Impact of toceranib/piroxicam/cyclophosphamide maintenance therapy on outcome of dogs with appendicular osteosarcoma following amputation and carboplatin chemotherapy: A multi-institutional study

Cheryl A. London; Heather L. Gardner; Tamra Mathie; Nicole Stingle; Roberta Portela; Michael L. Pennell; Craig A. Clifford; Mona P. Rosenberg; David M. Vail; Laurel E. Williams; Kim L. Cronin; Heather Wilson-Robles; Antonella Borgatti; Carolyn J. Henry; Dennis B. Bailey; Jennifer Locke; Nicole C. Northrup; Martin Crawford-Jakubiak; Virginia L. Gill; Mary K. Klein; David M. Ruslander; Doug H. Thamm; Brenda Phillips; Gerald Post

doi:10.1371/journal.pone.0124889

Impact of toceranib/piroxicam/cyclophosphamide maintenance therapy on outcome of dogs with appendicular osteosarcoma following amputation and carboplatin chemotherapy: A multi-institutional study

Cheryl A. London, Heather L. Gardner, Tamra Mathie, Nicole Stingle, Roberta Portela, Michael L. Pennell, Craig A. Clifford, Mona P. Rosenberg, David M. Vail, Laurel E. Williams, Kim L. Cronin, Heather Wilson-Robles, Antonella Borgatti, Carolyn J. Henry, Dennis B. Bailey, Jennifer Locke, Nicole C. Northrup, Martin Crawford-Jakubiak, Virginia L. Gill, Mary K. KleinDavid M. Ruslander, Doug H. Thamm, Brenda Phillips, Gerald Post

Veterinary Clinical Sciences

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Abstract

Background: We hypothesized that the addition of toceranib to metronomic cyclophosphamide/piroxicam therapy would significantly improve disease-free interval (DFI) and overall survival (OS) in dogs with appendicular osteosarcoma (OSA) following amputation and carboplatin chemotherapy. Methods and Findings: This was a randomized, prospective clinical trial in which dogs with OSA free of gross metastatic disease (n = 126) received carboplatin chemotherapy (4 doses) following amputation. On study entry, dogs were randomized to receive piroxicam/cyclophosphamide with or without toceranib (n = 63 each) after completing chemotherapy. Patient demographics were not significantly different between both groups. During or immediately following carboplatin chemotherapy, 32 dogs (n = 13 toceranib; n = 19 control) developed metastatic disease, and 13 dogs left the study due to other medical conditions or owner preference. Following carboplatin chemotherapy, 81 dogs (n = 46 toceranib; n = 35 control) received the metronomic treatment; 35 dogs (n = 20 toceranib; n = 15 control) developed metastatic disease during the maintenance therapy, and 26 dogs left the study due to other medical conditions or owner preference. Nine toceranib-treated and 11 control dogs completed the study without evidence of metastatic disease 1-year following amputation. Toceranib-treated dogs experienced more episodes of diarrhea, neutropenia and weight loss than control dogs, although these toxicities were low-grade and typically resolved with supportive care. More toceranib-treated dogs (n = 8) were removed from the study for therapy-associated adverse events compared to control dogs (n = 1). The median DFI for control and toceranib treated dogs was 215 and 233 days, respectively (p = 0.274); the median OS for control and toceranib treated dogs was 242 and 318 days, respectively (p = 0.08). The one year survival rate for control dogs was 35% compared to 38% for dogs receiving toceranib. Conclusions: The addition of toceranib to metronomic piroxicam/cyclophosphamide therapy following amputation and carboplatin chemotherapy did not improve median DFI, OS or the 1-year survival rate in dogs with OSA.

Original language	English (US)
Article number	e0124889
Journal	PloS one
Volume	10
Issue number	4
DOIs	https://doi.org/10.1371/journal.pone.0124889
State	Published - Apr 29 2015

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© 2015 London et al.

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London, C. A., Gardner, H. L., Mathie, T., Stingle, N., Portela, R., Pennell, M. L., Clifford, C. A., Rosenberg, M. P., Vail, D. M., Williams, L. E., Cronin, K. L., Wilson-Robles, H., Borgatti, A., Henry, C. J., Bailey, D. B., Locke, J., Northrup, N. C., Crawford-Jakubiak, M., Gill, V. L., ... Post, G. (2015). Impact of toceranib/piroxicam/cyclophosphamide maintenance therapy on outcome of dogs with appendicular osteosarcoma following amputation and carboplatin chemotherapy: A multi-institutional study. PloS one, 10(4), Article e0124889. https://doi.org/10.1371/journal.pone.0124889

Impact of toceranib/piroxicam/cyclophosphamide maintenance therapy on outcome of dogs with appendicular osteosarcoma following amputation and carboplatin chemotherapy: A multi-institutional study. / London, Cheryl A.; Gardner, Heather L.; Mathie, Tamra et al.
In: PloS one, Vol. 10, No. 4, e0124889, 29.04.2015.

