Interventions for improving adherence to iron chelation therapy in people with sickle cell disease or thalassaemia.
Journal
The Cochrane database of systematic reviews
ISSN: 1469-493X
Titre abrégé: Cochrane Database Syst Rev
Pays: England
ID NLM: 100909747
Informations de publication
Date de publication:
06 03 2023
06 03 2023
Historique:
pmc-release:
06
03
2024
entrez:
6
3
2023
pubmed:
7
3
2023
medline:
9
3
2023
Statut:
epublish
Résumé
Regularly transfused people with sickle cell disease (SCD) and people with thalassaemia are at risk of iron overload. Iron overload can lead to iron toxicity in vulnerable organs such as the heart, liver and endocrine glands, which can be prevented and treated with iron-chelating agents. The intensive demands and uncomfortable side effects of therapy can have a negative impact on daily activities and wellbeing, which may affect adherence. To identify and assess the effectiveness of different types of interventions (psychological and psychosocial, educational, medication interventions, or multi-component interventions) and interventions specific to different age groups, to improve adherence to iron chelation therapy compared to another listed intervention, or standard care in people with SCD or thalassaemia. We searched CENTRAL (Cochrane Library), MEDLINE, PubMed, Embase, CINAHL, PsycINFO, ProQuest Dissertations & Global Theses, Web of Science & Social Sciences Conference Proceedings Indexes and ongoing trial databases (13 December 2021). We searched the Cochrane Cystic Fibrosis and Genetic Disorders Group's Haemoglobinopathies Trials Register (1 August 2022). For trials comparing medications or medication changes, only randomised controlled trials (RCTs) were eligible for inclusion. For studies including psychological and psychosocial interventions, educational interventions, or multi-component interventions, non-randomised studies of interventions (NRSIs), controlled before-after studies, and interrupted time series studies with adherence as a primary outcome were also eligible for inclusion. For this update, two authors independently assessed trial eligibility and risk of bias, and extracted data. We assessed the certainty of the evidence using GRADE. We included 19 RCTs and one NRSI published between 1997 and 2021. One trial assessed medication management, one assessed an education intervention (NRSI) and 18 RCTs were of medication interventions. Medications assessed were subcutaneous deferoxamine, and two oral chelating agents, deferiprone and deferasirox. We rated the certainty of evidence as very low to low across all outcomes identified in this review. Four trials measured quality of life (QoL) with validated instruments, but provided no analysable data and reported no difference in QoL. We identified nine comparisons of interest. 1. Deferiprone versus deferoxamine We are uncertain whether or not deferiprone affects adherence to iron chelation therapy (four RCTs, unpooled, very low-certainty evidence), all-cause mortality (risk ratio (RR) 0.47, 95% confidence interval (CI) 0.18 to 1.21; 3 RCTs, 376 participants; very low-certainty evidence), or serious adverse events (SAEs) (RR 1.43, 95% CI 0.83 to 2.46; 1 RCT, 228 participants; very low-certainty evidence). Adherence was reported as "good", "high" or "excellent" by all seven trials, though the data could not be analysed formally: adherence ranged from 69% to 95% (deferiprone, mean 86.6%), and 71% to 93% (deferoxamine, mean 78.8%), based on five trials (474 participants) only. 2. Deferasirox versus deferoxamine We are uncertain whether or not deferasirox affects adherence to iron chelation therapy (three RCTs, unpooled, very low-certainty evidence), although medication adherence was high in all trials. We are uncertain whether or not there is any difference between the drug therapies in serious adverse events (SAEs) (SCD or thalassaemia) or all-cause mortality (thalassaemia). 3. Deferiprone versus deferasirox We are uncertain if there is a difference between oral deferiprone and deferasirox based on a single trial in children (average age 9 to 10 years) with any hereditary haemoglobinopathy in adherence, SAEs and all-cause mortality. 