Multi-center, Placebo-controlled, Double-blind, Randomized Study of Oral Toceranib Phosphate (SU11654), a Receptor Tyrosine Kinase Inhibitor, for the Treatment of Dogs with Recurrent (Either Local or Distant) Mast Cell Tumor Following Surgical Excision

London, Cheryl A.; Malpas, Phyllis B.; Wood-Follis, Stacey L.; Boucher, Joseph F.; Rusk, Anthony; Rosenberg, Mona P.; Henry, Carolyn J.; Mitchener, Kathy L.; Klein, Mary K.; Hintermeister, John G.; Bergman, Philip J.; Couto, Guillermo; Mauldin, G. Neal; Michels, Gina M.

doi:10.1158/1078-0432.ccr-08-1860

Cited by 355 publications

(478 citation statements)

References 47 publications

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“…Metastatic MCT represents a major health problem in the canine population, but the introduction of a novel class of targeted antineoplastic agents directed against KIT, TKI, has significantly changed the therapeutic options available for these dogs 7, 8. Indeed, the important role of targeted therapy against molecules contributing to tumor development, progression, and metastasis has attracted considerable attention 31…”

Section: Discussionmentioning

confidence: 99%

“…Although TKI‐based therapy is used in dogs with MCT to also treat metastatic disease in the lymph nodes,7 c‐kit status is generally evaluated in the primary lesions because metastatic sites are rarely removed or biopsied before treatment. However, it is still unknown whether c‐kit status differs in metastases compared with primary tumors.…”

mentioning

confidence: 99%

“…Moreover, the treatment with TKIs is associated with potential toxicity and high costs; additionally, resistance to certain TKIs is often caused by secondary mutations of c‐kit 7, 16; therefore, it is important to critically review all aspects of the mutational testing to enhance upfront patient selection.…”

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confidence: 99%

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Concordance of c‐kit Mutational Status in Matched Primary and Metastatic Cutaneous Canine Mast Cell Tumors at Baseline

Marconato

Zorzan

Giantin

et al. 2013

Veterinary Internal Medicne

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BackgroundMutation analysis of proto‐oncogene c‐kit (c‐kit) is advisable before starting treatment with tyrosine kinase inhibitors in dogs with mast cell tumor (MCT), including those with metastatic disease. Testing is usually performed on primary tumors, assuming that c‐kit mutation status does not change in metastasis.Hypothesis/ObjectivesTo give an insight into the mutational processes and to make a recommendation on the use of c‐kit mutational analysis in the clinical setting.AnimalsTwenty‐one client‐owned dogs with metastatic MCT.MethodsDogs undergoing resection or biopsy for both primary and matched metastatic MCT were prospectively enrolled. Total RNA or DNA was extracted from primary MCT and corresponding metastases. Exons 8, 9, and 11 were amplified by PCR and sequenced. Genetic features between primary MCT and metastases were compared. Their correlation with clinicopathologic features was investigated.ResultsConcordance (mutated or wild‐type) of mutational status, evaluable in 21 primary and matched metastatic (20 nodal and 1 splenic) MCTs, was 100%. Three new c‐kit mutations were identified. No significant correlation was detected between c‐kit mutation and clinicopathologic features.Conclusions and Clinical ImportanceProto‐oncogene c‐kit mutational status is conserved between any primary and its matched secondary tumor, suggesting that both can be used for c‐kit mutational testing. Targeted therapies might be also used to treat metastatic disease.

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Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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Concordance of c‐kit Mutational Status in Matched Primary and Metastatic Cutaneous Canine Mast Cell Tumors at Baseline

Marconato

Zorzan

Giantin

et al. 2013

Veterinary Internal Medicne

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“…47 This study supports the use of feline SCC as a model for HNSCC, an approach that could potentially benefit both felines and humans alike. During the development of a TKI against KIT (SU11654, toceranib) 48 the human field benefited greatly from the canine studies, 47 and the development of acquired resistance to single-agent TKIs in dogs with mast cell tumors is of particular interest. 47 Further studies in cats with SCCs using EGFR targeting siRNA based therapies in combination with radiotherapy would potentially advance the treatment of the disease in both species.…”

confidence: 99%

Studies on the inhibition of feline EGFR in squamous cell carcinoma: Enhancement of radiosensitivity and rescue of resistance to small molecule inhibitors

