This clinical trial aims to investigate the efficacy of Calcipotriol ointment combined with 5-fluorouracil cream as an immunotherapy for actinic keratosis in Organ Transplant Recipients (OTRs) before transplantation and determine whether it can prevent cutaneous squamous cell carcinoma (SCC) in OTRs post-transplant.

Start Date01 Jan 2026

Sponsor / Collaborator

The General Hospital Corp.

[+1]

NCT04642287 / Not yet recruitingPhase 2

Calcipotriol Plus 5-Fluorouracil Immunotherapy for Skin Cancer Prevention in Organ Transplant Recipients

This clinical trial aims to investigate the efficacy of Calcipotriol ointment combined with 5-FU cream in Organ Transplant Recipients (OTRs) to determine if it can stimulate the immune cells against actinic keratoses precancerous skin lesions after transplantation and prevent cutaneous squamous cell carcinoma (SCC) in long-term.

Start Date01 Jan 2026

Sponsor / Collaborator

The General Hospital Corp.

[+1]

NCT06522360 / Not yet recruitingPhase 2

Brigatinib Plus Chemotherapy or Local Consolidation Therapy in ALK Positive Advanced Non-small Cell Lung Cancer (BrightStar-2)

The goal of this clinical research study is to learn if the combination of brigatinib and either local consolidation therapy (such as radiotherapy or surgery) or chemotherapy (pemetrexed and carboplatin) can help to control the disease compared with brigatinib alone. The safety of these combinations will also be studied.

Start Date01 Dec 2025

Sponsor / Collaborator

M.D. Anderson International España SA

100 Clinical Results associated with TYMS

100 Translational Medicine associated with TYMS

0 Patents (Medical) associated with TYMS

5,913

Literatures (Medical) associated with TYMS

01 Nov 2024·INTERNATIONAL IMMUNOPHARMACOLOGY

Capecitabine mitigates cardiac allograft rejection via inhibition of TYMS-Mediated Th1 differentiation in mice

Article

Author: Duan, Jinliang ; Cao, Lei ; Yang, Ruining ; Wang, Zhenglu ; Hou, Wen ; Zhang, Weiqi ; Bromberg, Jonathan S ; Kong, Dejun ; Shen, Zhongyang ; Song, Zhuolun ; Chen, Tao ; Wang, Hao ; Ren, Jiashu ; Yoshida, Sei ; Nian, Yeqi ; Lu, Jianing ; Liu, Tao ; Zheng, Hong

01 Nov 2024·EUROPEAN JOURNAL OF PHARMACEUTICAL SCIENCES

Genetic polymorphisms and their association with methotrexate polyglutamates during maintenance treatment in Korean children and young adults with acute lymphoblastic leukemia

Article

Author: Kim, Min-Ji ; Ju, Hee Young ; Choi, Rihwa ; Lee, Soo-Youn ; Lee, Ji Won

The aim of this study was to investigate the impact of genetic polymorphisms on methotrexate (MTX) metabolism in Korean children and young adults with acute lymphoblastic leukemia, specifically focusing on MTX polyglutamates (MTX-PGs) in erythrocytes, which have been rarely studied. Korean children and young adult patients undergoing maintenance therapy for acute lymphoblastic leukemia, who were receiving weekly oral MTX doses of 20 mg/m²/week, were prospectively included. We investigated erythrocyte MTX-PG (PG1 to PG5) levels, MTX-PG/MTX dose ratios, and 222 genetic polymorphisms spanning 78 genes and three intergenic areas related to MTX transport, folate cycle metabolism, purine/pyrimidine pathways, and non-pathway genes (including TPMT and NUDT15 genotypes) to explore their association with MTX metabolism. MTX-PG levels were associated with MTX dose (p < 0.05), and MTX-PG3 comprised the majority of the total MTX-PGs, with a median of 39.3%. Various polymorphisms within the same gene demonstrated differing associations with each type of MTX-PG, underscoring the complexity of MTX pharmacogenetics. Among the polymorphisms examined, 14 across 13 genes showed significant associations with MTX-PG2-5 levels, even after adjusting for the false discovery rate (ABCC5, ATG16L1, CEP72, FSTL5, GMPS, HTR3A, IMPDH1, NT5C2, SLC28A3, SLCO1B3, SUCLA2, TPMT, and TYMS). This study enhances our understanding of genetic polymorphisms in MTX metabolism and therapeutic monitoring for MTX maintenance, promoting personalized medicine in acute lymphoblastic leukemia patients.

