Synthetic small molecule furin inhibitors derived from 2,5-dideoxystreptamine

Jiao, Guan-Sheng; Cregar, Lynne; Wang, Jinzhi; Millis, Sherri Z.; Tang, Cho; O’Malley, Sean; Johnson, A. T. Charlie; Sareth, Sina; Larson, Jason; Thomas, Gary

doi:10.1073/pnas.0606555104

Cited by 81 publications

(113 citation statements)

References 42 publications

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“…Much more potent furin inhibitors have been generated recently by derivatization of 2,5-dideoxytryptamine with the addition of guanidinylated aryl groups (Jiao et al, 2006) and by using cell-based assays for screening (Coppola et al, 2007). For example, guanidinylated aryl compounds exhibit nanomolar K i values and possess excellent specificity (Jiao et al, 2006). These data support the idea that convertases can be specifically and potently inhibited by small molecules.…”

Section: Discussionsupporting

confidence: 55%

“…Andrographolide paniculata diterpines of the labdane family were the first example of such nonpeptide convertase inhibitors (Basak et al, 1999); however, inhibition was quite weak and nonspecific. Much more potent furin inhibitors have been generated recently by derivatization of 2,5-dideoxytryptamine with the addition of guanidinylated aryl groups (Jiao et al, 2006) and by using cell-based assays for screening (Coppola et al, 2007). For example, guanidinylated aryl compounds exhibit nanomolar K i values and possess excellent specificity (Jiao et al, 2006).…”

Section: Discussionmentioning

confidence: 99%

“…Many smallmolecule inhibitors have been reported to date against the proprotein convertase furin (Basak et al, 1999;Podsiadlo et al, 2004;Jiao et al, 2006); these may be useful in blocking many furin-dependent pathological processes (Fugere and Day, 2005). However, no small-molecule inhibitors of proprotein convertases other than furin have yet been identified.…”

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confidence: 99%

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Synthetic Small-Molecule Prohormone Convertase 2 Inhibitors

et al. 2008

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The proprotein convertases are believed to be responsible for the proteolytic maturation of a large number of peptide hormone precursors. Although potent furin inhibitors have been identified, thus far, no small-molecule prohormone convertase 1/3 or prohormone convertase 2 (PC2) inhibitors have been described. After screening 38 small-molecule positional scanning libraries against recombinant mouse PC2, two promising chemical scaffolds were identified: bicyclic guanidines, and pyrrolidine bis-piperazines. A set of individual compounds was designed from each library and tested against PC2. Pyrrolidine bis-piperazines were irreversible, time-dependent inhibitors of PC2, exhibiting noncompetitive inhibition kinetics; the most potent inhibitor exhibited a K i value for PC2 of 0.54 M. In contrast, the most potent bicyclic guanidine inhibitor exhibited a K i value of 3.3 M. Cross-reactivity with other convertases was limited: pyrrolidine bis-piperazines exhibited K i values greater than 25 M for PC1/3 or furin, whereas the K i values of bicyclic guanidines for these other convertases were more than 15 M. We conclude that pyrrolidine bis-piperazines and bicyclic guanidines represent promising initial leads for the optimization of therapeutically active PC2 inhibitors. PC2-specific inhibitors may be useful in the pharmacological blockade of PC2-dependent cleavage events, such as glucagon production in the pancreas and ectopic peptide production in small-cell carcinoma, and to study PC2-dependent proteolytic events, such as opioid peptide production.

