Delving into the Latest Updates on Domatinostat tosylate with Synapse

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

Domatinostat

Target

HDACs x KDM1A

Action

inhibitors

Mechanism

HDAC inhibitors(Histone deacetylase inhibitors), KDM1A inhibitors(Lysine-specific histone demethylase 1 inhibitors)

Therapeutic Areas

NeoplasmsInfectious DiseasesDigestive System Disorders+ [2]

Active Indication

Metastatic Merkel Cell CarcinomaGastrointestinal NeoplasmsMelanoma, Cutaneous Malignant

Inactive Indication

Bladder CancerBreast CancerColorectal Cancer+ [5]

Originator Organization

Takeda Pharmaceutical Co., Ltd.

Active Organization

4SC AG

Netherlands Cancer Insitute

Takeda Pharmaceutical Co., Ltd.

Inactive Organization

Merck KGaA

Drug Highest PhasePhase 2

First Approval Date-

Regulation-

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Structure/Sequence

Molecular FormulaC23H21N5O3S

InChIKeyPRXXYMVLYKJITB-IZZDOVSWSA-N

CAS Registry910462-43-0

View All Structures (2)

DONIMI is a phase 1b trial testing the combination of domatinostat + nivolumab or nivolumab monotherapy in IFN-gamma signature high patients and of domatinostat + nivolumab or domatinostat + nivolumab + ipilimumab in IFN-gamma signature low patients with de-novo or recurrent macroscopic stage III cutaneous or unknown primary melanoma.
The trial will include 45 stage III cutaneous or unknown primary melanoma patients with RECIST 1.1 measurable de-novo or recurrent disease (short axis lymph node metastasis ≥1.5cm).
NanoString IFN-gamma signature high patients will be randomized to be treated pre-surgically for 6 weeks with nivolumab (arm A; 10 patients) or domatinostat + nivolumab (arm B; 10 patients).
IFN-gamma signature low patients will be randomized to be treated pre-surgically for 6 weeks with domatinostat + nivolumab (arm C; 10 patients) or domatinostat + nivolumab + ipilimumab (arm D; 15 patients). Patients will be stratified according to center.
Post-surgery (starting at week 12), the patients will start with adjuvant nivolumab or pembrolizumab for 52 weeks according to institute's standard. BRAF V600E/K mutation positive patients with no pathologic response after neoadjuvant therapy may also receive adjuvant BRAF + MEK inhibition if commercially available and according to the patient's and the treating physician's decision.
Follow-up after the adjuvant therapy will be for 2 years, according to the institutes' standard.
Toxicity and pathologic response rates will be descriptive. In case of 2/5 or 4/10 patients not undergoing their lymph node dissection at week 6 +/- 1 week due to treatment related toxicity, this arm will be declared unfeasible.

Start Date07 Jan 2020

Sponsor / Collaborator

Netherlands Cancer Insitute

[+1]

100 Clinical Results associated with Domatinostat tosylate

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100 Translational Medicine associated with Domatinostat tosylate

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100 Patents (Medical) associated with Domatinostat tosylate

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41

Literatures (Medical) associated with Domatinostat tosylate

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

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.

28 Nov 2024·Journal of Medicinal Chemistry

Discovery of Novel 5-Cyano-3-phenylindole-Based LSD1/HDAC Dual Inhibitors for Colorectal Cancer Treatment

Article

Author: Dai, Wen-Jing ; Zhang, Meng-Yao ; Ban, Yi-Bo ; Li, Shi-Jie ; Zhou, Xiao-Xiao ; Shi, Xiao-Jing ; Xu, Yong-Tao ; Wang, Sai-Qi ; Zhang, Yi-Zhe ; Duan, Ying-Chao ; Zhu, Hui-Juan ; Zhou, Hui-Min ; Xu, Zhen ; Lu, Jia-Rui ; Zheng, Meng-Jie

