Hinge Binder Scaffold Hopping Identifies Potent Calcium/Calmodulin-Dependent Protein Kinase Kinase 2 (CAMKK2) Inhibitor Chemotypes

Eduful, Benjamin J.; O’Byrne, Sean; Temme, Louisa; Asquith, Christopher R. M.; Liang, Yue; Picado, Alfredo; Pilotte, Joseph; Hossain, Mohammad Anwar; Wells, Carrow; Zuercher, William J.; Catta-Preta, Carolina Moura Costa; Ramos, Priscila Zonzini; Santiago, André de S.; Counago, R.M.; Langendorf, Christopher G.; Nay, Kévin; Oakhill, Jonathan S.; Pulliam, Thomas L.; Lin, Chenchu; Awad, Dominik; Willson, Timothy M.; Frigo, Daniel E.; Scott, John W.; Drewry, David H.

doi:10.1021/acs.jmedchem.0c02274

Cited by 24 publications

(26 citation statements)

References 75 publications

(196 reference statements)

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“…Efforts are ongoing by multiple groups to develop new potent and selective CAMKK2 inhibitors with the goal to create a clinical-grade drug for use in patient trials [24,34-38]. The data presented here indicate that CAMKK2 inhibitors may have additional benefits for patients beyond what was initially anticipated.…”

Section: Discussionmentioning

confidence: 84%

“…However, prior reports suggesting roles for CAMKK2 in an AR-cell line in culture [33] and here in vivo indicate roles for CAMKK2 even in AR-indifferent prostate cancers. Given the lack of effective treatments for this highly aggressive cancer subtype, it suggests that the use of CAMKK2 inhibitors, which are currently in development [24,34-38], warrant further investigation for the treatment of NEPC.…”

Section: Discussionmentioning

confidence: 99%

“…Protein concentrations were measured using Bradford’s reagent. Immunoblotting was conducted as before [24].…”

Section: Methodsmentioning

confidence: 99%

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Systemic ablation of Camkk2 impairs metastatic colonization and improves insulin sensitivity in TRAMP mice: Evidence for cancer cell-extrinsic CAMKK2 functions in prostate cancer

Pulliam

Awad

Han

et al. 2022

Preprint

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Despite early studies linking calcium-calmodulin protein kinase kinase 2 (CAMKK2) to prostate cancer cell migration and invasion, the role of CAMKK2 in metastasis in vivo remains unclear. Moreover, while CAMKK2 is known to regulate systemic metabolism, whether CAMKK2′s effects on whole body metabolism would impact prostate cancer progression and/or related comorbidities is not known. Here, we demonstrate that germline ablation of Camkk2 slows, but does not stop, primary prostate tumorigenesis in the TRansgenic Adenocarcinoma Mouse Prostate (TRAMP) genetic mouse model. Consistent with prior epidemiological reports supporting a link between obesity and prostate cancer aggressiveness, TRAMP mice fed a high-fat diet exhibited a pronounced increase in the colonization of lung metastases. We demonstrated that this effect on metastatic spread was dependent on CAMKK2. Notably, diet-induced lung metastases exhibited a highly aggressive neuroendocrine phenotype. Concurrently, Camkk2 deletion improved insulin sensitivity in the same mice. Histological analyses revealed that cancer cells were smaller in the TRAMP;Camkk2-/- mice compared to TRAMP;Camkk2+/+ controls. Given the differences in circulating insulin levels, a known regulator of cell growth, we hypothesized that systemic CAMKK2 could promote prostate cancer cell growth and disease progression in part through cancer cell-extrinsic mechanisms. Accordingly, host deletion of Camkk2 impaired the growth of syngeneic murine prostate tumors in vivo, confirming nonautonomous roles for CAMKK2 in prostate cancer. Cancer cell size and mTOR signaling was diminished in tumors propagated in Camkk2-null mice. Together, these data indicate that, in addition to cancer cell-intrinsic roles, CAMKK2 promotes prostate cancer progression via tumor-extrinsic mechanisms. Further, we propose that CAMKK2 inhibition may also help combat common metabolic comorbidities in men with advanced prostate cancer.

