Inhibiting Histone Deacetylase as a Means to Reverse Resistance to Angiogenesis Inhibitors: Phase I Study of Abexinostat Plus Pazopanib in Advanced Solid Tumor Malignancies

Aggarwal, Rahul; Thomas, Scott; Pawłowska, Nela; Bartelink, Imke H.; Grabowsky, Jennifer A.; Jahan, Thierry; Cripps, Amy; Harb, Armand; Leng, Jim; Reinert, Anne; Mastroserio, Ilaria; Truong, Thach Giao; Ryan, Charles J.; Münster, Pamela N.

doi:10.1200/jco.2016.70.5350

Cited by 81 publications

(68 citation statements)

References 23 publications

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“…While only in a small number of patients, we also show an increase in [ 18 F]fluciclatide uptake in those lesions that progressed on CT imaging following pazopanib therapy. Resistance to VEGF inhibitors is inevitable, the mechanism of which is postulated to be the overexpression and stabilization of hypoxia-inducible factor (HIF)-1α that directly regulates VEGF expression, and our results clearly illustrate this failure of functional blockade [58]. Taken together, the [ 18 F]fluciclatide-PET data suggest that the PET parameters obtained are consistent with the PD endpoint of pazopanib.…”

Section: Discussionsupporting

confidence: 67%

[18F]Fluciclatide PET as a biomarker of response to combination therapy of pazopanib and paclitaxel in platinum-resistant/refractory ovarian cancer

Sharma

Valls

Inglese

et al. 2019

Eur J Nucl Med Mol Imaging

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Background Angiogenesis is a driver of platinum resistance in ovarian cancer. We assessed the effect of combination pazopanib and paclitaxel followed by maintenance pazopanib in patients with platinum-resistant/refractory ovarian cancer. Integrins α v β 3 and α v β 5 are both upregulated in tumor-associated vasculature. [ 18 F]Fluciclatide is a novel PET tracer that has high affinity for integrins α v β 3/5 , and was used to assess the anti-angiogenic effect of pazopanib. Patients and methodsWe conducted an open-label, phase Ib study in patients with platinum-resistant/refractory ovarian cancer. Patients received 1 week of single-agent pazopanib (800 mg daily) followed by combination therapy with weekly paclitaxel (80 mg/m 2 ). Following completion of 18 weeks of combination therapy, patients continued with single-agent pazopanib until disease progression. Dynamic [ 18 F]fluciclatide-PET imaging was conducted at baseline and after 1 week of pazopanib. Response (RECIST 1.1), toxicities, and survival outcomes were recorded. Circulating markers of angiogenesis were assessed with therapy. Results Fourteen patients were included in the intention-to-treat analysis. Complete and partial responses were seen in seven patients (54%). Median progression-free survival (PFS) was 10.63 months, and overall survival (OS) was 18.5 months. Baseline [ 18 F]fluciclatide uptake was predictive of long PFS. Elevated baseline circulating angiopoietin and fibroblast growth factor (FGF) were predictive of greater reduction in SUV 60,mean following pazopanib. Kinetic modeling of PET data indicated a reduction in K 1 and K i following pazopanib indicating reduced radioligand delivery and retention. Conclusions Combination therapy followed by maintenance pazopanib is effective and tolerable in platinum-resistant/refractory ovarian cancer. [ 18 F]Fluciclatide-PET uptake parameters predict clinical outcome with pazopanib therapy indicating an antiangiogenic response.

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Section: Discussionsupporting

confidence: 67%

[18F]Fluciclatide PET as a biomarker of response to combination therapy of pazopanib and paclitaxel in platinum-resistant/refractory ovarian cancer

Sharma

Valls

Inglese

et al. 2019

Eur J Nucl Med Mol Imaging

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“…In a latest reported phase I trial, the addition of HDI abexinostat to pazopanib is well tolerated and resulted in durable responses in patients who experienced prior progression during treatment with VEGF inhibitors. Peripheral blood histone acetylation and HDAC2 gene expression were associated with durable response to treatment, which supports epigenetically mediated reversal of treatment resistance 116 . In a phase I dose-escalation study of the mTOR inhibitor sirolimus and the HDI vorinostat in patients with advanced malignancy, stable disease was observed in patient with fibromyxoid sarcoma 117 .…”

