Improvement of Pharmacokinetics of Radioiodinated Tyr<sup>3</sup>-Octreotide by Conjugation with Carbohydrates

Schottelius, Margret; Wester, Hans‐Jürgen; Reubi, Jean Claude; Senekowitsch–Schmidtke, Reingard; Schwaiger, Markus

doi:10.1021/bc0200069

Cited by 99 publications

(134 citation statements)

References 45 publications

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“…1) [1][2][3][4][5] has been determined ( Table 2). The corresponding 19 F reference compounds all showed very high hsst 2 affinity comparable with that of native somatostatin 28, including no affinity to hsst 1 , very low affinity to hsst 3 , and moderate affinity to hsst 4 and hsst 5 . Compared with iodinated Tyr 3 -octreotide, which is used as the internal reference in the dual tracer internalization studies performed in this study, the hsst 2 affinity of Gluc-Lys(FP)-TOCA, Gluc-S-Dpr(FP)TOCA, and Gluc-S-Dpr(FBOA)TOCA is decreased by a factor of two, whereas it is comparable for the Cel-S-Dpr(FBOA) analog.…”

Section: Synthesismentioning

confidence: 96%

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First 18F-Labeled Tracer Suitable for Routine Clinical Imaging of sst Receptor-Expressing Tumors Using Positron Emission Tomography

Schottelius

Poethko

Herz

et al. 2004

Clinical Cancer Research

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Section: Synthesismentioning

confidence: 96%

“…It has been demonstrated for a series of glycosylated, radioiodinated TOC derivatives that the extent of hepatic and intestinal accumulation correlates with ligand lipophilicity (19 18 F-labeled TOCA derivatives investigated in this study (Fig. 7).…”

mentioning

confidence: 99%

First 18F-Labeled Tracer Suitable for Routine Clinical Imaging of sst Receptor-Expressing Tumors Using Positron Emission Tomography

Schottelius

Poethko

Herz

et al. 2004

Clinical Cancer Research

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“…3A) because of the highly lipophilic character of the SiFA synthon. The introduction of a carbohydrate moiety (30) (Fig. 3B).…”

Section: Sifa Labeling Chemistrymentioning

confidence: 99%

In Vivo Evaluation of ¹⁸F-SiFAlin–Modified TATE: A Potential Challenge for ⁶⁸Ga-DOTATATE, the Clinical Gold Standard for Somatostatin Receptor Imaging with PET

et al. 2015

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Radiolabeled peptides for tumor imaging with PET that can be produced with kits are currently in the spotlight of radiopharmacy and nuclear medicine. The diagnosis of neuroendocrine tumors in particular has been a prime example for the usefulness of peptides labeled with a variety of different radionuclides. Among those, 68 Ga and 18 F stand out because of the ease of radionuclide introduction (e.g., 68 Ga isotope) or optimal nuclide properties for PET imaging (slightly favoring the 18 F isotope). The in vivo properties of good manufacturing practice-compliant, newly developed kitlike-producible 18 F-SiFA-and 18 F-SiFAlin-(SiFA 5 silicon-fluoride acceptor) modified TATE derivatives were compared with the current clinical gold standard 68 Ga-DOTATATE for high-quality imaging of somatostatin receptor-bearing tumors. Methods: SiFA-and SiFAlin-derivatized somatostatin analogs were synthesized and radiolabeled using cartridge-based dried 18 F and purified via a C18 cartridge (radiochemical yield 49.8% ± 5.9% within 20-25 min) without high-performance liquid chromatography purification. Tracer lipophilicity and stability in human serum were tested in vitro. Competitive receptor binding affinity studies were performed using AR42J cells. The most promising tracers were evaluated in vivo in an AR42J xenograft mouse model by ex vivo biodistribution and in vivo PET/CT imaging studies for evaluation of their pharmacokinetic profiles, and the results were compared with those of the current clinical gold standard 68 Ga-DOTATATE. Results: Synthetically easily accessible 18 F-labeled silicon-fluoride acceptor-modified somatostatin analogs were developed. They exhibited high binding affinities to somatostatin receptor-positive tumor cells (1.88-14.82 nM). The most potent compound demonstrated comparable pharmacokinetics and an even slightly higher absolute tumor accumulation level in ex vivo biodistribution studies as well as higher tumor standardized uptake values in PET/CT imaging than 68 Ga-DOTATATE in vivo. The radioactivity uptake in nontumor tissue was higher than for 68 Ga-DOTATATE. Conclusion: The introduction of the novel SiFA building block SiFAlin and of hydrophilic auxiliaries enables a favorable in vivo biodistribution profile of the modified TATE peptides, resulting in high tumorto-background ratios although lower than those observed with 68 Ga-DOTATATE. As further advantage, the SiFA methodology enables a kitlike labeling procedure for 18 F-labeled peptides advantageous for routine clinical application.

