Last update 21 Mar 2024

DKK3

Dickkopf-related protein 3

Last update 21 Mar 2024

Basic Info

Synonyms

CRRL, dickkopf (Xenopus laevis) homolog 3, dickkopf 3 homolog (Xenopus laevis)

+ [9]

Introduction

Antagonizes canonical Wnt signaling by inhibiting LRP5/6 interaction with Wnt and by forming a ternary complex with the transmembrane protein KREMEN that promotes internalization of LRP5/6. DKKs play an important role in vertebrate development, where they locally inhibit Wnt regulated processes such as antero-posterior axial patterning, limb development, somitogenesis and eye formation. In the adult, Dkks are implicated in bone formation and bone disease, cancer and Alzheimer disease (By similarity).

Drugs associated with DKK3

REIC gene therapy(Momotaro-Gene Inc.)

Target

DKK3

Mechanism

DKK3 stimulants [+2]

Active Org.

Momotaro-Gene, Inc.

Originator Org.

Momotaro-Gene, Inc.

Active Indication

Malignant Pleural Mesothelioma

Inactive Indication

Liver Cancer [+1]

Drug Highest PhasePhase 2

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

Ad-SGE-DKK3 gene therapy(KYORIN Pharmaceutical Co. Ltd.)

Target

DKK3

Mechanism

DKK3 gene transference [+1]

Active Org.

Momotaro-Gene, Inc. [+2]

Originator Org.

KYORIN Pharmaceutical Co., Ltd.

Active Indication

Mesothelioma

Inactive Indication-

Drug Highest PhasePhase 2

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

HG-1232

Target

DKK3

Mechanism

DKK3 modulators

Active Org.-

Originator Org.

Human Genome Sciences, Inc.

Active Indication-

Inactive Indication

Neoplasms [+1]

Drug Highest PhasePending

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

Clinical Trials associated with DKK3

NCT04013334 / Active, not recruitingPhase 2

A Phase 2, Open-Label, Single-Center Study of MTG201 in Combination With Nivolumab in Patients With Relapsed Malignant Pleural Mesothelioma

Twelve patients with relapsed malignant pleural mesothelioma will be treated with intratumoral injections of MTG201, a replication incompetent adenovirus, modified by the insertion of the reduced expression in immortalized cells (REIC)/Dikkopf (Dkk)-3 gene, on Days 1, 8, 22, and 50. Patients will also receive every 4 weekly intravenous infusions of nivolumab, 480 mg, starting on Day 2. Safety and anti-tumor activity will be monitored at regular intervals throughout the study.

Start Date15 Aug 2019

Sponsor / Collaborator

Momotaro-Gene, Inc.

[+2]

JPRN-jRCT2080223982 / CompletedPhase 2

A phase II study of Ad-SGE-REIC

Start Date03 Aug 2018

Sponsor / Collaborator

KYORIN Pharmaceutical Co., Ltd.

JPRN-JapicCTI-152998 / Unknown statusPhase 1/2

A phase I/II clinical trial of Ad-SGE-REIC for malignant pleural mesothelioma

Start Date25 Sep 2015

Sponsor / Collaborator

KYORIN Pharmaceutical Co., Ltd.

100 Clinical Results associated with DKK3

100 Translational Medicine associated with DKK3

0 Patents (Medical) associated with DKK3

658

Literatures (Medical) associated with DKK3

23 Feb 2024·Nature immunology

CD200⁺ fibroblasts form a pro-resolving mesenchymal network in arthritis.

