Phase 1 dose escalation multicenter trial of pracinostat alone and in combination with azacitidine in patients with advanced hematologic malignancies

Abaza, Yasmin; Kadia, Tapan M.; Jabbour, Elias; Konopleva, Marina; Borthakur, Gautam; Ferrajoli, Alessandra; Estrov, Zeev; Wierda, William G.; Alfonso, Ana; Chong, Toh Han; Chuah, Charles; Koh, Liang Piu; Goh, Boon Cher; Chang, Elizabeth; Durkes, Daniel E.; Foudray, Maria Cielo; Kantarjian, Hagop M.; Dong, Xiao-Qiao; Garcia‐Manero, Guillermo

doi:10.1002/cncr.30949

Cited by 47 publications

(23 citation statements)

References 35 publications

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“…Injectable azacitidine 75 mg/m 2 /day, administered intravenously (IV) or subcutaneously (SC) for 7 days per 28-day treatment cycle, is approved in several countries for treatment of myelodysplastic syndromes (MDS) and acute myeloid leukemia (AML) [1,2]. Azacitidine has also been investigated in a variety of other hematologic malignancies and solid tumors [3][4][5][6]. In addition to direct cytotoxicity of proliferating malignant cells, azacitidine is incorporated into both RNA and DNA (in human AML KG1a cells, the RNA:DNA incorporation ratio was 65:35 [7]) and reduces hypermethylation in promoter regions of DNA, leading to re-expression of tumor suppressor genes and promoting differentiation of hematopoietic progenitor cells [7][8][9].…”

Section: Introductionmentioning

confidence: 99%

Evaluation of the bioequivalence and food effect on the bioavailability of CC-486 (oral azacitidine) tablets in adult patients with cancer

Babiker

Milhem

Aisner

et al. 2020

Cancer Chemother Pharmacol

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Purpose CC-486 is an oral formulation of azacitidine that allows for extended dosing schedules to prolong azacitidine exposure to malignant cells and maximize clinical activity. CC-486 300 mg daily, administered for 14 or 21 days of 28-day treatment cycles, is currently under investigation in two ongoing phase III trials. The 300-mg daily dose in these studies is administered as two 150-mg tablets (Formulation A). Methods We evaluated the bioequivalence of one 300-mg CC-486 tablet (Formulation B) with Formulation A and food effect on Formulation B, in adult patients with cancer in a 2-stage crossover design study. Results The ratios of the geometric means of the maximum azacitidine plasma concentration (C max ) and of the area under the plasma concentration-time curve from time 0 extrapolated to infinity (AUC ∞ ) were 101.5% and 105.7%, demonstrating the bioequivalence of Formulations A and B. Formulation B was rapidly absorbed under fasted and fed conditions. The geometric mean of C max was significantly decreased by ~ 21% in the fed state. Median T max was reached at 2 h and 1 h post-dose in fed and fasted states, respectively (P < 0.001). Nevertheless, systemic drug exposure (AUC) in fed and fasted states was within the 80-125% boundaries of bioequivalence and differences in C max and T max are not expected to have a clinical impact. Conclusion The single 300-mg CC-486 tablet was bioequivalent to two 150-mg tablets, which have shown to be efficacious and generally well-tolerated in clinical trials, and can be taken with or without food.

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Section: Introductionmentioning

confidence: 99%

Evaluation of the bioequivalence and food effect on the bioavailability of CC-486 (oral azacitidine) tablets in adult patients with cancer

Babiker

Milhem

Aisner

et al. 2020

Cancer Chemother Pharmacol

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“…Preclinical and pilot clinical experiences suggested the potential benefit of adding HDAC inhibitors to HMA as combination epigenetic therapy in myeloid malignancies. Data from a prior study that evaluated an HMA/pracinostat combination in subjects with MDS demonstrated preliminary clinical activity (Abaza et al , ). Based on these findings, we designed the current study to assess the safety and efficacy of the addition of pracinostat in MDS patients failing treatment with single agent HMA.…”

Section: Discussionmentioning

confidence: 99%

“…Vorinostat, panobinostat and pracinostat are oral, pan‐HDAC inhibitors. Each of these demonstrated early promise when used in combination with HMAs in single arm phase I trials (Dokmanovic et al , ; Prebet & Vey, ; Abaza et al , ). However, more recent multi‐arm randomized controlled trials have shown mixed or, in some cases, negative outcomes when combination therapy was compared with HMA monotherapy.…”

