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Last update 23 Jan 2025

TWEAK

Last update 23 Jan 2025

Basic Info

Synonyms

APO3 ligand, APO3L, DR3LG

+ [9]

Introduction

Binds to FN14 and possibly also to TNRFSF12/APO3. Weak inducer of apoptosis in some cell types. Mediates NF-kappa-B activation. Promotes angiogenesis and the proliferation of endothelial cells. Also involved in induction of inflammatory cytokines. Promotes IL8 secretion.

Drugs associated with TWEAK

Withaferin A

Target

ADAM8 x ANGPTL2 x BRMS1 x CSF-1R x HSP90 x IL-6 x TWEAK x tPA x uPA

Mechanism

ADAM8 antagonists [+8]

Active Org.

University of Louisville

Originator Org.

University of Louisville

Active Indication

Recurrent ovarian cancer

Inactive Indication-

Drug Highest PhasePhase 1/2

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

MRT-101

Target

TWEAK

Mechanism

TWEAK modulators

Active Org.

Mirata Biopharma LLCStartup

Originator Org.

Clayton Foundation for Research

Active Indication

Breast Cancer [+2]

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

L-524-0366

Target

FGF14 x TWEAK

Mechanism

FGF14 inhibitors [+1]

Active Org.

TGen Foundation [+2]

Originator Org.

Translational Genomics Research Institute

Active Indication

Glioblastoma

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

Clinical Trials associated with TWEAK

NCT05610735

/ RecruitingPhase 1/2IIT

Combination Therapy With Liposomal Doxorubicin and Withaferin A (Ashwagandha, ASWD) in Recurrent Ovarian Cancer

The proposed study "combination therapy with liposomal doxorubicin and withaferin A (Ashwagandha, ASWD) in recurrent ovarian cancer" is focused to determine the feasibility and maximum tolerance dose of Ashwagandha with liposomal doxorubicin (DOXIL) in recurrent ovarian cancer patients. The study contains two parts. In part 1 (phase I), 18 patients with recurrent ovarian cancer eligible for DOXIL therapy will be recruited and three doses of Ashwagandha (2.0 g, 4.0 g and 8.0 g) in the form of tablets along with DOXIL will be evaluated for feasibility and tolerance of ASWD. In part 2 (phase II), 54 patients with recurrent ovarian cancer will be recruited and treated with DOXIL and Ashwagandha (dose determined from part 1) to evaluate the complete response (CR), partial response (PR), and stable disease (SD).

Start Date01 May 2024

Sponsor / Collaborator

University of Louisville

[+1]

CTRI/2023/07/055361

/ Not yet recruitingPhase 2IIT

A Phase II Clinical Trial of Standardized Withaferin-A for the treatment of Steroid Refractory acute Graft versus Host Disease.

Start Date31 Jul 2023

Sponsor / Collaborator

Tata Memorial Centre

PER-086-13

/ Unknown statusPhase 2

A DOSE-BLINDED, 2-DOSE LEVEL, PARALLEL-GROUP, MULTICENTER, LONG-TERM EXTENSION STUDY TO EVALUATE THE LONG-TERM SAFETY, EFFICACY, AND IMMUNOGENICITY OF BIIB023 IN SUBJECTS WITH LUPUS NEPHRITIS

Start Date26 Jun 2014

Sponsor / Collaborator

Biogen Idec Research Ltd.

100 Clinical Results associated with TWEAK

100 Translational Medicine associated with TWEAK

0 Patents (Medical) associated with TWEAK

1,080

Literatures (Medical) associated with TWEAK

01 Feb 2025·Biometrical Journal

To Tweak or Not to Tweak. How Exploiting Flexibilities in Gene Set Analysis Leads to Overoptimism

Article

Author: Wünsch, Milena ; Hinske, Ludwig Christian ; Herrmann, Moritz ; Boulesteix, Anne‐Laure ; Sauer, Christina