Research output: Contribution to journal › Article › peer-review

London, CA, Gardner, HL, Mathie, T, Stingle, N, Portela, R, Pennell, ML, Clifford, CA, Rosenberg, MP, Vail, DM, Williams, LE, Cronin, KL, Wilson-Robles, H, Borgatti, A, Henry, CJ, Bailey, DB, Locke, J, Northrup, NC, Crawford-Jakubiak, M, Gill, VL, Klein, MK, Ruslander, DM, Thamm, DH, Phillips, B & Post, G 2015, 'Impact of toceranib/piroxicam/cyclophosphamide maintenance therapy on outcome of dogs with appendicular osteosarcoma following amputation and carboplatin chemotherapy: A multi-institutional study', PloS one, vol. 10, no. 4, e0124889. https://doi.org/10.1371/journal.pone.0124889

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title = "Impact of toceranib/piroxicam/cyclophosphamide maintenance therapy on outcome of dogs with appendicular osteosarcoma following amputation and carboplatin chemotherapy: A multi-institutional study",

abstract = "Background: We hypothesized that the addition of toceranib to metronomic cyclophosphamide/piroxicam therapy would significantly improve disease-free interval (DFI) and overall survival (OS) in dogs with appendicular osteosarcoma (OSA) following amputation and carboplatin chemotherapy. Methods and Findings: This was a randomized, prospective clinical trial in which dogs with OSA free of gross metastatic disease (n = 126) received carboplatin chemotherapy (4 doses) following amputation. On study entry, dogs were randomized to receive piroxicam/cyclophosphamide with or without toceranib (n = 63 each) after completing chemotherapy. Patient demographics were not significantly different between both groups. During or immediately following carboplatin chemotherapy, 32 dogs (n = 13 toceranib; n = 19 control) developed metastatic disease, and 13 dogs left the study due to other medical conditions or owner preference. Following carboplatin chemotherapy, 81 dogs (n = 46 toceranib; n = 35 control) received the metronomic treatment; 35 dogs (n = 20 toceranib; n = 15 control) developed metastatic disease during the maintenance therapy, and 26 dogs left the study due to other medical conditions or owner preference. Nine toceranib-treated and 11 control dogs completed the study without evidence of metastatic disease 1-year following amputation. Toceranib-treated dogs experienced more episodes of diarrhea, neutropenia and weight loss than control dogs, although these toxicities were low-grade and typically resolved with supportive care. More toceranib-treated dogs (n = 8) were removed from the study for therapy-associated adverse events compared to control dogs (n = 1). The median DFI for control and toceranib treated dogs was 215 and 233 days, respectively (p = 0.274); the median OS for control and toceranib treated dogs was 242 and 318 days, respectively (p = 0.08). The one year survival rate for control dogs was 35% compared to 38% for dogs receiving toceranib. Conclusions: The addition of toceranib to metronomic piroxicam/cyclophosphamide therapy following amputation and carboplatin chemotherapy did not improve median DFI, OS or the 1-year survival rate in dogs with OSA.",

author = "London, {Cheryl A.} and Gardner, {Heather L.} and Tamra Mathie and Nicole Stingle and Roberta Portela and Pennell, {Michael L.} and Clifford, {Craig A.} and Rosenberg, {Mona P.} and Vail, {David M.} and Williams, {Laurel E.} and Cronin, {Kim L.} and Heather Wilson-Robles and Antonella Borgatti and Henry, {Carolyn J.} and Bailey, {Dennis B.} and Jennifer Locke and Northrup, {Nicole C.} and Martin Crawford-Jakubiak and Gill, {Virginia L.} and Klein, {Mary K.} and Ruslander, {David M.} and Thamm, {Doug H.} and Brenda Phillips and Gerald Post",

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T1 - Impact of toceranib/piroxicam/cyclophosphamide maintenance therapy on outcome of dogs with appendicular osteosarcoma following amputation and carboplatin chemotherapy

T2 - A multi-institutional study

AU - London, Cheryl A.

AU - Gardner, Heather L.

AU - Mathie, Tamra

AU - Stingle, Nicole

AU - Portela, Roberta

AU - Pennell, Michael L.

AU - Clifford, Craig A.

AU - Rosenberg, Mona P.

AU - Vail, David M.

AU - Williams, Laurel E.

AU - Cronin, Kim L.

