Delving into the Latest Updates on Mocetinostat Dihydrobromide with Synapse

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

Mocetinostat, Mocetinostat dihydrobromide (USAN), 726169-73-9

+ [4]

Target

HDAC1 x HDAC11 x HDAC2 x HDAC3 x HDAC8

Action

inhibitors

Mechanism

HDAC1 inhibitors(Histone deacetylase 1 inhibitors), HDAC11 inhibitors(histone deacetylase 11 inhibitors), HDAC2 inhibitors(Histone deacetylase 2 inhibitors)

Therapeutic Areas

NeoplasmsOther Diseases

Active Indication

Rhabdomyosarcoma

Inactive Indication

Acute Myeloid LeukemiaAdvanced cancerAdvanced Malignant Solid Neoplasm+ [17]

Originator Organization

Mirati Therapeutics, Inc.

Active Organization

Mirati Therapeutics, Inc.

Inactive Organization

New York University School of Medicine

NYU Langone Health

Drug Highest PhasePhase 1

First Approval Date-

RegulationOrphan Drug (United States)

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Structure/Sequence

Molecular FormulaC23H22Br2N6O

InChIKeyACPWZKZFDFBALX-UHFFFAOYSA-N

CAS Registry944537-89-7

This phase I trial studies the side effects and best dose of mocetinostat when given together with vinorelbine to see how well it works in treating children, adolescents, and young adults with rhabdomyosarcoma that has spread to nearby tissues or lymph nodes and cannot be removed by surgery (locally advanced unresectable) or has spread to other places in the body (metastatic), and does not respond to treatment (refractory) or has come back (relapsed). Mocetinostat may stop the growth of tumor cells by blocking some of the enzymes needed for cell growth. Drugs used in chemotherapy, such as vinorelbine, work in different ways to stop the growth of tumor cells, either by killing the cells, by stopping them from dividing, or by stopping them from spreading. Giving mocetinostat and vinorelbine may work better in treating children, adolescents, and young adults with rhabdomyosarcoma compared to vinorelbine alone.

Start Date14 May 2020

Sponsor / Collaborator

Jonsson Comprehensive Cancer Center

[+2]

NCT03565406

/ TerminatedPhase 1IIT

A Phase 1b Study of the Selective HDAC Inhibitor Mocetinostat in Combination With Ipilimumab and Nivolumab in Patients With Unresectable Stage III or Stage IV Melanoma

This is a Phase 1b, open-label, dose-escalation cohort study. The study will consist of a dose escalation assessment of the safety and tolerability of Mocetinostat administered concurrently in combination with ipilimumab and nivolumab to patients with advanced melanoma. Treatment will be divided into induction and maintenance phases. It is anticipated that this clinical study will enable selection of the RP2D and dose schedule of this 3-drug combination for further clinical testing. The trial will include an assessment of the pharmacodynamic activity of Mocetinostat administered in combination with ipilimumab and nivolumab.

Start Date25 Apr 2018

Sponsor / Collaborator

NYU Langone Health

NCT02993991

/ WithdrawnPhase 1IIT

Pre-operative Mocetinostat (MGCD0103) and Durvalumab (MEDI4736) (PRIMED) for Squamous Cell Carcinoma of the Oral Cavity

This is a Phase 1 Window of Opportunity study to evaluate the pharmacodynamic and immune effects of pre-operative therapy with Mocetinostat and Durvalumab on patients with squamous cell carcinoma of the oral cavity.

Start Date10 Oct 2017

Sponsor / Collaborator

University Health Network

[+2]

100 Clinical Results associated with Mocetinostat Dihydrobromide

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100 Translational Medicine associated with Mocetinostat Dihydrobromide

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100 Patents (Medical) associated with Mocetinostat Dihydrobromide

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306

Literatures (Medical) associated with Mocetinostat Dihydrobromide

01 Apr 2025·World Journal of Oncology

Comprehensive Investigation of a Tyrosine Kinase Inhibitor-Resistant Gene Zeste White 10 in Hepatocellular Carcinoma

Article

Author: Tang, Yu Lu ; Chen, Gang ; He, Rong Quan ; Dang, Yi Wu ; Su, Qin Yan ; He, Han ; Chi, Bang Teng ; Huang, Qing Ling ; Li, Shi De ; Zhang, Guan Lan ; Lin, Qian

Background:

Tyrosine kinase inhibitors (TKIs) are first-line therapies for hepatocellular carcinoma (HCC), but the drug resistance restricts the long-term clinical outcomes. This study aimed to investigate the expression patterns and possible clinical significance of a TKI-resistant gene zeste white 10 (ZW10) in HCC.

