Delving into the Latest Updates on Uprosertib with Synapse

Overview

Basic Info

Drug Type

Small molecule drug

Synonyms

Uprosertib (USAN/INN), GSK-2141795, GSK-2141795C

+ [4]

Target

Akt

Action

inhibitors

Mechanism

Akt inhibitors(Proto-oncogene proteins c-akt inhibitors)

Therapeutic Areas

NeoplasmsEye DiseasesSkin and Musculoskeletal Diseases+ [4]

Active Indication

Uveal MelanomaProteus SyndromeTelangiectasia, Hereditary Hemorrhagic

Inactive Indication

Adult Acute Myeloblastic LeukemiaAdvanced Triple-Negative Breast CarcinomaBRAF mutation positive Melanoma+ [34]

Originator Organization

GSK Plc

Active Organization

National Cancer Institute

Laekna Therapeutics (Shanghai) Co., Ltd.

Inactive Organization

GSK Plc

Novartis Pharmaceuticals Corp.

The University of California, San Francisco

+ [1]

License Organization

Laekna Therapeutics (Shanghai) Co., Ltd.

Novartis AG

GSK Plc

Drug Highest PhasePhase 2

First Approval Date-

Regulation-

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Structure/Sequence

Molecular FormulaC18H16Cl2F2N4O2

InChIKeyAXTAPYRUEKNRBA-JTQLQIEISA-N

CAS Registry1047634-65-0

This randomized phase II trial studies how well trametinib with or without Akt inhibitor GSK2141795 (GSK2141795) works in treating patients with uveal melanoma that has spread to other parts of the body (metastatic). Trametinib and GSK2141795 may stop the growth of tumor cells by blocking some of the enzymes needed for cell growth. It is not yet known whether trametinib is more effective with or without GSK2141795 in treating patients with metastatic uveal melanoma.

Start Date21 Nov 2013

Sponsor / Collaborator

National Cancer Institute

NCT01989598

/ CompletedPhase 2IIT

A Phase 2 Study of Sequential Trametinib and GSK2141795 in Relapsed or Refractory Multiple Myeloma

This phase II trial studies how well trametinib and Akt inhibitor GSK2141795 work in treating patients with multiple myeloma that has come back (relapsed) or that does not respond to treatment (refractory). Trametinib and Akt inhibitor GSK2141795 may stop the growth of cancer cells by blocking some of the enzymes needed for cell growth.

Start Date30 Oct 2013

Sponsor / Collaborator

National Cancer Institute

NCT01902173

/ CompletedPhase 1/2IIT

Phase I/II Study of the Safety and Efficacy of the AKT Inhibitor GSK2141795 in Combination With Dabrafenib and Trametinib in Patients With BRAF Mutant Cancer

This phase I/II trial studies the side effects and the best dose of uprosertib when given together with dabrafenib and trametinib and to see how well they work in treating patients with stage IIIC-IV cancer. Uprosertib, dabrafenib, and trametinib may stop the growth of tumor cells by blocking some of the enzymes needed for cell growth. Giving uprosertib with dabrafenib and trametinib may be a better treatment for cancer.

Start Date08 Oct 2013

Sponsor / Collaborator

National Cancer Institute

[+2]

100 Clinical Results associated with Uprosertib

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100 Translational Medicine associated with Uprosertib

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100 Patents (Medical) associated with Uprosertib

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69

Literatures (Medical) associated with Uprosertib

01 Apr 2025·MOLECULAR DIVERSITY

An in silico approach to identify novel and potential Akt1 (protein kinase B-alpha) inhibitors as anticancer drugs

Article

Author: Etikyala, Umadevi ; Dalimba, Udayakumar ; Manga, Vijjulatha ; Reddyrajula, Rajkumar ; Vani, T ; Kuchana, Vinutha

Akt1 (protein kinase B) has become a major focus of attention due to its significant functionality in a variety of cellular processes and the inhibition of Akt1 could lead to a decrease in tumour growth effectively in cancer cells. In the present work, we discovered a set of novel Akt1 inhibitors by using multiple computational techniques, i.e. pharmacophore-based virtual screening, molecular docking, binding free energy calculations, and ADME properties. A five-point pharmacophore hypothesis was implemented and validated with AADRR38. The obtained R² and Q² values are in the acceptable region with the values of 0.90 and 0.64, respectively. The generated pharmacophore model was employed for virtual screening to find out the potential Akt1 inhibitors. Further, the selected hits were subjected to molecular docking, binding free energy analysis, and refined using ADME properties. Also, we designed a series of 6-methoxybenzo[b]oxazole analogues by comprising the structural characteristics of the hits acquired from the database. Molecules D1-D10 were found to have strong binding interactions and higher binding free energy values. In addition, Molecular dynamic simulation was performed to understand the conformational changes of protein-ligand complex.

