Randomized, Double-Blind, Phase II Study of Ruxolitinib or Placebo in Combination With Capecitabine in Patients With Metastatic Pancreatic Cancer for Whom Therapy With Gemcitabine Has Failed

Hurwitz, Herbert I.; Uppal, Nikhil; Wagner, Stéphanie; Bendell, Johanna C.; Beck, J. Thaddeus; Wade, Seaborn Mcdonald; Nemunaitis, John; Stella, Philip J.; Pipas, J. Marc; Wainberg, Zev A.; Manges, Robert; Garrett, William M.; Hunter, Deborah; Clark, Jason; Leopold, Lance; Sandor, Victor; Levy, Richard S.

doi:10.1200/jco.2015.61.4578

Cited by 240 publications

(170 citation statements)

References 60 publications

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“…Secondly, it would support the hypothesis that routine markers of the systemic inflammatory response, and in particular the mGPS, may aid in the identification and selection of patients likely to benefit from such targeted therapies (50). In keeping with such a scheme, one recent clinical trial of a JAK inhibitor in patients with metastatic pancreatic cancer found an increase in overall survival only in those patients with an elevated CRP or mGPS (51). Therefore, it is clear that markers of the host inflammatory response should be incorporated into future studies of agents targeting the IL-6/JAK/STAT3 pathway in cancer.…”

Section: P=0039)mentioning

confidence: 80%

Signal Transduction and Activator of Transcription-3 (STAT3) in Patients with Colorectal Cancer: Associations with the Phenotypic Features of the Tumor and Host

Park

Wyk

McMillan

et al. 2017

Clinical Cancer Research

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(2017) Signal transduction and activator of transcription-3 (STAT3) in patients with colorectal cancer: associations with the phenotypic features of the tumour and host. Clinical Cancer Research, 23(7), pp. 1698 -1709 . (doi:10.1158 /1078 -0432.CCR-16-1416 This is the author's final accepted version.There may be differences between this version and the published version. You are advised to consult the publisher's version if you wish to cite from it.http://eprints.gla.ac.uk/129347/ Experimental DesignImmunohistochemical assessment of STAT3/pSTAT3 expression was performed using a tissue microarray and tumour cell expression divided into tertiles using the weighted histoscore. The relationship between STAT3/pSTAT3 expression and local inflammatory The combination of nuclear STAT3/pSTAT3 stratified five-year survival from 81% to 62% (P=0.012), however was not associated with survival independent of venous invasion, tumour perforation or tumour budding. ConclusionIn patients undergoing CRC resection, STAT3 expression was associated with adverse host inflammatory responses and reduced survival. Up-regulation of tumour STAT3 may be an important mechanism whereby the tumour deregulates local and systemic inflammatory responses.5

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Section: P=0039)mentioning

confidence: 80%

Signal Transduction and Activator of Transcription-3 (STAT3) in Patients with Colorectal Cancer: Associations with the Phenotypic Features of the Tumor and Host

Park

Wyk

McMillan

et al. 2017

Clinical Cancer Research

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“…The fact that therapies with a broader mechanism of action will become available for research projects in the near future is equally important. In addition to the omnipresent immunotherapy, stromal depletion, e.g., with hyaluronidase [55] and anti-inflammatory concepts [56] , appear most promising.…”

Section: Resultsmentioning

confidence: 99%

Perioperative treatment options in resectable pancreatic cancer - how to improve long-term survival

Sinn

Bahra

Denecke

et al. 2016

WJGO

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“…In preclinical pancreatic cancer models, the JAK/STAT and related inflammatory pathways were found to drive cancer progression. Ruxolitinib is a JAK 1/2 inhibitor which has been evaluated in refractory pancreatic cancer with or without capecitabine in a randomized phase II study (65). In a pre-specified subgroup of patients with systemic inflammation as measured by elevated serum C-reactive protein (CRP >13 mg/L), survival significantly favored the ruxolitinib arm (3 and 6 months survivals of 48% and 42% vs. 29% and 11%, respectively).…”

Section: Janus Kinase (Jak) 1/2mentioning

confidence: 99%

Personalized medicine in sporadic pancreatic cancer without homologous recombination-deficiency: are we any closer?

Vijayvergia

Cohen

2016

J. Gastrointest. Oncol.

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In 2015, pancreatic cancer was the 10th most commonly diagnosed cancer and the fourth leading cause of cancer death in the United States. The incidence of pancreatic cancer has been slowly rising over the past 10 years. It is estimated that about 53,000 new cases were diagnosed and 42,000 people died from pancreatic cancer in 2015 (1). The small difference between the incidence and death rate of pancreatic cancer reflect the early distant spread and inadequacy of current therapies. The 5-year survival rates for localized and advanced pancreatic cancer are 27% and less than 5%, respectively, lower than all other common cancers (2). The majority of patients are diag nosed at an advanced stage and are not eligible for surgical resection (2). These patients are often symptomatic and quickly deteriorate in the absence of effective therapy and many are unable to receive second and third line therapies for the same reason. Hence, finding the optimal first line regimen may be the key to improving outcomes. Increases in our knowledge of hu man and cancer genomics provide opportunities to un derstand the impact of genetic alterations on pancreatic cancer outcomes and develop predictive biomarkers for newer targeted therapies (3,4). Unfortunately, the amount of tissue obtained by fine needle aspiration of the primary pancreatic tumor is usually insufficient to perform adequate molecular analysis. As we move into the era of personalized medicine, obtaining core biopsy samples from metastatic sites, like liver, may help eliminate this problem. What do we know about pancreatic cancer genetically?Pancreatic cancer is a disease of significant genetic variability. Recent whole exome and genome sequencing have identified a wide range of genetic alterations including mutations and copy number variations that characterize pancreatic cancer (4,5). Some of these are recurrent and are clearly needed to identify subsets of patients likely to benefit from these therapies. Advances in our understanding of the molecular drivers of pancreatic cancer offer the hope of personalized therapy that may benefit our patients. In this review, we summarize the current knowledge about the biology of pancreatic cancer and its implication for treatment. We discuss recent advances in targeted therapies and the role of potential biomarkers in predicting response to established therapies. We also review novel therapeutic approaches that may be able to fulfill the promise of personalized therapy for pancreatic cancer.

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Randomized, Double-Blind, Phase II Study of Ruxolitinib or Placebo in Combination With Capecitabine in Patients With Metastatic Pancreatic Cancer for Whom Therapy With Gemcitabine Has Failed

Cited by 240 publications

References 60 publications

Signal Transduction and Activator of Transcription-3 (STAT3) in Patients with Colorectal Cancer: Associations with the Phenotypic Features of the Tumor and Host

Signal Transduction and Activator of Transcription-3 (STAT3) in Patients with Colorectal Cancer: Associations with the Phenotypic Features of the Tumor and Host

Perioperative treatment options in resectable pancreatic cancer - how to improve long-term survival

Personalized medicine in sporadic pancreatic cancer without homologous recombination-deficiency: are we any closer?

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