Synthesis and Evaluation of New Trivalent Ligands for Hepatocyte Targeting via the Asialoglycoprotein Receptor

Reshitko, Galina S; Yamansarov, Emil Yu.; Evteev, Sergei A; Lopatukhina, Elena V.; Shkil, Dmitry O.; Saltykova, Irina V.; Lopukhov, Anton V; Ковалев, С. В.; Лобов, А. Н.; Kislyakov, Ivan V; Burenina, Olga Y.; Klyachko, Natalia L.; Garanina, Anastasiia S.; Донцова, О. А.; Ivanenkov, Yan A.; Erofeev, Alexander; Gorelkin, Peter; Белоглазкина, Е. К.; Majouga, Alexander G.

doi:10.1021/acs.bioconjchem.0c00202

Cited by 13 publications

(7 citation statements)

References 54 publications

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“…Therefore, the contribution of this ASGPR-specific mechanism is highly significant in the case of hepatocytes and allows faster internalization of conjugate 9 in line with the literature data reporting that effective cellular uptake of ASGPR-targeted compounds occurs even within the first 10 min of treatment followed by further slow accumulation up to 30–40 min . The specificity of GalNAc-mediated cellular uptake was proved in parallel experiments in the presence of high concentrations of competing monovalent (GalNAc) or trivalent (GalNAc) 3 ligands (10 mM, 10 6 to 10 4 molar excess), which efficiently inhibit internalization of compound 9 (Figure ) but not compound 8 in HepG2 (compare Figure S7a,b, middle and bottom panels, Supporting Information). Such high inhibiting concentrations of GalNAc were reported previously .…”

Section: Microscopy Experimentssupporting

confidence: 87%

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New Small-Molecule Glycoconjugates of Docetaxel and GalNAc for Targeted Delivery to Hepatocellular Carcinoma

et al. 2020

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In this work, we have developed covalent and low molecular weight docetaxel delivery systems based on conjugation with N-acetyl-d-galactosamine and studied their properties related to hepatocellular carcinoma cells. The resulting glycoconjugates have an excellent affinity to the asialoglycoprotein receptor (ASGPR) in the nanomolar range of concentrations and a high cytotoxicity level comparable to docetaxel. Likewise, we observed the 21–75-fold increase in water solubility in comparison with parent docetaxel and prodrug lability to intracellular conditions with half-life values from 25.5 to 42 h. We also found that the trivalent conjugate possessed selective toxicity against hepatoma cells vs control cell lines (20–35 times). The absence of such selectivity in the case of monovalent conjugates indicates the effect of ligand valency. Specific ASGPR-mediated cellular uptake of conjugates was proved in vitro using fluorescent-labeled analogues. In addition, we showed an enhanced generation of reactive oxygen species in the HepG2 cells, which could be inhibited by the natural ligand of ASGPR. Overall, the obtained results highlight the potential of ASGPR-directed cytostatic taxane drugs for selective therapy of hepatocellular carcinoma.

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Section: Microscopy Experimentssupporting

confidence: 87%

“…Representative fluorescence (top) and bright-field (bottom) microscopy images of HepG2 cells treated with 1 μM of compound 9 either alone or in the presence of 10 mM of ASGPR-blocking ligands: monovalent GalNAc or trivalent (GalNAc) 3 . (For details see Supporting Information.…”

Section: Microscopy Experimentsmentioning

confidence: 99%

New Small-Molecule Glycoconjugates of Docetaxel and GalNAc for Targeted Delivery to Hepatocellular Carcinoma

et al. 2020

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“…In other words, the hepatocyte-targeting capacity followed the W-1-5 (monoga-lactose) < W-2-9 (digalactose) < W-3-8 (trigalactose) order, obeying the rules of the galactose-recognition cluster effect toward ASGPR. Interestingly, it was reported that the galactose-modified bis-fluorophore conjugate, 24 the galactosamine-modified betulin conjugate, 25 and the trivalent galactosamine-modified Cy5 dye 26 showed a similar hepatocytetargeted tendency, also confirming the reliability of our results.…”

