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A safe and effective method for converting cancer patients from intravenous to transdermal fentanyl.
Cancer. 2001 Dec 15; 92(12):3056-61.C

Abstract

BACKGROUND

Therapeutic fentanyl blood levels are reached approximately 12-16 hours after the initial application of transdermal fentanyl patches. For this reason, fentanyl patches should not be used to treat acute exacerbations of cancer pain. Acute cancer-related pain can be treated with fentanyl administered by continuous intravenous infusion (CII) in combination with patient-controlled analgesia (PCA). Patients then can be switched from intravenous (IV) to transdermal fentanyl once stable pain relief has been achieved. The objective of the current case series was to evaluate and describe the safety and effectiveness of a method for converting hospitalized patients with cancer-related pain from IV to transdermal fentanyl.

METHODS

The authors prospectively evaluated 15 consecutive cancer patients during the conversion from IV to transdermal fentanyl. In all patients, a transdermal patch delivering fentanyl at a rate equivalent to that of the final continuous IV infusion was applied. The CII rate was decreased by 50% 6 hours after application of the fentanyl patch and then discontinued after another 6 hours. Demand boluses of IV fentanyl equivalent in dosage to 50-100% of the final CII rate remained available via PCA during the 24 hours after patch application. Pain intensity (on a scale of 0-10), sedation (on a scale of 0-3), and hourly PCA administration (microg/hr) were assessed and recorded immediately prior to application of the fentanyl patch and 6, 12, 18, and 24 hours thereafter.

RESULTS

Pain intensity, sedation, and hourly PCA administration appeared to remain stable throughout the transition from IV to transdermal fentanyl.

CONCLUSIONS

The results of the current study demonstrate that the conversion from IV to transdermal fentanyl can be accomplished safely and effectively using a 1:1 (IV:transdermal) conversion ratio and a two-step taper of the CII over 12 hours.

Authors+Show Affiliations

Kornick CA
Pain and Palliative Care Service, Department of Neurology, Memorial Sloan-Kettering Cancer Center, New York, New York 10021, USA.
Santiago-Palma J
No affiliation info available
Khojainova N
No affiliation info available
Primavera LH
No affiliation info available
Payne R
No affiliation info available
Manfredi PL
No affiliation info available

MeSH

Administration, CutaneousAdultAgedAnalgesics, OpioidFemaleFentanylHumansInfusions, IntravenousMaleMiddle AgedNeoplasmsPainProspective Studies

Pub Type(s)

Clinical Trial
Journal Article
Research Support, Non-U.S. Gov't
Research Support, U.S. Gov't, P.H.S.

Language

eng

PubMed ID

11753984

Citation

Kornick, C A., et al. "A Safe and Effective Method for Converting Cancer Patients From Intravenous to Transdermal Fentanyl." Cancer, vol. 92, no. 12, 2001, pp. 3056-61.
Kornick CA, Santiago-Palma J, Khojainova N, et al. A safe and effective method for converting cancer patients from intravenous to transdermal fentanyl. Cancer. 2001;92(12):3056-61.
Kornick, C. A., Santiago-Palma, J., Khojainova, N., Primavera, L. H., Payne, R., & Manfredi, P. L. (2001). A safe and effective method for converting cancer patients from intravenous to transdermal fentanyl. Cancer, 92(12), 3056-61.
Kornick CA, et al. A Safe and Effective Method for Converting Cancer Patients From Intravenous to Transdermal Fentanyl. Cancer. 2001 Dec 15;92(12):3056-61. PubMed PMID: 11753984.
* Article titles in AMA citation format should be in sentence-case
TY - JOUR T1 - A safe and effective method for converting cancer patients from intravenous to transdermal fentanyl. AU - Kornick,C A, AU - Santiago-Palma,J, AU - Khojainova,N, AU - Primavera,L H, AU - Payne,R, AU - Manfredi,P L, PY - 2001/12/26/pubmed PY - 2002/1/18/medline PY - 2001/12/26/entrez SP - 3056 EP - 61 JF - Cancer JO - Cancer VL - 92 IS - 12 N2 - BACKGROUND: Therapeutic fentanyl blood levels are reached approximately 12-16 hours after the initial application of transdermal fentanyl patches. For this reason, fentanyl patches should not be used to treat acute exacerbations of cancer pain. Acute cancer-related pain can be treated with fentanyl administered by continuous intravenous infusion (CII) in combination with patient-controlled analgesia (PCA). Patients then can be switched from intravenous (IV) to transdermal fentanyl once stable pain relief has been achieved. The objective of the current case series was to evaluate and describe the safety and effectiveness of a method for converting hospitalized patients with cancer-related pain from IV to transdermal fentanyl. METHODS: The authors prospectively evaluated 15 consecutive cancer patients during the conversion from IV to transdermal fentanyl. In all patients, a transdermal patch delivering fentanyl at a rate equivalent to that of the final continuous IV infusion was applied. The CII rate was decreased by 50% 6 hours after application of the fentanyl patch and then discontinued after another 6 hours. Demand boluses of IV fentanyl equivalent in dosage to 50-100% of the final CII rate remained available via PCA during the 24 hours after patch application. Pain intensity (on a scale of 0-10), sedation (on a scale of 0-3), and hourly PCA administration (microg/hr) were assessed and recorded immediately prior to application of the fentanyl patch and 6, 12, 18, and 24 hours thereafter. RESULTS: Pain intensity, sedation, and hourly PCA administration appeared to remain stable throughout the transition from IV to transdermal fentanyl. CONCLUSIONS: The results of the current study demonstrate that the conversion from IV to transdermal fentanyl can be accomplished safely and effectively using a 1:1 (IV:transdermal) conversion ratio and a two-step taper of the CII over 12 hours. SN - 0008-543X UR - https://www.unboundmedicine.com/medline/citation/11753984/A_safe_and_effective_method_for_converting_cancer_patients_from_intravenous_to_transdermal_fentanyl_ L2 - https://medlineplus.gov/pain.html DB - PRIME DP - Unbound Medicine ER -