Principles and functions of condensate modifying drugs

Patel, Avinash; Mitrea, Diana M.; Namasivayam, Vigneshwaran; Murcko, Mark A.; Wagner, Michael; Klein, I.

doi:10.3389/fmolb.2022.1007744

Cited by 13 publications

(8 citation statements)

References 84 publications

(113 reference statements)

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“…An advantage of using covalent small molecules for ligand discovery is rapid target and binding site identifications using quantitative chemical proteomics. Target deconvolution represents an important, but often challenging, first step toward understanding mode of action for condensate-modifying compounds. , The binding profiles obtained from chemical proteomics enable global selectivity profiling and bioinformatics-mediated discovery of enriched protein functions and domains underlying the PB- and SG-modulating activity of hit compounds.…”

Section: Resultsmentioning

confidence: 99%

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Global Discovery of Covalent Modulators of Ribonucleoprotein Granules

et al. 2023

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Stress granules (SGs) and processing-bodies (PBs, P-bodies) are ubiquitous and widely studied ribonucleoprotein (RNP) granules involved in cellular stress response, viral infection, and the tumor microenvironment. While proteomic and transcriptomic investigations of SGs and PBs have provided insights into molecular composition, chemical tools to probe and modulate RNP granules remain lacking. Herein, we combine an immunofluorescence (IF)-based phenotypic screen with chemoproteomics to identify sulfonyl-triazoles (SuTEx) capable of preventing or inducing SG and PB formation through liganding of tyrosine (Tyr) and lysine (Lys) sites in stressed cells. Liganded sites were enriched for RNA-binding and protein–protein interaction (PPI) domains, including several sites found in RNP granule-forming proteins. Among these, we functionally validate G3BP1 Y40, located in the NTF2 dimerization domain, as a ligandable site that can disrupt arsenite-induced SG formation in cells. In summary, we present a chemical strategy for the systematic discovery of condensate-modulating covalent small molecules.

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Section: Resultsmentioning

confidence: 99%

“…Compounds that target SG proteins have been reported, but direct binding remains to be demonstrated . Thus, apart from approved drugs with condensate modifying activity discovered after the fact, RNP granule modulators consist largely of toxic compounds or lead hits from HTS that lack known direct binding targets.…”

Section: Introductionmentioning

confidence: 99%

Global Discovery of Covalent Modulators of Ribonucleoprotein Granules

et al. 2023

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“…Knowing the interactions and any molecular condensates in which sPLA2 is involved is of paramount importance. Molecular condensates regulate a variety of cellular activities and are involved in numerous pathological processes [ 69 , 91 ], therefore, they are being studied for the development of molecules that can induce their formation, alter, or even dissolve them [ 92 ].…”

Section: How To Target Spla2s In Inflammation-associated Human Diseasesmentioning

confidence: 99%

Secretory Phospholipases A2, from Snakebite Envenoming to a Myriad of Inflammation Associated Human Diseases—What Is the Secret of Their Activity?

Tonello

2023

IJMS

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Secreted phospholipases of type A2 (sPLA2s) are proteins of 14–16 kDa present in mammals in different forms and at different body sites. They are involved in lipid transformation processes, and consequently in various immune, inflammatory, and metabolic processes. sPLA2s are also major components of snake venoms, endowed with various toxic and pharmacological properties. The activity of sPLA2s is not limited to the enzymatic one but, through interaction with different types of molecules, they exert other activities that are still little known and explored, both outside and inside the cells, as they can be endocytosed. The aim of this review is to analyze three features of sPLA2s, yet under-explored, knowledge of which could be crucial to understanding the activity of these proteins. The first feature is their disulphide bridge pattern, which has always been considered immutable and necessary for their stability, but which might instead be modulable. The second characteristic is their ability to undergo various post-translational modifications that would control their interaction with other molecules. The third feature is their ability to participate in active molecular condensates both on the surface and within the cell. Finally, the implications of these features in the design of anti-inflammatory drugs are discussed.

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“…[17][18][19][20][21] Experiments on BCs have advanced to the point that they are being synthetically designed to modulate biochemical and cellular functions, [22][23][24][25][26][27][28] and mined for novel drug targets. [29][30][31] A better understanding of how BCs are coupled (or not) to their crowded environment would assist in deciphering their cellular roles and constructing synthetic BCs. [32][33][34][35][36][37][38] The complexity of living cells has driven research on model condensates, which typically use unphysiologically-high concentrations of one, or at most a few, species of IDP in buffer, although their relevance to living cells has been strongly questioned.…”

Section: Introductionmentioning

confidence: 99%

“…[17-21] Experiments on BCs have advanced to the point that they are being synthetically designed to modulate biochemical and cellular functions,[22-28] and mined for novel drug targets. [29-31] A better understanding of how BCs are coupled (or not) to their crowded environment would assist in deciphering their cellular roles and constructing synthetic BCs. [32-38]…”

Section: Introductionmentioning

confidence: 99%

Macromolecular crowding is surprisingly unable to deform the structure of a model biomolecular condensate

Shillcock

Thomas

Ipsen

et al. 2022

Preprint

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The crowded interior of a living cell makes experiments on simpler systems attractive. Although these reveal interesting phenomena, their biological relevance can be questionable. A topical example is the phase separation of intrinsically disordered proteins into biomolecular condensates, which is proposed to underlie the membraneless compartmentalisation of many cellular functions. How a cell reliably controls biochemical reactions in compartments open to the compositionally varying cytoplasm is an important question for understanding cellular homeostasis. Computer simulations are often used to study the phase behaviour of model biomolecular condensates, but the number of relevant parameters explodes as the number of protein components increases. It is unfeasible to exhaustively simulate such models for all parameter combinations, although interesting phenomena are almost certainly hidden in the jungle of their high dimensional parameter space. Here we have studied the phase behaviour of a model biomolecular condensate in the presence of a polymeric crowding agent. We used a novel compute framework to execute dozens of simultaneous simulations spanning the protein crowder concentration space. We then combined the results into a graphical representation for human interpretation, which provided an efficient way to search the high-dimensional parameter space. We found that steric repulsion from the crowder drives a near-critical system across the phase boundary, but the molecular arrangement within the resulting biomolecular condensate is rather insensitive to the crowder concentration and molecular weight. We propose that a cell may use the local cytoplasmic concentration to assist formation of biomolecular condensates, while relying on the dense phase reliably providing a stable, structured, fluid milieu for cellular biochemistry despite being open to its changing environment.

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Principles and functions of condensate modifying drugs

Cited by 13 publications

References 84 publications

Global Discovery of Covalent Modulators of Ribonucleoprotein Granules

Global Discovery of Covalent Modulators of Ribonucleoprotein Granules

Secretory Phospholipases A2, from Snakebite Envenoming to a Myriad of Inflammation Associated Human Diseases—What Is the Secret of Their Activity?

Macromolecular crowding is surprisingly unable to deform the structure of a model biomolecular condensate

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