ABSTRACTGene set analysis, a popular approach for analyzing high‐throughput gene expression data, aims to identify sets of genes that show enriched expression patterns between two conditions. In addition to the multitude of methods available for this task, users are typically left with many options when creating the required input and specifying the internal parameters of the chosen method. This flexibility can lead to uncertainty about the “right” choice, further reinforced by a lack of evidence‐based guidance. Especially when their statistical experience is scarce, this uncertainty might entice users to produce preferable results using a “trial‐and‐error” approach. While it may seem unproblematic at first glance, this practice can be viewed as a form of “cherry‐picking” and cause an optimistic bias, rendering the results nonreplicable on independent data. After this problem has attracted a lot of attention in the context of classical hypothesis testing, we now aim to raise awareness of such overoptimism in the different and more complex context of gene set analyses. We mimic a hypothetical researcher who systematically selects the analysis variants yielding their preferred results, thereby considering three distinct goals they might pursue. Using a selection of popular gene set analysis methods, we tweak the results in this way for two frequently used benchmark gene expression data sets. Our study indicates that the potential for overoptimism is particularly high for a group of methods frequently used despite being commonly criticized. We conclude by providing practical recommendations to counter overoptimism in research findings in gene set analysis and beyond.

01 Feb 2025·Brain, Behavior, and Immunity

Implications of the choroid plexus in Niemann-Pick disease Type C neuropathogenesis

Article

Author: Velakoulis, Dennis ; Pantelis, Christos ; Ren, Boyu ; Hastings, Caroline ; Upadhyay, Jaymin ; Al-Hertani, Walla ; Berry-Kravis, Elizabeth M ; Brodeur, Kailey ; Di Biase, Maria ; van Gool, Raquel ; Shinn, Ann K ; Yang, Edward ; Lee, Pui Y ; Golden, Emma ; Walterfang, Mark ; Cropley, Vanessa ; Goodlett, Benjamin ; Reilly, Tom ; Cay, Mariesa

BACKGROUNDNiemann-Pick Disease Type C (NPC) is an ultra-rare disorder characterized by progressive psychiatric and neurologic manifestations, with late infantile, juvenile, and adolescent/adult presentations. We examined morphological properties of the choroid plexus, a protective blood-cerebrospinal fluid barrier, in NPC, and their relationship with neurodegeneration, clinical status, and circulatory markers. This study also determined whether choroid plexus morphology differentiates between NPC and more prevalent illnesses, schizophrenia (SZ) and bipolar disorder (BD), which have overlapping psychiatric symptoms with adolescent and adult-onset NPC and are associated with misdiagnosis.METHODSPatients with NPC were assessed using neuroimaging, clinical instruments, and plasma protein quantification focusing on inflammatory markers. Morphological properties (i.e., choroid plexus volumes) were compared between patients with NPC (n = 17), SZ (n = 20), BD (n = 24), and healthy controls (HCs, n = 106).RESULTSChoroid plexus enlargement (p < 0.05) and reduced thalamic volumes (p < 0.05) were observed in NPC patients versus HCs and SZ or BD patients. A logistic regression model with choroid plexus and thalamic volumes as predictors yielded high prediction accuracy for NPC vs. HCs, NPC vs. SZ, and NPC vs. BD (area under the receiver operating characteristics curve [AUROC] of 1). Choroid plexus volumes were negatively correlated with left (p = 0.009-0.012) and right (p = 0.007-0.025) thalamic volumes, left (r = -0.69, p = 0.003) and right (r = -0.71, p = 0.002) crus I of the cerebellum, and greater severity on the NPC-Suspicion Index psychiatric subscale (ρ = 0.72, p = 0.042). Targeted protein expression quantification revealed differential expression of TGFA, HLA-DRA, TNFSF12, EGF, INFG, and IL-18 in NPC patients vs. HCs (p < 0.05), with higher choroid plexus volumes correlating with IL-18 levels (ρ = 0.71, p = 0.047).CONCLUSIONThe choroid plexus may play a critical role in NPC neuropathogenesis and serve as a novel biomarker for monitoring neurodegenerative and inflammatory processes in NPC.