4. Deferasirox film-coated tablet (FCT) versus deferasirox dispersible tablet (DT) One RCT compared deferasirox in different tablet forms. There may be a preference for FCTs, shown through a trend for greater adherence (RR 1.10, 95% CI 0.99 to 1.22; 1 RCT, 88 participants), although medication adherence was high in both groups (FCT 92.9%; DT 85.3%). We are uncertain if there is a benefit in chelation-related AEs with FCTs. We are uncertain if there is a difference in the incidence of SAEs, all-cause mortality or sustained adherence. 5. Deferiprone and deferoxamine combined versus deferiprone alone We are uncertain if there is a difference in adherence, though reporting was usually narrative as triallists report it was "excellent" in both groups (three RCTs, unpooled). We are uncertain if there is a difference in the incidence of SAEs and all-cause mortality. 6. Deferiprone and deferoxamine combined versus deferoxamine alone We are uncertain if there is a difference in adherence (four RCTs), SAEs (none reported in the trial period) and all-cause mortality (no deaths reported in the trial period). There was high adherence in all trials. 7. Deferiprone and deferoxamine combined versus deferiprone and deferasirox combined There may be a difference in favour of deferiprone and deferasirox (combined) in rates of adherence (RR 0.84, 95% CI 0.72 to 0.99) (one RCT), although it was high (> 80%) in both groups. We are uncertain if there is a difference in SAEs, and no deaths were reported in the trial, so we cannot draw conclusions based on these data (one RCT). 8. Medication management versus standard care We are uncertain if there is a difference in QoL (one RCT), and we could not assess adherence due to a lack of reporting in the control group. 9. Education versus standard care One quasi-experimental (NRSI) study could not be analysed due to the severe baseline confounding. The medication comparisons included in this review had higher than average adherence rates not accounted for by differences in medication administration or side effects, though often follow-up was not good (high dropout over longer trials), with adherence based on a per protocol analysis. Participants may have been selected based on higher adherence to trial medications at baseline. Also, within the clinical trial context, there is increased attention and involvement of clinicians, thus high adherence rates may be an artefact of trial participation. Real-world, pragmatic trials in community and clinic settings are needed that examine both confirmed or unconfirmed adherence strategies that may increase adherence to iron chelation therapy. Due to lack of evidence this review cannot comment on intervention strategies for different age groups.
Sections du résumé
BACKGROUND
Regularly transfused people with sickle cell disease (SCD) and people with thalassaemia are at risk of iron overload. Iron overload can lead to iron toxicity in vulnerable organs such as the heart, liver and endocrine glands, which can be prevented and treated with iron-chelating agents. The intensive demands and uncomfortable side effects of therapy can have a negative impact on daily activities and wellbeing, which may affect adherence.
OBJECTIVES
To identify and assess the effectiveness of different types of interventions (psychological and psychosocial, educational, medication interventions, or multi-component interventions) and interventions specific to different age groups, to improve adherence to iron chelation therapy compared to another listed intervention, or standard care in people with SCD or thalassaemia.
SEARCH METHODS
We searched CENTRAL (Cochrane Library), MEDLINE, PubMed, Embase, CINAHL, PsycINFO, ProQuest Dissertations & Global Theses, Web of Science & Social Sciences Conference Proceedings Indexes and ongoing trial databases (13 December 2021). We searched the Cochrane Cystic Fibrosis and Genetic Disorders Group's Haemoglobinopathies Trials Register (1 August 2022).
SELECTION CRITERIA
For trials comparing medications or medication changes, only randomised controlled trials (RCTs) were eligible for inclusion. For studies including psychological and psychosocial interventions, educational interventions, or multi-component interventions, non-randomised studies of interventions (NRSIs), controlled before-after studies, and interrupted time series studies with adherence as a primary outcome were also eligible for inclusion.
DATA COLLECTION AND ANALYSIS
For this update, two authors independently assessed trial eligibility and risk of bias, and extracted data. We assessed the certainty of the evidence using GRADE.