Methods:

Clustered regularly interspaced short palindromic repeats (CRISPR) screening was conducted to obtain TKI-resistant genes. Pan-cancer analysis was employed to analyze the expression landscape of the critical TKI-resistant gene ZW10. Transcriptional expression data for ZW10 were obtained from 76 centers, including 3,312 HCC samples and 2,703 noncancerous tissues. A summary receiver operating characteristic (SROC) curve was built to evaluate ZW10 expression characteristics in HCC. Unpaired two-sample Wilcoxon method was conducted to analyze ZW10 expression levels in HCC of various etiologies. Univariate Cox method was employed to assess the prognostic value of ZW10. Moreover, the gene function within HCC cell lines, the TKI treatment responses, key pathways, and tumor microenvironment of ZW10 were bioinformatically investigated. Drug prediction and molecular docking techniques were used to explore the potency of ZW10 as a novel therapeutic target.

Results:

The abundance of small guide RNA (sgRNA) corresponding to ZW10 gene was decreased in the whole genome CRISPR knockout library (LogFC = -1.19), indicating that ZW10 may participate in TKI resistance. The differential expression landscape of ZW10 was found in various malignancies including HCC, which was associated with poorer prognosis. Pooled standardized mean difference (SMD) of ZW10 mRNA expression was 0.47 (95% confidence interval (CI): 0.32 - 0.63), the area under SROC was 0.76 (95% CI: 0.72 - 0.79), the sensitivity was 0.63 (95% CI: 0.53 - 0.72), and the specificity was 0.77 (95% CI: 0.67 - 0.84). ZW10 was investigated significant for the growth of HCC cells. Nucleocytoplasmic transport was the possible pathway that ZW10 involved. High level of ZW10 was reversely associated with TKI responses and the abundance of immune cell infiltration. Mocetinostat and capecitabine were predicted to be the potential inhibitors targeting ZW10 with a minimum binding energy of -8.2 and -7.1 kcal/mol, respectively.

Conclusions:

ZW10 is considered a TKI-resistant and tumor-supportive gene, which is also a promising novel prognostic biomarker for HCC or a therapeutic target for overcoming TKI resistance.

01 Mar 2025·JOURNAL OF INVESTIGATIVE MEDICINE

Investigation of the synergic effect of mocetinostat and capecitabine in a triple-negative breast neoplasms mouse model

Article

Author: Eroğlu, Onur ; Kaya Çakir, Hacer

Combined administration of two or more drugs is emerging as a new strategy in triple-negative breast neoplasms. This is the first study to investigate the combination of the histone deacetylase inhibitor mocetinostat and the antimetabolite drug capecitabine in triple-negative mammary neoplasms in a preclinical mouse model. Thirty-five female mice were grouped into the control group, capecitabine group, mocetinostat group, and combined drugs group. At the end of the experimental period, body weight, and tumor weight were measured and tumor tissue and lung tissue were histologically examined. The results showed that the body weight of mice in the drug-treated groups was reduced by about 18%. Tumor weights were also reduced by 21% in the mocetinostat group, 27.5% in the capecitabine group, and 45% in the combined group. The combination of mocetinostat and capecitabine decreased the formation of tumors and metastases in lung tissue. In summary, the combination of mocetinostat and capecitabine was more effective than either drug alone in reducing the size of triple-negative breast neoplasms in a mouse model.

