To evaluate the safety and tolerability of escalating doses of ERAS-801 in study participants with recurrent glioblastoma multiforme (GBM).
To determine the Maximum Tolerated Dose (MTD) and/or Recommended Dose (RD) of ERAS-801.
To evaluate the antitumor activity of ERAS-801.
To evaluate the PK profile of ERAS-801.

Start Date25 Feb 2022

Sponsor / Collaborator

Erasca, Inc.

100 Clinical Results associated with ERAS-801

100 Translational Medicine associated with ERAS-801

100 Patents (Medical) associated with ERAS-801

Literatures (Medical) associated with ERAS-801

01 Apr 2012·Osteoarthritis and cartilageQ2 · MEDICINE

Insulin-like growth factor-1 boosts the developing process of condylar hyperplasia by stimulating chondrocytes proliferation

Q2 · MEDICINE

Article

Author: J. Li ; W. Fang ; J. Ke ; H. Cai ; Q. Meng ; X. Long ; S. Chen ; Y. Chen ; M. Deng

OBJECTIVE:

The etiology of Condylar hyperplasia (CH) of human temporomandibular joint (TMJ) remains largely unknown. Our previous study has demonstrated that enriched insulin-like growth factor-1(IGF-1) was expressed in the proliferation and hypertrophic layers of CH cartilage. Accordingly, this study was aimed to investigate whether IGF-1 regulates CH chondrocytes proliferation in condylar cartilage overgrowth and explore the molecular mechanism of IGF-1 involved in.

METHODS:

Chondrocytes were isolated from 6 CH and 3 normal cartilage (NC) specimens and cultured in alginate beads or monolayer, treated with IGF-1 or specific inhibitors such as 7-[trans-3-[(azetidin-1-yl)methyl]cyclobutyl]-5-(3-benzyloxyphenyl)-7H-pyrrolo[2,3-d]pyrimidin-4-amine (NVP-AEW541), U0126, and LY294002. Thereafter, cellular proliferation capacity was evaluated by Cell Viability Analyzer (alginate beads culture) or 3-(4,5-dimethylthiazo(-2-yl)-2,5-diphenyltetrazolium bromide (MTT) (monolayer culture). Gene expression levels of IGF-1, IGF-1 receptor (IGF-1R), collagen type II, type X and those genes associated with proliferation were evaluated by realtime PCR. Protein levels of IGF-1 and IGF-1R synthesized by CH chondrocytes were accessed by enzyme-linked immunosorbent assay (ELISA) and western blotting.

RESULTS:

CH chondrocytes enhanced cellular proliferation capacity and expressed significantly higher levels of messenger RNA (mRNA) and protein expressions of IGF-1 and IGF-1R, as compared with NC chondrocytes. Furthermore, enriched IGF-1 enhanced CH chondrocytes proliferation, up-regulated the expressions of specific genes associated with cellular proliferation and elevated the gene expression of collagen type II A1 (COL2A1). Besides, IGF-1-mediated CH chondrocytes proliferation mainly depended on the mitogen-activated protein kinase (MAPK)-ERK pathway.

CONCLUSIONS:

IGF-1 promotes human TMJ cartilage overgrowth in the developing process of CH by enhancing chondrocytes proliferation via MAPK-ERK pathway.

01 Jun 2008·European journal of pharmacologyQ3 · MEDICINE

Role of brain nicotinic acetylcholine receptor in centrally administered corticotropin-releasing factor-induced elevation of plasma corticosterone in rats

Q3 · MEDICINE

Article

Author: Junichi Arai ; Kunihiko Yokotani ; Naoko Yamaguchi-Shima ; Takahiro Shimizu ; Shoshiro Okada ; Hiroshi Wakiguchi ; Lu Lianyi

