Redifferentiation and/or Enhancement of Radioiodine Uptake for 131I Therapy: A Review of the Literature

Introduction: Metastatic differentiated thyroid cancer CDRC) cells not infrequently lose their ability to take up ¹³¹I,.  Heretofore and in these patients, ¹³¹I therapy is no longer a therapeutic option.  However, with further developments with genomic test and molecular imaging of DTC, selected patients and selected agents may reestablish ¹³¹I uptake in metastatic DTC, thereby allowing additional ¹³¹I therapies. This education exhibit is a review of the publications to date regarding the patients and agents were administered to either re-differentiate (i.e., re-establish ¹³¹I uptake) or enhance (i.e., increase ¹³¹I uptake in patients who had visible but low ¹³¹I uptake).

Methods: A literature search was perform using multiple search tools (e.g., Pub Med, Google Scholar, etc.)  Medical subject heading (MESH) were used including but not limited to differentiated thyroid cancer, ¹³¹I, therapy, radioiodine refractory, BRAF, RAS, etc., selumetinib , trametinib, dabrafenib, etc.  Articles prior to 2013 such as those evaluating rosiglitazone were not evaluated. 

Results: Of the articles identified, the author selected nine articles that were subsequently evaluated for the use of agents to re-differentiate and/or enhance ¹³¹I uptake for potential subsequent ¹³¹I therapy. The review tabulated—when available--the following information:  1) age, 2) gender, 3) molecular profile, 4)  radioiodine scan (including isotope, activity and time of administration of that isotope) prior to treatment with a potential redifferentiation/enhancement (R/E) agent, and the results of that scan, 5) R /E agent(s) administered including dose, frequency, and duration of administration of those agents before subsequent radioiodine scan and ¹³¹I treatment, 6) isotope, activity and time of administration of isotope and results of radioiodine scan after the treatment with a potential (R/E)agent, and the results of that scan , 7) number of patients who received an subsequent ¹³¹I therapy, the therapeutic activity administered, and reported outcomes, and 8) the results of any patients receiving a second R/E evaluation with or without a second ¹³¹I therapy

Conclusions:  Strong preliminary data report that select agents offer significant potential for re-establishing ¹³¹I uptake in patients with metastatic differentiating thyroid cancer who have no visible ¹³¹I uptake on either a diagnostic or a prior post-therapy radioiodine scan.  Equally exiting. is the potential that these agents may have utility in patients who have already demonstrate ¹³¹I uptake in metastatic DTC but in cases where the ^131I uptake is low, thereby potential allowing more Gy (rad) to be delivered per GBq (mCi) of activity administered in turning increase the likelihood of a better therapeutic effect and/or a reduction in the administered activity accomplishing the same desired therapeutic effect while reducing the Gy (rad) delivered to non-target organs such as bone marrow and salivary glands.  This is a very exciting area of research.