01 Mar 2025·VIROLOGY

A high-throughput, microplate reader-based method to monitor in vitro HIV latency reversal in the absence of flow cytometry

Article

Author: Nkwelle, Chantal Emade ; Esemu, Seraphine N ; Ndip, Roland N ; Liang, Kimberly ; Ntie-Kang, Fidele ; Tietjen, Ian ; Cassel, Joel ; Salvino, Joseph M ; Stephens, Unique ; Montaner, Luis J

J-Lat cells are derivatives of the Jurkat CD4⁺ T cell line that contain a non-infectious, inducible HIV provirus with a GFP tag. While these cells have substantially advanced our understanding of HIV latency, their use by many laboratories in low and middle-income countries is restricted by limited access to flow cytometry. To overcome this barrier, we describe a modified J-Lat assay using a standard microplate reader that detects HIV-GFP expression following treatment with latency-reversing agents (LRAs). We show that HIV reactivation by control LRAs like prostratin and romidepsin is readily detected with dose dependence and with significant correlation and sensitivity to standard flow cytometry. For example, 10 μM prostratin induced a 20.1 ± 3.3-fold increase in GFP fluorescence in the microplate reader assay, which corresponded to 64.2 ± 5.0% GFP-positive cells detected by flow cytometery. Similarly, 0.3 μM prostratin induced a 1.7 ± 1.2-fold increase compared to 8.7 ± 5.7% GFP-positive cells detected. Using this method, we screen 79 epigenetic modifiers and identify CUDC-101, molibresib, and quisinostat as novel LRAs. This microplate reader-based method offers accessibility to researchers in resource-limited regions to work with J-Lat cells and more actively participate in global HIV cure research efforts.

2

News (Medical) associated with Mocetinostat Dihydrobromide

06 Feb 2008

·www.biospace.com

MethylGene Opts-Out of Collaboration with EnVivo Pharmaceuticals, Inc.

Montreal, Quebec and Watertown, Massachusetts. February 6, 2008 - MethylGene Inc. (TSX:MYG) and EnVivo Pharmaceuticals today announced that MethylGene has exercised its right to opt-out of further funding in its collaboration with EnVivo signed in February 2005. EnVivo will continue to research and develop histone deacetylase (HDAC) inhibitors for neurodegenerative disorders such as Huntington’s, Alzheimer’s and Parkinson’s diseases under license from MethylGene. A lead compound has been identified during the collaboration and designated as a clinical candidate by EnVivo. MethylGene will receive royalties on net sales of any approved product as well as a share of any sublicense income from future partnerships EnVivo may enter into with other companies for neurodegenerative programs. “The collaboration with EnVivo has been successful in leveraging our library of HDAC inhibitors beyond oncology. A lead candidate has been identified and we expect EnVivo will move this compound into clinical trials later this year. MethylGene has decided to exercise its right to opt out of the collaboration at the development stage for this non-core indication in order to strategically focus resources on our oncology development programs and other preclinical programs,” said Donald F. Corcoran, President and Chief Executive Officer of MethylGene. “We wish EnVivo well with the program and look forward to the opportunity to participate in the upside potential.” “The collaboration has been very productive and has provided us with a rich base from which we can move into several of the neurodegenerative diseases,” added Kees Been, President and Chief Executive Officer of EnVivo. “We look forward to advancing the lead compound towards clinical trials later this year. This would be the first brain-penetrant orally-available HDAC inhibitor that is being pursued for use as a cognition enhancing agent in neurodegenerative diseases with a potential for disease modification.” About MethylGene MethylGene Inc. (TSX: MYG) is a publicly-traded biopharmaceutical company focused on the discovery, development and commercialization of novel therapeutics for cancer. The Company's lead product, MGCD0103, is an oral isotype-selective HDAC inhibitor presently in multiple clinical trials for solid tumors and hematological malignancies, including Phase II monotherapy and Phase I and Phase II combination trials with Vidaza(R), Gemzar(R) and Taxotere(R). MGCD265 is an oral kinase inhibitor targeting the c-Met, Tie-2, Ron and VEGF receptor tyrosine kinases. In addition, MethylGene’s preclinical programs include: MGCD290 an HDAC inhibitor in combination with azoles for fungal infections and a sirtuins program for cancer. MethylGene's development and commercialization partners include Pharmion Corporation, Taiho Pharmaceutical and EnVivo Pharmaceuticals. Please visit our website at About EnVivo Pharmaceuticals EnVivo Pharmaceuticals (located in Watertown, MA) is a biopharmaceutical company dedicated to discovering and developing small molecule therapeutics for disorders of the central nervous system (CNS), currently focusing on Alzheimer’s disease, Parkinson’s disease, Huntington’s disease, and cognition. The Company’s lead program, a Nicotinic Acetylcholine Receptor Agonist Program for cognition disorders in Alzheimer’s disease and Schizophrenia, has completed Phase I clinical testing. The Company’s preclinical programs include a Histone Deacetylase inhibitor (HDACi) program for Huntington’s disease, a Gamma Secretase Modulator program, and a PDE10 inhibitor program. For more information about EnVivo, please visit Investor Relations Contacts: MethylGene Inc. Rhonda Chiger Rx Communications Group, LLC Phone: 917-322-2569 rchiger@rxir.com Donald F. Corcoran President & CEO MethylGene Inc. Phone: 514-337-3333 ext. 373 mctavishk@methylgene.com EnVivo Pharmaceuticals Inc. Kees Been President & CEO EnVivo Pharmaceuticals Inc. Phone: 617-225-4250 kbeen@envivopharma.com