Section: ■ Introductionsupporting

confidence: 90%

Development of Asialoglycoprotein-Mediated Hepatocyte-Targeting Antitumor Prodrugs Triggered by Glutathione

Wang

Liu

et al. 2021

J. Med. Chem.

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One antitumor β-elemene derivative W-105 and three novel hepatocyte-targeting prodrugs (W-1-5, W-2-9, and W-3-8) were designed and synthesized. W-105 (IC 50 6.107 μM) could cause cell apoptosis through upregulating the activity of caspase-3. The hepatocytetargeting capacities of the aimed compounds followed the W-105 (parent compound) < W-1-5 (monodentate-galactose) < W-2-9 (bidentategalactose) < W-3-8 (tridentate-galactose) order, which is attributed to the excellent affinity of the galactose ligand to ASGPR and the galactosecluster recognition effect. Furthermore, prodrugs W-3-8 exhibited good antitumor activity and low toxic side effects. The liquid chromatographymass spectrometry (LC-MS) assays revealed that prodrugs (W-1-5, W-2-9, and W-3-8) could release the antitumor pharmacophore in the presence of GSH (mimic the condition of the tumor cell) and maintain the low-toxic structures in the absence of GSH (mimic the condition of the normal cell). The release mechanisms of prodrugs were also proposed. Overall, these prodrugs developed in this study had potential in the treatment of liver cancer.

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“…Initially, two azide derivatives of N-acetyl-D-galactosamine 1 and 2 and also N-acetyl-D-glucosamine (GlcNAc) azide 3 were synthesized (Figure 1). We used β-azido glycosylation (FeCl 3 / TMSN 3 ) 32 or β-O-glycosylation (TMSOTf/2-azidoethanol) 33 reactions of β-D-galactosamine pentaacetate according to the previously published procedures, followed by alcoholysis of the O-acetyl groups by MeONa/MeOH. Esters 4−6 containing a residual 5-hexynoic acid moiety as a linker (Scheme 1) were synthesized in the second step.…”

Section: ■ Results and Discussionmentioning

confidence: 99%

Discovery of Bivalent GalNAc-Conjugated Betulin as a Potent ASGPR-Directed Agent against Hepatocellular Carcinoma

et al. 2021

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Herein, we describe the design, synthesis, and biological evaluation of novel betulin and N-acetyl-d-galactosamine (GalNAc) glycoconjugates and suggest them as targeted agents against hepatocellular carcinoma. We prepared six conjugates derived via the C-3 and C-28 positions of betulin with one or two saccharide ligands. These molecules demonstrate high affinity to the asialoglycoprotein receptor (ASGPR) of hepatocytes assessed by in silico modeling and surface plasmon resonance tests. Cytotoxicity studies in vitro revealed a bivalent conjugate with moderate activity, selectivity of action, and cytostatic properties against hepatocellular carcinoma cells HepG2. An additional investigation confirmed the specific engagement with HepG2 cells by the enhanced generation of reactive oxygen species. Stability tests demonstrated its lability to acidic media and to intracellular enzymes. Therefore, the selected bivalent conjugate represents a new potential agent targeted against hepatocellular carcinoma. Further extensive studies of the cellular uptake in vitro and the real-time microdistribution in the murine liver in vivo for fluorescent dye-labeled analogue showed its selective internalization into hepatocytes due to the presence of GalNAc ligand in comparison with reference compounds. The betulin and GalNAc glycoconjugates can therefore be considered as a new strategy for developing therapeutic agents based on natural triterpenoids.

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Synthesis and Evaluation of New Trivalent Ligands for Hepatocyte Targeting via the Asialoglycoprotein Receptor

Cited by 13 publications

References 54 publications

New Small-Molecule Glycoconjugates of Docetaxel and GalNAc for Targeted Delivery to Hepatocellular Carcinoma

New Small-Molecule Glycoconjugates of Docetaxel and GalNAc for Targeted Delivery to Hepatocellular Carcinoma

Development of Asialoglycoprotein-Mediated Hepatocyte-Targeting Antitumor Prodrugs Triggered by Glutathione

Discovery of Bivalent GalNAc-Conjugated Betulin as a Potent ASGPR-Directed Agent against Hepatocellular Carcinoma

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