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The variable phenotype and low-risk nature of RAS-positive thyroid nodules

Authors :
Ellen Marqusee
Jeffrey F. Krane
Daniel T. Ruan
Atul A. Gawande
Nancy L. Cho
Francis D. Moore
Matthew I. Kim
Trevor E. Angell
Norra Kwong
Carol B. Benson
Marco Medici
Justine A. Barletta
Erik K. Alexander
Edmund S. Cibas
Mary C. Frates
Source :
BMC Medicine
Publication Year :
2015
Publisher :
Springer Science and Business Media LLC, 2015.

Abstract

Background Oncogenic mutations are common in thyroid cancers. While the frequently detected RAS-oncogene mutations have been studied for diagnostic use in cytologically indeterminate thyroid nodules, no investigation has studied such mutations in an unselected population of thyroid nodules. No long-term study of RAS-positive thyroid nodules has been performed. Methods We performed a prospective, blinded cohort study in 362 consecutive patients presenting with clinically relevant (>1 cm) thyroid nodules. Fine needle aspiration cytology and mutational testing were obtained for all nodules. Post-operative histopathology was obtained for malignant or indeterminate nodules, and benign nodules were sonographically followed. Histopathological features were compared between RAS- and BRAF-positive malignancies. RAS-positive benign nodules were analyzed for growth or cellular change from prior aspirations. Results Overall, 17 of 362 nodules were RAS-positive. Nine separate nodules were BRAF-positive, of which eight underwent surgery and all proved malignant (100 %). Out of the 17 RAS-positive nodules, ten underwent surgery, of which eight proved malignant (47 %). All RAS-positive malignancies were low risk – all follicular variants of papillary carcinoma, without extrathyroidal extension, metastases, or lymphovascular invasion. RAS-positivity was associated with malignancy in younger patients (P = 0.028). Of the nine RAS-positive benign nodules, five had long-term prospective sonographic follow-up (mean 8.3 years) showing no growth or signs of malignancy. Four of these nodules also had previous aspirations (mean 5.8 years prior), all with similar benign results. Conclusions While RAS-oncogene mutations increase malignancy risk, these data demonstrate a low-risk phenotype for most RAS-positive cancers. Furthermore, cytologically benign, yet RAS-positive nodules behave in an indolent fashion over years. RAS-positivity alone should therefore not dictate clinical decisions.

Details

ISSN :
17417015
Volume :
13
Database :
OpenAIRE
Journal :
BMC Medicine
Accession number :
edsair.doi.dedup.....f77a11970a3660aabf76ac26ebced2a2
Full Text :
https://doi.org/10.1186/s12916-015-0419-z