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Endocrinología, Diabetes y Nutrición (English ed.)
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Inicio Endocrinología, Diabetes y Nutrición (English ed.) Priapism associated with cabergoline in a young adult
Información de la revista
Vol. 68. Núm. 2.
Páginas 139-140 (febrero 2021)
Vol. 68. Núm. 2.
Páginas 139-140 (febrero 2021)
Scientific letter
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Priapism associated with cabergoline in a young adult
Priapismo asociado al uso de cabergolina en un adulto joven
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Alex Mesaa,
Autor para correspondencia
almesa@clinic.cat

Corresponding author.
, Ignacio Congeta,b,c, Clara Viñalsa
a Servicio de Endocrinología y Nutrición, Hospital Clínic de Barcelona, Barcelona, Spain
b Institut d’investigacions biomèdiques August Pi I Sunyer (IDIBAPS), Barcelona, Spain
c Centro de Investigación Biomédica en Red de Diabetes y Enfermedades Metabólicas Asociadas (CIBERDEM), Madrid, Spain
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Prolactinomas are the most prevalent pituitary adenomas. While these lesions are more common in women (gender proportion 10:1), in males they tend to manifest in the form of macroprolactinomas. Although such lesions may manifest through a mass effect as headaches and vision disturbances, central hypogonadism is the main manifesting syndrome regardless of tumour size. Dopamine agonists such as cabergoline constitute an effective treatment for prolactinomas, achieving a normalization of prolactin levels and a decrease in tumour size. Their side effects include cardiac valve alterations and, less commonly, compulsive behaviour and hypersexuality.1 Only one case of priapism as a side effect of cabergoline has been reported in the literature to date.2 We report another case in a young adult with macroprolactinoma.

An 18-year-old male with a history of type 1 diabetes mellitus since 10 months of age presented with a weight gain of 10kg over the past year (weight 79.5kg, height 1.70cm), incomplete pubertal development (Tanner stage III–IV, testicular volume 12cc) and a bone age of 16.5 years. The laboratory tests revealed hypogonadotropic hypogonadism with total testosterone levels of 2.41ng/mL (2.6–10ng/mL), LH 1.68IU/L, and FSH 3.33IU/L. Hyperprolactinemia (192μg/L) was also observed, with all other pituitary hormone levels and IGF-1 within normal ranges (228.6ng/mL). Magnetic resonance imaging showed the presence of a macroadenoma measuring 12×9mm in size, with no suprasellar extension, causing contralateral displacement of the pituitary stalk, in the absence of headache and vision disturbances in confrontation visual field examination. Cabergoline 0.25mg twice weekly was started as treatment.

After six months of treatment, the patient showed a marked decrease in prolactinemia (0.59μg/L) associated with clinical (Tanner stage IV–V, testicular volume 16cc) and laboratory test pubertal development (total testosterone 8.89ng/mL [2.6–10ng/mL], LH 3.43IU/L, and FSH 5.14IU/L), as well as a weight loss of 8.6kg and a 1-cm increase in height. Despite the good clinical course, over the following months he experienced weekly episodes of painful, very prolonged erections, always in the absence of sexual stimulation, and had to report to the emergency room up to 6 times for lack of spontaneous detumescence after several hours. Aspirated corpus cavernosum blood gas testing revealed acidosis, hypercapnia and hypoxia suggestive of ischemic priapism. Reversal of the priapism episodes required intracavernous sympathomimetic agents (epinephrine or ephedrine), and blood aspiration in some instances. The patient denied any use of recreational drugs or other medications apart from cabergoline and his regular treatment in the form of subcutaneous multiple dose insulin.

An outpatient study by the reference urologist, with Doppler ultrasound of the cavernous arteries, yielded no relevant findings, the case being oriented as priapism probably secondary to cabergoline. Given this situation, and after completing one year of treatment, with low prolactin levels and tumour reduction (7mm), the decision was made to reduce the cabergoline dose to 0.25mg/week. Following the dose reduction, the patient experienced weekly episodes of painful erections lasting less than an hour and with spontaneous detumescence over the following months, without having to again visit the emergency room. In the presence of low serum prolactin (0.66ng/mL), the cabergoline dose was reduced to 0.125mg/week, followed by no further episodes of priapism and the maintenance of low prolactin levels (6.96ng/mL) and radiological stability (6mm).

Ischemic or low-flow priapism is regarded as a urological emergency. If sustained over time, it may cause structural damage to the erectile tissue, with necrosis and fibrosis of the corpora cavernosa. For this reason, a rapid diagnosis is required, with suppression of the possible triggering factors. Priapism may occur as a side effect of different drug treatments, the most common being those used for erectile dysfunction. There have also been reports of cases associated with the use of antidepressants, antipsychotics and antihypertensive drugs. In the reported cases of drug-induced priapism, no associations have been found with the dosage or the duration of the treatments, priapism being able to manifest after the first dose or after a period of treatment. Our patient had been treated with cabergoline for 6 months.

In addition, due to the evident time coincidence and improvement following cabergoline dose reduction, the suspected cause-effect relationship is based on biological plausibility, since dopamine is a key neurotransmitter involved in erection and the central control of sexual function, acting upon the hypothalamic paraventricular area.3 In fact, apomorphine, a dopaminergic D1/D2 receptor agonist, is useful for the management of erectile dysfunction.

Although we have only found one previously reported case of priapism secondary to cabergoline,2 there are several documented cases involving short half-life and the daily transdermal administration dopamine agonists used in Parkinson’s disease, such as rotigotine.4 A case of clitoral priapism secondary to bromocriptine has also been reported in a female patient.5

In the present case, priapism could also be related to the increase in testosterone levels experienced by the patient after starting cabergoline. Although it has been described in the course of treatment with testosterone,6 we have found no cases of priapism after the resolution of hypogonadism in patients with hyperprolactinemia.

Although priapism is a very uncommon adverse effect of cabergoline, we consider it relevant to report this case in order to enhance awareness of this association and thus facilitate earlier diagnosis and treatment.

References
[1]
M.E. Molitch.
Diagnosis and treatment of pituitary adenomas.
[2]
E. De La Peña Zarzuelo, V. Hernández Cañas, C. Llorente Abarca.
Priapismo secundario a tratamiento por cabergolina: primera descripción de esta asociación.
Actas Urol Esp, 34 (2010), pp. 487-488
[3]
U. Simonsen, S. Comerma-Steffensen, K.-E. Andersson.
Modulation of dopaminergic pathways to treat erectile dysfunction.
Basic Clin Pharmacol Toxicol, 119 (2016), pp. 63-74
[4]
A. Cannas, M. Meloni, M.M. Mascia, P. Solla, G. Orofino, R. Farris, et al.
Priapism and hypersexuality associated with rotigotine in an elderly Parkinsonian patient.
Clin Neuropharmacol, 39 (2016), pp. 162-163
[5]
O. Blin, U.S. Schwertschlag, G. Serratrice.
Painful clitoral tumescence during bromocriptine therapy.
Lancet, 337 (1991), pp. 1231-1232
[6]
A. Albrecht, T. Penger, M. Marx, K. Hirsch, H.G. Dörr.
Short-term adverse effects of testosterone used for priming in prepubertal boys before growth hormone stimulation test.
J Pediatr Endocrinol Metab, 31 (2018), pp. 21-24

Please cite this article as: Mesa A, Conget I, Viñals C. Priapismo asociado al uso de cabergolina en un adulto joven. Endocrinol Diabetes Nutr. 2021;68:139–140.

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