01 Jan 2025·Journal of Ethnopharmacology

Fu-Zheng-Li-Fei Recipe (FZLFR) in the treatment of cancer cachexia: Exploration of the efficacy and molecular mechanism based on chemical characterization, experimental research and network pharmacology

Article

Author: Yin, Aining ; Li, Honglin ; Dong, Peipei ; Wang, Tingxin ; Fu, Yu ; Yao, Wei ; Ye, Xueke ; Wang, Xiufang

ETHNOPHARMACOLOGICAL RELEVANCEFZLFR was derived from a classic traditional Chinese medicine recipe, the Shiquan-Dabu decoction. FZLFR is commonly used in clinical practice to address muscle loss and associated cancer cachexia. However, the mechanism of by which FZLFR acts in cancer cachexia remains unclear.AIMThis study aimed to assess the effects and explore the potential mechanism of action of FZLFR in treating cancer cachexia.METHODSCancer cachexia was induced by inoculating Lewis lung carcinoma cells into the right flank of male C57BL/6 mice. The efficacy of FZLFR was evaluated by comparing changes in body weight, tumor mass, food intake, survival time, weight, and cross-sectional area of the gastrocnemius and anterior tibial muscles. Moreover, inflammatory cytokines, such as TNF-α and IL-6, were detected by ELISA. The chemical components of FZLFR were analyzed using ultra-performance liquid chromatography-coupled with time-of-flight mass spectrometry. Network pharmacology analysis was performed to screen the core targets and potential pathways involved in FZLFR treatment of cancer cachexia. Molecular docking was used to analyze the binding ability of the core targets and key compounds. The expression levels of core targets and targets correlated with skeletal muscle atrophy were also assessed using western blotting.RESULTSFZLFR enhanced the food intake and survival rate of mice with cancer cachexia. It also alleviated tumor-induced body weight loss, tumor growth, and muscle fiber atrophy in these mice. Additionally, it improved the weight and cross-sectional area of the gastrocnemius and anterior tibial muscles. FZLFR down-regulated the serum levels of TNF-α and IL-6. UPLC-ESI-Q-TOF-MS analysis identified 184 compounds in FZLFR. Network pharmacology analysis predicted that TNF signaling pathway, ErbB signaling pathway and VEGF signaling pathway might be essential in FZLFR action. Molecular docking showed that kaempferol, upafolin, apigenin, and luteolin might play key roles in FZLFR treatment. Moreover, FZLFR decreased MAFBx1, MURF1, NF-κB, TWEAK, MAPK8, and EGFR expression levels. FZLFR enhanced the expression of VEGFA and ESR1, as demonstrated by western blotting.CONCLUSIONSFZLFR increased food intake and alleviated muscle atrophy in mice with cancer cachexia. The potential pharmacological mechanisms underlying its anticachexia effects include reducing inflammation, enhancing muscle vascular growth, inhibiting tumor angiogenesis, and modulating estrogen receptors.

News (Medical) associated with TWEAK

08 Dec 2023

·www.fiercebiotech.com

Graphite breaks apart, with founder inking deal for abandoned sickle cell prospect, gene-editing tech

Graphite entered into a license and option agreement with an undisclosed third party in August Matthew Porteus, M.D., Ph.D., is trying to write another chapter for his sickle cell disease project. Three years after Graphite Bio launched to build on his work, Porteus has struck a deal to save the floundering project and advance deeper into the clinic under a new biotech. Porteus studied the use of CRISPR to correct the mutation that drives sickle cell at his Stanford University lab. The studies led to Graphite, which listed Porteus as a scientific founder when it emerged with a $45 million series A round in 2020. Graphite’s story quickly took a dark turn, with the biotech seeing a serious adverse event in the first patient it dosed and halting development of the candidate weeks later. Those events marked the beginning of the end for Graphite, which went from raising a $238 million IPO to entering into a reverse merger in less than 30 months. But Porteus has given the sickle cell program a chance of outliving the biotech that first tried to bring it to market. The Stanford professor has co-founded a new biotech, Kamau Therapeutics, to emerge from the ashes of Graphite. Kamau “received an option to acquire all genome editing assets” through a “strategic transaction with Graphite.” The newly minted biotech plans to study the sickle cell asset, nulabeglogene autogedtemcel (nula-cel), that Graphite walked away from in the wake of the adverse event. Investigators have now tracked the patient who received nula-cel for one year. Ahead of the release of the one-year data Monday, Kamau shared a look at six-month results, identifying “lower-than-expected cell survival rate, necessitating platelet and red blood cell transfusions due to low platelet counts” as a problem and fingering eltrombopag as the cause of the adverse event. Eltrombopag is used to treat low platelets in the blood and was not initially part of the trial protocol. The findings have informed a focus on manufacturing. Kamau is working with an outsourcing partner to increase cell yield and improve overall cell health. The goal is to establish a more robust manufacturing framework. Graphite entered into a license and option agreement with an undisclosed third party in August. Under the terms of the deal, the third party secured an option on nula-cel and related assets and gave Graphite a 20% stake in its business. The option was contingent on the timely achievement of “a financing milestone” by the third party. Graphite’s last update described a tweak it made to the agreement in September. Meanwhile, what's left of Graphite folded into vision-loss biotech LENZ Therapeutics in November.