MAIN RESULTS
We included 19 RCTs and one NRSI published between 1997 and 2021. One trial assessed medication management, one assessed an education intervention (NRSI) and 18 RCTs were of medication interventions. Medications assessed were subcutaneous deferoxamine, and two oral chelating agents, deferiprone and deferasirox. We rated the certainty of evidence as very low to low across all outcomes identified in this review. Four trials measured quality of life (QoL) with validated instruments, but provided no analysable data and reported no difference in QoL. We identified nine comparisons of interest. 1. Deferiprone versus deferoxamine We are uncertain whether or not deferiprone affects adherence to iron chelation therapy (four RCTs, unpooled, very low-certainty evidence), all-cause mortality (risk ratio (RR) 0.47, 95% confidence interval (CI) 0.18 to 1.21; 3 RCTs, 376 participants; very low-certainty evidence), or serious adverse events (SAEs) (RR 1.43, 95% CI 0.83 to 2.46; 1 RCT, 228 participants; very low-certainty evidence). Adherence was reported as "good", "high" or "excellent" by all seven trials, though the data could not be analysed formally: adherence ranged from 69% to 95% (deferiprone, mean 86.6%), and 71% to 93% (deferoxamine, mean 78.8%), based on five trials (474 participants) only. 2. Deferasirox versus deferoxamine We are uncertain whether or not deferasirox affects adherence to iron chelation therapy (three RCTs, unpooled, very low-certainty evidence), although medication adherence was high in all trials. We are uncertain whether or not there is any difference between the drug therapies in serious adverse events (SAEs) (SCD or thalassaemia) or all-cause mortality (thalassaemia). 3. Deferiprone versus deferasirox We are uncertain if there is a difference between oral deferiprone and deferasirox based on a single trial in children (average age 9 to 10 years) with any hereditary haemoglobinopathy in adherence, SAEs and all-cause mortality. 4. Deferasirox film-coated tablet (FCT) versus deferasirox dispersible tablet (DT) One RCT compared deferasirox in different tablet forms. There may be a preference for FCTs, shown through a trend for greater adherence (RR 1.10, 95% CI 0.99 to 1.22; 1 RCT, 88 participants), although medication adherence was high in both groups (FCT 92.9%; DT 85.3%). We are uncertain if there is a benefit in chelation-related AEs with FCTs. We are uncertain if there is a difference in the incidence of SAEs, all-cause mortality or sustained adherence. 5. Deferiprone and deferoxamine combined versus deferiprone alone We are uncertain if there is a difference in adherence, though reporting was usually narrative as triallists report it was "excellent" in both groups (three RCTs, unpooled). We are uncertain if there is a difference in the incidence of SAEs and all-cause mortality. 6. Deferiprone and deferoxamine combined versus deferoxamine alone We are uncertain if there is a difference in adherence (four RCTs), SAEs (none reported in the trial period) and all-cause mortality (no deaths reported in the trial period). There was high adherence in all trials. 7. Deferiprone and deferoxamine combined versus deferiprone and deferasirox combined There may be a difference in favour of deferiprone and deferasirox (combined) in rates of adherence (RR 0.84, 95% CI 0.72 to 0.99) (one RCT), although it was high (> 80%) in both groups. We are uncertain if there is a difference in SAEs, and no deaths were reported in the trial, so we cannot draw conclusions based on these data (one RCT). 8. Medication management versus standard care We are uncertain if there is a difference in QoL (one RCT), and we could not assess adherence due to a lack of reporting in the control group. 9. Education versus standard care One quasi-experimental (NRSI) study could not be analysed due to the severe baseline confounding.
AUTHORS' CONCLUSIONS
The medication comparisons included in this review had higher than average adherence rates not accounted for by differences in medication administration or side effects, though often follow-up was not good (high dropout over longer trials), with adherence based on a per protocol analysis. Participants may have been selected based on higher adherence to trial medications at baseline. Also, within the clinical trial context, there is increased attention and involvement of clinicians, thus high adherence rates may be an artefact of trial participation. Real-world, pragmatic trials in community and clinic settings are needed that examine both confirmed or unconfirmed adherence strategies that may increase adherence to iron chelation therapy. Due to lack of evidence this review cannot comment on intervention strategies for different age groups.
Identifiants
pubmed: 36877640
doi: 10.1002/14651858.CD012349.pub3
pmc: PMC9987409
doi:
Substances chimiques
Chelating Agents
0
Deferoxamine
J06Y7MXW4D
Iron
E1UOL152H7
Types de publication
Journal Article
Review
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
CD012349Commentaires et corrections
Type : UpdateOf
Informations de copyright
Copyright © 2023 The Cochrane Collaboration. Published by John Wiley & Sons, Ltd.
