BIIB021, an orally available, fully synthetic small-molecule inhibitor of the heat shock protein Hsp90

Lundgren, Karen; Zhang, Hong; Brekken, John; Huser, Nanni; Powell, Rachel E.; Timple, Noel; Busch, David J.; Neely, Laura; Sensintaffar, John; Yang, Yong-Ching; McKenzie, Andres; Friedman, Jessica; Scannevin, Robert H.; Kamal, Adeela; Hong, Kevin; Kasibhatla, Srinivas Rao; Boehm, Marcus F.; Burrows, Francis

doi:10.1158/1535-7163.mct-08-0758

Cited by 158 publications

(146 citation statements)

References 37 publications

(48 reference statements)

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“…3A and Supplementary Fig. S1), as previously reported (9,11,35,36), TAS-116 was more rapidly eliminated from retina (t 1/2 ¼ 3.4 hours) than the other HSP90 inhibitors (t 1/2 ¼ 7.1-19.1 hours), thereby demonstrating its lower retinal distribution profile (Fig. 3A and Supplementary Table S3).…”

Section: Tas-116 Shows Antitumor Activity Without Inducing Eye Injurysupporting

confidence: 82%

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TAS-116, a Highly Selective Inhibitor of Heat Shock Protein 90α and β, Demonstrates Potent Antitumor Activity and Minimal Ocular Toxicity in Preclinical Models

Ohkubo

Kodama

Muraoka

et al. 2015

Molecular Cancer Therapeutics

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The molecular chaperone HSP90 plays a crucial role in cancer cell growth and survival by stabilizing cancer-related proteins. A number of HSP90 inhibitors have been developed clinically for cancer therapy; however, potential off-target and/or HSP90-related toxicities have proved problematic. The 4-(1H-pyrazolo [3,4-b]pyridine-1-yl)benzamide TAS-116 is a selective inhibitor of cytosolic HSP90a and b that does not inhibit HSP90 paralogs such as endoplasmic reticulum GRP94 or mitochondrial TRAP1. Oral administration of TAS-116 led to tumor shrinkage in human tumor xenograft mouse models accompanied by depletion of multiple HSP90 clients, demonstrating that the inhibition of HSP90a and b alone was sufficient to exert antitumor activity in certain tumor models. One of the most notable HSP90-related adverse events universally observed to differing degrees in the clinical setting is visual disturbance. A two-week administration of the isoxazole resorcinol NVP-AUY922, an HSP90 inhibitor, caused marked degeneration and disarrangement of the outer nuclear layer of the retina and induced photoreceptor cell death in rats. In contrast, TAS-116 did not produce detectable photoreceptor injury in rats, probably due to its lower distribution in retinal tissue. Importantly, in a rat model, the antitumor activity of TAS-116 was accompanied by a higher distribution of the compound in subcutaneously xenografted NCI-H1975 non-small cell lung carcinoma tumors than in retina. Moreover, TAS-116 showed activity against orthotopically transplanted NCI-H1975 lung tumors. Together, these data suggest that TAS-116 has a potential to maximize antitumor activity while minimizing adverse effects such as visual disturbances that are observed with other compounds of this class.

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Section: Tas-116 Shows Antitumor Activity Without Inducing Eye Injurysupporting

confidence: 82%

“…It is possible that this excess liver toxicity is related to the quinone structure of ansamycin (16). The second generation of HSP90 inhibitors are based on a diverse variety of chemical scaffolds and exhibit less liver toxicity (11,13). However, these compounds cause other doselimiting toxicities, some of which are difficult to manage.…”

Section: Introductionmentioning

confidence: 99%

TAS-116, a Highly Selective Inhibitor of Heat Shock Protein 90α and β, Demonstrates Potent Antitumor Activity and Minimal Ocular Toxicity in Preclinical Models

Ohkubo

Kodama

Muraoka

et al. 2015

Molecular Cancer Therapeutics

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“…In these xenograft tumors, the suppression of specific sensitive client proteins lasted up to 72 h. HSP90 client proteins were suppressed for 24-48 h with NVP-AUY922, (30) for only 24 h following treatment with SNX-5422 (the pro-drug of SNX-2112), (20) and <24 h following treatment with BIIB021. (31) An overall review of the data for different HSP90 inhibitors in clinical development suggests a correlation between the potency of the inhibitors and their duration of action in tumors. The estimated K d of AT13387 for HSP90 was 0.7 nM, making it the most potent inhibitor at the N-terminal ATP site reported to date compared with other inhibitors (e.g.…”

Section: Discussionmentioning

confidence: 99%

“…(25)(26)(27) While there are many similarities in the pharmacology of these different agents, (28,29) one prominent variable is the duration of the pharmacodynamic effect reported. (20,30,31) We have used fragment-based drug discovery to identify the high-affinity, long-acting HSP90 inhibitor, AT13387, which is currently being evaluated in clinical trials. In the studies described here, we have used this inhibitor to demonstrate that maximizing the duration of effect in the target tissue enabled sustained client protein depletion and extended tumor growth inhibition with less frequent dosing of AT13387.…”

mentioning

confidence: 99%

The heat shock protein 90 inhibitor, AT13387, displays a long duration of action in vitro and in vivo in non‐small cell lung cancer

