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Last update 08 May 2025

WHO Grade III Mixed Glioma

Last update 08 May 2025

Basic Info

Synonyms

Anaplastic Mixed Glioma, Anaplastic Oligoastrocytoma, Anaplastic Oligoastrocytoma, NOS

+ [8]

Introduction

A central nervous system tumor with morphological features of anaplastic oligoastrocytoma in which there is insufficient information on the IDH genes status.

Drugs associated with WHO Grade III Mixed Glioma

Gallium GA-68 Gozetotide

Target

PSMA

Mechanism

PSMA inhibitors

Active Org.

Mayo Clinic [+14]

Originator Org.

The University of California, San Francisco

Active Indication

PSMA-Positive Prostatic Cancer [+13]

Inactive Indication

Adenocarcinoma of prostate [+3]

Drug Highest PhaseApproved

First Approval Ctry. / Loc.

United States

First Approval Date01 Dec 2020

Selinexor

Target

ACADS x XPO1

Mechanism

ACADS inhibitors [+1]

Active Org.

Karyopharm Therapeutics, Inc. [+9]

Originator Org.

Karyopharm Therapeutics, Inc.

Active Indication

Follicular Lymphoma [+72]

Inactive Indication

Acute Myeloid Leukemia with FLT3/ITD Mutation [+59]

Drug Highest PhaseApproved

First Approval Ctry. / Loc.

United States

First Approval Date03 Jul 2019

Palbociclib

Target

CDK4 x CDK6

Mechanism

CDK4 inhibitors [+1]

Active Org.

Hoffmann-La Roche, Inc. [+19]

Originator Org.

Pfizer Inc.

Active Indication

Breast cancer recurrent [+115]

Inactive Indication

acute leukemia [+46]

Drug Highest PhaseApproved

First Approval Ctry. / Loc.

United States

First Approval Date03 Feb 2015

102

Clinical Trials associated with WHO Grade III Mixed Glioma

NCT06444412

/ RecruitingPhase 2IIT

GA-68 PSMA-11 PET to Evaluate Malignant Glioma Recurrence - a Pilot Study

This clinical trial evaluates whether gallium-68 (Ga-68) prostate specific membrane antigen (PSMA)-11 positron emission tomography (PET)/computed tomography (CT) imaging is useful in differentiating between disease that has come back after a period of improvement (recurrence) or that is growing, spreading, or getting worse (progression) and treatment effect in patients with glioma. Patients with glioma undergo frequent imaging for assessment of disease status. After first-line treatment however, the correlation between imaging findings and tumor activity can be confused, and surgery is often required for definitive diagnosis. The PET/CT scanner is an imaging machine that combines 2 types of imaging in a single scan. The PET scanner detects and takes pictures of where the radioactive imaging agent (68Ga PSMA-11) has gone in the body and the CT scanner uses x-rays to take structural pictures inside the body. PSMA PET also binds to neoplastic blood vessels, including those in gliomas. This study may help researchers learn whether GA-68 PSMA-11 PET/CT is useful for improving detection of tumor recurrence or progression, as opposed to treatment effects, in patients with gliomas.

Start Date26 Jul 2024

Sponsor / Collaborator

Mayo Clinic

NCT05984667

/ RecruitingNot ApplicableIIT

C-SMART for Patients With Primary Brain Tumors: A Feasibility and Acceptability Pilot of a Novel Neuropsychological Intervention

The goal of Phase IIa Trial is to determine the feasibility and acceptability of telehealth C-SMART for patients with primary brain tumor and mild neurocognitive deficits (N=36) and their caregivers (N=36) A subset (n=10) of participants will undergo rs-fMRI both pre- and post-C-SMART to test feasibility of advanced functional imaging in this population.

Start Date15 Sep 2023

Sponsor / Collaborator

Virginia Commonwealth University

[+2]

ACTRN12623000096651

/ RecruitingPhase 2IIT

LUMOS2: Low & Anaplastic Grade Glioma Umbrella Study of Molecular Guided TherapieS

Start Date11 Sep 2023

Sponsor / Collaborator

The University of Sydney

100 Clinical Results associated with WHO Grade III Mixed Glioma

100 Translational Medicine associated with WHO Grade III Mixed Glioma

0 Patents (Medical) associated with WHO Grade III Mixed Glioma

527

Literatures (Medical) associated with WHO Grade III Mixed Glioma

07 Mar 2025·Neuro-Oncology

Reappraisal of prognostic factors in CNS WHO grade 3 oligodendrogliomas IDH-mutant and 1p/19q co-deleted: Lessons from the French POLA cohort