Article

Author: Simon Rauber ; Hashem Mohammadian ; Christian Schmidkonz ; Armin Atzinger ; Alina Soare ; Christoph Treutlein ; Samuel Kemble ; Christopher B Mahony ; Manuel Geisthoff ; Mario R Angeli ; Maria G Raimondo ; Cong Xu ; Kai-Ting Yang ; Le Lu ; Hannah Labinsky ; Mina S A Saad ; Charles A Gwellem ; Jiyang Chang ; Kaiyue Huang ; Eleni Kampylafka ; Johannes Knitza ; Rostyslav Bilyy ; Jörg H W Distler ; Megan M Hanlon ; Ursula Fearon ; Douglas J Veale ; Frank W Roemer ; Tobias Bäuerle ; Hans M Maric ; Simone Maschauer ; Arif B Ekici ; Christopher D Buckley ; Adam P Croft ; Torsten Kuwert ; Olaf Prante ; Juan D Cañete ; Georg Schett ; Andreas Ramming

Fibroblasts are important regulators of inflammation, but whether fibroblasts change phenotype during resolution of inflammation is not clear. Here we use positron emission tomography to detect fibroblast activation protein (FAP) as a means to visualize fibroblast activation in vivo during inflammation in humans. While tracer accumulation is high in active arthritis, it decreases after tumor necrosis factor and interleukin-17A inhibition. Biopsy-based single-cell RNA-sequencing analyses in experimental arthritis show that FAP signal reduction reflects a phenotypic switch from pro-inflammatory MMP3⁺/IL6⁺ fibroblasts (high FAP internalization) to pro-resolving CD200⁺DKK3⁺ fibroblasts (low FAP internalization). Spatial transcriptomics of human joints indicates that pro-resolving niches of CD200⁺DKK3⁺ fibroblasts cluster with type 2 innate lymphoid cells, whereas MMP3⁺/IL6⁺ fibroblasts colocalize with inflammatory immune cells. CD200⁺DKK3⁺ fibroblasts stabilized the type 2 innate lymphoid cell phenotype and induced resolution of arthritis via CD200-CD200R1 signaling. Taken together, these data suggest a dynamic molecular regulation of the mesenchymal compartment during resolution of inflammation.

22 Feb 2024·Experimental cell research

ICBP90, an epigenetic regulator, induces DKK3 promoter methylation, promotes glioma progression, and reduces sensitivity to cis-platinum.

Article

Author: Qinchen Cao ; Xinxin Wang ; Jie Liu ; Yang Dong ; Xiaolong Wu ; Yin Mi ; Ke Liu ; Mingzhi Zhang ; Yonggang Shi ; Ruitai Fan

Glioma is the most common brain malignancy, characterized by high morbidity, high mortality, and treatment-resistance. Inverted CCAAT box Binding Protein of 90 kDa (ICBP90) has been reported to be involved in tumor progression and the maintenance of DNA methylation. Herein, we constructed ICBP90 over-expression and knockdown glioma cell lines, and found that ICBP90 knockdown inhibited glioma cell proliferation, migration, and invasion. ICBP90 silencing potentially enhanced cellular sensitivity to cis-platinum (DDP) and exacerbated DDP-induced pyroptosis, manifested by the elevated levels of gasdermin D-N-terminal and cleaved caspase 1; whereas, ICBP90 over-expression exhibited the opposite effects. Consistently, ICBP90 knockdown inhibited tumor growth in an in vivo mouse xenograft study using U251 cells stably expressing sh-ICBP90 and oe-ICBP90. Further experiments found that ICBP90 reduced the expression of Dickkopf 3 homolog (DKK3), a negative regulator of β-catenin, by binding its promoter and inducing DNA methylation. ICBP90 knockdown prevented the nuclear translocation of β-catenin and suppressed the expression of c-Myc and cyclin D1. Besides, DKK3 over-expression restored the effects of ICBP90 over-expression on cell proliferation, migration, invasion and DDP sensitivity. Our findings suggest that ICBP90 inhibits the expression of DKK3 in glioma by maintaining DKK3 promoter methylation, thereby conducing to ICBP90-mediated carcinogenesis and drug insensitivity.

19 Feb 2024·Nature communications

A single cell atlas of frozen shoulder capsule identifies features associated with inflammatory fibrosis resolution.