The present study was undertaken to clarify the central mechanisms involved in the intracerebroventricularly administered corticotropin-releasing factor-induced elevation of plasma corticosterone in urethane- and alpha-chloralose-anesthetized rats using microdialysis and immunohistochemical techniques. When corticotropin-releasing factor was given at 0.5, 1.5, and 3.0 nmol/animal intracerebroventricularly, it dose-dependently increased noradrenaline release but not adrenaline release in the hypothalamic paraventricular nucleus. The 1.5 nmol/animal dose of corticotropin-releasing factor-induced noradrenaline release was attenuated by CP-154,526 (butyl-ethyl-{2,5-dimethyl-7-(2,4,6 trimethylphenyl)-7H-pyrrolo[2,3-d]pyrimidin-4-yl}amine), a selective corticotropin-releasing factor receptor 1 antagonist, at 1.3 micromol/animal, intracerebroventricularly, and was also abolished by phentolamine at 0.66 micromol/animal, intracerebroventricularly. In addition, the corticotropin-releasing factor-induced elevation of noradrenaline release in the hypothalamic paraventricular nucleus and plasma corticosterone were abolished by hexamethonium, a non-selective nicotinic acetylcholine receptor antagonist, at 1.8 micromol/animal, intracerebroventricularly, and alpha-conotoxin MII, a potent alpha(3)beta(2) nicotinic acetylcholine receptor antagonist, at 30 nmol/animal, i.c.v. Corticotropin-releasing factor at 1.5 nmol/animal, i.c.v. evoked a significant expression of Fos, an immediate-early transcription factor in neurons, on the dopamine-beta-hydroxylase-containing neurons and alpha(3) nicotinic acetylcholine receptor subunit-expressing neurons in the locus coeruleus, but not in the medullary A(1) and A(2) regions containing noradrenergic neurons. These results suggest that centrally administered corticotrophin-releasing factor elevates plasma corticosterone by the corticotropin-releasing factor 1 receptor and alpha(3) subunit-containing nicotinic acetylcholine receptor (probably alpha(3)beta(2) nicotinic acetylcholine receptor) mediated activation of the locus coeruleus noradrenergic neurons projecting to the paraventricular nucleus in rats.

01 Nov 2001·European journal of pharmacologyQ3 · MEDICINE

Effects of CP-154,526 on responding during extinction from cocaine self-administration in rats

Q3 · MEDICINE

Article

Author: Nick E Goeders ; Olga Gurkovskaya

Conditioned cues associated with cocaine induce craving and relapse. Although the role of corticotropin releasing hormone (CRH) in stress- and cocaine-induced relapse has been reported, its involvement in cue-induced behavior has not been established. Using responding during extinction as a model of cue-induced craving, we tested the effects of a selective CRH1 receptor antagonist, CP-154,526 (butyl-ethyl-[2,5-dimethyl-7-(2,4,6-trimethyl-phenyl)-7H-pyrrolo[2,3-d]pyrimidin-4-yl]-amine). Rats were trained to respond on a multiple schedule of cocaine self-administration and food reinforcement. On extinction test days, saline was substituted for cocaine. Pretreatment with CP-154,526 (20 mg/kg, i.p.) decreased responding on the cocaine-associated lever during extinction, suggesting an involvement of CRH1 receptors in cue-induced craving.

