X‐ray Structures and Feasibility Assessment of CLK2 Inhibitors for Phelan–McDermid Syndrome

Kallen, Joerg; Bergsdorf, Christian; Arnaud, Bertrand; Bernhard, Mario; Brichet, Murielle; Cobos-Correa, Amanda; Elhajouji, Azeddine; Freuler, Felix; Galimberti, Ivan; Guibourdenche, C.; Haenni, Simon; Holzinger, Sandra; Hunziker, Johannes C.; Izaac, Aude; Kaufmann, Markus; Leder, Lukas; Martus, Hans-Joerg; Matt, Peter; Polyakov, Valery; Roethlisberger, Patrik; Roma, Guglielmo; Stiefl, Nikolaus; Uteng, Marianne; Lerchner, Andreas

doi:10.1002/cmdc.201800344

Cited by 24 publications

(56 citation statements)

References 23 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Table 2 contains the published values obtained in primary biochemical assays; however, for their direct comparison it is important to keep in mind that these data were often obtained from various sources/assays or from the same (similar) assay but under unequal conditions (e.g., using different concentrations of ATP). On the other hand, some studies report a direct comparison of several (usually two or three) inhibitors from different classes/publications, profiling them in the same assay [ 76 , 133 , 134 , 135 , 136 ].…”

Section: Small-molecule Clk Inhibitorsmentioning

confidence: 99%

See 1 more Smart Citation

Cdc-Like Kinases (CLKs): Biology, Chemical Probes, and Therapeutic Potential

Moyano

Němec

Paruch

2020

IJMS

View full text Add to dashboard Cite

Protein kinases represent a very pharmacologically attractive class of targets; however, some members of the family still remain rather unexplored. The biology and therapeutic potential of cdc-like kinases (CLKs) have been explored mainly over the last decade and the first CLK inhibitor, compound SM08502, entered clinical trials only recently. This review summarizes the biological roles and therapeutic potential of CLKs and their heretofore published small-molecule inhibitors, with a focus on the compounds’ potential to be utilized as quality chemical biology probes.

show abstract

Section: Small-molecule Clk Inhibitorsmentioning

confidence: 99%

“…CX-4945 ( Figure 10 ) has been primarily reported, marketed, and used as a highly selective and potent inhibitor of CK2 since 2011 [ 140 ]. However, CX-4945 strongly inhibits also CLKs and DYRK1A [ 133 ]. In addition, it interacts significantly with other kinases such as HIPKs or PIM kinases [ 133 , 139 ].…”

Section: Small-molecule Clk Inhibitorsmentioning

confidence: 99%

Cdc-Like Kinases (CLKs): Biology, Chemical Probes, and Therapeutic Potential

Moyano

Němec

Paruch

2020

IJMS

View full text Add to dashboard Cite

show abstract

“…Protein names are provided alongside its kinase group. Locations for αC‐β4 loops are provided: 93–135 in scCKA1 (PDB ID: 4jr7), 147–160 in SRPK2 (PDB ID: 2x7g), 253–262 in HIPK2 (PDB ID: 6p5s), 212–222 in CLK3 (PDB ID: 6fyr), 92–112 in VRK1 (PDB ID: 6bru), 95–106 in Gilgamesh (PDB ID: 4 nt4), and 322–340 in Rhoptry kinase (PDB ID: 3byv) . More information about these structures can be found in Table .…”

Section: Conservation and Variation In The αC‐β4 Loop Of Protein Kinasesmentioning

confidence: 99%

Emerging roles of the αC‐β4 loop in protein kinase structure, function, evolution, and disease

2020

View full text Add to dashboard Cite

The faithful propagation of cellular signals in most organisms relies on the coordinated functions of a large family of protein kinases that share a conserved catalytic domain. The catalytic domain is a dynamic scaffold that undergoes large conformational changes upon activation. Most of these conformational changes, such as movement of the regulatory αC-helix from an "out"to "in" conformation, hinge on a conserved, but understudied, loop termed the αC-β4 loop, which mediates conserved interactions to tether flexible structural elements to the kinase core. We previously showed that the αC-β4 loop is a unique feature of eukaryotic protein kinases. Here, we review the emerging roles of this loop in kinase structure, function, regulation, and diseases. Through a kinome-wide analysis, we define the boundaries of the loop for the first time and show that sequence and structural variation in the loop correlate with conformational and regulatory variation. Many recurrent disease mutations map to the αC-β4 loop and contribute to drug resistance and abnormal kinase activation by relieving key auto-inhibitory interactions associated with αC-helix and interlobe movement. The αC-β4 loop is a hotspot for post-translational modifications, protein-protein interaction, and Hsp90 mediated folding. Our kinome-wide analysis provides insights for hypothesis-driven characterization of understudied kinases and the development of allosteric protein kinase inhibitors.

show abstract

“…We tested a panel of inhibitors known to act on HIPK2 and a broad range of CMGC family kinases (58 -60). Under the conditions tested, HIPK2 crystallized in the presence of the CK2␣ ATP-competitive inhibitor CX-4945, previously shown to inhibit HIPK2, HIPK3, and a number of other kinases (62,76), and crystallized in complex with CK2␣, the proviral integration site for Moloney murine leukemia virus-1 kinase (Pim1), and CLK2-4 kinases (63)(64)(65).…”

Section: Overall Structure Of the Hipk2 Kinase Domainmentioning

confidence: 99%

“…In HIPK2, the ATP-pocket is formed by Leu 205 , Val 213 , Ala 226 , Val 261 , Phe 277 , Met 279 , Leu 280 , Met 331 , and Ile 345 . The naphthyridine ring of CX-4945 is tightly bound by the R-spine residues Previous crystal structures have determined the mode of CX-4945 binding to CK2␣ (63,76), Pim1 (64), and CLK2-4 (65). The core hydrophobic active-site residues are well-conserved between HIPK2, CK2␣, and the CLKs, whereas the sequence of the Pim1 hinge region is different at several posi- EDITORS' PICK: Structure of HIPK2 bound to CX-4945 tions, which make contact with CX-4945 ( Fig.…”

Section: Binding Of Cx-4945 To the Atp Site Of Hipk2mentioning

confidence: 99%