Section: Clinical Trials Of Hdis In Sarcomamentioning

confidence: 67%

Therapeutic applications of histone deacetylase inhibitors in sarcoma

Tang

Choy

et al. 2017

Cancer Treatment Reviews

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Sarcomas are a rare group of malignant tumors originating from mesenchymal stem cells. Surgery, radiation and chemotherapy are currently the only standard treatments for sarcoma. However, their response rates to chemotherapy are quite low. Toxic side effects and multi-drug chemoresistance make treatment even more challenging. Therefore, better drugs to treat sarcomas are needed. Histone deacetylase inhibitors (HDAC inhibitors, HDACi, HDIs) are epigenetic modifying agents that can inhibit sarcoma growth in vitro and in vivo through a variety of pathways, including inducing tumor cell apoptosis, causing cell cycle arrest, impairing tumor invasion and preventing metastasis. Importantly, preclinical studies have revealed that HDIs can not only sensitize sarcomas to chemotherapy and radiotherapy, but also increase treatment responses when combined with other chemotherapeutic drugs. Several phase I and II clinical trials have been conducted to assess the efficacy of HDIs either as monotherapy or in combination with standard chemotherapeutic agents or targeted therapeutic drugs for sarcomas. Combination regimen for sarcomas appear to be more promising than monotherapy when using HDIs. This review summarizes our current understanding and therapeutic applications of HDIs in sarcomas.

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“…In addition, there are FDA‐approved small‐molecule VEGFR‐2 inhibitors such as sunitinib ( 13 ), sorafenib ( 11 ), and vandetanib ( 38 ), which were approved for the treatment of various types of cancers including renal cell carcinoma, gastrointestinal stromal tumor, hepatocellular carcinoma, and thyroid cancer . Unfortunately, the increased resistance rates against VEGR inhibitors terminated their success, so many strategies to overcome this resistance were adopted, one of them is to develop chimeric VEGFR/HDAC inhibitors, especially when there is great synergy between RTK and HDAC inhibitors as previously mentioned . Peng et al .…”

Section: Design Of Dual Protein Tyrosine Kinase (Ptk) Hdac Inhibitorsmentioning

confidence: 99%

“…45 Unfortunately, the increased resistance rates against VEGR inhibitors terminated their success, so many strategies to overcome this resistance were adopted, 46 one of them is to develop chimeric VEGFR/HDAC inhibitors, especially when there is great synergy between RTK and HDAC inhibitors as previously mentioned. 47 Peng et al 48 in 2015 developed a dual VEGFR/HDAC inhibitor by combining pharmacophores of two reference drugs, vandetanib (38), which acts as a VEGFR inhibitor, and SAHA, which acts as an HDAC inhibitor, to yield series of chimeric compounds with the most potent compound 38a ( Figure 10). Hybrid 38a showed HDAC isoform and kinase selectivity as well as improving its physiochemical properties.…”

Section: Chimeric Bcr-abl Tyrosine Kinase-hdac Inhibitorsmentioning

confidence: 99%

Chimeric HDAC inhibitors: Comprehensive review on the HDAC‐based strategies developed to combat cancer

Hesham

Lasheen

Abouzid

2018

Medicinal Research Reviews

113

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Recently, molecular hybridization paradigm became an interesting and smart way to defeat the multifaceted cancer disease by a single molecular entity that acts via several mechanisms just like a magic bullet. Also, HDAC is an important epigenetic target in drug discovery, and the HDAC inhibitors showed successful pattern as cytotoxic agents. Because of their flexible structure activity relationship, it was easy to link them to other anticancer scaffolds. So, many dual action HDAC inhibitors have been developed and most of these hybrids have higher potency than the constituting parents in fighting of the cancer cells. This review describes potential applications of chimeric HDAC inhibitors, which simultaneously modulate not only HDAC but also multiple targets, in treatment of relapsing and drug-resistant cancers. We have nearly collected most of the reported dual action HDAC inhibitors yet to provide a comprehensive guide for the drug discovery process for developing more efficient anticancer agents.

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Inhibiting Histone Deacetylase as a Means to Reverse Resistance to Angiogenesis Inhibitors: Phase I Study of Abexinostat Plus Pazopanib in Advanced Solid Tumor Malignancies

Cited by 81 publications

References 23 publications

[18F]Fluciclatide PET as a biomarker of response to combination therapy of pazopanib and paclitaxel in platinum-resistant/refractory ovarian cancer

[18F]Fluciclatide PET as a biomarker of response to combination therapy of pazopanib and paclitaxel in platinum-resistant/refractory ovarian cancer

Therapeutic applications of histone deacetylase inhibitors in sarcoma

Chimeric HDAC inhibitors: Comprehensive review on the HDAC‐based strategies developed to combat cancer

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