CUDC-907 in relapsed/refractory diffuse large B-cell lymphoma, including patients with MYC-alterations: results from an expanded phase I trial

Oki, Yasuhiro; Kelly, Kevin R.; Flinn, Ian W.; Patel, Manish R.; Gharavi, Robert; Ma, Anna; Parker, Jefferson; Hafeez, Amir; Tuck, David; Younes, Anas

doi:10.3324/haematol.2017.172882

Cited by 101 publications

(88 citation statements)

References 46 publications

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“…Of note, the sensitivity of CLL cells to BCL‐2 inhibitors shown in these figures is consistent with previous reports . These data suggest that CLL cells are highly sensitive to CUDC‐907 at concentrations that are within the expected therapeutic levels that can be achieved in vivo, which range from 27 to 70 ng/mL …”

Section: Resultssupporting

confidence: 91%

“…The simultaneous inhibition of HDAC and PI3K signalling has been previously shown to promote the inhibition on tumour cell growth and induction of apoptosis in different cancers, including hematopoietic malignancies . Indeed, CUDC‐907 has recently been shown to be safe and effective in patients with relapsed/refractory DLBCL . In hematopoietic cells, PI3K signalling activation is normally mediated by the p110δ isoform of PI3K, and it has been suggested that its inhibition has therapeutic value for CLL patients .…”

Section: Discussionmentioning

confidence: 99%

“…CUDC‐907 is a dual inhibitor targeting class I PI3Ks as well as class I and II HDACs, and has been reported to induce apoptosis in various cancer cells in vitro . Recent clinical trials showed the safety, tolerability, and a promising activity of CUDC‐907 in patients with relapsed or refractory lymphoma or multiple myeloma, or DLBCL, particularly in MYC mutant malignancies . In this study, we investigated the efficacy of CUDC‐907 in CLL cells and found that it effectively disrupted multiple pro‐survival signalling pathways to overcome the microenvironment protection and induce apoptosis.…”

Section: Introductionmentioning

confidence: 97%

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CUDC‐907 blocks multiple pro‐survival signals and abrogates microenvironment protection in CLL

Chen

Peubez

Smith

et al. 2018

J Cellular Molecular Medi

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CUDC‐907, a dual PI3K/HDAC inhibitor, has been proposed to have therapeutic potential in hematopoietic malignancies. However, the molecular mechanisms of its effects in chronic lymphocytic leukaemia (CLL) remain elusive. We show that CLL cells are sensitive to CUDC‐907, even under conditions similar to the protective microenvironment of proliferation centres. CUDC‐907 inhibited PI3K/AKT and HDAC activity, as expected, but also suppressed RAF/MEK/ERK and STAT3 signalling and reduced the expression of anti‐apoptotic BCL‐2 family proteins BCL‐2, BCL‐xL, and MCL‐1. Moreover, CUDC‐907 downregulated cytokines BAFF and APRIL and their receptors BAFFR, TACI, and BCMA, thus blocking BAFF‐induced NF‐κB signalling. T cell chemokines CCL3/4/17/22 and phosphorylation of CXCR4 were also reduced by CUDC‐907. These data indicated that CUDC‐907 abrogates different protective signals and suggested that it might sensitize CLL cells to other drugs. Indeed, combinations of low concentrations of CUDC‐907 with inhibitors of BCL2, BTK, or the NF‐κB pathway showed a potent synergistic effect. Our data indicate that, apart from its known functions, CUDC‐907 blocks multiple pro‐survival pathways to overcome microenvironment protection in CLL cells. This provides a rationale to evaluate the clinical relevance of CUDC‐907 in combination therapies with other targeted inhibitors.

