An implantable drug delivery system (IDDS) for refractory cancer pain provides sustained pain control, less drug-related toxicity, and possibly better survival compared with comprehensive medical management (CMM)

T. J. Smith; P. J. Coyne; P. S. Staats; T. Deer; L. J. Stearns; R. L. Rauck; R. L. Boortz-Marx; E. Buchser; E. Català; D. A. Bryce; M. Cousins; G. E. Pool; M. Wallace; T. Yaksh; S. Magnuson; A. Leung; F. Ahadian; S. Bullock; M. McBeth; A. Hoye; R. Miguel; M. A. Weitzner; L. Balducci; K. Follett; P. Hitchon; W. S. Minore; H. Weiss; J. Jaworowicz; S. Croy; S. Davis; S. Grossman; M. Grieb; L. Carson; S. Mitchell; M. Stuckey; S. Charapata; M. McCracken; R. Sorensen; J. Calava; J. Dunn; P. Kosek; S. Weinstein; T. K. Banerjee; D. Caraway; C. Kim; M. Serafini; K. McNeil; J. Frame; G. Orlandini; A. Siragusa; F. Aliaga; A. Lopez-Pousa; C. Pericay; L. Perey; C. Muriel; F. Boyle; A. Molloy; C. Brooker; S. E. Walker

doi:10.1093/annonc/mdi156

An implantable drug delivery system (IDDS) for refractory cancer pain provides sustained pain control, less drug-related toxicity, and possibly better survival compared with comprehensive medical management (CMM)

T. J. Smith, P. J. Coyne, P. S. Staats, T. Deer, L. J. Stearns, R. L. Rauck, R. L. Boortz-Marx, E. Buchser, E. Català, D. A. Bryce, M. Cousins, G. E. Pool, M. Wallace, T. Yaksh, S. Magnuson, A. Leung, F. Ahadian, S. Bullock, M. McBeth, A. HoyeR. Miguel, M. A. Weitzner, L. Balducci, K. Follett, P. Hitchon, W. S. Minore, H. Weiss, J. Jaworowicz, S. Croy, S. Davis, S. Grossman, M. Grieb, L. Carson, S. Mitchell, M. Stuckey, S. Charapata, M. McCracken, R. Sorensen, J. Calava, J. Dunn, P. Kosek, S. Weinstein, T. K. Banerjee, D. Caraway, C. Kim, M. Serafini, K. McNeil, J. Frame, G. Orlandini, A. Siragusa, F. Aliaga, A. Lopez-Pousa, C. Pericay, L. Perey, C. Muriel, F. Boyle, A. Molloy, C. Brooker, S. E. Walker

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

126 Scopus citations

Abstract

Background: The randomized clinical trial of implantable drug delivery systems (IDDS) plus comprehensive medical management (CMM) versus CMM alone showed better clinical success at 4 weeks for IDDS patients. This 'as treated' analysis assessed if improvements in pain control, drug toxicity and survival were maintained over time. Patients and methods: We compared those who received IDDS with those who did not receive IDDS (non-IDDS). All patients had Visual Analogue Scores (VAS) for pain ≥5/10 on at least 200 mg morphine or equivalent daily. Results: At 4 weeks, 46 of 52 (88.5%) IDDS patients achieved clinical success compared with 65 of 91 (71.4%; P=0.02) non-IDDS patients, and more often achieved ≥20% reduction in both pain VAS and toxicity [35 of 52 (67.3%) versus 33 of 91 patients (36.3%); P = 0.0003]. By 12 weeks, 47 of 57 (82.5%) IDDS patients had clinical success compared with 35 of 45 (77.8%; P=0.55) non-IDDS patients, and more often had a ≥20% reduction in both pain VAS and toxicity [33 of 57 (57.9%) versus 15 of 45 patients (33.3%); P=0.01]. At 12 weeks the IDDS VAS pain scores decreased from 7.81 to 3.89 (47% reduction) compared with 7.21 to 4.53 for non-IDDS patients (42% reduction; P = 0.23). The 12 week drug toxicity scores for IDDS patients decreased from 6.68 to 2.30 (66% reduction), and for non-IDDS patients from 6.73 to 4.13 (37% reduction; P = 0.01). All individual drug toxicities improved with IDDS at both 4 and 12 weeks. At 6 months, only 32% of the group randomized to CMM and who did not cross over to IDDS were alive, compared with 52%-59% for patients in those groups who received IDDS. Conclusions: IDDS improved clinical success, reduced pain scores, relieved most toxicity of pain control drugs, and was associated with increased survival for the duration of this 6 month trial.

