Analysis of progress and challenges for various patterns of c-MET-targeted molecular imaging: a systematic review

Han, Zhaoguo; Wu, Yongyi; Wang, Kai; Xiao, Yadi; Cheng, Zhen; Sun, Xilin; Shen, Baogen

doi:10.1186/s13550-017-0286-z

Cited by 16 publications

(18 citation statements)

References 75 publications

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“…Over decades, c‐Met has increasingly been utilized as a biomarker for molecular imaging. Various c‐Met‐targeted imaging agents have been developed based on the HGF ligand, antibodies, peptides, genetically encoded proteins, anticalins, and small molecules (Han et al., ). Evidently, whether it is a HGF ligand, antibody, peptide, or small molecule has unique advantages and disadvantages.…”

Section: Discussionmentioning

confidence: 99%

Preliminary application of micro‐SPECT/CT imaging by ^99mTc‐tricine‐EDDA‐HYNIC‐c‐Met for non‐small‐cell lung cancer

Zhang

Ли

et al. 2018

Chem Biol Drug Des

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Objective A novel 99mTc‐tricine‐EDDA‐Hynic‐c‐Met molecular probe was synthetized, and nude mice models of human non‐small‐cell lung cancer (NSCLC) were established in order to preliminarily investigate that whether the molecular probe can be used to screen c‐Met inhibitor for targeted drug therapy in NSCLC. Methods With Hynic as the chelating agent, 99mTcO4‐labeled c‐Met receptor was used to synthetize 99mTc‐tricine‐EDDA‐HYNIC‐c‐Met. Two nude mice successfully transplanted with H1993 tumor and two nude mice transplanted with H292 tumor were injected with 99mTc‐tricine‐EDDA‐HYNIC‐c‐Met through the tail vein. After 2 and 4 hr, micro‐SPECT/CT imaging was performed. Results micro‐SPECT/CT imaging of nude mice transplanted with H1993 and H292 tumors using 99mTc‐tricine‐EDDA‐HYNIC‐c‐Met showed that uptake of 99mTc‐tricine‐EDDA‐HYNIC‐c‐Met was high in H1993 tumor, while it was mild in H292 tumor both at 2 and 4 hr postinjection. Semiquantitative analysis of the ratio of radioactivity intensity at tumor site to radioactivity intensity of adjacent muscles (T/N value) showed that the average T/N value of H1993 and H292 tumors at 2 hr was 3.90 and 2.85, while it was 4.88 and 2.36 at 4 hr. Conclusion micro‐SPECT/CT imaging through 99mTc‐tricine‐EDDA‐HYNIC‐c‐Met can be used to screen c‐Met indicators of NSCLC in H1993 nude mice models for targeted drug therapy.

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Section: Discussionmentioning

confidence: 99%

Preliminary application of micro‐SPECT/CT imaging by ^99mTc‐tricine‐EDDA‐HYNIC‐c‐Met for non‐small‐cell lung cancer

Zhang

Ли

et al. 2018

Chem Biol Drug Des

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“…Due to a limited number of validated MET mAbs that work in formalin-fixed and paraffin embedded biopsy samples, immunohistochemical evaluation of MET expression is a challenge [ 282 ]. Since HGF has been recognized to have a high binding affinity and specificity to MET, initial studies on targeted molecular imaging of MET were therefore mainly based on HGF ligands [ 283 ]. The recombinant human HGF was [ 64 Cu]-labeled ([ 64 Cu]Cu-rh-HGF) and PET imaging revealed specific and prominent uptake of the radiopharmaceutical in MET positive U87MG GB tumors [ 284 ].…”

Section: Receptor Tyrosine Kinase Inhibitors (Rtkis) For Gb Therapymentioning

confidence: 99%

“…The recombinant human HGF was [ 64 Cu]-labeled ([ 64 Cu]Cu-rh-HGF) and PET imaging revealed specific and prominent uptake of the radiopharmaceutical in MET positive U87MG GB tumors [ 284 ]. One concern for these radiopharmaceuticals based on the HGF ligand is their potential to stimulate tumor growth by activating c-met and competition with the endogenous ligand, hindering clinical translation [ 27 , 283 , 284 ]. Hence, the mAb-based PET radiopharmaceuticals [ 89 Zr]Zr-onartuzumab and [ 76 Br]Br-onartuzumab were developed that specifically target MET in vitro and in vivo.…”

