Warning: Undefined array key "mm" in /www/wwwroot/www.ai-bt.com/si.php on line 10 Deprecated: trim(): Passing null to parameter #1 ($string) of type string is deprecated in /www/wwwroot/www.ai-bt.com/si.php on line 10 Breakthrough Cancer Pain in Patients Receiving Low Doses of Opioids for Background Pain.

Literature DB >> 31862860

Breakthrough Cancer Pain in Patients Receiving Low Doses of Opioids for Background Pain.

Sebastiano Mercadante^1,2, Augusto Caraceni³, Francesco Masedu⁴, Teresa Scipioni⁵, Federica Aielli⁵.

Abstract

BACKGROUND: This study aimed to assess the characteristics of breakthrough cancer pain (BTcP) in patients receiving low doses of opioids for background pain in comparison with patients receiving at least 60 mg of oral morphine equivalents (OME).
MATERIALS AND METHODS: Patients with advanced cancer receiving less than 60 mg/day of OME with episodes of BTcP were included in the analysis (group L). Data were compared with patients receiving doses of opioids ≥60 mg of OME (group H). Pain intensity, current analgesic therapy, number of BTcP episodes, intensity of BTcP, its predictability and triggers, onset duration, interference with daily activities, BTcP medications, and time to meaningful pain relief were collected. Adverse effects imputable to a BTcP medication were recorded.
RESULTS: A total of 1,418 and 2,474 patients were included in groups L and H, respectively. A lower number of BTcP episodes (p = .005), a lower BTcP intensity (p = .0001), a faster BTcP onset (p = .024), and a longer time to meaningful pain relief after taking a BTcP medication (p = .009) were found in group L as compared with group H. In group L, BTcP interference on daily activity was less than in group H (p = .009). Patients in group L were less likely to be prescribed an opioid as BTcP medication in comparison with patients in group H (p = .0001). Opioid doses used for BTcP were significantly higher in group H. Patients in group L were more likely to be less satisfied (p = .003) than patients in group H. No adverse effects of severe intensity were reported in both groups.
CONCLUSION: Patients receiving lower doses of opioids exhibit some differences in BTcP presentation: fewer episodes with lower intensity and a faster onset, a longer time to meaningful pain relief, and less satisfaction with BTcP medication. A relevant percentage of patients was receiving fentanyl preparations normally reserved for patients receiving higher doses of opioids. IMPLICATIONS FOR PRACTICE: Breakthrough pain is present in patients receiving low doses of opioids. It has its own peculiarities: less frequent, lower intensity, faster onset, longer time to meaningful pain relief, and less satisfaction with medication. Many patients were prescribed fentanyl preparations, which are normally reserved for patients receiving higher doses of opioids. © AlphaMed Press 2019.

Entities: Chemical Disease Species

Keywords: Breakthrough cancer pain; Doses; Opioids

Mesh：

Substances：
Analgesics, Opioid

Year: 2019 PMID： 31862860 PMCID： PMC7011660 DOI： 10.1634/theoncologist.2019-0542

Source DB: PubMed Journal: Oncologist ISSN： 1083-7159

15 in total

1. Effect of Opioid Exposure on Efficacy and Tolerability of Sublingual Fentanyl and Subcutaneous Morphine for Severe Cancer Pain Episodes. Secondary Analysis From a Double-Blind Double-Dummy, Randomized Trial.

Authors: Francesca Ricchini; Augusto Caraceni; Ernesto Zecca; Alessandra Pigni; Fabio Centurioni; Andrea Manzoni; Stein Kaasa; Cinzia Brunelli
Journal: J Pain Symptom Manage Date: 2019-06-21 Impact factor: 3.612

2. The management of cancer-related breakthrough pain: recommendations of a task group of the Science Committee of the Association for Palliative Medicine of Great Britain and Ireland.

Authors: Andrew N Davies; Andrew Dickman; Colette Reid; Anna-Marie Stevens; Giovambattista Zeppetella
Journal: Eur J Pain Date: 2008-08-15 Impact factor: 3.931

Review 3. From "Breakthrough" to "Episodic" Cancer Pain? A European Association for Palliative Care Research Network Expert Delphi Survey Toward a Common Terminology and Classification of Transient Cancer Pain Exacerbations.