01 Apr 2025·FEBS LETTERS

Distinct dysregulated pathways in sporadic and Lynch syndrome‐associated colorectal cancer offer insights for targeted treatment

Article

Author: Musalula Sinkala ; Raj Ramesar ; May J. Krause

Lynch syndrome (LS) is a hereditary disorder that increases the risk of colorectal cancer (CRC) due to constitutional pathogenic variants in mismatch repair (MMR) genes. When coupled with somatic mutations in the same gene, MMR deficiency occurs. However, the mechanisms driving cancer development remain unclear. This study aimed to identify distinct molecular drivers in LS‐associated and sporadic CRC. We found that PI3K–Akt signalling is dysregulated in LS‐associated CRC, while Wnt signalling predominates in sporadic CRC. Moreover, our findings highlight the therapeutic potential of PI3K–Akt pathway inhibitors, such as taselisib, for LS‐associated CRC patients with high pathway dependency. Similarly, Wnt signalling pathway inhibitors, such as XAV939, offer a promising therapeutic approach for sporadic CRC. These findings underscore the importance of understanding the biological basis of disease for developing targeted therapies tailored to CRC subtype‐specific oncogenic pathways.

01 Feb 2025·ADVANCED FUNCTIONAL MATERIALS

Advanced Hierarchical Computational Modeling‐Based Rational Development of Platinum (II) Nanocomplex to Improve Lung Cancer Therapy

Article

Author: Yang, Da ; Li, Song ; Huang, Haozhe ; Chen, Shangyu ; Ji, Beihong ; Li, Shichen ; Huang, Yixian ; Burns, Timothy F ; Luo, Zhangyi ; Sun, Jingjing ; Wang, Junmei ; Chen, Yuang ; Li, Sihan ; Bain, Daniel J

Abstract:

Cancer stem cells (CSCs) are known to be one of the determining factors that contribute to therapeutic resistance. However, much remains to be understood about the reprogramming network leading to the generation of CSCs driven by chemotherapy. In this study, guided by bioinformatics study, deeper insight is uncovered and provided into the CSC enrichment mechanism driven by cisplatin (CDDP) treatment. It is discovered that CDDP can repopulate the level of CSC by activating AKT1 oncogenic pathway that is further enhanced by COX‐2 inflammatory signaling. Simultaneously blocking these two pathways can synergistically restrain the number of CSCs. Under the guidance of advanced hierarchical computational modeling, including molecular docking, molecular dynamics (MD) simulation and binding free energy analysis, MK‐2206 is selected as the AKT1 inhibitor to achieve optimal codelivery of CDDP, MK‐2206 and 5‐ASA (COX‐2 inhibitor) through 5‐ASA‐derivatized dual functional immunostimulatory nanocarrier (PASA). This triple combination (PASA/CDDP/MK‐2206) significantly reduces tumor burden in both orthotopic and metastatic lung cancer models. Mechanistic studies show that this improved therapeutic activity is due to elimination of CSCs and reversal of the immunosuppressive tumor microenvironment. This study suggests that PASA/CDDP/MK‐2206 may represent a simple and effective lung cancer therapy via reversing CSCs‐associated chemoresistance.

3

News (Medical) associated with Uprosertib

31 Jul 2025

·ryvu.com

Ryvu announces publication of novel target discovery data in colorectal cancer from the ONCO Prime platform - RYVU