News (Medical) associated with ERAS-801

17 May 2024

·www.fiercebiotech.com

Erasca lays off 18% while swapping out KRAS program for fresh anti-tumor options

Most of the affected roles at Erasca are located in drug discovery functions or deprioritized programs, the company said. Erasca is spending a combined $22.5 million upfront to import fresh preclinical KRAS and molecular glue assets while clearing space in its own pipeline and laying off 18% of its employees in the process. The San Diego-based biotech, which focuses on treatments for cancers driven by the RAS/MAPK pathway, is paying Medshine Discovery $10 million upfront for the worldwide rights to the KRAS inhibitor ERAS-4001. Erasca described the candidate as having “potential to provide an improved therapeutic window relative to RAS inhibitors and prevent KRAS wildtype-mediated resistance relative to mutant-selective approaches.” Medshine will be in line for up to $160 million in milestone payments as well as a low single-digit percentage of the royalties should the drug make it to market. To make room for ERAS-4001—and working on the assumption that Medshine will also be providing some ERAS-4 molecules as backup compounds—Erasca will call time on its internal pan-KRAS program. Erasca had already amended this program a year ago, when it blamed the “increasingly competitive landscape” for its decision to shelve a KRAS G12C inhibitor despite believing that the candidate was potentially differentiated. It's not the only licensing deal Erasca announced yesterday evening. The company is also handing over $12.5 million to Joyo Pharmatech for the ex-China rights to a pan-RAS molecular glue called ERAS-0015. The candidate, which has now entered human trials, has demonstrated “5- to 10-fold greater in vitro and in vivo potency and favorable absorption, distribution, metabolism, and excretion properties and pharmacokinetic properties in multiple animal species,” Erasca explained in the release. As part of the licensing agreement, China’s Joyo will also be in line for up to $176.5 million in milestone payments. “We’re thrilled to add ERAS-0015 and ERAS-4001 to our pipeline,” Erasca CEO Jonathan Lim, M.D., said in the release. “Over the long term, we have a unique opportunity to combine these two best-in-class molecules with distinct and complementary RAS inhibitory mechanisms to ‘clamp’ RAS and shut down MAPK signaling for the benefit of patients with these common RAS mutations.” In addition to its KRAS work, Erasca will be deprioritizing two other programs to ensure it has space for both ERAS-4001 and ERAS-0015. One of these is ERAS-007, an ERK inhibitor that was in a phase 1b trial in combination with Braftovi and Erbitux in EC-naïve patients with BRAF-mutant colorectal cancer. Clinical efficacy data to date “do not support continued evaluation,” the biotech explained. The final amendment to its R&D strategy affects ERAS-801, a central nervous system-penetrant EGFR inhibitor being evaluated for recurrent glioblastoma. The biotech said that “due to the desire to focus internal resources” on its pan-RAF inhibitor naporafenib—which is due to enter a phase 3 melanoma trial in the coming weeks—as well as its broader RAS-targeting franchise, “Erasca is exploring further advancement of ERAS-801 via select investigator-sponsored trial(s).” These pipeline changes will be accompanied by a workforce reduction that will see 18% of staff heading for the exits, with most of the affected roles located in drug discovery functions or the deprioritized programs. “Erasca is deeply committed to easing this transition for its impacted colleagues and will offer comprehensive severance packages and career transition services,” the biotech added in the release. “With the in-licensing of these RAS-targeting programs, we have made the difficult but necessary decision to deprioritize or externalize resourcing of our pipeline (ERAS-007, ERAS-801, and ERAS-4),” Lim explained. “This change has unfortunately impacted certain team members. We believe that further focusing our resources will allow us to advance the programs with the highest probability of success and largest potential for patient impact.”

Phase 1License out/in

17 May 2024

·endpts.com

Erasca revamps pipeline, laying off staff as it licenses cancer drugs from China and nabs $160M

Erasca is looking for a refresh as it drops several early-stage cancer assets, picks up new ones from China and raises cash to help push its lead candidate to the finish line. The San Diego biotech said late Thursday that it is deprioritizing its ERK 1/2 inhibitor ERAS-007 and pan-KRAS candidate ERAS-4. As for the EFGR inhibitor ERAS-801, patient enrolment will be paused according to Mizuho analysts, citing a conversation with Erasca execs, but Erasca said the drug will be further explored in investigator-led trials. You’ll get access to free articles each month, plus you can customize what newsletters get delivered to your inbox each week, including breaking news.

