Potent Vinblastine C20′ Ureas Displaying Additionally Improved Activity Against a Vinblastine-Resistant Cancer Cell Line

Barker, Timothy J.; Duncan, Katharine K.; Otrubova, Katerina; Boger, Dale L.

doi:10.1021/ml400281w

Cited by 50 publications

(59 citation statements)

References 46 publications

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“…Methods that measure competitive binding at the vinblastine tubulin binding site are more predictive, and these typically involve measurement of the competitive displacement of radiolabeled vinblastine or fluorescently labeled vinblastine probes. We have previously used the competitive displacement of 3 H-vinblastine to assess the tubulin binding of selected members of the vinblastine C20′ ureas (20,21). This assay involves filtering coincubation solutions through DE-81 filter disks, which sequester tubulin and its bound ligands from solution (28,29).…”

Section: Resultsmentioning

confidence: 99%

“…One general observation made in these studies is that, although modifications to the key structural features of vinblastine typically result in reductions in biological activity, addition of structural features can substantially improve them (20,21,35,36). This includes not only our demonstration of the impact of the addition of an indole C10′ fluorine substituent (35) and the incorporation of the C20′ ethyl group into a benign more complex cis-fused C15′-C20′ six-membered ring (36), but also the discovery of the improved activity of C20′ urea replacements for the tertiary alcohol (20,21). Herein, we reported the discovery of compounds in this latter series that are now a stunning 100-fold more potent than vinblastine.…”

Section: Discussionmentioning

confidence: 99%

“…In subsequent studies, we identified the key structural features of such ureas that contribute to their activity, including the importance of the H-bond donor site on the C20′ nitrogen substituent (20). We additionally defined a trend in activity where substitution of the urea terminal nitrogen improves the differential in activity of the derivatives against matched sensitive and resistant tumor cell lines (NR 2 > NHR > NH 2 ), discovered a series of potent disubstituted C20′ ureas (e.g., 8 and 9) that displayed further improved activity against resistant tumor cell lines, and established that sterically demanding C20′ ureas were surprisingly well tolerated (20,21).…”

Section: Significancementioning

confidence: 98%

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Ultrapotent vinblastines in which added molecular complexity further disrupts the target tubulin dimer–dimer interface

Carney

Lukesh

Brody

et al. 2016

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

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Approaches to improving the biological properties of natural products typically strive to modify their structures to identify the essential pharmacophore, or make functional group changes to improve biological target affinity or functional activity, change physical properties, enhance stability, or introduce conformational constraints. Aside from accessible semisynthetic modifications of existing functional groups, rarely does one consider using chemical synthesis to add molecular complexity to the natural product. In part, this may be attributed to the added challenge intrinsic in the synthesis of an even more complex compound. Herein, we report synthetically derived, structurally more complex vinblastines inaccessible from the natural product itself that are a stunning 100-fold more active (IC50 values, 50–75 pM vs. 7 nM; HCT116), and that are now accessible because of advances in the total synthesis of the natural product. The newly discovered ultrapotent vinblastines, which may look highly unusual upon first inspection, bind tubulin with much higher affinity and likely further disrupt the tubulin head-to-tail α/β dimer–dimer interaction by virtue of the strategic placement of an added conformationally well-defined, rigid, and extended C20′ urea along the adjacent continuing protein–protein interface. In this case, the added molecular complexity was used to markedly enhance target binding and functional biological activity (100-fold), and likely represents a general approach to improving the properties of other natural products targeting a protein–protein interaction.

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Significancementioning

confidence: 98%

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Ultrapotent vinblastines in which added molecular complexity further disrupts the target tubulin dimer–dimer interface

Carney

Lukesh

Brody

et al. 2016

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

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“…In efforts that have targeted key members of the Aspidosperma alkaloids, including minovine, 1 (−)-aspidospermine and (+)-spegazzinine, 2 (+)- N -methylaspidospermidine, (−)-vindorosine and (−)-vindoline, 3 as well as their extension to the total synthesis of vinblastine 4 and related natural products including vincristine 5 and key analogues, 6 we introduced a powerful intramolecular tandem [4 + 2]/[3 + 2] cycloaddition cascade of 1,3,4-oxadiazoles that provides the stereochemically-rich pentacyclic core of the natural products in a single step. 7,8 We have subsequently disclosed the use of the common Aspidosperma -like pentacyclic intermediate 1 , assembled using this key cycloaddition cascade and bearing a functionalized C5 ethyl substituent (primary alcohol), in the divergent 9 total synthesis of a series of additional alkaloids.…”

Section: Introductionmentioning

confidence: 99%

Total synthesis of (−)-kopsinine and ent-(+)-kopsinine

Lee

Boger

2015

Tetrahedron

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The total synthesis of (−)-kopsinine and its unnatural enantiomer is detailed, enlisting a late-stage SmI2-mediated transannular free radical conjugate addition reaction for construction of the core bicyclo[2.2.2]octane ring system with strategic C21–C2 bond formation. Key to the approach is assemblage of the underlying skeleton by an intramolecular [4+2]/[3+2] cycloaddition cascade of a 1,3,4-oxadiazole that provided the precursor C21 functionalized pentacyclic ring system 1 in a single step in which the C3 methyl ester found in the natural product served as a key 1,3,4-oxadiazole substituent, activating it for participation in the initiating Diels–Alder reaction and stabilizing the intermediate 1,3-dipole.

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“…9 Among the most significant of the observations made to date in these studies is that while removal of individual substituents or key structural components of the natural products typically results in reductions in biological activity, 8–14 addition of structural features can substantially improve biological properties. 15,16 As a result of our demonstration of the importance of the addition of a key indole C10′ substituent (10′-fluorovinblasine) 15 and with the discovery of the remarkable impact of select C20′ alcohol replacements (C20′ ureas), 16 it appeared that the spatial placement of the indole at one end of velbanamine and the C20′ ethyl group at the other are two especially important features of the structure. The X-ray structure of tubulin-bound vinblastine 5 (Figure 2) indicates both fit into well-defined protein pockets on the tubulin α and β subunits, respectively, deeply embedded in the tubulin binding site with each occupying corners of a T-shaped bound conformation of vinblastine.…”

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confidence: 99%

Synthesis of a Potent Vinblastine: Rationally Designed Added Benign Complexity

et al. 2016

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Many natural products, including vinblastine, have not been easily subjected to simplifications in their structures by synthetic means or modifications by late-stage semi-synthetic derivatization in ways that enhance their biological potency. Herein, we detail a synthetic vinblastine that incorporates added benign complexity (ABC), which improves activity 10-fold, and is now accessible as a result of advances in the total synthesis of the natural product. The compound incorporates designed added molecular complexity but no new functional groups, and maintains all existing structural and conformational features of the natural product. It constitutes a member of an analogue class presently inaccessible by semi-synthetic derivatization of the natural product, by its late-stage functionalization, or by biosynthetic means. Rather, it was accessed by synthetic means, using an appropriately modified powerful penultimate single-step vindoline-catharanthine coupling strategy that proceeds with a higher diastereoselectivity than found for the natural product itself.

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Potent Vinblastine C20′ Ureas Displaying Additionally Improved Activity Against a Vinblastine-Resistant Cancer Cell Line

Cited by 50 publications

References 46 publications

Ultrapotent vinblastines in which added molecular complexity further disrupts the target tubulin dimer–dimer interface

Ultrapotent vinblastines in which added molecular complexity further disrupts the target tubulin dimer–dimer interface

Total synthesis of (−)-kopsinine and ent-(+)-kopsinine

Synthesis of a Potent Vinblastine: Rationally Designed Added Benign Complexity

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