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Section: Resultssupporting

confidence: 91%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 97%

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CUDC‐907 blocks multiple pro‐survival signals and abrogates microenvironment protection in CLL

Chen

Peubez

Smith

et al. 2018

J Cellular Molecular Medi

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“…In particular, treatment with CUDC‐907 52 gave a reduction in MYC gene expression in MYC‐driven tumor model, whose overexpression has been reported to be among the worst prognostic factors in relapsed refractory diffuse large B‐cell lymphoma (DLBCL) . Dose escalation and expansion of CUDC‐907 52 in DLBCL and MYC‐altered disease, with and without the monoclonal antibody rituximab (25 patients received monotherapy treatment while 12 received the combination) (NCT 01742988) showed a median duration of the overall response of 11.2 months (of 13.6 months in MYC‐altered patients, 7.8 months in those with unknown MYC status, and 6.0 months in MYC unaltered patient), a durable antitumor activity (in particular in MYC‐altered patients) as well as a safety and tolerable profile . CUDC‐907 52 has been reported to downregulate FLT3 expression in AML cells.…”

Section: The Mtdl Approachmentioning

confidence: 99%

Epigenetic polypharmacology: A new frontier for epi‐drug discovery

Tomaselli

Lucidi

Rotili

et al. 2019

Medicinal Research Reviews

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Recently, despite the great success achieved by the so‐called “magic bullets” in the treatment of different diseases through a marked and specific interaction with the target of interest, the pharmacological research is moving toward the development of “molecular network active compounds,” embracing the related polypharmacology approach. This strategy was born to overcome the main limitations of the single target therapy leading to a superior therapeutic effect, a decrease of adverse reactions, and a reduction of potential mechanism(s) of drug resistance caused by robustness and redundancy of biological pathways. It has become clear that multifactorial diseases such as cancer, neurological, and inflammatory disorders, may require more complex therapeutic approaches hitting a certain biological system as a whole. Concerning epigenetics, the goal of the multi‐epi‐target approach consists in the development of small molecules able to simultaneously and (often) reversibly bind different specific epi‐targets. To date, two dual histone deacetylase/kinase inhibitors (CUDC‐101 and CUDC‐907) are in an advanced stage of clinical trials. In the last years, the growing interest in polypharmacology encouraged the publication of high‐quality reviews on combination therapy and hybrid molecules. Hence, to update the state‐of‐the‐art of these therapeutic approaches avoiding redundancy, herein we focused only on multiple medication therapies and multitargeting compounds exploiting epigenetic plus nonepigenetic drugs reported in the literature in 2018. In addition, all the multi‐epi‐target inhibitors known in literature so far, hitting two or more epigenetic targets, have been included.

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“…69 These data support further exploration of Ven + R-CHOP in a high-risk population of BCL2+ and DHL patients. Epigenetics-based treatments using BET bromodomain inhibition (BAY1238097 [NCT02369029], CPI-0610 [NCT01949883], OTX015[NCT01713582], and JQ1) and histone deacetylase inhibition (HDACi) are other avenues for these subtypes 20,70. Recently, the interim analysis of a phase II trial (NCT02753647) evaluating the efficacy and safety of the HDAC inhibitor chidamide in combination with R-CHOP in elderly, newly diagnosed DLBCL, showed ORR of 90.3% (CR 85.4%), 1-year PFS was 92.1%, and 1-year OS was 94.7%.…”

mentioning

confidence: 99%

Frontline treatment of diffuse large B‐cell lymphoma: Beyond R‐CHOP

Mondello

Mian

2019

Hematological Oncology

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Although the majority of patients with diffuse large B‐cell lymphoma (DLBCL) can be cured with the standard immunochemotherapy R‐CHOP, one‐third of them relapses with a dismal outcome in most cases. In the recent years, remarkable advances have been achieved based on the discovery of molecular genetics in DLBCL. In addition to the major cell‐of‐origin designations of germinal center B‐cell and activated B‐cell subtypes, next‐generation sequencing has unveiled the remarkable complexity of DLBCL and identified potential molecular targets for tailored therapies. Despite these findings, the current standard of care for DLBCL patients is still R‐CHOP, and optimization of frontline therapy remains an important goal. In this review, we summarize recent updates on the evolution of frontline therapies for DLBCL.

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CUDC-907 in relapsed/refractory diffuse large B-cell lymphoma, including patients with MYC-alterations: results from an expanded phase I trial

Cited by 101 publications

References 46 publications

CUDC‐907 blocks multiple pro‐survival signals and abrogates microenvironment protection in CLL

CUDC‐907 blocks multiple pro‐survival signals and abrogates microenvironment protection in CLL

Epigenetic polypharmacology: A new frontier for epi‐drug discovery

Frontline treatment of diffuse large B‐cell lymphoma: Beyond R‐CHOP

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