Original language	English (US)
Pages (from-to)	825-833
Number of pages	9
Journal	Annals of Oncology
Volume	16
Issue number	5
DOIs	https://doi.org/10.1093/annonc/mdi156
State	Published - May 2005
Externally published	Yes

Keywords

Cancer
Implantable devices
Intraspinal therapy
Intrathecal therapy
Opioids
Pain

ASJC Scopus subject areas

Hematology
Oncology

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10.1093/annonc/mdi156

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Smith, T. J., Coyne, P. J., Staats, P. S., Deer, T., Stearns, L. J., Rauck, R. L., Boortz-Marx, R. L., Buchser, E., Català, E., Bryce, D. A., Cousins, M., Pool, G. E., Wallace, M., Yaksh, T., Magnuson, S., Leung, A., Ahadian, F., Bullock, S., McBeth, M., ... Walker, S. E. (2005). An implantable drug delivery system (IDDS) for refractory cancer pain provides sustained pain control, less drug-related toxicity, and possibly better survival compared with comprehensive medical management (CMM). Annals of Oncology, 16(5), 825-833. https://doi.org/10.1093/annonc/mdi156

An implantable drug delivery system (IDDS) for refractory cancer pain provides sustained pain control, less drug-related toxicity, and possibly better survival compared with comprehensive medical management (CMM). / Smith, T. J.; Coyne, P. J.; Staats, P. S. et al.
In: Annals of Oncology, Vol. 16, No. 5, 05.2005, p. 825-833.

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

Smith, TJ, Coyne, PJ, Staats, PS, Deer, T, Stearns, LJ, Rauck, RL, Boortz-Marx, RL, Buchser, E, Català, E, Bryce, DA, Cousins, M, Pool, GE, Wallace, M, Yaksh, T, Magnuson, S, Leung, A, Ahadian, F, Bullock, S, McBeth, M, Hoye, A, Miguel, R, Weitzner, MA, Balducci, L, Follett, K, Hitchon, P, Minore, WS, Weiss, H, Jaworowicz, J, Croy, S, Davis, S, Grossman, S, Grieb, M, Carson, L, Mitchell, S, Stuckey, M, Charapata, S, McCracken, M, Sorensen, R, Calava, J, Dunn, J, Kosek, P, Weinstein, S, Banerjee, TK, Caraway, D, Kim, C, Serafini, M, McNeil, K, Frame, J, Orlandini, G, Siragusa, A, Aliaga, F, Lopez-Pousa, A, Pericay, C, Perey, L, Muriel, C, Boyle, F, Molloy, A, Brooker, C & Walker, SE 2005, 'An implantable drug delivery system (IDDS) for refractory cancer pain provides sustained pain control, less drug-related toxicity, and possibly better survival compared with comprehensive medical management (CMM)', Annals of Oncology, vol. 16, no. 5, pp. 825-833. https://doi.org/10.1093/annonc/mdi156

@article{c16ca0c80c344070807e980728ac28d7,

title = "An implantable drug delivery system (IDDS) for refractory cancer pain provides sustained pain control, less drug-related toxicity, and possibly better survival compared with comprehensive medical management (CMM)",

abstract = "Background: The randomized clinical trial of implantable drug delivery systems (IDDS) plus comprehensive medical management (CMM) versus CMM alone showed better clinical success at 4 weeks for IDDS patients. This 'as treated' analysis assessed if improvements in pain control, drug toxicity and survival were maintained over time. Patients and methods: We compared those who received IDDS with those who did not receive IDDS (non-IDDS). All patients had Visual Analogue Scores (VAS) for pain ≥5/10 on at least 200 mg morphine or equivalent daily. Results: At 4 weeks, 46 of 52 (88.5%) IDDS patients achieved clinical success compared with 65 of 91 (71.4%; P=0.02) non-IDDS patients, and more often achieved ≥20% reduction in both pain VAS and toxicity [35 of 52 (67.3%) versus 33 of 91 patients (36.3%); P = 0.0003]. By 12 weeks, 47 of 57 (82.5%) IDDS patients had clinical success compared with 35 of 45 (77.8%; P=0.55) non-IDDS patients, and more often had a ≥20% reduction in both pain VAS and toxicity [33 of 57 (57.9%) versus 15 of 45 patients (33.3%); P=0.01]. At 12 weeks the IDDS VAS pain scores decreased from 7.81 to 3.89 (47% reduction) compared with 7.21 to 4.53 for non-IDDS patients (42% reduction; P = 0.23). The 12 week drug toxicity scores for IDDS patients decreased from 6.68 to 2.30 (66% reduction), and for non-IDDS patients from 6.73 to 4.13 (37% reduction; P = 0.01). All individual drug toxicities improved with IDDS at both 4 and 12 weeks. At 6 months, only 32% of the group randomized to CMM and who did not cross over to IDDS were alive, compared with 52%-59% for patients in those groups who received IDDS. Conclusions: IDDS improved clinical success, reduced pain scores, relieved most toxicity of pain control drugs, and was associated with increased survival for the duration of this 6 month trial.",