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Section: Discussionsupporting

confidence: 55%

Section: Discussionmentioning

confidence: 99%

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confidence: 99%

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Synthetic Small-Molecule Prohormone Convertase 2 Inhibitors

et al. 2008

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“…The intact toxins and viral proteins are incapable of accomplishing these processes. Evidence suggests that the inhibition of cellular furin prevents aggressive disease (2,5). These results lead to the logical suggestion that furin is a promising drug target in infectious diseases; an experimental confirmation, however, has been limited because research efforts have been focused primarily on anthrax (5-7).…”

mentioning

confidence: 99%

Targeting Host Cell Furin Proprotein Convertases as a Therapeutic Strategy against Bacterial Toxins and Viral Pathogens

Shiryaev

Remacle

Ratnikov

et al. 2007

Journal of Biological Chemistry

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Pathogens or their toxins, including influenza virus, Pseudomonas, and anthrax toxins, require processing by host proprotein convertases (PCs) to enter host cells and to cause disease. Conversely, inhibiting PCs is likely to protect host cells from multiple furin-dependent, but otherwise unrelated, pathogens. To determine if this concept is correct, we designed specific nanomolar inhibitors of PCs modeled from the extended cleavage motif TPQRERRRKKR2GL of the avian influenza H5N1 hemagglutinin. We then confirmed the efficacy of the inhibitory peptides in vitro against the fluorescent peptide, anthrax protective antigen (PA83), and influenza hemagglutinin substrates and also in mice in vivo against two unrelated toxins, anthrax and Pseudomonas exotoxin. Peptides with Phe/Tyr at P1 were more selective for furin. Peptides with P1 Thr were potent against multiple PCs. Our strategy of basing the peptide sequence on a furin cleavage motif known for an avian flu virus shows the power of starting inhibitor design with a known substrate. Our results confirm that inhibiting furin-like PCs protects the host from the distinct furin-dependent infections and lay a foundation for novel, host cell-focused therapies against acute diseases.

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“…The PCs are also involved in a large number of pathologies, including bacterial and viral infections, as well as cancer and metastasis. Therefore, these enzymes are intensely investigated as drug targets (3), using for example, peptide-derived compounds (4)(5)(6)(7)(8)(9), nonpeptidic small molecule compounds (10,11), and protein-based inhibitors (12)(13)(14)(15).…”

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confidence: 99%

Structure of the unliganded form of the proprotein convertase furin suggests activation by a substrate-induced mechanism

Dahms

Arciniega

Steinmetzer

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

200

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Proprotein convertases (PCs) are highly specific proteases required for the proteolytic modification of many secreted proteins. An unbalanced activity of these enzymes is connected to pathologies like cancer, atherosclerosis, hypercholesterolaemia, and infectious diseases. Novel protein crystallographic structures of the prototypical PC family member furin in different functional states were determined to 1.8-2.0 Å. These, together with biochemical data and modeling by molecular dynamics calculations, suggest essential elements underlying its unusually high substrate specificity. Furin shows a complex activation mechanism and exists in at least four defined states: (i) the "off state," incompatible with substrate binding as seen in the unliganded enzyme; (ii) the active "on state" seen in inhibitor-bound furin; and the respective (iii) calcium-free and (iv) calcium-bound forms. The transition from the off to the on state is triggered by ligand binding at subsites S1 to S4 and appears to underlie the preferential recognition of the four-residue sequence motif of furin. The molecular dynamics simulations of the four structural states reflect the experimental observations in general and provide approximations of the respective stabilities. Ligation by calcium at the PC-specific binding site II influences the active-site geometry and determines the rotamer state of the oxyanion holeforming Asn295, and thus adds a second level of the activity modulation of furin. The described crystal forms and the observations of different defined functional states may foster the development of new tools and strategies for pharmacological intervention targeting furin.serine-protease | activation | specificity | conformational transition

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Synthetic small molecule furin inhibitors derived from 2,5-dideoxystreptamine

Cited by 81 publications

References 42 publications

Synthetic Small-Molecule Prohormone Convertase 2 Inhibitors

Synthetic Small-Molecule Prohormone Convertase 2 Inhibitors

Targeting Host Cell Furin Proprotein Convertases as a Therapeutic Strategy against Bacterial Toxins and Viral Pathogens

Structure of the unliganded form of the proprotein convertase furin suggests activation by a substrate-induced mechanism

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