Determinants of Atrial Fibrillation Development among Patients undergoing Ibrutinib Therapy
| Author | Onitilo, Adedayo A. |
| Author | Piwuna, Tinuade O. |
| Author | Islam, Nazmul |
| Author | Furuya-Kanamori, Luis |
| Author | Kumar, Sanjay |
| Author | Doi, Suhail A.R. |
| Available date | 2023-02-22T05:47:56Z |
| Publication Date | 2022-03-01 |
| Publication Name | Clinical Medicine and Research |
| Identifier | http://dx.doi.org/10.3121/cmr.2021.1693 |
| Citation | Onitilo AA, Piwuna TO, Islam N, Furuya-Kanamori L, Kumar S, Doi SAR. Determinants of Atrial Fibrillation Development among Patients undergoing Ibrutinib Therapy. Clin Med Res. 2022 Mar;20(1):16-22. doi: 10.3121/cmr.2021.1693. |
| ISSN | 15394182 |
| Abstract | Objective: Within the last decade, the use of ibrutinib, a first-generation, non-selective, irreversible Burton's tyrosine kinase inhibitor for the treatment of hematological malignancies has proven highly effective in improving patient outcomes.Background: Ibrutinib has been associated with an increase in atrial fibrillation (AF). The predisposing factors are thought to be pre-existing cardiovascular risk factors, but these have not been directly evaluated.Methods: We conducted a nested case-control study, recruiting consecutive ibrutinib treated subjects to evaluate cardiovascular risk factors associated with the development of AF in patients diagnosed with hematological B-cell malignancies.Results: Of the 189 patients treated with ibrutinib and without AF at baseline, 54 (29%) developed AF. Cardiovascular risk factors associated with AF development were, older age, prior hypertension (HTN), history of heart failure (HF) and congenital heart disease. A patient with HF at baseline had a 1,2, 6, and 12 month cumulative hazard of AF of 40%, 48%, 64%, and 71%, respectively. Patients with prior HTN without HF at baseline had a 1,2, 6, and 12 month cumulative hazard of AF of 5%, 10%, 23%, and 31%, respectively while on ibrutinib therapy.Conclusions: The relationship between ibrutinib, cardiovascular comorbidities, and AF is through pre-existing cardiovascular disease. An individualized, multidisciplinary approach involving cardiologists should be considered when initiating ibrutinib, particularly when there is a history of HTN, HF or congenital heart disease. In such patients, there should be close cardiovascular monitoring and prompt intervention when AF develops to improve patient outcomes. |
| Language | en |
| Publisher | Marshfield Clinic |
| Subject | Atrial fibrillation B-cell malignancies Bruton’s tyrosine kinase Hematological malignancies Ibrutinib Risk factors |
| Type | Article |
| Pagination | 16-22 |
| Issue Number | 1 |
| Volume Number | 20 |
| ESSN | 1554-6179 |
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