The dual inhibition of histone lysine-specific demethylase 1 (LSD1) and histone deacetylase (HDAC) has emerged as a promising strategy for cancer therapy. In this study, we report the discovery of novel 5-cyano-3-phenylindole-based LSD1/HDAC dual inhibitors, evaluated through both in vitro and in vivo assays. Among these inhibitors, compound 20c was identified as particularly potent, exhibiting high inhibitory activity against LSD1 (IC₅₀ = 39.0 nM) and HDAC1/2/3/6/8 (IC₅₀ = 1.4, 1.0, 1.3, 2.9, and 16.0 nM, respectively). Compound 20c effectively modulated the expression of biomarkers associated with LSD1 and HDAC inhibition and demonstrated superior antiproliferative activity compared to SAHA and 4SC-202 across multiple colorectal cancer cell lines. Following pharmacokinetic studies, 20c was further assessed in HCT-116 and HT-29 xenograft mouse models. It demonstrated significantly enhanced antitumor efficacy compared to SAHA, without causing observable toxicity. These findings highlight the potential of LSD1/HDAC dual inhibitors for the treatment of malignant cancers.

01 Apr 2024·ESMO Open

Phase II trial of domatinostat (4SC-202) in combination with avelumab in patients with previously treated advanced mismatch repair proficient oesophagogastric and colorectal adenocarcinoma: EMERGE

Article

Author: Smyth, E ; Rao, S ; Terlizzo, M ; Kohoutova, D ; Fribbens, C ; Mansoor, W ; Cartwright, E ; Slater, S ; Turkes, F ; Starling, N ; Tran, A ; Chau, I ; Saffery, C ; Sanna, I ; Rana, I ; Zhitkov, O ; Aresu, M ; Smith, G ; Johnston, E W ; Cunningham, D

BACKGROUNDMost oesophagogastric adenocarcinomas (OGAs) and colorectal cancers (CRCs) are mismatch repair proficient (MMRp), responding poorly to immune checkpoint inhibition. We evaluated the safety and efficacy of domatinostat (histone deacetylase inhibitor) plus avelumab (anti-PD-L1 antibody) in patients with previously treated inoperable, advanced/metastatic MMRp OGA and CRC.PATIENTS AND METHODSEligible patients were evaluated in a multicentre, open-label dose escalation/dose expansion phase II trial. In the escalation phase, patients received escalating doses of domatinostat [100 mg once daily (OD), 200 mg OD, 200 mg twice daily (BD)] orally for 14 days followed by continuous dosing plus avelumab 10 mg/kg administered intravenously 2-weekly (2qw) to determine the recommended phase II dose (RP2D). The trial expansion phase evaluated the best objective response rate (ORR) during 6 months by RECIST version 1.1 using a Simon two-stage optimal design with 2/9 and 1/10 responses required to proceed to stage 2 in the OGA and CRC cohorts, respectively.RESULTSPatients (n = 40) were registered between February 2019 and October 2021. Patients in the dose escalation phase (n = 12) were evaluated to confirm the RP2D of domatinostat 200 mg BD plus avelumab 10 mg/kg. No dose-limiting toxicities were observed. Twenty-one patients were treated at the RP2D, 19 (9 OGA and 10 CRC) were assessable for the best ORR; 2 patients with CRC did not receive combination treatment and were not assessable for the primary endpoint analysis. Six patients were evaluated in the dose escalation and expansion phases. In the OGA cohort, the best ORR was 22.2% (95% one-sided confidence interval lower bound 4.1) and the median duration of disease control was 11.3 months (range 9.9-12.7 months). No responses were observed in the CRC cohort. No treatment-related grade 3-4 adverse events were reported at the RP2D.CONCLUSIONSResponses in the OGA cohort met the criteria to expand to stage 2 of recruitment with an acceptable safety profile. There was insufficient signal in the CRC cohort to progress to stage 2.TRIAL REGISTRATIONNCT03812796 (registered 23^rd January 2019).

1

News (Medical) associated with Domatinostat tosylate

30 Sep 2019

·www.bioportfolio.com

4SC AG: First domatinostat combination data from Phase Ib/II SENSITIZE study presented at ESMO

DGAP-News: 4SC AG / Key word(s): Study 30.09.2019 / 12:00 The issuer is solely responsible for the content of this announcement.