AU - Wilson-Robles, Heather

AU - Borgatti, Antonella

AU - Henry, Carolyn J.

AU - Bailey, Dennis B.

AU - Locke, Jennifer

AU - Northrup, Nicole C.

AU - Crawford-Jakubiak, Martin

AU - Gill, Virginia L.

AU - Klein, Mary K.

AU - Ruslander, David M.

AU - Thamm, Doug H.

AU - Phillips, Brenda

AU - Post, Gerald

PY - 2015/4/29

Y1 - 2015/4/29

N2 - Background: We hypothesized that the addition of toceranib to metronomic cyclophosphamide/piroxicam therapy would significantly improve disease-free interval (DFI) and overall survival (OS) in dogs with appendicular osteosarcoma (OSA) following amputation and carboplatin chemotherapy. Methods and Findings: This was a randomized, prospective clinical trial in which dogs with OSA free of gross metastatic disease (n = 126) received carboplatin chemotherapy (4 doses) following amputation. On study entry, dogs were randomized to receive piroxicam/cyclophosphamide with or without toceranib (n = 63 each) after completing chemotherapy. Patient demographics were not significantly different between both groups. During or immediately following carboplatin chemotherapy, 32 dogs (n = 13 toceranib; n = 19 control) developed metastatic disease, and 13 dogs left the study due to other medical conditions or owner preference. Following carboplatin chemotherapy, 81 dogs (n = 46 toceranib; n = 35 control) received the metronomic treatment; 35 dogs (n = 20 toceranib; n = 15 control) developed metastatic disease during the maintenance therapy, and 26 dogs left the study due to other medical conditions or owner preference. Nine toceranib-treated and 11 control dogs completed the study without evidence of metastatic disease 1-year following amputation. Toceranib-treated dogs experienced more episodes of diarrhea, neutropenia and weight loss than control dogs, although these toxicities were low-grade and typically resolved with supportive care. More toceranib-treated dogs (n = 8) were removed from the study for therapy-associated adverse events compared to control dogs (n = 1). The median DFI for control and toceranib treated dogs was 215 and 233 days, respectively (p = 0.274); the median OS for control and toceranib treated dogs was 242 and 318 days, respectively (p = 0.08). The one year survival rate for control dogs was 35% compared to 38% for dogs receiving toceranib. Conclusions: The addition of toceranib to metronomic piroxicam/cyclophosphamide therapy following amputation and carboplatin chemotherapy did not improve median DFI, OS or the 1-year survival rate in dogs with OSA.

AB - Background: We hypothesized that the addition of toceranib to metronomic cyclophosphamide/piroxicam therapy would significantly improve disease-free interval (DFI) and overall survival (OS) in dogs with appendicular osteosarcoma (OSA) following amputation and carboplatin chemotherapy. Methods and Findings: This was a randomized, prospective clinical trial in which dogs with OSA free of gross metastatic disease (n = 126) received carboplatin chemotherapy (4 doses) following amputation. On study entry, dogs were randomized to receive piroxicam/cyclophosphamide with or without toceranib (n = 63 each) after completing chemotherapy. Patient demographics were not significantly different between both groups. During or immediately following carboplatin chemotherapy, 32 dogs (n = 13 toceranib; n = 19 control) developed metastatic disease, and 13 dogs left the study due to other medical conditions or owner preference. Following carboplatin chemotherapy, 81 dogs (n = 46 toceranib; n = 35 control) received the metronomic treatment; 35 dogs (n = 20 toceranib; n = 15 control) developed metastatic disease during the maintenance therapy, and 26 dogs left the study due to other medical conditions or owner preference. Nine toceranib-treated and 11 control dogs completed the study without evidence of metastatic disease 1-year following amputation. Toceranib-treated dogs experienced more episodes of diarrhea, neutropenia and weight loss than control dogs, although these toxicities were low-grade and typically resolved with supportive care. More toceranib-treated dogs (n = 8) were removed from the study for therapy-associated adverse events compared to control dogs (n = 1). The median DFI for control and toceranib treated dogs was 215 and 233 days, respectively (p = 0.274); the median OS for control and toceranib treated dogs was 242 and 318 days, respectively (p = 0.08). The one year survival rate for control dogs was 35% compared to 38% for dogs receiving toceranib. Conclusions: The addition of toceranib to metronomic piroxicam/cyclophosphamide therapy following amputation and carboplatin chemotherapy did not improve median DFI, OS or the 1-year survival rate in dogs with OSA.

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Impact of toceranib/piroxicam/cyclophosphamide maintenance therapy on outcome of dogs with appendicular osteosarcoma following amputation and carboplatin chemotherapy: A multi-institutional study

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