Structure–Activity Relationship of 3-Methylcytidine-5′-α,β-methylenediphosphates as CD73 Inhibitors

Scortichini, Mirko; Idris, Riham M.; Moschütz, Susanne; Keim, Antje; Salmaso, Veronica; Dobelmann, Clemens; Oliva, Paola; Losenkova, Karolina; Irjala, Heikki; Vaittinen, Samuli; Sandholm, Jouko; Yegutkin, Gennady G.; Sträter, Norbert; Junker, Anna; Müller, Christian

doi:10.1021/acs.jmedchem.1c01852

Cited by 10 publications

(8 citation statements)

References 77 publications

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“…1 H NMR (400 MHz, chloroformd) δ 4.31 (q, J = 7.1 Hz, 4H), 1.32 (t, J = 7.1 Hz, 6H). (20). Compound 18 (1.20 g, 4.33 mmol) was dissolved with 200 mL of toluene, then 19 (1.20 g, 6.49 mmol) and rhodium acetate dimer (0.096 g, 0.22 mmol) were added.…”

Section: Methodsmentioning

confidence: 99%

“…19 Since the dephosphorylation products of the above nucleoside inhibitors are derivatives of adenosine, the strategy of MRS4620 ( 6) is to replace adenine with methylcytosine, thereby reducing the possibility of activating the adenosine pathway. 20 Therefore, non-nucleoside inhibitors have more significance in pharmacology. Among them, benzotriazole analogue 7b cocrystallized with CD73 in the closed conformation exhibits a competitive binding mode.…”

Section: Introductionmentioning

confidence: 99%

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Discovery of Novel Non-Nucleoside Inhibitors Interacting with Dizinc Ions of CD73

Shi,

Chang,

Wang

et al. 2024

J. Med. Chem.

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High extracellular concentrations of adenosine triphosphate (ATP) in the tumor microenvironment generate adenosine by sequential dephosphorylation of CD39 and CD73, resulting in potent immunosuppression to inhibit T cell and natural killer (NK) cell function. CD73, as the determining enzyme for adenosine production, has been shown to correlate with poor clinical tumor prognosis. Conventional inhibitors as analogues of adenosine 5′-monophosphate (AMP) may have a risk of further metabolism to adenosine analogues. Here, we report a new series of malonic acid non-nucleoside inhibitors coordinating with zinc ions of CD73. Compound 12f was found to be a superior CD73 inhibitor (IC 50 = 60 nM) by structural optimization, and its pharmacokinetic properties were investigated. In mouse tumor models, compound 12f showed excellent efficacy and reversal of immunosuppression in combination with chemotherapeutic agents or checkpoint inhibitors, suggesting that it deserves further development as a novel CD73 inhibitor.

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Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Discovery of Novel Non-Nucleoside Inhibitors Interacting with Dizinc Ions of CD73

Shi,

Chang,

Wang

et al. 2024

J. Med. Chem.

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“…Adenosine generated by overexpressed h-ecto-5′-NT accumulates in the tumor microenvironment, where it activates immunosuppressive pathways that favor the development of neoplasia. − Accumulated adenosine can also regulate angiogenesis and proliferation, migration, differentiation, and apoptosis of parenchymal cancer cells, contributing to tumor progression and metastasis. − The effects of h-ecto-5′-NT overexpression in tumorigenesis and its role in tumor immune escape and tumor metastasis have been shown in vivo . − In addition to its participation in tumor progression, h-ecto-5′-NT plays a central role in the course of several pathophysiological events and diseases, including inflammation and autoimmune, infectious, and neurological diseases. , Therefore, h-ecto-5′-NT has been recognized as a well-established biological target for cancer therapy and for the treatment of many other diseases. Several h-ecto-5′-NT inhibitors have been reported so far, ,− some of which are currently being tested in clinical trials. , Nevertheless, as discussed in the literature, ,, many of the known inhibitors have physicochemical and/or pharmacological characteristics that limit their applicability as drug candidates, such as low inhibitory potency, poor water solubility, and lack of selectivity. For this reason, considerable efforts have been made by the scientific community and the pharmaceutical industry to search for novel h-ecto-5′-NT inhibitors …”