01 Nov 2024·Journal of biomolecular structure & dynamics

A computational investigation of thymidylate synthase inhibitors through a combined approach of 3D-QSAR and pharmacophore modelling

Article

Author: Bhaskar, Vaishnav ; Manisha, Deepthi S. ; Rajappan Krishnendu, Prayaga ; Ghoneim, Mohammed M. ; Abdelgawad, Mohamed A. ; TP, Aneesh ; Pappachen, Leena. K. ; Naguib, Ibrahim A. ; Mathew, Bijo ; Benny, Sonu ; Mary Zachariah, Subin ; Kumar, Sunil

Thymidylate synthase (TS) is a crucial target of cancer drug discovery and is mainly involved in the De novo synthesis of the DNA precursor thymine. In the present study, to generate reliable models and identify a few promising molecules, we combined QSAR modelling with the pharmacophore hypothesis-generating technique. Input molecules were clustered on their similarity, and a cluster of 74 molecules with a pyrimidine moiety was chosen as the set for 3D-QSAR and pharmacophore modelling. Atom-based and field-based 3D-QSAR models were generated and statistically validated with R² > 0.90 and Q² > 0.75. The common pharmacophore hypothesis(CPH) generation identified the best six-point model ADHRRR. Using these best models, a library of FDA-approved drugs was screened for activity and filtered via molecular docking, ADME profiling, and molecular dynamics simulations. The top ten promising TS-inhibiting candidates were identified, and their chemical features profitable for TS inhibitors were explored.Communicated by Ramaswamy H. Sarma.

News (Medical) associated with TYMS

16 Aug 2024

·www.globenewswire.com

CV6 Therapeutics Announces Initiation of Patient Dosing in Phase 1a Clinical Trial Evaluating the Investigational First-In-Class, Specific dUTPase Inhibitor CV6-168

– Study will assess the safety, pharmacokinetic and pharmacodynamic profiles and anti-tumor activity for CV6-168 in the treatment of multiple solid cancers, including colon, gastric, breast, ovarian, lung, and other solid tumors – CV6-168 is a dUTPase-specific, first-in-class DNA Uracilation agent, the first of the company’s innovative pipeline targeting Uracil-DNA metabolism to enter clinical trials Aug. 15, 2024 -- CV6 Therapeutics (NI) Ltd. (“CV6”), a clinical-stage pharmaceutical company dedicated to improving the lives of patients with cancer and inflammatory diseases by developing novel, first-in-class, small molecules targeting Uracil-DNA metabolism, today announced the successful dosing of the second patient in its Phase 1a study evaluating CV6-168 + infusional 5-fluorouracil (5-FU) in cancer patients. This Phase 1 part of this modular, first-in-human Phase 1a clinical trial (ISRCTN12434145) is a multicenter, open-label, dose-escalation study of CV6-168 in patients with advanced metastatic solid tumors refractory to standard treatment. The primary objectives of the study are to determine the following parameters for CV6-168: safety profile, potential optimal biologically relevant doses, maximum tolerated dose, and anti-tumor activity. “CV6-168 induces DNA Uracilation, a novel mechanism of action, and is our first drug candidate to enter the clinic. CV6-168 has the potential to treat a variety of commonly occurring cancers in combination with cornerstone therapies that are used to treat millions of patients per year globally,” said Dr Robert D. Ladner, founder, and chief executive officer at CV6. “CV6-168 accelerates the translation of Uracil-DNA biology by inducing the misincorporation of uracil into cancer cell DNA resulting in uracil-repair-mediated DNA damage, immune modulation and cell death into clinical applications. The dosing of the second patient in our first clinical trial marks an important milestone as CV6 works to deliver new and effective first-in-class small molecules with a novel mechanism of action to patients facing common, difficult-to-treat cancers.” CV6-168 is a novel, targeted, small molecule, dUTPase-specific inhibitor in development for the treatment of multiple, high-incidence cancers. In preclinical studies, it has demonstrated robust anti-tumor activity in cell line and animal models with no added toxicity. CV6-168 targets the nucleotide metabolism enzyme dUTPase, with high specificity, avoiding drug-drug interactions with its drug combination partners that include thymidylate synthase (TS) inhibitors like 5-fluorouracil (5-FU). CV6 is a clinical-stage biopharmaceutical company focused on the development and commercialization of novel therapeutic agents for patients with cancer and inflammatory diseases. CV6 develops innovative, first-in-class therapies with a novel mechanism of action by targeting dUTPase and Uracil-DNA Metabolism - an area of research that its founder helped pioneer. Its lead oncology drug candidate CV6-168 is in a Phase 1a clinical trial in advanced cancers. Investors include QUBIS, the commercialization arm of Queen’s University in Belfast, Invest Northern Ireland, CoFund NI, managed by Clarendon Fund Managers, and Techstart Ventures, as well as US, UK, European, and Australian-based private investors. CV6 is headquartered in Belfast, Northern Ireland, UK, with research facilities at Queen’s University Belfast in the Patrick G Johnston Centre for Cancer Research. The content above comes from the network. if any infringement, please contact us to modify.