License out/inGene TherapyAcquisition

12 Sep 2022

·www.biopharmadive.com

Mitochondrial drugs, with a twist: Pretzel Therapeutics launches with $72.5M in funding

With a name like Pretzel Therapeutics, some may think the fledgling biotechnology company specializes in baking.The startup, officially launched Monday by a trio of European mitochondrial biology researchers, is instead looking at rare genetic disorders and diseases of aging such as Alzheimers and Parkinsons.With $72.5 million in Series A funding, Pretzel plans to advance more than five research programs using technologies that involve gene editing as well as control mitochondrial gene expression and health.Pretzels name was inspired by the shape of mitochondria, which resembles the twists of the German bread.A mitochondrion supplies cells with the power they need to survive. They turn the energy the body gets from food into fuel that cells use for a variety of chemical reactions.When their DNA, or mtDNA, mutates in certain ways, mitochondria produce less energy, preventing cells from functioning properly. Mitochondrial dysfunction is the cause of dozens of rare genetic diseases, and is thought to be a factor in common age-related disorders such as Alzheimer's.Pretzels scientists aim to use gene editing to remove mutated mtDNA that other genome manipulation techniques such as CRISPR cant reach because of the organelles tiny size, said Jay Parrish, Pretzels CEO.The company also hopes to control mitochondrial genome expression by targeting with small molecule drugs the enzymes involved in mtDNA replication, transcription and translation. Small molecule drugs might also be used to tweak the mitochondrias systems for quality control.A handful of other companies are focused on mitochondrial diseases. Stealth BioTherapeutics, which until recently traded under the stock ticker MITO, is one of the most advanced, with a drug candidate in late-stage testing. But its hit several significant setbacks, falling short in a previous Phase 3 study and getting a drug application rejected by the Food and Drug Administration.Elsewhere, Mitobridge, a biotech bought by Astellas in 2017, is in clinical testing with two drugs. Vincere Biosciences is researching small molecules to improve mitochondrial quality, while Reneo Pharmaceuticals is developing drugs to treat rare genetic diseases caused by mitochondrial dysfunction.But Pretzel claims it is looking at mitochondrial disease more broadly than others in the field.People have been working with the mitochondria for a long time but this is a different approach, Parrish said. The mitochondria itself is an amazing organelle that does all these cool things beyond just energy production. There are drugs that hit it, but it has untapped potential.The company will consider raising another round of private funding in one to two years, but Parrish declined to say when it expects to advance a drug into the clinic. By then, Pretzel also hopes to have begun research on how its platform can treat diseases that arent directly caused by mitochondrial dysfunction, such as rare cancers.Arch Venture Partners and Mubadala Capital first began building Pretzel in early 2020, aiming to create a platform biotech company. Then, Paul Thurk, the Arch partner leading the project, suddenly died in January 2021.Three investors Parrish, Arch managing director Kristina Burow and Mubadala executive director Alaa Halawa forged on with the project in honor of Thurk.We were able to recover due to the team who are not just great scientists or great investors, but really great people, said Gabriel Martinez, one of Pretzels directors.Pretzel will be based in Waltham, Mass. with a research facility in Gothenburg, Sweden.Arch and Mubadala, a sovereign venture capital fund from the United Arab Emirates, invested $15 million apiece in the company. GV, Invus and Angelini Ventures filled out the round along with more than half a dozen other investors.Though Pretzel isn't disclosing exactly which diseases its targeting, its investors see a wide range of possibilities.Were more intrigued and excited by the hard-to-reach fruits like Alzheimer's and diabetes, which we believe this company is poised to address, Halawa said. '

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TWEAK

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