2015
DOI: 10.1021/acs.bioconjchem.5b00510
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Next Generation of SiFAlin-Based TATE Derivatives for PET Imaging of SSTR-Positive Tumors: Influence of Molecular Design on In Vitro SSTR Binding and In Vivo Pharmacokinetics

Abstract: The Silicon-Fluoride-Acceptor (SiFA)-(18)F-labeling strategy has been shown before to enable the straightforward and efficient (18)F-labeling of complex biologically active substances such as proteins and peptides. Especially in the case of peptides, the radiolabeling proceeds kit-like in short reaction times and without the need of complex product workup. SiFA-derivatized, (18)F-labeled Tyr(3)-octreotate (TATE) derivatives demonstrated, besides strong somatostatin receptor (SSTR) binding, favorable in vivo ph… Show more

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Cited by 36 publications
(54 citation statements)
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“…Both peptides were synthesized by standard solid phase peptide synthesis (SPPS) methods [ 13 , 21 ] by successive conjugation of the respective N α -Fmoc-amino acids after HBTU activation to the respective rink amide resin and finally modified on resin with bis -Boc-aminooxy acetic acid, giving aminooxy-PESIN ( 1 ) and [Lys 4 (aminooxy),Trp 5 ,Nle 7 ]BVD 15 ( 2 ) ( Figure 3 ). In case of PESIN, the aminooxy functionality was introduced at the N -terminal end as the peptide can be modified in this position without considerable alterations in binding affinity.…”
Section: Resultsmentioning
confidence: 99%
“…Both peptides were synthesized by standard solid phase peptide synthesis (SPPS) methods [ 13 , 21 ] by successive conjugation of the respective N α -Fmoc-amino acids after HBTU activation to the respective rink amide resin and finally modified on resin with bis -Boc-aminooxy acetic acid, giving aminooxy-PESIN ( 1 ) and [Lys 4 (aminooxy),Trp 5 ,Nle 7 ]BVD 15 ( 2 ) ( Figure 3 ). In case of PESIN, the aminooxy functionality was introduced at the N -terminal end as the peptide can be modified in this position without considerable alterations in binding affinity.…”
Section: Resultsmentioning
confidence: 99%
“…Just as the development of [ 11 C]CO 2 fixation technologies 56 , 193 , 194 led to a surge in development of imaging agents for both HDAC and FAAH, other new radiosynthetic technologies are likely to drive the development of new tracers for imaging a wide array of hydrolytic enzymes. Exciting and convenient (“kit-like”) new approaches have been recently reported that could easily drive the future development of tracers for imaging hydrolytic enzymes, such as reactions with uncommon nuclei 195 including [ 18 F]trifluoroborates, 196 - 198 [ 18 F]silicon fluoride, 199 , 200 [ 18 F]sulfonyl fluoride-containing prosthetic groups, 201 and chelation of Al[ 18 F]F. 202 The major drawback to many of these techniques as they currently exist is that they require attachment of prosthetic groups or chelators to facilitate radiolabeling, which are chemical moieties that add steric bulk and can change the polarity and biodistribution of the attached drug. Another promising area of future development are new reactions for rapidly forming aryl carbon–[ 18 F]fluorine bonds.…”
Section: Discussionmentioning
confidence: 99%
“…Cys‐TATE (0.1 mmol) was synthesized on a solid support according to a published standard Fmoc‐based solid phase peptide synthesis approach on an Fmoc‐Thr(tBu)‐Wang resin as described elsewhere . For the chemical structure of the peptide and a schematic description of the coupling process, please see the Supporting Information S0.…”
Section: Methodsmentioning
confidence: 98%