CollaborateSmall molecular drugLicense out/in

15 Dec 2006

·www.biospace.com

MethylGene Will Not Pursue Additional Cinical Trials For MG98; Company To Increase Investment In HDAC And Kinase 'c-MET' Small Molecule Programs

Montreal, Quebec. December 15, 2006 – MethylGene Inc. (TSX: MYG) today announced that based on recent R&D successes in its small molecule oncology programs and a strategic review of its cancer pipeline, it will not pursue additional clinical trials for MG98, its second generation antisense compound targeting DNA methyltransferase. This decision is made with its North American co-development partner for the compound, MGI PHARMA, INC. The companies have agreed to seek alternative development partners or arrangements for the MG98 program. MethylGene will continue to focus its clinical development investment in more commercially attractive alternatives such as MGCD0103, its oral isotype-selective histone deacetylase (HDAC) inhibitor which is currently in Phase II monotherapy and Phase I/II combination trials; and MGCD265, its recently selected oral, multi-targeted kinase (c-MET) clinical candidate. The company will also continue to concentrate its efforts in other HDAC programs including MG3290, an HDAC inhibitor to overcome antifungal resistance to azoles, and HDAC inhibitors for Huntington’s disease for which clinical candidates and potential Investigational New Drug (IND) applications are expected in 2007. “We believe this decision along with the positive data recently disclosed at ASH for MGCD0103 and the selection of our multi-targeted kinase (c-MET) clinical candidate will enhance shareholder value as we build upon the positive momentum achieved to date.” commented Donald F. Corcoran, President and Chief Executive Officer, MethylGene. “While we are encouraged by the positive data reported on MG98 at ASCO in June, prioritization of our pipeline is key to success and it is important to allocate resources to the most promising and commercially attractive compounds and activities. We hope to attract new partners or arrangements for MG98, where the compound will be a priority and may advance based on its own merits.” By not initiating additional MG98 clinical trials, approximately $3 million will be reallocated to these other programs in 2007 and 2008 and the company will still maintain its forecast of sufficient cash resources into the fourth quarter of 2008. No significant financial contribution from MGI PHARMA, INC. was expected over this period. About MethylGene MethylGene is a publicly-traded biopharmaceutical company focused on the discovery, development and commercialization of novel therapeutics in cancer. The cancer product candidate MGCD0103 is currently in clinical development with partners Pharmion Corporation and Taiho Pharmaceutical Co., Ltd. MethylGene has an exclusive license agreement with Merck & Co. for the development and commercialization of small molecule beta-lactamase inhibitors to overcome antibiotic resistance. MethylGene has partnered its non-oncology HDAC program for neurodegenerative diseases with EnVivo Pharmaceuticals. MethylGene has a portfolio of preclinical programs for its multi-targeted kinase (c-MET) and histone deacetylase (HDAC) inhibitors for both oncology and non-oncology indications, and continues to seek partnering opportunities in these areas. Please visit our website at Certain statements contained in this news release, other than statements of fact that are independently verifiable at the date hereof, may constitute forward-looking statements. Such statements, based as they are on the current expectations of management of MethylGene, inherently involve numerous risks and uncertainties, known and unknown, many of which are beyond MethylGene's control. These risks and uncertainties could cause future results, performance or achievements to differ significantly from the results, performance or achievements expressed or implied by such forward-looking statements. Such results, performance or achievements include, but are not limited to, the timing and effects of regulatory action; the continuation of collaborations; the results of clinical trials; the timing of enrollment or completion of clinical trials; the success, efficacy or safety of MGCD0103, MGCD265 or MG98; and the relative success or the lack of success in developing and gaining regulatory approval and/or market acceptance for any compound or new product including MGCD0103, MGCD265 and MG98. Such risks include, but are not limited to, the impact of general economic conditions, economic conditions in the pharmaceutical industry, changes in the regulatory environment in the jurisdictions in which MethylGene does business, stock market volatility, fluctuations in costs, expectations with respect to our intellectual property position and our ability to protect our intellectual property and operate our business without infringing upon the intellectual property rights of others, changes in the competitive landscape including changes in the standard of care for the various indications in which MethylGene is involved, and changes to the competitive environment due to consolidation, as well as other risks, which you are urged to read, as described in MethylGene's Annual Information Form for the fiscal year ending December 31 2005, under the heading "risk factors,” that can be found at Consequently, actual future results may differ materially from the anticipated results expressed in the forward-looking statements. The reader should not place undue reliance on the forward-looking statements included in this presentation. These statements speak only as an update on the date they are made and MethylGene is under no obligation to revise such statements as a result of any event, circumstance or otherwise except in accordance with law. Investor Relations Contacts: Rhonda Chiger Donald F. Corcoran Rx Communications Group, LLC President & CEO Phone: 917-322-2569 MethylGene Inc. rchiger@rxir.com Phone: 514-337-3333 ext. 373 mctavishk@methylgene.com >>> Discuss This Story

