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Pituitary iron and volume predict hypogonadism in transfusional iron overload

医学 垂体 内科学 铁蛋白 地中海贫血 内分泌学 胃肠病学 磁共振成像 心脏病学 激素 放射科
作者
Leila Noetzli,Ashok Panigrahy,Steven D. Mittelman,Aleya Hyderi,Ani Dongelyan,Thomas D. Coates,John C. Wood
出处
期刊:American Journal of Hematology [Wiley]
卷期号:87 (2): 167-171 被引量:131
标识
DOI:10.1002/ajh.22247
摘要

Abstract Hypogonadism is the most common morbidity in patients with transfusion‐dependent anemias such as thalassemia major. We used magnetic resonance imaging (MRI) to measure pituitary R 2 (iron) and volume to determine at what age these patients develop pituitary iron overload and volume loss. We recruited 56 patients (47 with thalassemia major, five with chronically transfused thalassemia intermedia and four with Blackfan‐Diamond syndrome) to have pituitary MRIs to measure pituitary R 2 and volume. Hypogonadism was defined clinically based on the timing of secondary sexual characteristics or the need for sex hormone replacement therapy. Patients with transfusional iron overload begin to develop pituitary iron overload in the first decade of life; however, clinically significant volume loss was not observed until the second decade of life. Severe pituitary iron deposition ( Z > 5) and volume loss ( Z < −2.5) were independently predictive of hypogonadism. Pituitary R 2 correlated significantly with serum ferritin as well as liver, pancreatic, and cardiac iron deposition by MRI. Log pancreas R 2* was the best single predictor for pituitary iron, with an area under the receiving operator characteristic curve of 0.88, but log cardiac R 2* and ferritin were retained on multivariate regression with a combined r 2 of 0.71. Pituitary iron overload and volume loss were independently predictive of hypogonadism. Many patients with moderate‐to‐severe pituitary iron overload retained normal gland volume and function, representing a potential therapeutic window. The subset of hypogonadal patients having preserved gland volumes may also explain improvements in pituitary function observed following intensive chelation therapy. Am. J. Hematol. 2011. © 2011 Wiley Periodicals, Inc.

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