PF-00477736 Mediates Checkpoint Kinase 1 Signaling Pathway and Potentiates Docetaxel-Induced Efficacy in Xenografts

Zhang, Cathy; Yan, Zhengming; Painter, Cory L.; Zhang, Qin; Chen, Enhong; Arango, Maria E.; Kuszpit, Kyle; Zasadny, Kenneth R.; Hallin, Max; Hallin, Jill; Wong, Anthony; Buckman, Dana; Sun, Guizhen; Qiu, Ming; Anderes, Kenna; Christensen, James G.

doi:10.1158/1078-0432.ccr-08-3272

Cited by 53 publications

(40 citation statements)

References 42 publications

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“…Therefore, we examined the in vivo tolerability of the dual and triple combinations. Because we and others (21) have found that concurrent treatment was effective, we administered CHK1i concurrently with gemcitabine instead of a 24-hour delay (7). Dosing schedules of 50 mg/kg gemcitabine and 15 mg/kg (7.5 mg/kg twice daily, b.i.d.)…”

Section: Tolerability and Efficacy Of Gemcitabine Chk1i And Egfr-dimentioning

confidence: 99%

Gemcitabine and CHK1 Inhibition Potentiate EGFR-Directed Radioimmunotherapy against Pancreatic Ductal Adenocarcinoma

Al-Ejeh

Shi

Kalimutho

et al. 2014

Clinical Cancer Research

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Purpose: To develop effective combination therapy against pancreatic ductal adenocarcinoma (PDAC) with a combination of chemotherapy, CHK1 inhibition, and EGFR-targeted radioimmunotherapy.Experimental Design: Maximum tolerated doses were determined for the combination of gemcitabine, the CHK1 inhibitor PF-477736, and Lutetium-177 ( 177 Lu)-labeled anti-EGFR antibody. This triple combination therapy was investigated using PDAC models from well-established cell lines, recently established patient-derived cell lines, and fresh patient-derived xenografts. Tumors were investigated for the accumulation of 177 Lu-anti-EGFR antibody, survival of tumor-initiating cells, induction of DNA damage, cell death, and tumor tissue degeneration.Results: The combination of gemcitabine and CHK1 inhibitor PF-477736 with 177 Lu-anti-EGFR antibody was tolerated in mice. This triplet was effective in established tumors and prevented the recurrence of PDAC in four cell line-derived and one patient-derived xenograft model. This exquisite response was associated with the loss of tumor-initiating cells as measured by flow cytometric analysis and secondary implantation of tumors from treated mice into treatment-na€ ve mice. Extensive DNA damage, apoptosis, and tumor degeneration were detected in the patient-derived xenograft. Mechanistically, we observed CDC25A stabilization as a result of CHK1 inhibition with consequent inhibition of gemcitabine-induced S-phase arrest as well as a decrease in canonical (ERK1/2 phosphorylation) and noncanonical EGFR signaling (RAD51 degradation) as a result of EGFR inhibition. Conclusions: Our study developed an effective combination therapy against PDAC that has potential in the treatment of PDAC.

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Section: Tolerability and Efficacy Of Gemcitabine Chk1i And Egfr-dimentioning

confidence: 99%

Gemcitabine and CHK1 Inhibition Potentiate EGFR-Directed Radioimmunotherapy against Pancreatic Ductal Adenocarcinoma

Al-Ejeh

Shi

Kalimutho

et al. 2014

Clinical Cancer Research

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“…FLT-PET and CT imaging was done using a microPET Focus F220 scanner (Siemens Medical Solutions) and a GE eXplore microCT scanner (GE Healthcare), respectively, as described previously (21). Tumor-bearing mice were anesthetized and administered 250 mCi (1-2 mg/kg) of […”

Section: Immunohistochemical Stainingmentioning

confidence: 99%

[18F]FLT–PET Imaging Does Not Always “Light Up” Proliferating Tumor Cells

Zhang

Yan

et al. 2012

Clinical Cancer Research

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“…Other selective Chk1 inhibitors were also shown to abrogate the S-phase delay induced by topoisomerase inhibitors (Chen et al, 2006;Tse et al, 2007) and to potentiate the cytotoxicity of g-radiation in p53-deficient cells (Chen et al, 2006). These effects were associated with increased mitotic entry, induction of DSB and apoptosis, as well as marked inhibition of proliferation (Chen et al, 2006;Tse et al, 2007;Blasina et al, 2008;Zhang et al, 2009). The synergy between replication stress inducers and Chk1 inhibitors was translated into a dose-dependent increase in tumor growth delay in vivo (Tse et al, 2007;Blasina et al, 2008;Zhang et al, 2009).…”

Section: Combinations Of Dna-repair Inhibitorsmentioning

confidence: 99%

“…These effects were associated with increased mitotic entry, induction of DSB and apoptosis, as well as marked inhibition of proliferation (Chen et al, 2006;Tse et al, 2007;Blasina et al, 2008;Zhang et al, 2009). The synergy between replication stress inducers and Chk1 inhibitors was translated into a dose-dependent increase in tumor growth delay in vivo (Tse et al, 2007;Blasina et al, 2008;Zhang et al, 2009).…”

Section: Combinations Of Dna-repair Inhibitorsmentioning

confidence: 99%

Harnessing the complexity of DNA-damage response pathways to improve cancer treatment outcomes

et al. 2010

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PF-00477736 Mediates Checkpoint Kinase 1 Signaling Pathway and Potentiates Docetaxel-Induced Efficacy in Xenografts

Cited by 53 publications

References 42 publications

Gemcitabine and CHK1 Inhibition Potentiate EGFR-Directed Radioimmunotherapy against Pancreatic Ductal Adenocarcinoma

Gemcitabine and CHK1 Inhibition Potentiate EGFR-Directed Radioimmunotherapy against Pancreatic Ductal Adenocarcinoma

[18F]FLT–PET Imaging Does Not Always “Light Up” Proliferating Tumor Cells

Harnessing the complexity of DNA-damage response pathways to improve cancer treatment outcomes

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