Authors: Erik Torbjørn Løhre; Pål Klepstad; Michael I Bennett; Cinzia Brunelli; Augusto Caraceni; Robin L Fainsinger; Anne Kari Knudsen; Sebastiano Mercadante; Per Sjøgren; Stein Kaasa
Journal: J Pain Symptom Manage Date: 2016-02-26 Impact factor: 3.612

4. Breakthrough cancer pain: twenty-five years of study.

Authors: Sebastiano Mercadante; Russell K Portenoy
Journal: Pain Date: 2016-12 Impact factor: 6.961

5. The use of low doses of a sublingual fentanyl formulation for breakthrough pain in patients receiving low doses of opioids.

Authors: Sebastiano Mercadante; Claudio Adile; Arturo Cuomo; Federica Aielli; Franco Marinangeli; Alessandra Casuccio
Journal: Support Care Cancer Date: 2016-10-15 Impact factor: 3.603

Review 6. Breakthrough pain and its treatment: critical review and recommendations of IOPS (Italian Oncologic Pain Survey) expert group.

Authors: Sebastiano Mercadante; Paolo Marchetti; Arturo Cuomo; Massimo Mammucari; Augusto Caraceni
Journal: Support Care Cancer Date: 2015-10-05 Impact factor: 3.603

7. Prevalence and characteristics of breakthrough pain in cancer patients admitted to a hospice.

Authors: G Zeppetella; C A O'Doherty; S Collins
Journal: J Pain Symptom Manage Date: 2000-08 Impact factor: 3.612

8. The prevalence of episodic pain in cancer: a survey of hospice patients on admission.

Authors: M Swanwick; M Haworth; R F Lennard
Journal: Palliat Med Date: 2001-01 Impact factor: 4.762

9. Response to Oral Immediate-Release Opioids for Breakthrough Pain in Patients with Advanced Cancer with Adequately Controlled Background Pain.

Authors: Ahsan Azhar; Yu Jung Kim; Ali Haider; David Hui; Vishidha R Balankari; Margeaux Chiou Epner; Minjeong Park; Diane D Liu; Janet Williams; Susan E Frisbee-Hume; Julio A Allo; Eduardo Bruera
Journal: Oncologist Date: 2018-09-25

10. Breakthrough cancer pain: prevalence and characteristics in patients in Catalonia, Spain.

Authors: Xavier Gómez-Batiste; Federico Madrid; Francisco Moreno; Albert Gracia; Jordi Trelis; Maria Nabal; Ramón Alcalde; Josep Planas; Helena Camell
Journal: J Pain Symptom Manage Date: 2002-07 Impact factor: 3.612

4 in total

1. Understanding the Chameleonic Breakthrough Cancer Pain.

Authors: Sebastiano Mercadante; Russell K Portenoy
Journal: Drugs Date: 2021-01-30 Impact factor: 9.546

2. Efficacy of adenosylmethionine combined with Si Mo Tang in treatment of neonatal jaundice.

Authors: Ling Li; Jingqun Wang; Shuxia Geng; Fang Liu; Lili Ping; Xiaohong Gu; Xueai Fan; Mei Yang; Lixia Liang; Wei Guo
Journal: Am J Transl Res Date: 2022-06-15 Impact factor: 3.940

Review 3. Prostate cancer induced bone pain: pathobiology, current treatments and pain responses from recent clinical trials.

Authors: A E Smith; A Muralidharan; M T Smith
Journal: Discov Oncol Date: 2022-10-18

4. Characterizing Breakthrough Cancer Pain Using Ecological Momentary Assessment with a Smartphone App: Feasibility and Clinical Findings.

Authors: Francisco Villegas; Verónica Martínez-Borba; Carlos Suso-Ribera; Diana Castilla; Irene Zaragoza; Azucena García-Palacios; Carlos Ferrer
Journal: Int J Environ Res Public Health Date: 2021-06-03 Impact factor: 4.614

4 in total