Article

Author: Dehais, Caroline ; Hamdan, N ; Bauchet, L ; Aubriot-Lorton, H ; Tortel, MC ; Joubert, C ; Rousselot-Denis, C ; Bernier, M ; Meyronet, D ; Gaultier, C ; Labrousse, F ; Dhermain, F ; Uro-Coste, E ; Wager, M ; Carpentier, A ; Campone, M ; Quintin-Roué, I ; Khallil, T ; Forest, F ; Adam, C ; Vauleon, E ; Cruel, T ; Ducray, François ; Dehais, C ; Seizeur, R ; Colin, Carole ; Chinot, O ; Colin, P ; Ghiringhelli, F ; Carpiuc, I ; Blechet, C ; Bronnimann, C ; Rousseau, A ; Abad, M ; Gauchotte, G ; Carpentier, Catherine ; Noel, G ; Adle-Biassette, H ; Bourg, V ; Cohen-Moyal, E ; Andraud, M ; Khettab, M ; Parker, F ; Uro-Coste, Emmanuelle ; Ducray, F ; Lopez, S ; Faillot, T ; Rigau, V ; Touat, Mehdi ; Figarella-Branger, D ; Desenclos, C ; Motso-Fotso, MJ ; Idbaih, Ahmed ; Tabouret, Emeline ; Maurage, CA ; Younan, N ; Menei, P ; Chiforeanu, D ; Cazals-Hatem, D ; Seyve, Antoine ; Langlois, O ; Bielle, F ; Diebold, MD ; Figarella-Branger, Domique ; Guillamo, J-S ; Milin, S ; Gueye, EM ; Ricard, D ; Appay, Romain ; Djelad, A ; Guillain, N ; Mokhtari, Karima ; Lhermitte, B ; Taillandier, L ; Zemmoura, I ; Vandenbos-Burel, F ; Richard, P ; Loussouarn, D ; Roger, P ; Marguet, F ; Chotard, G ; Godfraind, C

AbstractBackgroundIn the POLA cohort, 3 pathological groups of CNS WHO grade 3 oligodendroglioma IDH-mutant and 1p/19q co-deleted have been described: group 1 (high mitotic count only), group 2 (microvascular proliferation MVP and no necrosis), and group 3 (MVP and necrosis).Methods494 patients from the POLA cohort, with a median follow-up of 96 months were included. To identify the impact of the pathological groups and contrast enhancement (CE) in group 1 on overall survival (OS) or progression-free survival (PFS), survival curves were obtained (Kaplan–Meier method) and compared (log-rank test). The prognostic value of clinical factors and CDKN2A homozygous deletion HD were also tested. Multivariate analysis was performed.ResultsSurvival analysis demonstrated that the pathological groups were associated with both progression-free survival (PFS P = .01) and overall survival (OS P = .001). In group 1, patients with CE (1CE+) had a poorer prognosis compared to those without (OS P = .028, PFS P = .006). Further stratification into group 1CE−, group 1CE+, group 2, and group 3 provided clearer prognostic distinctions (OS P = .002, PFS P < .0001). Other prognostic factors included age (OS P < .0001, PFS P = .002), extent of surgical resection (OS P = .001, PFS P = .003), KPS (OS P < .0001, PFS P = 0.002), postoperative treatment (OS P = .007, PFS P < .0001), and CDKN2A HD (OS and PFS P < .0001). The pathological groups remained of prognostic significance for PFS in multivariate analysis.ConclusionsNecrosis and CDKN2A HD are adverse prognostic factors of WHO grade 3 oligodendrogliomas, IDH-mutant, and 1p/19q co-deleted. Besides, in group 1 patients, lack of CE is a factor of better prognosis.

01 Feb 2025·BMJ Open

Low & Anaplastic Grade Glioma Umbrella Study of MOlecular Guided TherapieS (LUMOS-2): study protocol for a phase 2, prospective, multicentre, open-label, multiarm, biomarker-directed, signal-seeking, umbrella, clinical trial for recurrent IDH mutant, grade 2/3 glioma

Article

Author: Simes, John ; Ballinger, Mandy L ; Yip, Sonia ; Sebastian, Lucille ; Thomas, David M ; Pitz, Marshall ; De Abreu Lourenco, Richard ; Thavaneswaran, Subotheni ; O'Callaghan, Christopher ; Wheeler, Patrick J ; Hawkins, Cynthia ; Kong, Benjamin ; McParland, Kristen ; Barnes, Elizabeth H ; Sim, Hao-Wen ; Spyridopoulos, Desma ; Koh, Eng-Siew ; Gan, Hui K