Krakow, Poland – July 31, 2025 – Ryvu Therapeutics (WSE: RVU), a clinical-stage drug discovery and development company focused on novel therapies targeting emerging oncology indications, announces the publication of data from its proprietary ONCO Prime target discovery platform in the peer-reviewed Scientific Reports journal, part of Nature Portfolio. The manuscript is entitled “Integrated transcriptomic and functional modeling reveals AKT and mTOR synergy in colorectal cancer” and is now available online on the Scientific Reports Krzysztof Brzozka, PhD, Chief Scientific Officer of Ryvu Therapeutics, said: We are honored to have data from our ONCO Prime platform published and reviewed by expert peers in Nature Scientific Reports. The manuscript highlights the unique potential of our patient-derived primary cell cultures to reflect more accurately the complexity of patient tumors and therefore act as an ideal medium for novel therapeutic target discovery. The publication on AKT and mTOR synergy in colorectal cancer is just one example of the broad potential of the ONCO Prime platform across multiple tumor types as we continue to expand the platform. The publication focuses on the discovery of a synergistic therapeutic relationship between mTOR inhibition and AKT inhibition in colorectal cancer cells as one example of the potential of the ONCO Prime platform. Ryvu developed a drug discovery platform using patient-derived primary CRC cultures. Importantly, Ryvu’s engineered model and patient-derived cells reflect the complexity and heterogeneity of primary tumors, not observed with standard immortalized cell lines. High-throughput screening (HTS) of 4255 compounds identified 33 with selective efficacy against CRC cells, sparing normal, healthy epithelial cells. Among the tested combinations, everolimus (mTOR inhibitor) and uprosertib (AKT inhibitor) demonstrated promising synergy with favorable therapeutic window. This synergy might have been overlooked in traditional immortalized cell lines, highlighting the translational advantage of patient-derived systems. The integration of machine learning into the HTS pipeline significantly improved scalability, cost-efficiency, and predictive accuracy. These findings underscore the potential of patient-derived materials combined with machine learning-enhanced drug discovery to advance personalized therapies. Specifically, mTOR-AKT inhibition emerges as a promising strategy for CRC treatment, paving the way for more effective and targeted therapeutic approaches. Beyond the results published in this manuscript, the ONCO Prime platform has already led to the discovery of several other novel targets with therapeutic potential in CRC. These undisclosed, potential novel targets are currently being advanced through the drug discovery process at Ryvu. In addition, the ONCO Prime platform is expanding to other tumor types. Scientific Reports is a peer-reviewed, open-access journal, part of Nature Portfolio, publishing original research across the natural sciences, psychology, medicine and engineering. From nature.com: “Scientific Reports is the 5th most-cited journal in the world, with more than 734,000 citations in 2023, and receives widespread attention in policy documents and the media.” Project is co-financed by the European Union under the Operational Programme European Funds for Modern Economy 2021-2027. Project title: “ONCO Prime: new possibilities for personalised anti-cancer therapy based on patient-derived primary cell cultures, omics characterisation, and functional assays”. Grant Agreement no: FENG.01.01-IP.02-0095/23.

29 Jan 2024

·www.fiercebiotech.com

After GSK and Novartis handoffs, Laekna's drug fails ovarian cancer trial

After handoffs from GSK and then Novartis, afuresertib landed at Laekna. Shanghai-based biotech Laekna's oral cancer drug afuresertib has failed to significantly improve progression-free survival for ovarian cancer patients in a phase 2 trial. Originally developed by GSK, afuresertib swapped Big Pharma hands, previously falling under Novartis’ possession until being out-licensed to Laekna in 2018. That deal encompassed two oral pan-Akt kinase inhibitors—afuresertib and uprosertib—both of which originated at GSK. The two drugs have been tested against ovarian and gastric cancers, multiple myeloma, melanoma and other diseases. Now, afuresertib has failed to meet the primary target of a global phase 2 registrational trial in platinum-resistant ovarian cancer (PROC) conducted in the U.S. and China, according to a Jan. 28 release (PDF). The open-label study, dubbed PROFECTA II, assessed afuresertib alongside the chemotherapy paclitaxel in a total of 150 patients. In the study, 94 patients received the investigational combo, while 47 received solo paclitaxel. The drug failed to reach statistical significance on the trial’s primary endpoint of progression-free survival. However, Laekna said a phosphor-AKT positive biomarker subgroup experienced significantly improved PFS, with their median PFS reaching 5.4 months compared to 2.9 months. The biotech reported a manageable and tolerable safety profile, with adverse events consistent with the known safety profiles of the individual treatments. Further data from the trial will be presented at an unnamed medical conference, according to the company release. Laekna said it expects to discuss the results with regulatory authorities in hopes of identifying a registration path for PROC patients who may benefit from afuresertib.