Article

Author: Michael T H Ng ; Rowie Borst ; Hamez Gacaferi ; Sarah Davidson ; Jessica E Ackerman ; Peter A Johnson ; Caio C Machado ; Ian Reekie ; Moustafa Attar ; Dylan Windell ; Mariola Kurowska-Stolarska ; Lucy MacDonald ; Stefano Alivernini ; Micon Garvilles ; Kathrin Jansen ; Ananya Bhalla ; Angela Lee ; James Charlesworth ; Rajat Chowdhury ; Paul Klenerman ; Kate Powell ; Carl-Philip Hackstein ; ICECAP Consortium ; Dominic Furniss ; Jonathan Rees ; Derek Gilroy ; Mark Coles ; Andrew J Carr ; Stephen N Sansom ; Christopher D Buckley ; Stephanie G Dakin

Frozen shoulder is a spontaneously self-resolving chronic inflammatory fibrotic human disease, which distinguishes the condition from most fibrotic diseases that are progressive and irreversible. Using single-cell analysis, we identify pro-inflammatory MERTK^lowCD48⁺ macrophages and MERTK + LYVE1 + MRC1+ macrophages enriched for negative regulators of inflammation which co-exist in frozen shoulder capsule tissues. Micro-cultures of patient-derived cells identify integrin-mediated cell-matrix interactions between MERTK+ macrophages and pro-resolving DKK3+ and POSTN+ fibroblasts, suggesting that matrix remodelling plays a role in frozen shoulder resolution. Cross-tissue analysis reveals a shared gene expression cassette between shoulder capsule MERTK+ macrophages and a respective population enriched in synovial tissues of rheumatoid arthritis patients in disease remission, supporting the concept that MERTK+ macrophages mediate resolution of inflammation and fibrosis. Single-cell transcriptomic profiling and spatial analysis of human foetal shoulder tissues identify MERTK + LYVE1 + MRC1+ macrophages and DKK3+ and POSTN+ fibroblast populations analogous to those in frozen shoulder, suggesting that the template to resolve fibrosis is established during shoulder development. Crosstalk between MerTK+ macrophages and pro-resolving DKK3+ and POSTN+ fibroblasts could facilitate resolution of frozen shoulder, providing a basis for potential therapeutic resolution of persistent fibrotic diseases.