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“…NOTA octreotide (IMP466) labelled with 18 F, or 68 Ga, is readily taken up by AR42J on mice resulting in high tumour/kidney ratios [65]. Glycosylated octreotide analogues have been labelled with 211 At, or 125 I, with maintained SSTR2 affinity and improved pharmacokinetics in AR42J-bearing rats [66,67]. 213 Bi-labelled DOTATOC has been produced and given promising therapeutic results in one animal model [68].…”

Section: General Methods Including Individualizationmentioning

confidence: 99%

Radionuclide Therapy via SSTR: Future Aspects from Experimental Animal Studies

Forssell-Aronsson¹,

Spetz²,

Ahlman

2012

Neuroendocrinology

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There is need for better therapeutic options for neuroendocrine tumours. The aim of this review was to summarize results of experimental animal studies and raise ideas for future radionuclide therapy based on high expression of somatostatin (SS) receptors by many neuroendocrine tumours. In summary, one of the major options is individualized treatment for each patient, including choice of SS analogues, radionuclides and treatment schedules. Other options are methods to increase the treatment effect on tumour tissue (increasing tumour uptake and retention by upregulation of receptor expression and avoiding saturation of receptor binding), methods to increase the tumour tissue response (by choice of radionuclides, SS analogues or combined therapies), and methods to reduce side effects (diminished uptake and retention in critical organs and reduced normal tissue response). Furthermore, combination therapy with other radiopharmaceuticals, cytotoxic drugs or radiosensitizers can be considered to enhance the effects of radiolabelled SS analogues.

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Improvement of Pharmacokinetics of Radioiodinated Tyr³-Octreotide by Conjugation with Carbohydrates

Cited by 99 publications

References 45 publications

First 18F-Labeled Tracer Suitable for Routine Clinical Imaging of sst Receptor-Expressing Tumors Using Positron Emission Tomography

First 18F-Labeled Tracer Suitable for Routine Clinical Imaging of sst Receptor-Expressing Tumors Using Positron Emission Tomography

In Vivo Evaluation of ¹⁸F-SiFAlin–Modified TATE: A Potential Challenge for ⁶⁸Ga-DOTATATE, the Clinical Gold Standard for Somatostatin Receptor Imaging with PET

Radionuclide Therapy via SSTR: Future Aspects from Experimental Animal Studies

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Improvement of Pharmacokinetics of Radioiodinated Tyr3-Octreotide by Conjugation with Carbohydrates

Cited by 99 publications

References 45 publications

First 18F-Labeled Tracer Suitable for Routine Clinical Imaging of sst Receptor-Expressing Tumors Using Positron Emission Tomography

First 18F-Labeled Tracer Suitable for Routine Clinical Imaging of sst Receptor-Expressing Tumors Using Positron Emission Tomography

In Vivo Evaluation of 18F-SiFAlin–Modified TATE: A Potential Challenge for 68Ga-DOTATATE, the Clinical Gold Standard for Somatostatin Receptor Imaging with PET

Radionuclide Therapy via SSTR: Future Aspects from Experimental Animal Studies

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Product

Resources

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Improvement of Pharmacokinetics of Radioiodinated Tyr³-Octreotide by Conjugation with Carbohydrates

In Vivo Evaluation of ¹⁸F-SiFAlin–Modified TATE: A Potential Challenge for ⁶⁸Ga-DOTATATE, the Clinical Gold Standard for Somatostatin Receptor Imaging with PET