Phase 2Clinical ResultPhase 3

01 Aug 2018

·www.biospace.com

China’s Laekna Inks Two-Drug Deal with Novartis

Laekna, headquartered in Shanghai, China, signed a deal with Novartis Pharma AG for exclusive worldwide rights to two oral Novartis clinical-stage cancer drugs. Laekna, headquartered in Shanghai, China, signed a deal with Novartis Pharma AG for exclusive worldwide rights to two oral Novartis clinical-stage cancer drugs. The compounds are oral pan-Akt kinase inhibitors, afuresertib (ASB183) and uprosertib (UPB795). More than 10 clinical Phase I/II studies have been performed on the drugs for a variety of cancer indications, including ovarian and gastric cancer, multiple myeloma, melanoma, and others. The Pten/PI3K/Akt signaling axis is an important pathway linked to cancer growth. Drugs that inhibit this pathway have been shown to be effective in slowing cancer growth. Laekna has “mapped out several clear registration paths for NDA approval potentially as the first in class medicine,” according to a company statement. Novartis picked up the two drugs several years ago from GlaxoSmithKline when they swapped vaccines for cancer products. As part of the deal, Novartis will acquire an equity stake in Laekna, in addition to upfront fees and development milestones. There are also royalties on future sales, although details have not been disclosed. “Novartis is a global leader in oncology drug innovation,” said Chris Lu, founder and chief executive officer of Laekna, in a statement. “This is the second licensing agreement between Laekna and Novartis, adding to the previous licensing of CFG920 less than a year ago. We have demonstrated to Novartis that Laekna is a valuable collaborator with our strong commitment, experienced team and financing support from the top investment partners.” CFG920 is a CYP17 inhibitor, an oral androgen inhibitor, for prostate cancer. Prior to the in-licensing, Novartis reported positive data from a proof-of-concept clinical trial of the compound in patients with metastatic castration-resistant prostate cancer. BioPharmaDive writes, “The deal fits with the larger trend of big pharma divesting non-core assets in a push to focus more narrowly on core therapeutic areas. AstraZeneca , Pfizer and GlaxoSmithKline have all been particularly active in recent years. Novartis is doing much of the same, both in smaller deals like this one and its more sweeping plans to spin out its Alcon eye care business into a standalone device company. While Novartis considers oncology one of its key growth areas, the company has recently chosen to focus more on the immuno-oncology space and cell therapies in hopes of gaining an edge, while also advancing some targeted oncology therapies.” On July 10, Novartis signed a deal with another Chinese company, Adlai Nortye Biopharma. Under that deal, except for a few rights Novartis is keeping, Adlai Nortye picked up exclusive development and commercialization rights to buparlisib. Buparlisib, or BKM120, is an oral pan-PI3K inhibitor targeting all class 1 PI3K isoforms and is active in hematologic cancers and solid tumors. It has shown efficacy in a combination with paclitaxel in head and neck squamous cell carcinoma (HNSCC) and received Fast Track Designation from the U.S. Food and Drug Administration (FDA) . “Buparlisib has been extensively profiled in breast cancer and other tumor types,” said Carsten Lu, chief executive officer of Adlai Nortye in a statement. “Buparlisib when combined with other therapies has shown impressive anti-cancer efficacy in HNSCC. It has very good market prospects when combined with paclitaxel, and we are planning to carry out clinical trials of combination of buparlisib and immune check point inhibitor treatment.” No financial details were divulged for that deal, either.

License out/inFast TrackPhase 1

100 Deals associated with Uprosertib

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External Link

KEGG	Wiki	ATC	Drug Bank
D10674	-	-	DB11969

R&D Status

10 top R&D records.

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Indication	Highest Phase	Country/Location	Organization	Date
Uveal Melanoma	Phase 2	United States	National Cancer Institute	21 Nov 2013
Uveal Melanoma	Phase 2	France	National Cancer Institute	21 Nov 2013
Uveal Melanoma	Phase 2	United Kingdom	National Cancer Institute	21 Nov 2013
Recurrent Multiple Myeloma	Phase 2	Canada	National Cancer Institute	30 Oct 2013
Refractory Multiple Myeloma	Phase 2	Canada	National Cancer Institute	30 Oct 2013
Relapse multiple myeloma	Phase 2	Canada	National Cancer Institute	30 Oct 2013
BRAF V600E mutant Colorectal Cancer	Phase 2	United States	GSK Plc	08 Oct 2013
BRAF V600E mutant Colorectal Cancer	Phase 2	United States	Novartis Pharmaceuticals Corp.	08 Oct 2013
Hematologic Neoplasms	Phase 2	United States	GSK Plc	08 Oct 2013
Hematologic Neoplasms	Phase 2	United States	Novartis Pharmaceuticals Corp.	08 Oct 2013