Section: Discussionmentioning

confidence: 99%

“…The anti‐tumour activity of pracinostat has been demonstrated in several xenograft mouse models of solid and haematological malignancies as well as in phase I and pilot phase II clinical trials (Yong et al , ; Razak et al , ; Novotny‐Diermayr et al , ; Quintas‐Cardama et al , ; Eigl et al , ). Synergistic interactions have also been observed with multiple cytotoxic and targeted anti‐cancer therapeutics, notably with azacitidine (Novotny‐Diermayr et al , ; Abaza et al , ). Recent data from a pilot phase I trial suggested clinical activity of an HMA/pracinostat combination in heavily treated patients with higher‐risk MDS and in acute myeloid leukaemia (AML) (Quintás‐Cardama et al , ; Garcia Manero et al , ).…”

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confidence: 99%

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A phase II study of addition of pracinostat to a hypomethylating agent in patients with myelodysplastic syndromes who have not responded to previous hypomethylating agent therapy

et al. 2019

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Summary Hypomethylating agents (HMAs) are standard of care for higher‐risk myelodysplastic syndromes (MDS). However, less than half of patients achieve objective responses and most eventually lose their response. Pracinostat is a pan‐histone deacetylase inhibitor with demonstrated activity in advanced myeloid malignancies. This phase II study explored the benefit of adding pracinostat to HMAs in MDS patients who did not respond to single‐agent HMA treatment. The goal was to estimate the clinical improvement rate [complete remission (CR), marrow CR, partial response (PR) and haematological improvement]. Group 1 included patients with primary/secondary HMA failures; Group 2 included those who did not achieve response but had stable disease (SD) after single‐agent HMAs. Forty‐five patients (39 Group 1, 6 Group 2) received a median of 3 cycles. Among all patients, 1 (2%) had CR, 7 (16%) had marrow CR and 18 (40%) had SD; disease progression occurred in 3 (7%). Median overall survival was 5·7/5·6 months for Group 1/2. Grade ≥3 adverse events occurred in 38 patients (84%) leading to treatment discontinuation in 12 (33%). Adding pracinostat to HMAs did not improve outcomes in patients previously treated with HMAs. Frequent dose modifications/early discontinuation resulted in suboptimal drug exposure. A reduced pracinostat dose may improve tolerability and efficacy.

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“…The hydroxamic acid‐based compounds are among those HDAC inhibitors, which received the widely studies (Mottamal, Zheng, Huang, & Wang, ). Among them, Pracinostat 1 is a promising compound, which has been granted breakthrough therapy designation by FDA for the treatment of patients with newly diagnosed acute myelocytic leukemia (AML) who are ≥75 years of age or unfit for intensive chemotherapy(Abaza et al., ; Garcia‐Manero et al., ). Currently, Pracinostat is undergoing phase III clinical trials (Abaza et al., ; Ganai, ; Garcia‐Manero et al., ; Kang et al., ; Novotny‐Diermayr et al., ).…”

Section: Introductionmentioning

confidence: 99%

Minor structural modifications to Pracinostat produce big changes in its biological responses

et al. 2019

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A series of compounds similar to Pracinostat that contained benzimidazole ring and N-hydroxyacrylamide attached at 5-or 6-position were designed, synthesized, and evaluated as HDAC inhibitors. It was interesting to find that the corresponding derivative 1 with N-hydroxyacrylamide attached at 5-position was a potent HDAC inhibitor while the others at 6-position were not. This is the first time to demonstrate the position difference plays important role in the HDAC inhibitory activities of the cinnamic hydroxamates. K E Y W O R D S HDAC inhibitors, histone deacetylases, hydroxamic acids, Pracinostat, synthesisThis is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

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Phase 1 dose escalation multicenter trial of pracinostat alone and in combination with azacitidine in patients with advanced hematologic malignancies

Cited by 47 publications

References 35 publications

Evaluation of the bioequivalence and food effect on the bioavailability of CC-486 (oral azacitidine) tablets in adult patients with cancer

Evaluation of the bioequivalence and food effect on the bioavailability of CC-486 (oral azacitidine) tablets in adult patients with cancer

A phase II study of addition of pracinostat to a hypomethylating agent in patients with myelodysplastic syndromes who have not responded to previous hypomethylating agent therapy

Minor structural modifications to Pracinostat produce big changes in its biological responses

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