Mechanisms of Specific versus Nonspecific Interactions of Aggregation-Prone Inhibitors and Attenuators

Boulton, Stephen; Selvaratnam, Rajeevan; Ahmed, Rashik; Van, Katherine; Cheng, Xiaodong; Melacini, Giuseppe

doi:10.1021/acs.jmedchem.9b00258

Cited by 23 publications

(70 citation statements)

References 102 publications

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“…Some Epac small-molecule inhibitors, including ESI-09, are prone to aggregation-based inhibition leading to false positives arising from nonspecific binding. The mechanisms by which additives such as Triton X-100 and serum albumin can attenuate this adverse effect have been studied in detail by combination of biophysical techniques [36]. Biochemical characterization and SAR studies indeed suggested that ESI-09 inhibited activity of both Epac1 and Epac2 at concentrations well below those that induce protein denaturation [37].…”

Section: Epac1 Competitive Inhibitorsmentioning

confidence: 99%

The Epac1 Protein: Pharmacological Modulators, Cardiac Signalosome and Pathophysiology

Bouvet

Blondeau

Lezoualc’h

2019

Cells

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The second messenger 3′,5′-cyclic adenosine monophosphate (cAMP) is one of the most important signalling molecules in the heart as it regulates many physiological and pathophysiological processes. In addition to the classical protein kinase A (PKA) signalling route, the exchange proteins directly activated by cAMP (Epac) mediate the intracellular functions of cAMP and are now emerging as a new key cAMP effector in cardiac pathophysiology. In this review, we provide a perspective on recent advances in the discovery of new chemical entities targeting the Epac1 isoform and illustrate their use to study the Epac1 signalosome and functional characterisation in cardiac cells. We summarize the role of Epac1 in different subcompartments of the cardiomyocyte and discuss how cAMP–Epac1 specific signalling networks may contribute to the development of cardiac diseases. We also highlight ongoing work on the therapeutic potential of Epac1-selective small molecules for the treatment of cardiac disorders.

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Section: Epac1 Competitive Inhibitorsmentioning

confidence: 99%

The Epac1 Protein: Pharmacological Modulators, Cardiac Signalosome and Pathophysiology

Bouvet

Blondeau

Lezoualc’h

2019

Cells

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“…This property may limit the maximum CE3F4R concentration used in therapeutic applications and increases susceptibility to non-specific effects such as aggregation-based inhibition. This led Boulton et al to investigate CE3F4R’s non-specific interactions with EPAC1 using diverse techniques with varying degrees of resolution [47]. The formation of CE3F4R aggregates in vitro was studied using two commonly-used techniques, namely dynamic light scattering (DLS) and transmission electron microscopy (TEM) [34,35,42,47].…”

Section: Specific and Non-specific Inhibition Of Epac1 By Ce3f4rmentioning

confidence: 99%

“…This led Boulton et al to investigate CE3F4R’s non-specific interactions with EPAC1 using diverse techniques with varying degrees of resolution [47]. The formation of CE3F4R aggregates in vitro was studied using two commonly-used techniques, namely dynamic light scattering (DLS) and transmission electron microscopy (TEM) [34,35,42,47]. With both techniques, sub-micrometer aggregates were observed with sizes between 60 to 900 nm [47].…”

Section: Specific and Non-specific Inhibition Of Epac1 By Ce3f4rmentioning

confidence: 99%

“…The formation of CE3F4R aggregates in vitro was studied using two commonly-used techniques, namely dynamic light scattering (DLS) and transmission electron microscopy (TEM) [34,35,42,47]. With both techniques, sub-micrometer aggregates were observed with sizes between 60 to 900 nm [47]. According to TEM, however, unlike most aggregation-prone inhibitors, CE3F4R aggregates display a more varied, irregular morphology [34,35].…”

Section: Specific and Non-specific Inhibition Of Epac1 By Ce3f4rmentioning

confidence: 99%

“…The objective of this review is to summarize both the specific interactions underlying EPAC inhibition by two promising EPAC-specific inhibitors—CE3F4R [45] and ESI-09 [46]—as well as the non-specific interactions that result from their colloidal aggregate formation and subsequent aggregation-based EPAC inhibition in aqueous systems [47]. In this manner, we hope to provide key biophysical insight to the EPAC community in evaluating the inhibitory potential of current commercially available aggregation-prone EPAC inhibitors, in optimizing existing lead compounds, and in informing the future development of EPAC-specific inhibitors.…”

Section: Introductionmentioning

confidence: 99%

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Recent Advances in EPAC-Targeted Therapies: A Biophysical Perspective

Ahmed

Boulton

Shao

et al. 2019

Cells

Self Cite

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The universal second messenger cAMP regulates diverse intracellular processes by interacting with ubiquitously expressed proteins, such as Protein Kinase A (PKA) and the Exchange Protein directly Activated by cAMP (EPAC). EPAC is implicated in multiple pathologies, thus several EPAC-specific inhibitors have been identified in recent years. However, the mechanisms and molecular interactions underlying the EPAC inhibition elicited by such compounds are still poorly understood. Additionally, being hydrophobic low molecular weight species, EPAC-specific inhibitors are prone to forming colloidal aggregates, which result in non-specific aggregation-based inhibition (ABI) in aqueous systems. Here, we review from a biophysical perspective the molecular basis of the specific and non-specific interactions of two EPAC antagonists—CE3F4R, a non-competitive inhibitor, and ESI-09, a competitive inhibitor of EPAC. Additionally, we discuss the value of common ABI attenuators (e.g., TX and HSA) to reduce false positives at the expense of introducing false negatives when screening aggregation-prone compounds. We hope this review provides the EPAC community effective criteria to evaluate similar compounds, aiding in the optimization of existing drug leads, and informing the development of the next generation of EPAC-specific inhibitors.

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Experiences in Academic and Industry Partnerships – Forging a Path to Translational Drug Discovery

Dolle

Barrault²,

Carragher³

et al. 2021

Burger's Medicinal Chemistry and Drug Discovery

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Mechanisms of Specific versus Nonspecific Interactions of Aggregation-Prone Inhibitors and Attenuators

Cited by 23 publications

References 102 publications

The Epac1 Protein: Pharmacological Modulators, Cardiac Signalosome and Pathophysiology

The Epac1 Protein: Pharmacological Modulators, Cardiac Signalosome and Pathophysiology

Recent Advances in EPAC-Targeted Therapies: A Biophysical Perspective

Experiences in Academic and Industry Partnerships – Forging a Path to Translational Drug Discovery

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