumors and positively associated with genotoxic therapy resistance (Vispe et al, 1998;Collis et al, 2001;Raderschall et al, 2002;Slupianek et al, 2002Slupianek et al, , 2006. Leukemias and lymphomas expressing BCR/ABL-related FTKs, such as TEL/ABL, TEL/ PDGFbR, TEL/JAK2, NPM/ALK and ZNF198/ FGFR1, display elevated levels of RAD51 and enhanced HRR activity (Slupianek et al, , 2002Heath and Cross, 2004).…”

Section: Consequences Of Ftks Expressionmentioning

confidence: 99%

“…Elevated levels of RAD51 have been observed in various tumors and positively associated with genotoxic therapy resistance (Vispe et al, 1998;Collis et al, 2001;Raderschall et al, 2002;Slupianek et al, 2002Slupianek et al, , 2006. Leukemias and lymphomas expressing BCR/ABL-related FTKs, such as TEL/ABL, TEL/ PDGFbR, TEL/JAK2, NPM/ALK and ZNF198/ FGFR1, display elevated levels of RAD51 and enhanced HRR activity (Slupianek et al, , 2002Heath and Cross, 2004). Although Deutsch et al (2001) indicated that DNA-PKcs, an important kinase in NHEJ, may be downregulated in CML cells, subsequent reports employing various in vitro and in vivo methods detected enhanced activity of NHEJ in BCR/ABLtransformed leukemia cells and CML patient cells (Gaymes et al, 2002;Brady et al, 2003;Nowicki et al, 2004;Slupianek et al, 2006).…”

Section: Consequences Of Ftks Expressionmentioning

confidence: 99%

“…FTKs may stimulate antiapoptotic proteins such as BCL2 and BCL-X L and inhibit proapoptotic proteins BAD and BAX, thus preventing the release of cytochrome c from the mitochondria and activation of caspase-3 (Skorski, 2002;Slupianek et al, 2002).…”

Section: Inhibition Of Apoptosismentioning

confidence: 99%

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Fusion tyrosine kinases: a result and cause of genomic instability

Penserga

Skórski

2006

Oncogene

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Section: Consequences Of Ftks Expressionmentioning

confidence: 99%

Section: Consequences Of Ftks Expressionmentioning

confidence: 99%

Section: Consequences Of Ftks Expressionmentioning

confidence: 99%

Section: Consequences Of Ftks Expressionmentioning

confidence: 99%

Section: Inhibition Of Apoptosismentioning

confidence: 99%

See 3 more Smart Citations

Fusion tyrosine kinases: a result and cause of genomic instability

Penserga

Skórski

2006

Oncogene

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Genetic instability in inherited and sporadic leukemias

Popp

Bohlander

2010

Genes Chromosomes & Cancer

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Genetic instability due to increased DNA damage and altered DNA repair is of central significance in the initiation and progression of inherited and sporadic human leukemias. Although very rare, some inherited DNA repair insufficiency syndromes (e.g., Fanconi anemia, Bloom's syndrome) have added substantially to our understanding of crucial mechanisms of leukemogenesis in recent years. Conversely, sporadic leukemias account for the main proportion of leukemias and here DNA damaging reactive oxygen species (ROS) play a central role. Although the exact mechanisms of increased ROS production remain largely unknown and no single pathway has been detected thus far, some oncogenic proteins (e.g., the activated tyrosine kinases BCR-ABL1 and FLT3-ITD) seem to play a key role in driving genetic instability by increased ROS generation which influences the disease course (e.g., blast crisis in chronic myeloid leukemia or relapse in FLT3-ITD positive acute myeloid leukemia). Of course other mechanisms, which promote genetic instability in leukemia also exist. A newly emerging mechanism is the genome-wide alteration of epigenetic marks (e.g., hypomethylation of histone H3K79), which promotes chromosomal instability. Taken together genetic instability plays a critical role both in inherited and sporadic leukemias and emerges as a common theme in both inherited and sporadic leukemias. Beyond its theoretical impact, the analysis of genetic instability may lead the way to the development of innovative therapy strategies.

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RAD51 overexpression is a negative prognostic marker for colorectal adenocarcinoma

Tennstedt

Fresow

Simon

et al. 2012

Intl Journal of Cancer

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RAD51 is the central protein in the homologous recombination pathway and is therefore of great relevance in terms of both therapy resistance as well as genomic stability. By using a tissue microarray analysis of 1,213 biopsies taken from colorectal adenocarcinomas (CRCs), we investigated whether RAD51 expression can be used as a prognostic marker as well as potential associations between this and the expression of other proteins known to be related to CRC. Strong RAD51 expression was observed in 1% of CRC, moderate in 11%, weak in 34% and no expression in 44%. No correlation was found between RAD51 expression and clinicopathological parameters. RAD51 expression correlated significantly (p 5 0.001) with overall survival, with a median survival of 11 months for patients with strong, 46 with moderate, 76 with weak and 68 with negative expression. Multivariate analyses revealed that in addition to tumor stage (p < 0.0001) and nodal status (p < 0.0001), RAD51 expression is also an independent prognostic parameter (p 5 0.011). Strong RAD51 expression was found to be associated with the loss of the two DNA mismatch repair proteins MSH (p 5 0.0003), MLH (p 5 0.002) and b-catenin (p 5 0.012) as well as with elevated p21 (p 5 0.003) and EGFR expression (p 5 0.0001). However, a correlation with overall survival could only be found for EGFR expression (p 5 0.008), although no added benefit in risk stratification could be determined when evaluated together with RAD51. Overexpression of RAD51 is a predictor of poor outcome in CRC. This finding indicated the promise of future studies using RAD51 as a prognostic marker and therapeutic target.Colorectal cancer (CRC) is one of the most frequent cancers, with over 1 million new cases worldwide each year and a disease-specific mortality of 33-40%.

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Fusion Tyrosine Kinases Induce Drug Resistance by Stimulation of Homology-Dependent Recombination Repair, Prolongation of G₂/M Phase, and Protection from Apoptosis

Cited by 193 publications

References 86 publications

Fusion tyrosine kinases: a result and cause of genomic instability

Fusion tyrosine kinases: a result and cause of genomic instability

Genetic instability in inherited and sporadic leukemias

RAD51 overexpression is a negative prognostic marker for colorectal adenocarcinoma

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Fusion Tyrosine Kinases Induce Drug Resistance by Stimulation of Homology-Dependent Recombination Repair, Prolongation of G2/M Phase, and Protection from Apoptosis

Cited by 193 publications

References 86 publications

Fusion tyrosine kinases: a result and cause of genomic instability

Fusion tyrosine kinases: a result and cause of genomic instability

Genetic instability in inherited and sporadic leukemias

RAD51 overexpression is a negative prognostic marker for colorectal adenocarcinoma

Contact Info

Product

Resources

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Fusion Tyrosine Kinases Induce Drug Resistance by Stimulation of Homology-Dependent Recombination Repair, Prolongation of G₂/M Phase, and Protection from Apoptosis