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Section: Discussionmentioning

confidence: 84%

Section: Discussionmentioning

confidence: 99%

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Systemic ablation of Camkk2 impairs metastatic colonization and improves insulin sensitivity in TRAMP mice: Evidence for cancer cell-extrinsic CAMKK2 functions in prostate cancer

Pulliam

Awad

Han

et al. 2022

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

“…Pieces of mouse brains (specifically cerebellum) were resected and homogenized using a handheld homogenizer in 1 mL ice-cold RIPA buffer and agitated at 4 °C for 1 h. Protein concentrations were measured using Bradford’s reagent (Protein Assay Dye Reagent Concentrate, Cat #5000006; Bio-Rad Laboratories, Hercules, CA, USA). Immunoblotting was conducted as before [ 27 ].…”

Section: Methodsmentioning

confidence: 99%

Systemic Ablation of Camkk2 Impairs Metastatic Colonization and Improves Insulin Sensitivity in TRAMP Mice: Evidence for Cancer Cell-Extrinsic CAMKK2 Functions in Prostate Cancer

Pulliam

Awad

Han

et al. 2022

Cells

Self Cite

View full text Add to dashboard Cite

Despite early studies linking calcium-calmodulin protein kinase kinase 2 (CAMKK2) to prostate cancer cell migration and invasion, the role of CAMKK2 in metastasis in vivo remains unclear. Moreover, while CAMKK2 is known to regulate systemic metabolism, whether CAMKK2’s effects on whole-body metabolism would impact prostate cancer progression and/or related comorbidities is not known. Here, we demonstrate that germline ablation of Camkk2 slows, but does not stop, primary prostate tumorigenesis in the TRansgenic Adenocarcinoma Mouse Prostate (TRAMP) genetic mouse model. Consistent with prior epidemiological reports supporting a link between obesity and prostate cancer aggressiveness, TRAMP mice fed a high-fat diet exhibited a pronounced increase in the colonization of lung metastases. We demonstrated that this effect on the metastatic spread was dependent on CAMKK2. Notably, diet-induced lung metastases exhibited a highly aggressive neuroendocrine phenotype. Concurrently, Camkk2 deletion improved insulin sensitivity in the same mice. Histological analyses revealed that cancer cells were smaller in the TRAMP;Camkk2−/− mice compared to TRAMP;Camkk2+/+ controls. Given the differences in circulating insulin levels, a known regulator of cell growth, we hypothesized that systemic CAMKK2 could promote prostate cancer cell growth and disease progression in part through cancer cell-extrinsic mechanisms. Accordingly, host deletion of Camkk2 impaired the growth of syngeneic murine prostate tumors in vivo, confirming nonautonomous roles for CAMKK2 in prostate cancer. Cancer cell size and mTOR signaling was diminished in tumors propagated in Camkk2-null mice. Together, these data indicate that, in addition to cancer cell-intrinsic roles, CAMKK2 mediates prostate cancer progression via tumor-extrinsic mechanisms. Further, we propose that CAMKK2 inhibition may also help combat common metabolic comorbidities in men with advanced prostate cancer.

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“…However, this potentially could be the accumulated effect of several inhibited kinases [122]. The process to develop small-molecule inhibitors is ongoing, with the hinge region of CAMKK2 as the main target for achieving CAMKK2 inhibition [122,125,126].…”

Section: Cammk2 Signallingmentioning

confidence: 99%

Unravelling the Role of Kinases That Underpin Androgen Signalling in Prostate Cancer

Miller

Asim

2022

Cells

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The androgen receptor (AR) signalling pathway is the key driver in most prostate cancers (PCa), and is underpinned by several kinases both upstream and downstream of the AR. Many popular therapies for PCa that target the AR directly, however, have been circumvented by AR mutation, such as androgen receptor variants. Some upstream kinases promote AR signalling, including those which phosphorylate the AR and others that are AR-regulated, and androgen regulated kinase that can also form feed-forward activation circuits to promotes AR function. All of these kinases represent potentially druggable targets for PCa. There has generally been a divide in reviews reporting on pathways upstream of the AR and those reporting on AR-regulated genes despite the overlap that constitutes the promotion of AR signalling and PCa progression. In this review, we aim to elucidate which kinases—both upstream and AR-regulated—may be therapeutic targets and require future investigation and ongoing trials in developing kinase inhibitors for PCa.

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Hinge Binder Scaffold Hopping Identifies Potent Calcium/Calmodulin-Dependent Protein Kinase Kinase 2 (CAMKK2) Inhibitor Chemotypes

Cited by 24 publications

References 75 publications

Systemic ablation of Camkk2 impairs metastatic colonization and improves insulin sensitivity in TRAMP mice: Evidence for cancer cell-extrinsic CAMKK2 functions in prostate cancer

Systemic ablation of Camkk2 impairs metastatic colonization and improves insulin sensitivity in TRAMP mice: Evidence for cancer cell-extrinsic CAMKK2 functions in prostate cancer

Systemic Ablation of Camkk2 Impairs Metastatic Colonization and Improves Insulin Sensitivity in TRAMP Mice: Evidence for Cancer Cell-Extrinsic CAMKK2 Functions in Prostate Cancer

Unravelling the Role of Kinases That Underpin Androgen Signalling in Prostate Cancer

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