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100 Deals associated with Mocetinostat Dihydrobromide

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External Link

KEGG	Wiki	ATC	Drug Bank
D09357	-	-	DB11830

R&D Status

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
metastatic non-small cell lung cancer	Phase 2	United States	Mirati Therapeutics, Inc.	07 Nov 2016
Advanced cancer	Phase 2	United States	Mirati Therapeutics, Inc.	01 Jun 2016
Advanced Malignant Solid Neoplasm	Phase 2	United States	Mirati Therapeutics, Inc.	01 Jun 2016
Metastatic urothelial carcinoma	Phase 2	United States	Mirati Therapeutics, Inc.	01 Oct 2014
Urothelial Carcinoma of the Urinary Bladder	Phase 2	United States	Mirati Therapeutics, Inc.	01 Oct 2014
Follicular Lymphoma	Phase 2	United States	Mirati Therapeutics, Inc.	01 Oct 2007
Hodgkin's Lymphoma	Phase 2	United States	Mirati Therapeutics, Inc.	01 Oct 2007
Non-Hodgkin's lymphoma refractory	Phase 2	United States	Mirati Therapeutics, Inc.	01 Oct 2007
Chronic lymphocytic leukaemia refractory	Phase 2	United States	Mirati Therapeutics, Inc.	01 Jan 2007
Chronic lymphocytic leukaemia refractory	Phase 2	Canada	Mirati Therapeutics, Inc.	01 Jan 2007

