10029 Background: Somatostatin receptors are highly expressed in several pediatric solid tumors, including neuroblastoma, medulloblastoma and neuroendocrine tumors. We hypothesize that molecularly targeted somatostatin analog, 90Y-DOTA- tyr3-Octreotide which binds with high affinity to somatostatin receptor type 2 (sst2), will be an effective therapy for pediatric malignancies that express sst2. Methods: A Phase I, dose/toxicity trial of 90Y-DOTA-tyr3-Octreotide was conducted at 30 (cohort 1), 40 (cohort2), and 50 (cohort 3) mCi/m2 with concomitant Aminosyn II infusion. Subjects received 3 cycles of treatment, 6 weeks apart. Eligibility criteria included: recurrent or progressive malignancy with at least one Octreoscan positive lesion; age 2–25 yrs; bone marrow cellularity >40%; GFR >80 ml/min/m2; no radiation therapy for 3 months; no chemotherapy for 30 days. Escalation was based on 3/3 or 4/6 subjects with no dose limiting toxicity. Additionally, subjects were limited to <21Gy calculated radiation dose to kidneys, including any previous external beam radiotherapy received prior to 90Y-DOTA-tyr3- Octreotide dosing. Results: Twelve subjects completed 3 cycles (5, 3 and 4 subjects in cohorts 1,2, 3, respectively). Diagnoses included gastrinoma (3), foregut carcinoid (3), neuroblastoma (2), paraganglioma (2), MENIIb, and anaplastic astrocytoma. Five subjects (38%) had a PR (>50% decrease in target lesion); four subjects had a positive response (>25%<50% decrease in target lesion); three subjects had stable disease for > 4 months; seven subjects remain alive without progression 2 months to 3.5 years after completion of therapy. Four subjects withdrew from the study after one cycle and had progressive disease within 6 weeks. No dose limiting toxicities were observed; specifically, no Grade III or greater renal or hematologic toxicity was observed. Conclusions: Based on intent to treat, 53% of children and young adults with recurrent, sst2 positive tumor had a positive response to 90Y-DOTA-tyr3- Octreotide. PR was obtained in at least one subject at each dose level. No dose limiting toxicities were observed with 50 mCi/m2, the recommended dose for Phase II studies. Author Disclosure Employment or Leadership Consultant or Advisory Role Stock Ownership Honoraria Research Expert Testimony Other Remuneration Molecular Insight Pharmaceuticals Milecular Insight Pharmaceuticals, Novartis Pharmaceuticals, Inc. Molecular Insight Pharmaceuticals
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