Section: Introductionmentioning

confidence: 99%

“…The elucidation of the h-ecto-5′-NT 3D structure by X-ray crystallography (resolution values ranging from 1.05 to 2.90 Å), ,,,,,,,,− in its open and closed conformations (Figure ), has provided the basis for structure-based design of inhibitors of this target enzyme . The available crystal structures reveal that h-ecto-5′-NT consists of a homodimer, , in contrast to the monomeric bacterial 5′-nucleotidases. , As shown in Figure , each dimer subunit is formed by two structural domains: the C-terminal domain, which contains the substrate binding site, and the N-terminal domain, which contains the binding sites of two zinc ions that are essential for catalysis. , The dimerization interface is formed by C-terminal domain residues of each dimer subunit, which interact via a network of hydrogen-bonds and hydrophobic interactions .…”

Section: Introductionmentioning

confidence: 99%

Molecular Dynamics Simulations of the Human Ecto-5′-Nucleotidase (h-ecto-5′-NT, CD73): Insights into Protein Flexibility and Binding Site Dynamics

Viviani

Kokh

Wade

et al. 2023

J. Chem. Inf. Model.

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Human ecto-5′-nucleotidase (h-ecto-5′-NT, CD73) is a homodimeric Zn 2+ -binding metallophosphoesterase that hydrolyzes adenosine 5′-monophosphate (5′-AMP) to adenosine and phosphate. h-Ecto-5′-NT is a key enzyme in purinergic signaling pathways and has been recognized as a promising biological target for several diseases, including cancer and inflammatory, infectious, and autoimmune diseases. Despite its importance as a biological target, little is known about h-ecto-5′-NT dynamics, which poses a considerable challenge to the design of inhibitors of this target enzyme. Here, to explore h-ecto-5′-NT flexibility, all-atom unbiased molecular dynamics (MD) simulations were performed. Remarkable differences in the dynamics of the open (catalytically inactive) and closed (catalytically active) conformations of the apo-h-ecto-5′-NT were observed during the simulations, and the nucleotide analogue inhibitor AMPCP was shown to stabilize the protein structure in the closed conformation. Our results suggest that the large and complex domain motion that enables the h-ecto-5′-NT open/closed conformational switch is slow, and therefore, it could not be completely captured within the time scale of our simulations. Nonetheless, we were able to explore the faster dynamics of the h-ecto-5′-NT substrate binding site, which is mainly located at the C-terminal domain and well conserved among the protein's open and closed conformations. Using the TRAPP ("Transient Pockets in Proteins") approach, we identified transient subpockets close to the substrate binding site. Finally, conformational states of the substrate binding site with higher druggability scores than the crystal structure were identified. In summary, our study provides valuable insights into h-ecto-5′-NT structural flexibility, which can guide the structure-based design of novel h-ecto-5′-NT inhibitors.

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“…34,35 In addition, molecular dynamics simulation has been widely employed to study the binding mode of potential inhibitors in the active site of the target for designing new compounds. 36,37 These studies provide valuable clues for drug design, while the MM MD simulations are usually used to capture static binding for the target ligand in the binding site. The inhibitor delivery process always involves its recognition and delivery, which may also influence its efficacy.…”

Section: Introductionmentioning

confidence: 99%

Combination of multiple methods and views for recognition, transportation, and structure-guided modification of lysine-specific demethylase phenylcyclopropylamine inhibitor

Liu

Zhang

She

et al. 2022

Phys. Chem. Chem. Phys.

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Structure–Activity Relationship of 3-Methylcytidine-5′-α,β-methylenediphosphates as CD73 Inhibitors

Cited by 10 publications

References 77 publications

Discovery of Novel Non-Nucleoside Inhibitors Interacting with Dizinc Ions of CD73

Discovery of Novel Non-Nucleoside Inhibitors Interacting with Dizinc Ions of CD73

Molecular Dynamics Simulations of the Human Ecto-5′-Nucleotidase (h-ecto-5′-NT, CD73): Insights into Protein Flexibility and Binding Site Dynamics

Combination of multiple methods and views for recognition, transportation, and structure-guided modification of lysine-specific demethylase phenylcyclopropylamine inhibitor

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