Oligonucleotide

14 Dec 2023

·www.biospace.com

CV6 Therapeutics Receives MHRA Approval for Novel Cancer Therapy Phase 1a Clinical Trial

BELFAST, United Kingdom, Dec. 14, 2023 (GLOBE NEWSWIRE) -- CV6 Therapeutics (‘CV6’), a drug development biotechnology company that specializes in innovative small molecule therapeutics for cancer and inflammatory diseases, announces it has received approval from the UK’s medicines regulator, the MHRA, for the company’s first-in-human Phase 1a clinical trial of its lead oncology therapeutic, CV6-168, in patients with colorectal and other cancers. CV6-168 is a first-in-class DNA uracilation agent that selectively targets the enzyme dUTPase. Cancer cell DNA uracilation by CV6-168 is aided by combination with standard cancer therapies including thymidylate synthase (TS) inhibitors such as 5-fluorouracil (5-FU). These CV6-168 drug combinations result in targeted uracil-based DNA damage and cancer cell death while simultaneously stimulating the immune system to further enhance the anticancer effect. DNA uracilation is a novel therapeutic strategy that has demonstrated effectiveness and safety in pre-clinical models with no added toxicity when combined with standard-of-care anti-cancer drugs. The UK multi-centre Phase 1a clinical trial will combine CV6-168 with infusional 5-FU to treat gastrointestinal cancer patients, such as colon, gastric, and pancreatic cancers as well as other tumor types such as melanoma, lung, and ovarian cancers. It will focus on safety, measuring how CV6-168 is absorbed by the body, identifying optimal dosing levels, and gathering initial indications of anti-cancer activity. The initial trial is for up to 50 patients, taking part at leading cancer hospitals in Belfast, Glasgow, Newcastle, and the Royal Marsden in London that are within the UK Experimental Cancer Medicine Centre (ECMC) network. The trial is expected to have dosed its first patient in Q1 2024, with trial read-outs expected in H1 2025. CV6 CEO and Founder Dr Robert Ladner said, “This regulatory approval is a key milestone as we progress CV6-168 into a first-in-human Phase 1a clinical trial. Our innovative oncology therapeutic unlocks the potential of DNA uracilation as a promising new therapeutic approach to cancer treatment, with the opportunity to significantly improve outcomes for patients across multiple cancer types. CV6-168 is a specific, first-in-class dUTPase inhibitor that has a value-driven therapeutic approach, is globally scalable, and can potentially treat many millions of patients annually across multiple high-incidence cancer types.” The Chief Investigator for this trial is Richard Wilson, who is Professor of Gastrointestinal Oncology in the University of Glasgow and specialises in early and late phase cancer clinical trials. He said, “Despite recent advances, there is still huge unmet need for new treatments for colorectal and many other cancers. CV6-168 in combination with 5-FU has the potential to improve on existing treatments, where 5-FU and similar drugs are currently used, in over 8 million people with cancer annually across the world. What sets CV6-168 apart is that the DNA uracilation mechanism selectively damages cancer cell DNA but also triggers signals to the immune system opening up the potential to unleash our natural immunity against the cancer cells. CV6-168 is given by mouth which makes it very easy to combine with other drugs and lessens the burden on patients receiving it. If CV6-168 fulfils its’ promise, then this will give us a new therapeutic option that is easy to take alongside existing standard anti-cancer drugs, and with minimal additional side-effects.” CV6 Therapeutics, originally founded in Los Angeles, is now headquartered in the Patrick G. Johnston Centre for Cancer Research at Queen’s University Belfast. About CV6 Therapeutics CV6 Therapeutics, (NI) Ltd., is a drug development biotechnology company that specializes in value-based, first-in-class, small molecule therapeutics that are scalable to address global unmet medical needs for cancer and inflammatory diseases. Its lead oncology drug candidate CV6-168 has successfully completed all pre-clinical development milestones. The company has UK regulatory approval to start a first-in-human phase 1a clinical trial of CV6-168 in advanced cancers in 2024. The company’s inflammatory disease asset CV6-1271 is in preclinical-development. CV6 has a Grant for R&D from Invest Northern Ireland to support the Phase 1a trial. (1). Investors include QUBIS, the commercialization arm of Queen’s University in Belfast, Invest Northern Ireland, CoFund NI, managed by Clarendon Fund Managers, Techstart Ventures as well as US and UK-based private investors. CV6 Therapeutics, originally founded in Los Angeles, is now headquartered in the Patrick G. Johnston Centre for Cancer Research at Queen’s University Belfast. For more information see our website here and LinkedIn here. References (1) Invest Northern Ireland’s R&D support is part financed by the European Regional Development Fund under the EU Investment for Growth and Jobs Programme 2014–2020. Media Contacts CV6 Therapeutics Dr Robert Ladner, CEO +44 (0) 7500 444287 rladner@cv6t.com Scius Communications Katja Stout +447789435990 katja@sciuscommunications.com Daniel Gooch +447747875479 daniel@sciuscommunications.com