keywords = "Cancer, Implantable devices, Intraspinal therapy, Intrathecal therapy, Opioids, Pain",

author = "Smith, {T. J.} and Coyne, {P. J.} and Staats, {P. S.} and T. Deer and Stearns, {L. J.} and Rauck, {R. L.} and Boortz-Marx, {R. L.} and E. Buchser and E. Catal{\`a} and Bryce, {D. A.} and M. Cousins and Pool, {G. E.} and M. Wallace and T. Yaksh and S. Magnuson and A. Leung and F. Ahadian and S. Bullock and M. McBeth and A. Hoye and R. Miguel and Weitzner, {M. A.} and L. Balducci and K. Follett and P. Hitchon and Minore, {W. S.} and H. Weiss and J. Jaworowicz and S. Croy and S. Davis and S. Grossman and M. Grieb and L. Carson and S. Mitchell and M. Stuckey and S. Charapata and M. McCracken and R. Sorensen and J. Calava and J. Dunn and P. Kosek and S. Weinstein and Banerjee, {T. K.} and D. Caraway and C. Kim and M. Serafini and K. McNeil and J. Frame and G. Orlandini and A. Siragusa and F. Aliaga and A. Lopez-Pousa and C. Pericay and L. Perey and C. Muriel and F. Boyle and A. Molloy and C. Brooker and Walker, {S. E.}",

note = "Funding Information: Mr Pool was formerly employed by Medtronic, Inc. Authors Smith, Coyne, Staats, Rauck, Buchser, Stearns, and Boortz-Marks have received honoraria from Medtronic for lectures or consulting. Authors Smith and Staats had grant support from Medtronic to the academic institutions to perform the trial.",

year = "2005",

month = may,

doi = "10.1093/annonc/mdi156",

language = "English (US)",

volume = "16",

pages = "825--833",

journal = "Annals of Oncology",

issn = "0923-7534",

publisher = "Oxford University Press",

number = "5",

}

TY - JOUR

T1 - An implantable drug delivery system (IDDS) for refractory cancer pain provides sustained pain control, less drug-related toxicity, and possibly better survival compared with comprehensive medical management (CMM)

AU - Smith, T. J.

AU - Coyne, P. J.

AU - Staats, P. S.

AU - Deer, T.

AU - Stearns, L. J.

AU - Rauck, R. L.

AU - Boortz-Marx, R. L.

AU - Buchser, E.

AU - Català, E.

AU - Bryce, D. A.

AU - Cousins, M.

AU - Pool, G. E.

AU - Wallace, M.

AU - Yaksh, T.

AU - Magnuson, S.

AU - Leung, A.

AU - Ahadian, F.

AU - Bullock, S.

AU - McBeth, M.

AU - Hoye, A.

AU - Miguel, R.

AU - Weitzner, M. A.

AU - Balducci, L.

AU - Follett, K.

AU - Hitchon, P.

AU - Minore, W. S.

AU - Weiss, H.

AU - Jaworowicz, J.

AU - Croy, S.

AU - Davis, S.

AU - Grossman, S.

AU - Grieb, M.

AU - Carson, L.

AU - Mitchell, S.

AU - Stuckey, M.

AU - Charapata, S.

AU - McCracken, M.

AU - Sorensen, R.

AU - Calava, J.

AU - Dunn, J.

AU - Kosek, P.

AU - Weinstein, S.

AU - Banerjee, T. K.

AU - Caraway, D.

AU - Kim, C.

AU - Serafini, M.

AU - McNeil, K.

AU - Frame, J.

AU - Orlandini, G.

AU - Siragusa, A.

AU - Aliaga, F.

AU - Lopez-Pousa, A.

AU - Pericay, C.

AU - Perey, L.

AU - Muriel, C.

AU - Boyle, F.

AU - Molloy, A.

AU - Brooker, C.

AU - Walker, S. E.

