Somatostatin-based radiotherapy with [⁹⁰Y-DOTA]-TOC in neuroendocrine tumors: long-term outcome of a phase I dose escalation study

Neuroendocrine tumors comprise a spectrum of different malignancies with a yearly increasing incidence and prevalence [1]. Most of these tumors express subtypes of the somatostatin receptor [2], which permits binding and internalization of the natural ligand, the 14 amino acid peptide somatostatin (Figure 1A). Stepwise modifications of the somatostatin sequence led to the development of the biologically more stable 8 amino acid somatostatin analogue Octreotide [3, 4] (OC, Figure 1B), which nowadays has become a valuable tool for the treatment of symptomatic neuroendocrine tumors [5, 6].

Introduction of a tyrosine into the third position of the Octreotide sequence resulted in Tyr³-Octreotide (TOC, Figure 1C), which allowed for iodination of the tyrosine residue with the γ-emitter ¹²³I and subsequent somatostatin receptor targeted imaging [7]. The success of somatostatin receptor targeted imaging finally provided the rational for somatostatin receptor targeted radiotherapy.

For the use in somatostatin receptor targeted radiotherapy we coupled TOC with the chelator DOTA, which led to the octapeptide DOTA-TOC [8] (Figure 1D). DOTA-TOC can be labeled with various radioisotopes, including the γ-emitter ¹¹¹In and the β-emitters ¹⁷⁷Lu and ⁹⁰Y. In an in-vivo treatment model ⁹⁰Y-DOTA]-TOC was able to completely eliminate somatostatin receptor expressing xenografts [9]. Based on these promising in-vivo results we introduced ⁹⁰Y-DOTA]-TOC into the clinic within a phase I dose escalation study.

The present work reports the long-term outcome of the dose escalation study with [⁹⁰Y-DOTA]-TOC in patients with progressive neuroendocrine tumors.

The results of this dose escalation study suggest increasing hematological toxicities with increasing [⁹⁰Y-DOTA]-TOC activities. Especially the high dose protocol was associated with a low but present risk of grade 4 hematotoxicities and a higher risk of kidney toxicities. Remarkably, the post hoc analyses suggested a potentially longer survival under the low dose protocol.

Hematotoxicity is an acute toxicity that can be due to irradiation from ⁹⁰Y-DOTA]-TOC circulating through the body or binding to somatostatin receptors on bone marrow cells [19] or due to the small fraction of free ⁹⁰Y that is administered during treatment cycles and that integrates into the bone matrix [20]. The present study suggests higher risk of anemia, leukopenia and thrombocytopenia at higher administered activities of ⁹⁰Y-DOTA]-TOC. These results might represent a step towards preventing severe hematotoxicity by tailoring the applied ⁹⁰Y-DOTA]-TOC activities, e.g. in patients with preexisting hematological toxicities.

Renal toxicity, on the other hand, is a late toxicity of ⁹⁰Y-DOTA]-TOC. It is mainly due to the glomerular filtration and the tubular retention of the radiopeptide and its fragments and usually develops several months or years after treatment. Renal toxicity still represents the dose limiting toxicity in somatostatin based radiopeptide therapy. Renal toxicity rates between 0% and 24% have been reported for treatment with the radiopeptides ⁹⁰Y-DOTA]-TOC and ¹⁷⁷Lu-DOTA]-TOC [21‐26]. These studies have used different inclusion criteria, especially regarding the baseline kidney function; they have used different treatment protocols, different follow-up schemes and different definitions of renal toxicity. Intra-study comparisons are highly warranted to allow for a comparison of the benefits and harms of both radiopeptides. The present results, however, suggest that fractionated low dose protocols might help to reduce this main toxicity of ⁹⁰Y-DOTA]-TOC.

High dose ⁹⁰Y-DOTA]-TOC therapy was introduced in our department in 1999 and had become the standard treatment regime, as the extent of short-term hematological and renal toxicities had shown to be acceptable [14]. The high dose protocol, in comparison to more fractionated dosage protocols, specifically allowed for a significant reduction of travelling efforts for patients recruited from Europe, North America, South America, Africa and Asia. Due to the systematic evaluation of the long-term outcome of all patients treated with ⁹⁰Y-DOTA]-TOC [13] we were now able to also analyze the long-term outcome after the different dosage protocols. These present results reveal that fractionated low dose protocols might help to reduce the toxicity and improve the survival after ⁹⁰Y-DOTA]-TOC.

Strengths of the present study include the comprehensive recruitment of 365 patients, the sufficiently long follow-up to detect renal toxicities months or years after [⁹⁰Y-DOTA]-TOC treatment and the use of competing risk models to assess the long-term toxicities of [⁹⁰Y-DOTA]-TOC.

The longer survival under the low dose protocol, nevertheless, represents an unexpected finding. However, in the present study survival was not a primary outcome. Furthermore, treatment allocation occurred in a non-randomized fashion, as naturally, the clinical introduction of a novel anti-cancer drug is done in a dose escalation study. Dose escalation studies may principally underestimate the outcome of patients receiving the initial dosage regime due to recruitment of very advanced cases to initially receive a new drug or due to advances in supportive care during the enrollment period. Still, in the present analysis, which was adjusted for all baseline characteristics and the cumulative administered activity, the longest survival was found for the initial dosage step. A randomized trial is warranted in order to confirm the results on survival and long-term toxicity of fractionated versus high dose ⁹⁰Y-DOTA]-TOC therapy. Such a prospective trial should use the ECOG status [27], the ENETS grading system [28] and RECIST criteria [29] to investigate potential differences in response as well as differences in the time-to-progression at different dosage schemes. Furthermore, such a trial should examine a possible correlation of pre-existing diabetes, hypertension and proteinuria on kidney toxicity after ⁹⁰Y-DOTA]-TOC.

In conclusion, herein we describe the outcome after clinical introduction and dose escalation of [⁹⁰Y-DOTA]-TOC for somatostatin receptor targeted therapy in patients with metastasized neuroendocrine tumors. This study compares survival, acute toxicities and long-term toxicities of the different [⁹⁰Y-DOTA]-TOC dosage protocols applied. Increasing [⁹⁰Y-DOTA]-TOC activities may be associated with increasing hematological toxicity. The dose related hematotoxicity profile of [⁹⁰Y-DOTA]-TOC could facilitate tailoring [⁹⁰Y-DOTA]-TOC in patients with preexisting hematotoxicities. The results on the long-term outcome suggest that fractionated [⁹⁰Y-DOTA]-TOC treatment might allow to reduce renal toxicity and to improve the overall survival.