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Bupivacaine administered intrathecally versus rectally in the management of intractable rectal cancer pain in palliative care

BACKGROUND: Unacceptable adverse effects, contraindications to and/or ineffectiveness of World Health Organization step III “pain ladder” drugs causes needless suffering among a population of cancer patients. Successful management of severe cancer pain may require invasive treatment. However, a pati...

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Autores principales: Zaporowska-Stachowiak, Iwona, Kowalski, Grzegorz, Łuczak, Jacek, Kosicka, Katarzyna, Kotlinska-Lemieszek, Aleksandra, Sopata, Maciej, Główka, Franciszek
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Dove Medical Press 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4199793/
https://www.ncbi.nlm.nih.gov/pubmed/25336967
http://dx.doi.org/10.2147/OTT.S61768
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author Zaporowska-Stachowiak, Iwona
Kowalski, Grzegorz
Łuczak, Jacek
Kosicka, Katarzyna
Kotlinska-Lemieszek, Aleksandra
Sopata, Maciej
Główka, Franciszek
author_facet Zaporowska-Stachowiak, Iwona
Kowalski, Grzegorz
Łuczak, Jacek
Kosicka, Katarzyna
Kotlinska-Lemieszek, Aleksandra
Sopata, Maciej
Główka, Franciszek
author_sort Zaporowska-Stachowiak, Iwona
collection PubMed
description BACKGROUND: Unacceptable adverse effects, contraindications to and/or ineffectiveness of World Health Organization step III “pain ladder” drugs causes needless suffering among a population of cancer patients. Successful management of severe cancer pain may require invasive treatment. However, a patient’s refusal of an invasive procedure necessitates that clinicians consider alternative options. OBJECTIVE: Intrathecal bupivacaine delivery as a viable treatment of intractable pain is well documented. There are no data on rectal bupivacaine use in cancer patients or in the treatment of cancer tenesmoid pain. This study aims to demonstrate that bupivacaine administered rectally could be a step in between the current treatment options for intractable cancer pain (conventional/conservative analgesia or invasive procedures), and to evaluate the effect of the mode of administration (intrathecal versus rectal) on the bupivacaine plasma concentration. CASES: We present two Caucasian, elderly inpatients admitted to hospice due to intractable rectal/tenesmoid pain. The first case is a female with vulvar cancer, and malignant infiltration of the rectum/vagina. Bupivacaine was used intrathecally (0.25–0.5%, 1–2 mL every 6 hours). The second case is a female with ovarian cancer and malignant rectal infiltration. Bupivacaine was adminstered rectally (0.05–0.1%, 100 mL every 4.5–11 hours). METHODS: Total bupivacaine plasma concentrations were determined using the high-performance liquid chromatography-ultraviolet method. RESULTS: Effective pain control was achieved with intrathecal bupivacaine (0.077–0.154 mg·kg(−1)) and bupivacaine in enema (1.820 mg·kg(−1)). Intrathecal bupivacaine (0.5%, 2 mL) caused a drop in blood pressure; other side effects were absent in both cases. Total plasma bupivacaine concentrations following intrathecal and rectal bupivacaine application did not exceed 317.2 ng·mL(−1) and 235.7 ng·mL(−1), respectively. Bupivacaine elimination was slower after rectal than after intrathecal administration (t(½)= 5.50 versus 2.02 hours, respectively). LIMITATIONS: This study reports two cases only, and there could be inter-patient variation. CONCLUSION: Bupivacaine in boluses administered intrathecally (0.25%, 2 mL) provided effective, safe analgesia in advanced cancer patients. Bupivacaine enema (100 mg·100 mL(−1)) was shown to be a valuable option for control of end-of-life tenesmoid cancer pain.