News (Medical) associated with DKK3

14 Dec 2023

·www.prnewswire.com

MTG201 + Nivolumab for MPM: Emerging Drug Insights and Market Forecast to 2032

DUBLIN, Dec. 13, 2023 /PRNewswire/ -- The "MTG201 + nivolumab Emerging Drug Insight and Market Forecast - 2032" report has been added to ResearchAndMarkets.com's offering. This report provides comprehensive insights about MTG201 + nivolumab for malignant pleural mesothelioma (MPM) in the seven major markets. A detailed picture of the MTG201 + nivolumab for MPM in the 7MM, i.e., the United States, EU4 (Germany, France, Italy, and Spain) and the United Kingdom, and Japan for the study period 2019 -2032 is provided in this report along with a detailed description of the MTG201 + nivolumab for MPM. The report provides insights about mechanism of action, dosage and administration, as well as research and development including regulatory milestones, along with other developmental activities. Further, it also consists of future market assessments inclusive of the MTG201 + nivolumab market forecast analysis for MPM in the 7MM, SWOT, analysts' views, comprehensive overview of market competitors, and brief about other emerging therapies in MPM. Drug Summary MTG201 is novel investigational gene therapy with unique dual mechanisms of action capable of addressing a range of cancers. The drug candidate leverages the company's proprietary adenoviral vector technology platform to deliver the reduced expression in immortalized Cells/Dickkopf-3 gene (REIC/Dkk-3 gene) into cancer cells, where the expression of the gene is markedly downregulated. The resulting increase in REIC/Dkk-3 gene expression in cancer cells triggers immunogenic cell death selectively in cancer cells. At the same time, increased expression of the REIC/Dkk3 gene in normal cell components in tumor tissue promotes antitumor immunity by activating dendritic cells and natural killer (NK) cells while suppressing immune-suppressive regulatory T cells (Tregs) and myeloid-derived suppressor cells (MDSC). Based on these novel dual mechanisms, MTG201 is believed to be well-positioned to work synergistically with checkpoint inhibitors such as nivolumab. The Phase II trial (NCT04013334), conducted at the Baylor College of Medicine in Houston, Texas, is an open-label, single-arm study designed to assess the efficacy, safety, and tolerability of intratumoral administration of MTG201 in combination with nivolumab. The trial enrolled up to twelve patients with malignant mesothelioma who have failed front-line systemic platin-based chemotherapy. The study's primary objective is to assess the efficacy of the treatment combination, with the primary endpoint being objective response rate (ORR). MTG201 + nivolumab Analytical Perspective In-depth MTG201 + nivolumab Market Assessment This report provides a detailed market assessment of MTG201 + nivolumab for malignant pleural mesothelioma (MPM) in the seven major markets, i.e., the United States, EU4 (Germany, France, Italy, and Spain) and the United Kingdom, and Japan. This segment of the report provides forecasted sales data from 2024 to 2032. MTG201 + nivolumab Clinical Assessment The report provides the clinical trials information of MTG201 + nivolumab for MPM covering trial interventions, trial conditions, trial status, start and completion dates. Report Highlights In the coming years, the market scenario for malignant pleural mesothelioma (MPM) is set to change due to the extensive research and incremental healthcare spending across the world; which would expand the size of the market to enable the drug manufacturers to penetrate more into the market. The companies are developing therapies that focus on novel approaches to treat/improve the disease condition, assess challenges, and seek opportunities that could influence MTG201 + nivolumab dominance. Other emerging products for MPM are expected to give tough market competition to MTG201 + nivolumab and launch of late-stage emerging therapies in the near future will significantly impact the market. A detailed description of regulatory milestones, and developmental activities, provide the current development scenario of MTG201 + nivolumab in MPM. This in-depth analysis of the forecasted sales data of MTG201 + nivolumab from 2024 to 2032 will support the clients in the decision-making process regarding their therapeutic portfolio by identifying the overall scenario of the MTG201 + nivolumab in MPM. Key Topics Covered: 1. Report Introduction 2. MTG201 + nivolumab Overview in MPM 2.1. Product Detail 2.2. Clinical Development 2.2.1. Clinical studies 2.2.2. Clinical trials information 2.2.3. Safety and efficacy 2.3. Other Developmental Activities 2.4. Product Profile 3. Competitive Landscape (Marketed Therapies) 4. Competitive Landscape (Late-stage Emerging Therapies) 5. MTG201 + nivolumab Market Assessment 5.1. Market Outlook of MTG201 + nivolumab in MPM 5.2. 7MM Analysis 5.2.1. Market Size of MTG201 + nivolumab in the 7MM for MPM 5.3. Country-wise Market Analysis 5.3.1. Market Size of MTG201 + nivolumab in the United States for MPM 5.3.2. Market Size of MTG201 + nivolumab in Germany for MPM 5.3.3. Market Size of MTG201 + nivolumab in France for MPM 5.3.4. Market Size of MTG201 + nivolumab in Italy for MPM 5.3.5. Market Size of MTG201 + nivolumab in Spain for MPM 5.3.6. Market Size of MTG201 + nivolumab in the United Kingdom for MPM 5.3.7. Market Size of MTG201 + nivolumab in Japan for MPM 6. SWOT Analysis 7. Analysts' Views For more information about this report visit About ResearchAndMarkets.com ResearchAndMarkets.com is the world's leading source for international market research reports and market data. We provide you with the latest data on international and regional markets, key industries, the top companies, new products and the latest trends. Media Contact: Research and Markets Laura Wood, Senior Manager [email protected] For E.S.T Office Hours Call +1-917-300-0470 For U.S./CAN Toll Free Call +1-800-526-8630 For GMT Office Hours Call +353-1-416-8900 U.S. Fax: 646-607-1907 Fax (outside U.S.): +353-1-481-1716 Logo - SOURCE Research and Markets