N1 - Funding Information: Mr Pool was formerly employed by Medtronic, Inc. Authors Smith, Coyne, Staats, Rauck, Buchser, Stearns, and Boortz-Marks have received honoraria from Medtronic for lectures or consulting. Authors Smith and Staats had grant support from Medtronic to the academic institutions to perform the trial.

PY - 2005/5

Y1 - 2005/5

N2 - Background: The randomized clinical trial of implantable drug delivery systems (IDDS) plus comprehensive medical management (CMM) versus CMM alone showed better clinical success at 4 weeks for IDDS patients. This 'as treated' analysis assessed if improvements in pain control, drug toxicity and survival were maintained over time. Patients and methods: We compared those who received IDDS with those who did not receive IDDS (non-IDDS). All patients had Visual Analogue Scores (VAS) for pain ≥5/10 on at least 200 mg morphine or equivalent daily. Results: At 4 weeks, 46 of 52 (88.5%) IDDS patients achieved clinical success compared with 65 of 91 (71.4%; P=0.02) non-IDDS patients, and more often achieved ≥20% reduction in both pain VAS and toxicity [35 of 52 (67.3%) versus 33 of 91 patients (36.3%); P = 0.0003]. By 12 weeks, 47 of 57 (82.5%) IDDS patients had clinical success compared with 35 of 45 (77.8%; P=0.55) non-IDDS patients, and more often had a ≥20% reduction in both pain VAS and toxicity [33 of 57 (57.9%) versus 15 of 45 patients (33.3%); P=0.01]. At 12 weeks the IDDS VAS pain scores decreased from 7.81 to 3.89 (47% reduction) compared with 7.21 to 4.53 for non-IDDS patients (42% reduction; P = 0.23). The 12 week drug toxicity scores for IDDS patients decreased from 6.68 to 2.30 (66% reduction), and for non-IDDS patients from 6.73 to 4.13 (37% reduction; P = 0.01). All individual drug toxicities improved with IDDS at both 4 and 12 weeks. At 6 months, only 32% of the group randomized to CMM and who did not cross over to IDDS were alive, compared with 52%-59% for patients in those groups who received IDDS. Conclusions: IDDS improved clinical success, reduced pain scores, relieved most toxicity of pain control drugs, and was associated with increased survival for the duration of this 6 month trial.

AB - Background: The randomized clinical trial of implantable drug delivery systems (IDDS) plus comprehensive medical management (CMM) versus CMM alone showed better clinical success at 4 weeks for IDDS patients. This 'as treated' analysis assessed if improvements in pain control, drug toxicity and survival were maintained over time. Patients and methods: We compared those who received IDDS with those who did not receive IDDS (non-IDDS). All patients had Visual Analogue Scores (VAS) for pain ≥5/10 on at least 200 mg morphine or equivalent daily. Results: At 4 weeks, 46 of 52 (88.5%) IDDS patients achieved clinical success compared with 65 of 91 (71.4%; P=0.02) non-IDDS patients, and more often achieved ≥20% reduction in both pain VAS and toxicity [35 of 52 (67.3%) versus 33 of 91 patients (36.3%); P = 0.0003]. By 12 weeks, 47 of 57 (82.5%) IDDS patients had clinical success compared with 35 of 45 (77.8%; P=0.55) non-IDDS patients, and more often had a ≥20% reduction in both pain VAS and toxicity [33 of 57 (57.9%) versus 15 of 45 patients (33.3%); P=0.01]. At 12 weeks the IDDS VAS pain scores decreased from 7.81 to 3.89 (47% reduction) compared with 7.21 to 4.53 for non-IDDS patients (42% reduction; P = 0.23). The 12 week drug toxicity scores for IDDS patients decreased from 6.68 to 2.30 (66% reduction), and for non-IDDS patients from 6.73 to 4.13 (37% reduction; P = 0.01). All individual drug toxicities improved with IDDS at both 4 and 12 weeks. At 6 months, only 32% of the group randomized to CMM and who did not cross over to IDDS were alive, compared with 52%-59% for patients in those groups who received IDDS. Conclusions: IDDS improved clinical success, reduced pain scores, relieved most toxicity of pain control drugs, and was associated with increased survival for the duration of this 6 month trial.

KW - Cancer

KW - Implantable devices

KW - Intraspinal therapy

KW - Intrathecal therapy

KW - Opioids

KW - Pain

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DO - 10.1093/annonc/mdi156

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AN - SCOPUS:20044390021

SN - 0923-7534

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An implantable drug delivery system (IDDS) for refractory cancer pain provides sustained pain control, less drug-related toxicity, and possibly better survival compared with comprehensive medical management (CMM)

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Keywords

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