Section: Receptor Tyrosine Kinase Inhibitors (Rtkis) For Gb Therapymentioning

confidence: 99%

Novel Receptor Tyrosine Kinase Pathway Inhibitors for Targeted Radionuclide Therapy of Glioblastoma

et al. 2021

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Glioblastoma (GB) remains the most fatal brain tumor characterized by a high infiltration rate and treatment resistance. Overexpression and/or mutation of receptor tyrosine kinases is common in GB, which subsequently leads to the activation of many downstream pathways that have a critical impact on tumor progression and therapy resistance. Therefore, receptor tyrosine kinase inhibitors (RTKIs) have been investigated to improve the dismal prognosis of GB in an effort to evolve into a personalized targeted therapy strategy with a better treatment outcome. Numerous RTKIs have been approved in the clinic and several radiopharmaceuticals are part of (pre)clinical trials as a non-invasive method to identify patients who could benefit from RTKI. The latter opens up the scope for theranostic applications. In this review, the present status of RTKIs for the treatment, nuclear imaging and targeted radionuclide therapy of GB is presented. The focus will be on seven tyrosine kinase receptors, based on their central role in GB: EGFR, VEGFR, MET, PDGFR, FGFR, Eph receptor and IGF1R. Finally, by way of analyzing structural and physiological characteristics of the TKIs with promising clinical trial results, four small molecule RTKIs were selected based on their potential to become new therapeutic GB radiopharmaceuticals.

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“…11 Several strategies to image MET expression in vivo has been explored, predominantly using peptides or monoclonal antibodies. 13 For radiotracers based on small molecular weight compounds targeting the intracellular domain of MET, there is so far only one report. 14 As therapeutic PKIs bind intracellularly, radiotracers binding to the same active site may be important to properly asses target expression and engagement.…”

Section: Introductionmentioning

confidence: 99%

Synthesis and Preclinical Evaluation of [18F]PF04217903, a Selective MET PET Tracer

Lien¹,

Hauge²,

Nuruddin³

et al. 2020

Preprint

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The tyrosine kinase MET (hepatocyte growth factor receptor) is abnormally activated in a wide range of cancers and is often correlated with a poor prognosis. Precision medicine with positron emission tomography (PET) can potentially aid in the assessment of tumor biochemistry and heterogeneity, which can prompt the selection of the most effective therapeutic regimes. The selective MET inhibitor PF04217903 (1) formed the basis for a bioisosteric replacement to the deoxyfluorinated analogue [18F]2, intended as a PET tracer for MET. [18F]2 could be synthesized with a “hydrous fluoroethylation” protocol in 6.3 ± 2.6% radiochemical yield and a molar activity of >50 GBq/µmol. In vitro autoradiography indicated that [18F]2 specifically binds to MET in PC3 tumor tissue, and in vivo biodistribution in mice showed predominantly a hepatobiliary excretion along with a low retention of radiotracer in other organs.

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Analysis of progress and challenges for various patterns of c-MET-targeted molecular imaging: a systematic review

Cited by 16 publications

References 75 publications

Preliminary application of micro‐SPECT/CT imaging by ^99mTc‐tricine‐EDDA‐HYNIC‐c‐Met for non‐small‐cell lung cancer

Preliminary application of micro‐SPECT/CT imaging by ^99mTc‐tricine‐EDDA‐HYNIC‐c‐Met for non‐small‐cell lung cancer

Novel Receptor Tyrosine Kinase Pathway Inhibitors for Targeted Radionuclide Therapy of Glioblastoma

Synthesis and Preclinical Evaluation of [18F]PF04217903, a Selective MET PET Tracer

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Analysis of progress and challenges for various patterns of c-MET-targeted molecular imaging: a systematic review

Cited by 16 publications

References 75 publications

Preliminary application of micro‐SPECT/CT imaging by 99mTc‐tricine‐EDDA‐HYNIC‐c‐Met for non‐small‐cell lung cancer

Preliminary application of micro‐SPECT/CT imaging by 99mTc‐tricine‐EDDA‐HYNIC‐c‐Met for non‐small‐cell lung cancer

Novel Receptor Tyrosine Kinase Pathway Inhibitors for Targeted Radionuclide Therapy of Glioblastoma

Synthesis and Preclinical Evaluation of [18F]PF04217903, a Selective MET PET Tracer

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Preliminary application of micro‐SPECT/CT imaging by ^99mTc‐tricine‐EDDA‐HYNIC‐c‐Met for non‐small‐cell lung cancer

Preliminary application of micro‐SPECT/CT imaging by ^99mTc‐tricine‐EDDA‐HYNIC‐c‐Met for non‐small‐cell lung cancer