Hair and Nail Changes During Long-term Therapy With Ibrutinib for Chronic Lymphocytic Leukemia

Abstract: Importance Ibrutinib (Imbruvica®), a Bruton tyrosine kinase (BTK) inhibitor, is a new targeted agent approved by the US Food and Drug Administration for the treatment of chronic lymphocytic leukemia (CLL), mantle cell lymphoma, and Waldenström macroglobulinemia. Ibrutinib is overall well-tolerated but requires long-term treatment until disease progression or intolerable toxicity occurs. Little is known regarding its cutaneous adverse effects. Objective To describe the hair and nail manifestations associated … Show more

“…Dermatological toxicities have also been reported in 2-27% of treated patients (Ransohoff & Kwong, 2017;Iberri et al, 2018), mainly mild-to-moderate rash, neutrophilic panniculitis, progressive hair and nail changes, skin infections, bruising, petechiae and purpuric eruption (Fabbro et al, 2015;Bitar et al, 2016;Ransohoff & Kwong, 2017;Iberri et al, 2018). In contrast, oral toxicity with ibrutinib has rarely been described.…”

Cell‐of‐origin in diffuse large B‐cell lymphoma: findings from the UK's population‐based Haematological Malignancy Research Network

“…Dermatological toxicities have also been reported in 2-27% of treated patients (Ransohoff & Kwong, 2017;Iberri et al, 2018), mainly mild-to-moderate rash, neutrophilic panniculitis, progressive hair and nail changes, skin infections, bruising, petechiae and purpuric eruption (Fabbro et al, 2015;Bitar et al, 2016;Ransohoff & Kwong, 2017;Iberri et al, 2018). In contrast, oral toxicity with ibrutinib has rarely been described.…”

Cell‐of‐origin in diffuse large B‐cell lymphoma: findings from the UK's population‐based Haematological Malignancy Research Network

“…In contrast, oral toxicity with ibrutinib has rarely been described. A prospective dermatological survey did not observe any mucosal involvement in a cohort of 66 consecutive patients (Bitar et al , ). However, a recent pivotal study reported all‐grade and high‐grade stomatitis in 11% and 1% of treated patients, respectively, but the clinical aspects were not documented (Byrd et al , ).…”

“…However, the rate of grade ≥3 adverse events remains low and treatment discontinuation due to toxicity (Byrd et al , , ) is uncommon and mostly related to infections (Byrd et al , , ; Burger et al , ; Puła et al , ; Tran & O'Brien, ). Dermatological toxicities have also been reported in 2–27% of treated patients (Ransohoff & Kwong, ; Iberri et al , ), mainly mild‐to‐moderate rash, neutrophilic panniculitis, progressive hair and nail changes, skin infections, bruising, petechiae and purpuric eruption (Fabbro et al , ; Bitar et al , ; Ransohoff & Kwong, ; Iberri et al , ). In contrast, oral toxicity with ibrutinib has rarely been described.…”

“…It would be reminiscent of a localized adaptive cellular immune response where ibrutinib‐conjugated peptides would be presented to host immune cells via a major histocompatibility complex, leading to a T‐cell‐driven immune response and bystander tissue destruction (Fabbro et al , ). Moreover, although ibrutinib demonstrates high selectivity for BTK, it also exerts off‐target effects on other kinases, including irreversible binding to epidermal growth factor receptor (EGFR) or HER2 (Bitar et al , ). This mechanism could partly explain the pathogenesis of ibrutinib‐associated oral ulcers, even though anti‐EGFR‐related mucositis mostly occurs in the first weeks of treatment, solely involves nonkeratinized mucosae (similar to other kinase inhibitors, including mTOR inhibitors) and remains of low grade (Vigarios et al , ).…”

Dose‐limiting stomatitis associated with ibrutinib therapy: a case series

“…[35] Brittle nails and textural hair changes have been reported during long-term therapy of CLL with ibrutinib, but the underlying mechanisms remain unknown. [86]…”

Pharmacokinetic and pharmacodynamic evaluation of ibrutinib for the treatment of chronic lymphocytic leukemia: rationale for lower doses