Graham¹,

Curry²,

Smyth³

et al. 2012

Cancer Science

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A ubiquitously expressed chaperone, heat shock protein 90 (HSP90) is of considerable interest as an oncology target because tumor cells and oncogenic proteins are acutely dependent on its activity. AT13387 (2,4-dihydroxy-5-isopropyl-phenyl)-[5-(4-methyl-piperazin-1-ylmethyl)-1,3-dihydro-isoindol-2-yl] methanone, L-lactic acid salt) a novel, high-affinity HSP90 inhibitor, which is currently being clinically tested, has shown activity against a wide array of tumor cell lines, including lung cancer cell lines. This inhibitor has induced the degradation of specific HSP90 client proteins for up to 7 days in tumor cell lines in vitro. The primary driver of cell growth (mutant epidermal growth factor receptors) was particularly sensitive to HSP90 inhibition. The long duration of client protein knockdown and suppression of phospho-signaling seen in vitro after treatment with AT13387 was also apparent in vivo, with client proteins and phospho-signaling suppressed for up to 72 h in xenograft tumors after treatment with a single dose of AT13387. Pharmacokinetic analyses indicated that while AT13387 was rapidly cleared from blood, its retention in tumor xenografts was markedly extended, and it was efficacious in a range of xenograft models. AT13387's long duration of action enabled, in particular, its efficacious once weekly administration in human lung carcinoma xenografts. The use of longer-acting HSP90 inhibitors, such as AT13387, on less frequent dosing regimens has the potential to maintain antitumor efficacy as well as minimize systemic exposure and unwanted effects on normal tissues. (Cancer Sci 2012; 103: 522-527) T he super-chaperone system is involved in the folding and maturation of newly synthesized proteins.(1,2) HSP90 in particular aids in the folding and maturation of a distinct subset of proteins, which includes kinases, cell surface receptors and transcription factors. (3,4) The N-terminal domain ATPase activity of HSP90 is essential for this function.(5) Inhibition of this domain induces remodeling of the HSP90 chaperone complex, resulting in the recruitment of ubiquitin ligases, polyubiquitination and subsequent proteasomal degradation of HSP90 client proteins.(6,7) Through this mechanism, the inhibition of a single target enzyme can have a wide effect on the stability and, hence, the function of a large set of client proteins. As many oncogenic proteins are HSP90 clients, HSP90 inhibition has been found to have broad antitumor effects.(8-10) In contrast to more recent targeted therapies, where the appearance of new driver mutations or resistance mutations result in a loss of efficacy, client protein mutation increases dependence on HSP90 chaperoning activity as these mutations tend to render the proteins less stable. (11)(12)(13) Previous studies have also demonstrated that the constitutively activated mutant forms of EGFR are particularly dependent on HSP90 both in vitro and in vivo, (14)(15)(16) indicating an HSP90 inhibitor may be particularly efficacious in mutant EGFR tumors.After HSP90 inhibiti...

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“…Antitumor efficacy ranges from minimal effects to tumor growth stasis but rarely tumor regression (9,14,15,(18)(19)(20). The variance in response between xenograft models may be attributable to differences in client protein dependence on Hsp90, tumor dependence on the client protein, kinetics of client protein degradation, and resynthesis, as well as, drug pharmacokinetic and pharmacologic properties.…”

Section: Introductionmentioning

confidence: 99%

The Novel Oral Hsp90 Inhibitor NVP-HSP990 Exhibits Potent and Broad-spectrum Antitumor ActivitiesIn VitroandIn Vivo

Menezes

Taverna

Jensen

et al. 2012

Molecular Cancer Therapeutics

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A novel oral Hsp90 inhibitor, NVP-HSP990, has been developed and characterized in vitro and in vivo. In vitro, NVP-HSP990 exhibits single digit nanomolar IC 50 values on three of the Hsp90 isoforms (Hsp90a, Hsp90b, and GRP94) and 320 nanomolar IC 50 value on the fourth (TRAP-1), with selectivity against unrelated enzymes, receptors, and kinases. In c-Met amplified GTL-16 gastric tumor cells, NVP-HSP990 dissociated the Hsp90-p23 complex, depleted client protein c-Met, and induced Hsp70. NVP-HSP990 potently inhibited the growth of human cell lines and primary patient samples from a variety of tumor types. In vivo, NVP-HSP990 exhibits drug-like pharmaceutical and pharmacologic properties with high oral bioavailability. In the GTL-16 xenograft model, a single oral administration of 15 mg/kg of NVP-HSP990 induced sustained downregulation of c-Met and upregulation of Hsp70. In repeat dosing studies, NVP-HSP990 treatment resulted in tumor growth inhibition of GTL-16 and other human tumor xenograft models driven by well-defined oncogenic Hsp90 client proteins. On the basis of its pharmacologic profile and broad-spectrum antitumor activities, clinical trials have been initiated to evaluate NVP-HSP990 in advanced solid tumors.

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BIIB021, an orally available, fully synthetic small-molecule inhibitor of the heat shock protein Hsp90

Cited by 158 publications

References 37 publications

TAS-116, a Highly Selective Inhibitor of Heat Shock Protein 90α and β, Demonstrates Potent Antitumor Activity and Minimal Ocular Toxicity in Preclinical Models

TAS-116, a Highly Selective Inhibitor of Heat Shock Protein 90α and β, Demonstrates Potent Antitumor Activity and Minimal Ocular Toxicity in Preclinical Models

The heat shock protein 90 inhibitor, AT13387, displays a long duration of action in vitro and in vivo in non‐small cell lung cancer

The Novel Oral Hsp90 Inhibitor NVP-HSP990 Exhibits Potent and Broad-spectrum Antitumor ActivitiesIn VitroandIn Vivo

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