Bergkvist¹,

Argyle²,

Pang³

et al. 2011

Cancer Biology & Therapy

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“…The presence of these mutations is associated with higher-grade tumors. 20,29,38 Mutations result in constitutive activation of KIT, initiating signaling cascades leading to proliferation, survival, and invasion. 9,[15][16][17][18]21,22,29 One group reported that the presence of ITD mutations of c-KIT or aberrant cytoplasmic KIT protein localization was significantly associated with higher values of Ki67.…”

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confidence: 99%

Canine Subcutaneous Mast Cell Tumors

Thompson

Yager²,

Best³

et al. 2010

Vet Pathol

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Molecular assays are widely used to prognosticate canine cutaneous mast cell tumors (MCT). There is limited information about these prognostic assays used on MCT that arise in the subcutis. The aims of this study were to evaluate the utility of KIT immunohistochemical labeling pattern, c-KIT mutational status (presence of internal tandem duplications in exon 11), and proliferation markers-including mitotic index, Ki67, and argyrophilic nucleolar organizing regions (AgNOR)-as independent prognostic markers for local recurrence and/or metastasis in canine subcutaneous MCT. A case-control design was used to analyze 60 subcutaneous MCT from 60 dogs, consisting of 24 dogs with subsequent local recurrence and 12 dogs with metastasis, as compared to dogs matched by breed, age, and sex with subcutaneous MCT that did not experience these events. Mitotic index, Ki67, the combination of Ki67 and AgNOR, and KIT cellular localization pattern were significantly associated with local recurrence and metastasis, thereby demonstrating their prognostic value for subcutaneous MCT. No internal tandem duplication mutations were detected in exon 11 of c-KIT in any tumors. Because c-KIT mutations have been demonstrated in only 20 to 30% of cutaneous MCT and primarily in tumors of higher grade, the number of subcutaneous MCT analyzed in this study may be insufficient to draw conclusions on the role c-KIT mutations in these tumors. KeywordsAgNOR, canine, case-control study, c-KIT, Ki67, mast cell tumor, mitotic index, prognostic markers Subcutaneous mast cell tumors (MCT) are located in the subcutis, usually surrounded by fat. Until recently, 24,35 this type was not investigated separately from its cutaneous counterpart. Subcutaneous MCT are classified by many as grade II MCT, based on current grading schemes.10,27 Because intermediate (grade II) tumors have a highly variable prognosis 10,25,26 and low interobserver agreement among pathologists, 25,26 accurate prognostic data for the subcutaneous variant of MCT are needed. In a recent retrospective survival analysis of subcutaneous MCT from 306 dogs, 35 we demonstrated that the majority of subcutaneous MCT do not behave aggressively, thus confirming the conclusion of a prior smaller study of subcutaneous MCT.24 Furthermore, our results showed that a strong predictor of survival time, time to local recurrence, and metastasis was mitotic index (MI), assessed as the number of mitotic figures per 10 high-power fields. 35MI is a valuable prognostic test 7,31 and an integral part of grading schemes for cutaneous MCT. 3,10,27 Despite this, there are drawbacks to using MI as a sole determinant for assessment of cellular proliferation. Accurate counting of mitotic figures may be influenced by field selection, plane of section, field diameter, intensity of cytoplasmic granularity (or presence of crush artifact), necrosis, and/or apoptotic cells. All of these variables can contribute to interobserver disagreement. In addition, MI detects only cells in the mitotic phase rather than the enti...

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Multi-center, Placebo-controlled, Double-blind, Randomized Study of Oral Toceranib Phosphate (SU11654), a Receptor Tyrosine Kinase Inhibitor, for the Treatment of Dogs with Recurrent (Either Local or Distant) Mast Cell Tumor Following Surgical Excision

Cited by 355 publications

References 47 publications

Concordance of c‐kit Mutational Status in Matched Primary and Metastatic Cutaneous Canine Mast Cell Tumors at Baseline

Concordance of c‐kit Mutational Status in Matched Primary and Metastatic Cutaneous Canine Mast Cell Tumors at Baseline

Studies on the inhibition of feline EGFR in squamous cell carcinoma: Enhancement of radiosensitivity and rescue of resistance to small molecule inhibitors

Canine Subcutaneous Mast Cell Tumors

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