Therapeutic administration of 131I for differentiated thyroid cancer, radiation dose to ovaries and outcome of

J. P. Garsi; M. Schlumberger; C. Rubino; M. Ricard; M. Labbé; C. Ceccarelli; C. Schvartz; H. Henri-Amar; S. Bardet; F. De Vathaire

doi:10.1051/radiopro:2008698

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Volume 43 / Numéro 5 (2008)

Radioprotection, 43 5 (2008) 039

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Numéro		Radioprotection Volume 43, Numéro 5, 2008 36th annual meeting of the European Radiation Research Society


Numéro d'article		039
Nombre de pages		1
Section		Poster Presentation - Epidemiology
DOI		https://doi.org/10.1051/radiopro:2008698
Publié en ligne		3 septembre 2008

Radioprotection 2008, Vol. 43, n° 5

Therapeutic administration of 131I for differentiated thyroid cancer, radiation dose to ovaries and outcome of

J. P. Garsi¹, M. Schlumberger¹, C. Rubino¹, M. Ricard¹, M. Labbé¹, C. Ceccarelli², C. Schvartz³, H. Henri-Amar⁴, S. Bardet⁴ and F. De Vathaire¹

¹ INSERM 605 - Institut Gustave Roussy, 39 rue Camille Desmoulins, 94805 Villejuif, France
² University of Piza, Piza, Piza, Italy
³ Francim, Réseau des Registres des Cancers, F-31000 Toulouse, France
⁴ Centre Antoine Baclesse, 3, Avenue Général Harris, 14000 Caen, France

Abstract

Background: Radiation is known to be mutagenic. In thyroid cancer treatment, 131I is usually administered, for the first treatment, at a 3700MBq activity, corresponding to an estimated radiation dose of 140mGy to the ovaries. However data on the effects of 131I therapy on pregnancy outcomes, especially untoward, are scarce.

Methods: Data on 2673 pregnancies were obtained by interviewing female patients treated for thyroid carcinoma who had not received significant external radiation to the ovaries, in three French hospitals and one Italian hospital.

Results: The incidence of miscarriages was 10% before any treatment for thyroid cancer ; this percentage increased after surgery for thyroid cancer, both before (20%) and after (19%) 131I treatment, with no variation according to the cumulative dose. Miscarriages were not significantly more frequent in women treated with 131I during the year before conception, even in subjects who had received more than 370MBq during that year, as compared to women never treated with 131I. The incidence of stillbirths, preterm births, a low birth weight, congenital malformation and death during the first year of life was not significantly different before or after 131I therapy. The incidence of thyroid and non thyroidal cancers was similar in children born either before or after the mother’s exposure to 131I.

Conclusion: In our data, we found no evidence that exposure to 131I affects the outcome of subsequent pregnancies and offspring. Whether the number of malformations, or thyroid and non thyroidal cancers are related to gonadal irradiation remains to be established. Our findings allowed us to fuel the debate on the doubling dose: the concept is still heatedly debated and the value of 1 Gy as the doubling dose in humans should be rediscussed.

Key words: Differentiated thyroid carcinoma / 131I therapy / pregnancy outcome

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