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

Journal ArticleOPEN ACCESS

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 (2005) 16(5) 825-833

DOI: 10.1093/annonc/mdi156

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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. © 2005 European Society for Medical Oncology.

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Smith, T. J., Coyne, P. J., Staats, P. S., Deer, T., Stearns, L. J., Rauck, R. L., … 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)

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