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Clinical Result

Indication

Phase

Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT02954991 (MRTX-500, CTgov)	Phase 2	metastatic non-small cell lung cancer	161	Glesatinib+nivolumab	yivljflpsy(vhtxnmpfyu) = dkoejohzqh xfyarkrdba (wnfqgtfxgt, jnocfuejwn - otoxeivrxw) View more	-	22 Apr 2024
NCT02282358 (CTgov)	Phase 1/2	Follicular Lymphoma \| Diffuse large B-cell lymphoma recurrent	7	Mocetinostat	ixcsttslzm(hnrfybqjat) = wagclrgkro boyttuwerf (vssqlypajk, gexisakmbp - rzstnivdqt) View more	-	08 Mar 2024
NCT04299113 (ASCO2022) Manual	Phase 1	Rhabdomyosarcoma	7	vinorelbine+mocetinostat	ziejyintwg(psiymiszdc) = The only grade 3 or 4 treatment related AEs were neutropenia, lymphopenia and anemia. lsdxcerzvh (dzfubrftih )	Positive	02 Jun 2022
NCT02236195 (Pubmed \| Cancer) Manual	Phase 2	Locally Advanced Urothelial Carcinoma	17	Mocetinostat	jbuvjgrjeq(bcfxnrdyjr) = nausea (77%) and fatigue (71%) awrtiuvsee (mpsnzqckrg )	Negative	15 Feb 2019
NCT02303262 (SARC018, CTgov)	Phase 2	Leiomyosarcoma	20	Mocetinostat+Gemcitabine	oorhcpdkre = hdziwrjnss jlpzcbzcme (lutzhsguds, nentjqgsfd - biinltascv) View more	-	29 Jan 2019
NCT00372437 (Pubmed) Manual	Phase 1/2	HR-positive/HER2-low Solid Tumors \| Pancreatic Cancer	48	gemcitabine+mocetinostat (Phase I)	pbitikczwx(kjgoiatibt) = Grade ≥ 3 treatment-related adverse events (AEs) were reported by 81% of all patients, the most frequent being fatigue (38%) and thrombocytopenia (19%). oluuqkmxys (ltmlhepsuq ) View more	Negative	01 Feb 2018
NCT00372437 (Pubmed) Manual	Phase 1/2	HR-positive/HER2-low Solid Tumors \| Pancreatic Cancer	48	gemcitabine+mocetinostat (Phase II)		Negative	01 Feb 2018
NCT00324220 (ASCO2013)	Phase 2	Myelodysplastic Syndromes	20	Mocetinostat	jixbgkyaub(hevsrurrqj) = gedfqjzijy rnfdungpuu (oreqvlmmxc )	-	20 May 2013
NCT00359086 (ASCO2013)	Phase 2	Diffuse Large B-Cell Lymphoma	69	Mocetinostat	xpoooafmjf(gcmrlovhph) = 4 each prkshpdmfw (bnskripljn ) View more	-	20 May 2013
NCT00358982 (Pubmed \| Lancet Oncol)	Phase 2	Relapsing classical Hodgkin lymphoma	51	Mocetinostat 85 mg	lpollgpran(ftjcnftltk) = gwxmuecikl gbbwjgwzpf (gqybgcqump )	Positive	01 Dec 2011
Trial 008 (ASCO2010)	Phase 2	Recurrent Follicular Lymphoma	28	MGCD0103	vhkhxnnmbh(cqneczistn) = Pericardial SAEs were observed in other MGCD0103 trials and hence the studies were voluntarily suspended for further investigation. In total, 437 patients have been treated with MGCD0103. There were 19 patients (4.3%) with a SAE where one of the listed terms involved the pericardium. Patients with Hodgkin Lymphoma were more likely (9.5%) to experience a pericardial SAE as compared to other diagnosis, while patients with solid tumors had an incidence of only 0.9%. Most pericardial SAEs (14) occurred during Cycle 1 of treatment. There were no clear relationships with the starting dose level, exposure, cumulative dose, drug lots, prior history of chest pain/arrhythmia or other cardiac diseases, prior therapies, prior mediastinal or thoracic radiotherapy, presence of mediastinal lesions, PD markers of HDAC activity or inflammation, low albumin levels at baseline, pneumonia, sepsis or infection. Statistically significant associations were found with patients who had a history of pericardial disease, presence of lung lesions, and on-study reports of chest pain or pleural effusion. tdbwhvemkt (cvramekmyg )	-	20 May 2010