100 Deals associated with Domatinostat tosylate

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External Link

KEGG	Wiki	ATC	Drug Bank
-	-	-	DB13101

R&D Status

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Metastatic Merkel Cell Carcinoma	Phase 2	Spain	4SC AG	13 Oct 2020
Metastatic Merkel Cell Carcinoma	Phase 2	France	4SC AG	13 Oct 2020
Metastatic Merkel Cell Carcinoma	Phase 2	Belgium	4SC AG	13 Oct 2020
Metastatic Merkel Cell Carcinoma	Phase 2	Italy	4SC AG	13 Oct 2020
Melanoma, Cutaneous Malignant	Phase 2	Australia	Netherlands Cancer Insitute	07 Jan 2020
Melanoma, Cutaneous Malignant	Phase 2	Netherlands	Netherlands Cancer Insitute	07 Jan 2020
Gastrointestinal Neoplasms	Phase 2	-	Takeda Pharmaceutical Co., Ltd.	-
Colorectal Cancer	Discovery	United Kingdom	4SC AG	03 Jan 2019
Esophageal Carcinoma	Discovery	United Kingdom	4SC AG	25 Dec 2018
Metastatic melanoma	Discovery	Germany	4SC AG	21 Aug 2017

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Clinical Result

Indication

Phase

Evaluation

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Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT03812796 (EMERGE, Pubmed) Manual	Phase 2	Gastrointestinal Neoplasms \| \|	31	Domatinostatavelumab	(rlttynnufn) = edrvrusmik jnhvglcsbu (jtuicisfsp )	Positive	21 Mar 2024
NCT04133948 (DONIMI, ESMO2022) Manual	Phase 1/2	Melanoma Neoadjuvant IFN-γ	44	nivolumab (IFN-γ sign high + Arm A)	(fhgsrxsnmm) = befqqivzpc iyuectwbsf (ouqyhxewjy ) View more	Positive	10 Sep 2022
NCT04133948 (DONIMI, ESMO2022) Manual	Phase 1/2	Melanoma Neoadjuvant IFN-γ	44	nivolumab +domatinostat (IFN-γ sign high + Arm B)	(fhgsrxsnmm) = zzqkswfoqw iyuectwbsf (ouqyhxewjy ) View more	Positive	10 Sep 2022
NCT03812796 (PD-2 EMERGE, ESMO_GI2022)	Phase 2	Advanced Colorectal Adenocarcinoma MMRp	21	Domatinostat plus Avelumab	(adlxmhsyjl) = uxrultvjtq iyqyedduxr (jsstlsfyoa, 2.8 - 60.0) View more	Positive	02 Jul 2022
NCT03812796 (EMERGE, ESMO2021) Manual	Phase 2	Colorectal Cancer \| Gastrointestinal Neoplasms Mismatch Repair	13	domatinostat+avelumab	(ggthzuodab) = none jypwtmrhqh (lajyllnahz ) View more	Positive	16 Sep 2021
NCT03278665 (SENSITIZE, ASCO 12021 \| ASCO 22021) Manual	Phase 1	Locally Advanced Melanoma	40	pembrolizumab+domatinostat	(emolyejdcq) = kvwkecsoro xvjfzpdlrk (yhrgqrkcut ) View more	Positive	28 May 2021
NCT01344707 (Pubmed \| Eur J Haematol) Manual	Phase 1	Hematologic Neoplasms	24	4SC-202	(hdqmakioac) = 200 mg BID，grade 4 hypercalcemia ymkfeijwfu (ydhzscwsdu ) View more	Positive	01 Feb 2019
NCT01344707 (TOPAS, ASCO2014)	Phase 1	Hematologic Neoplasms	24	4SC-202	(noyqjzqtkp) = Treatment was very well tolerated by heavily pre-treated patients up to the highest dose group. Possibly drug-related AE were less frequent, e.g. low-grade GI complaints such as nausea. Higher-grade hematological toxicity e.g. leading to treatment changes was not observed. Elevation of liver enzymes was observed at 200mg BID during continuous dosing. wkjlgrclzl (brmwyufafd )	-	20 May 2014