Phase 2Clinical ResultGene Therapy

04 Jun 2021

·www.biospace.com

Three Biopharma Companies Raise Millions in Separate Series A Financing Rounds

Stablix Therapeutics launched with a $63 million Series A financing round that will be used to develop the company’s and advance a portfolio of protein stabilizers towards the clinic. New York-based Stablix’s TPS platform, dubbed RESTORED, “generates heterobifunctional small molecules (RESTORACS) that recruit deubiquitinase enzymes to remove ubiquitin from targeted proteins and consequently stabilize or increase target protein levels and activity,” according to the company announcement. Stablix will initially aim the platform to develop programs that treat rare diseases, cancer, and immunological disorders. With the RESTORED platform, Stablix said it’s possible to inhibit the ubiquitin-proteasome system in a target-selective manner to treat some of these diseases. “Stablix possesses a first-in-category platform that can restore protein stability and function in a target-selective manner,” Carlo Rizzuto, a partner at Versant and acting Chief Executive Officer of Stablix said in a statement. “We are very pleased to launch this company to address this important therapeutic white space for numerous devastating diseases.” The company pointed to cystic fibrosis as a disease that could benefit from its approach. Stablix said mutations in the CFTR gene produce a functional protein that is subject to excessive ubiquitination. This can lead to rapid degradation through the proteasome. Excess ubiquitination is also a hallmark of some cancers, where E3 ubiquitin ligases are “frequently upregulated or amplified.” This drives the degradation of tumor suppressor proteins, the company added. The Series A financing round was led by Versant Ventures, the founding investor of Stablix. NEA, Cormorant, Euclidean Capital and Alexandria Real Estate Equities also contributed. Stablix wasn’t the only company to announced funds from a Series A financing round this morning. Texas-based Stellanova Therapeutics, a resident company at JLABS @ TMC, closed a $15.5 million Series A financing round. Funds will be used to support the development of antibody drugs and a discovery platform targeting pro-tumorigenic factors produced by fibroblasts in the tumor microenvironment, which can render resistant cancers treatable. Stellanova aims to advance its lead antibody asset into the clinic. Stellanova is focused on targeting pro-tumorigenic effects enabled by the activity of carcinoma-associated fibroblasts (known as CAFs) in the tumor microenvironment. These CAFs play significant roles in promoting cancer growth and metastasis. They spur angiogenesis, suppress anti-tumor immunity, and foster chemoresistance. Stellanova’s lead antibody candidate is designed to neutralize DKK3, a factor secreted by CAFs that acts on neighboring cancer cells and immune cells to promote tumor progression and therapy resistance. Rosa Hwang, co-founder of Stellanova, said the company’s lead antibody shows robust anti-tumor activity, alone or together with immune therapy, in highly refractory preclinical models of the pancreas and triple negative breast cancer. The Series A financing round was led by Sporos Bioventures, LLC. Belgium-based Amyl Therapeutics raised €18.3 million ($22.3 million) in Series A funding. The company will use funds from the round to advance the discovery and development of preclinical therapeutic candidates that can target multiple misfolded proteins implicated in both progressive peripheral and rare neurodegenerative diseases. The company’s amyloid fibrils specific technology platform dubbed ClariTY was developed for the treatment of all forms of Amyloidosis, which can be seen in diseases such as Alzheimer’s and Parkinson’s. Therapeutic assets based on the ClariTY platform are designed to prevent the further accumulation of these amyloid aggregates and clear existing aggregates from the peripheral organs and the brain. Also, they are designed to block further “cell-to-cell spread of misfolded proteins.” The company believes these therapies may offer a breakthrough approach to treat protein misfolding diseases. The financing round was composed of an €8.6 million equity investment led by Belgium-based Noshaq, with participation from Merieux Participations, Sambrinvest, and other private investors. Additionally, a non-dilutive funding of €9.7 million was made by the DG06, a Belgium-based policy-design and implementing body.