17 May 2024

·firstwordpharma.com

Erasca spring clean leaves no room for internal assets

Erasca is undertaking some housekeeping, with a pipeline refresh that brings in two external preclinical programmes and deprioritises a number of existing assets, whilst also trimming its workforce by 18%. In addition the company priced a $160-million equity offering.“We believe that further focusing our resources will allow us to advance the programmes with the highest probability of success and largest potential for patient impact,” remarked CEO Jonathan Lim.While analysts were broadly positive on the pipeline additions, those at Mizhuo Securities said they have “come away a bit mixed on the totality of the…surprise updates.” Meanwhile, Morgan Stanley analysts noted that since going public in 2021, when it raised $345 million to fund its RAS/MAPK portfolio, Erasca’s “entire pipeline has…been replaced by externally-sourced assets.” Joyo, Medshine drugsErasca in-licensed the pan-RAS molecular glue ERAS-0015 from Joyo Pharmatech for an upfront cash payment of $12.5 million, with the latter eligible for further milestones of up to $176.5 million plus a low- to mid-single digit percentage sales royalty. Erasca initially has rights in all countries excluding China, Hong Kong and Macau, although this can be converted to a global licence for a one-time payment.It also in-licensed the pan-KRAS inhibitor ERAS-4001 from Medshine Discovery for an upfront cash payment of $10 million, with the latter eligible for up to $160 million in additional milestones, as well as a low-single digit percentage sales royalties. “Based on the compelling preclinical data generated to date, we believe both molecules have the potential to demonstrate best-in-class profiles within their respective categories of RAS inhibition,” Lim noted.To make room for the new assets, Erasca plans to discontinue its internal pan-KRAS programme, dubbed ERAS-4, while also stopping work on the ERK inhibitor ERAS-007. According to the company, data from the HERKULES-3 trial – investigating ERAS-007 in combination with Erbitux (cetuximab) and Braftovi (encorafenib) in certain patients with BRAF-mutated colorectal cancer – “do not support continued evaluation.”Erasca is also pulling back on its CNS-penetrant EGFR inhibitor ERAS-801 in recurrent glioblastoma, although it will explore options to advance the programme via investigator-sponsored trials. As a result of the reprioritisation, the company is cutting employees across drug discovery functions.ASCO Daily Digest – your go-to-source for the key developments emerging from this year's American Society of Clinical Oncology (ASCO) annual meeting. Exclusively for PLUS subscribers – sign up here!

License out/inASCO

100 Deals associated with ERAS-801

R&D Status

10 top R&D records.

to view more data

Indication	Highest Phase	Country/Location	Organization	Date
Glioblastoma Multiforme	Phase 1	US	Erasca, Inc.	25 Feb 2022
Recurrent Glioblastoma	Phase 1	US	Erasca, Inc.	25 Feb 2022
EGFR mutation Glioblastoma	Preclinical	US	Erasca, Inc.	-

Clinical Result

Indication

Phase

Evaluation

View All Results

Study	Phase	Population	Analyzed Enrollment	Group	Results	Evaluation	Publication Date


NCT05222802 (THUNDERBBOLT-1 , GlobeNewswire) Manual	Phase 1	Recurrent Glioblastoma	33	ERAS-801	dqmsvamxll(pcwidgyfpu) = MTD identified as 240 mg once a day (QD) and MTD-1 identified as 160 mg QD for ERAS-801 hlqjlcipsh (imdizojhxv ) View more	Positive	28 Nov 2023

Translational Medicine

Boost your research with our translational medicine data.

view full example data

Deal

Boost your decision using our deal data.

view full example data

Core Patent

Boost your research with our Core Patent data.

view full example data

Clinical Trial

Identify the latest clinical trials across global registries.

view full example data

Approval

Accelerate your research with the latest regulatory approval information.

view full example data

Regulation

Understand key drug designations in just a few clicks with Synapse.

view full example data

Chat with Hiro

Get started for free today!

Accelerate Strategic R&D decision making with Synapse, PatSnap’s AI-powered Connected Innovation Intelligence Platform Built for Life Sciences Professionals.

Start your data trial now!

Synapse data is also accessible to external entities via APIs or data packages. Empower better decisions with the latest in pharmaceutical intelligence.

Bio

Bio Sequences Search & Analysis

Chemical

Chemical Structures Search & Analysis

ERAS-801

Overview

Basic Info

Related

R&D Status

Clinical Result

Translational Medicine

Deal

Core Patent

Clinical Trial

Approval

Regulation