Safety and Efficacy of Bromodomain and Extra-Terminal Inhibitors for the Treatment of Hematological Malignancies and Solid Tumors: A Systematic Study of Clinical Trials

Sun, Ying; Han, Jie; Wang, Zhanzhao; Li, Xuening; Sun, Yihong; Hu, Zhenbo

doi:10.3389/fphar.2020.621093

Cited by 82 publications

(94 citation statements)

References 52 publications

(42 reference statements)

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“…Among iBETs, BMS-986158 has notable pharmacodynamics profile with a longer half-life. [ 721 ]. RO6870810 (also termed RG6146 and TEN-0) is a novel iBET, resembling the JQ1 class.…”

Section: Myc Inhibitorsmentioning

confidence: 99%

MYC: a multipurpose oncogene with prognostic and therapeutic implications in blood malignancies

et al. 2021

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MYC oncogene is a transcription factor with a wide array of functions affecting cellular activities such as cell cycle, apoptosis, DNA damage response, and hematopoiesis. Due to the multi-functionality of MYC, its expression is regulated at multiple levels. Deregulation of this oncogene can give rise to a variety of cancers. In this review, MYC regulation and the mechanisms by which MYC adjusts cellular functions and its implication in hematologic malignancies are summarized. Further, we also discuss potential inhibitors of MYC that could be beneficial for treating hematologic malignancies.

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“…Among iBETs, BMS-986158 has notable pharmacodynamics profile with a longer half-life. [ 721 ]. RO6870810 (also termed RG6146 and TEN-0) is a novel iBET, resembling the JQ1 class.…”

Section: Myc Inhibitorsmentioning

confidence: 99%

MYC: a multipurpose oncogene with prognostic and therapeutic implications in blood malignancies

et al. 2021

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“…In relation to this, sensitivity to treatment with the BET inhibitor JQ1 has been recently shown in two human erythroleukemia cell lines edited to incorporate a previously described homozygous STAG2 mutation (Antony et al, 2020). Both BRD4 and NIPBL are indispensable for the proper hematopoietic development (Dey et al, 2019;Mazzola et al, 2020) and both have been related with hematological defects: it has been detected an increased incidence of thrombocytopenia in CdLS patients (Lambert et al, 2011) and in clinical trials where BRD4 inhibitors have been essayed to treat diverse types of cancer, a prominent highly common toxic effect is thrombocytopenia (reviewed in (Sun et al, 2020)). In all these models where BRD4 and NIPBL functions converge in common regulatory processes, it might be interesting to investigate the effect of interfering with their interaction.…”

Section: Nipbl-brd4 Interactionmentioning

confidence: 99%

BETting on a Transcriptional Deficit as the Main Cause for Cornelia de Lange Syndrome

García-Gutiérrez

García-Domínguez

2021

Front. Mol. Biosci.

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Cornelia de Lange Syndrome (CdLS) is a human developmental syndrome with complex multisystem phenotypic features. It has been traditionally considered a cohesinopathy together with other phenotypically related diseases because of their association with mutations in subunits of the cohesin complex. Despite some overlap, the clinical manifestations of cohesinopathies vary considerably and, although their precise molecular mechanisms are not well defined yet, the potential pathomechanisms underlying these diverse developmental defects have been theoretically linked to alterations of the cohesin complex function. The cohesin complex plays a critical role in sister chromatid cohesion, but this function is not affected in CdLS. In the last decades, a non-cohesion-related function of this complex on transcriptional regulation has been well established and CdLS pathoetiology has been recently associated to gene expression deregulation. Up to 70% of CdLS cases are linked to mutations in the cohesin-loading factor NIPBL, which has been shown to play a prominent function on chromatin architecture and transcriptional regulation. Therefore, it has been suggested that CdLS can be considered a transcriptomopathy. Actually, CdLS-like phenotypes have been associated to mutations in chromatin-associated proteins, as KMT2A, AFF4, EP300, TAF6, SETD5, SMARCB1, MAU2, ZMYND11, MED13L, PHIP, ARID1B, NAA10, BRD4 or ANKRD11, most of which have no known direct association with cohesin. In the case of BRD4, a critical highly investigated transcriptional coregulator, an interaction with NIPBL has been recently revealed, providing evidence on their cooperation in transcriptional regulation of developmentally important genes. This new finding reinforces the notion of an altered gene expression program during development as the major etiological basis for CdLS. In this review, we intend to integrate the recent available evidence on the molecular mechanisms underlying the clinical manifestations of CdLS, highlighting data that favors a transcription-centered framework, which support the idea that CdLS could be conceptualized as a transcriptomopathy.

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“…BET inhibitors also demonstrated antiangiogenic effects in FP-RMS xenograft models [116]. In adult clinical trials BET inhibitors have had limited efficacy and are not yet FDA-approved [117]. There is an ongoing trial evaluating the BET inhibitor BMS-986158 in children but results are not yet available (NCT03936465).…”

Section: Other Targeted Agentsmentioning

confidence: 99%

Prioritization of Novel Agents for Patients with Rhabdomyosarcoma: A Report from the Children’s Oncology Group (COG) New Agents for Rhabdomyosarcoma Task Force

Pacenta

Allen‐Rhoades

Langenau

et al. 2021

JCM

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Rhabdomyosarcoma is the most common soft tissue sarcoma diagnosed in children and adolescents. Patients that are diagnosed with advanced or relapsed disease have exceptionally poor outcomes. The Children’s Oncology Group (COG) convened a rhabdomyosarcoma new agent task force in 2020 to systematically evaluate novel agents for inclusion in phase 2 or phase 3 clinical trials for patients diagnosed with rhabdomyosarcoma, following a similar effort for Ewing sarcoma. The task force was comprised of clinicians and basic scientists who collectively identified new agents for evaluation and prioritization in clinical trial testing. Here, we report the work of the task force including the framework upon which the decisions were rendered and review the top classes of agents that were discussed. Representative agents include poly-ADP-ribose polymerase (PARP) inhibitors in combination with cytotoxic agents, mitogen-activated protein kinase (MEK) inhibitors in combination with type 1 insulin-like growth factor receptor (IGFR1) inhibitors, histone deacetylase (HDAC) inhibitors, and novel cytotoxic agents.

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Safety and Efficacy of Bromodomain and Extra-Terminal Inhibitors for the Treatment of Hematological Malignancies and Solid Tumors: A Systematic Study of Clinical Trials

Cited by 82 publications

References 52 publications

MYC: a multipurpose oncogene with prognostic and therapeutic implications in blood malignancies

MYC: a multipurpose oncogene with prognostic and therapeutic implications in blood malignancies

BETting on a Transcriptional Deficit as the Main Cause for Cornelia de Lange Syndrome

Prioritization of Novel Agents for Patients with Rhabdomyosarcoma: A Report from the Children’s Oncology Group (COG) New Agents for Rhabdomyosarcoma Task Force

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