Références
Blood. 2011 Jul 28;118(4):884-93
pubmed: 21628399
Caspian J Intern Med. 2022 Winter;13(1):61-69
pubmed: 35178209
Br J Haematol. 2022 Jan;196(1):17-18
pubmed: 34786706
Br J Haematol. 1995 Sep;91(1):224-9
pubmed: 7577638
Blood Adv. 2022 Feb 22;6(4):1243-1254
pubmed: 34847228
JAMA. 2014 Sep 10;312(10):1033-48
pubmed: 25203083
Ann N Y Acad Sci. 2005;1054:486-91
pubmed: 16339703
Haematologica. 2006 Oct;91(10):1343-51
pubmed: 17018383
Br J Haematol. 2003 Apr;121(1):187-9
pubmed: 12670352
Hemoglobin. 2019 May;43(3):198-203
pubmed: 31422722
Blood. 2014 Mar 6;123(10):1447-54
pubmed: 24385534
Health Qual Life Outcomes. 2006 Sep 28;4:73
pubmed: 17007645
Infect Disord Drug Targets. 2015;15(3):189-95
pubmed: 26239735
Am J Hematol. 2017 May;92(5):420-428
pubmed: 28142202
Ayu. 2014 Jan;35(1):15-21
pubmed: 25364194
Cochrane Database Syst Rev. 2018 May 08;5:CD012349
pubmed: 29737522
J Caring Sci. 2019 Sep 01;8(3):149-155
pubmed: 31616644
J Pediatr Psychol. 2020 Jul 1;45(6):593-606
pubmed: 32417887
J Clin Pharmacol. 2016 Sep;56(9):1094-103
pubmed: 26785826
Acta Haematol. 2008;119(3):133-41
pubmed: 18408362
N Engl J Med. 2014 Nov 13;371(20):1908-16
pubmed: 25390741
Hemoglobin. 2011;35(3):206-16
pubmed: 21599433
Phytother Res. 2018 Mar;32(3):496-503
pubmed: 29235162
Anemia. 2012;2012:297641
pubmed: 22924125
Indian Pediatr. 2004 Jan;41(1):21-7
pubmed: 14767084
Br J Haematol. 2007 Feb;136(3):501-8
pubmed: 17233848
J Med Econ. 2016;19(3):292-303
pubmed: 26618853
Circulation. 2007 Apr 10;115(14):1876-84
pubmed: 17372174
Br J Haematol. 2019 Sep;186(6):e209-e211
pubmed: 31344255
Eur J Haematol. 2018 Sep;101(3):272-282
pubmed: 29904950
Basic Clin Pharmacol Toxicol. 2017 Apr;120(4):354-359
pubmed: 27800664
J Pediatr Hematol Oncol. 2006 Jan;28(1):11-6
pubmed: 16394886
J Cardiovasc Magn Reson. 2011 Jul 06;13:34
pubmed: 21733147
Am J Hematol. 2015 Jul;90(7):634-8
pubmed: 25809173
Br J Haematol. 2011 Aug;154(3):387-97
pubmed: 21592110
Adv Ther. 2008 Aug;25(8):725-42
pubmed: 18704280
Qual Life Res. 2014 Oct;23(8):2277-88
pubmed: 24682717
Blood. 2006 May 1;107(9):3455-62
pubmed: 16352812
Lancet Haematol. 2020 Oct;7(10):e713-e714
pubmed: 32976750
Med J Islam Repub Iran. 2020 Jul 22;34:83
pubmed: 33306059
Br J Haematol. 2014 Jun;165(6):745-55
pubmed: 24646011
Br J Haematol. 2009 Apr;145(2):245-54
pubmed: 19236376
Br J Clin Pharmacol. 2017 Mar;83(3):593-602
pubmed: 27641003
Transfus Apher Sci. 2019 Aug;58(4):429-433
pubmed: 31229401
Hematology. 2015 Jun;20(5):297-303
pubmed: 25181014
Phytother Res. 2018 Sep;32(9):1828-1835
pubmed: 29806132
Blood. 2006 May 1;107(9):3738-44
pubmed: 16352815
Health Qual Life Outcomes. 2012 Dec 07;10:148
pubmed: 23216870
J Pharm Pract. 2023 Aug;36(4):749-755
pubmed: 35473439
Pediatrics. 2014 Dec;134(6):1175-83
pubmed: 25404717
F1000Res. 2020 Sep 16;9:1136
pubmed: 33024552
Pediatr Blood Cancer. 2018 Aug;65(8):e27081
pubmed: 29693797
Eur J Haematol. 2015 Nov;95(5):411-20
pubmed: 25600572
