Discovery of an enzyme and substrate selective inhibitor of ADAM10 using an exosite-binding glycosylated substrate

Madoux, Franck; Dreymüller, Daniela; Pettiloud, Jean-Phillipe; Santos, Radleigh; Becker‐Pauly, Christoph; Ludwig, Andreas; Fields, Gregg B.; Bannister, Thomas D.; Spicer, Timothy; Čudić, Mare; Scampavia, Louis; Minond, Dmitriy

doi:10.1038/s41598-016-0013-4

Cited by 114 publications

(84 citation statements)

References 57 publications

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“…MSCs on TCP upregulated monocyte chemoattractant protein-1 ( CCL2 ), galectin-9 ( GAL9 ), and TNFα-stimulated gene 6 ( TNFAIP6 ) after an initial pulse stimulation (Figure 5d and Figure S13), which was consistent with previous studies on MSC polarization to an immunomodulatory phenotype. [31] The gene expression levels of PTGS2 and TNFAIP6 were further upregulated as the stiffness (G’) was increased in the Alg hydrogels (Figure 5c–d). The levels were also plotted versus loss angle at each G’, which showed a viscoelastic-dependent increase in expression at 0.5 and 2.5 kPa G’.…”

Section: Resultsmentioning

confidence: 99%

Sequential modes of crosslinking tune viscoelasticity of cell-instructive hydrogels

2019

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Materials that can mimic the fibrillar architecture of native extracellular matrix (ECM) while allowing for independent regulation of viscoelastic properties may serve as ideal, artificial ECM (aECM) to regulate cell functions. Here we describe an interpenetrating network of click-functionalized alginate, crosslinked with a combination of ionic and covalent crosslinking, and fibrillar collagen type I. Varying the mode and magnitude of crosslinking enables tunable stiffness and viscoelasticity, while altering neither the hydrogel’s microscale architecture nor diffusional transport of molecules with molecular weight relevant to typical nutrients. Further, appropriately timing sequential ionic and covalent crosslinking permits self-assembly of collagen into fibrillar structures within the network. Culture of human mesenchymal stem cells (MSCs) in this mechanically-tunable ECM system revealed that MSC expression of immunomodulatory markers is differentially impacted by the viscoelasticity and stiffness of the matrix. Together, these results describe and validate a novel material system for investigating how viscoelastic mechanical properties of ECM regulate cellular behavior.

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Section: Resultsmentioning

confidence: 99%

Sequential modes of crosslinking tune viscoelasticity of cell-instructive hydrogels

2019

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“…Here, we aim to study the carry-over effects of sublethal herbicides on the F1 generation of A. retroflexus L. as an invasive plant using parent plants in the vegetative or reproductive periods treated by atrazine or tribenuron-methyl, which are two commonly used herbicides in Chinese arable cereal crops 33 and also commonly used to control A. retroflexus in China 34, 35 . Our objectives were: (i) to determine whether there was a carry-over effect of atrazine and tribenuron-methyl on the F1 generation of A. retroflexus , (ii) to compare the germination and growth of the F1 generation of A. retroflexus treated with herbicides during different growth periods (vegetative and reproductive), and (iii) to determine if an increased sublethal dose to the parent plant increases the toxic effect on the F1 generation.…”

Section: Introductionmentioning

confidence: 99%

Germination of Seeds and Seedling Growth of Amaranthus retroflexus L. Following Sublethal Exposure of Parent Plants to Herbicides

Yan

et al. 2017

Sci Rep

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Herbicides have long-term effects on the vegetative parts and reproduction of plants; however, the carry-over effects of herbicides on the F1 generation of invasive plants remain unclear. The objectives of this work were to investigate the germination and growth of the F1 generation of A. retroflexus, an invasion plant, treated by sublethal herbicides. The results demonstrated that atrazine or tribenuron-methyl had carry-over effects on the F1 generation of A. retroflexus. Atrazine or tribenuron-methyl exposure during the vegetative and reproductive periods significantly inhibited the germination and growth of the F1 generation; a lower sublethal dose of atrazine or tribenuron-methyl did not weaken the inhibition of germination or growth of the F1 generation. Our results suggest that although herbicides have a carry-over inhibition effect on the F1 generation of invasive plants, they may have a more serious carry-over effect on native plants and cause changes in weed species composition and weed diversity.

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“…In recent years there has been a shift from active site to a secondary substrate binding site (exosite) inhibitor discovery . We described enzyme‐ and substrate‐selective non‐Zn 2+ binding inhibitors of ADAM17 and ADAM10 (Figure ) which are currently being tested in several pre‐clinical disease models. Both ADAM10 (CID 3117694) and ADAM17 (compound 19 in) leads were discovered as a result of screening efforts using a glycosylated, exosite‐binding substrate based on the TNFα sequence .…”

Section: Adam Inhibitors: General Considerationsmentioning

confidence: 99%

“…We described enzyme‐ and substrate‐selective non‐Zn 2+ binding inhibitors of ADAM17 and ADAM10 (Figure ) which are currently being tested in several pre‐clinical disease models. Both ADAM10 (CID 3117694) and ADAM17 (compound 19 in) leads were discovered as a result of screening efforts using a glycosylated, exosite‐binding substrate based on the TNFα sequence . Mechanistic studies showed that both inhibitors acted via a non‐Zn 2+ binding mechanism, which explained their selectivity toward ADAM10 and ADAM17 (Table ).…”

Section: Adam Inhibitors: General Considerationsmentioning

confidence: 99%

Clinical Implications of Compounds Designed to Inhibit ECM‐Modifying Metalloproteinases

2017

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Remodeling of the extracellular matrix (ECM) is crucial in development and homeostasis, but also has a significant role in disease progression. Two metalloproteinase families, the matrix metalloproteinases (MMPs) and a disintegrin and metalloproteases (ADAMs), participate in the remodeling of the ECM, either directly or through the liberation of growth factors and cell surface receptors. The correlation of MMP and ADAM activity to a variety of diseases has instigated numerous drug development programs. However, broad-based and Zn -chelating MMP and ADAM inhibitors have fared poorly in the clinic. Selective MMP and ADAM inhibitors have been described recently based on (a) antibodies or antibody fragments or (b) small molecules designed to take advantage of protease secondary binding sites (exosites) or allosteric sites. Clinical trials have been undertaken with several of these inhibitors, while others are in advanced pre-clinical stages.

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Discovery of an enzyme and substrate selective inhibitor of ADAM10 using an exosite-binding glycosylated substrate

Cited by 114 publications

References 57 publications

Sequential modes of crosslinking tune viscoelasticity of cell-instructive hydrogels

Sequential modes of crosslinking tune viscoelasticity of cell-instructive hydrogels

Germination of Seeds and Seedling Growth of Amaranthus retroflexus L. Following Sublethal Exposure of Parent Plants to Herbicides

Clinical Implications of Compounds Designed to Inhibit ECM‐Modifying Metalloproteinases

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