IntroductionAll grade 2/3 gliomas are incurable and at the time of inevitable relapse, patients have significant unmet needs with few effective treatments. This study aims to improve outcomes by molecular profiling of patients at relapse, then matching them with the best available drug based on their molecular profile, maximising the chances of patient benefit while simultaneously testing multiple novel drugs.Methods and analysisLow & Anaplastic Grade Glioma Umbrella Study of MOlecular Guided TherapieS (LUMOS-2) will be an international, phase 2, multicentre, open-label, biomarker-directed, umbrella clinical trial for recurrent isocitrate dehydrogenase mutant, histologically grade 2/3 gliomas. Investigational treatment will be assigned based on molecular profiling of contemporaneous tissue obtained at disease relapse using next-generation sequencing. LUMOS-2 will begin with three therapeutic treatment arms: paxalisib, cadonilimab and selinexor. Patient molecular profiles will be assessed by an expert, multidisciplinary Molecular Tumour Advisory Panel. Patients whose molecular profile is considered suitable for a targeted agent like paxalisib will be allocated to that arm, others will be randomised to the available arms of the trial. The primary endpoint is progression-free survival at 6 months. Secondary objectives include assessment of overall survival, response rate, safety and quality of life measures. Two additional therapeutic arms are currently in development.Ethics and disseminationCentral ethics approval was obtained from the Sydney Local Health District Ethics Review Committee, Royal Prince Alfred Hospital Zone, Sydney, Australia (Approval: 2022/ETH02230). Other clinical sites will provide oversight through local governance processes, including obtaining informed consent from suitable participants. A report describing the results of the study will be submitted to international meetings and peer-reviewed journals.Trial registration numberACTRN12623000096651.

15 Jan 2025·Zhongguo xiu fu chong jian wai ke za zhi = Zhongguo xiufu chongjian waike zazhi = Chinese journal of reparative and reconstructive surgery

[Relationship between knee meniscus and posterior tibial slope in healthy adults and patients with anteromedial osteoarthritis in Heilongjiang province].

Article

Author: Guo, Shuxin ; Huan, Rui ; Guan, Shikun ; Liu, Ning

ObjectiveTo measure and analyze the relationships among the posterior tibial slope (PTS), meniscal slope (MS), and meniscus posterior horn thickness (MPHT) of the medial and lateral tibial plateau in healthy people and patients with anteromedial osteoarthritis (AMOA) in Heilongjiang province, so as to provide reference basis for appropriate tibial osteotomy and prosthesis placement angles in knee joint surgeries.MethodsA retrospective collection of imaging data from knee joint MRI examinations conducted prior to AMOA for various reasons was performed. A total of 103 healthy individuals (healthy group) and 30 AMOA patients (AMOA group) were included. There was no significant difference in the gender composition ratio, side, and body mass index between the two groups ( P>0.05); however, the comparison of ages between the two groups showed a significant difference ( P<0.05). The collected DICOM format image data was imported into the RadiAnt DICOM Viewer software and measured the medial PTS (MPTS), lateral PTS (LPTS), medial MS (MMS), lateral MS (LMS), medial MPHT (MMPHT), and lateral MPHT (LMPHT) with standard methods. The differences of the above indexes between the two groups and between different genders and sides in the two groups were compared, and Pearson correlation analysis was carried out. At the same time, the measured data of healthy group were compared with the relevant literature reported in the past.ResultsCompared to the healthy group, the AMOA group exhibited significantly smaller MPTS and LPTS, as well as significantly greater MMPHT and LMPHT, with significant differences ( P<0.05). However, there was no significant difference in the MMS and LMS between the two groups ( P>0.05). The differences in various indicators between genders and sides within the two groups were not significant ( P>0.05). The correlation analysis and regression curves indicated that both MPTS and LPTS in the two groups were positively correlated with their respective ipsilateral MS and MPHT ( P<0.05); as PTS increased, the rate of increase in MS and MPHT tend to plateau. Compared to previous related studies, the MPTS and LPTS measured in healthy group were comparable to those of the Turkish population, exhibiting smaller values than those reported in other studies, while MMS and LMS were relatively larger, and MMPHT and LMPHT were smaller.ConclusionIn healthy people and AMOA patients in Heilongjiang province, PTS has great individual differences, but there is no significant individual difference in MS. MPHT can play a certain role in retroversion compensation, and its thickness increase may be used as one of the indicators to predict the progression of AMOA. The above factors should be taken into account when UKA is performed, and the posterior tilt angle of tibial osteotomy should be set reasonably after preoperative examination and evaluation.