AntibodySmall molecular drug

10 Apr 2021

·www.globenewswire.com

Gennao Bio Presents New Data on Novel Gene Monoclonal

~ Preclinical data show the utility of Gennao’s proprietary first-in-class monoclonal antibody 3E10-D31N (GMABD31N), a cell penetrating antibody, to non-covalently bind to and systemically deliver therapeutic levels of multiple types of nucleic acid payloads to cells in vitro and tumors in vivo ~ ~ GMABD31N combined with a RIG-I ligand 3pRNA (GMABD31N/3pRNA) efficiently targets and delivers a known RIG-I agonist to tumors in vivo and effectively prevents tumor growth in a mouse model of melanoma, comparable to anti-CTLA-4 ~ NEW HAVEN, Conn., April 10, 2021 (GLOBE NEWSWIRE) -- Gennao Bio, a privately-held genetic medicines company developing first-in-class, targeted nucleic acid therapeutics, today announced a late-breaking poster detailing preclinical results for its proprietary, non-viral gene monoclonal antibody (GMAB) nucleic acid delivery system. The data were presented at the American Association for Cancer Research (AACR) Annual Meeting 2021. The GMAB technology platform, exclusively licensed from Yale University, utilizes a proprietary, cell-penetrating antibody to non-covalently bind to and deliver therapeutic levels of multiple types of nucleic acids, including synthetic RNA (ribonucleic acid) messenger RNA, small interfering RNA, deoxyribonucleic acids, antisense oligonucleotides and gene editing molecules. The preclinical data presented in the poster show the utility of the monoclonal antibody 3E10-D31N (GMABD31N) to deliver nucleic acids to cells in vitro and to tumors in vivo. This antibody, a modified version of 3E10, forms non-covalent complexes with RNAs and can mediate highly specific delivery broadly into tumors via intravenous injection by targeting the nucleoside transporter ENT2. ENT2 is highly expressed in multiple tumor types as well as skeletal and cardiac muscle. Studies completed with labeled RNAs and messenger RNAs expressing a green fluorescent protein reporter gene show tumor specific delivery and functional expression by imaging, with minimal delivery to healthy tissues. Cell culture studies show antibody-mediated delivery of a series of retinoic acid-inducible gene I (RIG-I) ligands, including hairpin RNAs and synthetic double-stranded RNA (poly(I:C)), resulting in robust RIG-I stimulation and induction of type-1 interferon signaling. Most importantly, when using a mouse B16 melanoma tumor model, substantial tumor growth suppression was observed upon intravenous injection of GMABD31N non-covalently bound to 3pRNA, an 89-nucleotide, single-stranded RNA. In this study, the tumor suppression observed was comparable to the tumor suppression that was observed using anti-CTLA-4. “The preclinical results presented today highlight the ability of GMABD31N to systemically deliver immunostimulatory RNAs in a targeted, non-invasive manner,” said Peter M. Glazer, M.D., Ph.D., Chair of the Department of Therapeutic Radiology, Professor of Genetics and Robert E. Hunter Professor of Therapeutic Radiology at the Yale School of Medicine. “This approach has the potential to offer new and significant treatment advantages over current delivery methods that are associated with systemic toxicity or rely on direct intra-tumoral injection, which is therapeutically sub-optimal, especially for metastatic disease. I look forward to working with Gennao Bio on the continued development of the GMAB platform to develop effective therapeutics for the treatment of oncology indications, as well as monogenic skeletal and cardiac muscle diseases.” The full abstract and poster presentation can be accessed on the AACR annual meeting website, , through June 21, 2021. About Gennao Bio Gennao Bio is a privately-held genetic medicines company developing first-in-class targeted nucleic acid therapeutics utilizing its proprietary gene monoclonal antibody (GMAB) platform technology. GMAB technology utilizes a novel, cell-penetrating antibody to non-covalently bind to and deliver therapeutic levels of a wide variety of nucleic acid payloads to select cells. This non-viral delivery platform offers significant advantages over traditional gene delivery systems as it can deliver multiple types of nucleic acids, allows for repeat dosing and dose optimization, and can be easily and affordably manufactured. Gennao Bio is developing this delivery system with an initial focus on oncology and monogenic skeletal muscle diseases. Investor and Media Contact: Gennao BioChris Duke732-735-0330cduke@gennaobio.com Source: Gennao Bio

CollaborateSmall molecular drugAntibodyFirst in ClassOligonucleotide

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DKK3

Dickkopf-related protein 3

Basic Info

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