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spelling pubmed-41997932014-10-21 Bupivacaine administered intrathecally versus rectally in the management of intractable rectal cancer pain in palliative care Zaporowska-Stachowiak, Iwona Kowalski, Grzegorz Łuczak, Jacek Kosicka, Katarzyna Kotlinska-Lemieszek, Aleksandra Sopata, Maciej Główka, Franciszek Onco Targets Ther Case Series BACKGROUND: Unacceptable adverse effects, contraindications to and/or ineffectiveness of World Health Organization step III “pain ladder” drugs causes needless suffering among a population of cancer patients. Successful management of severe cancer pain may require invasive treatment. However, a patient’s refusal of an invasive procedure necessitates that clinicians consider alternative options. OBJECTIVE: Intrathecal bupivacaine delivery as a viable treatment of intractable pain is well documented. There are no data on rectal bupivacaine use in cancer patients or in the treatment of cancer tenesmoid pain. This study aims to demonstrate that bupivacaine administered rectally could be a step in between the current treatment options for intractable cancer pain (conventional/conservative analgesia or invasive procedures), and to evaluate the effect of the mode of administration (intrathecal versus rectal) on the bupivacaine plasma concentration. CASES: We present two Caucasian, elderly inpatients admitted to hospice due to intractable rectal/tenesmoid pain. The first case is a female with vulvar cancer, and malignant infiltration of the rectum/vagina. Bupivacaine was used intrathecally (0.25–0.5%, 1–2 mL every 6 hours). The second case is a female with ovarian cancer and malignant rectal infiltration. Bupivacaine was adminstered rectally (0.05–0.1%, 100 mL every 4.5–11 hours). METHODS: Total bupivacaine plasma concentrations were determined using the high-performance liquid chromatography-ultraviolet method. RESULTS: Effective pain control was achieved with intrathecal bupivacaine (0.077–0.154 mg·kg(−1)) and bupivacaine in enema (1.820 mg·kg(−1)). Intrathecal bupivacaine (0.5%, 2 mL) caused a drop in blood pressure; other side effects were absent in both cases. Total plasma bupivacaine concentrations following intrathecal and rectal bupivacaine application did not exceed 317.2 ng·mL(−1) and 235.7 ng·mL(−1), respectively. Bupivacaine elimination was slower after rectal than after intrathecal administration (t(½)= 5.50 versus 2.02 hours, respectively). LIMITATIONS: This study reports two cases only, and there could be inter-patient variation. CONCLUSION: Bupivacaine in boluses administered intrathecally (0.25%, 2 mL) provided effective, safe analgesia in advanced cancer patients. Bupivacaine enema (100 mg·100 mL(−1)) was shown to be a valuable option for control of end-of-life tenesmoid cancer pain. Dove Medical Press 2014-10-06 /pmc/articles/PMC4199793/ /pubmed/25336967 http://dx.doi.org/10.2147/OTT.S61768 Text en © 2014 Zaporowska-Stachowiak et al. This work is published by Dove Medical Press Limited, and licensed under Creative Commons Attribution – Non Commercial (unported, v3.0) License The full terms of the License are available at http://creativecommons.org/licenses/by-nc/3.0/. Non-commercial uses of the work are permitted without any further permission from Dove Medical Press Limited, provided the work is properly attributed.
spellingShingle Case Series
Zaporowska-Stachowiak, Iwona
Kowalski, Grzegorz
Łuczak, Jacek
Kosicka, Katarzyna
Kotlinska-Lemieszek, Aleksandra
Sopata, Maciej
Główka, Franciszek
Bupivacaine administered intrathecally versus rectally in the management of intractable rectal cancer pain in palliative care
title Bupivacaine administered intrathecally versus rectally in the management of intractable rectal cancer pain in palliative care
title_full Bupivacaine administered intrathecally versus rectally in the management of intractable rectal cancer pain in palliative care
title_fullStr Bupivacaine administered intrathecally versus rectally in the management of intractable rectal cancer pain in palliative care
title_full_unstemmed Bupivacaine administered intrathecally versus rectally in the management of intractable rectal cancer pain in palliative care
title_short Bupivacaine administered intrathecally versus rectally in the management of intractable rectal cancer pain in palliative care
title_sort bupivacaine administered intrathecally versus rectally in the management of intractable rectal cancer pain in palliative care
topic Case Series
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4199793/
https://www.ncbi.nlm.nih.gov/pubmed/25336967
http://dx.doi.org/10.2147/OTT.S61768
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