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5 results on '"Ricardo A. M. Serafim"'

2. Chemical probes for understudied kinases: challenges and opportunities

Author

William J. Zuercher, Ricardo A. M. Serafim, Matthias Gehringer, Stefan Laufer, and Jonathan M. Elkins

Subjects
Kinase, medicine.drug_class, Chemistry, Computational biology, Protein kinase inhibitor, Molecular Probes, Drug Discovery, medicine, Animals, Humans, Molecular Medicine, Kinome, Protein Kinase Inhibitors, Protein Kinases
Abstract

Over 20 years after the approval of the first-in-class protein kinase inhibitor imatinib, the biological function of a significant fraction of the human kinome remains poorly understood while most research continues to be focused on few well-validated targets. Given the strong genetic evidence for involvement of many kinases in health and disease, the understudied fraction of the kinome holds a large and unexplored potential for future therapies. Specific chemical probes are indispensable tools to interrogate biology enabling proper preclinical validation of novel kinase targets. In this Perspective, we highlight recent case studies illustrating the development of high-quality chemical probes for less-studied kinases and their application in target validation. We spotlight emerging techniques and approaches employed in the generation of chemical probes for protein kinases and beyond and discuss the associated challenges and opportunities.

Published
2021
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3. Discovery of a Potent and Highly Isoform-Selective Inhibitor of the Neglected Ribosomal Protein S6 Kinase Beta 2 (S6K2)

Author

Stefan Laufer, Mark Kudolo, Ricardo A. M. Serafim, Martin Schröder, Apirat Chaikuad, Valentin Wydra, Stefan Gerstenecker, Stefan Knapp, Martin P. Schwalm, Lisa Haarer, and Matthias Gehringer

Subjects
Gene isoform, Cancer Research, protein kinases, Kinase, Chemistry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, P70-S6 Kinase 1, Glutathione, S6K2, p70S6Kb, Small molecule, Article, chemistry.chemical_compound, RPS6KB2, chemical probes, Oncology, Biochemistry, Fibroblast growth factor receptor, Ribosomal protein s6, covalent inhibitors, p70S6K2, RC254-282, Cysteine
Abstract

Simple Summary The two human p70 ribosomal S6 kinases, S6K1 and S6K2, have been associated with a variety of cellular processes and human pathologies, especially cancer. Thus far, only S6K1 was thoroughly studied and selectively addressed by small molecule inhibitors. Despite growing evidence suggesting S6K2 as a promising anticancer target, this isoform has been severely neglected, which can partly be attributed to the lack of isoform-selective inhibitors to study its function. By exploiting a cysteine residue exclusive to S6K2, we were able to generate the first known isoform-selective S6K2 inhibitor. Besides its excellent selectivity against S6K1 and other human kinases, the compound showed weak intrinsic reactivity and promising in vitro metabolic stability. Our proof-of-concept study provides a basis for the development of high quality S6K2 chemical probes to validate this kinase as a target for therapeutic interventions. Abstract The ribosomal protein S6 kinase beta 2 (S6K2) is thought to play an important role in malignant cell proliferation, but is understudied compared to its closely related homolog S6 kinase beta 1 (S6K1). To better understand the biological function of S6K2, chemical probes are needed, but the high similarity between S6K2 and S6K1 makes it challenging to selectively address S6K2 with small molecules. We were able to design the first potent and highly isoform-specific S6K2 inhibitor from a known S6K1-selective inhibitor, which was merged with a covalent inhibitor engaging a cysteine located in the hinge region in the fibroblast growth factor receptor kinase (FGFR) 4 via a nucleophilic aromatic substitution (SNAr) reaction. The title compound shows a high selectivity over kinases with an equivalently positioned cysteine, as well as in a larger kinase panel. A good stability towards glutathione and Nα-acetyl lysine indicates a non-promiscuous reactivity pattern. Thus, the title compound represents an important step towards a high-quality chemical probe to study S6K2-specific signaling.

Published
2021

4. N-(6-Chloro-3-nitropyridin-2-yl)-5-(1-methyl-1H-pyrazol-4-yl)isoquinolin-3-amine

Author

Ricardo A. M. Serafim, Matthias Gehringer, Stanislav Andreev, Teodor Dimitrov, Stefan Gerstenecker, Valentin Wydra, Dieter Schollmeyer, and Stefan Laufer

Subjects
Imine, nucleophilic aromatic substitution, Infrared spectroscopy, 01 natural sciences, Biochemistry, Medicinal chemistry, 03 medical and health sciences, chemistry.chemical_compound, Buchwald–Hartwig arylamination, Nucleophilic aromatic substitution, Benzophenone, lcsh:Inorganic chemistry, Physical and Theoretical Chemistry, 030304 developmental biology, 0303 health sciences, 010405 organic chemistry, Chemistry, Organic Chemistry, Regioselectivity, Nuclear magnetic resonance spectroscopy, lcsh:QD146-197, 0104 chemical sciences, 3-nitropyridines, protein kinase inhibitors, covalent inhibitors, Amine gas treating, Two-dimensional nuclear magnetic resonance spectroscopy
Abstract

Here we describe the synthesis of N-(6-chloro-3-nitropyridin-2-yl)5-(1-methyl-1H-pyrazol-4-yl)isoquinolin-3-amine via a three-step procedure including a Buchwald–Hartwig arylamination with benzophenone imine and a highly regioselective nucleophilic aromatic substitution. The title compound was analyzed by nuclear magnetic resonance spectroscopy (1H, 13C, HSQC, HMBC, COSY, DEPT90 and NOESY), high resolution mass spectrometry (ESI-TOF-HRMS) and infrared spectroscopy (ATR-IR) and its structure was confirmed by single crystal X-ray diffraction. The inhibitory potency of the title compound was evaluated for selected kinases harboring a rare cysteine in the hinge region (MPS1, MAPKAPK2 and p70S6Kβ/S6K2).

Published
2021

5. Development of pyridine-based inhibitors for the human vaccinia-related kinases 1 and 2

Author

Jessica Takarada, Fulvia Di Pillo, Jonathan M. Elkins, A.S. Santiago, Ricardo A. M. Serafim, Fernando H. de Souza Gama, Hatylas Azevedo, Luiz A Dutra, C.R.W. Guimaraes, Opher Gileadi, A. Mascarello, Stanley Nunes Siqueira Vasconcelos, Caio V. dos Reis, Katlin B. Massirer, and Rafael M. Couñago

Subjects
pyridine, Letter, Cell division, Kinase, structure-based compound development, Substituent, Cellular functions, 3. Good health, chemistry.chemical_compound, chemistry, Biochemistry, Vaccinia-related kinases, Pyridine, kinase inhibitors, Vaccinia, difluorophenol
Abstract

Vaccinia-related kinases 1 and 2 (VRK1 and VRK2) are human Ser/Thr protein kinases associated with increased cell division and neurological disorders. Nevertheless, the cellular functions of these proteins are not fully understood. Despite their therapeutic potential, there are no inhibitors available for VRK1 or VRK2. We report here the discovery and elaboration of an aminopyridine scaffold as a basis for VRK1 and VRK2 inhibitors. The most potent compounds displayed KD values of 190 nM and 401 nM for VRK1 and VRK2, respectively. Differences in compound binding mode and substituent preferences between the two VRKs were identified by the series structure-activity relationship combined with the crystallographic analysis of key compounds. We expect that our results will serve as a starting point for the design of specific and potent inhibitors against each of the two VRKs based on a pyridine scaffold.

Published
2019

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