Synthesis of a 2-Aryl-3-aroyl Indole Salt (OXi8007) Resembling Combretastatin A-4 with Application as a Vascular Disrupting Agent

Hadimani, Mallinath B.; MacDonough, Matthew T.; Ghatak, Anjan; Strecker, Tracy E.; Lopez, Ramona; Sriram, Madhavi; Nguyen, Benson L.; Hall, John J.; Kessler, Raymond J.; Shirali, Anupama; Liu, Li; Garner, Charles M.; Pettit, George R.; Hamel, Ernest; Chaplin, David J.; Mason, Ralph P.; Trawick, Mary Lynn; Pinney, Kevin G.

doi:10.1021/np400374w

Cited by 51 publications

(55 citation statements)

References 49 publications

(79 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

Section: Introductionmentioning

confidence: 95%

“…Our previous studies demonstrated that OXi8006 was a potent inhibitor of tubulin polymerization (IC 50 = 1.1 µM) and competed with radiolabeled colchicine at the colchicine binding site of tubulin [17]. We also found OXi8006 to be cytotoxic against three evaluated human cancer cell lines, NCI-H460, DU-145 and SK-OV-3, with an average GI 50 of 25.7 nM [17]. The core indole molecular structure is now widely represented as a key component of a variety of inhibitors of tubulin assembly [18], but OXi8006 remains one of the most active compounds in this group with respect to tubulin binding and cytotoxicity.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

The vascular disrupting activity of OXi8006 in endothelial cells and its phosphate prodrug OXi8007 in breast tumor xenografts

et al. 2015

Self Cite

View full text Add to dashboard Cite

This study describes the vascular disrupting ability and the mechanism of action of the indole-based tubulin-binding compound, OXi8006, and its water-soluble phosphate prodrug OXi8007. Treatment of rapidly proliferating human umbilical vein endothelial cells (HUVECs), used as a model for the tumor vasculature, with OXi8006 or OXi8007 caused potent microtubule disruption followed by extensive reorganization of the cytoskeletal network. The mechanism of action involved an increase in focal adhesion formation associated with an increase in phosphorylation of both non-muscle myosin light chain and focal adhesion kinase. These effects were dramatically diminished by an inhibitor of RhoA kinase, a downstream effector of RhoA. Cell cycle blockade at G2/M and cytotoxicity towards rapidly proliferating HUVECs were also observed. Capillary-like networks of HUVECs were disrupted by the action of both OXi8006 and OXi8007. The prodrug OXi8007 exhibited potent and rapid dose-dependent antivascular activity assessed by dynamic bioluminescence imaging (BLI) in an MDA-MB-231-luc breast cancer xenograft mouse model. By 6 hours post treatment, over 93% of the BLI signal was abolished with only a slight recovery at 24 hours. These findings were confirmed by histology. The results from this study demonstrate that OXi8007 is a potent vascular disrupting agent acting through an anti-microtubule mechanism involving RhoA.

show abstract

Section: Introductionmentioning

confidence: 95%

Section: Introductionmentioning

confidence: 99%

The vascular disrupting activity of OXi8006 in endothelial cells and its phosphate prodrug OXi8007 in breast tumor xenografts

et al. 2015

Self Cite

View full text Add to dashboard Cite

show abstract

“…As recently discussed, 34 the reason for this apparent inconsistency is not completely clear, but there are several factors that may contribute to explain this experimental fact. One factor could be that the stoichiometry (compound versus tubulin concentration) required in the tubulin (cell-free) assay to achieve an IC 50 value might be completely different from the stoichiometry that exists when inhibiting tubulin in cell culture.…”

Section: Vascular Disrupting Agents (Vdas)mentioning

confidence: 96%

“…In addition, there may be factors directly linked to the limitations and sensitivity of the protein assay. 34 2 36 Combretastatin A-4 derivatives have also been reviewed by Shan et al, 37 Marrelli et al, 38 and very recently by Patil et al 39 A review focusing on cis-restricted isomers has been published by Rajak et al 40 For those particularly interested in the synthetic pathways applied to obtain these compounds, relevant information can be obtained in the review article of Kaur et al 41 Other authors have performed a classification of the compounds based on structural and docking studies, as the exhaustive review of Alvarez et al 42 An overview of the role played by computational approaches in the context of the colchicine-binding domain has also been recently reported by Massarotti et al 43 In our survey through the different families of compounds that behave as VDAs, we have centered our attention on those compounds that are active in the nM range in cell culture and/ or for which animal experiments have been conducted as proof of concept of their VDA capacity. However, no comparison between data coming from different laboratories has been performed.…”

Section: Vascular Disrupting Agents (Vdas)mentioning

confidence: 99%

Blocking Blood Flow to Solid Tumors by Destabilizing Tubulin: An Approach to Targeting Tumor Growth

et al. 2016

View full text Add to dashboard Cite

The unique characteristics of the tumor vasculature offer the possibility to selectively target tumor growth and vascularization using tubulin-destabilizing agents. Evidence accumulated with combretastatin A-4 (CA-4) and its prodrug CA-4P support the therapeutic value of compounds sharing this mechanism of action. However, the chemical instability and poor solubility of CA-4 demand alternative compounds that are able to surmount these limitations. This Perspective illustrates the different classes of compounds that behave similar to CA-4, analyzes their binding mode to αβ-tubulin according to recently available structural complexes, and includes described approaches to improve their delivery. In addition, dissecting the mechanism of action of CA-4 and analogues allows a closer insight into the advantages and drawbacks associated with these tubulin-destabilizing agents that behave as vascular disrupting agents (VDAs).

show abstract

“…The synthetic route to 13 C-labeled bromoacetophenone intermediate 16 followed a similar sequence as the non-labeled bromoacetophenone intermediate from our previous studies with the indole based vascular disrupting agent (VDA) OXi8006 6–7,33 along with related work by von Angerer and co-workers, 34 and simply replaces the traditional methylation step reagents to install the 13 C carbon atom at the alpha position (Scheme 6). …”

Section: Introductionmentioning

confidence: 99%

Mechanistic considerations in the synthesis of 2-aryl-indole analogues under Bischler–Mohlau conditions

MacDonough

Shi

Pinney

2015

Tetrahedron Letters

Self Cite

View full text Add to dashboard Cite

Mechanistic insight into the pathway of the Bischler-Mohlau indole formation reaction is provided by isotopic labeling utilizing judicious incorporation of a 13C atom within the α-bromoacetophenone analogue reactant. The resulting rearranged 2-aryl indole, isolated as the major product, located the 13C isotope label at the methine carbon of the fused five-membered heterocyclic ring, which suggested that the mechanistic pathway of cyclization, in this specific example, required two equivalents of the aniline analogue reactant partner and proceeded through an imine intermediate rather than by direct formation of the corresponding 3-aryl indole accompanied by a concomitant 1,2-aryl shift rearrangement.

show abstract

Synthesis of a 2-Aryl-3-aroyl Indole Salt (OXi8007) Resembling Combretastatin A-4 with Application as a Vascular Disrupting Agent

Cited by 51 publications

References 49 publications

The vascular disrupting activity of OXi8006 in endothelial cells and its phosphate prodrug OXi8007 in breast tumor xenografts

The vascular disrupting activity of OXi8006 in endothelial cells and its phosphate prodrug OXi8007 in breast tumor xenografts

Blocking Blood Flow to Solid Tumors by Destabilizing Tubulin: An Approach to Targeting Tumor Growth

Mechanistic considerations in the synthesis of 2-aryl-indole analogues under Bischler–Mohlau conditions

Contact Info

Product

Resources

About