Am J Prev Med. 2011 Dec;41(6 Suppl 4):S398-405
pubmed: 22099364
Am J Hematol. 2019 Jan;94(1):E15-E17
pubmed: 30346059
Bull World Health Organ. 2008 Jun;86(6):480-7
pubmed: 18568278
Am J Hematol. 2022 Jul;97(7):924-932
pubmed: 35472008
Adv Ther. 2010 Aug;27(8):533-46
pubmed: 20652657
Haematologica. 2006 Sep;91(9):1187-92
pubmed: 16956817
Cochrane Database Syst Rev. 2016 Sep;2016(9):
pubmed: 27713668
Expert Opin Drug Metab Toxicol. 2020 Mar;16(3):179-193
pubmed: 32067512
N Engl J Med. 2005 Sep 15;353(11):1135-46
pubmed: 16162884
Haematologica. 2006 Sep;91(9):1241-3
pubmed: 16956824
Ann Hematol. 2008 Jul;87(7):545-50
pubmed: 18351337
Lancet Haematol. 2020 Jun;7(6):e469-e478
pubmed: 32470438
Blood. 2008 Jan 15;111(2):583-7
pubmed: 17951527
Electron Physician. 2016 May 25;8(5):2425-31
pubmed: 27382454
J Clin Pharmacol. 1995 Mar;35(3):295-7
pubmed: 7608320
Blood Cells Mol Dis. 2014 Dec;53(4):265-71
pubmed: 24814618
Caspian J Intern Med. 2017 Summer;8(3):159-164
pubmed: 28932366
Eur J Haematol. 2016 Mar;96(3):318-26
pubmed: 26018112
Eur J Haematol. 2015 Sep;95(3):244-53
pubmed: 25418187
Child Care Health Dev. 2004 Nov;30(6):647-65
pubmed: 15527475
Iran J Pediatr. 2016 Jun 01;26(5):e3869
pubmed: 28203323
Pediatr Hematol Oncol. 2014 Oct;31(7):624-37
pubmed: 25116329
Int J Nurs Pract. 2014 Jun;20(3):265-74
pubmed: 24888999
J Natl Med Assoc. 2009 Oct;101(10):1022-33
pubmed: 19860302
Lancet. 2013 Jan 12;381(9861):142-51
pubmed: 23103089
Cochrane Database Syst Rev. 2014 Apr 29;(4):CD007768
pubmed: 24777444
Haematologica. 2012 Jun;97(6):835-41
pubmed: 22180427
Br J Haematol. 2008 Aug;142(4):679-80
pubmed: 18537970
Complement Ther Med. 2017 Dec;35:25-32
pubmed: 29154063
Clin Pract Epidemiol Ment Health. 2009 Feb 23;5:5
pubmed: 19236719
Am J Hematol. 2019 Apr;94(4):E96-E99
pubmed: 30663129
Int J Hematol Oncol Stem Cell Res. 2021 Jan 1;15(1):27-34
pubmed: 33613898
J Pediatr Hematol Oncol. 2009 Oct;31(10):739-44
pubmed: 19734806
Hemoglobin. 2021 Sep;45(5):296-302
pubmed: 34758688
Lancet. 2010 Dec 11;376(9757):2018-31
pubmed: 21131035
J Am Pharm Assoc (2003). 2005 Sep-Oct;45(5):573-9
pubmed: 16295642
Haematologica. 2007 Dec;92(12):1599-606
pubmed: 18055982
Clin Nurs Res. 2014 Aug;23(4):421-41
pubmed: 23572406
Nature. 2014 Nov 13;515(7526):S1
pubmed: 25390134
Am J Hematol. 2015 Feb;90(2):91-6
pubmed: 25345697
Ann Nutr Metab. 2017;71(3-4):136-144
pubmed: 28881347
J Pediatr Psychol. 2016 May;41(4):406-18
pubmed: 26384715
J Ayub Med Coll Abbottabad. 2014 Jul-Sep;26(3):297-300
pubmed: 25671931
Cochrane Database Syst Rev. 2013 Aug 21;(8):CD004450
pubmed: 23963793
Hemoglobin. 2008;32(1-2):41-7
pubmed: 18274982
Turk J Haematol. 2004 Dec 5;21(4):173-6
pubmed: 27264280
Int J Hematol Oncol Stem Cell Res. 2019 Jan 1;13(1):12-19
pubmed: 31205623
Health Qual Life Outcomes. 2018 Nov 19;16(1):216
pubmed: 30453981
BMC Hematol. 2016 Aug 04;16:21
pubmed: 27493757
Nature. 2014 Nov 13;515(7526):S2-3
pubmed: 25390139
Am J Hematol. 2018 Feb;93(2):262-268
pubmed: 29119631