News (Medical) associated with WHO Grade III Mixed Glioma

13 Apr 2021

·www.biospace.com

Celularity Receives Orphan Drug Designation for Natural Killer Cell Therapy CYNK-001 in the Treatment of Malignant Gliomas

FLORHAM PARK, N.J., April 13, 2021 (GLOBE NEWSWIRE) -- Celularity Inc. (“Celularity”), a clinical-stage biotechnology company, leading the next evolution in cellular medicine with the development of off-the-shelf allogeneic therapies derived from the postpartum human placenta, announced today the U.S. Food and Drug Administration (FDA) has granted Orphan Drug Designation to the company’s non-genetically modified cryopreserved human placental hematopoietic stem cell-derived natural killer (NK) cell therapy, CYNK-001, for the treatment of patients with malignant gliomas. CYNK-001 is currently being investigated in a phase 1 clinical trial (NCT04489420) for the treatment of patients with glioblastoma multiforme (GBM), an indication within the scope of this orphan designation. “We are very pleased the FDA has granted Orphan Designation in malignant gliomas to continue to develop off-the-shelf therapies for serious unmet clinical needs,” said Robert J. Hariri, M.D., Ph.D., founder, Chairperson and Chief Executive Officer of Celularity. “Building on the FDA’s recent decision to grant Fast Track status to CYNK-001, we view the Orphan Drug Designation as yet another milestone on our journey to deliver patients a potentially novel treatment. To date, we have observed the potential of CYNK-001 in multiple preclinical models as well as early evidence of activity in the clinic and believe this approach may shift the paradigm in augmenting the body’s natural immune response to diseases such as glioblastoma, other cancer indications and infectious diseases. We are very excited to continue working with the FDA on the development of this exciting therapy.” About Orphan Drug Designation The Orphan Drug Act (ODA) encourages biotechnology and pharmaceutical companies to develop drugs for conditions which affect fewer than 200,000 people in the United States by providing economic incentives. To qualify for orphan designation, both the drug and the condition must meet criteria specified in the ODA and FDA’s implementing regulations 21 CFR Part 316. Orphan designation qualifies the drug sponsor for development incentives including tax credits for qualified expenses, reduction in the FDA user fee, and seven years of exclusivity for a drug that obtains approval. About Malignant Gliomas Glioma is a type of tumor that occurs in the brain and spinal cord. Malignant gliomas consist of glioblastoma multiforme (GBM), anaplastic astrocytoma, anaplastic oligodendroglioma, anaplastic oligoastrocytoma, anaplastic ependymoma, and anaplastic ganglioglioma. Malignant gliomas are associated with high morbidity and mortality. GBM accounts for the majority of malignant gliomas. Currently there are no effective long-term treatments for the disease. Patients with GBM usually survive less than 15 months following diagnosis. In most patients, the rapidly growing malignant tumor tends to recur within 6-8 months following treatment. Patients with recurrent GBM have even poorer prognosis. Therefore, malignant gliomas, such as GBM, are serious diseases with high unmet medical needs. About CYNK-001 Celularity’s lead therapeutic program based on its placental-derived unmodified NK cell type is CYNK-001, an allogeneic unmodified NK cell being developed as a treatment for hematologic malignancies, solid tumors, and infectious diseases. About Celularity Celularity, headquartered in Florham Park, N.J., is a clinical stage biotechnology company leading the next evolution in cellular medicine by developing off-the-shelf placental-derived allogeneic cell therapies, including unmodified NK cells, genetically-modified NK cells, T cells engineered with a CAR (CAR T-cells), and mesenchymal-like adherent stromal cells (ASCs) targeting indications across cancer, infectious and degenerative diseases. Celularity believes that by harnessing the placenta’s unique biology and ready availability, it will be able to develop therapeutic solutions that address significant unmet global needs for effective, accessible, and affordable therapies. In January 2021, Celularity entered into a definitive merger agreement with GX Acquisition Corp. to create a publicly listed leader in allogeneic cellular therapy. GX Acquisition Corp. is listed on Nasdaq under the ticker symbol “GXGX.” Upon closing of the business combination, expected to be completed in the second quarter of 2021, shares of the combined company will be listed on Nasdaq under the ticker symbol "CELU." To learn more, visit celularity.com. Celularity Investor Contacts: Carlos Ramirez Celularity carlos.ramirez@celularity.com Alexandra Roy Solebury Trout aroy@troutgroup.com Celularity Media Contact Jason Braco, Ph.D. LifeSci Communications (646)-751-4361 jbraco@lifescicomms.com

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WHO Grade III Mixed Glioma

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