Phase 1IND

02 Nov 2022

·www.biospace.com

CV6 Therapeutics Secures $9.2m to Progress Novel Cancer Drug to Phase 1a Trial

Belfast, UK, 2 November 2022 – CV6 Therapeutics (‘CV6’), a drug development biotechnology company that specializes in innovative small molecule therapeutics for cancer and inflammatory diseases, announces it has secured $9.2m to progress the company’s lead oncology asset CV6-168 into a first-in-human Phase 1a clinical trial and perform further scientific development work. Investors participating in the financing include QUBIS, the commercialization arm of Queen’s University in Belfast, Invest Northern Ireland, CoFund NI, managed by Clarendon Fund Managers, Techstart Ventures as well as US and UK-based private investors. CV6 has also received a Grant for R&D from Invest Northern Ireland* to support the Phase 1a trial. CV6 is developing CV6-168, a novel, first-in-class DNA uracilation agent that selectively targets the enzyme dUTPase. Cancer cell DNA uracilation by CV6-168 is aided by combination with standard cancer therapies such as thymidylate synthase (TS) inhibitors and results in uracil-based DNA damage and cell death while simultaneously stimulating the immune system to further enhance the anticancer effect. DNA uracilation is a novel therapeutic strategy that has demonstrated effectiveness and safety in pre-clinical models with no added toxicity with drug combinations. CV6-168 is set to enter a Phase 1a clinical trial in 2023 that will focus on safety, measuring how the drug is absorbed by the body, identifying optimal dosing levels and gathering initial indications of anti-cancer activity. CV6 CEO and Founder Dr Robert Ladner said, “CV6-168 unlocks the potential of DNA uracilation as a promising new therapeutic approach to cancer treatment, with the opportunity to significantly improve outcomes for patients across multiple cancer types. Securing this financing and a grant for R&D from Invest Northern Ireland will allow us to advance CV6-168 into a first-in-human Phase 1a clinical trial, representing a key milestone for CV6.” CV6 Therapeutics is headquartered in the Patrick G. Johnston Centre for Cancer Research at Queen’s University Belfast. * Invest Northern Ireland’s R&D support is part financed by the European Regional Development Fund under the EU Investment for Growth and Jobs Programme 2014–2020. Notes to Editors About CV6 Therapeutics CV6 Therapeutics, (NI) Ltd., is a drug development biotechnology company that specializes in innovative small molecule therapeutics for cancer and inflammatory diseases. Lead oncology drug candidate CV6-168 has successfully completed all pre-clinical development milestones. The company plans to start a first-in-human phase 1a clinical trial of CV6-168 in advanced cancers in 2023. Inflammatory disease asset CV6-1271 is in preclinical-development. The company was originally founded in 2013 in Los Angeles, California and moved to Northern Ireland to establish the company at Queen’s University in 2015. For more information see our website here and LinkedIn here. Media Contacts CV6 Therapeutics Dr Robert Ladner, CEO +44 (0) 7500 444287 rladner@cv6t.com Scius Communications Katja Stout +447789435990 katja@sciuscommunications.com Daniel Gooch +447747875479 daniel@sciuscommunications.com

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