Somatostatin receptor-targeted radionuclide therapy of tumors: Preclinical and clinical findings
In preclinical studies in rats we evaluated biodistribution and therapeutic effects of different somatostatin analogs, [ 111In-DTPA]octreotide, [ 90Y-DOTA, Tyr 3]octreotide and [ 177Lu-DOTA, Tyr 3]octreotate, currently also being applied in clinical radionuclide therapy studies. [Tyr 3]octreotide an...
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Veröffentlicht in: | Seminars in nuclear medicine 2002-04, Vol.32 (2), p.133-140 |
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Zusammenfassung: | In preclinical studies in rats we evaluated biodistribution and therapeutic effects of different somatostatin analogs, [
111In-DTPA]octreotide, [
90Y-DOTA, Tyr
3]octreotide and [
177Lu-DOTA, Tyr
3]octreotate, currently also being applied in clinical radionuclide therapy studies. [Tyr
3]octreotide and [Tyr
3] octreotate, chelated with DTPA or DOTA, both showed high affinity binding to somatostatin receptor subtype 2 (sst
2) in vitro. The radiolabelled compounds all showed high tumor uptake in sst
2-positive tumors in vivo in rats, the highest uptake being reached with [
177Lu-DOTA, Tyr
3]octreotate. In preclinical therapy studies in vivo in rats, excellent, dose dependent, tumor size responses were found, responses appeared to be dependent on tumor size at therapy start. These preclinical data showed the great promise of radionuclide therapy with radiolabelled somatostatin analogues. They emphasised the concept that especially the combination of somatostatin analogs radiolabeled with different radionuclides, like
90Y and
177Lu, is most promising to reach a wider tumor size region of high curability.
Furthermore, different phase I clinical studies, using [
111In-DTPA]octreotide, [
90Y-DOTA, Tyr
3]octreotide or [
177Lu-DOTA, Tyr
3]octreotate are described. Fifty patients with somatostatin receptor-positive tumors were treated with multiple doses of [
111In-DTPA
0]octreotide. Forty patients were evaluable after cumulative doses of at least 20 GBq up to 160 GBq. Therapeutic effects were seen in 21 patients: partial remission in 1 patient, minor remissions in 6 patients, and stabilization of previously progressive tumors in 14 patients. The toxicity was generally mild bone marrow toxicity, but 3 of the 6 patients who received more than 100 GBq developed a myelodysplastic syndrome or leukemia. Radionuclide therapy with [
90Y-DOTA, Tyr
3]octreotide started in 3 different phase I trials. Overall, antimitotic effects have been observed: about 20% partial response and 60% stable disease (N=92) along with complete symptomatic cure of several malignant insulinoma and gastrinoma patients. Maximum cumulative [
90Y-DOTA, Tyr
3]octreotide dose was about 26 GBq, without reaching the maximum tolerable dose. New is the use of [
177Lu-DOTA, Tyr
3]octreotate, which shows the highest tumor uptake of all tested octreotide analogs so far, with excellent tumor-to-kidney ratios. Radionuclide therapy with this analog in a phase 1 trial started recently in our center in 63 patients (2 |
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ISSN: | 0001-2998 1558-4623 |
DOI: | 10.1053/snuc.2002.31027 |