Comparative Efficacy of CK2 Inhibitors CX-4945 and SGC-CK2-2 on CK2 Signaling
Francesca Noventa, Rina Venerando, Valentina Bosello Travain, Mauro Salvi

TL;DR
This study compares two CK2 inhibitors, CX-4945 and SGC-CK2-2, to understand their effects on cancer cell signaling and viability.
Contribution
The study reveals that partial CK2 inhibition does not significantly impact cell viability, while near-complete inhibition leads to cell death.
Findings
CK2 phospho-substrates show differential sensitivity to CX-4945 and SGC-CK2-2.
Partial CK2 inhibition does not significantly affect cell viability.
Near-complete suppression of CK2 signaling leads to cell death induction.
Abstract
The pleiotropic kinase CK2 plays a crucial role in numerous cellular processes and is frequently deregulated in human diseases. Specifically, elevated CK2 expression and/or activity have been observed in human cancers, thus rendering its inhibition a promising pharmacological strategy for treating malignancies. The most widely used CK2 inhibitor, CX-4945 (Silmitarsetib), was developed by Cylene Pharmaceuticals in 2010. It has been tested in clinical trials for various cancers and, more recently, as a potential therapy for COVID-19 patients. However, it has been demonstrated that CX-4945’s specificity is limited, as CX-4945 also inhibits other kinases beyond CK2. A recently developed derivative of CX-4945, SGC-CK2-2, has demonstrated enhanced specificity compared with CX-4945, albeit with reduced potency. In this study, we conducted a detailed analysis of the effects of SGC-CK2-2 in two…
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Taxonomy
TopicsChronic Myeloid Leukemia Treatments · Drug Transport and Resistance Mechanisms · Protein Kinase Regulation and GTPase Signaling