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Clinical Result

Indication

Phase

Evaluation

View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT01902173 (SWOG S1221, CTgov)	Phase 1/2	Locally Advanced Malignant Solid Neoplasm \| Metastatic Solid Tumor \| Melanoma, Cutaneous Malignant ... View more	27	dabrafenib+GSK2141795 (Phase 1 Doublet Regimen)	reidadpvtd = tbiqzbaqcf wloskidjru (ydlvbtcskz, fehakoaffq - jshsfckipf)	-	14 Oct 2020
NCT01902173 (SWOG S1221, CTgov)	Phase 1/2		27	dabrafenib+trametinib+GSK2141795 (Phase 1 Triplet Regimen)	reidadpvtd = jmhxfhtnyi zbrrzmxfea (lasogzlbet, cyqsccaxle - fljvemjadb)	-	14 Oct 2020
NCT01138085 (Pubmed) Manual	Phase 1	Solid tumor	126	uprosertib+trametinib	sqwekalaar(ooowfexnwu) = Adverse events (AEs) were consistent with those reported in monotherapy studies but occurred at lower doses and with greater severity. uuxocknrft (agvpgrakvy )	Negative	01 Apr 2020
NCT01964924 (CTgov)	Phase 2	Breast cancer recurrent \| Metastatic breast cancer \| Invasive Mammary Carcinoma ... View more	37	Laboratory Biomarker Analysis+Akt Inhibitor GSK2141795+Trametinib	aqakgdtimp = kajoatocmh hxqmbriypl (almwmfxcuc, xvhnlelbkw - irrzeidfwd) View more	-	20 Sep 2019
NCT01907815 (Pubmed \| Clin Lymphoma Myeloma Leuk) Manual	Phase 2	Acute Myeloid Leukemia RAS Mutation	23	Trametinib+GSK2141795	fntkwiehzl(qakhiurxms) = No complete remissions were identified in either cohort nvbellaxbf (stssajxjjk ) View more	Positive	01 Jul 2019
NCT01958112 (Pubmed \| Obstet Gynecol Surv) Manual	Phase 2	Uterine Cervical Cancer PI3K \| RAS	14	trametinib+GSK2141795	yieyknzflf(cjnjgqkcsh) = ajnjuqiyjt egdagjrhzf (tnxahvafzw ) View more	Negative	01 Jul 2019
NCT01958112 (CTgov)	Phase 2	Recurrent Cervical Cancer	14	GSK1120212 (trametinib)+GSK2141795	yjldoytltp(eirrvccbeq) = uvcnznfnlh mxeowtckxc (nuowbyheuk, njajbcaqsf - sovzhqczdu) View more	-	02 Jan 2019
NCT00920257 (Pubmed \| Invest New Drugs) Manual	Phase 1	Solid tumor	77	GSK2141795	todackebbl(aksvrvmobk) = eflvpsmtew msgszjvrnp (gcljrvhnfq ) View more	Positive	01 Dec 2018
NCT01907815 (CTgov)	Phase 2	Adult Acute Myeloblastic Leukemia	24	GSK2141795+Trametinib (Trametinib 2.0 mg + GSK2141795 25 mg)	iuyjazfuhy = wybrojlbow dyweimfbaz (vbxpcnlkpi, josdppvkax - byasytfsao) View more	-	06 Apr 2018
NCT01907815 (CTgov)	Phase 2	Adult Acute Myeloblastic Leukemia	24	GSK2141795+Trametinib (Trametinib 1.5 mg + GSK2141795 50 mg)	iuyjazfuhy = zqjhzmyywq dyweimfbaz (vbxpcnlkpi, rlbvworvjk - yxdwahnwbu) View more	-	06 Apr 2018
NCT01941927 (Pubmed \| Pigment Cell Melanoma Res) Manual	Phase 2	NRAS Mutant Melanoma NRAS Mutation \| BRAF Wild-type \| NRAS Wild-type	20	trametinib+GSK2141795 (NRAS-mutant patients)	jxjarpphhr(ipscwrugbe) = No objective responses were noted in either cohort. chvsmvxvel (pohfkbtezk ) View more	Negative	01 Jan 2018
NCT01941927 (Pubmed \| Pigment Cell Melanoma Res) Manual	Phase 2		20	trametinib+GSK2141795 (BRAFWT NRASWT patients)		Negative	01 Jan 2018
NCT01902173 (SWOG S1221, ASCO 12017 \| ASCO 22017) Manual	Phase 1	BRAF mutation Solid Tumors BRAF V600 mutant	19	dabrafenib+GSK2141795	vchqloeohi(wvnekyblff) = At the highest triplet dose with dabrafenib 150 mg bid, trametinib 2 mg qd with GSK2141795 75 mg qd, 1 of 2 evaluable pts had a DLT of grade 3 febrile neutropenia and grade 3 maculo-papular rash efilyfwwow (tbabztplry )	Positive	05 Jun 2017
NCT01902173 (SWOG S1221, ASCO 12017 \| ASCO 22017) Manual	Phase 1	BRAF mutation Solid Tumors BRAF V600 mutant	19	dabrafenib+trametinib+GSK2141795		Positive	05 Jun 2017