Haematologica (Jan 2021)

Risk factors for endocrine complications in transfusion-dependent thalassemia patients on chelation therapy with deferasirox: a risk assessment study from a multi-center nation-wide cohort

  • Maddalena Casale,
  • Gian Luca Forni,
  • Elena Cassinerio,
  • Daniela Pasquali,
  • Raffaella Origa,
  • Marilena Serra,
  • Saveria Campisi,
  • Angelo Peluso,
  • Roberta Renni,
  • Alessandro Cattoni,
  • Elisa De Michele,
  • Massimo Allò,
  • Maurizio Poggi,
  • Francesca Ferrara,
  • Rosanna Di Concilio,
  • Filomena Sportelli,
  • Antonella Quarta,
  • Maria Caterina Putti,
  • Lucia Dora Notarangelo,
  • Antonella Sau,
  • Saverio Ladogana,
  • Immacolata Tartaglione,
  • Stefania Picariello,
  • Alessia Marcon,
  • Patrizia Sturiale,
  • Domenico Roberti,
  • Antonio Ivan Lazzarino,
  • Silverio Perrotta

DOI
https://doi.org/10.3324/haematol.2020.272419
Journal volume & issue
Vol. 107, no. 2

Abstract

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Transfusion-dependent patients typically develop iron-induced cardiomyopathy, liver disease, and endocrine complications. We aimed to estimate the incidence of endocrine disorders in transfusiondependent thalassemia (TDT) patients during long-term iron-chelation therapy with deferasirox (DFX). We developed a multi-center follow-up study of 426 TDT patients treated with once-daily DFX for a median duration of 8 years, up to 18.5 years. At baseline, 118, 121, and 187 patients had 0, 1, or ≥2 endocrine diseases respectively. 104 additional endocrine diseases were developed during the follow-up. The overall risk of developing a new endocrine complication within 5 years was 9.7% (95% Confidence Interval [CI]: 6.3–13.1). Multiple Cox regression analysis identified three key predictors: age showed a positive log-linear effect (adjusted hazard ratio [HR] for 50% increase 1.2, 95% CI: 1.1–1.3, P=0.005), the serum concentration of thyrotropin showed a positive linear effect (adjusted HR for 1 mIU/L increase 1.3, 95% CI: 1.1–1.4, P<0.001) regardless the kind of disease incident, while the number of previous endocrine diseases showed a negative linear effect: the higher the number of diseases at baseline the lower the chance of developing further diseasess (adjusted HR for unit increase 0.5, 95% CI: 0.4–0.7, P<0.001). Age and thyrotropin had similar effect sizes across the categories of baseline diseases. The administration of levothyroxine as a covariate did not change the estimates. Although in DFX-treated TDT patients the risk of developing an endocrine complication is generally lower than the previously reported risk, there is considerable risk variation and the burden of these complications remains high. We developed a simple risk score chart enabling clinicians to estimate their patients’ risk. Future research will look at increasing the amount of variation explained from our model and testing further clinical and laboratory predictors, including the assessment of direct endocrine magnetic resonance imaging.